Background

ResProt

JMIR Res Protoc

JMIR Research Protocols

1929-0748

JMIR Publications

Toronto, Canada

v6i9e177

28864428

10.2196/resprot.8362

Protocol

Legacy Effect of Delayed Blood Pressure-Lowering Pharmacotherapy in Middle-Aged Individuals Stratified by Absolute Cardiovascular Disease Risk: Protocol for a Systematic Review

Eysenbach

Gunther

Sever

Peter

Chau Le Bao

MD 1

Menzies Institute for Medical Research University of Tasmania

Private Bag 23

Hobart, TAS, 7001

Australia 61 406656898 61 0362267764 chau.ho@utas.edu.au

http://orcid.org/0000-0001-7454-6995

Sanders

Sharon

BSc, MPH, PhD 2

http://orcid.org/0000-0001-7966-9708

Doust

Jenny

BMBS, FRACGP, PhD 2

http://orcid.org/0000-0002-4024-9308

Breslin

Monique

PhD 1

http://orcid.org/0000-0002-8135-3136

Reid

Christopher M

MA, MSc, PhD 3 4

http://orcid.org/0000-0001-9173-3944

Nelson

Mark Raymond

MBBS, MFM, FRACGP, FAFPHM, PhD 1 4

http://orcid.org/0000-0001-9941-7161

¹ Menzies Institute for Medical Research University of Tasmania

Hobart, TAS

Australia ² Centre for Research in Evidence-Based Practice Bond University

Gold Coast, QLD

Australia ³ School of Public Health Curtin University

Perth, WA

Australia ⁴ Centre of Cardiovascular Research & Education in Therapeutics, School of Public Health and Preventive Medicine Monash University

Melbourne, VIC

Australia

Corresponding Author: Chau Le Bao Ho chau.ho@utas.edu.au

092017

01 09 2017

6 9

e177

6 7 2017 15 7 2017 20 7 2017 21 7 2017

©Chau Le Bao Ho, Sharon Sanders, Jenny Doust, Monique Breslin, Christopher M Reid, Mark Raymond Nelson. Originally published in JMIR Research Protocols (http://www.researchprotocols.org), 01.09.2017.

2017

This is an open-access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work, first published in JMIR Research Protocols, is properly cited. The complete bibliographic information, a link to the original publication on http://www.researchprotocols.org, as well as this copyright and license information must be included.

Background

Many national and international guidelines recommend that the initiation of blood pressure (BP)-lowering drug treatment for the primary prevention of cardiovascular disease (CVD) should no longer be based on BP level alone, but on absolute cardiovascular risk. While BP-lowering drug treatment is beneficial in high-risk individuals at any level of elevated BP, clinicians are concerned about legacy effects on patients with low-to-moderate risk and mildly elevated BP who remain “untreated”.

Objective

We aim to investigate the legacy effect of delayed BP-lowering pharmacotherapy in middle-aged individuals (45-65 years) with mildly elevated BP (systolic BP 140-159 mmHg and/or diastolic BP 90-99 mmHg) stratified by absolute risk for primary prevention of CVD, but particularly in the low-risk (<10% five-year absolute risk) group.

Methods

Randomized trials of BP-lowering therapy versus placebo or pretreated subjects in active comparator studies with posttrial follow-up will be identified using a 2-step process. First, randomized trials of BP-lowering therapy will be identified by (1) retrieving the references of trials included in published systematic reviews of BP-lowering therapy, (2) retrieving studies published by the Blood Pressure Lowering Treatment Trialists’ Collaboration (BPLTTC), and (3) checking studies referenced in the 1993 World Health Organization/International Society of Hypertension meeting memorandum on BP management. Posttrial follow-up studies will then be identified by forward citation searching the randomized trials identified in step 1 through Web of Science. The search will include randomized controlled trials with at least 1-year in-trial period and a posttrial follow-up phase. Age is the major determinant of absolute cardiovascular risk, so the participants in our review will be restricted to middle-aged adults who are more likely to have a lower cardiovascular risk profile. The primary outcome will be all-cause mortality. Secondary outcomes will include cardiovascular mortality, fatal stroke, fatal myocardial infarction, and death due to heart failure.

Results

The searches for existing systematic reviews and BPLTTC studies were piloted and modified. The study is expected to be completed before June 2018.

Conclusions

The findings of this study will contribute to the body of knowledge concerning the beneficial, neutral, or harmful effects of delayed BP-lowering drug treatment on the primary prevention of CVD in patients with mildly elevated BP and low-to-moderate CVD risk.

Trial Registration

PROSPERO International Prospective Register of Systematic Reviews: CRD42017058414; https://www.crd.york.ac.uk/PROSPERO/display_record.asp?ID=CRD42017058414 (Archived by WebCite® at http://www.webcitation.org/6t6sa8O2Q)

legacy effect high blood pressure cardiovascular disease

Introduction

Despite improvements in the management of cardiovascular disease (CVD) over the past five decades, it remains the leading cause of death and disability in the world [1]. CVD was responsible for approximately 17.5 million deaths worldwide in 2012 [1]. In updated guidelines for the primary prevention of CVD from Australasia [2,3], the United Kingdom [4], and Europe [5], blood pressure (BP)-lowering pharmacotherapy is indicated by absolute CVD risk, not BP level alone. In contrast, the US guideline (the Eighth Joint National Committee) [6] is still heavily focused on BP level and age, despite the fact that BP-lowering therapy is beneficial for the reduction of CVD mortality and morbidity at sufficiently high CVD absolute risk, regardless of the level of BP elevation [7]. The use of BP-lowering drug treatment in high-risk settings has achieved consensus in Australasian [2,3], European [5], and the US guidelines [6]. In low-risk individuals, BP-lowering drugs are not recommended by guidelines in Australia [2], New Zealand [3] or the United Kingdom [4], unless BP exceeds a level of 160/100 mmHg, whereas the European [5] and US [6] guidelines recommended an early initiation at a BP level of 140/90 mmHg. However, both approaches raised many concerns from clinicians and a gap still exists between guidelines and clinical practice [8].

An international expert consultation was recently performed to solve the controversy of whether adults with grade 1 hypertension (<140/90 mmHg) and low-to-moderate CVD risk should be treated by drug therapy [9]. Morales-Salinas et al [9] recommended an early initiation of BP-lowering pharmacotherapy primarily from the results of the Heart Outcomes Prevention Evaluation (HOPE-3) trial [10] and a meta-analysis by Thomopoulos et al [11] for adults with grade 1 hypertension and moderate CVD risk; however, the two studies were likely to include a number of high-risk participants. In the HOPE-3 trial [10], participants with an INTERHEART risk score higher than 16 (a value of 16 or higher indicates a high CVD risk) accounted for 32.5% of the total sample [12]. In the meta-analysis by Thomopoulos et al [11], the CVD risk was calculated by CVD death rate in the control group, while the CVD risk score used in most guidelines is for fatal and nonfatal CVD events. Thus, the benefits of BP-lowering pharmacotherapy in low-to-moderate-risk individuals remain unclear, as opposed to the benefits achieved by treating high risk individuals. Most clinicians use BP-lowering pharmacotherapy based on BP criteria alone, due to the perceived potential risk of irreversible target organ damage (the “legacy effect”) for delayed therapy [5]. Studies that would help us to answer this question include those that have extended follow-up in the posttrial period. Such studies include the Systolic Hypertension in the Elderly Program trial [13] of approximately 22 years, the Hypertension Detection and Follow-Up Program [14] of 8.3 years, and the second Australian National Blood Pressure study [15] of 10.6 years. Participants in these studies are still likely to be at high baseline risk of CVD due to the advanced age and diabetic status in the inclusion criteria of the trials [13-15]. Hence, the concern of legacy effects on low-to-moderate-risk individuals has not been addressed. Age is the most important determinant of adverse cardiovascular risk, so the participants in our review are restricted to middle-aged adults who are more likely to have a broader cardiovascular risk profile. Therefore, in this systematic review and meta-analysis, we will investigate the effects of BP-lowering drug treatments in middle-aged individuals with mildly elevated BP, stratified by absolute CVD risk.

Methods Review Objectives Aim 1

We will conduct a systematic review and meta-analysis of published and unpublished studies of randomized placebo control trials with a posttrial follow-up phase that included middle-aged participants without overt CVD, and examine these studies for CVD mortality and all-cause mortality.

Aim 2

We will conduct a subgroup analysis (where possible) of participants in these trials classified as low-, moderate-, and high-absolute CVD risk by the Framingham Risk Score (FRS) used in the Australia guideline [2], or the risk calculator used by the Blood Pressure Lowering Treatment Trialists’ Collaboration (BPLTTC) [16] which uses routine clinical information if information on cholesterol levels is not available for fatal and nonfatal CVD events and all-cause mortality. We will conduct an individual patient data meta-analysis, if data are available.

Primary Null Hypothesis

There will be no significant difference in CVD mortality or all-cause mortality between patients who have drug therapy initiated earlier (active treatment arm) versus delayed or not initiated (control arm) in individuals at low-absolute CVD risk.

Secondary Hypotheses Hypothesis 1

Hypothesis 2

Hypothesis 3

In-trial CVD events (fatal and nonfatal) will be incremental by risk classification estimated by FRS or equivalent risk calculated at baseline.

Criteria for Considering Studies in the Review Population

The study will include men and nonpregnant women from 45 to 65 years of age. At least 80% of participants from each trial must have had mildly elevated BP at baseline, defined as a systolic BP of 140- 159 mmHg and/or diastolic BP 90- 99 mmHg. Furthermore, all included participants must not have exhibited any history of CVD at baseline: myocardial infarction, angina pectoris, coronary bypass surgery, coronary angioplasty, stroke, transient ischaemic attack, carotid endarterectomy, surgery for peripheral vascular disease, intermittent claudication or renal failure (creatinine >1.5 times the upper limit of normal). If trials included participants different than those of interest (eg, secondary prevention, moderately-elevated or highly-elevated BP), we will attempt to access individual patient data and subsequently select participants that meet specific criteria.

Intervention

The study will focus on all types of BP-lowering drugs, except for some types that have limited clinical use due to the risk of side effects and availability (eg, ganglion blockers, reserpine, rauwolfia).

Comparison

The study will compare the effects of BP-lowering drug treatments in active treatment groups versus control treatment groups. However, if comparative trials with two active comparators had an extended posttrial follow-up phase and individual data are available, we will perform a legacy effect analysis per Nelson et al [15]. We will reclassify participants into previous treatment (early treatment) groups and treatment naïve (delayed treatment) groups. The previous treatment group will include participants who were on BP-lowering drug treatments at trial registration and then went on a specific drug withdrawal program. The treatment naïve group will include those who were not on any treatments at trial registration.

Outcomes

Primary outcomes will include all-cause mortality in both randomization and follow-up periods. Secondary outcomes will include CVD mortality (defined as deaths due to stroke, myocardial infarction, and heart failure), fatal stroke, fatal myocardial infarction, and fatal heart failure. Nonfatal CVD events will be included if the measurements of outcomes are similar between trials. Vital status in posttrial periods must be assessed by national death databases or equivalent records.

Study Design

Randomized controlled trials with at least 1-year in-trial period and a posttrial follow-up phase.

Language

No restriction (English and non-English studies).

Publication Type

Published and unpublished studies reported in peer-reviewed journals, reports, conference abstracts, and theses.

Search Methods for Identification of Studies

Randomized trials of BP-lowering therapies versus placebo or active comparator with posttrial follow-up periods will be identified using a 2-step process. First, randomized trials of BP-lowering therapy will be identified by (1) retrieving the references of trials included in published systematic reviews of BP-lowering therapy, (2) retrieving studies published by the BPLTTC, and (3) checking studies referenced in the 1993 WHO/ISH (World Health Organization/International Society of Hypertension) meeting memorandum on BP management [17]. To identify existing systematic reviews, we will search Medline Ovid using a combination of Medical Subject Headings and text word terms for BP-lowering regimes and high BP with a systematic review filter (see Multimedia Appendix 1). Web of Science will be used to retrieve the references of studies cited by the systematic reviews, and these will be exported to an Endnote file. To identify studies from the BPLTTC, a text word search in the title, abstract, and author fields will be conducted in Ovid Medline and the retrieved references will be exported to the Endnote file. Web of Science will be used to retrieve the references of studies cited in the WHO/ISH meeting memorandum and these will be exported to the Endnote file. After removing duplications, the Endnote file will be screened to identify randomized trials of BP-lowering therapies versus placebo or active comparators. In the second step of the search, posttrial follow-up studies will be identified by forward citation searching the randomized trials identified in step 1. Web of Science will be used for forward citation searches of each of the original trials, with the citations exported to another Endnote file. After the removal of duplications in the Endnote file, the file will be searched using terms related to extended follow-up (see Multimedia Appendix 2). The resulting titles and abstracts will be screened independently by two reviewers using the review eligibility criteria.

Study Selection

First, two independent reviewers will screen a small sample of papers found in the search to revise any unclear or inappropriate inclusion criteria. In the full selection process, two reviewers will independently scan the results of the search and determine the eligibility of the studies. In the initial screening of titles and abstracts, the studies will be included if they meet the inclusion criteria or they do not have enough information for exclusion. Rejected citations will be recorded and classified as irrelevant studies. All potentially relevant articles will be screened through full text for a final decision. If a paper does not have sufficient information to assess eligibility, we will attempt to contact the authors; the paper will be classified as a potentially relevant article and checked in sensitivity analyses if authors do not reply after one month. If we identify trials that meet our inclusion criteria but lack data on the posttrial follow-up period, we will run a forward citation search from those studies. If a study has multiple citations, we will report separate citations but analyze these reports as a single study. We will also liaise with the BPLTTC for any individual patient data from trials meeting our inclusion criteria.

Data Extraction and Quality Assessment

Data extraction forms (detailed in Textbox 1) and quality assessment forms will be piloted on a small group of studies. Two reviewers will independently perform data extraction and quality assessment in the prespecified form. If any disagreements arise, the reviewers will discuss consensus or consult with the third reviewer. A report of correction or amendments to the prespecified form will be recorded.

Information required for data extraction.

General information: reviewer performing data extraction, date of data extraction, and identification features of the study (eg, record number, authors, article title, type of publication, country of origin, the source of funding)

Study characteristics: aims of the study, study design, study inclusion and exclusion criteria, recruitment procedures (details of randomization, blinding), and unit of allocation (participant, GP practice)

Participant characteristics: baseline characteristics (age, gender, ethnicity, socioeconomic status, comorbidities, systolic BP, diastolic BP, weight, height, smoking status, serum total cholesterol, serum creatinine level), and the number of participants in active treatment group and control group

Intervention and setting: type and dose of BP-lowering regimen

Outcome data:

For each outcome: whether reported, definition, length of follow-up, number of events, number of participants in each event, odds ratio, risk ratio, and hazard ratio

For both intervention groups: number of participants enrolled; number of participants included in analysis; and number of withdrawals, exclusions, and lost to follow-up

Type of analysis used in the study: intention to treat or per protocol

Quality Assessment

The risk of bias will be assessed by two reviewers following the Cochrane Risk of bias tool [18] which includes the following criteria: random sequence generation (selection bias); allocation concealment (selection bias); blinding of participants, personnel, and outcome (performance and detection bias); and incomplete outcome data (attrition bias). The bias will be assessed as unclear, low-risk, or high-risk. Publication bias will be judged by observing the asymmetry of funnel plots; if they are asymmetric, contour-enhanced funnel plots will then be analyzed to examine whether publication bias alone caused the asymmetry. We will also use Egger’s meta-regression model to assess the relationship between the observed effect sizes and the size of studies [19].

Data Synthesis and Analysis

After pooling all eligible studies, we will design a fixed-effect model and assess the heterogeneity by visually inspecting the forest plots, Chi-squared tests, and I²tests. Statistical heterogeneity will be recorded when the studies’ confidence intervals exhibit poor overlap, the P-value of the test of heterogeneity is 0.1 or lower, or the I²value is 0.5 or greater. In these cases, we will also perform an analysis using a random-effects model. All trial endpoints will be treated as dichotomous variables and grouped by time from randomization. In the fixed-effect model, the Mantel-Haenszel method model will be used to combine risk ratios of each outcome [20]. We will conduct a subgroup analysis in which available risk calculators will be used to stratify participants by the baseline absolute CVD risk for fatal and nonfatal CVD events. In a sensitivity analysis, each study will be removed (one at a time) to assess the impact of each study on the pooled outcomes. The Cochrane software (Revman) [21] will be used for meta-analysis, selective reporting, and other sources of bias.

Ethics and Dissemination

This systematic review will analyze nonidentifiable data; thus, a formal ethics approval is unlikely to be crucial. The study protocol was registered with the International Prospective Register of Systematic Review (PROSPERO) with the reference number CRD42017058414. The current study will contribute a chapter of a PhD thesis (CH).

Results

We are currently in the process of developing the search strategy. The search in Medline via Ovid has been piloted and modified. The analysis is expected to complete before June 2018.

Discussion

Given the strong beliefs held by many clinicians that early treatment of elevated BP is necessary to prevent CVD events, it is not possible to conduct a randomized controlled trial of early versus late treatment at present. This is particularly true for patients with mildly elevated BP and low CVD risk, as studies would require a large sample size of participants or a long follow-up period because approximately 10% of CVD events are expected to occur within 10 years. In addition, clinicians are questioning the real benefits, adverse effects, and medical costs of the life-long intervention of BP-lowering drug treatment. The findings of this study will contribute to the body of knowledge concerning the beneficial, neutral, or harmful effects of delayed BP-lowering drug treatment in patients with mildly elevated BP and low-to-moderate CVD risk.

Limitations

Due to the changes in definitions of CVD and diagnostic methods used over time, we predict that it will be difficult to combine these outcomes in a meta-analysis. This issue inherently generates bias in selection, detection, attrition, and reporting.

Multimedia Appendix 1

Search strategy developed for Medline via Ovid to identify existing systematics review.

Multimedia Appendix 2

Search terms related to extended follow-up.

Abbreviations

blood pressure

BPLTTC

Blood Pressure Lowering Treatment Trialists’ Collaboration

CVD

cardiovascular disease

FRS

Framingham Risk Score

HOPE-3

Heart Outcomes Prevention Evaluation trial

WHO/ISH

World Health Organization/International Society of Hypertension

CLBH is a PhD candidate at Menzies Institute for Medical Research, and has received a PhD scholarship from Merle Weaver Postgraduate Scholarship. JD is supported by National Health and Medical Research Council Screening and Test Evaluation Program Grant 633003. CR is supported by a National Health and Medical Research Council Senior Research Fellowship (1045862).

MRN has served on an advisory board for AMGEN in the last 5 years. All other authors declare no conflicts of interest.

World Health Organization

Fact sheet - Cardiovascular disease (CVDs) 2016

2017-03-22

http://www.who.int/mediacentre/factsheets/fs317/en/

National Vascular Disease Prevention Alliance

Guidelines for the management of absolute cardiovascular disease risk 2012

2017-08-27

http://www.cvdcheck.org.au/index.php?option=com_content&view=article&id=47&Itemid=27

New Zealand Guidelines Group

The assessment and management of cardiovascular risk 2003

2017-08-27

Wellington, New Zealand

https://www.health.govt.nz/system/files/documents/publications/cvd_risk_full.pdf

National Clinical Guideline Centre UK

Hypertension: the clinical management of primary hypertension in adults: update of clinical guidelines 18 and 34

National Institute for Health and Clinical Excellence: Guidance 2011 08

22855971

Mancia

Fagard

Narkiewicz

Redon

Zanchetti

Böhm

Christiaens

Cifkova

De Backer

Dominiczak

Galderisi

Grobbee

Jaarsma

Kirchhof

Kjeldsen

Laurent

Manolis

Nilsson

Ruilope

Schmieder

Sirnes

Sleight

Viigimaa

Waeber

Zannad

Task Force for the Management of Arterial Hypertension of the European Society of Hypertension and the European Society of Cardiology

2013 ESH/ESC practice guidelines for the management of arterial hypertension

Blood Press 2014 02 23 1 3 16

10.3109/08037051.2014.868629

24359485

James

Oparil

Carter

Cushman

Dennison-Himmelfarb

Handler

Lackland

LeFevre

MacKenzie

Ogedegbe

Smith

Svetkey

Taler

Townsend

Wright

Narva

Ortiz

2014 evidence-based guideline for the management of high blood pressure in adults: report from the panel members appointed to the Eighth Joint National Committee (JNC 8)

JAMA 2014 02 05 311 5 507 20

10.1001/jama.2013.284427

24352797

1791497

Law

Morris

Wald

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 05 19 338 b1665

19454737

PMC2684577

Jansen

Bonner

McKinn

Irwig

Glasziou

Doust

Teixeira-Pinto

Hayen

Turner

McCaffery

General practitioners' use of absolute risk versus individual risk factors in cardiovascular disease prevention: an experimental study

BMJ Open 2014 05 15 4 5 e004812

10.1136/bmjopen-2014-004812

24833688

bmjopen-2014-004812

PMC4025465

Morales

Coca

Olsen

Sanchez

Sebba-Barroso

Kones

Bertomeu-Martinez

Sobrino

Alcocer

Pineiro

Lanas

Machado

Aguirre-Palacios

Ortellado

Perez

Sabio

Landrove

Rodriguez-Leyva

Duenas-Herrera

Rodriguez

Parra-Carrillo

Piskorz

Bryce-Moncloa

Waisman

Yano

Ventura

Orias

Prabhakaran

Sundström

Wang

Burrell

Schutte

Lopez-Jaramillo

Barbosa

Redon

Weber

Lavie

Ramirez

Ordunez

Yusuf

Zanchetti

Clinical perspective on antihypertensive drug treatment in adults with grade 1 hypertension and low-to-moderate cardiovascular risk: an international expert consultation

Curr Probl Cardiol 2017 07 42 7 198 225

10.1016/j.cpcardiol.2017.03.001

28552207

S0146-2806(17)30043-9

Lonn

Bosch

López-Jaramillo

Zhu

Liu

Pais

Diaz

Xavier

Sliwa

Dans

Avezum

Piegas

Keltai

Chazova

Peters

RJG

Held

Yusoff

Lewis

Jansky

Parkhomenko

Khunti

Toff

Reid

Varigos

Leiter

Molina

McKelvie

Pogue

Wilkinson

Jung

Dagenais

Yusuf

HOPE-3 Investigators

Blood-pressure lowering in intermediate-risk persons without cardiovascular disease

N Engl J Med 2016 05 26 374 21 2009 20

10.1056/NEJMoa1600175

27041480

Thomopoulos

Parati

Zanchetti

Effects of blood pressure lowering on outcome incidence in hypertension: 2. Effects at different baseline and achieved blood pressure levels--overview and meta-analyses of randomized trials

J Hypertens 2014 12 32 12 2296 304

10.1097/HJH.0000000000000379

25259547

McGorrian

Yusuf

Islam

Jung

Rangarajan

Avezum

Prabhakaran

Almahmeed

Rumboldt

Budaj

Dans

Gerstein

Teo

Anand

INTERHEART Investigators

Estimating modifiable coronary heart disease risk in multiple regions of the world: the INTERHEART Modifiable Risk Score

Eur Heart J 2011 03 32 5 581 9

10.1093/eurheartj/ehq448

21177699

ehq448

Kostis

Cabrera

Cheng

Cosgrove

Deng

Pressel

Davis

Association between chlorthalidone treatment of systolic hypertension and long-term survival

JAMA 2011 12 21 306 23 2588 93

10.1001/jama.2011.1821

22187278

306/23/2588

Hypertension Detection and Follow-up Program Cooperative Group

Persistence of reduction in blood pressure and mortality of participants in the Hypertension Detection and Follow-up Program

JAMA 1988 04 08 259 14 2113 22

3346988

Nelson

Chowdhury

Doust

Reid

Wing

Ten-year legacy effects of baseline blood pressure 'treatment naivety' in the Second Australian National Blood Pressure study

J Hypertens 2015 11 33 11 2331 7

10.1097/HJH.0000000000000709

26335432

Blood Pressure Lowering Treatment Trialists' Collaboration Sundström

Arima

Woodward

Jackson

Karmali

Lloyd-Jones

Baigent

Emberson

Rahimi

MacMahon

Patel

Perkovic

Turnbull

Neal

Blood pressure-lowering treatment based on cardiovascular risk: a meta-analysis of individual patient data

Lancet 2014 08 16 384 9943 591 8

10.1016/S0140-6736(14)61212-5

25131978

S0140-6736(14)61212-5

Zanchetti

Chalmers

Arakawa

Gyarfas

Hamet

Hansson

Julius

MacMahon

Mancia

Ménard

The 1993 guidelines for the management of mild hypertension: memorandum from a WHO/ISH meeting

Blood Press 1993 06 2 2 86 100

8180730

Higgins

Altman

Gøtzsche

Jüni

Moher

Oxman

Savovic

Schulz

Weeks

Sterne

Cochrane Bias Methods Group Cochrane Statistical Methods Group

The Cochrane Collaboration's tool for assessing risk of bias in randomised trials

BMJ 2011 10 18 343 d5928

22008217

PMC3196245

Chaimani

Mavridis

Salanti

A hands-on practical tutorial on performing meta-analysis with Stata

Evid Based Ment Health 2014 11 17 4 111 6

10.1136/eb-2014-101967

25288685

eb-2014-101967

Mantel

Haenzel

Statistical aspects of the analysis of data from retrospective studies of disease

J Natl Cancer Inst 1959 04 22 4 719 48

13655060

The Cochrane Collaboration

Review Manager (RevMan) 2014

2017-08-29

Copenhagen: The Nordic Cochrane Centre

[Computer program]. Version 5.3 http://community.cochrane.org/tools/review-production-tools/revman-5/about-revman-5