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Journal ArticleDOI

Global and regional mortality from 235 causes of death for 20 age groups in 1990 and 2010: a systematic analysis for the Global Burden of Disease Study 2010

Rafael Lozano1, Mohsen Naghavi1, Kyle J Foreman2, Stephen S Lim1  +192 moreInstitutions (95)
15 Dec 2012-The Lancet (Elsevier)-Vol. 380, Iss: 9859, pp 2095-2128
TL;DR: The Global Burden of Diseases, Injuries, and Risk Factors Study 2010 aimed to estimate annual deaths for the world and 21 regions between 1980 and 2010 for 235 causes, with uncertainty intervals (UIs), separately by age and sex, using the Cause of Death Ensemble model.
About: This article is published in The Lancet.The article was published on 2012-12-15 and is currently open access. It has received 11809 citations till now. The article focuses on the topics: Mortality rate & Years of potential life lost.

Summary (6 min read)

Jump to: [Introduction][Data and methods][Database development][Population-based cancer registries][Police reports][Health facility data][Cause of Death Ensemble modeling (CODEm)][Negative binomial models][Fixed proportion models][Natural History Models][Mortality Shock Regressions][Combining Results for Individual Causes of Death to Generate Final Estimates][Ranking lists][Epidemiological Factors][Global Causes of Death][Discussion][Author Contributions][Figures and Tables] and [70 Bates M, O’Grady J, Mudenda V, Shibemba A, Zumla A. New global estimates of malaria deaths.]

Introduction

  • Cause-specific mortality is arguably one of the most fundamental metrics of population health.
  • For the remaining deaths which are not medically certified, many different data sources and diagnostic approaches must be used from surveillance systems, demographic research sites, surveys, censuses, disease registries, and police records to construct a consolidated picture of causes of death in various populations.
  • These efforts often include very specific steps undertaken for different data sources and are frequently poorly documented.
  • GBD revisions for 1999, 2000, 2001, 2002, 2004, and 2008 have used these compositional models to allocate deaths according to three broad cause groups: communicable, maternal, neonatal, and nutritional causes; noncommunicable diseases; and injuries.
  • 38 Given the profusion of statistical modeling options, an important innovation has been the reporting of out-of-sample predictive validity to document the performance of complex models.

Data and methods

  • Some general aspects of the analytical framework such as the creation of the 21 GBD regions and the full hierarchical cause list including the mapping of the International Classification of Diseases and Injuries (ICD) to the GBD cause list are reported elsewhere.
  • While results are reported in this paper at the regional level for 1990 and 2010, the cause of death analysis has been undertaken at the country level for 187 countries from 1980 to 2010.
  • Using longer time series improves the performance of many types of estimation models; data prior to 1980, however, are much sparser for developing countries so the authors have restricted the analysis to 1980-2010.

Database development

  • Over the five year duration of the GBD 2010 study, the authors have sought to identify all published and unpublished data sources relevant to estimating causes of death for 187 countries from 1980 to 2010.
  • Web Table 1a provides a summary of the siteyears of data identified by broad type of data system and, similarly, Web Table 1b illustrates the number of site-years by GBD region.
  • Of the GBD regions, subSaharan Africa Central has the most limited evidence base with data on only 27 causes from at least one country.
  • In addition, there is country to country variation in the detail used to report causes of death included in national reporting lists, namely the basic tabulation list for ICD9, the ICD10 tabulation list, three digit and four digit detail, and special reporting lists.
  • Verbal autopsy data collected through sample registration systems, demographic surveillance systems, or surveys Verbal autopsy (VA) is a means for ascertaining the cause of death of individuals and the cause-specific mortality fractions in populations with incomplete vital registration systems.

Population-based cancer registries

  • Population-based cancer registries provide an important source of data on incidence of cancers in various countries.
  • The authors identified 2,715 site-years of cancer registry data across 93 countries.
  • The log of the MI ratio has been estimated as a function of national income per capita with random effects for country, year, and age.
  • The estimated mortality to incidence ratios have been used to map cancer registry data on incidence to expected deaths which have been incorporated into the database.
  • MI ratios by country, age, and sex are available on request.

Police reports

  • In most countries, police and crime reports are an important source of information for some types of injuries, notably road injuries and inter-personal violence.
  • The police reports used in this analysis were collected from published studies, national agencies, and institutional surveys such as the United Nations Crime Trends survey and the WHO Global Status Report on Road Safety Survey.30,41.
  • The authors identified 32 site-years of burial and mortuary data in 11 countries from ministries of health, published reports, and mortuaries themselves.
  • The authors also identified 52 surveys/censuses covering injury mortality across 65 survey/census years.
  • Surveillance data on the number of maternal deaths, or the maternal mortality ratio multiplied by births, were converted into cause fractions by dividing by the total number of deaths estimated in the reproductive age groups.

Health facility data

  • The authors chose to only incorporate deaths due to injury from this source because of known bias.
  • In settings where a data source does not capture all deaths in a population, the cause composition of deaths captured may be different than those that are not.
  • At the global level, the number of deaths estimated in 2010 for ARI and diarrhea for example differ by 0·9% and 1·2%, respectively, between models that include all data and those that exclude data where under-five death registration is below 70% complete.
  • Garbage codes are causes of death that should not be identified as underlying causes of death but have been entered as the underlying cause of death on death certificates.
  • For the GBD 2010, the authors have identified causes that should not be assigned as underlying cause of death at a much more detailed level.

Cause of Death Ensemble modeling (CODEm)

  • For all major causes of death except for HIV/AIDS and measles, the authors have used cause of death ensemble modeling – 133 causes in the cause list and three other special aggregates.
  • In addition, four families of statistical models are developed using covariates: mixed effects linear models of the log of the death rate, mixed effects linear models of the logit of the cause fraction, spatial-temporal Gaussian process regression (ST-GPR) models of the log of the death rate, and ST-GPR of the logit of the cause fraction.
  • 3) Based on out-of-sample predictive validity, the best performing model or ensemble is selected.
  • Web Table 6 summarizes the performance of the CODEm models developed for 133 causes in the cause list for which the authors exclusively use CODEm and three special aggregates in the GBD 2010.
  • In all cases the out-of-sample performance is worse (larger RMSE) than the in-sample performance.

Negative binomial models

  • For 13 causes, the number of deaths observed in the database is too low to generate stable estimates of out-of-sample predictive validity.
  • For these causes, the authors developed negative binomial models using plausible covariates.
  • These causes are identified in Web Table 5.
  • For these negative binomial models, standard model building practice was followed where plausible covariates were included in the model development and reverse stepwise procedures followed for covariate inclusion.
  • Uncertainty distributions were estimated using both uncertainty in the regression betas for the covariates and from the gamma distribution of the negative binomial.

Fixed proportion models

  • In 28 cases where death is a rare event, the authors have first modeled the parent cause in the GBD hierarchy using CODEm and then allocated deaths to specific causes using a fixed proportion.
  • Proportions have been computed using all available data in the database and are fixed over time, but, depending on data density, allowed to vary by region, age, or sex.
  • Finally, cellulitis, decubitus ulcer, other skin and subcutaneous diseases, abscess, impetigo, and other bacterial skin diseases all varied by age and sex.
  • The meta-regression have generated region-age-sex estimates with uncertainty of etiological fractions for diarrhea, LRI, meningitis, chronic kidney disease, maternal conditions, cirrhosis.
  • In the cases of cirrhosis, liver cancer, maternal conditions, and chronic kidney disease, the studies or datasets on etiology identify primary cause as assessed clinically; for diarrhea, LRI, and meningitis, etiology is based on laboratory findings.

Natural History Models

  • For a few selected causes, there is evidence that cause of death data systems do not capture sufficient information for one of two reasons.
  • Second, there are reasons to believe that there is systematic misclassification of deaths in cause of death data sources, particularly for congenital syphilis,54,55 whooping cough,56 measles,57 and HIV/AIDS.58.
  • In the case of HIV/AIDS, a hybrid approach has been used.
  • For 36 countries, with complete and high quality vital registration systems, the authors have used CODEm, in consultation with UNAIDS.
  • For the remaining countries, the authors have used the estimates with uncertainty by age and sex provided directly by UNAIDS based on their 2012 revision.

Mortality Shock Regressions

  • To estimate deaths directly due to natural disasters or collective violence, the authors use a different approach.
  • Details of this approach are outlined in Murray et al.59.
  • To develop the covariate on battle deaths during collective violence, the authors used data from the Armed Conflict Database from the International Institute for Strategic Studies (1997-2011), the Uppsala Conflict Data Program(UCDP)/PRIO Armed Conflict Dataset (1946-present), and available data from complete VR systems.
  • The relationships between under-five mortality and adult mortality and the disaster and collective violence covariates are estimated using 43 empirical observations for disasters and 206 empirical observations for collective violence (only years with over 1 per 10,000 crude death rate from shocks are kept in this analysis).
  • The relationship is estimated for excess mortality from these data sources by first subtracting from observed mortality rates the expected death rates in shock years using the methods outlined in Murray et al.59.

Combining Results for Individual Causes of Death to Generate Final Estimates

  • Given that the authors develop single cause models, it is imperative as a final step to ensure that individual cause estimates sum to the all-cause mortality estimate for each age-sex-country-year group.
  • The authors use a simple algorithm called CoDCorrect; at the level of each draw from the posterior distribution of each cause, they proportionately rescale each cause such that the sum of the cause-specific estimates equals the number of deaths from all causes generated from the demographic analysis.47.
  • The authors have chosen levels for each cause based on consideration of the amount and quality of available data.
  • Because there are substantially more data on all cardiovascular causes from verbal autopsy studies than for specific cardiovascular causes, the authors have designated “all cardiovascular” as a level 1 cause for CoDCorrect.

Ranking lists

  • For the presentation of leading causes of death, the level at which one ranks causes is subject to debate.
  • Given the GBD cause list tree structure, multiple options are possible such as all cancers versus sitespecific cancers.
  • The authors have opted to produce tables of rankings using the level of disaggregation that seems most relevant for public health decision-making.
  • The reference standard has been constructed using the lowest observed death rate in each age group across countries with a population greater than five million (see Murray et al39 for details).
  • Because the all-cause mortality analysis is undertaken, however, for more detailed age-groups up to age 110, the authors are able to take into account the mean age of death over 80 in each country-year-sex group in computing YLLs.

Epidemiological Factors

  • To help understand the drivers of change in the numbers of deaths by cause or region, the authors have decomposed change from 1990 to 2010 into growth in total population, change in population age- and sex-structure, and change in age- and sex-specific rates.
  • The difference between 2010 deaths and the population growth and aging scenario is the difference in death numbers due to epidemiological change in age- and sex-specific death rates.
  • Each of these three differences is also presented as a percent change with reference to the 1990 observed death number.
  • Further details on the data and methods used for specific causes of death is available on request.

Global Causes of Death

  • The GBD cause list divides causes into three broad groups.
  • With declining age-specific death rates from all three groups of causes, including noncommunicable diseases, the global shift towards noncommunicable diseases and injuries as leading causes of death is being driven by population growth and aging, and not by increases in age-sex-cause specific death rates.
  • Among communicable diseases, notably lower respiratory infections (194 thousand), diarrhea (77 thousand) and meningitis (46 thousand) account for the remaining neonatal deaths.
  • A number of causes have much larger uncertainty intervals than adjacent causes in the rank list.
  • At both time periods, there is substantial variation across regions in the relative importance of different causes, with communicable diseases and related causes being much more important in parts of sub-Saharan Africa and parts of Asia than in North Africa, and vascular diseases and cancer predominating in most other regions.

Discussion

  • The GBD 2010 is the most comprehensive and systematic analysis of causes of death undertaken to date.
  • The global health community can now draw on annual estimates of mortality, by age and sex, for 21 regions of the world, for each year from 1980 to 2010, for 235 separate causes, each with 95% uncertainty intervals to aid interpretation.
  • An innovative dimension of the GBD 2010 has been the addition of estimates of deaths due to different diarrhea and lower respiratory infection (LRI) pathogens.
  • First, cause of death data even in settings with medical certification may not always accurately capture the underlying cause of death.

Author Contributions

  • CJLM, ADL, and RL prepared the first draft.
  • RL, MN, KF, SL, KS, ADL, and CJLM finalized the draft based on comments from other authors and reviewer feedback.
  • ADL and CJLM conceived of the study and provided overall guidance.
  • All other authors developed cause-specific models, reviewed results, provided guidance on the selection of key covariates, and reviewed the manuscript.

Figures and Tables

  • Decomposition analysis of the change of global death numbers by broad cause groups from 1990 to 2010 into total population growth, population aging and changes in age-,sex-and cause-specific death rates.
  • Percentage of global deaths for females and males in 1990 and 2010 by cause and age.
  • The colors represent the various level one causes; blue is for non-communicable diseases, red is for communicable, maternal, neonatal and nutritional conditions, and green is for injuries.
  • The dashed lines signify descending order in rank, while the solid lines signify ascending order in rank.
  • Some cause abbreviations used in the figure are lower respiratory infections (“LRI”); ischemic heart disease (“IHD”); chronic obstructive pulmonary disorder (“COPD”); protein energy malnutrition (“PEM”); tuberculosis (“TB”); neonatal encephalopathy (“N Enceph”); neonatal sepsis (“N Sepsis”); road injuries (“Road Inj”); cancer (“CA”); and chronic kidney disease (“CKD”).

70 Bates M, O’Grady J, Mudenda V, Shibemba A, Zumla A. New global estimates of malaria deaths.

  • Global Enterics Mutli-Center Study (GEMS): University of Maryland School of Medicine.
  • Differences in the etiology of communityacquired pneumonia according to site of care: A population-based study.
  • Respiratory syncytial virus infection in elderly and high-risk adults.
  • Lancet 2011; 377: 1438–47. 92 Beaglehole R, Yach D. Globalisation and the prevention and control of non-communicable disease: the neglected chronic diseases of adults.
  • Population Health Metrics Research Consortium gold standard verbal autopsy validation study: design, implementation, and development of analysis datasets.

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Citations
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The early diagnosis and monitoring of squamous cell carcinoma via saliva metabolomics

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Qihui Wang1, Pan Gao1, Xiaoyi Wang1, Yixiang Duan1
Sichuan University1
01 May 2015-Scientific Reports
TL;DR: A comprehensive saliva metabonomics analysis for identifying potential biomarkers to early diagnose oral squamous cell carcinoma is successfully demonstrated, which has the advantages of non-invasive, simple, reliable, and low-cost.
Abstract: Early diagnosis of oral squamous cell carcinoma (OSCC) is an attractive strategy to increase survival rate of patient. An integrated separation approach of reversed phase liquid chromatography and hydrophilic interaction chromatography combining with time of flight mass spectrometer has been firstly developed for performing global saliva metabonomics analysis for early diagnosis of OSCC. This approach was designed to overcome the limitations of a single chromatographic method due to different polarity of endogenous metabolites. As a result, 14 potential salivary metabolites were identified. Eight biomarkers up-regulated in OSCC patients are compared with control and six down-regulated groups. Receiver operating characteristic analysis was exploited to evaluate the diagnostic power of the candidate biomarkers, and related metabolic pathways have also been studied. Five salivary biomarkers (propionylcholine, N-Acetyl-L-phenylalanine, sphinganine, phytosphingosine, and S-carboxymethyl-L-cysteine) in combination yielded satisfactory accuracy (AUC = 0.997), sensitivity (100%), and specificity (96.7%) in distinguishing early stage of OSCC from the control. In this study, a comprehensive saliva metabonomics analysis for identifying potential biomarkers to early diagnose OSCC is successfully demonstrated, which has the advantages of non-invasive, simple, reliable, and low-cost. These novel metabolic biomarkers have obvious clinical utility that will help to diagnose OSCC at its early stage.

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The Theory and Practice of “Nudging”: Changing Health Behaviors

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Ivo Vlaev1, Dominic King2, Paul Dolan3, Ara Darzi2
University of Warwick1, Imperial College London2, London School of Economics and Political Science3
01 Jul 2016-Public Administration Review
TL;DR: In this article, the authors consider the theoretical basis for why nudges might work and review the evidence in health behavior change and conclude that insights from behavioral economics offer powerful policy tools for influencing behavior in health care.
Abstract: Many of the most significant challenges in health care—such as smoking, overeating, and poor adherence to evidence-based guidelines—will only be resolved if we can influence behavior. The traditional policy tools used when thinking about influencing behavior include legislation, regulation, and information provision. Recently, policy analysts have shown interest in policies that “nudge” people in particular directions, drawing on advances in understanding that behavior is strongly influenced in largely automatic ways by the context within which it is placed. This article considers the theoretical basis for why nudges might work and reviews the evidence in health behavior change. The evidence is structured according to the Mindspace framework for behavior change. The conclusion is that insights from behavioral economics offer powerful policy tools for influencing behavior in health care. This article provides public administration practitioners with an accessible summary of this literature, putting these insights into practical use.

115 citations

Cites background from "Global and regional mortality from ..."

  • ...…Editor A significant part of the years of healthy life now lost worldwide are due to ‘lifestyle’ factors such as smoking, alcohol misuse and poor diet, with roughly one half of all deaths in the United States attributable to personal behaviors (Mokdad et al., 2004; WHO, 2009; Lozano et al., 2012)....

    [...]

  • ...A significant part of the years of healthy life now lost worldwide are due to ‘lifestyle’ factors such as smoking, alcohol misuse and poor diet, with roughly one half of all deaths in the United States attributable to personal behaviors (Mokdad et al., 2004; WHO, 2009; Lozano et al., 2012)....

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Journal ArticleDOI
The Elevated Susceptibility to Diabetes in India: An Evolutionary Perspective.

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Jonathan C. K. Wells1, Emma Pomeroy2, Subhash R. Walimbe, Barry M. Popkin3, Chittaranjan S. Yajnik4 
UCL Institute of Child Health1, McDonald Institute for Archaeological Research2, University of North Carolina at Chapel Hill3, King Edward Memorial Hospital4
07 Jul 2016-Frontiers in Public Health
TL;DR: Using stature as a marker of metabolic capacity, archeological and historical evidence is reviewed to highlight long-term declines in Indian stature associated with adaptation to several ecological stresses and the interpretation that elevated diabetic risk among Indian populations results from the high metabolic load imposed by westernized lifestyles.
Abstract: India has rapidly become a "diabetes capital" of the world, despite maintaining high rates of under-nutrition. Indians develop diabetes at younger age and at lower body weights than other populations. Here, we interpret these characteristics in terms of a "capacity-load" model of glucose homeostasis. Specifically, we assume that glycemic control depends on whether the body's "metabolic capacity," referring to traits, such as pancreatic insulin production and muscle glucose clearance, is able to resolve the "metabolic load" generated by high levels of body fat, high dietary glycemic load, and sedentary behavior. We employ data from modern cohorts to support the model and the interpretation that elevated diabetic risk among Indian populations results from the high metabolic load imposed by westernized lifestyles acting on a baseline of low metabolic capacity. We attribute this low metabolic capacity to the low birth weight characteristic of Indian populations, which is associated with short stature and low lean mass in adult life. Using stature as a marker of metabolic capacity, we review archeological and historical evidence to highlight long-term declines in Indian stature associated with adaptation to several ecological stresses. Underlying causes may include increasing population density following the emergence of agriculture, the spread of vegetarian diets, regular famines induced by monsoon failure, and the undermining of agricultural security during the colonial period. The reduced growth and thin physique that characterize Indian populations elevate susceptibility to truncal obesity, and increase the metabolic penalties arising from sedentary behavior and high glycemic diets. Improving metabolic capacity may require multiple generations; in the meantime, efforts to reduce the metabolic load will help ameliorate the situation.

114 citations

Journal ArticleDOI
Viral hepatitis and the Global Burden of Disease: a need to regroup

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Graham S Cooke1, Maud Lemoine, Mark Thursz, Charles Gore, Tracy Swan2, Adeeba Kamarulzaman, Philipp duCros, Nathan Ford3 
Imperial College London1, Treatment Action Group2, University of Cape Town3
01 Sep 2013-Journal of Viral Hepatitis
TL;DR: The publication of the updated Global Burden of Disease (GBD) provides a broad overview of the challenges to global health, with regrouped data indicating that viral hepatitis accounts for the loss of approximately 42 779 000 DALYs, just behind neonatal sepsis.
Abstract: The publication of the updated Global Burden of Disease (GBD) [1,2] provides a broad overview of the challenges to global health. As with the previous surveys [3], it is likely that over the coming years, the GBD will be used (and abused) to justify greater resources to combat different diseases. Whatever concerns there might exist about the robustness of the data, in the absence of any other systematic attempt to describe global disease, these data matter. How they are presented matters too, particularly in relation to viral hepatitis. In this survey, as in previous surveys, liver disease does not feature prominently in the overall global disease rankings. Cirrhosis, the highest liver-specific diagnosis, is ranked 23rd (C.I. 19–27) in the overall causes of disease (the same ranking as in the 1990 survey). Whilst of undoubted clinical and public health importance, cirrhosis is the final common end point for many different diseases, as is hepatocellular carcinoma (HCC). The same data can be presented differently to estimate the global needs for treatment and prevention of liver disease, in particular viral hepatitis. These data are important, given the progress in medical science that creates the potential for tackling viral hepatitis globally. The 2010 GBD spreads the burden of disease attributable to viral hepatitis across different categories, with lost Disability Adjusted Life Years (DALYs) presented separately for acute infection, cirrhosis and hepatocellular carcinoma (HCC). The choice of how different causes of disease are clustered for comparative ranking is often the cause for debate, and decisions are, in part, made ‘because of considerations related to public health programmes’ [1]. In this context, whether cirrhosis is the most useful grouping for overall rankings can be questioned, and regrouping the data can give an estimate for the global burden of viral hepatitis (see Table 1). These data are not perfect. In some cases, for example, the methodology for estimation uses prevalence data for infection rather than measures of disease itself [4], but high-quality prevalence data are lacking for many parts of the world. Estimating the burden of acute infection and end-stage disease requires assumptions that are open for debate. Nonetheless, these regrouped data indicate that viral hepatitis accounts for the loss of approximately 42 779 000 DALYs. How this would translate to a disease ranking is harder to predict as the final rankings are based on multiple simulation, but viral hepatitis would sit around 17th, just behind neonatal sepsis. Grouped together, viral hepatitis accounts for a greater loss of DALYs than many other communicable diseases (e.g. pneumococcal pneumonia). Taking a similar approach to mortality data alone (as opposed to DALYs) would put viral hepatitis into the top 10 leading causes of mortality, above TB and malaria. Such regrouped estimates may yet be underestimates given experience in Western settings [5]. For example, a substantial proportion of global HIV-related morbidity and mortality may be due to co-infection with viral hepatitis. How diseases are grouped together matters when it comes to allocation of public health resources and research funding. By bundling several widespread, treatable disorders that do not individually feature in the global burden of disease, the concept of neglected tropical diseases (NTDs) has proven helpful in increasing political attention, research and development funding, and disease control programmes for diseases such as schistosomiasis and trachoma, which would otherwise struggle to be visible. Even grouped together, the NTDs have a far lower burden of disease (as measured by DALYs) than viral hepatitis. Should viral hepatitis be bundled with all liver diseases to improve their profile? There are some reasons that this might be helpful, not least the existing professional organizations focussed on liver disease, and such organizations have an important role to play in improving the quality of hepatology services throughout the world. Amongst DALYs lost due to other liver diseases, alcohol provides by far the largest contribution. By grouping together alcohol-related liver disease with viral hepatitis, liver disease would rank above TB and diabetes in the 2010 GBD. However, if the

114 citations

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Alcohol Consumption and Mortality From Coronary Heart Disease: An Updated Meta-Analysis of Cohort Studies

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Jinhui Zhao1, Tim Stockwell1, Tim Stockwell2, Audra Roemer1, Timothy S. Naimi3, Tanya Chikritzhs2 
University of Victoria1, Curtin University2, Boston University3
21 May 2017-Journal of Studies on Alcohol and Drugs
TL;DR: In this paper, a meta-analysis of all 45 studies found significantly reduced CHD mortality for current low-volume drinkers (relative risk [RR] = 0.80, 95% CI [0.69, 0.93]) and all current drinkers (RR =0.88, 96% CI[0.78, 0., 0.99]).
Abstract: Objective:Previous meta-analyses estimate that low-volume alcohol consumption protects against coronary heart disease (CHD). Potential errors in studies include systematic misclassification of drinkers as abstainers, inadequate measurement, and selection bias across the life course.Method:Prospective studies of alcohol consumption and CHD mortality were identified in scholarly databases and reference lists. Studies were coded for potential abstainer biases and other study characteristics. The alcohol–CHD risk relationship was estimated in mixed models with controls for potential biases. Stratified analyses were performed based on variables identified as potential effect modifiers.Results:Fully adjusted meta-analysis of all 45 studies found significantly reduced CHD mortality for current low-volume drinkers (relative risk [RR] = 0.80, 95% CI [0.69, 0.93]) and all current drinkers (RR = 0.88, 95% CI [0.78, 0.99]). There was evidence of effect modification by cohort age, gender, ethnicity, and heart health a...

114 citations

References
More filters
Journal ArticleDOI
Estimates of worldwide burden of cancer in 2008: GLOBOCAN 2008.

[...]

Jacques Ferlay1, Hai-Rim Shin1, Freddie Bray1, David Forman1, Colin Mathers2, Donald Maxwell Parkin3 
International Agency for Research on Cancer1, World Health Organization2, University of Oxford3
15 Dec 2010-International Journal of Cancer
TL;DR: The results for 20 world regions are presented, summarizing the global patterns for the eight most common cancers, and striking differences in the patterns of cancer from region to region are observed.
Abstract: Estimates of the worldwide incidence and mortality from 27 cancers in 2008 have been prepared for 182 countries as part of the GLOBOCAN series published by the International Agency for Research on Cancer. In this article, we present the results for 20 world regions, summarizing the global patterns for the eight most common cancers. Overall, an estimated 12.7 million new cancer cases and 7.6 million cancer deaths occur in 2008, with 56% of new cancer cases and 63% of the cancer deaths occurring in the less developed regions of the world. The most commonly diagnosed cancers worldwide are lung (1.61 million, 12.7% of the total), breast (1.38 million, 10.9%) and colorectal cancers (1.23 million, 9.7%). The most common causes of cancer death are lung cancer (1.38 million, 18.2% of the total), stomach cancer (738,000 deaths, 9.7%) and liver cancer (696,000 deaths, 9.2%). Cancer is neither rare anywhere in the world, nor mainly confined to high-resource countries. Striking differences in the patterns of cancer from region to region are observed.

21,040 citations

The Global Burden of Disease Study

[...]

Christopher J L Murray, Alan D. Lopez
01 Jan 2003

11,232 citations

Journal ArticleDOI
Chronic kidney disease and the risks of death, cardiovascular events, and hospitalization

[...]

Alan S. Go1, Glenn M. Chertow, Dongjie Fan, Charles E. McCulloch, Chi-yuan Hsu 
Kaiser Permanente1
23 Sep 2004-The New England Journal of Medicine
TL;DR: The longitudinal glomerular filtration rate was estimated among 1,120,295 adults within a large, integrated system of health care delivery in whom serum creatinine had been measured between 1996 and 2000 and who had not undergone dialysis or kidney transplantation.
Abstract: Background End-stage renal disease substantially increases the risks of death, cardiovascular disease, and use of specialized health care, but the effects of less severe kidney dysfunction on these outcomes are less well defined. Methods We estimated the longitudinal glomerular filtration rate (GFR) among 1,120,295 adults within a large, integrated system of health care delivery in whom serum creatinine had been measured between 1996 and 2000 and who had not undergone dialysis or kidney transplantation. We examined the multivariable association between the estimated GFR and the risks of death, cardiovascular events, and hospitalization. Results The median follow-up was 2.84 years, the mean age was 52 years, and 55 percent of the group were women. After adjustment, the risk of death increased as the GFR decreased below 60 ml per minute per 1.73 m2 of body-surface area: the adjusted hazard ratio for death was 1.2 with an estimated GFR of 45 to 59 ml per minute per 1.73 m2 (95 percent confidence interval, 1....

9,642 citations

Journal ArticleDOI
A comparative risk assessment of burden of disease and injury attributable to 67 risk factors and risk factor clusters in 21 regions, 1990-2010: a systematic analysis for the Global Burden of Disease Study 2010

[...]

Stephen S Lim1, Theo Vos, Abraham D. Flaxman1, Goodarz Danaei2  +207 moreInstitutions (92)
15 Dec 2012-The Lancet
TL;DR: In this paper, the authors estimated deaths and disability-adjusted life years (DALYs; sum of years lived with disability [YLD] and years of life lost [YLL]) attributable to the independent effects of 67 risk factors and clusters of risk factors for 21 regions in 1990 and 2010.

9,324 citations

Book
The global burden of disease: a comprehensive assessment of mortality and disability from diseases injuries and risk factors in 1990 and projected to 2020.

[...]

Christopher J L Murray, Alan D. Lopez
01 Jan 1996
TL;DR: This is the first in a planned series of 10 volumes that will attempt to "summarize epidemiological knowledge about all major conditions and most risk factors" and use historical trends in main determinants to project mortality and disease burden forward to 2020.
Abstract: This is the first in a planned series of 10 volumes that will attempt to "summarize epidemiological knowledge about all major conditions and most risk factors;...generate assessments of numbers of deaths by cause that are consistent with the total numbers of deaths by age sex and region provided by demographers;...provide methodologies for and assessments of aggregate disease burden that combine--into the Disability-Adjusted Life Year or DALY measure--burden from premature mortality with that from living with disability; and...use historical trends in main determinants to project mortality and disease burden forward to 2020." This first volume includes chapters summarizing results from the project as a whole. (EXCERPT)

7,154 citations

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Global, regional, and national age-sex specific all-cause and cause-specific mortality for 240 causes of death, 1990-2013: A systematic analysis for the Global Burden of Disease Study 2013

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10 Jan 2015-The Lancet
Mohsen Naghavi, Haidong Wang, Rafael Lozano  +729 more
Frequently Asked Questions (15)
Q1. What have the authors contributed in "Global and regional mortality from 235 causes of death for 20 age- groups in 1990 and 2010: a systematic analysis" ?

In this paper, the authors proposed a method to provide timely and accurate information on causes of death by age and sex. 

Improved estimation of mortality from HIV/AIDS including uncertainty in the future will come both from continued progress in the estimation of the time course of the HIV epidemic by UNAIDS as well as further data on the levels of adult mortality in some key countries such as Nigeria. These are important both for the prioritization of existing treatments, such as rotavirus or pneumococcal vaccines, but also for the development of future technologies. When large multi-center studies such as GEMS publish their results this will be an important addition to the analysis ; future revisions of the GBD should make use of these results as they become available. The authors believe that for causes where the magnitude of these corrections is comparatively large, future research should be targeted to trying to build a better understanding of the strengths and weaknesses of the various data sources, whether epidemiological or demographic. 

Because of known bias in the epidemiological composition of burial and mortuary data, the authors only use information on the fraction of injuries due to specific sub-causes from these sources. 

Much could be learned about causes of death in countries where death certification is poor through the more widespread testing and application of recent advances in verbal autopsy methods which greatly reduce heterogeneity in diagnostic practices across populations where VA is currently used. 

By the post-neonatal period, causes of death are dominated by diarrhea, LRI, and other infectious diseases such as measles, among others. 

Because of the variety of data sources and their associated biases, cause of death assessments are inherently uncertain and subject to vigorous debate. 

The ambition to estimate mortality from 235 causes with uncertainty for 187 countries over time from 1980 to 2010 means that many choices about data sources, quality adjustments to data and modeling strategies had to be made. 

Although the authors report more disaggregated causes, because of considerations related to public health programs, the authors have chosen to include diarrheal diseases, lower respiratory infections, maternal causes, cerebrovascular disease, liver cancer, cirrhosis, drug use, road injury, exposure to mechanical forces, animal contact, homicide, and congenital causes in the ranking list. 

In addition, four families of statistical models are developed using covariates: mixed effects linear models of the log of the death rate, mixed effects linear models of the logit of the cause fraction, spatial-temporal Gaussian process regression (ST-GPR) models of the log of the death rate, and ST-GPR of the logit of the cause fraction. 

60–62The relationships between under-five mortality and adult mortality and the disaster and collective violence covariates are estimated using 43 empirical observations for disasters and 206 empirical observations for collective violence (only years with over 1 per 10,000 crude death rate from shocks are kept in this analysis). 

For 13 causes, the number of deaths observed in the database is too low to generate stable estimates of out-of-sample predictive validity. 

Opportunities for strengthening death registration, cause of death certification, and the more widespread use of verbal autopsy exist. 

The coefficients from these regressions and the disaster and collective violence covariates are used to predict excess deaths from these two causes. 

There are reasons, however, to also be concerned that deaths recorded in systems with low coverage may be biased towards selected causes that are more likely to occur in hospital. 

Although at the draw level the same scalar is applied to all causes, the net effect of CoDCorrect is to change the size of more uncertain causes by more than is done for more certain causes, a desirable property.