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产后存活、表皮屏障功能、毛囊发育及胸腺稳态均需要胃蛋白酶/MT-SP1。

Matriptase/MT-SP1 is required for postnatal survival, epidermal barrier function, hair follicle development, and thymic homeostasis.

作者信息

List Karin, Haudenschild Christian C, Szabo Roman, Chen WanJun, Wahl Sharon M, Swaim William, Engelholm Lars H, Behrendt Niels, Bugge Thomas H

机构信息

Oral and Pharyngeal Cancer Branch, National Institute of Dental and Craniofacial Research, National Institutes of Health, 30 Convent Drive, Bethesda, Maryland, MD 20892, USA.

出版信息

Oncogene. 2002 May 23;21(23):3765-79. doi: 10.1038/sj.onc.1205502.

DOI:10.1038/sj.onc.1205502
PMID:12032844
Abstract

Matriptase/MT-SP1 is a novel tumor-associated type II transmembrane serine protease that is highly expressed in the epidermis, thymic stroma, and other epithelia. A null mutation was introduced into the Matriptase/MT-SP1 gene of mice to determine the role of Matriptase/MT-SP1 in epidermal development and neoplasia. Matriptase/MT-SP1-deficient mice developed to term but uniformly died within 48 h of birth. All epidermal surfaces of newborn mice were grossly abnormal with a dry, red, shiny, and wrinkled appearance. Matriptase/MT-SP1-deficiency caused striking malformations of the stratum corneum, characterized by dysmorphic and pleomorphic corneocytes and the absence of vesicular bodies in transitional layer cells. This aberrant skin development seriously compromised both inward and outward epidermal barrier function, leading to the rapid and fatal dehydration of Matriptase/MT-SP1-deficient pups. Loss of Matriptase/MT-SP1 also seriously affected hair follicle development resulting in generalized follicular hypoplasia, absence of erupted vibrissae, lack of vibrissal hair canal formation, ingrown vibrissae, and wholesale abortion of vibrissal follicles. Furthermore, Matriptase/MT-SP1-deficiency resulted in dramatically increased thymocyte apoptosis, and depletion of thymocytes. This study demonstrates that Matriptase/MT-SP1 has pleiotropic functions in the development of the epidermis, hair follicles, and cellular immune system.

摘要

胃蛋白酶/MT-SP1是一种新型的肿瘤相关II型跨膜丝氨酸蛋白酶,在表皮、胸腺基质和其他上皮组织中高度表达。在小鼠的胃蛋白酶/MT-SP1基因中引入无效突变,以确定胃蛋白酶/MT-SP1在表皮发育和肿瘤形成中的作用。胃蛋白酶/MT-SP1基因缺陷的小鼠足月出生,但在出生后48小时内全部死亡。新生小鼠的所有表皮表面均明显异常,呈现干燥、发红、发亮和起皱的外观。胃蛋白酶/MT-SP1缺乏导致角质层出现明显畸形,其特征为角质形成细胞形态异常和多形性,以及过渡层细胞中无囊泡体。这种异常的皮肤发育严重损害了表皮的内外屏障功能,导致胃蛋白酶/MT-SP1基因缺陷的幼崽迅速致命脱水。胃蛋白酶/MT-SP1的缺失也严重影响毛囊发育,导致普遍的毛囊发育不全、触须未萌出、触须毛囊管未形成、触须向内生长以及触须毛囊大量流产。此外,胃蛋白酶/MT-SP1缺乏导致胸腺细胞凋亡显著增加和胸腺细胞耗竭。这项研究表明,胃蛋白酶/MT-SP1在表皮、毛囊和细胞免疫系统的发育中具有多效性功能。

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