Disruptive natural selection by male reproductive potential prevents underexpression of protein-coding genes on the human Y chromosome as a self-domestication syndrome.

IF 2.9 Q2 Biochemistry, Genetics and Molecular Biology BMC Genetics Pub Date : 2020-10-22 DOI:10.1186/s12863-020-00896-6
Mikhail Ponomarenko, Maxim Kleshchev, Petr Ponomarenko, Irina Chadaeva, Ekaterina Sharypova, Dmitry Rasskazov, Semyon Kolmykov, Irina Drachkova, Gennady Vasiliev, Natalia Gutorova, Elena Ignatieva, Ludmila Savinkova, Anton Bogomolov, Ludmila Osadchuk, Alexandr Osadchuk, Dmitry Oshchepkov
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引用次数: 8

Abstract

Background: In population ecology, the concept of reproductive potential denotes the most vital indicator of chances to produce and sustain a healthy descendant until his/her reproductive maturity under the best conditions. This concept links quality of life and longevity of an individual with disease susceptibilities encoded by his/her genome. Female reproductive potential has been investigated deeply, widely, and comprehensively in the past, but the male one has not received an equal amount of attention. Therefore, here we focused on the human Y chromosome and found candidate single-nucleotide polymorphism (SNP) markers of male reproductive potential.

Results: Examining in silico (i.e., using our earlier created Web-service SNP_TATA_Z-tester) all 1206 unannotated SNPs within 70 bp proximal promoters of all 63 Y-linked genes, we found 261 possible male-reproductive-potential SNP markers that can significantly alter the binding affinity of TATA-binding protein (TBP) for these promoters. Among them, there are candidate SNP markers of spermatogenesis disorders (e.g., rs1402972626), pediatric cancer (e.g., rs1483581212) as well as male anxiety damaging family relationships and mother's and children's health (e.g., rs187456378). First of all, we selectively verified in vitro both absolute and relative values of the analyzed TBP-promoter affinity, whose Pearson's coefficients of correlation between predicted and measured values were r = 0.84 (significance p <  0.025) and r = 0.98 (p <  0.025), respectively. Next, we found that there are twofold fewer candidate SNP markers decreasing TBP-promoter affinity relative to those increasing it, whereas in the genome-wide norm, SNP-induced damage to TBP-promoter complexes is fourfold more frequent than SNP-induced improvement (p <  0.05, binomial distribution). This means natural selection against underexpression of these genes. Meanwhile, the numbers of candidate SNP markers of an increase and decrease in male reproductive potential were indistinguishably equal to each other (p <  0.05) as if male self-domestication could have happened, with its experimentally known disruptive natural selection. Because there is still not enough scientific evidence that this could have happened, we discuss the human diseases associated with candidate SNP markers of male reproductive potential that may correspond to domestication-related disorders in pets.

Conclusions: Overall, our findings seem to support a self-domestication syndrome with disruptive natural selection by male reproductive potential preventing Y-linked underexpression of a protein.

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男性生殖潜能的破坏性自然选择阻止了人类Y染色体上蛋白质编码基因的低表达,这是一种自我驯化综合征。
背景:在种群生态学中,生殖潜力的概念是指在最佳条件下生育和维持健康后代直至生殖成熟的机会的最重要指标。这一概念将个人的生活质量和寿命与其基因组编码的疾病易感性联系起来。过去,人们对女性的生殖潜力进行了深入、广泛和全面的研究,但对男性的生殖潜力却没有得到同等的重视。因此,本文以人类Y染色体为研究对象,寻找男性生殖潜力的候选单核苷酸多态性(SNP)标记。结果:在计算机上检查(即使用我们之前创建的web服务SNP_TATA_Z-tester)所有63个y连锁基因的70 bp近端启动子内的所有1206个未注释的SNP,我们发现261个可能的男性生殖潜在SNP标记可以显著改变tata结合蛋白(TBP)对这些启动子的结合亲和力。其中,有精子发生障碍(如rs1402972626)、儿童癌症(如rs1483581212)以及男性焦虑损害家庭关系和母婴健康(如rs187456378)的候选SNP标记。首先,我们选择性地在体外验证了所分析的tbp启动子亲和力的绝对值和相对值,其预测值和实施值之间的Pearson相关系数为r = 0.84(显著性p)。结论:总体而言,我们的研究结果似乎支持一种自我驯化综合征,即男性生殖潜能通过破坏性自然选择阻止y相关蛋白的低表达。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
BMC Genetics
BMC Genetics 生物-遗传学
CiteScore
4.30
自引率
0.00%
发文量
77
审稿时长
4-8 weeks
期刊介绍: BMC Genetics is an open access, peer-reviewed journal that considers articles on all aspects of inheritance and variation in individuals and among populations.
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