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散发性乳腺癌中的循环瘦素、可溶性瘦素受体、游离瘦素指数、内脂素以及特定的瘦素和瘦素受体基因多态性

Circulating leptin, soluble leptin receptor, free leptin index, visfatin and selected leptin and leptin receptor gene polymorphisms in sporadic breast cancer.

作者信息

Rodrigo Chrishani, Tennekoon Kamani Hemamala, Karunanayake Eric Hamilton, De Silva Kanishka, Amarasinghe Indrani, Wijayasiri Ananda

机构信息

Institute of Biochemistry, Molecular Biology and Biotechnology, University of Colombo, Colombo 03, 00300, Sri Lanka.

National Cancer Institute, Maharagama 10280, Sri Lanka.

出版信息

Endocr J. 2017 Apr 29;64(4):393-401. doi: 10.1507/endocrj.EJ16-0448. Epub 2017 Feb 11.

Abstract

Leptin and visfatin are implicated in breast cancer risk but studies accounting for bioavailability of leptin are sparse. Reports on the association of leptin gene (LEP) and leptin receptor gene (LEPR) polymorphisms with breast cancer are also inconsistent. Only a very few studies have examined biochemical and genetic variables concomitantly in the same cohort. A matched pairs study was carried out to ascertain whether plasma leptin, soluble leptin receptor, free leptin index (leptin/soluble leptin receptor), serum visfatin and selected LEP and LEPR polymorphisms are risk factors for sporadic breast cancer. Newly diagnosed sporadic breast cancer patients (N=80) were matched for age, body mass index (BMI) and menopausal status with healthy controls. Plasma leptin, soluble leptin receptor and serum visfatin were measured by enzyme-immunoassay. LEP -2548 A/G and LEPR K109R, LEPR Q223R polymorphisms were determined by genotyping. Leptin (p=0.0234), leptin/BMI (p=0.0468), free leptin index (p<0.0001) and visfatin (p=0.0002) were significantly higher and soluble leptin receptor (p<0.0001) was significantly lower in patients. LEPR gene K109R A/G polymorphism increased breast cancer risk (odds ratio: 4.125). Multivariate analysis confirmed that leptin, soluble leptin receptor, free leptin index and G109 (R109) allele of the LEPR gene K109R polymorphism are risk factors for breast cancer. When stratified by menopausal status free leptin index and soluble leptin receptor remained as risk factors irrespective of menopausal status while LEPR gene K109R A/G polymorphism remained as a risk factor only in the postmenopausal group.

摘要

瘦素和内脂素与乳腺癌风险有关,但考虑到瘦素生物利用度的研究较少。关于瘦素基因(LEP)和瘦素受体基因(LEPR)多态性与乳腺癌关联的报道也不一致。仅有极少数研究在同一队列中同时检测了生化和遗传变量。开展了一项配对研究,以确定血浆瘦素、可溶性瘦素受体、游离瘦素指数(瘦素/可溶性瘦素受体)、血清内脂素以及选定的LEP和LEPR多态性是否为散发性乳腺癌的危险因素。将新诊断的散发性乳腺癌患者(N = 80)与健康对照在年龄、体重指数(BMI)和绝经状态方面进行匹配。采用酶免疫分析法测定血浆瘦素、可溶性瘦素受体和血清内脂素。通过基因分型确定LEP -2548 A/G以及LEPR K109R、LEPR Q223R多态性。患者的瘦素(p = 0.0234)、瘦素/BMI(p = 0.0468)、游离瘦素指数(p < 0.0001)和内脂素(p = 0.0002)显著更高,而可溶性瘦素受体(p < 0.0001)显著更低。LEPR基因K109R A/G多态性增加了乳腺癌风险(比值比:4.125)。多变量分析证实,瘦素、可溶性瘦素受体、游离瘦素指数以及LEPR基因K109R多态性的G109(R109)等位基因是乳腺癌的危险因素。按绝经状态分层时,无论绝经状态如何,游离瘦素指数和可溶性瘦素受体均为危险因素,而LEPR基因K109R A/G多态性仅在绝经后组中为危险因素。

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