线粒体遗传变异与乳腺癌风险的关联:多民族队列研究。
Association between mitochondrial genetic variation and breast cancer risk: The Multiethnic Cohort.
机构信息
Department of Epidemiology and Biostatistics, School of Medicine, University of California, San Francisco, California, United States of America.
Theoretical Biology and Biophysics, Los Alamos National Laboratory, Los Alamos, New Mexico.
出版信息
PLoS One. 2019 Oct 2;14(10):e0222284. doi: 10.1371/journal.pone.0222284. eCollection 2019.
BACKGROUND
The mitochondrial genome encodes for thirty-seven proteins, among them thirteen are essential for the oxidative phosphorylation (OXPHOS) system. Inherited variation in mitochondrial genes may influence cancer development through changes in mitochondrial proteins, altering the OXPHOS process and promoting the production of reactive oxidative species.
METHODS
To investigate the association between mitochondrial genetic variation and breast cancer risk, we tested 314 mitochondrial SNPs (mtSNPs), capturing four complexes of the mitochondrial OXPHOS pathway and mtSNP groupings for rRNA and tRNA, in 2,723 breast cancer cases and 3,260 controls from the Multiethnic Cohort Study.
RESULTS
We examined the collective set of 314 mtSNPs as well as subsets of mtSNPs grouped by mitochondrial OXPHOS pathway, complexes, and genes, using the sequence kernel association test and adjusting for age, sex, and principal components of global ancestry. We also tested haplogroup associations using unconditional logistic regression and adjusting for the same covariates. Stratified analyses were conducted by self-reported maternal race/ethnicity. No significant mitochondrial OXPHOS pathway, gene, and haplogroup associations were observed in African Americans, Asian Americans, Latinos, and Native Hawaiians. In European Americans, a global test of all genetic variants of the mitochondrial genome identified an association with breast cancer risk (P = 0.017, q = 0.102). In mtSNP-subset analysis, the gene MT-CO2 (P = 0.001, q = 0.09) in Complex IV (cytochrome c oxidase) and MT-ND2 (P = 0.004, q = 0.19) in Complex I (NADH dehydrogenase (ubiquinone)) were significantly associated with breast cancer risk.
CONCLUSIONS
In summary, our findings suggest that collective mitochondrial genetic variation and particularly in the MT-CO2 and MT-ND2 may play a role in breast cancer risk among European Americans. Further replication is warranted in larger populations and future studies should evaluate the contribution of mitochondrial proteins encoded by both the nuclear and mitochondrial genomes to breast cancer risk.
背景
线粒体基因组编码 37 种蛋白质,其中 13 种对于氧化磷酸化(OXPHOS)系统至关重要。线粒体基因的遗传变异可能会通过改变线粒体蛋白影响癌症的发展,改变 OXPHOS 过程并促进活性氧化物质的产生。
方法
为了研究线粒体遗传变异与乳腺癌风险之间的关联,我们在多民族队列研究中对 2723 例乳腺癌病例和 3260 例对照进行了 314 个线粒体单核苷酸多态性(mtSNP)的测试,这些 mtSNP 捕获了线粒体 OXPHOS 途径的四个复合物以及 mtSNP 分组的 rRNA 和 tRNA。
结果
我们使用序列核关联检验并调整年龄、性别和全球祖先的主要成分,对 314 个 mtSNP 的整体集合以及按线粒体 OXPHOS 途径、复合物和基因分组的 mtSNP 子集进行了检测。我们还使用无条件逻辑回归并调整相同的协变量来检测单倍群关联。按自我报告的母亲种族/族裔进行分层分析。在非裔美国人、亚裔美国人、拉丁裔和夏威夷原住民中,没有观察到线粒体 OXPHOS 途径、基因和单倍群的显著关联。在欧洲裔美国人中,对线粒体基因组的所有遗传变异的全局测试与乳腺癌风险相关(P = 0.017,q = 0.102)。在 mtSNP 子集分析中,复合物 IV(细胞色素 c 氧化酶)中的 MT-CO2 基因(P = 0.001,q = 0.09)和复合物 I(NADH 脱氢酶(泛醌))中的 MT-ND2 基因(P = 0.004,q = 0.19)与乳腺癌风险显著相关。
结论
总之,我们的研究结果表明,线粒体遗传变异的总体情况,特别是 MT-CO2 和 MT-ND2 可能在欧洲裔美国人的乳腺癌风险中发挥作用。需要在更大的人群中进行进一步的复制,未来的研究应评估核基因组和线粒体基因组编码的线粒体蛋白对乳腺癌风险的贡献。
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