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首页> 外文期刊>BMC Evolutionary Biology >Molecular decay of enamel matrix protein genes in turtles and other edentulous amniotes
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Molecular decay of enamel matrix protein genes in turtles and other edentulous amniotes

机译:乌龟和其他无齿羊膜中釉基质蛋白基因的分子衰减

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Background Secondary edentulism (toothlessness) has evolved on multiple occasions in amniotes including several mammalian lineages (pangolins, anteaters, baleen whales), birds, and turtles. All edentulous amniote clades have evolved from ancestors with enamel-capped teeth. Previous studies have documented the molecular decay of tooth-specific genes in edentulous mammals, all of which lost their teeth in the Cenozoic, and birds, which lost their teeth in the Cretaceous. By contrast with mammals and birds, tooth loss in turtles occurred in the Jurassic (201.6-145.5 Ma), providing an extended time window for tooth gene degradation in this clade. The release of the painted turtle and Chinese softshell turtle genomes provides an opportunity to recover the decayed remains of tooth-specific genes in Testudines. Results We queried available genomes of Testudines (Chrysemys picta [painted turtle], Pelodiscus sinensis [Chinese softshell turtle]), Aves (Anas platyrhynchos [duck], Gallus gallus [chicken], Meleagris gallopavo [turkey], Melopsittacus undulatus [budgerigar], Taeniopygia guttata [zebra finch]), and enamelless mammals (Orycteropus afer [aardvark], Choloepus hoffmanni [Hoffmann’s two-toed sloth], Dasypus novemcinctus [nine-banded armadillo]) for remnants of three enamel matrix protein (EMP) genes with putative enamel-specific functions. Remnants of the AMBN and ENAM genes were recovered in Chrysemys and retain their original synteny. Remnants of AMEL were recovered in both testudines, although there are no shared frameshifts. We also show that there are inactivated copies of AMBN, AMEL and ENAM in representatives of divergent avian lineages including Galloanserae, Passeriformes, and Psittaciformes, and that there are shared frameshift mutations in all three genes that predate the basal split in Neognathae. Among enamelless mammals, all three EMP genes exhibit inactivating mutations in Orycteropus and Choloepus. Conclusions Our results highlight the power of combining fossil and genomic evidence to decipher macroevolutionary transitions and characterize the functional range of different loci involved in tooth development. The fossil record and phylogenetics combine to predict the occurrence of molecular fossils of tooth-specific genes in the genomes of edentulous amniotes, and in every case these molecular fossils have been discovered. The widespread occurrence of EMP pseudogenes in turtles, birds, and edentulous/enamelless mammals also provides compelling evidence that in amniotes, the only unique, non-redundant function of these genes is in enamel formation.
机译:背景技术继发性无牙病(无牙)在羊膜动物中多次进化,包括几种哺乳动物谱系(穿山甲,食蚁兽,鲸鱼),鸟类和乌龟。所有无牙的羊膜进化枝都是由牙釉质覆盖的祖先演变而来。先前的研究已证明,在无牙的哺乳动物中,牙齿特异性基因的分子衰减,所有这些牙齿都在新生代失去了牙齿,而鸟类的牙齿在白垩纪失去了牙齿。与哺乳动物和鸟类相比,侏罗纪(201.6-145.5 Ma)龟发生牙齿脱落,为该进化枝中的牙齿基因降解提供了延长的时间窗口。彩绘乌龟和中国软壳乌龟基因组的释放提供了一个机会,可以恢复睾丸中牙齿特异基因的残骸。结果我们查询了睾丸(Chrysemys picta [彩绘的乌龟],Pelodiscus sinensis [中华shell]),Aves(Anas platyrhynchos [鸭子],Gallus gallus [鸡],Meleagris gallopavo [火鸡],Melopsittacus undulatus [budgerigar])的可用基因组, Taeniopygia guttata [斑胸草雀])和无搪瓷的哺乳动物(Orycteropus afer [aardvark],Choloepus hoffmanni [Hoffmann的两趾树懒],Dasypus novemcinctus [九带犰狳]),带有三个搪瓷基质蛋白(EMP)基因的残留物搪瓷专用功能。 AMBN和ENAM基因的残基在Chrysemys中被回收,并保留了它们的原始同系物。尽管没有共享的移码,但两个测试中都回收了AMEL的残余物。我们还显示,在不同的鸟类谱系(包括Galloanserae,Passeriformes和Psittaciformes)的代表中,存在AMBN,AMEL和ENAM的失活拷贝,并且在新gna的基础分裂之前的所有三个基因中都有共享的移码突变。在无牙釉质的哺乳动物中,所有三个EMP基因在Orycteropus和Choloepus中均表现出失活突变。结论我们的研究结果突出了将化石和基因组证据相结合来解密宏观进化转变的能力,并表征了参与牙齿发育的不同基因座的功能范围。化石记录和系统发育学相结合,可预测无齿羊膜基因组中牙齿特异性基因的分子化石的发生,并且在每种情况下都发现了这些分子化石。 EMP假基因在海龟,鸟类和无牙/无牙釉质的哺乳动物中广泛存在,也提供了令人信服的证据,表明在羊膜动物中,这些基因的唯一独特的,非冗余的功能是牙釉质的形成。

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