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首页> 外文期刊>Molecular Biology and Evolution >Identification of Novel Mammalian Caspases Reveals an Important Role of Gene Loss in Shaping the Human Caspase Repertoire
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Identification of Novel Mammalian Caspases Reveals an Important Role of Gene Loss in Shaping the Human Caspase Repertoire

机译:新型哺乳动物胱天蛋白酶的鉴定揭示了基因损失在塑造人类半胱天冬酶库中的重要作用

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Proteases of the caspase family play central roles in apoptosis and inflammation. Recently, we have described a new gene encoding caspase-15 that has been inactivated independently in different mammalian lineages. To determine the dynamics of gene duplication and loss in the entire caspase gene family, we performed a comprehensive evolutionary analysis of mammalian caspases. By comparative genomics and reverse transcriptase–polymerase chain reaction analyses, we identified 3 novel mammalian caspase genes, which we tentatively named caspases-16 through -18. Caspase-16, which is most similar in sequence to caspase-14, has been conserved in marsupials and placental mammals, including humans. Caspase-17, which is most similar to caspase-3, has been conserved among fish, frog, chicken, lizard, and the platypus but is absent from marsupials and placental mammals. Caspase-18, which is most similar to caspase-8, has been conserved among chicken, platypus, and opossum but is absent from placental mammals. These gene distribution patterns suggest that, in the evolutionary lineage leading to humans, caspase-17 was lost after the split of protherian and therian mammals and caspase-18 was lost after the split of marsupials and placental mammals. In the canine genome, the number of caspases has been reduced by the fusion of the neighboring genes caspases-1 and -4, resulting in a single coding region. Further lineage-specific gene inactivations were found for caspase-10 in murine rodents and caspase-12 in humans, rabbit, and cow. Lineage-specific gene duplications were found for caspases-1, -3, and -12 in opossum and caspase-4 in primates. Other caspases were generally conserved in all mammalian species investigated. Using the positions of introns as stable characters during recent vertebrate evolution, we define 3 phylogenetic clades of caspase genes: caspases-1/-2/-4/-5/-9/-12/-14/-15/-16 (clade I), caspases-3/-6/-7/-17 (clade II), and caspases-8/-10/-18/CFLAR (clade III). We conclude that gene inactivations have occurred in each of the 3 caspase clades and that gene loss has been as critical as gene duplication in the evolution of the human repertoire of caspases.
机译:半胱天冬酶家族的蛋白酶在细胞凋亡和炎症中起重要作用。最近,我们描述了编码caspase-15的新基因,该基因已在不同的哺乳动物谱系中独立失活。为了确定整个半胱天冬酶基因家族中基因重复和丢失的动力学,我们对哺乳动物的半胱天冬酶进行了全面的进化分析。通过比较基因组学和逆转录酶-聚合酶链反应分析,我们鉴定了3个新颖的哺乳动物半胱天冬酶基因,我们暂定将其命名为caspases-16至-18。 Caspase-16与caspase-14的序列最相似,已在有袋动物和胎盘哺乳动物(包括人类)中保存下来。 Caspase-17与caspase-3最相似,已在鱼类,青蛙,鸡,蜥蜴和鸭嘴兽中保存下来,但有袋动物和胎盘哺乳动物中却没有。 Caspase-18与caspase-8最相似,已在鸡,鸭嘴兽和负鼠中被保存,但胎盘哺乳动物中却不存在。这些基因分布模式表明,在导致人类的进化谱系中,protherian和therian哺乳动物分裂后,caspase-17丢失,有袋动物和胎盘哺乳动物分裂后,caspase-18丢失。在犬基因组中,通过邻近基因caspases-1和-4的融合减少了caspases的数量,从而形成了一个编码区。在鼠类啮齿动物中发现了caspase-10的进一步谱系特异性基因失活,在人,兔和牛中发现了caspase-12。在灵长类动物的负鼠中发现caspases-1,-3和-12的谱系特异性基因重复,在灵长类动物中发现caspase-4。在所有研究的哺乳动物物种中,其他半胱天冬酶都通常是保守的。使用内含子的位置作为最近脊椎动物进化过程中的稳定特征,我们定义了3个半胱天冬酶基因的进化进化枝:caspases-1 / -2 / -4 / -5 / -9 / -12 / -14 / -15 / -16(进化枝I),caspases-3 / -6 / -7 / -17(进化枝II)和caspases-8 / -10 / -18 / CFLAR(进化枝III)。我们得出的结论是,在3个半胱天冬酶进化枝中均发生了基因失活,并且基因丢失在人类胱天蛋白酶谱系的进化中与基因复制一样重要。

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