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环状片层聚合:肝脏中Zα1-抗胰蛋白酶积累的结构基础。

Loop-sheet polymerization: the structural basis of Z alpha 1-antitrypsin accumulation in the liver.

作者信息

Lomas D A

机构信息

Department of Haematology, University of Cambridge, MRC Centre, U.K.

出版信息

Clin Sci (Lond). 1994 May;86(5):489-95. doi: 10.1042/cs0860489.

Abstract
  1. The Z deficiency variant of alpha 1-antitrypsin predisposes the homozygote to early-onset panlobular emphysema and results in the accumulation of antitrypsin within the hepatocyte, which leads to hepatocellular damage and cirrhosis. The mechanism of this accumulation has been shown to be due to the Z mutation (Glu-342-->Lys) perturbing the structure of the protein, allowing a unique interaction between the reactive-centre loop of one molecule and the A sheet of a second. This loop-sheet polymerization occurs spontaneously at 37 degrees C in purified plasma Z but not M antitrypsin. The rate of polymerization is greatly accelerated at 41 degrees C and is blocked by the insertion of a specific peptide into the A sheet of the antitrypsin molecule. Electron microscopy and circular dichroic spectral analysis confirm that the Z antitrypsin polymers formed in vitro have structural identity with those isolated from the liver of a Z homozygote. 2. That loop-sheet polymerization is a more general phenomenon was shown by the examination of a second deficiency variant, antitrypsin Siiyama (Ser-53-->Phe), which is also associated with liver inclusions. Electron microscopy confirmed that isolated antitrypsin Siiyama from the plasma of a homozygote was present as long chains of polymers identical with those of Z antitrypsin.
摘要
  1. α1 -抗胰蛋白酶的Z型缺陷变体使纯合子易患早发性全小叶型肺气肿,并导致抗胰蛋白酶在肝细胞内蓄积,进而导致肝细胞损伤和肝硬化。这种蓄积的机制已表明是由于Z突变(Glu - 342→Lys)扰乱了蛋白质结构,使得一个分子的反应中心环与另一个分子的A片层之间发生独特的相互作用。这种环片层聚合在纯化的血浆Z型抗胰蛋白酶中于37℃时自发发生,但在M型抗胰蛋白酶中不会发生。聚合速率在41℃时大大加快,并被向抗胰蛋白酶分子的A片层中插入特定肽所阻断。电子显微镜和圆二色光谱分析证实,体外形成的Z型抗胰蛋白酶聚合物与从Z型纯合子肝脏中分离出的聚合物具有结构同一性。2. 通过对第二种缺陷变体抗胰蛋白酶Siiyama(Ser - 53→Phe)的研究表明,环片层聚合是一种更普遍的现象,该变体也与肝脏内含物有关。电子显微镜证实,从纯合子血浆中分离出的抗胰蛋白酶Siiyama以与Z型抗胰蛋白酶相同的长链聚合物形式存在。

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