可信遗传因素与 GLP1-RA 和减肥手术导致的体重减轻之间的关系:对来自 9 个生物库的 10 960 人进行的一项多学科研究

Jakob German, Mattia Cordioli, Sarah Urbut, Veronica Tozzo, Kadri Arumae, Roelof A.J. Smit, Jiwoo Lee, Josephine Li, Adrian Janucik, Yi Ding, Akintunde Akinkuolie, Henrike Heyne, Andrea Eoli, Chadi Saad, Yasser Al-Sarraj, Rania Abdel-latif, Alexandra Barry, Zhe Wang, Estonian Biobank research team, Pradeep Natarajan, Samuli Ripatti, Anthony Philippakis, Bogdan Pasaniuc, Lukasz Szczerbinski, Adam Kretowski, Hamdi Mbarek, Ruth J.F. Loos, Uku Vainik, Andrea Ganna
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引用次数: 0

摘要

肥胖症是一个重大的公共卫生问题。主要用于治疗 2 型糖尿病的 GLP-1 受体激动剂(GLP1-RA)是一种很有前景的减肥药物,而减肥手术(BS)仍然是一种持久但具有侵入性的干预措施。尽管在减肥效果方面观察到了异质性,但尚未在大样本量中广泛探讨 GLP1-RA 和 BS 对减肥的遗传影响,而且大多数研究都侧重于种族和民族的差异,而不是遗传血统。我们对来自 6 个国家 9 项多血统生物库研究的 10,960 人进行了研究,以了解遗传因素(以前曾被证明会影响体重)是否会影响 GLP1-RA 治疗或 BS 的减肥效果。GLP1-RA使用者在开始治疗后6至12个月之间的平均体重变化为-3.93%,不同基因血统之间的差异很小。BS患者在手术后6至48个月之间的体重变化为-21.17%。经多重检验校正后,GLP1-RA导致的体重减轻与BMI或2型糖尿病的多基因评分或GLP1R、PCSK1和APOE基因中的特定错义变体之间没有明显关联。然而,BMI 的多基因评分越高,BS 后的体重减轻率就越低(多基因评分每变化 1 个标准差,体重减轻率为 +0.7%,P = 1.24x10-4)。相反,基线体重越高,体重减轻的幅度越大。我们的研究结果表明,现有的与体重和 2 型糖尿病有关的多基因评分以及药物靶基因中的错义变异对 GLP1-RA 的有效性影响不大。我们的研究结果还证实了这些疗法在所有主要大陆血统群体中的有效性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Association between plausible genetic factors and weight loss from GLP1-RA and bariatric surgery: a multi-ancestry study in 10 960 individuals from 9 biobanks
Obesity is a significant public health concern. GLP-1 receptor agonists (GLP1-RA), predominantly in use as a type 2 diabetes treatment, are a promising pharmacological approach for weight loss, while bariatric surgery (BS) remains a durable, but invasive, intervention. Despite observed heterogeneity in weight loss effects, the genetic effects on weight loss from GLP1-RA and BS have not been extensively explored in large sample sizes, and most studies have focused on differences in race and ethnicity, rather than genetic ancestry. We studied whether genetic factors, previously shown to affect body weight, impact weight loss due to GLP1-RA therapy or BS in 10,960 individuals from 9 multi-ancestry biobank studies in 6 countries. The average weight change between 6 and 12 months from therapy initiation was -3.93% for GLP1-RA users, with marginal differences across genetic ancestries. For BS patients the weight change between 6 and 48 months from the operation was -21.17%. There were no significant associations between weight loss due to GLP1-RA and polygenic scores for BMI or type 2 diabetes or specific missense variants in the GLP1R, PCSK1 and APOE genes, after multiple-testing correction. However, a higher polygenic score for BMI was significantly linked to lower weight loss after BS (+0.7% for 1 standard deviation change in the polygenic score, P = 1.24x10-4). In contrast, higher weight at baseline was associated with greater weight loss. Our findings suggest that existing polygenic scores related to weight and type 2 diabetes and missense variants in the drug target gene do not have a large impact on GLP1-RA effectiveness. Our results also confirm the effectiveness of these treatments across all major continental ancestry groups considered.
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