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首页> 外文期刊>Chemistry & biodiversity >Characterization of metal-responsive transcription factor (MTF-1) from the giant rodent capybara reveals features in common with human as well as with small rodents (mouse, rat). Short communication.
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Characterization of metal-responsive transcription factor (MTF-1) from the giant rodent capybara reveals features in common with human as well as with small rodents (mouse, rat). Short communication.

机译:巨大的啮齿动物水豚的金属响应转录因子(MTF-1)的特征揭示了人类和小型啮齿动物(小鼠,大鼠)的共同特征。简短的沟通。

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摘要

From mammals to insects, metal-responsive transcription factor 1 (MTF-1) is essential for the activation of metallothionein genes upon heavy-metal load. We have previously found that human MTF-1 induces a stronger metal response than mouse MTF-1. The latter differs from the human one in a number of amino acid positions and is also shorter by 78 aa at its C-terminus. We reasoned that the weaker metal inducibility might be associated with a lesser demand for tight metal homeostasis in a low-weight, short-lived animal, and thus set out to determine the sequence of MTF-1 from the largest living rodent, the Brazilian capybara that call reach 65 kg and also has a considerably longer life span than smaller rodents. An expression clone for capybara MTF-1 was then tested for its activity in both mouse and human cells. Our analysis revealed three unexpected features: i) capybara MTF-1 in terms of amino acid sequence is much more closely related to human than to mouse MTF-1, suggesting ail accelerated evolution of MTF-1 in the evolutionary branch leading to small rodents: ii) capybara MTF-1 is even 32 aa shorter at its C-terminus than Mouse MTF-1, and iii) in in activity test, it is not more active than mouse MTF-1. The latter two findings might indicate that capybara has evolved in in environment with low heavy-metal load.
机译:从哺乳动物到昆虫,金属响应转录因子1(MTF-1)对于重金属负载下金属硫蛋白基因的激活至关重要。先前我们已经发现,人MTF-1比小鼠MTF-1诱导更强的金属反应。后者在氨基酸位置上与人不同,在其C端也短了78aa。我们认为,金属诱导性较弱可能与重量轻,寿命短的动物对紧密金属稳态的需求减少有关,因此,我们着手确定最大活体啮齿动物巴西水豚的MTF-1序列。该称重达到65公斤,并且比小型啮齿动物具有更长的寿命。然后测试水豚MTF-1的表达克隆在小鼠和人类细胞中的活性。我们的分析揭示了三个出乎意料的特征:i)水豚MTF-1在氨基酸序列方面与人的关系比与小鼠MTF-1的关系密切得多,这表明MTF-1在进化分支中的全部加速进化导致了小啮齿动物: ii)水豚MTF-1在其C端比小鼠MTF-1短32aa,并且iii)在活性测试中,它的活性不比小鼠MTF-1高。后两个发现可能表明水豚在低重金属负载的环境中进化。

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