Clinical Review

Assessing preterm birth risk: from bulletin to bedside

OBG Manag. 2002 March;14(3):41-58

Weighing in on the key messages from ACOG’s recent Practice Bulletin, Errol Norwitz, MD, PhD, reviews the evidence on the utility of preterm birth screening modalities, including cervical ultrasound, fetal fibronectin, salivary estriol, and home uterine-activity monitoring.

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References

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2. American College of Obstetricians and Gynecologists. Assessment of risk for preterm birth. ACOG Practice Bulletin #31. Washington, DC: ACOG; October 2001.

3. American College of Obstetricians and Gynecologists. Preterm labor. ACOG Technical Bulletin #206. Washington, DC: ACOG; June 1995.

4. American College of Obstetricians and Gynecologists. Home uterineactivity monitoring. ACOG Committee Opinion #172. Washington, DC: ACOG; May 1996.

5. American College of Obstetricians and Gynecologists. SalEst’ as a predictor of risk for preterm labor. ACOG Committee Opinion #251. Washington, DC: ACOG; January 2001.

6. American College of Obstetricians and Gynecologists. Fetal fibronectin preterm labor risk test. ACOG Committee Opinion #187. Washington, DC: ACOG; September 1997.

7. American College of Obstetricians and Gynecologists. Bacterial vaginosis screening for prevention of preterm delivery. ACOG Committee Opinion #198. Washington, DC: ACOG; February 1998.

8. Iams JD, Johnson FF, O’Shaughnessy RW. A prospective random trial of home uterine activity monitoring in pregnancies at increased risk of preterm labor. Am J Obstet Gynecol. 1988;159:595-603.

9. Grimes DA, et al. Randomized controlled trials of home uterine activity monitoring: a review and critique. Obstet Gynecol. 1992;79:137-142.

10. Sachs BP, Hellerstein S, Freeman R, et al. Home monitoring of uterine activity. Does it prevent prematurity? N Engl J Med. 1991;325:1374-1377.

11. US. Preventative Services Task Force. Home uterine activity monitoring for preterm labor. Review article. JAMA. 1993;270:371-376.

12. Hanssens MC, Selby C, Symonds EM. Sex steroid hormone concentrations in preterm labour and the outcome of treatment with ritodrine. Br J Obstet Gynaecol. 1985;92:698-702.

13. Goodwin TM. A role for estriol in human labor, term and preterm. Am J Obstet Gynecol. 1999;180:S208-213.

14. Norwitz ER, et al. The control of labor. N Engl J Med. 1999;341:660-666.

15. Voss HF. Saliva as a fluid for measurement of estriol levels. Am J Obstet Gynecol. 1999;180:S226-231.

16. McGregor JA, Jackson GM, Lachlin GC, et al. Salivary estriol as risk assessment for preterm labor: a prospective trial. Am J Obstet Gynecol. 1995;173:1337-1342.

17. Heine RP, McGregor JA, Dullien VK. Accuracy of salivary estriol testing compared to traditional risk factor assessment in predicting preterm birth. Am J Obstet Gynecol. 1999;180:S214-218.

18. McGregor JA, et al. Diurnal variation in salivary estriol level during pregnancy: a pilot study. Am J Obstet Gynecol. 1999;180:S223-225.

19. Hendershott CM, Dullien V, Goodwin TM. Serial betamethasone administration: effect on maternal salivary estriol levels. Am J Obstet Gynecol. 1999;180:S219-222.

20. Goldenberg RL, et al. The preterm prediction study: cervical lactoferrin concentration, other markers of lower genital tract infection, and preterm birth. National Institute of Child Health and Human Development Maternal-Fetal Medicine Network. Am J Obstet Gynecol. 2000;182:631-635.

21. Berg AO. Screening for bacterial vaginosis in pregnancy. Recommendations and rationale. Am J Prev Med. 2001;20:59-61.

22. Brocklehurst P, Hannah M, McDonald H. Interventions for treating bacterial vaginosis in pregnancy (Cochrane Review). In: The Cochrane Library. Issue 2, 2001. Oxford: Update Software.

23. Morales WJ, et al. Effect of metronidazole in patients with preterm birth in preceding pregnancy and bacterial vaginosis: a placebo-controlled, double-blind study. Am J Obstet Gynecol. 1994;171:345-347.

24. Hauth JC, Goldenberg RL, Andrews WW, et al. Reduced incidence of preterm delivery with metronidazole and erythromycin in women with bacterial vaginosis. N Engl J Med. 1995;333:1732-1736.

25. McGregor JA, et al. Bacterial vaginosis is associated with prematurity and vaginal fluid mucinase and sialidase: results of a controlled trial of topical clindamycin cream. Am J Obstet Gynecol. 1994;170:1048-1059.

26. Creasy RK, Gummer BA, Liggins GC. System for predicting spontaneous preterm birth. Am J Obstet Gynecol. 1980;55:692-695.

27. Mercer BM, et al. The preterm prediction study: a clinical risk assessment system. Am J Obstet Gynecol. 1996;174:1885-1893.

28. Norwitz ER, Repke JT, Greene M. Cervical cerclage—elective and emergent. ACOG Update. 1999;24:1-11.

29. Mortensen OA, Franklin J, Lofstrand T, et al. Prediction of preterm birth. Acta Obstet Gynecol Scand. 1987;66:507-511.

30. Iams JD, Goldenberg RL, Meis PJ, et al. The length of the cervix and the risk of spontaneous premature delivery. N Engl J Med. 1996;334:567-572.

31. Heath VCF, Southall TR, Souka AP, et al. Cervical length at 23 weeks of gestation: prediction of spontaneous preterm delivery. Ultrasound Obstet Gynaecol. 1998;12:312-317.

32. SOGC Clinical Practice Guidelines 102: Ultrasound Cervical Assessment in Predicting Preterm Birth Ottawa, Ontario: Society of Obstetricians and Gynaecologists of Canada; 2001.

33. Lockwood CJ, et al. Fetal fibronectin in cervical and vaginal secretions as a predictor of preterm delivery. N Engl J Med. 1991;325:669-674.

34. Goldenberg RL, et al. The preterm prediction study: fetal fibronectin testing and spontaneous preterm birth. Obstet Gynecol. 1996;87:643-648.

35. Iams JD, et al. Fetal fibronectin improves the accuracy of diagnosis of preterm labor. Am J Obstet Gynecol. 1995;173:141-145.

36. Kurtzman JT, et al. Transvaginal versus transperineal ultrasonography: a blinded comparison in the assessment of cervical length at midgestation. Am J Obstet Gynecol. 1998;179:852-857.

37. Okitsu O, et al. Early prediction of preterm delivery by transvaginal ultrasonography. Ultrasound Obstet Gynecol. 1992;2:402-405.

38. Leituch H, Brunbauer M, Kaider A, Egarter C, Husslein P. Cervical length and dilatation of the internal cervical os detected by vaginal ultrasonography as markers for preterm delivery: a systematic review. Am J Obstet Gynecol. 1999;181:1465-1472.

39. Iams JD, Paraskos J, Landon MB, Teteris JN, Johnson FF. Cervical sonography in preterm labor. Obstet Gynecol. 1994;84:40-46.

40. Guzman ER, Rosenberg JC, Houlihan C, et al. A new method using vaginal ultrasound and transfundal pressure to evaluate the asymptomatic incompetent cervix. Obstet Gynecol. 1994;83:248-252.

41. Guzman ER, Vintzileos AM, McLean DA, et al. The natural history of a positive response to transfundal pressure in women at risk for cervical incompetence. Am J Obstet Gynecol. 1997;176:634-638.

42. Yost NP, et al. Pitfalls in ultrasonic cervical length measurement for predicting preterm birth. Obstet Gynecol. 1999;93:510-516.

43. Arabin B, et al. Maternal position and ultrasonic cervical assessment in multiple pregnancy. J Reprod Med. 1997;42:719-724.

44. Iams JD, Goldenberg RL, Mercer BM, et al. The preterm prediction study: recurrence risk of spontaneous preterm birth. National Institute of Child Health and Human Development Maternal-Fetal Medicine Network. Am J Obstet Gynecol. 1998;178:1035-1040.

45. Goldenberg RL, et al. The preterm prediction study: patterns of cervicovaginal fetal fibronectin as predictors of spontaneous preterm birth. National Institute of Child Health and Human Development Maternal-Fetal Medicine Network. Am J Obstet Gynecol. 1997;177:8-12.

46. Joffe GM, et al. Impact of the fetal fibronectin assay on admission for preterm labor. Am J Obstet Gynecol. 1999;180:581-586.

47. Giles W, Bisits A, Knox M, Madsen G, Smith R. The effect of fetal fibronectin testing on admissions to a tertiary maternal-fetal medicine unit and cost savings. Am J Obstet Gynecol. 2000;182:439-442.

48. Mercer BM, et al. Antimicrobial therapy in expectant management of P-PROM. Lancet. 1995;346:1271-1279.

49. Locksmith G, Duff P. Infection, antibiotics, and preterm delivery. Seminars in Perinatology. 2001;25:295-309.

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In much of medicine, the ability to identify which patients are at increased risk for a disease or health-threatening event is half the battle, as it paves the way for timely preventive intervention. As obstetricians know all too well, however, that’s hardly the case with preterm delivery (PTD). While recent years have seen significant advances in screening modalities, those gains have not been matched by comparable improvements in our ability to prevent premature birth. In fact, instead of decreasing, the incidence of PTD in the United States has increased from 9.4% of births in 1981 to 11.8% in 1999.¹

While the search for effective interventions continues, obstetricians and their patients still can derive considerable benefit from the enhanced ability to determine which women with worrisome symptoms are at low risk of PTD, thus avoiding costly and potentially harmful interventions, and which patients warrant heightened surveillance.

In October 2001, ACOG reviewed various modalities in its Practice Bulletin titled “Assessment of risk for preterm birth.” Here, Dr. Norwitz, assistant professor of obstetrics, gynecology, and reproductive sciences at Harvard Medical School and an attending Ob/Gyn in the division of maternal-fetal medicine at Brigham and Women’s Hospital in Boston, responds to OBG Management editors’ questions about the clinical implications of the bulletin and the screens and tests it discusses.

<huc>Q</huc> OBG Management: In what ways does this bulletin represent an evolution in the specialty’s thinking about preterm labor?

<huc>A</huc> NORWITZ: It represents an attempt by ACOG to synthesize the extensive and rapidly expanding body of literature on risk factors for PTD into a single, succinct, and practical document.² As such, it replaces prior ACOG publications on preterm labor,³ home uterine-activity monitoring (HUAM),⁴ salivary estriol testing,⁵ fetal fibronectin (fFN) testing,⁶ and bacterial vaginosis (BV) screening and treatment.⁷ However, the current Practice Bulletin is a far less ambitious document than the prior review of preterm labor,³ which dealt not only with risk factors for preterm irth, but also with its management.

Nonetheless, it represents an evolution in thinking about preterm birth, as it includes a detailed discussion of fetal fibronectin screening and sonographic assessment of cervical length.

<huc>Q</huc> OBG Management: According to the bulletin, “There are no current data to support the use of salivary estriol, HUAM, or BV screening as strategies to identify or prevent preterm birth.” How widely are each of these modalities being employed by Ob/Gyns? What impact do you see this statement having on their future use?

<huc>A</huc> NORWITZ: HUAM testing had largely fallen by the wayside even before this bulletin was published. Most obstetric-care providers were already aware of the extensive literature showing that HUAM does not prevent preterm birth or improve perinatal outcome.^8-11

As for salivary estriol, the development of a reliable endocrine assay to predict PTD would represent a significant advance in the field. Progesterone withdrawal is not a prerequisite for labor; nor are serum progesterone levels or progesterone/17ß-estradiol ratios predictive of preterm birth.^12,1

Lower-genital-tract BV may be a marker of upper-genital-tract infection, which in turn may be the real cause of preterm birth.

On the other hand, maternal serum estriol levels accurately reflect activation of the fetal hypothalamic-pituitary-adrenal axis, which occurs in all women prior to the onset of labor, both at term and preterm.^13,14 More-over, salivary estriol measurements correlate well with levels of biologically active (unconjugated) estriol in the circulation.¹⁵ The detection of elevated levels of estriol (≥2.1 ng/mL) in maternal saliva is predictive of delivery prior to 37 weeks in a high-risk population, with a sensitivity of 68% to 87% and a specificity of 77%.^16,17 Serial (weekly) measurements have been shown to be more accurate in predicting preterm birth than a single measurement.¹⁷

However, salivary estriol testing to identify women at high risk of PTD has not been widely accepted. The reasons: First, maternal estriol levels show diurnal variation, peaking at night,¹⁸ making it difficult to standardize such testing. Additionally, the false-positive rate of 23% to 35% is considered unacceptably high and may lead to unnecessary intervention.^16,17 Finally, salivary estriol levels may be suppressed by betamethasone administration, making the test unreliable in patients treated with corticosteroids.¹⁹ The statement in the latest ACOG bulletin that “trials with salivary estriol testing to predict preterm birth have failed to establish its usefulness for anything more than investigational purposes at present”² is likely to further limit the use of this test, and may have the unfortunate effect of discouraging future research in the field.

In regard to BV, recent data demonstrate conclusively that screening and treating low-risk asymptomatic pregnant women for BV does not prevent preterm birth.^20-22 However, the data for women at high risk for preterm birth are conflicting. Some studies suggest that the strategy of screening and treating asymptomatic BV in high-risk women may significantly decrease the incidence of preterm birth and low-birthweight infants.^22-24 But the statement by ACOG that “there are insufficient data to suggest screening and treating women at…high risk will reduce the overall rate of preterm birth”² is likely to limit the use of this strategy. The hypothesis that lower-genital-tract BV may be a marker of upper-genital-tract infection, which in turn is the real cause of preterm labor and delivery, is intriguing and deserves further attention.