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Do intercontraction intervals predict when a woman at term should seek evaluation of labor?
NO; HOWEVER, A REDUCTION IN the intercontraction interval is associated with active labor (strength of recommendation [SOR]: B, cohort study).
Most primigravidas who have had regular contractions for 2 hours and multigravidas who have had regular contractions for 1 hour haven’t transitioned into the active phase of labor (SOR: B, cohort study).
Evidence summary
Multiple cohort studies demonstrate that the expected events of normal labor form a bell-shaped curve. The range of labor experiences makes predicting when a particular woman will enter active labor difficult.
When does latent labor become active labor?
The first stage of labor includes latent and active phases. The latent phase is defined as the period between onset of labor and cervical dilatation of 3 to 4 cm or the time between onset of regular contractions and escalation in the rate of cervical dilation. Regular contractions must be intense, last 60 seconds, and occur in a predictable pattern. Escalating cervical dilation is marked by a change in the cervical examination over a short period of time (usually 2 hours).1
The World Health Organization defines active labor as cervical dilation between 4 and 9 cm, with dilation usually occurring at 1 cm per hour or faster and accompanied by the beginning of fetal descent.2
Latent labor was initially described in a large prospective cohort of 10,293 term gravidas (including 4175 nulliparas and 5599 multiparas) followed from presentation to delivery.1 Cervical dilation was assessed by examination every 30 to 120 minutes, almost always performed by the same examiner throughout labor. In primigravidas, latent labor averaged 6.4 hours, with 95% of women completing the latent phase in 20.6 hours. In multigravidas, the mean duration of latent labor was 4.8 hours, with 95% of women transitioning to active labor in 13.6 hours.
Shorter intercontraction interval linked to active labor
A recently published cohort study of women presenting to labor and delivery found that a relative decrease in the intercontraction interval was associated with a diagnosis of labor (odds ratio=1.42; 95% confidence interval, 1.06-1.90). The study failed to define either active labor or decrease in the intercontraction interval.3
Earlier admission leads to more interventions and poorer outcomes
Many studies have suggested that admitting women to the hospital during the latent phase of labor is associated with more interventions and poorer outcomes. Two large retrospective cohort studies (N=2697 and 3220) found increased rates of cesarean section in women admitted during the latent phase.4,5 They also reported increased use of oxytocin, epidural analgesia, intrauterine pressure catheters, and fetal scalp electrodes, and increased rates of chorioamnionitis, postpartum infection, and neonatal intubation.4,5 See the TABLE for a summary of the effects of latent-phase admission.
TABLE
Consequences of hospital admission during latent vs active labor
| Nulliparous | Parous | |||||
|---|---|---|---|---|---|---|
| Consequence | Latent (%) | Active (%) | NNH | Latent (%) | Active (%) | NNH |
| Oxytocin4 | 43 | 27 | 6* | 20 | 9 | 9* |
| Epidural4 | 82 | 61 | 5* | 58 | 40 | 6* |
| Assisted vaginal delivery4 | 27 | 25 | 50 | 8 | 6 | 50 |
| Cesarean4 | 10 | 4 | 17* | 8 | 6 | 50 |
| Cesarean5 † | 14 | 7 | 14* | 3 | 1 | 50* |
| pH <7.14 | 4 | 3 | 100 | 3 | 2 | 100 |
| Apgar <74 | 4 | 2 | 50 | 3 | 2 | 100 |
| NNH, number needed to harm. | ||||||
| *Indicates relationship significant at the level <.05. | ||||||
| †Study by Bailit5 also showed significant associations for oxytocin, scalp pH, intrauterine pressure catheter, fetal scalp electrode, epidural, neonatal intubation, amnionitis, and postpartum infection. Raw data are unavailable for abstraction | ||||||
Labor assessment program reduced time in the labor ward
Labor assessment programs attempt to delay admission during early active labor. One randomized clinical trial (N=209) among low-risk women with reassuring maternal and fetal assessments in early labor divided the women into 2 groups when they presented for labor and delivery. One group received advice, encouragement, and support along with instructions to walk or return home and come back when labor became more active (defined as regular, painful contractions and dilation of at least 3 cm). The other group was admitted directly to the labor and delivery ward. The study found that early labor assessment decreased use of analgesics and oxytocin and reduced time spent in the labor ward.6
Recommendations
The American College of Obstetricians and Gynecologists (ACOG) acknowledges in patient education literature that distinguishing true from false labor is difficult. ACOG lists characteristics of each and recommend that a woman monitor the frequency of contractions for an hour and call the doctor’s office or hospital if she thinks she’s in labor.7
Similarly, a patient handout from the American College of Nurse-Midwives recommends calling the health care provider if contractions are ≤5 minutes apart for more than 1 hour, several contractions are so painful that the woman cannot walk or talk, or her water breaks.8
A standard textbook describes normal uterine contractions during active labor as occurring every 2 to 5 minutes, and as often as every 2 to 3 minutes.9
1. Friedman EA, Kroll BH. Computer analysis of labor progression. 3. Pattern variations by parity. J Reprod Med. 1971;6:179-183.
2. World Health Organization. Managing Complications in Pregnancy and Childbirth: A Guide for Midwives and Doctors. Geneva, Switzerland: Department of Reproductive Health and Research, Family and Community Health, World Health Organization; 2003.
3. Ragusa A, Monsur M, Zanini A, et al. Diagnosis of labor: a prospective study. Med Gen Med. 2005;7:61.-
4. Holmes P, Oppenheimer LW, Wen SW. The relationship between cervical dilatation at initial presentation in labour and subsequent intervention. BJOG. 2001;108:1120-1124.
5. Bailit JL, Dierker LR, Blanchard MH, et al. Outcomes of women presenting in active versus latent phase of spontaneous labor. Obstet Gynecol. 2005;105:77-79.
6. McNiven PS, Williams JI, Hodnett E, et al. An early labor assessment program: a randomized, controlled trial. Birth. 1998;25:5-10.
7. How to Tell When Labor Begins. Washington, DC: American College of Obstetricians and Gynecologists; 1999. Available at: www.acog.org/publications/patient_education/bp004.cfm. Accessed November 8, 2008.
8. Am I in Labor? Silver Spring, Md: American College of Nurse-Midwives; 2003. Available at: www.midwife.org/siteFiles/news/sharewithwomen48_4.pdf. Accessed November 7, 2008.
9. Kilpatrick S, Garrison E. Normal labor and delivery. In: Gabbe SG, Niebyl JR, Simpson JL, eds. Obstetrics: Normal and Problem Pregnancies. 5th ed. Philadelphia: Churchill Livingstone/Elsevier; 2007:303–317.
NO; HOWEVER, A REDUCTION IN the intercontraction interval is associated with active labor (strength of recommendation [SOR]: B, cohort study).
Most primigravidas who have had regular contractions for 2 hours and multigravidas who have had regular contractions for 1 hour haven’t transitioned into the active phase of labor (SOR: B, cohort study).
Evidence summary
Multiple cohort studies demonstrate that the expected events of normal labor form a bell-shaped curve. The range of labor experiences makes predicting when a particular woman will enter active labor difficult.
When does latent labor become active labor?
The first stage of labor includes latent and active phases. The latent phase is defined as the period between onset of labor and cervical dilatation of 3 to 4 cm or the time between onset of regular contractions and escalation in the rate of cervical dilation. Regular contractions must be intense, last 60 seconds, and occur in a predictable pattern. Escalating cervical dilation is marked by a change in the cervical examination over a short period of time (usually 2 hours).1
The World Health Organization defines active labor as cervical dilation between 4 and 9 cm, with dilation usually occurring at 1 cm per hour or faster and accompanied by the beginning of fetal descent.2
Latent labor was initially described in a large prospective cohort of 10,293 term gravidas (including 4175 nulliparas and 5599 multiparas) followed from presentation to delivery.1 Cervical dilation was assessed by examination every 30 to 120 minutes, almost always performed by the same examiner throughout labor. In primigravidas, latent labor averaged 6.4 hours, with 95% of women completing the latent phase in 20.6 hours. In multigravidas, the mean duration of latent labor was 4.8 hours, with 95% of women transitioning to active labor in 13.6 hours.
Shorter intercontraction interval linked to active labor
A recently published cohort study of women presenting to labor and delivery found that a relative decrease in the intercontraction interval was associated with a diagnosis of labor (odds ratio=1.42; 95% confidence interval, 1.06-1.90). The study failed to define either active labor or decrease in the intercontraction interval.3
Earlier admission leads to more interventions and poorer outcomes
Many studies have suggested that admitting women to the hospital during the latent phase of labor is associated with more interventions and poorer outcomes. Two large retrospective cohort studies (N=2697 and 3220) found increased rates of cesarean section in women admitted during the latent phase.4,5 They also reported increased use of oxytocin, epidural analgesia, intrauterine pressure catheters, and fetal scalp electrodes, and increased rates of chorioamnionitis, postpartum infection, and neonatal intubation.4,5 See the TABLE for a summary of the effects of latent-phase admission.
TABLE
Consequences of hospital admission during latent vs active labor
| Nulliparous | Parous | |||||
|---|---|---|---|---|---|---|
| Consequence | Latent (%) | Active (%) | NNH | Latent (%) | Active (%) | NNH |
| Oxytocin4 | 43 | 27 | 6* | 20 | 9 | 9* |
| Epidural4 | 82 | 61 | 5* | 58 | 40 | 6* |
| Assisted vaginal delivery4 | 27 | 25 | 50 | 8 | 6 | 50 |
| Cesarean4 | 10 | 4 | 17* | 8 | 6 | 50 |
| Cesarean5 † | 14 | 7 | 14* | 3 | 1 | 50* |
| pH <7.14 | 4 | 3 | 100 | 3 | 2 | 100 |
| Apgar <74 | 4 | 2 | 50 | 3 | 2 | 100 |
| NNH, number needed to harm. | ||||||
| *Indicates relationship significant at the level <.05. | ||||||
| †Study by Bailit5 also showed significant associations for oxytocin, scalp pH, intrauterine pressure catheter, fetal scalp electrode, epidural, neonatal intubation, amnionitis, and postpartum infection. Raw data are unavailable for abstraction | ||||||
Labor assessment program reduced time in the labor ward
Labor assessment programs attempt to delay admission during early active labor. One randomized clinical trial (N=209) among low-risk women with reassuring maternal and fetal assessments in early labor divided the women into 2 groups when they presented for labor and delivery. One group received advice, encouragement, and support along with instructions to walk or return home and come back when labor became more active (defined as regular, painful contractions and dilation of at least 3 cm). The other group was admitted directly to the labor and delivery ward. The study found that early labor assessment decreased use of analgesics and oxytocin and reduced time spent in the labor ward.6
Recommendations
The American College of Obstetricians and Gynecologists (ACOG) acknowledges in patient education literature that distinguishing true from false labor is difficult. ACOG lists characteristics of each and recommend that a woman monitor the frequency of contractions for an hour and call the doctor’s office or hospital if she thinks she’s in labor.7
Similarly, a patient handout from the American College of Nurse-Midwives recommends calling the health care provider if contractions are ≤5 minutes apart for more than 1 hour, several contractions are so painful that the woman cannot walk or talk, or her water breaks.8
A standard textbook describes normal uterine contractions during active labor as occurring every 2 to 5 minutes, and as often as every 2 to 3 minutes.9
NO; HOWEVER, A REDUCTION IN the intercontraction interval is associated with active labor (strength of recommendation [SOR]: B, cohort study).
Most primigravidas who have had regular contractions for 2 hours and multigravidas who have had regular contractions for 1 hour haven’t transitioned into the active phase of labor (SOR: B, cohort study).
Evidence summary
Multiple cohort studies demonstrate that the expected events of normal labor form a bell-shaped curve. The range of labor experiences makes predicting when a particular woman will enter active labor difficult.
When does latent labor become active labor?
The first stage of labor includes latent and active phases. The latent phase is defined as the period between onset of labor and cervical dilatation of 3 to 4 cm or the time between onset of regular contractions and escalation in the rate of cervical dilation. Regular contractions must be intense, last 60 seconds, and occur in a predictable pattern. Escalating cervical dilation is marked by a change in the cervical examination over a short period of time (usually 2 hours).1
The World Health Organization defines active labor as cervical dilation between 4 and 9 cm, with dilation usually occurring at 1 cm per hour or faster and accompanied by the beginning of fetal descent.2
Latent labor was initially described in a large prospective cohort of 10,293 term gravidas (including 4175 nulliparas and 5599 multiparas) followed from presentation to delivery.1 Cervical dilation was assessed by examination every 30 to 120 minutes, almost always performed by the same examiner throughout labor. In primigravidas, latent labor averaged 6.4 hours, with 95% of women completing the latent phase in 20.6 hours. In multigravidas, the mean duration of latent labor was 4.8 hours, with 95% of women transitioning to active labor in 13.6 hours.
Shorter intercontraction interval linked to active labor
A recently published cohort study of women presenting to labor and delivery found that a relative decrease in the intercontraction interval was associated with a diagnosis of labor (odds ratio=1.42; 95% confidence interval, 1.06-1.90). The study failed to define either active labor or decrease in the intercontraction interval.3
Earlier admission leads to more interventions and poorer outcomes
Many studies have suggested that admitting women to the hospital during the latent phase of labor is associated with more interventions and poorer outcomes. Two large retrospective cohort studies (N=2697 and 3220) found increased rates of cesarean section in women admitted during the latent phase.4,5 They also reported increased use of oxytocin, epidural analgesia, intrauterine pressure catheters, and fetal scalp electrodes, and increased rates of chorioamnionitis, postpartum infection, and neonatal intubation.4,5 See the TABLE for a summary of the effects of latent-phase admission.
TABLE
Consequences of hospital admission during latent vs active labor
| Nulliparous | Parous | |||||
|---|---|---|---|---|---|---|
| Consequence | Latent (%) | Active (%) | NNH | Latent (%) | Active (%) | NNH |
| Oxytocin4 | 43 | 27 | 6* | 20 | 9 | 9* |
| Epidural4 | 82 | 61 | 5* | 58 | 40 | 6* |
| Assisted vaginal delivery4 | 27 | 25 | 50 | 8 | 6 | 50 |
| Cesarean4 | 10 | 4 | 17* | 8 | 6 | 50 |
| Cesarean5 † | 14 | 7 | 14* | 3 | 1 | 50* |
| pH <7.14 | 4 | 3 | 100 | 3 | 2 | 100 |
| Apgar <74 | 4 | 2 | 50 | 3 | 2 | 100 |
| NNH, number needed to harm. | ||||||
| *Indicates relationship significant at the level <.05. | ||||||
| †Study by Bailit5 also showed significant associations for oxytocin, scalp pH, intrauterine pressure catheter, fetal scalp electrode, epidural, neonatal intubation, amnionitis, and postpartum infection. Raw data are unavailable for abstraction | ||||||
Labor assessment program reduced time in the labor ward
Labor assessment programs attempt to delay admission during early active labor. One randomized clinical trial (N=209) among low-risk women with reassuring maternal and fetal assessments in early labor divided the women into 2 groups when they presented for labor and delivery. One group received advice, encouragement, and support along with instructions to walk or return home and come back when labor became more active (defined as regular, painful contractions and dilation of at least 3 cm). The other group was admitted directly to the labor and delivery ward. The study found that early labor assessment decreased use of analgesics and oxytocin and reduced time spent in the labor ward.6
Recommendations
The American College of Obstetricians and Gynecologists (ACOG) acknowledges in patient education literature that distinguishing true from false labor is difficult. ACOG lists characteristics of each and recommend that a woman monitor the frequency of contractions for an hour and call the doctor’s office or hospital if she thinks she’s in labor.7
Similarly, a patient handout from the American College of Nurse-Midwives recommends calling the health care provider if contractions are ≤5 minutes apart for more than 1 hour, several contractions are so painful that the woman cannot walk or talk, or her water breaks.8
A standard textbook describes normal uterine contractions during active labor as occurring every 2 to 5 minutes, and as often as every 2 to 3 minutes.9
1. Friedman EA, Kroll BH. Computer analysis of labor progression. 3. Pattern variations by parity. J Reprod Med. 1971;6:179-183.
2. World Health Organization. Managing Complications in Pregnancy and Childbirth: A Guide for Midwives and Doctors. Geneva, Switzerland: Department of Reproductive Health and Research, Family and Community Health, World Health Organization; 2003.
3. Ragusa A, Monsur M, Zanini A, et al. Diagnosis of labor: a prospective study. Med Gen Med. 2005;7:61.-
4. Holmes P, Oppenheimer LW, Wen SW. The relationship between cervical dilatation at initial presentation in labour and subsequent intervention. BJOG. 2001;108:1120-1124.
5. Bailit JL, Dierker LR, Blanchard MH, et al. Outcomes of women presenting in active versus latent phase of spontaneous labor. Obstet Gynecol. 2005;105:77-79.
6. McNiven PS, Williams JI, Hodnett E, et al. An early labor assessment program: a randomized, controlled trial. Birth. 1998;25:5-10.
7. How to Tell When Labor Begins. Washington, DC: American College of Obstetricians and Gynecologists; 1999. Available at: www.acog.org/publications/patient_education/bp004.cfm. Accessed November 8, 2008.
8. Am I in Labor? Silver Spring, Md: American College of Nurse-Midwives; 2003. Available at: www.midwife.org/siteFiles/news/sharewithwomen48_4.pdf. Accessed November 7, 2008.
9. Kilpatrick S, Garrison E. Normal labor and delivery. In: Gabbe SG, Niebyl JR, Simpson JL, eds. Obstetrics: Normal and Problem Pregnancies. 5th ed. Philadelphia: Churchill Livingstone/Elsevier; 2007:303–317.
1. Friedman EA, Kroll BH. Computer analysis of labor progression. 3. Pattern variations by parity. J Reprod Med. 1971;6:179-183.
2. World Health Organization. Managing Complications in Pregnancy and Childbirth: A Guide for Midwives and Doctors. Geneva, Switzerland: Department of Reproductive Health and Research, Family and Community Health, World Health Organization; 2003.
3. Ragusa A, Monsur M, Zanini A, et al. Diagnosis of labor: a prospective study. Med Gen Med. 2005;7:61.-
4. Holmes P, Oppenheimer LW, Wen SW. The relationship between cervical dilatation at initial presentation in labour and subsequent intervention. BJOG. 2001;108:1120-1124.
5. Bailit JL, Dierker LR, Blanchard MH, et al. Outcomes of women presenting in active versus latent phase of spontaneous labor. Obstet Gynecol. 2005;105:77-79.
6. McNiven PS, Williams JI, Hodnett E, et al. An early labor assessment program: a randomized, controlled trial. Birth. 1998;25:5-10.
7. How to Tell When Labor Begins. Washington, DC: American College of Obstetricians and Gynecologists; 1999. Available at: www.acog.org/publications/patient_education/bp004.cfm. Accessed November 8, 2008.
8. Am I in Labor? Silver Spring, Md: American College of Nurse-Midwives; 2003. Available at: www.midwife.org/siteFiles/news/sharewithwomen48_4.pdf. Accessed November 7, 2008.
9. Kilpatrick S, Garrison E. Normal labor and delivery. In: Gabbe SG, Niebyl JR, Simpson JL, eds. Obstetrics: Normal and Problem Pregnancies. 5th ed. Philadelphia: Churchill Livingstone/Elsevier; 2007:303–317.
Evidence-based answers from the Family Physicians Inquiries Network
What is the best way to evaluate secondary infertility?
The work-up for secondary infertility—the inability to conceive after 1 year of regular unprotected intercourse for a couple who have previously had a child1—should include a history and physical exam for both patients, plus evaluation of ovulation, semen analysis, and imaging of the uterus and fallopian tubes (strength of recommendation [SOR]: B, based on cohort studies).
Check the male partner for varicoceles: they are the leading cause of male secondary infertility. For the female partner, a hysterosalpingogram is an effective first test in the initial evaluation of the uterine cavity and tubal patency (SOR: B, based on cohort studies). Laparoscopy is indicated where there is evidence or strong suspicion of endometriosis, adhesions, or significant tubal disease (SOR: B, cohort studies). Routine postcoital testing is unnecessary (SOR: A, randomized controlled trial and cohort studies).
Simple steps may reveal treatable causes
Peter Danis, MD
St. John’s Mercy Medical Center, St. Louis, MO
Many times, family physicians are too quick to refer couples with infertility problems. Conception and early pregnancy require 6 basic elements of good quality: mucus, egg, sperm, timing, anatomy, and hormonal support. Couples that learn how to chart their cycles can provide physicians with valuable information such as bleeding pattern, quality of mucus, and luteal phase length. This can help the couple to focus on their time of maximal fertility.
A good working relationship with an obstetrician and urologist is important for more complicated workups and treatments. A couple with secondary infertility has shown that things were once working right; it’s up to the physician to determine what may have changed since that success.
Evidence summary
The prevalence of infertility in the US is approximately 15% to 17%.2,3 Secondary infertility may comprise 80% of these cases, though reports vary.2 Begin the evaluation of secondary infertility with a thorough history and physical, as outlined in the TABLE), followed by semen analysis and evaluation of ovulation.1,3,4
TABLE
Secondary infertility? Here’s what to cover in the history and exam
| HISTORY | |
| FEMALE | MALE |
| Prior pregnancies and complications; fertility in other relationships | Sexual dysfunction or impotence |
| Menstrual history: Age at menarche, cycle length, regularity, characteristics, dysmenorrhea | Testicular surgery, history of mumps, prior infections |
| Gyn history: Infections, prior surgeries, endometriosis, cervical dysplasia, DES exposure, prior contraceptive use | BOTH |
| Symptoms of thyroid disease, pelvic pain, abdominal pain, galactorrhea, hirsutism, and dyspareunia | Duration of infertility |
| Exercise and dietary history, presence of eating disorder | Previous evaluations and results |
| Current medications | Frequency of intercourse and use of lubricants |
| Occupational history | History of chemotherapy, radiation, and other environmental and occupational exposures like alcohol and drugs |
| Breast exam/secretions | Preconception counseling |
| PHYSICAL | |
| FEMALE | MALE |
| Genitourinary exam: Vaginal/cervical abnormalities or discharge, uterine size and shape, adnexal mass or tenderness | Genitourinary exam: testicular size and consistency, location of urethral meatus, presence of varicocele |
| Weight: body-mass index >29 or <19 | Weight/body habitus |
| Thyroid enlargement, nodules, or tenderness | Hair distribution |
| Presence of hirsutism | Breast development |
| Digital rectal exam | |
Evaluate the male partner for varicoceles
The semen sample can be taken after the patient abstains from ejaculation for 2 to 6 days. Analyze the sample for volume, pH, sperm concentration, motility, and total number. If the sample is abnormal, repeat the analysis within 3 months.1,5
Evaluate the male for varicoceles. A retrospective chart review compared 285 men with secondary infertility with 285 men with primary infertility. Varicoceles were the cause of secondary infertility in 177 (69%) of men with secondary infertility compared with 128 (50%) of men with primary infertility (P<.0001).6
Order tests to evaluate ovulation
To evaluate ovulation, look at menstrual history, serum progesterone, and urine luteinizing hormone (LH).1,3,4 If the woman has signs of androgenic dysfunction, draw tests for LH, thyroid-stimulating hormone, follicle-stimulating hormone (FSH), testosterone, prolactin, and 17-hydroxyprogesterone. A woman with irregular menses should have her LH and FSH checked.1
A hysterosalpingogram is an effective first test in the evaluation of the uterine cavity and tubal patency.1,7,8 If the woman has comorbidities—such as a history of pelvic inflammatory disease, previous ectopic pregnancy, or endometriosis—then laparoscopy should be the initial test.1,3 One study demonstrated increased diagnostic yield with a combined approach of hysteroscopy and laparoscopy, in communities where the risk of pelvic infection was great.9
Routine postcoital testing is unnecessary.10 A randomized controlled trial compared 227 couples who received the postcoital test with 217 couples who did not. Routine use of the postcoital test led to more tests and more treatments but had no significant effect on the pregnancy rate.
Recommendations from others
According to the Royal College of Obstetricians and Gynecologists:1
- The use of basal body temperature charts to confirm ovulation does not reliably predict ovulation and is not recommended.
- The routine measurement of thyroid function should not be offered.
- Women should not be offered an endometrial biopsy to evaluate the luteal phase because there is no evidence that medical treatment of luteal phase defect improves pregnancy rates.
- Women who are not known to have comorbidities (such as pelvic inflammatory disease, previous ectopic pregnancy, or endometriosis) should be offered hysterosalpingography to screen for tubal occlusion.
- Women who are thought to have comorbidities should be offered laparoscopy and dye so that tubal and other pelvic pathology can be assessed at the same time.
1. National Collaborating Centre for Women’s and Children’s Health. Fertility: Assessment and Treatment for People with Fertility Problems. London: RCOG Press; 2004:216.
2. Wyshak G. Infertility in American college alumnae. Intl J Gynaecol Obstet 2001;73:237-242.
3. Practice Committee of the American Society for Reproductive Medicine. Optimal evaluation of the infertile female. Fertil Steril 2004;82(Suppl 1):S169-S172.
4. Brigham and Women’s Hospital. Infertility: A Guide to Evaluation, Treatment, and Counseling. Boston, Mass: Brigham and Women’s Hospital; 2003:11.
5. Report on optimal evaluation of the infertile male. Baltimore, Md: American Urological Association; 2001:14.
6. Witt MA, Lipshultz LI. Varicocele: A progressive or static lesion? Urology 1993;42:541-543.
7. Valenzano M, Mistrangelo E, Lijoi D, et al. Transvaginal sonohysterographic evaluation of uterine malformations. Eur J Obstet Gynecol Reprod Biol 2006;124:246-249.
8. Roma Dalfó A, Ubeda B, Ubeda A, et al. Diagnostic value of hysterosalpingography in the detection of intrauterine abnormalities: a comparison with hysteroscopy. AJR Am J Roentgenol 2004;183:1405-1409.
9. Shokeir T, Shalan H, El-Shafei M. Combined diagnostic approach of laparoscopy and hysteroscopy in the evaluation of female infertility: Results of 612 patients. J Obstet Gynaecol Res 2004;30:9-14.
10. Oei SG, Helmerhorst F, Bloemenkamp K, Hollants F, Meerpoel D, Keirse M. Effectiveness of the postcoital test: randomized controlled trial. BMJ 1998;317:502-505.
The work-up for secondary infertility—the inability to conceive after 1 year of regular unprotected intercourse for a couple who have previously had a child1—should include a history and physical exam for both patients, plus evaluation of ovulation, semen analysis, and imaging of the uterus and fallopian tubes (strength of recommendation [SOR]: B, based on cohort studies).
Check the male partner for varicoceles: they are the leading cause of male secondary infertility. For the female partner, a hysterosalpingogram is an effective first test in the initial evaluation of the uterine cavity and tubal patency (SOR: B, based on cohort studies). Laparoscopy is indicated where there is evidence or strong suspicion of endometriosis, adhesions, or significant tubal disease (SOR: B, cohort studies). Routine postcoital testing is unnecessary (SOR: A, randomized controlled trial and cohort studies).
Simple steps may reveal treatable causes
Peter Danis, MD
St. John’s Mercy Medical Center, St. Louis, MO
Many times, family physicians are too quick to refer couples with infertility problems. Conception and early pregnancy require 6 basic elements of good quality: mucus, egg, sperm, timing, anatomy, and hormonal support. Couples that learn how to chart their cycles can provide physicians with valuable information such as bleeding pattern, quality of mucus, and luteal phase length. This can help the couple to focus on their time of maximal fertility.
A good working relationship with an obstetrician and urologist is important for more complicated workups and treatments. A couple with secondary infertility has shown that things were once working right; it’s up to the physician to determine what may have changed since that success.
Evidence summary
The prevalence of infertility in the US is approximately 15% to 17%.2,3 Secondary infertility may comprise 80% of these cases, though reports vary.2 Begin the evaluation of secondary infertility with a thorough history and physical, as outlined in the TABLE), followed by semen analysis and evaluation of ovulation.1,3,4
TABLE
Secondary infertility? Here’s what to cover in the history and exam
| HISTORY | |
| FEMALE | MALE |
| Prior pregnancies and complications; fertility in other relationships | Sexual dysfunction or impotence |
| Menstrual history: Age at menarche, cycle length, regularity, characteristics, dysmenorrhea | Testicular surgery, history of mumps, prior infections |
| Gyn history: Infections, prior surgeries, endometriosis, cervical dysplasia, DES exposure, prior contraceptive use | BOTH |
| Symptoms of thyroid disease, pelvic pain, abdominal pain, galactorrhea, hirsutism, and dyspareunia | Duration of infertility |
| Exercise and dietary history, presence of eating disorder | Previous evaluations and results |
| Current medications | Frequency of intercourse and use of lubricants |
| Occupational history | History of chemotherapy, radiation, and other environmental and occupational exposures like alcohol and drugs |
| Breast exam/secretions | Preconception counseling |
| PHYSICAL | |
| FEMALE | MALE |
| Genitourinary exam: Vaginal/cervical abnormalities or discharge, uterine size and shape, adnexal mass or tenderness | Genitourinary exam: testicular size and consistency, location of urethral meatus, presence of varicocele |
| Weight: body-mass index >29 or <19 | Weight/body habitus |
| Thyroid enlargement, nodules, or tenderness | Hair distribution |
| Presence of hirsutism | Breast development |
| Digital rectal exam | |
Evaluate the male partner for varicoceles
The semen sample can be taken after the patient abstains from ejaculation for 2 to 6 days. Analyze the sample for volume, pH, sperm concentration, motility, and total number. If the sample is abnormal, repeat the analysis within 3 months.1,5
Evaluate the male for varicoceles. A retrospective chart review compared 285 men with secondary infertility with 285 men with primary infertility. Varicoceles were the cause of secondary infertility in 177 (69%) of men with secondary infertility compared with 128 (50%) of men with primary infertility (P<.0001).6
Order tests to evaluate ovulation
To evaluate ovulation, look at menstrual history, serum progesterone, and urine luteinizing hormone (LH).1,3,4 If the woman has signs of androgenic dysfunction, draw tests for LH, thyroid-stimulating hormone, follicle-stimulating hormone (FSH), testosterone, prolactin, and 17-hydroxyprogesterone. A woman with irregular menses should have her LH and FSH checked.1
A hysterosalpingogram is an effective first test in the evaluation of the uterine cavity and tubal patency.1,7,8 If the woman has comorbidities—such as a history of pelvic inflammatory disease, previous ectopic pregnancy, or endometriosis—then laparoscopy should be the initial test.1,3 One study demonstrated increased diagnostic yield with a combined approach of hysteroscopy and laparoscopy, in communities where the risk of pelvic infection was great.9
Routine postcoital testing is unnecessary.10 A randomized controlled trial compared 227 couples who received the postcoital test with 217 couples who did not. Routine use of the postcoital test led to more tests and more treatments but had no significant effect on the pregnancy rate.
Recommendations from others
According to the Royal College of Obstetricians and Gynecologists:1
- The use of basal body temperature charts to confirm ovulation does not reliably predict ovulation and is not recommended.
- The routine measurement of thyroid function should not be offered.
- Women should not be offered an endometrial biopsy to evaluate the luteal phase because there is no evidence that medical treatment of luteal phase defect improves pregnancy rates.
- Women who are not known to have comorbidities (such as pelvic inflammatory disease, previous ectopic pregnancy, or endometriosis) should be offered hysterosalpingography to screen for tubal occlusion.
- Women who are thought to have comorbidities should be offered laparoscopy and dye so that tubal and other pelvic pathology can be assessed at the same time.
The work-up for secondary infertility—the inability to conceive after 1 year of regular unprotected intercourse for a couple who have previously had a child1—should include a history and physical exam for both patients, plus evaluation of ovulation, semen analysis, and imaging of the uterus and fallopian tubes (strength of recommendation [SOR]: B, based on cohort studies).
Check the male partner for varicoceles: they are the leading cause of male secondary infertility. For the female partner, a hysterosalpingogram is an effective first test in the initial evaluation of the uterine cavity and tubal patency (SOR: B, based on cohort studies). Laparoscopy is indicated where there is evidence or strong suspicion of endometriosis, adhesions, or significant tubal disease (SOR: B, cohort studies). Routine postcoital testing is unnecessary (SOR: A, randomized controlled trial and cohort studies).
Simple steps may reveal treatable causes
Peter Danis, MD
St. John’s Mercy Medical Center, St. Louis, MO
Many times, family physicians are too quick to refer couples with infertility problems. Conception and early pregnancy require 6 basic elements of good quality: mucus, egg, sperm, timing, anatomy, and hormonal support. Couples that learn how to chart their cycles can provide physicians with valuable information such as bleeding pattern, quality of mucus, and luteal phase length. This can help the couple to focus on their time of maximal fertility.
A good working relationship with an obstetrician and urologist is important for more complicated workups and treatments. A couple with secondary infertility has shown that things were once working right; it’s up to the physician to determine what may have changed since that success.
Evidence summary
The prevalence of infertility in the US is approximately 15% to 17%.2,3 Secondary infertility may comprise 80% of these cases, though reports vary.2 Begin the evaluation of secondary infertility with a thorough history and physical, as outlined in the TABLE), followed by semen analysis and evaluation of ovulation.1,3,4
TABLE
Secondary infertility? Here’s what to cover in the history and exam
| HISTORY | |
| FEMALE | MALE |
| Prior pregnancies and complications; fertility in other relationships | Sexual dysfunction or impotence |
| Menstrual history: Age at menarche, cycle length, regularity, characteristics, dysmenorrhea | Testicular surgery, history of mumps, prior infections |
| Gyn history: Infections, prior surgeries, endometriosis, cervical dysplasia, DES exposure, prior contraceptive use | BOTH |
| Symptoms of thyroid disease, pelvic pain, abdominal pain, galactorrhea, hirsutism, and dyspareunia | Duration of infertility |
| Exercise and dietary history, presence of eating disorder | Previous evaluations and results |
| Current medications | Frequency of intercourse and use of lubricants |
| Occupational history | History of chemotherapy, radiation, and other environmental and occupational exposures like alcohol and drugs |
| Breast exam/secretions | Preconception counseling |
| PHYSICAL | |
| FEMALE | MALE |
| Genitourinary exam: Vaginal/cervical abnormalities or discharge, uterine size and shape, adnexal mass or tenderness | Genitourinary exam: testicular size and consistency, location of urethral meatus, presence of varicocele |
| Weight: body-mass index >29 or <19 | Weight/body habitus |
| Thyroid enlargement, nodules, or tenderness | Hair distribution |
| Presence of hirsutism | Breast development |
| Digital rectal exam | |
Evaluate the male partner for varicoceles
The semen sample can be taken after the patient abstains from ejaculation for 2 to 6 days. Analyze the sample for volume, pH, sperm concentration, motility, and total number. If the sample is abnormal, repeat the analysis within 3 months.1,5
Evaluate the male for varicoceles. A retrospective chart review compared 285 men with secondary infertility with 285 men with primary infertility. Varicoceles were the cause of secondary infertility in 177 (69%) of men with secondary infertility compared with 128 (50%) of men with primary infertility (P<.0001).6
Order tests to evaluate ovulation
To evaluate ovulation, look at menstrual history, serum progesterone, and urine luteinizing hormone (LH).1,3,4 If the woman has signs of androgenic dysfunction, draw tests for LH, thyroid-stimulating hormone, follicle-stimulating hormone (FSH), testosterone, prolactin, and 17-hydroxyprogesterone. A woman with irregular menses should have her LH and FSH checked.1
A hysterosalpingogram is an effective first test in the evaluation of the uterine cavity and tubal patency.1,7,8 If the woman has comorbidities—such as a history of pelvic inflammatory disease, previous ectopic pregnancy, or endometriosis—then laparoscopy should be the initial test.1,3 One study demonstrated increased diagnostic yield with a combined approach of hysteroscopy and laparoscopy, in communities where the risk of pelvic infection was great.9
Routine postcoital testing is unnecessary.10 A randomized controlled trial compared 227 couples who received the postcoital test with 217 couples who did not. Routine use of the postcoital test led to more tests and more treatments but had no significant effect on the pregnancy rate.
Recommendations from others
According to the Royal College of Obstetricians and Gynecologists:1
- The use of basal body temperature charts to confirm ovulation does not reliably predict ovulation and is not recommended.
- The routine measurement of thyroid function should not be offered.
- Women should not be offered an endometrial biopsy to evaluate the luteal phase because there is no evidence that medical treatment of luteal phase defect improves pregnancy rates.
- Women who are not known to have comorbidities (such as pelvic inflammatory disease, previous ectopic pregnancy, or endometriosis) should be offered hysterosalpingography to screen for tubal occlusion.
- Women who are thought to have comorbidities should be offered laparoscopy and dye so that tubal and other pelvic pathology can be assessed at the same time.
1. National Collaborating Centre for Women’s and Children’s Health. Fertility: Assessment and Treatment for People with Fertility Problems. London: RCOG Press; 2004:216.
2. Wyshak G. Infertility in American college alumnae. Intl J Gynaecol Obstet 2001;73:237-242.
3. Practice Committee of the American Society for Reproductive Medicine. Optimal evaluation of the infertile female. Fertil Steril 2004;82(Suppl 1):S169-S172.
4. Brigham and Women’s Hospital. Infertility: A Guide to Evaluation, Treatment, and Counseling. Boston, Mass: Brigham and Women’s Hospital; 2003:11.
5. Report on optimal evaluation of the infertile male. Baltimore, Md: American Urological Association; 2001:14.
6. Witt MA, Lipshultz LI. Varicocele: A progressive or static lesion? Urology 1993;42:541-543.
7. Valenzano M, Mistrangelo E, Lijoi D, et al. Transvaginal sonohysterographic evaluation of uterine malformations. Eur J Obstet Gynecol Reprod Biol 2006;124:246-249.
8. Roma Dalfó A, Ubeda B, Ubeda A, et al. Diagnostic value of hysterosalpingography in the detection of intrauterine abnormalities: a comparison with hysteroscopy. AJR Am J Roentgenol 2004;183:1405-1409.
9. Shokeir T, Shalan H, El-Shafei M. Combined diagnostic approach of laparoscopy and hysteroscopy in the evaluation of female infertility: Results of 612 patients. J Obstet Gynaecol Res 2004;30:9-14.
10. Oei SG, Helmerhorst F, Bloemenkamp K, Hollants F, Meerpoel D, Keirse M. Effectiveness of the postcoital test: randomized controlled trial. BMJ 1998;317:502-505.
1. National Collaborating Centre for Women’s and Children’s Health. Fertility: Assessment and Treatment for People with Fertility Problems. London: RCOG Press; 2004:216.
2. Wyshak G. Infertility in American college alumnae. Intl J Gynaecol Obstet 2001;73:237-242.
3. Practice Committee of the American Society for Reproductive Medicine. Optimal evaluation of the infertile female. Fertil Steril 2004;82(Suppl 1):S169-S172.
4. Brigham and Women’s Hospital. Infertility: A Guide to Evaluation, Treatment, and Counseling. Boston, Mass: Brigham and Women’s Hospital; 2003:11.
5. Report on optimal evaluation of the infertile male. Baltimore, Md: American Urological Association; 2001:14.
6. Witt MA, Lipshultz LI. Varicocele: A progressive or static lesion? Urology 1993;42:541-543.
7. Valenzano M, Mistrangelo E, Lijoi D, et al. Transvaginal sonohysterographic evaluation of uterine malformations. Eur J Obstet Gynecol Reprod Biol 2006;124:246-249.
8. Roma Dalfó A, Ubeda B, Ubeda A, et al. Diagnostic value of hysterosalpingography in the detection of intrauterine abnormalities: a comparison with hysteroscopy. AJR Am J Roentgenol 2004;183:1405-1409.
9. Shokeir T, Shalan H, El-Shafei M. Combined diagnostic approach of laparoscopy and hysteroscopy in the evaluation of female infertility: Results of 612 patients. J Obstet Gynaecol Res 2004;30:9-14.
10. Oei SG, Helmerhorst F, Bloemenkamp K, Hollants F, Meerpoel D, Keirse M. Effectiveness of the postcoital test: randomized controlled trial. BMJ 1998;317:502-505.
Evidence-based answers from the Family Physicians Inquiries Network
Which UTI therapies are safe and effective during breastfeeding?
Trimethoprim/sulfamethoxazole (TMP/SMX) has a high success rate in eradicating bacteriuria for women with urinary tract infection and is compatible with breastfeeding (strength of recommendation: C, based on extrapolation from studies with nonlactating women and disease-oriented outcomes).
Quinolones (ciprofloxacin, ofloxacin) are effective and probably compatible with breastfeeding; however, their use has not been recommended by many investigators based on arthropathy in animal studies (SOR: C, based on extrapolation from case series and disease-oriented outcomes).
A 7-day course of nitrofurantoin has similar efficacy to TMP/SMX and is compatible with breastfeeding, but it should be avoided in populations at risk for glucose-6-phosphate dehydrogenase (G6PD) deficiency (also known as favism, most often found in patients of mediterranean or african descent) (SOR: C, extrapolation from studies in nonlactating women and disease-oriented outcomes).
An antibiotic that’s effective for mom and safe for baby is of paramount importance
Timothy Huber, MD
Oroville, Calif
Knowing the local resistance patterns can greatly aid in choosing a safe, effective antibiotic. Most local laboratories that do microbiology work either publish their antibiograms or make them available on a semiannual or annual basis. Keeping these readily available can be a time-saver when it comes to decision-making and writing a prescription.
Evidence summary
Urinary tract infections (UTIs) are common in reproductive-aged women. In lactating women, it’s important to select a therapy that is not only effective, but also safe for the breastfeeding infant. No studies in the literature address the safety or efficacy of UTI treatments in lactating women and their infants. Therefore, recommendations are extrapolated from studies of efficacy in the general population, studies of antibiotic penetration into breast milk, and effects of antibiotics given to infants directly.
How the efficacy of UTI treatments stack up
The best evidence for efficacy of UTI treatments comes from a 1999 meta-analysis of uncomplicated UTI in nonpregnant, nonlactating women.1 They found TMP/SMX to be the most widely studied antibiotic and to have a 93% bacterial eradication rate; it was therefore used as a standard for comparison of other treatments. Nitrofurantoin and quinolones (ofloxacin, ciprofloxacin, and others) had comparable eradication rates to TMP/SMX in the same study; 7-day courses of nitrofurantoin were more efficacious than shorter ones. TMP/SMX is not recommended if the local resistance rate is more than 10% to 20%.2
Three-day therapy for uncomplicated UTI is more effective than single-dose therapy and equal to longer courses for most antibiotics.1 A longer course (7 days) may be required for nitrofurantoin. Beta-lactams are associated with high levels of resistance and therefore not recommended in empiric treatment of UTI.2
A look at penetration into breast milk
Most of the data regarding antibiotic penetration into breast milk come from case series. One South African series measured breast milk levels of both trimethoprim and sulfamethoxazole among 50 Bantu women treated with TMP/SMX for various infections (including UTI).3 The women received 160 mg TMP and 800 mg SMX 2 or 3 times daily for up to 5 days. The average level of TMP in breast milk was 2 mcg/mL, and the level of SMX was 4.7 mcg/mL. Researchers calculated that the average breastfeeding infant would ingest only 1 mg of TMP and 2.5 mg of SMX per day. TMP/SMX is generally considered safe for infants in the absence of G6PD deficiency.
In a case series, 9 lactating mothers were given nitrofurantoin 100 mg orally every 6 hours for 1 day.4 On day 2, after a single 100 to 200 mg dose, drug levels in the breast milk 2 hours post-dose ranged from none (in 6 of the 9 women) to a maximum of 0.5 mcg/mL in one. Since even a very small amount of the drug may trigger a hemolytic reaction among G6PD-deficient individuals, the researchers called for caution when prescribing to mothers from high-risk populations.
A final case seriesadministered ciprofloxacin 750 mg, pefloxacin 400 mg, or ofloxacin 400 mg twice daily to 3 groups of 10 women each.5 Milk samples were obtained 6 times over 24 hours following the third dose of antibiotic. Maximum levels in breast milk occurred 2 hours after the dose, and were 3.79, 3.54, and 2.41 mcg/mL for ciprofloxacin, pefloxacin, and ofloxacin respectively. All 3 quinolones achieved higher concentrations in breast milk than in serum.
But are these drugs safe for children?
While TMP/SMX and nitrofurantoin are generally considered safe when given to infants and children (barring G6PD deficiency), data are mixed regarding the safety of quinolones. Ciprofloxacin’s FDA indication for pediatric patients is limited to postexposure anthrax prophylaxis due to evidence of fluoroquinolone-induced joint toxicity in animal studies.6 Despite this, they have been prescribed to tens of thousands of children for select scenarios such as chemotherapy-induced immuno-compromise, cystic fibrosis, complicated UTIs, and salmonella infections.7
A report was published summarizing safety data from the Bayer database of compassionate use of ciprofloxacin.8 The report indicates that 2030 treatment courses of ciprofloxacin were given to 1795 children up to age 17 for a variety of infections; only 3% were under age 5. Most patients received 21 to 40 mg/kg of ciprofloxacin per day; treatment duration was from 1 to 303 days. Arthralgia occurred in 1.5% of patients, most of whom had cystic fibrosis. Of the 31 patients affected, arthralgias resolved in 25, improved in 1, and remained unchanged in 1. (Data regarding resolution were unavailable for 4 patients.)
Recommendations from others
The American Academy of Pediatrics’ Committee on Drugsconsiders the following antibiotics typically used for UTI to be compatible with breastfeeding: ciprofloxacin, ofloxacin, nitrofurantoin (caution for infants with G6PD deficiency), and TMP/SMX.9
Drugs in Pregnancy and Lactation considers trimethoprim and sulfamethoxazole to be compatible with breastfeeding but cautions against sulfamethoxazole use in infants with known G6PD deficiency. The authors categorize nitrofurantoin, ciprofloxacin, and ofloxacin as “probably compatible/limited human data,” and advise caution with nitrofurantoin for infants with G6PD deficiency.10
1. Warren JW, Abrutyn J, Bebel R, et al. Guidelines for antimicrobial treatment of uncomplicated acute bacterial cystitis and acute pyelonephritis in women. Guidelines from the Infectious Diseases society of America. Clin Infect Dis 1999;29:745-758
2. Gupta K, Scholes D, Stamm WE. Increasing prevalence of antimicrobial resistance among uropathogens causing acute uncomplicated cystitis in women. JAMA 1999;281:736-758.
3. Miller RD, Salter AJ. The passage of trimethoprim/sulfamethoxazole into breast milk and its significance. Proceedings of the 8th International Congress of Chemotherapy, Athens. Hellenic Soc Chemother 1974;1:687-691.
4. Varsano I, Fischl J, Shochet S. The excretion of orally ingested nitrofurantoin in human milk [letter]. J Pediatr 1973;886-887.
5. Giamerellou H, Kolokythas E, Petrikkos G, et al. Pharmacokinetics of three newer quinolones in pregnant and lactating women. Am J Med 1989;87 (Suppl 5A):49s-51s.
6. Cipro package insert. West Haven, Conn: Bayer Pharmaceuticals Corporation; January 2004.
7. Grady R. Safety profile of quinolone antibiotics in the pediatric population. Pediatr Infect Dis J 2003;22:1128-1132.
8. Hampel B, Hullmann R, Schmidt H. Ciprofloxacin in pediatrics: worldwide clinical experience based on compassionate use-safety report. Pediatr Infect Dis J 1997;16:127-1209.
9. American Academy of Pediatrics Committee on Drugs. The transfer of drugs and other chemicals into human milk. Pediatrics 2001;108:776-789.
10. Briggs GG, Freeman RK, Yaffe SJ. Drugs during Pregnancy and Lactation. 7th ed. Baltimore, Md: Lippincott, Williams & Wilkins; 2005.
Trimethoprim/sulfamethoxazole (TMP/SMX) has a high success rate in eradicating bacteriuria for women with urinary tract infection and is compatible with breastfeeding (strength of recommendation: C, based on extrapolation from studies with nonlactating women and disease-oriented outcomes).
Quinolones (ciprofloxacin, ofloxacin) are effective and probably compatible with breastfeeding; however, their use has not been recommended by many investigators based on arthropathy in animal studies (SOR: C, based on extrapolation from case series and disease-oriented outcomes).
A 7-day course of nitrofurantoin has similar efficacy to TMP/SMX and is compatible with breastfeeding, but it should be avoided in populations at risk for glucose-6-phosphate dehydrogenase (G6PD) deficiency (also known as favism, most often found in patients of mediterranean or african descent) (SOR: C, extrapolation from studies in nonlactating women and disease-oriented outcomes).
An antibiotic that’s effective for mom and safe for baby is of paramount importance
Timothy Huber, MD
Oroville, Calif
Knowing the local resistance patterns can greatly aid in choosing a safe, effective antibiotic. Most local laboratories that do microbiology work either publish their antibiograms or make them available on a semiannual or annual basis. Keeping these readily available can be a time-saver when it comes to decision-making and writing a prescription.
Evidence summary
Urinary tract infections (UTIs) are common in reproductive-aged women. In lactating women, it’s important to select a therapy that is not only effective, but also safe for the breastfeeding infant. No studies in the literature address the safety or efficacy of UTI treatments in lactating women and their infants. Therefore, recommendations are extrapolated from studies of efficacy in the general population, studies of antibiotic penetration into breast milk, and effects of antibiotics given to infants directly.
How the efficacy of UTI treatments stack up
The best evidence for efficacy of UTI treatments comes from a 1999 meta-analysis of uncomplicated UTI in nonpregnant, nonlactating women.1 They found TMP/SMX to be the most widely studied antibiotic and to have a 93% bacterial eradication rate; it was therefore used as a standard for comparison of other treatments. Nitrofurantoin and quinolones (ofloxacin, ciprofloxacin, and others) had comparable eradication rates to TMP/SMX in the same study; 7-day courses of nitrofurantoin were more efficacious than shorter ones. TMP/SMX is not recommended if the local resistance rate is more than 10% to 20%.2
Three-day therapy for uncomplicated UTI is more effective than single-dose therapy and equal to longer courses for most antibiotics.1 A longer course (7 days) may be required for nitrofurantoin. Beta-lactams are associated with high levels of resistance and therefore not recommended in empiric treatment of UTI.2
A look at penetration into breast milk
Most of the data regarding antibiotic penetration into breast milk come from case series. One South African series measured breast milk levels of both trimethoprim and sulfamethoxazole among 50 Bantu women treated with TMP/SMX for various infections (including UTI).3 The women received 160 mg TMP and 800 mg SMX 2 or 3 times daily for up to 5 days. The average level of TMP in breast milk was 2 mcg/mL, and the level of SMX was 4.7 mcg/mL. Researchers calculated that the average breastfeeding infant would ingest only 1 mg of TMP and 2.5 mg of SMX per day. TMP/SMX is generally considered safe for infants in the absence of G6PD deficiency.
In a case series, 9 lactating mothers were given nitrofurantoin 100 mg orally every 6 hours for 1 day.4 On day 2, after a single 100 to 200 mg dose, drug levels in the breast milk 2 hours post-dose ranged from none (in 6 of the 9 women) to a maximum of 0.5 mcg/mL in one. Since even a very small amount of the drug may trigger a hemolytic reaction among G6PD-deficient individuals, the researchers called for caution when prescribing to mothers from high-risk populations.
A final case seriesadministered ciprofloxacin 750 mg, pefloxacin 400 mg, or ofloxacin 400 mg twice daily to 3 groups of 10 women each.5 Milk samples were obtained 6 times over 24 hours following the third dose of antibiotic. Maximum levels in breast milk occurred 2 hours after the dose, and were 3.79, 3.54, and 2.41 mcg/mL for ciprofloxacin, pefloxacin, and ofloxacin respectively. All 3 quinolones achieved higher concentrations in breast milk than in serum.
But are these drugs safe for children?
While TMP/SMX and nitrofurantoin are generally considered safe when given to infants and children (barring G6PD deficiency), data are mixed regarding the safety of quinolones. Ciprofloxacin’s FDA indication for pediatric patients is limited to postexposure anthrax prophylaxis due to evidence of fluoroquinolone-induced joint toxicity in animal studies.6 Despite this, they have been prescribed to tens of thousands of children for select scenarios such as chemotherapy-induced immuno-compromise, cystic fibrosis, complicated UTIs, and salmonella infections.7
A report was published summarizing safety data from the Bayer database of compassionate use of ciprofloxacin.8 The report indicates that 2030 treatment courses of ciprofloxacin were given to 1795 children up to age 17 for a variety of infections; only 3% were under age 5. Most patients received 21 to 40 mg/kg of ciprofloxacin per day; treatment duration was from 1 to 303 days. Arthralgia occurred in 1.5% of patients, most of whom had cystic fibrosis. Of the 31 patients affected, arthralgias resolved in 25, improved in 1, and remained unchanged in 1. (Data regarding resolution were unavailable for 4 patients.)
Recommendations from others
The American Academy of Pediatrics’ Committee on Drugsconsiders the following antibiotics typically used for UTI to be compatible with breastfeeding: ciprofloxacin, ofloxacin, nitrofurantoin (caution for infants with G6PD deficiency), and TMP/SMX.9
Drugs in Pregnancy and Lactation considers trimethoprim and sulfamethoxazole to be compatible with breastfeeding but cautions against sulfamethoxazole use in infants with known G6PD deficiency. The authors categorize nitrofurantoin, ciprofloxacin, and ofloxacin as “probably compatible/limited human data,” and advise caution with nitrofurantoin for infants with G6PD deficiency.10
Trimethoprim/sulfamethoxazole (TMP/SMX) has a high success rate in eradicating bacteriuria for women with urinary tract infection and is compatible with breastfeeding (strength of recommendation: C, based on extrapolation from studies with nonlactating women and disease-oriented outcomes).
Quinolones (ciprofloxacin, ofloxacin) are effective and probably compatible with breastfeeding; however, their use has not been recommended by many investigators based on arthropathy in animal studies (SOR: C, based on extrapolation from case series and disease-oriented outcomes).
A 7-day course of nitrofurantoin has similar efficacy to TMP/SMX and is compatible with breastfeeding, but it should be avoided in populations at risk for glucose-6-phosphate dehydrogenase (G6PD) deficiency (also known as favism, most often found in patients of mediterranean or african descent) (SOR: C, extrapolation from studies in nonlactating women and disease-oriented outcomes).
An antibiotic that’s effective for mom and safe for baby is of paramount importance
Timothy Huber, MD
Oroville, Calif
Knowing the local resistance patterns can greatly aid in choosing a safe, effective antibiotic. Most local laboratories that do microbiology work either publish their antibiograms or make them available on a semiannual or annual basis. Keeping these readily available can be a time-saver when it comes to decision-making and writing a prescription.
Evidence summary
Urinary tract infections (UTIs) are common in reproductive-aged women. In lactating women, it’s important to select a therapy that is not only effective, but also safe for the breastfeeding infant. No studies in the literature address the safety or efficacy of UTI treatments in lactating women and their infants. Therefore, recommendations are extrapolated from studies of efficacy in the general population, studies of antibiotic penetration into breast milk, and effects of antibiotics given to infants directly.
How the efficacy of UTI treatments stack up
The best evidence for efficacy of UTI treatments comes from a 1999 meta-analysis of uncomplicated UTI in nonpregnant, nonlactating women.1 They found TMP/SMX to be the most widely studied antibiotic and to have a 93% bacterial eradication rate; it was therefore used as a standard for comparison of other treatments. Nitrofurantoin and quinolones (ofloxacin, ciprofloxacin, and others) had comparable eradication rates to TMP/SMX in the same study; 7-day courses of nitrofurantoin were more efficacious than shorter ones. TMP/SMX is not recommended if the local resistance rate is more than 10% to 20%.2
Three-day therapy for uncomplicated UTI is more effective than single-dose therapy and equal to longer courses for most antibiotics.1 A longer course (7 days) may be required for nitrofurantoin. Beta-lactams are associated with high levels of resistance and therefore not recommended in empiric treatment of UTI.2
A look at penetration into breast milk
Most of the data regarding antibiotic penetration into breast milk come from case series. One South African series measured breast milk levels of both trimethoprim and sulfamethoxazole among 50 Bantu women treated with TMP/SMX for various infections (including UTI).3 The women received 160 mg TMP and 800 mg SMX 2 or 3 times daily for up to 5 days. The average level of TMP in breast milk was 2 mcg/mL, and the level of SMX was 4.7 mcg/mL. Researchers calculated that the average breastfeeding infant would ingest only 1 mg of TMP and 2.5 mg of SMX per day. TMP/SMX is generally considered safe for infants in the absence of G6PD deficiency.
In a case series, 9 lactating mothers were given nitrofurantoin 100 mg orally every 6 hours for 1 day.4 On day 2, after a single 100 to 200 mg dose, drug levels in the breast milk 2 hours post-dose ranged from none (in 6 of the 9 women) to a maximum of 0.5 mcg/mL in one. Since even a very small amount of the drug may trigger a hemolytic reaction among G6PD-deficient individuals, the researchers called for caution when prescribing to mothers from high-risk populations.
A final case seriesadministered ciprofloxacin 750 mg, pefloxacin 400 mg, or ofloxacin 400 mg twice daily to 3 groups of 10 women each.5 Milk samples were obtained 6 times over 24 hours following the third dose of antibiotic. Maximum levels in breast milk occurred 2 hours after the dose, and were 3.79, 3.54, and 2.41 mcg/mL for ciprofloxacin, pefloxacin, and ofloxacin respectively. All 3 quinolones achieved higher concentrations in breast milk than in serum.
But are these drugs safe for children?
While TMP/SMX and nitrofurantoin are generally considered safe when given to infants and children (barring G6PD deficiency), data are mixed regarding the safety of quinolones. Ciprofloxacin’s FDA indication for pediatric patients is limited to postexposure anthrax prophylaxis due to evidence of fluoroquinolone-induced joint toxicity in animal studies.6 Despite this, they have been prescribed to tens of thousands of children for select scenarios such as chemotherapy-induced immuno-compromise, cystic fibrosis, complicated UTIs, and salmonella infections.7
A report was published summarizing safety data from the Bayer database of compassionate use of ciprofloxacin.8 The report indicates that 2030 treatment courses of ciprofloxacin were given to 1795 children up to age 17 for a variety of infections; only 3% were under age 5. Most patients received 21 to 40 mg/kg of ciprofloxacin per day; treatment duration was from 1 to 303 days. Arthralgia occurred in 1.5% of patients, most of whom had cystic fibrosis. Of the 31 patients affected, arthralgias resolved in 25, improved in 1, and remained unchanged in 1. (Data regarding resolution were unavailable for 4 patients.)
Recommendations from others
The American Academy of Pediatrics’ Committee on Drugsconsiders the following antibiotics typically used for UTI to be compatible with breastfeeding: ciprofloxacin, ofloxacin, nitrofurantoin (caution for infants with G6PD deficiency), and TMP/SMX.9
Drugs in Pregnancy and Lactation considers trimethoprim and sulfamethoxazole to be compatible with breastfeeding but cautions against sulfamethoxazole use in infants with known G6PD deficiency. The authors categorize nitrofurantoin, ciprofloxacin, and ofloxacin as “probably compatible/limited human data,” and advise caution with nitrofurantoin for infants with G6PD deficiency.10
1. Warren JW, Abrutyn J, Bebel R, et al. Guidelines for antimicrobial treatment of uncomplicated acute bacterial cystitis and acute pyelonephritis in women. Guidelines from the Infectious Diseases society of America. Clin Infect Dis 1999;29:745-758
2. Gupta K, Scholes D, Stamm WE. Increasing prevalence of antimicrobial resistance among uropathogens causing acute uncomplicated cystitis in women. JAMA 1999;281:736-758.
3. Miller RD, Salter AJ. The passage of trimethoprim/sulfamethoxazole into breast milk and its significance. Proceedings of the 8th International Congress of Chemotherapy, Athens. Hellenic Soc Chemother 1974;1:687-691.
4. Varsano I, Fischl J, Shochet S. The excretion of orally ingested nitrofurantoin in human milk [letter]. J Pediatr 1973;886-887.
5. Giamerellou H, Kolokythas E, Petrikkos G, et al. Pharmacokinetics of three newer quinolones in pregnant and lactating women. Am J Med 1989;87 (Suppl 5A):49s-51s.
6. Cipro package insert. West Haven, Conn: Bayer Pharmaceuticals Corporation; January 2004.
7. Grady R. Safety profile of quinolone antibiotics in the pediatric population. Pediatr Infect Dis J 2003;22:1128-1132.
8. Hampel B, Hullmann R, Schmidt H. Ciprofloxacin in pediatrics: worldwide clinical experience based on compassionate use-safety report. Pediatr Infect Dis J 1997;16:127-1209.
9. American Academy of Pediatrics Committee on Drugs. The transfer of drugs and other chemicals into human milk. Pediatrics 2001;108:776-789.
10. Briggs GG, Freeman RK, Yaffe SJ. Drugs during Pregnancy and Lactation. 7th ed. Baltimore, Md: Lippincott, Williams & Wilkins; 2005.
1. Warren JW, Abrutyn J, Bebel R, et al. Guidelines for antimicrobial treatment of uncomplicated acute bacterial cystitis and acute pyelonephritis in women. Guidelines from the Infectious Diseases society of America. Clin Infect Dis 1999;29:745-758
2. Gupta K, Scholes D, Stamm WE. Increasing prevalence of antimicrobial resistance among uropathogens causing acute uncomplicated cystitis in women. JAMA 1999;281:736-758.
3. Miller RD, Salter AJ. The passage of trimethoprim/sulfamethoxazole into breast milk and its significance. Proceedings of the 8th International Congress of Chemotherapy, Athens. Hellenic Soc Chemother 1974;1:687-691.
4. Varsano I, Fischl J, Shochet S. The excretion of orally ingested nitrofurantoin in human milk [letter]. J Pediatr 1973;886-887.
5. Giamerellou H, Kolokythas E, Petrikkos G, et al. Pharmacokinetics of three newer quinolones in pregnant and lactating women. Am J Med 1989;87 (Suppl 5A):49s-51s.
6. Cipro package insert. West Haven, Conn: Bayer Pharmaceuticals Corporation; January 2004.
7. Grady R. Safety profile of quinolone antibiotics in the pediatric population. Pediatr Infect Dis J 2003;22:1128-1132.
8. Hampel B, Hullmann R, Schmidt H. Ciprofloxacin in pediatrics: worldwide clinical experience based on compassionate use-safety report. Pediatr Infect Dis J 1997;16:127-1209.
9. American Academy of Pediatrics Committee on Drugs. The transfer of drugs and other chemicals into human milk. Pediatrics 2001;108:776-789.
10. Briggs GG, Freeman RK, Yaffe SJ. Drugs during Pregnancy and Lactation. 7th ed. Baltimore, Md: Lippincott, Williams & Wilkins; 2005.
Evidence-based answers from the Family Physicians Inquiries Network
How safe is vaginal birth after cesarean section for the mother and fetus?
Compared with planned repeat low-transverse cesarean section, vaginal birth after cesarean section (VBAC) is not associated with increased risk of maternal or neonatal mortality (strength of recommendation [SOR]: B). Morbidity is slightly increased, as evidenced by higher uterine rupture rates and some neonatal outcome measures (SOR: B).
Risks of C-section and labor must be considered when counseling regarding route of delivery
Lynda DeArmond, MD
Waco Family Practice Residency Program, Waco, Texas
Another question to pose is: how safe is repeat cesarean section for the mother and fetus? How much do morbidity and mortality increase with each new intra-abdominal procedure? Each time the belly is opened there is new scar, with increased likelihood of adhesions and potential for future bowel obstruction. Consider these risks when counseling regarding route of delivery. Risk of uterine rupture appears to be higher in trials of labor (and confers a statistically significant but small increase in morbidity but not mortality). However, the uterine scar can silently fail without labor—as is sometimes discovered at a scheduled repeat section, usually without untoward effects on mother or fetus.
Remember that you are sending a young woman home with a new baby to care for (along with other children) and a major abdominal procedure (through an old scar) to recover from, which one could certainly define as morbidity. Cesarean section is an important tool, but we must be careful to practice best possible care and consider all patient factors and preferences. And data are still lacking to support the notion that VBAC is unsafe.
Evidence summary
Contrary to the goals of Healthy People 2010, the rate of cesarean sections is increasing.1 The repeat cesarean rate for low-risk women of all ages and racial groups is now 88.7%, the highest rate since the Centers for Disease Control and Prevention (CDC) began tracking the statistic in 1989. Is VBAC safe, or is a trial of labor no longer supported by the data?
The most recent Cochrane Review found that both VBAC and repeat lowtransverse cesarean section have benefits and risks associated with them; however, after reviewing the limited data, they concluded that no trial exists to adequately help women and their caregivers make an informed decision between the two.2 A strong theme in the Cochrane Review, echoed in most reviews, was the absence of high-quality prospective randomized data.
In an attempt to quantify the risks of VBAC, a systematic review determined that attempted VBAC, compared with repeat low-transverse cesarean section, increased the risk of uterine rupture by 2.7 per 1000 cases (95% confidence interval [CI], 0.73–4.73).3 This additional risk rate is often quoted in VBAC reviews and was cited in the Agency for Healthcare Research and Quality evidence report; it is based on 1 prospective, nonrandomized cohort trial and 1 retrospective cohort study.4,5
No randomized controlled trials exist for determining maternal safety of VBAC, although another recent systematic review found 2 nonrandomized prospective trials of sufficient quality to analyze. The authors concluded there were “no statistically significant differences between planned elective repeat cesarean section and planned VBAC.”6 Upon closer review in PubMed, one of the cited studies did not study 312 patients for VBAC outcomes as alleged; rather, it investigated patient attitudes towards VBAC.7
Since publication of that review, a large, multicenter, prospective, nonrandomized trial involving 33,699 patients found no significant difference between VBAC and planned cesarean for hysterectomy (0.2% vs 0.3%; odds ratio [OR]=0.77; 95% CI, 0.51–1.17), maternal death (0.02% vs 0.04%; OR=0.38; 95% CI, 0.1–1.46), and neonatal death (0.08% vs 0.05%; OR=1.82; 95% CI, 0.73–4.57).8 Significant associations were found for uterine rupture rates in spontaneous labor (24/6685 [0.4%] vs no cases; number needed to harm [NNH]=279) and neonatal hypoxic-ischemic encephalopathy (0.46 cases per 1000 vs no cases; NNH=2174).8
A retrospective Canadian cohort trial of 308,755 women also demonstrated an association of VBAC with uterine rupture(0.65% of trial-of-labor cases; OR=2.38; 95% CI, 2.12–2.67), and a trend towards higher maternal mortality in the cesarean group (1.6 per 100,000 for VBAC vs 5.6 per 100,000 for planned cesarean; OR=0.32; 95% CI, 0.07–1.47).9
The effect of VBAC on neonatal morbidity and mortality is unclear. In contrast to the negative larger trial,8 a smaller retrospective cohort of 24,529 births found a higher association of perinatal death for trial of labor (adjusted OR=11.7; 95% CI, 1.4–101.6).10 The perinatal death rate was similar to rates in nulliparous women. Regarding morbidity, one retrospective cohort trial showed VBAC was associated with an increase in neonatal sepsis (1% vs 0%; CI not given) compared with planned cesarean, but VBAC resulted in less transient tachypnea (5% vs 7%) and hyper-bilirubinemia (2% vs 6%).11
Recommendations from others
Both the American College of Obstetricians and Gynecologists and the Society of Obstetricians and Gynecologists of Canada state that women with 1 previous low-transverse cesarean section should be offered a trial of labor after appropriate counseling of the risks and benefits.12,13 Furthermore, induction with oxytocin is allowed, but the use of prostaglandins is not recommended. Based on expert opinion, both organizations encourage VBAC only in institutions staffed with surgeons and anesthesiologists immediately available to provide emergent cesarean.
Acknowledgments
The opinions and assertions contained herein are the private views of the author and are not to be construed as official, or as reflecting the views of the US Air Force medical department or the US Air Force at large.
1. Menacker F. Trends in cesarean rates for first births and repeat cesarean rates for low-risk women: United States, 1990-2003. Natl Vital Stat Rep 2005;54:1-8.
2. Dodd J, Crowther C, Huertas E, Guise J, Horey D. Planned elective repeat caesarean section versus planned vaginal birth for women with a previous caesarean birth. Cochrane Database Syst Rev 2005;(4):CD004224.
3. Guise J, McDonagh M, Osterweil P, Nygren P, Chan B, Helfand M. Systematic review of the incidence and consequences of uterine rupture in women with previous caesarean section. BMJ 2004;329:19-25.
4. Vaginal Birth After Cesarean (VBAC). Summary. Evidence Report/Technology Assessment, No. 71. AHRQ publication 03-E017. Rockville, Md: Agency for Healthcare Research and Quality; 2003. Available at: www.ahrq.gov/clinic/epcsums/vbacsum.htm. Accessed on January 9, 2006.
5. McMahon MJ, Luther ER, Bowes WA, Olshan AF. Comparison of a trial of labor with an elective second cesarean section. N Engl J Med 1996;335:689-695.
6. Dodd J, Crowther C. Vaginal birth after Caesarean versus elective repeat Caesarean for women with a single prior Caesarean birth: a systematic review of the literature. Aust N Z J Obstet Gynaecol 2004;44:387-391.
7. Abitbol MM, Castillo I, Taylor UB, Rochelson BL, Shmoys S, Monheit AG. Vaginal birth after cesarean section: the patient’s point of view. Am Fam Physician 1993;47:129-134.
8. Landon M, Hauth J, Leveno K, et al. for the National Institute of Child Health and Human Development Maternal-Fetal Medicine Units Network. Maternal and perinatal outcomes associated with a trial of labor after prior cesarean delivery. N Engl J Med 2004;351:2581-2589.
9. Wen S, Rusen I, Walker M, et al. Comparison of maternal mortality and morbidity between trial of labor and elective cesarean section among women with previous cesarean delivery. Am J Obstet Gynecol 2004;191:1263-1269.
10. Smith G, Pell J, Cameron A, Dobbie R. Risk of perinatal death associated with labor after previous cesarean delivery in uncomplicated term pregnancies. JAMA 2002;287:2684-2690.
11. Hook B, Kiwi R, Amini S, Fanaroff A, Hack M. Neonatal morbidity after elective repeat cesarean section and trial of labor. Pediatrics 1997;100:348-353.
12. American College of Obstetricians and Gynecologists Committee on Practice Bulletins—Obstetrics. ACOG Practice Bulletin. Vaginal Birth After Cesarean Delivery. Obstet Gynecol 2004;104:203-212.
13. Martel M, MacKinnon C, and the Clinical Practice Obstetrics Committee, Society of Obstetricians and Gynaecologists of Canada. Guidelines for vaginal birth after previous Caesarean birth. J Obstet Gynaecol Can 2005;27:164-188.
Compared with planned repeat low-transverse cesarean section, vaginal birth after cesarean section (VBAC) is not associated with increased risk of maternal or neonatal mortality (strength of recommendation [SOR]: B). Morbidity is slightly increased, as evidenced by higher uterine rupture rates and some neonatal outcome measures (SOR: B).
Risks of C-section and labor must be considered when counseling regarding route of delivery
Lynda DeArmond, MD
Waco Family Practice Residency Program, Waco, Texas
Another question to pose is: how safe is repeat cesarean section for the mother and fetus? How much do morbidity and mortality increase with each new intra-abdominal procedure? Each time the belly is opened there is new scar, with increased likelihood of adhesions and potential for future bowel obstruction. Consider these risks when counseling regarding route of delivery. Risk of uterine rupture appears to be higher in trials of labor (and confers a statistically significant but small increase in morbidity but not mortality). However, the uterine scar can silently fail without labor—as is sometimes discovered at a scheduled repeat section, usually without untoward effects on mother or fetus.
Remember that you are sending a young woman home with a new baby to care for (along with other children) and a major abdominal procedure (through an old scar) to recover from, which one could certainly define as morbidity. Cesarean section is an important tool, but we must be careful to practice best possible care and consider all patient factors and preferences. And data are still lacking to support the notion that VBAC is unsafe.
Evidence summary
Contrary to the goals of Healthy People 2010, the rate of cesarean sections is increasing.1 The repeat cesarean rate for low-risk women of all ages and racial groups is now 88.7%, the highest rate since the Centers for Disease Control and Prevention (CDC) began tracking the statistic in 1989. Is VBAC safe, or is a trial of labor no longer supported by the data?
The most recent Cochrane Review found that both VBAC and repeat lowtransverse cesarean section have benefits and risks associated with them; however, after reviewing the limited data, they concluded that no trial exists to adequately help women and their caregivers make an informed decision between the two.2 A strong theme in the Cochrane Review, echoed in most reviews, was the absence of high-quality prospective randomized data.
In an attempt to quantify the risks of VBAC, a systematic review determined that attempted VBAC, compared with repeat low-transverse cesarean section, increased the risk of uterine rupture by 2.7 per 1000 cases (95% confidence interval [CI], 0.73–4.73).3 This additional risk rate is often quoted in VBAC reviews and was cited in the Agency for Healthcare Research and Quality evidence report; it is based on 1 prospective, nonrandomized cohort trial and 1 retrospective cohort study.4,5
No randomized controlled trials exist for determining maternal safety of VBAC, although another recent systematic review found 2 nonrandomized prospective trials of sufficient quality to analyze. The authors concluded there were “no statistically significant differences between planned elective repeat cesarean section and planned VBAC.”6 Upon closer review in PubMed, one of the cited studies did not study 312 patients for VBAC outcomes as alleged; rather, it investigated patient attitudes towards VBAC.7
Since publication of that review, a large, multicenter, prospective, nonrandomized trial involving 33,699 patients found no significant difference between VBAC and planned cesarean for hysterectomy (0.2% vs 0.3%; odds ratio [OR]=0.77; 95% CI, 0.51–1.17), maternal death (0.02% vs 0.04%; OR=0.38; 95% CI, 0.1–1.46), and neonatal death (0.08% vs 0.05%; OR=1.82; 95% CI, 0.73–4.57).8 Significant associations were found for uterine rupture rates in spontaneous labor (24/6685 [0.4%] vs no cases; number needed to harm [NNH]=279) and neonatal hypoxic-ischemic encephalopathy (0.46 cases per 1000 vs no cases; NNH=2174).8
A retrospective Canadian cohort trial of 308,755 women also demonstrated an association of VBAC with uterine rupture(0.65% of trial-of-labor cases; OR=2.38; 95% CI, 2.12–2.67), and a trend towards higher maternal mortality in the cesarean group (1.6 per 100,000 for VBAC vs 5.6 per 100,000 for planned cesarean; OR=0.32; 95% CI, 0.07–1.47).9
The effect of VBAC on neonatal morbidity and mortality is unclear. In contrast to the negative larger trial,8 a smaller retrospective cohort of 24,529 births found a higher association of perinatal death for trial of labor (adjusted OR=11.7; 95% CI, 1.4–101.6).10 The perinatal death rate was similar to rates in nulliparous women. Regarding morbidity, one retrospective cohort trial showed VBAC was associated with an increase in neonatal sepsis (1% vs 0%; CI not given) compared with planned cesarean, but VBAC resulted in less transient tachypnea (5% vs 7%) and hyper-bilirubinemia (2% vs 6%).11
Recommendations from others
Both the American College of Obstetricians and Gynecologists and the Society of Obstetricians and Gynecologists of Canada state that women with 1 previous low-transverse cesarean section should be offered a trial of labor after appropriate counseling of the risks and benefits.12,13 Furthermore, induction with oxytocin is allowed, but the use of prostaglandins is not recommended. Based on expert opinion, both organizations encourage VBAC only in institutions staffed with surgeons and anesthesiologists immediately available to provide emergent cesarean.
Acknowledgments
The opinions and assertions contained herein are the private views of the author and are not to be construed as official, or as reflecting the views of the US Air Force medical department or the US Air Force at large.
Compared with planned repeat low-transverse cesarean section, vaginal birth after cesarean section (VBAC) is not associated with increased risk of maternal or neonatal mortality (strength of recommendation [SOR]: B). Morbidity is slightly increased, as evidenced by higher uterine rupture rates and some neonatal outcome measures (SOR: B).
Risks of C-section and labor must be considered when counseling regarding route of delivery
Lynda DeArmond, MD
Waco Family Practice Residency Program, Waco, Texas
Another question to pose is: how safe is repeat cesarean section for the mother and fetus? How much do morbidity and mortality increase with each new intra-abdominal procedure? Each time the belly is opened there is new scar, with increased likelihood of adhesions and potential for future bowel obstruction. Consider these risks when counseling regarding route of delivery. Risk of uterine rupture appears to be higher in trials of labor (and confers a statistically significant but small increase in morbidity but not mortality). However, the uterine scar can silently fail without labor—as is sometimes discovered at a scheduled repeat section, usually without untoward effects on mother or fetus.
Remember that you are sending a young woman home with a new baby to care for (along with other children) and a major abdominal procedure (through an old scar) to recover from, which one could certainly define as morbidity. Cesarean section is an important tool, but we must be careful to practice best possible care and consider all patient factors and preferences. And data are still lacking to support the notion that VBAC is unsafe.
Evidence summary
Contrary to the goals of Healthy People 2010, the rate of cesarean sections is increasing.1 The repeat cesarean rate for low-risk women of all ages and racial groups is now 88.7%, the highest rate since the Centers for Disease Control and Prevention (CDC) began tracking the statistic in 1989. Is VBAC safe, or is a trial of labor no longer supported by the data?
The most recent Cochrane Review found that both VBAC and repeat lowtransverse cesarean section have benefits and risks associated with them; however, after reviewing the limited data, they concluded that no trial exists to adequately help women and their caregivers make an informed decision between the two.2 A strong theme in the Cochrane Review, echoed in most reviews, was the absence of high-quality prospective randomized data.
In an attempt to quantify the risks of VBAC, a systematic review determined that attempted VBAC, compared with repeat low-transverse cesarean section, increased the risk of uterine rupture by 2.7 per 1000 cases (95% confidence interval [CI], 0.73–4.73).3 This additional risk rate is often quoted in VBAC reviews and was cited in the Agency for Healthcare Research and Quality evidence report; it is based on 1 prospective, nonrandomized cohort trial and 1 retrospective cohort study.4,5
No randomized controlled trials exist for determining maternal safety of VBAC, although another recent systematic review found 2 nonrandomized prospective trials of sufficient quality to analyze. The authors concluded there were “no statistically significant differences between planned elective repeat cesarean section and planned VBAC.”6 Upon closer review in PubMed, one of the cited studies did not study 312 patients for VBAC outcomes as alleged; rather, it investigated patient attitudes towards VBAC.7
Since publication of that review, a large, multicenter, prospective, nonrandomized trial involving 33,699 patients found no significant difference between VBAC and planned cesarean for hysterectomy (0.2% vs 0.3%; odds ratio [OR]=0.77; 95% CI, 0.51–1.17), maternal death (0.02% vs 0.04%; OR=0.38; 95% CI, 0.1–1.46), and neonatal death (0.08% vs 0.05%; OR=1.82; 95% CI, 0.73–4.57).8 Significant associations were found for uterine rupture rates in spontaneous labor (24/6685 [0.4%] vs no cases; number needed to harm [NNH]=279) and neonatal hypoxic-ischemic encephalopathy (0.46 cases per 1000 vs no cases; NNH=2174).8
A retrospective Canadian cohort trial of 308,755 women also demonstrated an association of VBAC with uterine rupture(0.65% of trial-of-labor cases; OR=2.38; 95% CI, 2.12–2.67), and a trend towards higher maternal mortality in the cesarean group (1.6 per 100,000 for VBAC vs 5.6 per 100,000 for planned cesarean; OR=0.32; 95% CI, 0.07–1.47).9
The effect of VBAC on neonatal morbidity and mortality is unclear. In contrast to the negative larger trial,8 a smaller retrospective cohort of 24,529 births found a higher association of perinatal death for trial of labor (adjusted OR=11.7; 95% CI, 1.4–101.6).10 The perinatal death rate was similar to rates in nulliparous women. Regarding morbidity, one retrospective cohort trial showed VBAC was associated with an increase in neonatal sepsis (1% vs 0%; CI not given) compared with planned cesarean, but VBAC resulted in less transient tachypnea (5% vs 7%) and hyper-bilirubinemia (2% vs 6%).11
Recommendations from others
Both the American College of Obstetricians and Gynecologists and the Society of Obstetricians and Gynecologists of Canada state that women with 1 previous low-transverse cesarean section should be offered a trial of labor after appropriate counseling of the risks and benefits.12,13 Furthermore, induction with oxytocin is allowed, but the use of prostaglandins is not recommended. Based on expert opinion, both organizations encourage VBAC only in institutions staffed with surgeons and anesthesiologists immediately available to provide emergent cesarean.
Acknowledgments
The opinions and assertions contained herein are the private views of the author and are not to be construed as official, or as reflecting the views of the US Air Force medical department or the US Air Force at large.
1. Menacker F. Trends in cesarean rates for first births and repeat cesarean rates for low-risk women: United States, 1990-2003. Natl Vital Stat Rep 2005;54:1-8.
2. Dodd J, Crowther C, Huertas E, Guise J, Horey D. Planned elective repeat caesarean section versus planned vaginal birth for women with a previous caesarean birth. Cochrane Database Syst Rev 2005;(4):CD004224.
3. Guise J, McDonagh M, Osterweil P, Nygren P, Chan B, Helfand M. Systematic review of the incidence and consequences of uterine rupture in women with previous caesarean section. BMJ 2004;329:19-25.
4. Vaginal Birth After Cesarean (VBAC). Summary. Evidence Report/Technology Assessment, No. 71. AHRQ publication 03-E017. Rockville, Md: Agency for Healthcare Research and Quality; 2003. Available at: www.ahrq.gov/clinic/epcsums/vbacsum.htm. Accessed on January 9, 2006.
5. McMahon MJ, Luther ER, Bowes WA, Olshan AF. Comparison of a trial of labor with an elective second cesarean section. N Engl J Med 1996;335:689-695.
6. Dodd J, Crowther C. Vaginal birth after Caesarean versus elective repeat Caesarean for women with a single prior Caesarean birth: a systematic review of the literature. Aust N Z J Obstet Gynaecol 2004;44:387-391.
7. Abitbol MM, Castillo I, Taylor UB, Rochelson BL, Shmoys S, Monheit AG. Vaginal birth after cesarean section: the patient’s point of view. Am Fam Physician 1993;47:129-134.
8. Landon M, Hauth J, Leveno K, et al. for the National Institute of Child Health and Human Development Maternal-Fetal Medicine Units Network. Maternal and perinatal outcomes associated with a trial of labor after prior cesarean delivery. N Engl J Med 2004;351:2581-2589.
9. Wen S, Rusen I, Walker M, et al. Comparison of maternal mortality and morbidity between trial of labor and elective cesarean section among women with previous cesarean delivery. Am J Obstet Gynecol 2004;191:1263-1269.
10. Smith G, Pell J, Cameron A, Dobbie R. Risk of perinatal death associated with labor after previous cesarean delivery in uncomplicated term pregnancies. JAMA 2002;287:2684-2690.
11. Hook B, Kiwi R, Amini S, Fanaroff A, Hack M. Neonatal morbidity after elective repeat cesarean section and trial of labor. Pediatrics 1997;100:348-353.
12. American College of Obstetricians and Gynecologists Committee on Practice Bulletins—Obstetrics. ACOG Practice Bulletin. Vaginal Birth After Cesarean Delivery. Obstet Gynecol 2004;104:203-212.
13. Martel M, MacKinnon C, and the Clinical Practice Obstetrics Committee, Society of Obstetricians and Gynaecologists of Canada. Guidelines for vaginal birth after previous Caesarean birth. J Obstet Gynaecol Can 2005;27:164-188.
1. Menacker F. Trends in cesarean rates for first births and repeat cesarean rates for low-risk women: United States, 1990-2003. Natl Vital Stat Rep 2005;54:1-8.
2. Dodd J, Crowther C, Huertas E, Guise J, Horey D. Planned elective repeat caesarean section versus planned vaginal birth for women with a previous caesarean birth. Cochrane Database Syst Rev 2005;(4):CD004224.
3. Guise J, McDonagh M, Osterweil P, Nygren P, Chan B, Helfand M. Systematic review of the incidence and consequences of uterine rupture in women with previous caesarean section. BMJ 2004;329:19-25.
4. Vaginal Birth After Cesarean (VBAC). Summary. Evidence Report/Technology Assessment, No. 71. AHRQ publication 03-E017. Rockville, Md: Agency for Healthcare Research and Quality; 2003. Available at: www.ahrq.gov/clinic/epcsums/vbacsum.htm. Accessed on January 9, 2006.
5. McMahon MJ, Luther ER, Bowes WA, Olshan AF. Comparison of a trial of labor with an elective second cesarean section. N Engl J Med 1996;335:689-695.
6. Dodd J, Crowther C. Vaginal birth after Caesarean versus elective repeat Caesarean for women with a single prior Caesarean birth: a systematic review of the literature. Aust N Z J Obstet Gynaecol 2004;44:387-391.
7. Abitbol MM, Castillo I, Taylor UB, Rochelson BL, Shmoys S, Monheit AG. Vaginal birth after cesarean section: the patient’s point of view. Am Fam Physician 1993;47:129-134.
8. Landon M, Hauth J, Leveno K, et al. for the National Institute of Child Health and Human Development Maternal-Fetal Medicine Units Network. Maternal and perinatal outcomes associated with a trial of labor after prior cesarean delivery. N Engl J Med 2004;351:2581-2589.
9. Wen S, Rusen I, Walker M, et al. Comparison of maternal mortality and morbidity between trial of labor and elective cesarean section among women with previous cesarean delivery. Am J Obstet Gynecol 2004;191:1263-1269.
10. Smith G, Pell J, Cameron A, Dobbie R. Risk of perinatal death associated with labor after previous cesarean delivery in uncomplicated term pregnancies. JAMA 2002;287:2684-2690.
11. Hook B, Kiwi R, Amini S, Fanaroff A, Hack M. Neonatal morbidity after elective repeat cesarean section and trial of labor. Pediatrics 1997;100:348-353.
12. American College of Obstetricians and Gynecologists Committee on Practice Bulletins—Obstetrics. ACOG Practice Bulletin. Vaginal Birth After Cesarean Delivery. Obstet Gynecol 2004;104:203-212.
13. Martel M, MacKinnon C, and the Clinical Practice Obstetrics Committee, Society of Obstetricians and Gynaecologists of Canada. Guidelines for vaginal birth after previous Caesarean birth. J Obstet Gynaecol Can 2005;27:164-188.
Evidence-based answers from the Family Physicians Inquiries Network