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对水蚤中可诱导家族成员的分析,促成了一种未被鉴定的热休克蛋白70谱系的发现。

The analysis of inducible family members in the water flea led to the identification of an uncharacterized lineage of heat shock protein 70.

作者信息

Wu Xiangyang, Zhang Zhiwei, Cui Wenfeng, Han Linfei, Liu Zijie, Song Xiaojun, Tan Jiabo

机构信息

Laboratory of Comparative Immunology, School of Marine Science and Engineering, Qingdao Agricultural University, Qingdao, 266109, China.

出版信息

Heliyon. 2024 May 3;10(9):e30288. doi: 10.1016/j.heliyon.2024.e30288. eCollection 2024 May 15.

Abstract

To explore the function and evolutionary relationships of inducible heat shock protein 70 (Hsp70) in , cDNAs of four Hsp70 family members (, , , ) were cloned. While all DmaHsp70s possess three function domains, it is noteworthy that only DmaHsp70 ends with a "EEVD" motif. Phylogenetic analysis indicates that the Hsp70-12 lineage is distanced from the rest, and therefore it is an uncharacterized lineage of Hsp70. The differences in isoelectric point and 3-dimensional (3D) conformation of the N-terminal nucleotide binding domain (NBD) of DmaHsp70s further support the theory. DmaHsp70s exhibit varied motif distribution patterns and the logo sequences of motifs have diverse signature characteristics, indicating that different mechanisms are involved in the regulation of ATP binding and hydrolysis for the DmaHsp70s. Protein-protein network together with the predicted subcellular locations of DmaHsp70s suggest that they likely fulfill distinct roles in cells. The transcription of four DmaHsp70s were changed during the recovery stage after thermal stress or oxidative stress. But the expression pattern of them were dissimilar. Collectively, these results collectively elucidated the identification of a previously uncharacterizedHsp70 lineage in animal and extended our understanding of the Hsp70 family.

摘要

为了探究诱导型热休克蛋白70(Hsp70)在[具体物种或情境未提及]中的功能及进化关系,克隆了四个Hsp70家族成员([具体成员未明确列出])的cDNA。虽然所有的DmaHsp70都具有三个功能结构域,但值得注意的是,只有DmaHsp70以“EEVD”基序结尾。系统发育分析表明,Hsp70 - 12谱系与其他谱系有距离,因此它是Hsp70的一个未被表征的谱系。DmaHsp70的N端核苷酸结合结构域(NBD)的等电点和三维(3D)构象的差异进一步支持了这一理论。DmaHsp70表现出不同的基序分布模式,且基序的序列标志具有不同的特征,表明DmaHsp70在ATP结合和水解的调节中涉及不同的机制。蛋白质 - 蛋白质网络以及DmaHsp70预测的亚细胞定位表明它们可能在细胞中发挥不同的作用。在热应激或氧化应激后的恢复阶段,四个DmaHsp70的转录发生了变化。但它们的表达模式不同。总体而言,这些结果共同阐明了在动物中鉴定出一个以前未被表征的Hsp70谱系,并扩展了我们对Hsp70家族的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/79d8/11098801/c634f9a673e3/gr1.jpg

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