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芳香化酶抑制剂相关的骨折:一项病例队列全基因组关联研究和功能基因组学

Aromatase inhibitor-associated bone fractures: a case-cohort GWAS and functional genomics.

作者信息

Liu Mohan, Goss Paul E, Ingle James N, Kubo Michiaki, Furukawa Yoichi, Batzler Anthony, Jenkins Gregory D, Carlson Erin E, Nakamura Yusuke, Schaid Daniel J, Chapman Judy-Anne W, Shepherd Lois E, Ellis Matthew J, Khosla Sundeep, Wang Liewei, Weinshilboum Richard M

机构信息

Division of Clinical Pharmacology (M.L., L.W., R.M.W.), Department of Molecular Pharmacology and Experimental Therapeutics; Departments of Oncology (J.N.I.) and Health Sciences Research (A.B., G.D.J., E.E.C., D.J.S.); and Division of Endocrinology (S.K.), Mayo Clinic, Rochester, Minnesota 55905; Massachusetts General Hospital (P.E.G.), Harvard University, Boston, Massachusetts 02114; Rikagaku Kenkyūsho Center for Integrative Medical Science (M.K., Y.F.), Yokohama, Japan 230-0045; School of Medicine (Y.N.), Chicago University, Chicago, Illinois 60637; National Cancer Institute of Canada Clinical Trials Group (J.-A.W.C., L.E.S.), Kingston, Ontario, Canada K7L 3N6; and Division of Oncology (M.J.E.), Department of Medicine, Washington University School of Medicine, St Louis, Missouri 63110.

出版信息

Mol Endocrinol. 2014 Oct;28(10):1740-51. doi: 10.1210/me.2014-1147. Epub 2014 Aug 22.

Abstract

Bone fractures are a major consequence of osteoporosis. There is a direct relationship between serum estrogen concentrations and osteoporosis risk. Aromatase inhibitors (AIs) greatly decrease serum estrogen levels in postmenopausal women, and increased incidence of fractures is a side effect of AI therapy. We performed a discovery case-cohort genome-wide association study (GWAS) using samples from 1071 patients, 231 cases and 840 controls, enrolled in the MA.27 breast cancer AI trial to identify genetic factors involved in AI-related fractures, followed by functional genomic validation. Association analyses identified 20 GWAS single nucleotide polymorphism (SNP) signals with P < 5E-06. After removal of signals in gene deserts and those composed entirely of imputed SNPs, we applied a functional validation "decision cascade" that resulted in validation of the CTSZ-SLMO2-ATP5E, TRAM2-TMEM14A, and MAP4K4 genes. These genes all displayed estradiol (E2)-dependent induction in human fetal osteoblasts transfected with estrogen receptor-α, and their knockdown altered the expression of known osteoporosis-related genes. These same genes also displayed SNP-dependent variation in E2 induction that paralleled the SNP-dependent induction of known osteoporosis genes, such as osteoprotegerin. In summary, our case-cohort GWAS identified SNPs in or near CTSZ-SLMO2-ATP5E, TRAM2-TMEM14A, and MAP4K4 that were associated with risk for bone fracture in estrogen receptor-positive breast cancer patients treated with AIs. These genes displayed E2-dependent induction, their knockdown altered the expression of genes related to osteoporosis, and they displayed SNP genotype-dependent variation in E2 induction. These observations may lead to the identification of novel mechanisms associated with fracture risk in postmenopausal women treated with AIs.

摘要

骨折是骨质疏松症的主要后果。血清雌激素浓度与骨质疏松症风险之间存在直接关系。芳香化酶抑制剂(AIs)可大幅降低绝经后女性的血清雌激素水平,而骨折发生率增加是AI治疗的一种副作用。我们利用参与MA.27乳腺癌AI试验的1071例患者(231例病例和840例对照)的样本进行了一项探索性病例队列全基因组关联研究(GWAS),以确定与AI相关骨折有关的遗传因素,随后进行功能基因组验证。关联分析确定了20个全基因组关联研究单核苷酸多态性(SNP)信号,其P值<5×10⁻⁶。在去除基因沙漠中的信号以及完全由推算SNP组成的信号后,我们应用了一个功能验证“决策级联”,结果验证了CTSZ-SLMO2-ATP5E、TRAM2-TMEM14A和MAP4K4基因。这些基因在用雌激素受体-α转染的人胎儿成骨细胞中均表现出雌二醇(E2)依赖性诱导,并且它们的敲低改变了已知骨质疏松症相关基因的表达。这些相同的基因在E2诱导中也表现出SNP依赖性变异,这与已知骨质疏松症基因(如骨保护素)的SNP依赖性诱导相似。总之,我们的病例队列GWAS在CTSZ-SLMO2-ATP5E、TRAM2-TMEM14A和MAP4K4基因内部或附近鉴定出与接受AI治疗的雌激素受体阳性乳腺癌患者骨折风险相关的SNP。这些基因表现出E2依赖性诱导,它们的敲低改变了与骨质疏松症相关基因的表达,并且它们在E2诱导中表现出SNP基因型依赖性变异。这些观察结果可能会导致识别出与接受AI治疗的绝经后女性骨折风险相关的新机制。

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