Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index: A meta-analysis of randomised trials

L. Agodoa; R. Estacio; R. Schrier; J. Lubsen; J. Chalmers; J. Cutler; B. Davis; L. Wing; N. R. Poulter; P. Sever; G. Remuzzi; P. Ruggenenti; S. Nissen; L. H. Lindholm; T. Fukui; T. Ogihara; T. Saruta; H. Black; P. Sleight; M. Lievre; H. Suzuki; K. Fox; L. Lisheng; T. Ohkubo; Y. Imai; S. Yusuf; C. J. Bulpitt; E. Lewis; M. Brown; C. Palmer; J. Wang; C. Pepine; M. Ishii; Y. Yui; K. Kuramoto; M. Pfeff Er; F. W. Asselbergs; W. H. Van Gilst; B. Byington; B. Pitt; B. Brenner; W. J. Remme; D. De Zeeuw; M. Rahman; G. Viberti; K. Teo; A. Zanchetti; E. Malacco; G. Mancia; J. Staessen; R. Fagard; R. Holman; L. Hansson; J. Kostis; Y. Kanno; S. Lueders; M. Matsuzaki; P. Poole-Wilson; J. Schrader; K. Rahimi; C. Anderson; N. Chapman; R. Collins; S. MacMahon; B. Neal; A. Rodgers; P. Whelton; M. Woodward

doi:10.1016/S0140-6736(14)61171-5

Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index: A meta-analysis of randomised trials

L. Agodoa, R. Estacio, R. Schrier, J. Lubsen, J. Chalmers, J. Cutler, B. Davis, L. Wing, N. R. Poulter, P. Sever, G. Remuzzi, P. Ruggenenti, S. Nissen, L. H. Lindholm, T. Fukui, T. Ogihara, T. Saruta, H. Black, P. Sleight, M. LievreH. Suzuki, K. Fox, L. Lisheng, T. Ohkubo, Y. Imai, S. Yusuf, C. J. Bulpitt, E. Lewis, M. Brown, C. Palmer, J. Wang, C. Pepine, M. Ishii, Y. Yui, K. Kuramoto, M. Pfeff Er, F. W. Asselbergs, W. H. Van Gilst, B. Byington, B. Pitt, B. Brenner, W. J. Remme, D. De Zeeuw, M. Rahman, G. Viberti, K. Teo, A. Zanchetti, E. Malacco, G. Mancia, J. Staessen, R. Fagard, R. Holman, L. Hansson, J. Kostis, Y. Kanno, S. Lueders, M. Matsuzaki, P. Poole-Wilson, J. Schrader, K. Rahimi, C. Anderson, N. Chapman, R. Collins, S. MacMahon, B. Neal, A. Rodgers, P. Whelton, M. Woodward

Bloomberg School of Public Health

Research output: Contribution to journal › Article › peer-review

24 Scopus citations

Abstract

Summary Background The cardiovascular benefits of blood pressure lowering in obese people compared with people of normal weight might depend on choice of drug. We compared the effects of blood pressure-lowering regimens on cardiovascular risk in groups of patients categorised by baseline body-mass index (BMI). Methods We used individual patient data from trials included in the Blood Pressure Lowering Treatment Trialists' Collaboration to compare the effects of different classes of blood pressure-lowering regimens for the primary outcome of total major cardiovascular events (stroke, coronary heart disease, heart failure, and cardiovascular death). We used meta-analyses and meta-regressions to assess interactions between treatment and BMI when fitted as either a categorical variable (<25 kg/m², 25 to <30 kg/m², and ≥30 kg/m²) or a continuous variable. Findings Analyses were based on 135 715 individuals from 22 trials who had 14 353 major cardiovascular events. None of the six primary comparisons showed evidence that protection varied by drug class across the three BMI groups (all p for trend >0·20). When analysed as a continuous variable, angiotensin-converting-enzyme inhibitors gave slightly greater protection for each 5 kg/m² higher BMI than did calcium antagonists (hazard ratio 0·93, 95% CI 0·89-0·98; p=0·004) or diuretics (0·93, 0·89-0·98; p=0·002). The meta-regressions showed no relation between BMI category and the risk reduction for a given fall in systolic blood pressure. By contrast with a previous report, we noted no relation between BMI and the efficacy of calcium antagonists compared with diuretics. Interpretation We found little evidence that selection of a particular class of blood pressure-lowering drug will lead to substantially different outcomes for individuals who are obese compared with those who are lean. Funding None.

Original language	English (US)
Pages (from-to)	867-874
Number of pages	8
Journal	The Lancet
Volume	385
Issue number	9971
DOIs	https://doi.org/10.1016/S0140-6736(14)61171-5
State	Published - Mar 7 2015

ASJC Scopus subject areas

General Medicine

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10.1016/S0140-6736(14)61171-5

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Agodoa, L., Estacio, R., Schrier, R., Lubsen, J., Chalmers, J., Cutler, J., Davis, B., Wing, L., Poulter, N. R., Sever, P., Remuzzi, G., Ruggenenti, P., Nissen, S., Lindholm, L. H., Fukui, T., Ogihara, T., Saruta, T., Black, H., Sleight, P., ... Woodward, M. (2015). Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index: A meta-analysis of randomised trials. The Lancet, 385(9971), 867-874. https://doi.org/10.1016/S0140-6736(14)61171-5

Agodoa, L, Estacio, R, Schrier, R, Lubsen, J, Chalmers, J, Cutler, J, Davis, B, Wing, L, Poulter, NR, Sever, P, Remuzzi, G, Ruggenenti, P, Nissen, S, Lindholm, LH, Fukui, T, Ogihara, T, Saruta, T, Black, H, Sleight, P, Lievre, M, Suzuki, H, Fox, K, Lisheng, L, Ohkubo, T, Imai, Y, Yusuf, S, Bulpitt, CJ, Lewis, E, Brown, M, Palmer, C, Wang, J, Pepine, C, Ishii, M, Yui, Y, Kuramoto, K, Pfeff Er, M, Asselbergs, FW, Van Gilst, WH, Byington, B, Pitt, B, Brenner, B, Remme, WJ, De Zeeuw, D, Rahman, M, Viberti, G, Teo, K, Zanchetti, A, Malacco, E, Mancia, G, Staessen, J, Fagard, R, Holman, R, Hansson, L, Kostis, J, Kanno, Y, Lueders, S, Matsuzaki, M, Poole-Wilson, P, Schrader, J, Rahimi, K, Anderson, C, Chapman, N, Collins, R, MacMahon, S, Neal, B, Rodgers, A, Whelton, P & Woodward, M 2015, 'Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index: A meta-analysis of randomised trials', The Lancet, vol. 385, no. 9971, pp. 867-874. https://doi.org/10.1016/S0140-6736(14)61171-5

@article{524ead7b1f88411ea4fc112f4f5fb466,

title = "Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index: A meta-analysis of randomised trials",

abstract = "Summary Background The cardiovascular benefits of blood pressure lowering in obese people compared with people of normal weight might depend on choice of drug. We compared the effects of blood pressure-lowering regimens on cardiovascular risk in groups of patients categorised by baseline body-mass index (BMI). Methods We used individual patient data from trials included in the Blood Pressure Lowering Treatment Trialists' Collaboration to compare the effects of different classes of blood pressure-lowering regimens for the primary outcome of total major cardiovascular events (stroke, coronary heart disease, heart failure, and cardiovascular death). We used meta-analyses and meta-regressions to assess interactions between treatment and BMI when fitted as either a categorical variable (<25 kg/m2, 25 to <30 kg/m2, and ≥30 kg/m2) or a continuous variable. Findings Analyses were based on 135 715 individuals from 22 trials who had 14 353 major cardiovascular events. None of the six primary comparisons showed evidence that protection varied by drug class across the three BMI groups (all p for trend >0·20). When analysed as a continuous variable, angiotensin-converting-enzyme inhibitors gave slightly greater protection for each 5 kg/m2 higher BMI than did calcium antagonists (hazard ratio 0·93, 95% CI 0·89-0·98; p=0·004) or diuretics (0·93, 0·89-0·98; p=0·002). The meta-regressions showed no relation between BMI category and the risk reduction for a given fall in systolic blood pressure. By contrast with a previous report, we noted no relation between BMI and the efficacy of calcium antagonists compared with diuretics. Interpretation We found little evidence that selection of a particular class of blood pressure-lowering drug will lead to substantially different outcomes for individuals who are obese compared with those who are lean. Funding None.",

author = "L. Agodoa and R. Estacio and R. Schrier and J. Lubsen and J. Chalmers and J. Cutler and B. Davis and L. Wing and Poulter, {N. R.} and P. Sever and G. Remuzzi and P. Ruggenenti and S. Nissen and Lindholm, {L. H.} and T. Fukui and T. Ogihara and T. Saruta and H. Black and P. Sleight and M. Lievre and H. Suzuki and K. Fox and L. Lisheng and T. Ohkubo and Y. Imai and S. Yusuf and Bulpitt, {C. J.} and E. Lewis and M. Brown and C. Palmer and J. Wang and C. Pepine and M. Ishii and Y. Yui and K. Kuramoto and {Pfeff Er}, M. and Asselbergs, {F. W.} and {Van Gilst}, {W. H.} and B. Byington and B. Pitt and B. Brenner and Remme, {W. J.} and {De Zeeuw}, D. and M. Rahman and G. Viberti and K. Teo and A. Zanchetti and E. Malacco and G. Mancia and J. Staessen and R. Fagard and R. Holman and L. Hansson and J. Kostis and Y. Kanno and S. Lueders and M. Matsuzaki and P. Poole-Wilson and J. Schrader and K. Rahimi and C. Anderson and N. Chapman and R. Collins and S. MacMahon and B. Neal and A. Rodgers and P. Whelton and M. Woodward",

note = "Funding Information: HA is supported by an Australian Research Council Fellowship. BN is supported by an Australian Research Council (ARC) Future Fellowship. BN and MW are supported by National Health and Medical Research Council of Australia (NHMRC) Senior Research Fellowships. VP has received grants from The Heart Foundation of Australia. BN, MW, and VP have received grants from the NHMRC. This work received no specific funding support. Funding Information: BN is on trial steering committees for Janssen, Dr Reddy's Laboratories, and Servier; his institution has received grant funding from AbbVie, Janssen, Novartis, Dr Reddy's Laboratories, Roche, and Servier; and he has received honoraria for meeting presentations from Abbott, AstraZeneca, Novartis, Pfizer, Roche, and Servier. VP has received honoraria for meeting presentations and/or advisory board participation from AbbVie, AstraZeneca, Baxter, Boehringer Ingelheim, Servier, and Vitae, and his employer has received trial funding from Abbvie, Baxter, Janssen, Novartis, Roche, and Servier. SC received honoraria for meeting presentations from Covidien, Servier, Novonordisk, and Sanofi; research grants from Novonordisk; and attended board meetings of AstraZeneca and Covidien. HA has received honoraria for meeting presentations from Takeda Pharmaceutical Company. MW is on a trial advisory committee for Novartis. AY, FT, and RH declare no competing interests. Publisher Copyright: {\textcopyright} 2015 Elsevier Ltd.",

year = "2015",

month = mar,

day = "7",

doi = "10.1016/S0140-6736(14)61171-5",

language = "English (US)",

volume = "385",

pages = "867--874",

journal = "The Lancet",

issn = "0140-6736",

publisher = "Elsevier Limited",

number = "9971",

}

TY - JOUR

T1 - Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index

T2 - A meta-analysis of randomised trials

AU - Agodoa, L.

AU - Estacio, R.

AU - Schrier, R.

AU - Lubsen, J.

AU - Chalmers, J.

AU - Cutler, J.

AU - Davis, B.

AU - Wing, L.

AU - Poulter, N. R.

AU - Sever, P.

AU - Remuzzi, G.

AU - Ruggenenti, P.

AU - Nissen, S.

AU - Lindholm, L. H.

AU - Fukui, T.

AU - Ogihara, T.

AU - Saruta, T.

AU - Black, H.

AU - Sleight, P.

AU - Lievre, M.

AU - Suzuki, H.

AU - Fox, K.

AU - Lisheng, L.

AU - Ohkubo, T.

AU - Imai, Y.

AU - Yusuf, S.

AU - Bulpitt, C. J.

AU - Lewis, E.

AU - Brown, M.

AU - Palmer, C.

AU - Wang, J.

AU - Pepine, C.

AU - Ishii, M.

AU - Yui, Y.

AU - Kuramoto, K.

AU - Pfeff Er, M.

AU - Asselbergs, F. W.

AU - Van Gilst, W. H.

AU - Byington, B.

AU - Pitt, B.

AU - Brenner, B.

AU - Remme, W. J.

AU - De Zeeuw, D.

AU - Rahman, M.

AU - Viberti, G.

AU - Teo, K.

AU - Zanchetti, A.

AU - Malacco, E.

AU - Mancia, G.

AU - Staessen, J.

AU - Fagard, R.

AU - Holman, R.

AU - Hansson, L.

AU - Kostis, J.

AU - Kanno, Y.

AU - Lueders, S.

AU - Matsuzaki, M.

AU - Poole-Wilson, P.

AU - Schrader, J.

AU - Rahimi, K.

AU - Anderson, C.

AU - Chapman, N.

AU - Collins, R.

AU - MacMahon, S.

AU - Neal, B.

AU - Rodgers, A.

AU - Whelton, P.

AU - Woodward, M.

N1 - Funding Information: HA is supported by an Australian Research Council Fellowship. BN is supported by an Australian Research Council (ARC) Future Fellowship. BN and MW are supported by National Health and Medical Research Council of Australia (NHMRC) Senior Research Fellowships. VP has received grants from The Heart Foundation of Australia. BN, MW, and VP have received grants from the NHMRC. This work received no specific funding support. Funding Information: BN is on trial steering committees for Janssen, Dr Reddy's Laboratories, and Servier; his institution has received grant funding from AbbVie, Janssen, Novartis, Dr Reddy's Laboratories, Roche, and Servier; and he has received honoraria for meeting presentations from Abbott, AstraZeneca, Novartis, Pfizer, Roche, and Servier. VP has received honoraria for meeting presentations and/or advisory board participation from AbbVie, AstraZeneca, Baxter, Boehringer Ingelheim, Servier, and Vitae, and his employer has received trial funding from Abbvie, Baxter, Janssen, Novartis, Roche, and Servier. SC received honoraria for meeting presentations from Covidien, Servier, Novonordisk, and Sanofi; research grants from Novonordisk; and attended board meetings of AstraZeneca and Covidien. HA has received honoraria for meeting presentations from Takeda Pharmaceutical Company. MW is on a trial advisory committee for Novartis. AY, FT, and RH declare no competing interests. Publisher Copyright: © 2015 Elsevier Ltd.

PY - 2015/3/7

Y1 - 2015/3/7

N2 - Summary Background The cardiovascular benefits of blood pressure lowering in obese people compared with people of normal weight might depend on choice of drug. We compared the effects of blood pressure-lowering regimens on cardiovascular risk in groups of patients categorised by baseline body-mass index (BMI). Methods We used individual patient data from trials included in the Blood Pressure Lowering Treatment Trialists' Collaboration to compare the effects of different classes of blood pressure-lowering regimens for the primary outcome of total major cardiovascular events (stroke, coronary heart disease, heart failure, and cardiovascular death). We used meta-analyses and meta-regressions to assess interactions between treatment and BMI when fitted as either a categorical variable (<25 kg/m2, 25 to <30 kg/m2, and ≥30 kg/m2) or a continuous variable. Findings Analyses were based on 135 715 individuals from 22 trials who had 14 353 major cardiovascular events. None of the six primary comparisons showed evidence that protection varied by drug class across the three BMI groups (all p for trend >0·20). When analysed as a continuous variable, angiotensin-converting-enzyme inhibitors gave slightly greater protection for each 5 kg/m2 higher BMI than did calcium antagonists (hazard ratio 0·93, 95% CI 0·89-0·98; p=0·004) or diuretics (0·93, 0·89-0·98; p=0·002). The meta-regressions showed no relation between BMI category and the risk reduction for a given fall in systolic blood pressure. By contrast with a previous report, we noted no relation between BMI and the efficacy of calcium antagonists compared with diuretics. Interpretation We found little evidence that selection of a particular class of blood pressure-lowering drug will lead to substantially different outcomes for individuals who are obese compared with those who are lean. Funding None.

AB - Summary Background The cardiovascular benefits of blood pressure lowering in obese people compared with people of normal weight might depend on choice of drug. We compared the effects of blood pressure-lowering regimens on cardiovascular risk in groups of patients categorised by baseline body-mass index (BMI). Methods We used individual patient data from trials included in the Blood Pressure Lowering Treatment Trialists' Collaboration to compare the effects of different classes of blood pressure-lowering regimens for the primary outcome of total major cardiovascular events (stroke, coronary heart disease, heart failure, and cardiovascular death). We used meta-analyses and meta-regressions to assess interactions between treatment and BMI when fitted as either a categorical variable (<25 kg/m2, 25 to <30 kg/m2, and ≥30 kg/m2) or a continuous variable. Findings Analyses were based on 135 715 individuals from 22 trials who had 14 353 major cardiovascular events. None of the six primary comparisons showed evidence that protection varied by drug class across the three BMI groups (all p for trend >0·20). When analysed as a continuous variable, angiotensin-converting-enzyme inhibitors gave slightly greater protection for each 5 kg/m2 higher BMI than did calcium antagonists (hazard ratio 0·93, 95% CI 0·89-0·98; p=0·004) or diuretics (0·93, 0·89-0·98; p=0·002). The meta-regressions showed no relation between BMI category and the risk reduction for a given fall in systolic blood pressure. By contrast with a previous report, we noted no relation between BMI and the efficacy of calcium antagonists compared with diuretics. Interpretation We found little evidence that selection of a particular class of blood pressure-lowering drug will lead to substantially different outcomes for individuals who are obese compared with those who are lean. Funding None.

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UR - http://www.scopus.com/inward/citedby.url?scp=84924254084&partnerID=8YFLogxK

U2 - 10.1016/S0140-6736(14)61171-5

DO - 10.1016/S0140-6736(14)61171-5

M3 - Article

AN - SCOPUS:84924254084

SN - 0140-6736

VL - 385

SP - 867

EP - 874

JO - The Lancet

JF - The Lancet

IS - 9971

ER -

Effects of blood pressure lowering on cardiovascular risk according to baseline body-mass index: A meta-analysis of randomised trials

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