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小鼠和人类肥大细胞的蛋白酶-蛋白聚糖复合物及其β-组织蛋白酶-肝素复合物在炎症和固有免疫中的重要性。

Protease-proteoglycan complexes of mouse and human mast cells and importance of their beta-tryptase-heparin complexes in inflammation and innate immunity.

作者信息

Stevens Richard L, Adachi Roberto

机构信息

Department of Medicine, Harvard Medical School, Brigham and Women's Hospital, Boston, MA, USA.

出版信息

Immunol Rev. 2007 Jun;217:155-67. doi: 10.1111/j.1600-065X.2007.00525.x.

DOI:10.1111/j.1600-065X.2007.00525.x
PMID:17498058
Abstract

Approximately 50% of the weight of a mature mast cell (MC) consists of varied neutral proteases stored in the cell's secretory granules ionically bound to serglycin proteoglycans that contain heparin and/or chondroitin sulfate E/diB chains. Mouse MCs express the exopeptidase carboxypeptidase A3 and at least 15 serine proteases [designated as mouse MC protease (mMCP) 1-11, transmembrane tryptase/tryptase gamma/protease serine member S (Prss) 31, cathepsin G, granzyme B, and neuropsin/Prss19]. mMCP-6, mMCP-7, mMCP-11/Prss34, and Prss31 are the four members of the chromosome 17A3.3 family of tryptases that are preferentially expressed in MCs. One of the challenges ahead is to understand why MCs express so many different protease-proteoglycan macromolecular complexes. MC-like cells that contain tryptase-heparin complexes in their secretory granules have been identified in the Ciona intestinalis and Styela plicata urochordates that appeared approximately 500 million years ago. Because sea squirts lack B cells and T cells, it is likely that MCs and their tryptase-proteoglycan granule mediators initially appeared in lower organisms as part of their innate immune system. The conservation of MCs throughout evolution suggests that some of these protease-proteoglycan complexes are essential to our survival. In support of this conclusion, no human has been identified that lacks MCs. Moreover, transgenic mice lacking the beta-tryptase mMCP-6 are unable to combat a Klebsiella pneumoniae infection effectively. Here we summarize the nature and function of some of the tryptase-serglycin proteoglycan complexes found in mouse and human MCs.

摘要

成熟肥大细胞(MC)约50%的重量由存储在细胞分泌颗粒中的多种中性蛋白酶组成,这些蛋白酶与含有肝素和/或硫酸软骨素E/diB链的丝甘氨酸蛋白聚糖离子结合。小鼠MC表达外肽酶羧肽酶A3和至少15种丝氨酸蛋白酶[命名为小鼠MC蛋白酶(mMCP)1 - 11、跨膜类胰蛋白酶/类胰蛋白酶γ/蛋白酶丝氨酸成员S(Prss)31、组织蛋白酶G、颗粒酶B和神经蛋白酶/Prss19]。mMCP - 6、mMCP - 7、mMCP - 11/Prss34和Prss31是17A3.3染色体上类胰蛋白酶家族的四个成员,它们在MC中优先表达。未来面临的挑战之一是理解为什么MC会表达如此多不同的蛋白酶 - 蛋白聚糖大分子复合物。在约5亿年前出现的海鞘和皱瘤海鞘尾索动物中,已鉴定出在其分泌颗粒中含有类胰蛋白酶 - 肝素复合物的类MC细胞。由于海鞘缺乏B细胞和T细胞,MC及其类胰蛋白酶 - 蛋白聚糖颗粒介质可能最初在低等生物中作为其固有免疫系统的一部分出现。MC在整个进化过程中的保守性表明,这些蛋白酶 - 蛋白聚糖复合物中的一些对我们的生存至关重要。支持这一结论的是,尚未发现缺乏MC的人类。此外,缺乏β - 类胰蛋白酶mMCP - 6的转基因小鼠无法有效抵抗肺炎克雷伯菌感染。在此,我们总结了在小鼠和人类MC中发现的一些类胰蛋白酶 - 丝甘氨酸蛋白聚糖复合物的性质和功能。

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