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由组织蛋白酶蛋白酶基因突变引起的遗传性疾病。

Inherited diseases caused by mutations in cathepsin protease genes.

作者信息

Ketterer Stephanie, Gomez-Auli Alejandro, Hillebrand Larissa E, Petrera Agnese, Ketscher Anett, Reinheckel Thomas

机构信息

Medical Faculty, Institute of Molecular Medicine and Cell Research, Albert-Ludwigs-University Freiburg, Germany.

Faculty of Biology, Albert-Ludwigs-University Freiburg, Germany.

出版信息

FEBS J. 2017 May;284(10):1437-1454. doi: 10.1111/febs.13980. Epub 2017 Jan 12.

Abstract

Lysosomal cathepsins are proteolytic enzymes increasingly recognized as prognostic markers and potential therapeutic targets in a variety of diseases. In those conditions, the cathepsins are mostly overexpressed, thereby driving the respective pathogenic processes. Although less known, there are also diseases with a genetic deficiency of cathepsins. In fact, nowadays 6 of the 15 human proteases called 'cathepsins' have been linked to inherited syndromes. However, only three of these syndromes are typical lysosomal storage diseases, while the others are apparently caused by defective cleavage of specific protein substrates. Here, we will provide an introduction on lysosomal cathepsins, followed by a brief description of the clinical symptoms of the various genetic diseases. For each disease, we focus on the known mutations of which many have been only recently identified by modern genome sequencing approaches. We further discuss the effect of the respective mutation on protease structure and activity, the resulting pathogenesis, and possible therapeutic strategies.

摘要

溶酶体组织蛋白酶是蛋白水解酶,在多种疾病中越来越被视为预后标志物和潜在的治疗靶点。在这些情况下,组织蛋白酶大多过度表达,从而推动各自的致病过程。虽然鲜为人知,但也存在组织蛋白酶基因缺陷的疾病。事实上,如今15种被称为“组织蛋白酶”的人类蛋白酶中有6种已与遗传综合征相关联。然而,这些综合征中只有三种是典型的溶酶体贮积病,而其他综合征显然是由特定蛋白质底物的切割缺陷引起的。在此,我们将介绍溶酶体组织蛋白酶,随后简要描述各种遗传疾病的临床症状。对于每种疾病,我们重点关注已知的突变,其中许多突变是最近才通过现代基因组测序方法鉴定出来的。我们还将讨论各自突变对蛋白酶结构和活性的影响、由此产生的发病机制以及可能的治疗策略。

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