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Loss and Gain of Function in SERPINB11: An Example of a Gene under Selection on Standing Variation with Implications for Host-Pathogen Interactions

机译:损失和功能的增益在sERpINB11:立地变化选择下的基因的一个例子与启示宿主 - 病原体相互作用

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摘要

Serine protease inhibitors (SERPINs) are crucial in the regulation of diverse biological processes including inflammation and immune response. SERPINB11, located in the 18q21 gene cluster, is a polymorphic gene/pseudogene coding for a non-inhibitory SERPIN. In a genome-wide scan for recent selection, SERPINB11 was identified as a potential candidate gene for adaptive evolution in Yoruba. The present study sought a better understanding of the evolutionary history of SERPINB11, with special focus on evaluating its selective signature. Through the resequencing of coding and noncoding regions of SERPINB11 in 20 Yorubans and analyzing primate orthologous sequences, we identified a full-length SERPINB11 variant encoding a non-inhibitory SERPIN as the putative candidate of selection – probably driven to higher frequencies by an adaptive response using preexisting variation. In addition, we detected contrasting evolutionary features of SERPINB11 in primates: While primate phylogeny as a whole is under purifying selection, the human lineage shows evidence of positive selection in a few codons, all associated with the active SERPINB11. Comparative modeling studies suggest that positively selected codons reduce SERPINB11's ability to undergo the conformational changes typical of inhibitory SERPINs – suggesting that it is evolving towards a new non-inhibitory function in humans. Significant correlations between SERPINB11 variants and the environmental variables, pastoralism and pathogen richness, have led us to propose a selective advantage through host-pathogen interactions, possibly linked to an adaptive response combating the emergence of infectious diseases in recent human evolution. This work represents the first description of a resurrected gene in humans, and may well exemplify selection on standing variation triggered by drastic ecological shifts.
机译:丝氨酸蛋白酶抑制剂(Serpins)在调节各种生物过程的规范中至关重要,包括炎症和免疫应答。 SerpinB11位于18Q21基因群中,是一种用于非抑制蛇素的多态基因/假蛋白编码。在最近选择的基因组扫描中,SerpInB11被鉴定为尤鲁巴适应性进化的潜在候选基因。本研究寻求更好地了解SerpinB11的进化历史,特别关注评估其选择性签名。通过在20氧鲁纳的塞浦保人的编码和非编码区重构并分析灵长类动物的序列,我们鉴定了一种用于编码非抑制蛇素的全长SerpinB11变体,作为选择的推定候选者 - 可能通过自适应响应驱动到更高的频率预先存在的变化。此外,我们在灵长类动物中检测到SerpinB11的对比进化特征:同时作为整体的灵长类动物,人类谱系显示在几个密码子中的阳性选择的证据,均与活性SerpinB11相关。比较建模研究表明,正面选择的密码子降低了SerpinB11经历典型血清典型变化的能力 - 这表明它正在发展在人类中的新的非抑制功能。 SerpinB11变体与环境变量,牧区和病原体丰富的显着相关性导致我们通过宿主 - 病原体相互作用提出选择性优势,可能与适应性反应进行适应性反应,打击近期人类演化中的传染病的出现。该作品代表了人类复活基因的第一个描述,并且可以透明地举例说明通过激烈生态转移触发的常设变化的选择。

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