Department of Biochemistry and Biophysics, Arrhenius Laboratories for Natural Science, Stockholm University, SE-10691 Stockholm, Sweden.
Physiol Plant. 2012 May;145(1):180-6. doi: 10.1111/j.1399-3054.2011.01531.x. Epub 2011 Nov 21.
A novel mitochondrial and chloroplast peptidasome, the Presequence Protease (PreP) degrades organellar targeting peptides as well as other unstructured peptides up to 65 amino acid residues in length. PreP belongs to the pitrilysin oligopeptidase family (M16C) containing an inverted zinc-binding motif. The crystal structure of Arabidopsis thaliana PreP, AtPreP, refined at 2.1 Å, revealed a novel mechanism of proteolysis in which two halves of the enzyme connected by a hinge region enclose a large catalytic chamber opening and closing in response to peptide binding. Double knock-out mutant of AtPreP1 and AtPreP2 results in a severe phenotype, including decreased size and growth rate, chlorosis and organellar abnormalities, such as altered chloroplast starch content, partial loss of the integrity of the inner mitochondrial membrane and reduced mitochondrial respiration. PreP homologues are also present in yeast and humans. Interestingly, human PreP has been associated with Alzheimer's disease as it is responsible for degradation of amyloid-β peptide in brain mitochondria.
一种新型的线粒体和叶绿体肽酶体,前导序列蛋白酶(PreP)可降解靶向细胞器的肽段以及其他长度达 65 个氨基酸残基的无规则肽段。PreP 属于包含反向锌结合基序的肽酶 M16C 家族。拟南芥 PreP(AtPreP)的晶体结构,经 2.1Å 精修,揭示了一种新的蛋白水解机制,其中通过铰链区连接的酶的两半包围一个大的催化腔,该腔响应肽结合而打开和关闭。AtPreP1 和 AtPreP2 的双敲除突变体导致严重的表型,包括大小和生长速度降低、黄化和细胞器异常,如改变叶绿体淀粉含量、部分丧失线粒体内膜的完整性和降低线粒体呼吸作用。酵母和人类中也存在 PreP 同源物。有趣的是,人类 PreP 与阿尔茨海默病有关,因为它负责降解大脑线粒体中的淀粉样β肽。
