Elsevier

The Lancet

Volume 360, Issue 9349, 14 December 2002, Pages 1903-1913
The Lancet

Articles
Age-specific relevance of usual blood pressure to vascular mortality: a meta-analysis of individual data for one million adults in 61 prospective studies*

https://doi.org/10.1016/S0140-6736(02)11911-8Get rights and content

Summary

Background

The age-specific relevance of blood pressure to cause-specific mortality is best assessed by collaborative meta-analysis of individual participant data from the separate prospective studies.

Methods

Information was obtained on each of one million adults with no previous vascular disease recorded at baseline in 61 prospective observational studies of blood pressure and mortality. During 12·7 million person-years at risk, there were about 56 000 vascular deaths (12 000 stroke, 34000 ischaemic heart disease [IHD], 10000 other vascular) and 66 000 other deaths at ages 40–89 years. Meta-analyses, involving “time-dependent” correction for regression dilution, related mortality during each decade of age at death to the estimated usual blood pressure at the start of that decade.

Findings

Within each decade of age at death, the proportional difference in the risk of vascular death associated with a given absolute difference in usual blood pressure is about the same down to at least 115 mm Hg usual systolic blood pressure (SBP) and 75 mm Hg usual diastolic blood pressure (DBP), below which there is little evidence. At ages 40–69 years, each difference of 20 mm Hg usual SBP (or, approximately equivalently, 10 mm Hg usual DBP) is associated with more than a twofold difference in the stroke death rate, and with twofold differences in the death rates from IHD and from other vascular causes. All of these proportional differences in vascular mortality are about half as extreme at ages 80–89 years as at ages 40–49 years, but the annual absolute differences in risk are greater in old age. The age-specific associations are similar for men and women, and for cerebral haemorrhage and cerebral ischaemia. For predicting vascular mortality from a single blood pressure measurement, the average of SBP and DBP is slightly more informative than either alone, and pulse pressure is much less informative.

Interpretation

Throughout middle and old age, usual blood pressure is strongly and directly related to vascular (and overall) mortality, without any evidence of a threshold down to at least 115/75 mm Hg.

Introduction

The observed relationships between blood pressure and vascular disease mortality in particular epidemiological studies are subject to appreciable random error, especially at lower blood pressure levels, for which the mortality rates are relatively low. As a consequence, different studies may produce apparently very different results, and unduly selective emphasis on some and not on others could introduce substantial biases. Hence, both to limit purely random errors and to minimise selective biases, meta-analyses of the observational studies of these relations are needed. By combining data from many studies, such meta-analyses can assess reliably the relevance of blood pressure to disease risk in a wide range of circumstances (including the extremes of the usual blood pressure distribution, and different ages). The present collaborative meta-analysis1 differs from previous meta-analyses2, 3, 4 in several ways that increase its reliability and informativeness: (i) it is large, involving 120 000 deaths among one million participants in 61 cohorts (with parallel analyses of the Multiple Risk Factor Intervention Trial [MRFIT] observational study5 that involve a further 17 000 vascular deaths); (ii) individual records are available for each of the participants in each study, allowing detailed analyses; (iii) individuals with pre-existing vascular disease recorded were excluded, limiting any effects of disease on blood pressure (ie, avoiding “reverse causality”); (iv) cause-specific mortality data, together with age at death, are generally available; and (v) information on 286 000 repeat measurements made during prolonged follow-up allows appropriate time-dependent correction for “regression dilution”.2, 6

Typically in prospective studies of the relevance to disease of risk factors such as blood pressure, various characteristics of a cohort are recorded at an initial baseline survey and these baseline characteristics of individuals who subsequently develop a particular disease are then compared with those of individuals who do not. But, because of fluctuations in the measured values of a risk factor at baseline, such comparisons often substantially underestimate the strength of the real association between the “usual” (ie, long-term average) level of that risk factor during a particular exposure period and the disease rate during that same, or a later, period.2 This regression dilution effect may be caused by measurement error, by short-term biological variability (including both transient fluctuations and any diurnal or seasonal variation), or by longer-term within-person fluctuations or trends in risk factor values (which may occur for several reasons, including physical activity, diet, treatment, disease, or age). Information from repeat measurements of the risk factor after just a year or two in a reasonably representative sample of individuals can be used to correct for the effects not only of random measurement error but also of short-term variability in risk factor levels.2 If, however, the aim is to estimate the usual risk factor levels 5, 10, or 15 years later then corrections based on remeasurements made relatively soon after baseline may not allow properly for the effects of longer-term within-person variability or trends. Moreover, since the interval between the baseline survey and the occurrence of an event in prospective studies is typically longer among those who suffer events at older ages, such underestimation may well be greater in the elderly. In order to make appropriate time-dependent corrections for these effects of regression dilution, remeasurements during prolonged follow-up can be used to estimate the usual risk factor levels at some particular fixed interval prior to death in each decade of age.6

Hence, by combination of individual participant data from many prospective observational studies in a systematic meta-analysis that is appropriately corrected for time-dependent regression dilution, the present report characterises, with greater precision and less bias than has previously been possible, the age-specific and sex-specific relevance of the usual blood pressure to the subsequent rates of death from stroke, ischaemic heart disease (IHD), other vascular causes, and the aggregate of all non-vascular causes.

Section snippets

Study selection criteria and data collection

As described previously,1 collaboration was sought from the investigators of all prospective observational studies in which data on blood pressure, blood cholesterol, date of birth (or age), and sex had been recorded at a baseline screening visit, and in which cause and date of death (or age at death) had been routinely sought for all screenees during more than 5000 person-years of follow-up (see appendix A; http://image.thelancet.com/extras/01art8300webappendixA.pdf). Relevant studies were

Study populations

Individual records for each of 958 074 participants in 61 studies were included in this meta-analysis, with 70% of the participants from Europe, 20% from North America or Australia, and the remainder from Japan or China (table Al in appendix A). During 12·7 million person-years at risk (mean of 12 years to death), there were 11 960 deaths attributed to stroke, 34 283 attributed to IHD, 10 092 attributed to other vascular causes, and 60 797 attributed to non-vascular causes (while a further 5584

Continuous positive associations between blood pressure and disease risk

In the present meta-analysis of data from 61 prospective observational studies on deaths from vascular disease among individuals without known vascular disease at baseline (and in parallel analyses of the large MRFIT study), blood pressure is associated strongly with the age-specific mortality rates from stroke, almost as strongly with the mortality rates from IHD and with those from other vascular causes, and much less strongly (although still positively) with the age-specific mortality rates

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