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首页> 外文期刊>The Lancet Global Health >Kidney damage and associated risk factors in rural and urban sub-Saharan Africa (AWI-Gen): a cross-sectional population study
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Kidney damage and associated risk factors in rural and urban sub-Saharan Africa (AWI-Gen): a cross-sectional population study

机译:农村和城市撒哈拉非洲(AWI-Gen)的肾脏损伤及相关危险因素:横截面人口研究

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Summary Background Rapid epidemiological health transitions occurring in vulnerable populations in Africa that have an existing burden of infectious and non-communicable diseases predict an increased risk and consequent prevalence of kidney disease. However, few studies have characterised the true burden of kidney damage and associated risk factors in Africans. We investigated the prevalence of markers for kidney damage and known risk factors in rural and urban settings in sub-Saharan Africa. Methods In this cross-sectional population study (Africa Wits-International Network for the Demographic Evaluation of Populations and their Health Partnership for Genomic Studies [AWI-Gen]), we recruited unrelated adult participants aged 40–60 years from four rural community research sites (Nanoro, Burkina Faso; Navrongo, Ghana; Agincourt and Dikgale, South Africa), and two urban community research sites (Nairobi, Kenya; and Soweto, South Africa). Participants were identified and selected using random sampling frames already in use at each site. Participants completed a lifestyle and medical history questionnaire, had anthropometric and blood pressure measurements taken, and blood and urine samples were collected. Markers of kidney damage were defined as low estimated glomerular filtration rate (eGFR; 60 mL/min per 1·73 m23 mg/mmol); or chronic kidney disease (low eGFR or albuminuria, or both). We calculated age-adjusted prevalence of chronic kidney disease, low eGFR, and albuminuria by site and sex and used logistic regression models to assess risk factors of kidney damage. Findings Between August, 2013, and August, 2016, we recruited 10?702 participants, of whom 8110 were analysable. 4120 (50·8%) of analysable participants were male, with a mean age of 49·9 years (SD 5·8). Age-standardised population prevalence was 2·4% (95% CI 2·1–2·8) for low eGFR, 9·2% (8·4–10·0) for albuminuria, and 10·7% (9·9–11·7) for chronic kidney disease, with higher prevalences in South African sites than in west African sites (14·0% [11·9–16·4] in Agincourt vs 6·6% [5·5–7·9] in Nanoro). Women had a higher prevalence of chronic kidney disease (12·0% [10·8–13·2] vs 9·5% [8·3–10·8]) and low eGFR (3·0% [2·6–3·6] vs 1·7% [1·3–2·3]) than did men, with no sex-specific differences for albuminuria (9·9% [8·8–11·0] vs 8·4% [7·3–9·7]). Risk factors for kidney damage were older age (relative risk 1·04, 95% CI 1·03–1·05; p0·0001), hypertension (1·97, 1·68–2·30; p0·0001), diabetes (2·22, 1·76–2·78; p0·0001), and HIV (1·65, 1·36–1·99; p0·0001); whereas male sex was protective (0·85, 0·73–0·98; p=0·02). Interpretation Regional differences in prevalence and risks of chronic kidney disease in sub-Saharan Africa relate in part to varying stages of sociodemographic and epidemiological health transitions across the area. Public health policy should focus on integrated strategies for screening, prevention, and risk factor management in the broader non-communicable disease and infectious diseases framework. Funding National Human Genome Research Institute, Office of the Director, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institute of Environmental Health Sciences, the Office of AIDS Research, and National Institute of Diabetes and Digestive and Kidney Diseases, all of the National Institutes of Health, and the South African Department of Science and Technology.
机译:摘要背景下存在于非洲脆弱群体中发生的快速流行病学健康转变,具有现有传染性和非传染性疾病的负担预测肾病的风险增加和随之而来的患病率。然而,很少有研究表征了非洲人肾脏损害的真正负担和相关的危险因素。我们调查了撒哈拉以南非洲农村和城市环境中肾脏损伤和已知风险因素的患病率。这种横断面口研究中的方法(非洲驾驶威尔士国际网络人口的人口和健康伙伴关系[AWI-Gen]),我们招募了40-60岁从四个农村社区研究网站的无关的成年参与者(Nanoro,Burkina Faso; Navrongo,加纳; agincourt和Dikgale,南非)和两个城市社区研究网站(内罗毕,肯尼亚;和南非Soweto和Soweto)。在每个站点上使用已使用的随机采样帧确定并选择参与者。参与者完成了一种生活方式和病史调查问卷,已经采取了人类测量和血压测量,并收集了血液和尿液样品。肾脏损伤标记被定义为低估计的肾小球过滤速率(EGFR;每1·73m 2 3 Mg / mmol的<60ml / min);或慢性肾病(低EGFR或白蛋白尿或两者)。我们通过现场和性别和使用逻辑回归模型计算慢性肾病,低EGFR和白蛋白尿的年龄调整的患病率,以评估肾脏损伤的风险因素。 2016年8月和2016年8月之间的调查结果,我们招募了10个?702名参与者,其中8110名分析。 4120(50·8%)分配参与者是男性,平均年龄为49·9岁(SD 5·8)。年龄标准化人口患病率为2·4%(95%CI 2·1-2·8),用于白蛋白尿的9·2%(8·4-10·0),10·7%(9· 9-11·7)对于慢性肾病,南非遗址普遍存在于西非网站(14·0%[11·9-16·4],agincourt与6·6%[5·5-7 ·9]在纳米洛)。女性患有慢性肾病的患病率较高(12·0%[10·8-13·2] Vs 9·5%[8·3-10·8])和低EGFR(3·0%[2·6 -3·6] Vs 1·7%[1·3-2·3])比男性没有性别特异性差异(9·9%[8·8-11·0] Vs 8·4 %[7·3-9·7])。肾脏损伤的危险因素较老龄(相对风险1·04,95%CI 1·03-1·05; P <0·0001),高血压(1·97,1·68-2·30; P <0 ·0001),糖尿病(2·22,1·76-2·78; P <0·0001),HIV(1·65,13-1·99; P <0·0001);虽然男性是保护性的(0·85,0·73-0·98; p = 0·02)。解释亚撒哈拉以南非洲慢性肾病患病率和风险的区域差异有关该地区各种社会造影和流行病学卫生转型的不同阶段。公共卫生政策应专注于在更广泛的非传染病和传染病框架中筛选,预防和危险因素管理的综合策略。资助国家人体基因组研究所,董事办公室,巩膜肯尼迪席位国家儿童健康与人类发展研究所,国家环境保健研究所,艾滋病研究所,以及国家糖尿病和消化和肾病,全部国家卫生研究院,以及南非科技系。

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