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一种不同于m型和μ型的新型哺乳动物钙依赖性蛋白酶的分子克隆。该mRNA在骨骼肌中的特异性表达。

Molecular cloning of a novel mammalian calcium-dependent protease distinct from both m- and mu-types. Specific expression of the mRNA in skeletal muscle.

作者信息

Sorimachi H, Imajoh-Ohmi S, Emori Y, Kawasaki H, Ohno S, Minami Y, Suzuki K

机构信息

Department of Molecular Biology, Tokyo Metropolitan Institute of Medical Science, Japan.

出版信息

J Biol Chem. 1989 Nov 25;264(33):20106-11.

PMID:2555341
Abstract

Two types of calcium-dependent protease with distinct calcium requirements (termed muCANP and mCANP) are known in mammalian tissues. These two isozymes consist of different large (80-kDa) subunits (mu- or m-types) and identical small (30-kDa) subunits. By screening human and rat muscle cDNA libraries with a cDNA probe for the chicken CANP large subunit, which has a structure similar to both the mammalian mu- and m-types, a cDNA clone encoding a novel member of the CANP large subunit family was obtained. The encoded protein (designated "p94") consists of 821 amino acid residues (Mr 94,084) and shows significant sequence homology with both human mu-type (54%) and m-type (51%) large subunits. p94 can be divided into four domains (I-IV) as reported for the CANP large subunit family. Domains II and IV are potential cysteine protease and calcium-binding domains, respectively, and have sequences homologous to the corresponding domains of other CANP large subunits. However, domain I of p94 is significantly different from others. Moreover, p94 contains two unique sequences of 62 and 77 residues in domains II and III, respectively. In contrast to the ubiquitous expression of mu- and m-types, Northern blot analysis revealed that the mRNA for p94 exists only in skeletal muscle with none detected in other tissues including heart muscle and smooth muscles such as intestine.

摘要

在哺乳动物组织中已知有两种对钙需求不同的钙依赖性蛋白酶(分别称为μ钙蛋白酶和m钙蛋白酶)。这两种同工酶由不同的大亚基(80 kDa)(μ型或m型)和相同的小亚基(30 kDa)组成。用鸡钙蛋白酶大亚基的cDNA探针筛选人和大鼠肌肉cDNA文库,该探针的结构与哺乳动物的μ型和m型均相似,从而获得了一个编码钙蛋白酶大亚基家族新成员的cDNA克隆。编码的蛋白质(命名为“p94”)由821个氨基酸残基组成(Mr 94,084),与人μ型大亚基(54%)和m型大亚基(51%)均有显著的序列同源性。p94可如钙蛋白酶大亚基家族报道的那样分为四个结构域(I-IV)。结构域II和IV分别是潜在的半胱氨酸蛋白酶结构域和钙结合结构域,与其他钙蛋白酶大亚基的相应结构域有同源序列。然而,p94的结构域I与其他结构域明显不同。此外,p94在结构域II和III中分别包含两个独特的62个和77个残基的序列。与μ型和m型的广泛表达不同,Northern印迹分析显示p94的mRNA仅存在于骨骼肌中,在包括心肌和肠道平滑肌等其他组织中未检测到。

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