Undiagnosed G6PD Deficiency in Black and Asian Individuals Is Prevalent and Contributes to Health Inequalities in Type 2 Diabetes Diagnosis and Complications.

IF 16.6
Diabetes care Pub Date : 2025-09-30 DOI:10.2337/dc25-0556
Susan Martin, Miriam Samuel, Daniel Stow, Alys M Ridsdale, Ji Chen, Katherine G Young, Harry D Green, Andrew T Hattersley, Veline L'Esperance, Trevelyan J McKinley, Sarah Finer, Inês Barroso
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Abstract

Objective: Glucose-6-phosphate dehydrogenase (G6PD) deficiency presents silently and is not routinely screened. It is associated with markedly lower HbA1c for the prevailing glucose levels. Since HbA1c is internationally recommended to diagnose and manage type 2 diabetes (T2D), we investigated the population-level impact of undiagnosed G6PD deficiency on T2D diagnosis and complications in the U.K.

Research design and methods: We used whole-exome sequencing and electronic health record data from UK Biobank (n = 467,368) and Genes & Health (n = 43,011) cohorts.

Results: In the U.K., we estimated that ∼1 in 7 Black and 1 in 63 Asian males carry G6PD deficiency alleles, compared with fewer than 1 in 10,000 White males. Despite this, less than 1 in 50 G6PD-deficient men are clinically recognized. Male G6PD carriers have considerably lower average HbA1c (0.9% [International Federation of Clinical Chemistry and Laboratory Medicine: 10.0 mmol/mol]) compared with noncarriers, while differences in average glucose were negligible. G6PD-deficient men had 1.37 (95% CI: 1.01, 1.86) higher odds of developing diabetes-related microvascular complications than noncarriers. Although risk factors were similar prior to diagnosis, male G6PD carriers diagnosed with T2D since 2011 were, on average, 4.1 years (95% CI: 0.6, 7.7) older at diagnosis compared with noncarriers. In addition, lower mean HbA1c values in G6PD carriers falsely underestimated their 10-year T2D risk.

Conclusions: Undiagnosed G6PD deficiency has significant impact on T2D diagnosis with HbA1c and associates with increased risk of diabetes complications. This has major implications for global populations using HbA1c for diagnosis and monitoring, and could contribute significantly to inequalities in diabetes outcomes.

未确诊的G6PD缺乏症在黑人和亚洲人中普遍存在,并导致2型糖尿病诊断和并发症的健康不平等。
目的:葡萄糖-6-磷酸脱氢酶(G6PD)缺乏症表现不明显,不能常规筛查。它与当前血糖水平的HbA1c显著降低有关。由于HbA1c在国际上被推荐用于诊断和治疗2型糖尿病(T2D),我们研究了未确诊的G6PD缺乏症对英国T2D诊断和并发症的人群水平影响。研究设计和方法:我们使用了来自英国生物银行(n = 467,368)和基因与健康(n = 43,011)队列的全外展子组测序和电子健康记录数据。结果:在英国,我们估计每7名黑人男性和63名亚洲男性中就有1名携带G6PD缺陷等位基因,相比之下,每10,000名白人男性中不到1名携带G6PD缺陷等位基因。尽管如此,只有不到1 / 50的g6pd缺陷男性被临床确诊。与非携带者相比,男性G6PD携带者的平均HbA1c显著降低(0.9%[国际临床化学和检验医学联合会:10.0 mmol/mol]),而平均葡萄糖的差异可以忽略不计。g6pd缺乏的男性发生糖尿病相关微血管并发症的几率比非携带者高1.37 (95% CI: 1.01, 1.86)。尽管诊断前的危险因素相似,但自2011年以来诊断为T2D的男性G6PD携带者在诊断时平均比非携带者老4.1岁(95% CI: 0.6, 7.7)。此外,G6PD携带者较低的平均HbA1c值错误地低估了其10年T2D风险。结论:未确诊的G6PD缺乏症对T2D的HbA1c诊断有显著影响,并与糖尿病并发症的风险增加相关。这对全球使用HbA1c进行诊断和监测的人群具有重要意义,并可能显著导致糖尿病结局的不平等。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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CiteScore
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