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ABCG2常见的功能失调变异体对高尿酸血症进展的影响比典型环境危险因素更强。

Common dysfunctional variants of ABCG2 have stronger impact on hyperuricemia progression than typical environmental risk factors.

作者信息

Nakayama Akiyoshi, Matsuo Hirotaka, Nakaoka Hirofumi, Nakamura Takahiro, Nakashima Hiroshi, Takada Yuzo, Oikawa Yuji, Takada Tappei, Sakiyama Masayuki, Shimizu Seiko, Kawamura Yusuke, Chiba Toshinori, Abe Junko, Wakai Kenji, Kawai Sayo, Okada Rieko, Tamura Takashi, Shichijo Yuka, Akashi Airi, Suzuki Hiroshi, Hosoya Tatsuo, Sakurai Yutaka, Ichida Kimiyoshi, Shinomiya Nariyoshi

机构信息

1] Department of Integrative Physiology and Bio-Nano Medicine, National Defense Medical College, 3-2 Namiki, Tokorozawa, Saitama 359-8513, Japan [2] Medical Group, Headquarters, Iwo-to Air Base Group, Japan Air Self-Defense Force, Iwo-to, Ogasawara, Tokyo 100-2100, Japan [3].

1] Department of Integrative Physiology and Bio-Nano Medicine, National Defense Medical College, 3-2 Namiki, Tokorozawa, Saitama 359-8513, Japan [2].

出版信息

Sci Rep. 2014 Jun 9;4:5227. doi: 10.1038/srep05227.

Abstract

Gout/hyperuricemia is a common multifactorial disease having typical environmental risks. Recently, common dysfunctional variants of ABCG2, a urate exporter gene also known as BCRP, are revealed to be a major cause of gout/hyperuricemia. Here, we compared the influence of ABCG2 dysfunction on serum uric acid (SUA) levels with other typical risk factors in a cohort of 5,005 Japanese participants. ABCG2 dysfunction was observed in 53.3% of the population investigated, and its population-attributable risk percent (PAR%) for hyperuricemia was 29.2%, much higher than those of the other typical environmental risks, i.e. overweight/obesity (BMI ≥ 25.0; PAR% = 18.7%), heavy drinking (>196 g/week (male) or >98 g/week (female) of pure alcohol; PAR% = 15.4%), and aging (≥60 years old; PAR% = 5.74%). SUA significantly increased as the ABCG2 function decreased (P = 5.99 × 10(-19)). A regression analysis revealed that ABCG2 dysfunction had a stronger effect than other factors; a 25% decrease in ABCG2 function was equivalent to "an increase of BMI by 1.97-point" or "552.1 g/week alcohol intake as pure ethanol" in terms of ability to increase SUA. Therefore, ABCG2 dysfunction originating from common genetic variants has a much stronger impact on the progression of hyperuricemia than other familiar risks. Our study provides a better understanding of common genetic factors for common diseases.

摘要

痛风/高尿酸血症是一种常见的多因素疾病,存在典型的环境风险。最近,尿酸转运蛋白基因ABCG2(也称为BCRP)的常见功能失调变异被发现是痛风/高尿酸血症的主要病因。在此,我们在一个由5005名日本参与者组成的队列中,比较了ABCG2功能障碍与其他典型风险因素对血清尿酸(SUA)水平的影响。在所调查的人群中,53.3%的人存在ABCG2功能障碍,其对高尿酸血症的人群归因风险百分比(PAR%)为29.2%,远高于其他典型环境风险因素,即超重/肥胖(BMI≥25.0;PAR% = 18.7%)、大量饮酒(男性纯酒精摄入量>196克/周或女性>98克/周;PAR% = 15.4%)和衰老(≥60岁;PAR% = 5.74%)。随着ABCG2功能下降,SUA显著升高(P = 5.99×10⁻¹⁹)。回归分析显示,ABCG2功能障碍比其他因素的影响更强;就增加SUA的能力而言,ABCG2功能降低25%相当于“BMI增加1.97个点”或“每周纯乙醇酒精摄入量增加552.1克”。因此,常见基因变异导致的ABCG2功能障碍对高尿酸血症进展的影响比其他常见风险因素更强。我们的研究有助于更好地理解常见疾病的常见遗传因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f0d/5381477/4d326f1ff126/srep05227-f1.jpg

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