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[哺乳动物磷酸核糖焦磷酸合成酶]

[Mammalian phosphoribosylpyrophosphate synthetase].

作者信息

Tatibana M

机构信息

Department of Biochemistry, Chiba University School of Medicine.

出版信息

Nihon Rinsho. 1996 Dec;54(12):3195-201.

PMID:8976091
Abstract

PRPP synthetase from rat liver exists as large molecular weight aggregates composed of at least four different components, i.e., two isoforms of 34 kDa catalytic subunits, PRSI and PRSII, and two associated proteins of 39 kDa and 41 kDa (PAP39 and PAP41). The four proteins have remarkably similar amino acid sequences and form a relatively large group of PRS family. PAPs, however, have extra regions of 40 to 50 amino acid residues, totally dissimilar to sequences of the catalytic subunits and thus form a subfamily. PAPs suppress the catalytic activity of PRS. They are very likely to be enzymatically inactive. The relative amounts of the mRNAs of the four components vary with the tissues, hence composition and properties of PRPP synthetase would also differ. Future studies on the physiology and pathology of PAPs are critical in elucidation of pathogenesis of some types of hyperuricemia.

摘要

大鼠肝脏中的磷酸核糖焦磷酸合成酶(PRPP合成酶)以大分子量聚集体的形式存在,该聚集体由至少四种不同成分组成,即34 kDa催化亚基的两种同工型PRSI和PRSII,以及两种分别为39 kDa和41 kDa的相关蛋白(PAP39和PAP41)。这四种蛋白质具有非常相似的氨基酸序列,形成了一个相对较大的PRS家族。然而,PAP具有40至50个氨基酸残基的额外区域,与催化亚基的序列完全不同,因此形成一个亚家族。PAP会抑制PRS的催化活性。它们很可能没有酶活性。这四种成分的mRNA相对含量随组织而异,因此PRPP合成酶的组成和性质也会有所不同。未来对PAP的生理学和病理学研究对于阐明某些类型高尿酸血症的发病机制至关重要。

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