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脊椎动物中Timezyme多样化的时间安排。

The timing of Timezyme diversification in vertebrates.

作者信息

Cazaméa-Catalan Damien, Besseau Laurence, Falcón Jack, Magnanou Elodie

机构信息

Sorbonne Universités, UPMC Univ Paris 06, UMR 7232, BIOM Biologie Intégrative des Organismes Marins, Observatoire Océanologique, Banyuls/Mer, France; CNRS, UMR 7232, BIOM Biologie Intégrative des Organismes Marins, Observatoire Océanologique, Banyuls/Mer, France.

出版信息

PLoS One. 2014 Dec 8;9(12):e112380. doi: 10.1371/journal.pone.0112380. eCollection 2014.

Abstract

All biological functions in vertebrates are synchronized with daily and seasonal changes in the environment by the time keeping hormone melatonin. Its nocturnal surge is primarily due to the rhythmic activity of the arylalkylamine N-acetyl transferase AANAT, which thus became the focus of many investigations regarding its evolution and function. Various vertebrate isoforms have been reported from cartilaginous fish to mammals but their origin has not been clearly established. Using phylogeny and synteny, we took advantage of the increasing number of available genomes in order to test whether the various rounds of vertebrate whole genome duplications were responsible for the diversification of AANAT. We highlight a gene secondary loss of the AANAT2 in the Sarcopterygii, revealing for the first time that the AAANAT1/2 duplication occurred before the divergence between Actinopterygii (bony fish) and Sarcopterygii (tetrapods, lobe-finned fish, and lungfish). We hypothesize the teleost-specific whole genome duplication (WDG) generated the appearance of the AANAT1a/1b and the AANAT2/2'paralogs, the 2' isoform being rapidly lost in the teleost common ancestor (ray-finned fish). We also demonstrate the secondary loss of the AANAT1a in a Paracantopterygii (Atlantic cod) and of the 1b in some Ostariophysi (zebrafish and cave fish). Salmonids present an even more diverse set of AANATs that may be due to their specific WGD followed by secondary losses. We propose that vertebrate AANAT diversity resulted from 3 rounds of WGD followed by previously uncharacterized secondary losses. Extant isoforms show subfunctionalized localizations, enzyme activities and affinities that have increased with time since their emergence.

摘要

在脊椎动物中,所有生物功能都通过计时激素褪黑素与环境中的每日和季节性变化保持同步。其夜间分泌高峰主要归因于芳基烷基胺N - 乙酰转移酶(AANAT)的节律性活动,因此AANAT成为了许多关于其进化和功能研究的焦点。从软骨鱼到哺乳动物,已经报道了各种脊椎动物的同工型,但它们的起源尚未明确确定。利用系统发育和共线性,我们利用越来越多的可用基因组来测试脊椎动物全基因组复制的各个轮次是否导致了AANAT的多样化。我们强调了肉鳍鱼中AANAT2的基因二次丢失,首次揭示了AAANAT1/2复制发生在辐鳍鱼(硬骨鱼)和肉鳍鱼(四足动物、叶鳍鱼和肺鱼)分化之前。我们假设硬骨鱼特异性全基因组复制(WDG)产生了AANAT1a/1b和AANAT2/2'旁系同源物的出现,2'同工型在硬骨鱼共同祖先(辐鳍鱼)中迅速丢失。我们还证明了在副鲈形目(大西洋鳕鱼)中AANAT1a的二次丢失以及在一些骨鳔总目(斑马鱼和洞穴鱼)中1b的二次丢失。鲑科鱼类呈现出一组更加多样化的AANATs,这可能是由于它们特定的全基因组复制随后发生了二次丢失。我们提出脊椎动物AANAT的多样性源于三轮全基因组复制,随后是此前未被表征的二次丢失。现存的同工型显示出亚功能化的定位、酶活性和亲和力,自它们出现以来随着时间的推移而增加。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/627b/4259306/6a1735e67126/pone.0112380.g001.jpg

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