How can pregnant women safely relieve low-back pain?

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How can pregnant women safely relieve low-back pain?
EVIDENCE-BASED ANSWER

ACETAMINOPHEN IS SAFE for use in pregnancy but lacks evidence of efficacy (strength of recommendation [SOR]: C, usual practice).

Both physical therapy and water aerobics reduce sick days caused by low-back pain (strength of recommendation [SOR]: B, randomized controlled trial [RCT]). Acupuncture, including auricular acupuncture, also relieves low-back pain and improves function (SOR: B, 2 RCTs).

Osteopathic manipulative therapy (OMT) slightly improves disability (SOR: B, RCT).

Corticosteroid injection at the sacrospinous ligament insertion decreases pain (SOR: B, RCT).

Insufficient evidence of efficacy exists for support garments (SOR: B, systematic review).

No serious maternal or fetal adverse effects have been reported with any of these therapies.

 

Evidence summary

Even though clinical research is lacking, acetaminophen is widely used to relieve low-back pain with no documented teratogenic effect (US Food and Drug Administration [FDA] category B). Nonsteroidal anti-inflammatory drugs are classified as FDA category D in the third trimester because of their documented association with oligohydramnios, premature closure of the ductus arteriosus, nephrotoxicity, and periventricular hemorrhage in the fetus.1 Opioids are category C and a poor choice to treat low-back pain in pregnancy.2

Physical therapy and water aerobics relieve pain, reduce sick days
A 2007 Cochrane review of interventions for treating back pain in pregnancy analyzed 8 studies with a total of 1305 patients that examined the effects of adding physical therapy and acupuncture to usual care.3 In one RCT, 407 patients with and without pain received 5 30-minute individualized physical therapy exercise sessions, 2 45-minute group physical therapy classes, or standard care.3,4 Low-back pain decreased with group physical therapy (P<.05; number needed to treat [NNT] = 3.2) and individual therapy (NNT = 2.1). Patients who received individual therapy had a 12% decrease in sick days.

A prospective trial of 258 patients, half of whom did water aerobics and half physical therapy, showed comparable results for the 2 interventions (NNT = 11.4 for decreased sick days; odds ratio = 0.38, 95% confidence interval [CI], 0.16-0.88).3

Acupuncture reduces pain and analgesic use
A prospective, randomized open study cited in the 2007 Cochrane review divided 72 patients at 24 to 37 weeks’ gestational age into a group that received acupuncture plus standard care and a standard-care-only control group.3,5 Treatment sessions occurred one or 2 times per week until delivery or recovery. The acupuncture group reported decreased pain (60% vs 14% for controls; P<.01; NNT = 2.2) and improved function (43% vs 9% for controls; P<.001; NNT = 2.9). There was also a difference in analgesic use: 0% for the acupuncture group vs 14% for controls; P<.05; NNT = 7.1.

A 2009 RCT divided 159 patients at 25 to 38 weeks’ gestational age into 3 groups: auricular acupuncture at specific points for one week, sham auricular acupuncture at nonspecific points for one week, and controls. At the end of Week 1, 80% of the acupuncture group had a clinically significant reduction in pain compared with 56% in the sham acupuncture group and 36% in the control group (P = .001 acupuncture vs sham, NNT = 4.2; P<.0001 acupuncture vs controls, NNT = 2.3).6

Osteopathic manipulative therapy (OMT) decreases disability, but not pain
A 2010 RCT divided 144 third trimester patients into 3 groups that received usual obstetric care, sham ultrasound therapy plus usual obstetric care, or OMT.7 Pain remained similar among the 3 groups throughout the study. Using the 24-point Roland-Morris Disability Questionnaire, OMT decreased disability by 0.72 points (95% CI, 0.31-1.14; P<.001) compared with 0.35 points in the usual obstetric-care-only group (95% CI, –0.06 to 0.76; P = .09). Ultrasound had no effect.

Corticosteroid injection reduces pain in a small trial
A small RCT of injection with the corticosteroid triamcinolone at the sacrospinous ligament insertion in 36 women with low-back pain showed significant reduction in pain in 17 of 18 women in the triamcinolone group compared with 9 of 18 women in the control group (P<.01; NNT = 2).8

Evidence lacking on maternity support garments
A poor-quality systematic review of 10 studies (N = 1909) of maternity support garments found insufficient evidence because of the heterogeneity of the trials.9

Recommendations

The American College of Obstetricians and Gynecologists suggests the following measures to prevent and treat low-back pain in pregnancy:10

  • wear low-heeled (not flat) shoes with good arch support
  • get help when lifting heavy objects
  • place one foot on a stool or box when standing for long periods
  • place a board between the mattress and box spring if the bed is too soft
  • squat down, bend knees, and keep back straight when lifting
  • sit in chairs with good back support or use a small pillow to provide support
  • sleep on side with pillows between knees for support
  • apply heat, cold, or massage to the painful area.
References

1. Black RA, Hill DA. Over-the-counter medications in pregnancy. Am Fam Physician. 2003;67:2517-2524.

2. Vermani E, Mittal R, Weeks A. Pelvic girdle pain and low back pain in pregnancy: a review. Pain Pract. 2010;10:60-71.

3. Pennick VE, Young G. Interventions for preventing and treating pelvic and back pain in pregnancy. Cochrane Database Syst Rev. 2007;(2):CD001139.-

4. Ostgaard HC, Zetherstrom G, Roos-Hansson E, et al. Reduction of back and posterior pelvic pain in pregnancy. Spine. 1994;19:894-900.

5. Kvorning N, Holmberg C, Grennert L, et al. Acupuncture relieves pelvic and low back pain in late pregnancy. Acta Obstet Gynecol Scand. 2004;83:246-250.

6. Wang SM, Dezinno P, Lin EC, et al. Auricular acupuncture as a treatment for pregnant women who have low back and posterior pelvic pain: a pilot study. Am J Obstet Gynecol. 2009;201:271.e1-271.e9.

7. Licciardone JC, Buchanan S, Hensel KL, et al. Osteopathic manipulative treatment of back pain and related symptoms during pregnancy: a randomized controlled trial. Am J Obstet Gynecol. 2010;202:43.e1-43.e8.

8. Torstensson T, Lindgren A, Kristiansson P. Corticosteroid injection treatment to the ischiadic spine reduced pain in women with long-lasting sacral low back pain with onset during pregnancy: a randomized, double blind, controlled trial. Spine. 2009;34:2254-2258.

9. Ho SS, Yu WW, Lao TT, et al. Effectiveness of maternity support belts in reducing low back pain during pregnancy: a review. J Clin Nurs. 2009;18:1523-1532.

10. American College of Obstetricians and Gynecologists. Patient education guidelines for easing back pain during pregnancy. August 2011. Available at: http://www.acog.org/~/media/For%20Patients/faq115.pdf?dmc=1&ts=20130118T1434071958. Accessed December 10, 2012.

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Roselyn Jan W. Clemente-Fuentes, MD
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Heather Pickett, DO
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Misty Carney, MLIS
Stimson Library, Fort Sam Houston, Tex

ASSISTANT EDITOR
Paul Crawford, MD
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

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Roselyn Jan W. Clemente-Fuentes; MD; Heather Pickett; DO; Misty Carney; MLIS; acetaminophen; pregnancy; physical therapy; water aerobics; auricular acupuncture; osteopathic manipulative therapy; OMT
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Roselyn Jan W. Clemente-Fuentes, MD
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Heather Pickett, DO
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Misty Carney, MLIS
Stimson Library, Fort Sam Houston, Tex

ASSISTANT EDITOR
Paul Crawford, MD
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Author and Disclosure Information

Roselyn Jan W. Clemente-Fuentes, MD
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Heather Pickett, DO
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

Misty Carney, MLIS
Stimson Library, Fort Sam Houston, Tex

ASSISTANT EDITOR
Paul Crawford, MD
Nellis Family Medicine Residency, Nellis Air Force Base, Nev

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EVIDENCE-BASED ANSWER

ACETAMINOPHEN IS SAFE for use in pregnancy but lacks evidence of efficacy (strength of recommendation [SOR]: C, usual practice).

Both physical therapy and water aerobics reduce sick days caused by low-back pain (strength of recommendation [SOR]: B, randomized controlled trial [RCT]). Acupuncture, including auricular acupuncture, also relieves low-back pain and improves function (SOR: B, 2 RCTs).

Osteopathic manipulative therapy (OMT) slightly improves disability (SOR: B, RCT).

Corticosteroid injection at the sacrospinous ligament insertion decreases pain (SOR: B, RCT).

Insufficient evidence of efficacy exists for support garments (SOR: B, systematic review).

No serious maternal or fetal adverse effects have been reported with any of these therapies.

 

Evidence summary

Even though clinical research is lacking, acetaminophen is widely used to relieve low-back pain with no documented teratogenic effect (US Food and Drug Administration [FDA] category B). Nonsteroidal anti-inflammatory drugs are classified as FDA category D in the third trimester because of their documented association with oligohydramnios, premature closure of the ductus arteriosus, nephrotoxicity, and periventricular hemorrhage in the fetus.1 Opioids are category C and a poor choice to treat low-back pain in pregnancy.2

Physical therapy and water aerobics relieve pain, reduce sick days
A 2007 Cochrane review of interventions for treating back pain in pregnancy analyzed 8 studies with a total of 1305 patients that examined the effects of adding physical therapy and acupuncture to usual care.3 In one RCT, 407 patients with and without pain received 5 30-minute individualized physical therapy exercise sessions, 2 45-minute group physical therapy classes, or standard care.3,4 Low-back pain decreased with group physical therapy (P<.05; number needed to treat [NNT] = 3.2) and individual therapy (NNT = 2.1). Patients who received individual therapy had a 12% decrease in sick days.

A prospective trial of 258 patients, half of whom did water aerobics and half physical therapy, showed comparable results for the 2 interventions (NNT = 11.4 for decreased sick days; odds ratio = 0.38, 95% confidence interval [CI], 0.16-0.88).3

Acupuncture reduces pain and analgesic use
A prospective, randomized open study cited in the 2007 Cochrane review divided 72 patients at 24 to 37 weeks’ gestational age into a group that received acupuncture plus standard care and a standard-care-only control group.3,5 Treatment sessions occurred one or 2 times per week until delivery or recovery. The acupuncture group reported decreased pain (60% vs 14% for controls; P<.01; NNT = 2.2) and improved function (43% vs 9% for controls; P<.001; NNT = 2.9). There was also a difference in analgesic use: 0% for the acupuncture group vs 14% for controls; P<.05; NNT = 7.1.

A 2009 RCT divided 159 patients at 25 to 38 weeks’ gestational age into 3 groups: auricular acupuncture at specific points for one week, sham auricular acupuncture at nonspecific points for one week, and controls. At the end of Week 1, 80% of the acupuncture group had a clinically significant reduction in pain compared with 56% in the sham acupuncture group and 36% in the control group (P = .001 acupuncture vs sham, NNT = 4.2; P<.0001 acupuncture vs controls, NNT = 2.3).6

Osteopathic manipulative therapy (OMT) decreases disability, but not pain
A 2010 RCT divided 144 third trimester patients into 3 groups that received usual obstetric care, sham ultrasound therapy plus usual obstetric care, or OMT.7 Pain remained similar among the 3 groups throughout the study. Using the 24-point Roland-Morris Disability Questionnaire, OMT decreased disability by 0.72 points (95% CI, 0.31-1.14; P<.001) compared with 0.35 points in the usual obstetric-care-only group (95% CI, –0.06 to 0.76; P = .09). Ultrasound had no effect.

Corticosteroid injection reduces pain in a small trial
A small RCT of injection with the corticosteroid triamcinolone at the sacrospinous ligament insertion in 36 women with low-back pain showed significant reduction in pain in 17 of 18 women in the triamcinolone group compared with 9 of 18 women in the control group (P<.01; NNT = 2).8

Evidence lacking on maternity support garments
A poor-quality systematic review of 10 studies (N = 1909) of maternity support garments found insufficient evidence because of the heterogeneity of the trials.9

Recommendations

The American College of Obstetricians and Gynecologists suggests the following measures to prevent and treat low-back pain in pregnancy:10

  • wear low-heeled (not flat) shoes with good arch support
  • get help when lifting heavy objects
  • place one foot on a stool or box when standing for long periods
  • place a board between the mattress and box spring if the bed is too soft
  • squat down, bend knees, and keep back straight when lifting
  • sit in chairs with good back support or use a small pillow to provide support
  • sleep on side with pillows between knees for support
  • apply heat, cold, or massage to the painful area.
EVIDENCE-BASED ANSWER

ACETAMINOPHEN IS SAFE for use in pregnancy but lacks evidence of efficacy (strength of recommendation [SOR]: C, usual practice).

Both physical therapy and water aerobics reduce sick days caused by low-back pain (strength of recommendation [SOR]: B, randomized controlled trial [RCT]). Acupuncture, including auricular acupuncture, also relieves low-back pain and improves function (SOR: B, 2 RCTs).

Osteopathic manipulative therapy (OMT) slightly improves disability (SOR: B, RCT).

Corticosteroid injection at the sacrospinous ligament insertion decreases pain (SOR: B, RCT).

Insufficient evidence of efficacy exists for support garments (SOR: B, systematic review).

No serious maternal or fetal adverse effects have been reported with any of these therapies.

 

Evidence summary

Even though clinical research is lacking, acetaminophen is widely used to relieve low-back pain with no documented teratogenic effect (US Food and Drug Administration [FDA] category B). Nonsteroidal anti-inflammatory drugs are classified as FDA category D in the third trimester because of their documented association with oligohydramnios, premature closure of the ductus arteriosus, nephrotoxicity, and periventricular hemorrhage in the fetus.1 Opioids are category C and a poor choice to treat low-back pain in pregnancy.2

Physical therapy and water aerobics relieve pain, reduce sick days
A 2007 Cochrane review of interventions for treating back pain in pregnancy analyzed 8 studies with a total of 1305 patients that examined the effects of adding physical therapy and acupuncture to usual care.3 In one RCT, 407 patients with and without pain received 5 30-minute individualized physical therapy exercise sessions, 2 45-minute group physical therapy classes, or standard care.3,4 Low-back pain decreased with group physical therapy (P<.05; number needed to treat [NNT] = 3.2) and individual therapy (NNT = 2.1). Patients who received individual therapy had a 12% decrease in sick days.

A prospective trial of 258 patients, half of whom did water aerobics and half physical therapy, showed comparable results for the 2 interventions (NNT = 11.4 for decreased sick days; odds ratio = 0.38, 95% confidence interval [CI], 0.16-0.88).3

Acupuncture reduces pain and analgesic use
A prospective, randomized open study cited in the 2007 Cochrane review divided 72 patients at 24 to 37 weeks’ gestational age into a group that received acupuncture plus standard care and a standard-care-only control group.3,5 Treatment sessions occurred one or 2 times per week until delivery or recovery. The acupuncture group reported decreased pain (60% vs 14% for controls; P<.01; NNT = 2.2) and improved function (43% vs 9% for controls; P<.001; NNT = 2.9). There was also a difference in analgesic use: 0% for the acupuncture group vs 14% for controls; P<.05; NNT = 7.1.

A 2009 RCT divided 159 patients at 25 to 38 weeks’ gestational age into 3 groups: auricular acupuncture at specific points for one week, sham auricular acupuncture at nonspecific points for one week, and controls. At the end of Week 1, 80% of the acupuncture group had a clinically significant reduction in pain compared with 56% in the sham acupuncture group and 36% in the control group (P = .001 acupuncture vs sham, NNT = 4.2; P<.0001 acupuncture vs controls, NNT = 2.3).6

Osteopathic manipulative therapy (OMT) decreases disability, but not pain
A 2010 RCT divided 144 third trimester patients into 3 groups that received usual obstetric care, sham ultrasound therapy plus usual obstetric care, or OMT.7 Pain remained similar among the 3 groups throughout the study. Using the 24-point Roland-Morris Disability Questionnaire, OMT decreased disability by 0.72 points (95% CI, 0.31-1.14; P<.001) compared with 0.35 points in the usual obstetric-care-only group (95% CI, –0.06 to 0.76; P = .09). Ultrasound had no effect.

Corticosteroid injection reduces pain in a small trial
A small RCT of injection with the corticosteroid triamcinolone at the sacrospinous ligament insertion in 36 women with low-back pain showed significant reduction in pain in 17 of 18 women in the triamcinolone group compared with 9 of 18 women in the control group (P<.01; NNT = 2).8

Evidence lacking on maternity support garments
A poor-quality systematic review of 10 studies (N = 1909) of maternity support garments found insufficient evidence because of the heterogeneity of the trials.9

Recommendations

The American College of Obstetricians and Gynecologists suggests the following measures to prevent and treat low-back pain in pregnancy:10

  • wear low-heeled (not flat) shoes with good arch support
  • get help when lifting heavy objects
  • place one foot on a stool or box when standing for long periods
  • place a board between the mattress and box spring if the bed is too soft
  • squat down, bend knees, and keep back straight when lifting
  • sit in chairs with good back support or use a small pillow to provide support
  • sleep on side with pillows between knees for support
  • apply heat, cold, or massage to the painful area.
References

1. Black RA, Hill DA. Over-the-counter medications in pregnancy. Am Fam Physician. 2003;67:2517-2524.

2. Vermani E, Mittal R, Weeks A. Pelvic girdle pain and low back pain in pregnancy: a review. Pain Pract. 2010;10:60-71.

3. Pennick VE, Young G. Interventions for preventing and treating pelvic and back pain in pregnancy. Cochrane Database Syst Rev. 2007;(2):CD001139.-

4. Ostgaard HC, Zetherstrom G, Roos-Hansson E, et al. Reduction of back and posterior pelvic pain in pregnancy. Spine. 1994;19:894-900.

5. Kvorning N, Holmberg C, Grennert L, et al. Acupuncture relieves pelvic and low back pain in late pregnancy. Acta Obstet Gynecol Scand. 2004;83:246-250.

6. Wang SM, Dezinno P, Lin EC, et al. Auricular acupuncture as a treatment for pregnant women who have low back and posterior pelvic pain: a pilot study. Am J Obstet Gynecol. 2009;201:271.e1-271.e9.

7. Licciardone JC, Buchanan S, Hensel KL, et al. Osteopathic manipulative treatment of back pain and related symptoms during pregnancy: a randomized controlled trial. Am J Obstet Gynecol. 2010;202:43.e1-43.e8.

8. Torstensson T, Lindgren A, Kristiansson P. Corticosteroid injection treatment to the ischiadic spine reduced pain in women with long-lasting sacral low back pain with onset during pregnancy: a randomized, double blind, controlled trial. Spine. 2009;34:2254-2258.

9. Ho SS, Yu WW, Lao TT, et al. Effectiveness of maternity support belts in reducing low back pain during pregnancy: a review. J Clin Nurs. 2009;18:1523-1532.

10. American College of Obstetricians and Gynecologists. Patient education guidelines for easing back pain during pregnancy. August 2011. Available at: http://www.acog.org/~/media/For%20Patients/faq115.pdf?dmc=1&ts=20130118T1434071958. Accessed December 10, 2012.

References

1. Black RA, Hill DA. Over-the-counter medications in pregnancy. Am Fam Physician. 2003;67:2517-2524.

2. Vermani E, Mittal R, Weeks A. Pelvic girdle pain and low back pain in pregnancy: a review. Pain Pract. 2010;10:60-71.

3. Pennick VE, Young G. Interventions for preventing and treating pelvic and back pain in pregnancy. Cochrane Database Syst Rev. 2007;(2):CD001139.-

4. Ostgaard HC, Zetherstrom G, Roos-Hansson E, et al. Reduction of back and posterior pelvic pain in pregnancy. Spine. 1994;19:894-900.

5. Kvorning N, Holmberg C, Grennert L, et al. Acupuncture relieves pelvic and low back pain in late pregnancy. Acta Obstet Gynecol Scand. 2004;83:246-250.

6. Wang SM, Dezinno P, Lin EC, et al. Auricular acupuncture as a treatment for pregnant women who have low back and posterior pelvic pain: a pilot study. Am J Obstet Gynecol. 2009;201:271.e1-271.e9.

7. Licciardone JC, Buchanan S, Hensel KL, et al. Osteopathic manipulative treatment of back pain and related symptoms during pregnancy: a randomized controlled trial. Am J Obstet Gynecol. 2010;202:43.e1-43.e8.

8. Torstensson T, Lindgren A, Kristiansson P. Corticosteroid injection treatment to the ischiadic spine reduced pain in women with long-lasting sacral low back pain with onset during pregnancy: a randomized, double blind, controlled trial. Spine. 2009;34:2254-2258.

9. Ho SS, Yu WW, Lao TT, et al. Effectiveness of maternity support belts in reducing low back pain during pregnancy: a review. J Clin Nurs. 2009;18:1523-1532.

10. American College of Obstetricians and Gynecologists. Patient education guidelines for easing back pain during pregnancy. August 2011. Available at: http://www.acog.org/~/media/For%20Patients/faq115.pdf?dmc=1&ts=20130118T1434071958. Accessed December 10, 2012.

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Which combination drug therapies are most effective for hypertension?

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Which combination drug therapies are most effective for hypertension?
EVIDENCE-BASED ANSWER

INSUFFICIENT EVIDENCE exists to determine which specific combinations most effectively decrease cardiovascular morbidity and mortality, although combinations of hypertension medications at lower doses generally reduce cardiovascular outcomes (stroke, coronary heart disease) more than monotherapy (strength of recommendation [SOR]: A, large meta-analyses).

The combination of benazepril and amlodipine reduces the composite endpoint of cardiovascular events and deaths more than benazepril plus hydrochlorothiazide with similar rates of adverse effects (SOR: A, randomized controlled trial [RCT]).

Combining an angiotensin converting enzyme inhibitor (ACE-I) with a thiazide, ß-blocker, or calcium channel blocker produces side effects similar to monotherapy, as does combining an angiotensin receptor blocker (ARB) with a thiazide or calcium channel blocker (SOR: A, meta-analyses). However, an ACE-I combined with an ARB increases the risk of renal complications and death more than monotherapy (SOR: A, RCT).

 

Evidence summary

A meta-analysis of 147 RCTs with a total of 464,000 patients demonstrated better cardiovascular outcomes for combination therapy vs monotherapy among patients 60 to 69 years of age with diastolic blood pressures 90 mm Hg or higher. Investigators randomized participants with no history of vascular disease, a history of coronary heart disease, or a history of stroke to monotherapy or a combination of 3 drugs from any class at half-standard doses. Combination therapy reduced both coronary heart disease and stroke (number needed to treat [NNT] to prevent 1 new case of coronary heart disease=4, NNT to prevent 1 stroke=3).1

Another meta-analysis of 61 prospective observational studies with a total of 1 million patients showed that for every coronary event or stroke prevented by doubling the dose of a single drug, 4 events were prevented by using combination therapy.2 A 3-point reduction in systolic blood pressure resulted in a 5% to 10% reduction in heart disease and stroke.1

A meta-analysis of 42 trials with a total of almost 11,000 patients found that combining any 2 drug classes at low doses decreased diastolic blood pressure more than doubling the dose of a single drug (9 mm Hg vs 6 mm Hg).3

ACE-I plus ß-blocker or calcium channnel blocker outperforms thiazide combos
The combination of an ACE-I plus a ß-blocker lowered systolic blood pressure more than ACE-I monotherapy (22.9 mm Hg vs 12.5 mm Hg) in an RCT with 48 patients.4 More patients taking an ACE-I plus a calcium channel blocker achieved the primary end point (reductions in systolic blood pressure ≥25 mm Hg) than did patients randomized to monotherapy (74.2% vs 53.9%; NNT=5).5

In an RCT of 11,506 patients, benazepril plus amlodipine decreased blood pressure more than benazepril plus hydrochlorothiazide (difference=0.9 mm Hg systolic, 1.1 mm Hg diastolic) and improved the composite outcome of cardiovascular events and deaths (absolute risk reduction=2.2%; NNT=45).6 Rates of adverse drug reactions were similar among patients taking ACE-I monotherapy and combinations of benazepril plus amlodipine or benazepril plus hydrochlorothiazide.4-6

 

 

 

ARB plus a thiazide lowers BP more than monotherapy
Five short-term RCTs comparing ARB-thiazide combinations with monotherapy measured changes in blood pressure rather than morbidity and mortality. In these studies, sponsored by pharmaceutical companies, combination treatment more often produced blood pressures within the goals of the Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure (JNC-VII) than monotherapy (62% vs 37%; NNT to reach goal=4 [approximately]).7-8 An ARB plus hydrochlorothiazide lowered blood pressure more effectively than either drug alone but produced more dizziness (8.5% vs 4.7%; P=.002).7

In an RCT of 926 patients who had failed monotherapy with an ARB, 74.8% treated with an ARB plus a calcium channel blocker achieved blood pressures <140/90.9 Adding a calcium channel blocker decreased blood pressures by about 19 mm Hg systolic and 11 mm Hg diastolic with few adverse drug reactions.

How safe is combination therapy?
Participants in a 6-year RCT of 25,260 patients had more adverse outcomes with an ARB plus ACE-I combination than monotherapy (number needed to harm=100 to cause composite endpoint of death, dialysis, or creatinine doubling).10 For most other combinations, the safety profile is unknown or similar to monotherapy.

The TABLE summarizes the efficacy and safety profiles of antihypertensive drug combinations.4-10

TABLE
Efficacy and safety of drug combinations for essential hypertension*

 Combined with
ACE-IARBß-blockerCalcium channel blockerThiazide
ACE-I efficacyN/A16-27 mm Hg systolic BP drop (based on RCT, N=25,260)1022.9 mm Hg systolic BP drop (based on RCT, N=48)413.7-20.9 mm Hg systolic BP drop (based on RCT, N= >10,000)512.9 mm Hg systolic BP drop (based on RCT, N=11,506)6,7
ACE-I safetyN/AIncreased risk of death, dialysis, doubled creatinine (NNH=100 for combined endpoint)10Side effects similar to ACE-I monotherapy4Side effects similar to ACE-I monotherapy5,6Side effects similar to ACE-I monotherapy6,7
ARB efficacy16-27 mm Hg systolic BP drop (based on RCT, N=25,260)10N/AUnknown12-20 mm Hg systolic BP drop (based on RCT, N=926)914-25 mm Hg systolic BP drop (based on subgroup analysis of large RCT and RCT, N=261)8
ARB safetyIncreased risk of death, dialysis, doubled creatinine (NNH=100 for combined endpoint)10N/AUnknownSide effects similar to ARB monotherapy9Combination increased dizziness more than ARB monotherapy (NNH=33)8
ACE-I, angiotensin converting enzyme inhibitor; ARB, angiotensin receptor blocker; BP, blood pressure; N/A, not applicable; NNH, number needed to harm; RCT, randomized controlled trial.
*The efficacy and safety of pairing the drugs in the column at left with those in the row at top. All combinations used approximately half the maximum dose of each component.
Significant decrease in cardiovascular mortality.

Recommendations

Both the 2003 JNC-VII and the 2008 Canadian Hypertension Education Program recommendations for managing hypertension advise lowering blood pressure to <140/90 mm Hg in all patients and <130/80 mm Hg in patients with diabetes and chronic kidney disease.11,12 Both guidelines also suggest starting therapy with 2 drugs when blood pressure is more than 20 mm Hg above systolic goal or 10 mm Hg above diastolic goal, but they do not endorse specific combinations.

References

1. Law MR, Morris JK, Wald NJ. Use of blood pressure lowering drugs in the prevention of cardiovascular disease: meta-analysis of 147 randomised trials in the context of expectations from prospective epidemiological studies. BMJ. 2009;338:b1665.-Available at: www.ncbi.nlm.nih.gov/pmc/articles/PMC2684577/?tool=pubmed. Accessed May 5, 2011.

2. Prospective Studies Collaboration. Age-specific relevance of usual blood pressure to vascular mortality: a meta-analysis of individual data for one million adults in 61 prospective studies. Lancet. 2002;360:1903-1913.

3. Wald DS, Law M, Morris JK, et al. Combination therapy versus monotherapy in reducing blood pressure: meta-analysis on 11,000 participants from 42 trials. Am J Med. 2009;122:290-300.

4. Wald DS, Law M, Mills S, et al. A 16-week, randomized, double-blind, placebo-controlled, crossover trial to quantify the combined effect of an angiotensin-converting enzyme inhibitor and a beta-blocker on blood pressure reduction. Clin Ther. 2008;30:2030-2039.

5. Jamerson KA, Nwose O, Jean-Louis L, et al. Initial angiotensin-converting enzyme inhibitor/calcium channel blocker combination therapy achieves superior blood pressure control compared with calcium channel blocker monotherapy in patients with stage 2 hypertension. Am J Hypertens. 2004;17:495-501.

6. Jamerson K, Weber MA, Bakris GL, et al. Benazepril plus amlodipine or hydrochlorothiazide for hypertension in high-risk patients. N Engl J Med. 2008;359:2417-2428.

7. Everett BM, Glynn RJ, Danielson E, et al. Combination therapy versus monotherapy as initial treatment for stage 2 hypertension: a prespecified subgroup analysis of a community-based, randomized, open-label trial. Clin Ther. 2008;30:661-672.

8. Oparil S, Abate N, Chen E, et al. A double-blind, randomized study evaluating losartan potassium monotherapy or in combination with hydrochlorothiazide versus placebo in obese patients with hypertension. Curr Med Res Opin. 2008;24:1101-1114.

9. Allemann Y, Fraile B, Lambert M, et al. Efficacy of the combination of amlodipine and valsartan in patients with hypertension uncontrolled with previous monotherapy: the Exforge in failure after single therapy (EX-FAST) study. J Clin Hypertens. 2008;10:185-194.

10. Mann JF, Schmieder RE, McQueen M, et al. Renal outcomes with telmisartan, ramipril, or both, in people at high vascular risk (the ONTARGET study): a multicentre, randomised, double-blind, controlled trial. Lancet. 2008;372:547-553.

11. Chobanian AV, Bakris GL, Black HR, et al. Seventh report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. 2003;42:1206-1252.Available at: www.nhlbi.nih.gov/guidelines/hypertension/jnc7full.pdf. Accessed May 5, 2011.

12. Khan NA, Hemmelgarn B, Herman RJ, et al. The 2008 Canadian hypertension education program recommendations for the management of hypertension: part 2—therapy. Can J Cardiol. 2008;24:465-475.Available at: www.ncbi.nlm.nih.gov/pmc/articles/PMC2643190/?tool=pubmed. Accessed February 18, 2011.

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Paul Crawford, MD
David Dy, DO
Nellis Family Medicine Residency, Las Vegas, Nev

Misty Carney, MLIS
Wilford Hall Medical Center, San Antonio, Tex

ASSISTANT EDITOR
Brian K. Crownover, MD
Nellis Air Force Base, Family Medicine Residency, Nellis AFB, Nev

The opinions and assertions herein represent those of the authors and not the United States Air Force Medical Service or the US Air Force at large.

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aul Crawford;MD; David Dy;DO; Misty Carney;MLIS; Brian K. Crownover;MD; hypertension; combination drug therapies; cardiovascular morbidity and mortality; cardiovascular outcomes; stroke; coronary heart disease; monotherapy; angiotensin converting enzyme inhibitor; ACE-I; ARB; angiotensin receptor blocker; thiazide; calcium channel blocker; benazepril; amiodipine; hydrochlorothiazide
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David Dy, DO
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Misty Carney, MLIS
Wilford Hall Medical Center, San Antonio, Tex

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Nellis Air Force Base, Family Medicine Residency, Nellis AFB, Nev

The opinions and assertions herein represent those of the authors and not the United States Air Force Medical Service or the US Air Force at large.

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Paul Crawford, MD
David Dy, DO
Nellis Family Medicine Residency, Las Vegas, Nev

Misty Carney, MLIS
Wilford Hall Medical Center, San Antonio, Tex

ASSISTANT EDITOR
Brian K. Crownover, MD
Nellis Air Force Base, Family Medicine Residency, Nellis AFB, Nev

The opinions and assertions herein represent those of the authors and not the United States Air Force Medical Service or the US Air Force at large.

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EVIDENCE-BASED ANSWER

INSUFFICIENT EVIDENCE exists to determine which specific combinations most effectively decrease cardiovascular morbidity and mortality, although combinations of hypertension medications at lower doses generally reduce cardiovascular outcomes (stroke, coronary heart disease) more than monotherapy (strength of recommendation [SOR]: A, large meta-analyses).

The combination of benazepril and amlodipine reduces the composite endpoint of cardiovascular events and deaths more than benazepril plus hydrochlorothiazide with similar rates of adverse effects (SOR: A, randomized controlled trial [RCT]).

Combining an angiotensin converting enzyme inhibitor (ACE-I) with a thiazide, ß-blocker, or calcium channel blocker produces side effects similar to monotherapy, as does combining an angiotensin receptor blocker (ARB) with a thiazide or calcium channel blocker (SOR: A, meta-analyses). However, an ACE-I combined with an ARB increases the risk of renal complications and death more than monotherapy (SOR: A, RCT).

 

Evidence summary

A meta-analysis of 147 RCTs with a total of 464,000 patients demonstrated better cardiovascular outcomes for combination therapy vs monotherapy among patients 60 to 69 years of age with diastolic blood pressures 90 mm Hg or higher. Investigators randomized participants with no history of vascular disease, a history of coronary heart disease, or a history of stroke to monotherapy or a combination of 3 drugs from any class at half-standard doses. Combination therapy reduced both coronary heart disease and stroke (number needed to treat [NNT] to prevent 1 new case of coronary heart disease=4, NNT to prevent 1 stroke=3).1

Another meta-analysis of 61 prospective observational studies with a total of 1 million patients showed that for every coronary event or stroke prevented by doubling the dose of a single drug, 4 events were prevented by using combination therapy.2 A 3-point reduction in systolic blood pressure resulted in a 5% to 10% reduction in heart disease and stroke.1

A meta-analysis of 42 trials with a total of almost 11,000 patients found that combining any 2 drug classes at low doses decreased diastolic blood pressure more than doubling the dose of a single drug (9 mm Hg vs 6 mm Hg).3

ACE-I plus ß-blocker or calcium channnel blocker outperforms thiazide combos
The combination of an ACE-I plus a ß-blocker lowered systolic blood pressure more than ACE-I monotherapy (22.9 mm Hg vs 12.5 mm Hg) in an RCT with 48 patients.4 More patients taking an ACE-I plus a calcium channel blocker achieved the primary end point (reductions in systolic blood pressure ≥25 mm Hg) than did patients randomized to monotherapy (74.2% vs 53.9%; NNT=5).5

In an RCT of 11,506 patients, benazepril plus amlodipine decreased blood pressure more than benazepril plus hydrochlorothiazide (difference=0.9 mm Hg systolic, 1.1 mm Hg diastolic) and improved the composite outcome of cardiovascular events and deaths (absolute risk reduction=2.2%; NNT=45).6 Rates of adverse drug reactions were similar among patients taking ACE-I monotherapy and combinations of benazepril plus amlodipine or benazepril plus hydrochlorothiazide.4-6

 

 

 

ARB plus a thiazide lowers BP more than monotherapy
Five short-term RCTs comparing ARB-thiazide combinations with monotherapy measured changes in blood pressure rather than morbidity and mortality. In these studies, sponsored by pharmaceutical companies, combination treatment more often produced blood pressures within the goals of the Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure (JNC-VII) than monotherapy (62% vs 37%; NNT to reach goal=4 [approximately]).7-8 An ARB plus hydrochlorothiazide lowered blood pressure more effectively than either drug alone but produced more dizziness (8.5% vs 4.7%; P=.002).7

In an RCT of 926 patients who had failed monotherapy with an ARB, 74.8% treated with an ARB plus a calcium channel blocker achieved blood pressures <140/90.9 Adding a calcium channel blocker decreased blood pressures by about 19 mm Hg systolic and 11 mm Hg diastolic with few adverse drug reactions.

How safe is combination therapy?
Participants in a 6-year RCT of 25,260 patients had more adverse outcomes with an ARB plus ACE-I combination than monotherapy (number needed to harm=100 to cause composite endpoint of death, dialysis, or creatinine doubling).10 For most other combinations, the safety profile is unknown or similar to monotherapy.

The TABLE summarizes the efficacy and safety profiles of antihypertensive drug combinations.4-10

TABLE
Efficacy and safety of drug combinations for essential hypertension*

 Combined with
ACE-IARBß-blockerCalcium channel blockerThiazide
ACE-I efficacyN/A16-27 mm Hg systolic BP drop (based on RCT, N=25,260)1022.9 mm Hg systolic BP drop (based on RCT, N=48)413.7-20.9 mm Hg systolic BP drop (based on RCT, N= >10,000)512.9 mm Hg systolic BP drop (based on RCT, N=11,506)6,7
ACE-I safetyN/AIncreased risk of death, dialysis, doubled creatinine (NNH=100 for combined endpoint)10Side effects similar to ACE-I monotherapy4Side effects similar to ACE-I monotherapy5,6Side effects similar to ACE-I monotherapy6,7
ARB efficacy16-27 mm Hg systolic BP drop (based on RCT, N=25,260)10N/AUnknown12-20 mm Hg systolic BP drop (based on RCT, N=926)914-25 mm Hg systolic BP drop (based on subgroup analysis of large RCT and RCT, N=261)8
ARB safetyIncreased risk of death, dialysis, doubled creatinine (NNH=100 for combined endpoint)10N/AUnknownSide effects similar to ARB monotherapy9Combination increased dizziness more than ARB monotherapy (NNH=33)8
ACE-I, angiotensin converting enzyme inhibitor; ARB, angiotensin receptor blocker; BP, blood pressure; N/A, not applicable; NNH, number needed to harm; RCT, randomized controlled trial.
*The efficacy and safety of pairing the drugs in the column at left with those in the row at top. All combinations used approximately half the maximum dose of each component.
Significant decrease in cardiovascular mortality.

Recommendations

Both the 2003 JNC-VII and the 2008 Canadian Hypertension Education Program recommendations for managing hypertension advise lowering blood pressure to <140/90 mm Hg in all patients and <130/80 mm Hg in patients with diabetes and chronic kidney disease.11,12 Both guidelines also suggest starting therapy with 2 drugs when blood pressure is more than 20 mm Hg above systolic goal or 10 mm Hg above diastolic goal, but they do not endorse specific combinations.

EVIDENCE-BASED ANSWER

INSUFFICIENT EVIDENCE exists to determine which specific combinations most effectively decrease cardiovascular morbidity and mortality, although combinations of hypertension medications at lower doses generally reduce cardiovascular outcomes (stroke, coronary heart disease) more than monotherapy (strength of recommendation [SOR]: A, large meta-analyses).

The combination of benazepril and amlodipine reduces the composite endpoint of cardiovascular events and deaths more than benazepril plus hydrochlorothiazide with similar rates of adverse effects (SOR: A, randomized controlled trial [RCT]).

Combining an angiotensin converting enzyme inhibitor (ACE-I) with a thiazide, ß-blocker, or calcium channel blocker produces side effects similar to monotherapy, as does combining an angiotensin receptor blocker (ARB) with a thiazide or calcium channel blocker (SOR: A, meta-analyses). However, an ACE-I combined with an ARB increases the risk of renal complications and death more than monotherapy (SOR: A, RCT).

 

Evidence summary

A meta-analysis of 147 RCTs with a total of 464,000 patients demonstrated better cardiovascular outcomes for combination therapy vs monotherapy among patients 60 to 69 years of age with diastolic blood pressures 90 mm Hg or higher. Investigators randomized participants with no history of vascular disease, a history of coronary heart disease, or a history of stroke to monotherapy or a combination of 3 drugs from any class at half-standard doses. Combination therapy reduced both coronary heart disease and stroke (number needed to treat [NNT] to prevent 1 new case of coronary heart disease=4, NNT to prevent 1 stroke=3).1

Another meta-analysis of 61 prospective observational studies with a total of 1 million patients showed that for every coronary event or stroke prevented by doubling the dose of a single drug, 4 events were prevented by using combination therapy.2 A 3-point reduction in systolic blood pressure resulted in a 5% to 10% reduction in heart disease and stroke.1

A meta-analysis of 42 trials with a total of almost 11,000 patients found that combining any 2 drug classes at low doses decreased diastolic blood pressure more than doubling the dose of a single drug (9 mm Hg vs 6 mm Hg).3

ACE-I plus ß-blocker or calcium channnel blocker outperforms thiazide combos
The combination of an ACE-I plus a ß-blocker lowered systolic blood pressure more than ACE-I monotherapy (22.9 mm Hg vs 12.5 mm Hg) in an RCT with 48 patients.4 More patients taking an ACE-I plus a calcium channel blocker achieved the primary end point (reductions in systolic blood pressure ≥25 mm Hg) than did patients randomized to monotherapy (74.2% vs 53.9%; NNT=5).5

In an RCT of 11,506 patients, benazepril plus amlodipine decreased blood pressure more than benazepril plus hydrochlorothiazide (difference=0.9 mm Hg systolic, 1.1 mm Hg diastolic) and improved the composite outcome of cardiovascular events and deaths (absolute risk reduction=2.2%; NNT=45).6 Rates of adverse drug reactions were similar among patients taking ACE-I monotherapy and combinations of benazepril plus amlodipine or benazepril plus hydrochlorothiazide.4-6

 

 

 

ARB plus a thiazide lowers BP more than monotherapy
Five short-term RCTs comparing ARB-thiazide combinations with monotherapy measured changes in blood pressure rather than morbidity and mortality. In these studies, sponsored by pharmaceutical companies, combination treatment more often produced blood pressures within the goals of the Seventh Report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure (JNC-VII) than monotherapy (62% vs 37%; NNT to reach goal=4 [approximately]).7-8 An ARB plus hydrochlorothiazide lowered blood pressure more effectively than either drug alone but produced more dizziness (8.5% vs 4.7%; P=.002).7

In an RCT of 926 patients who had failed monotherapy with an ARB, 74.8% treated with an ARB plus a calcium channel blocker achieved blood pressures <140/90.9 Adding a calcium channel blocker decreased blood pressures by about 19 mm Hg systolic and 11 mm Hg diastolic with few adverse drug reactions.

How safe is combination therapy?
Participants in a 6-year RCT of 25,260 patients had more adverse outcomes with an ARB plus ACE-I combination than monotherapy (number needed to harm=100 to cause composite endpoint of death, dialysis, or creatinine doubling).10 For most other combinations, the safety profile is unknown or similar to monotherapy.

The TABLE summarizes the efficacy and safety profiles of antihypertensive drug combinations.4-10

TABLE
Efficacy and safety of drug combinations for essential hypertension*

 Combined with
ACE-IARBß-blockerCalcium channel blockerThiazide
ACE-I efficacyN/A16-27 mm Hg systolic BP drop (based on RCT, N=25,260)1022.9 mm Hg systolic BP drop (based on RCT, N=48)413.7-20.9 mm Hg systolic BP drop (based on RCT, N= >10,000)512.9 mm Hg systolic BP drop (based on RCT, N=11,506)6,7
ACE-I safetyN/AIncreased risk of death, dialysis, doubled creatinine (NNH=100 for combined endpoint)10Side effects similar to ACE-I monotherapy4Side effects similar to ACE-I monotherapy5,6Side effects similar to ACE-I monotherapy6,7
ARB efficacy16-27 mm Hg systolic BP drop (based on RCT, N=25,260)10N/AUnknown12-20 mm Hg systolic BP drop (based on RCT, N=926)914-25 mm Hg systolic BP drop (based on subgroup analysis of large RCT and RCT, N=261)8
ARB safetyIncreased risk of death, dialysis, doubled creatinine (NNH=100 for combined endpoint)10N/AUnknownSide effects similar to ARB monotherapy9Combination increased dizziness more than ARB monotherapy (NNH=33)8
ACE-I, angiotensin converting enzyme inhibitor; ARB, angiotensin receptor blocker; BP, blood pressure; N/A, not applicable; NNH, number needed to harm; RCT, randomized controlled trial.
*The efficacy and safety of pairing the drugs in the column at left with those in the row at top. All combinations used approximately half the maximum dose of each component.
Significant decrease in cardiovascular mortality.

Recommendations

Both the 2003 JNC-VII and the 2008 Canadian Hypertension Education Program recommendations for managing hypertension advise lowering blood pressure to <140/90 mm Hg in all patients and <130/80 mm Hg in patients with diabetes and chronic kidney disease.11,12 Both guidelines also suggest starting therapy with 2 drugs when blood pressure is more than 20 mm Hg above systolic goal or 10 mm Hg above diastolic goal, but they do not endorse specific combinations.

References

1. Law MR, Morris JK, Wald NJ. Use of blood pressure lowering drugs in the prevention of cardiovascular disease: meta-analysis of 147 randomised trials in the context of expectations from prospective epidemiological studies. BMJ. 2009;338:b1665.-Available at: www.ncbi.nlm.nih.gov/pmc/articles/PMC2684577/?tool=pubmed. Accessed May 5, 2011.

2. Prospective Studies Collaboration. Age-specific relevance of usual blood pressure to vascular mortality: a meta-analysis of individual data for one million adults in 61 prospective studies. Lancet. 2002;360:1903-1913.

3. Wald DS, Law M, Morris JK, et al. Combination therapy versus monotherapy in reducing blood pressure: meta-analysis on 11,000 participants from 42 trials. Am J Med. 2009;122:290-300.

4. Wald DS, Law M, Mills S, et al. A 16-week, randomized, double-blind, placebo-controlled, crossover trial to quantify the combined effect of an angiotensin-converting enzyme inhibitor and a beta-blocker on blood pressure reduction. Clin Ther. 2008;30:2030-2039.

5. Jamerson KA, Nwose O, Jean-Louis L, et al. Initial angiotensin-converting enzyme inhibitor/calcium channel blocker combination therapy achieves superior blood pressure control compared with calcium channel blocker monotherapy in patients with stage 2 hypertension. Am J Hypertens. 2004;17:495-501.

6. Jamerson K, Weber MA, Bakris GL, et al. Benazepril plus amlodipine or hydrochlorothiazide for hypertension in high-risk patients. N Engl J Med. 2008;359:2417-2428.

7. Everett BM, Glynn RJ, Danielson E, et al. Combination therapy versus monotherapy as initial treatment for stage 2 hypertension: a prespecified subgroup analysis of a community-based, randomized, open-label trial. Clin Ther. 2008;30:661-672.

8. Oparil S, Abate N, Chen E, et al. A double-blind, randomized study evaluating losartan potassium monotherapy or in combination with hydrochlorothiazide versus placebo in obese patients with hypertension. Curr Med Res Opin. 2008;24:1101-1114.

9. Allemann Y, Fraile B, Lambert M, et al. Efficacy of the combination of amlodipine and valsartan in patients with hypertension uncontrolled with previous monotherapy: the Exforge in failure after single therapy (EX-FAST) study. J Clin Hypertens. 2008;10:185-194.

10. Mann JF, Schmieder RE, McQueen M, et al. Renal outcomes with telmisartan, ramipril, or both, in people at high vascular risk (the ONTARGET study): a multicentre, randomised, double-blind, controlled trial. Lancet. 2008;372:547-553.

11. Chobanian AV, Bakris GL, Black HR, et al. Seventh report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. 2003;42:1206-1252.Available at: www.nhlbi.nih.gov/guidelines/hypertension/jnc7full.pdf. Accessed May 5, 2011.

12. Khan NA, Hemmelgarn B, Herman RJ, et al. The 2008 Canadian hypertension education program recommendations for the management of hypertension: part 2—therapy. Can J Cardiol. 2008;24:465-475.Available at: www.ncbi.nlm.nih.gov/pmc/articles/PMC2643190/?tool=pubmed. Accessed February 18, 2011.

References

1. Law MR, Morris JK, Wald NJ. Use of blood pressure lowering drugs in the prevention of cardiovascular disease: meta-analysis of 147 randomised trials in the context of expectations from prospective epidemiological studies. BMJ. 2009;338:b1665.-Available at: www.ncbi.nlm.nih.gov/pmc/articles/PMC2684577/?tool=pubmed. Accessed May 5, 2011.

2. Prospective Studies Collaboration. Age-specific relevance of usual blood pressure to vascular mortality: a meta-analysis of individual data for one million adults in 61 prospective studies. Lancet. 2002;360:1903-1913.

3. Wald DS, Law M, Morris JK, et al. Combination therapy versus monotherapy in reducing blood pressure: meta-analysis on 11,000 participants from 42 trials. Am J Med. 2009;122:290-300.

4. Wald DS, Law M, Mills S, et al. A 16-week, randomized, double-blind, placebo-controlled, crossover trial to quantify the combined effect of an angiotensin-converting enzyme inhibitor and a beta-blocker on blood pressure reduction. Clin Ther. 2008;30:2030-2039.

5. Jamerson KA, Nwose O, Jean-Louis L, et al. Initial angiotensin-converting enzyme inhibitor/calcium channel blocker combination therapy achieves superior blood pressure control compared with calcium channel blocker monotherapy in patients with stage 2 hypertension. Am J Hypertens. 2004;17:495-501.

6. Jamerson K, Weber MA, Bakris GL, et al. Benazepril plus amlodipine or hydrochlorothiazide for hypertension in high-risk patients. N Engl J Med. 2008;359:2417-2428.

7. Everett BM, Glynn RJ, Danielson E, et al. Combination therapy versus monotherapy as initial treatment for stage 2 hypertension: a prespecified subgroup analysis of a community-based, randomized, open-label trial. Clin Ther. 2008;30:661-672.

8. Oparil S, Abate N, Chen E, et al. A double-blind, randomized study evaluating losartan potassium monotherapy or in combination with hydrochlorothiazide versus placebo in obese patients with hypertension. Curr Med Res Opin. 2008;24:1101-1114.

9. Allemann Y, Fraile B, Lambert M, et al. Efficacy of the combination of amlodipine and valsartan in patients with hypertension uncontrolled with previous monotherapy: the Exforge in failure after single therapy (EX-FAST) study. J Clin Hypertens. 2008;10:185-194.

10. Mann JF, Schmieder RE, McQueen M, et al. Renal outcomes with telmisartan, ramipril, or both, in people at high vascular risk (the ONTARGET study): a multicentre, randomised, double-blind, controlled trial. Lancet. 2008;372:547-553.

11. Chobanian AV, Bakris GL, Black HR, et al. Seventh report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. 2003;42:1206-1252.Available at: www.nhlbi.nih.gov/guidelines/hypertension/jnc7full.pdf. Accessed May 5, 2011.

12. Khan NA, Hemmelgarn B, Herman RJ, et al. The 2008 Canadian hypertension education program recommendations for the management of hypertension: part 2—therapy. Can J Cardiol. 2008;24:465-475.Available at: www.ncbi.nlm.nih.gov/pmc/articles/PMC2643190/?tool=pubmed. Accessed February 18, 2011.

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Which combination drug therapies are most effective for hypertension?
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aul Crawford;MD; David Dy;DO; Misty Carney;MLIS; Brian K. Crownover;MD; hypertension; combination drug therapies; cardiovascular morbidity and mortality; cardiovascular outcomes; stroke; coronary heart disease; monotherapy; angiotensin converting enzyme inhibitor; ACE-I; ARB; angiotensin receptor blocker; thiazide; calcium channel blocker; benazepril; amiodipine; hydrochlorothiazide
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aul Crawford;MD; David Dy;DO; Misty Carney;MLIS; Brian K. Crownover;MD; hypertension; combination drug therapies; cardiovascular morbidity and mortality; cardiovascular outcomes; stroke; coronary heart disease; monotherapy; angiotensin converting enzyme inhibitor; ACE-I; ARB; angiotensin receptor blocker; thiazide; calcium channel blocker; benazepril; amiodipine; hydrochlorothiazide
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