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关于蛋白质功能相关旁系同源物和直系同源物聚类的说明:以FK506结合蛋白(FKBPs)为例。

A note on clustering the functionally-related paralogues and orthologues of proteins: a case of the FK506-binding proteins (FKBPs).

作者信息

Galat Andrzej

机构信息

Département d'Ingénierie et d'Etudes des Protéines, Bat. 152, DSV/CEA, CE-Saclay, F-91191 Gif-sur-Yvette Cedex, France.

出版信息

Comput Biol Chem. 2004 Apr;28(2):129-40. doi: 10.1016/j.compbiolchem.2004.01.004.

Abstract

The expression patterns of 18 FK506-binding proteins (FKBPs) encoded in the human genome have been established whereas the functional significance of the numerous ORFs coding for FKBP-like sequences remains unknown. Nominal masses of the human FKBPs vary from 12 to 135 kDa. Some large FKBPs consist up to four repeats of the 12 kDa FK506-like binding domain (FKBD) whereas other large FKBPs contain one FKBD linked to different functional domains such as TPRs, leucine-zipper, calmodulin-binding domain etc. The genomes of other eukaryotic organisms, namely D. melanogaster, C. elegans, A. thaliana, S. pombe and S. cerevisiae encode different numbers of the FKBPs' paralogues some of which are orthologues to the human FKBPs. A library of novel algorithms was developed and used for computation of the level of conservation of the hydrophobicity and bulkiness profiles, and the amino acid compositions (AACs) of 247 aligned sequences of FKBPs. The pairwisely-compared hydrophobicity and bulkiness profiles for some combinations of the aligned sequences of the FKBDs yielded high values of the correlation coefficients (CCF). The AACs of some combinations of the aligned sequences of the FKBDs also differed to a low degree. The functionally-related orthologues and paralogues of the FKBPs were clustered by using the following criteria: 1 degrees apparent conservation of the crucial amino acid (AA) residues for peptidylprolyl cis/trans isomerase (PPIase) acitity and binding of some immunosuppressive drugs; 2 degrees convergence of the three mentioned above properties of the polypeptide chain; 3 degrees similarity in the sequence attributes pI and total hydrophobicity index (HI). The clustering method was used for setting up several hypotheses on the emergence of certain classes of the FKBPs in the eukaryotic kingdom.

摘要

人类基因组中编码的18种FK506结合蛋白(FKBPs)的表达模式已经确定,而众多编码FKBP样序列的开放阅读框的功能意义仍然未知。人类FKBPs的标称质量从12 kDa到135 kDa不等。一些大型FKBPs由多达四个12 kDa FK506样结合域(FKBD)重复组成,而其他大型FKBPs包含一个与不同功能域相连的FKBD,如TPRs、亮氨酸拉链、钙调蛋白结合域等。其他真核生物的基因组,即黑腹果蝇、秀丽隐杆线虫、拟南芥、粟酒裂殖酵母和酿酒酵母,编码不同数量的FKBPs旁系同源物,其中一些是人类FKBPs的直系同源物。开发了一个新算法库,并用于计算247个FKBPs比对序列的疏水性和体积轮廓以及氨基酸组成(AACs)的保守水平。FKBD比对序列的某些组合的成对比较疏水性和体积轮廓产生了高相关系数(CCF)值。FKBD比对序列的某些组合的AACs也有低度差异。通过使用以下标准对FKBPs的功能相关直系同源物和旁系同源物进行聚类:1. 肽基脯氨酰顺/反异构酶(PPIase)活性和某些免疫抑制药物结合的关键氨基酸(AA)残基的明显保守程度;2. 上述多肽链三种性质的趋同程度;3. 序列属性pI和总疏水指数(HI)的相似程度。聚类方法用于建立关于真核生物界中某些类FKBPs出现的几个假设。

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