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[牙龈卟啉单胞菌牙周致病蛋白酶与宿主细胞的研究]

[Studies on periodontal pathogenic proteinases from Porphyromonas gingivalis and host cells].

作者信息

Yamamoto K

机构信息

Department of Pharmacology, Kyushu University Faculty of Dentistry, Fukuoka, Japan.

出版信息

Nihon Yakurigaku Zasshi. 1995 May;105(5):345-55. doi: 10.1254/fpj.105.345.

Abstract

Progressive periodontal disease is characterized by acute progressive lesions of gingival connective tissues, excessive leukocyte infiltration, and occurrence of a characteristic microflora. A variety of proteolytic enzymes derived from oral bacteria and host cells are found in gingival crevices and thought to play an important role in the onset and development of progressive periodontal disease. The anaerobic bacterium Porphyromonas gingivalis has been implicated in the etiology of the disease. Recently, we have purified a novel arginine-specific cysteine proteinase, termed "argingipain", from the culture supernatant of the organism. The enzyme was shown to have two important abilities related to the virulence of the organism. One is direct association with periodontal tissue breakdown through its abilities to degrade physiologically important proteins such as human collagens (type I and IV) and to evade inactivation by internal protease inhibitors. The other is associated with disruption of the normal host defense mechanisms through its abilities to degrade immunoglobulins and to inhibit the bactericidal activity of polymorphonuclear leukocytes. The virulence of argingipain was further substantiated by disruption of argingipain-encoding genes on the chromosome by use of suicide plasmid systems. On the other hand, we have studied roles of host cell-derived proteinases in the periodontal tissue breakdown. Levels of lysosomal proteinases such as cathepsins B, H, L, G and medullasin were determined in gingival crevicular fluid from periodontitis patients and experimental gingivitis subjects by activity measurement and sensitive immunoassay. The results suggested that all of these enzymes would be involved in the development of both gingivitis and periodontitis.

摘要

进行性牙周病的特征是牙龈结缔组织的急性进行性病变、白细胞过度浸润以及特征性微生物群的出现。在牙龈沟中发现了多种源自口腔细菌和宿主细胞的蛋白水解酶,它们被认为在进行性牙周病的发生和发展中起重要作用。厌氧菌牙龈卟啉单胞菌被认为与该疾病的病因有关。最近,我们从该生物体的培养上清液中纯化了一种新型的精氨酸特异性半胱氨酸蛋白酶,称为“精氨酸牙龈蛋白酶”。该酶显示出与该生物体毒力相关的两种重要能力。一种是通过其降解生理上重要的蛋白质(如人类胶原蛋白(I型和IV型))的能力以及逃避内部蛋白酶抑制剂失活的能力,直接与牙周组织破坏相关。另一种是通过其降解免疫球蛋白和抑制多形核白细胞杀菌活性的能力,与破坏正常宿主防御机制相关。通过使用自杀质粒系统破坏染色体上精氨酸牙龈蛋白酶编码基因,进一步证实了精氨酸牙龈蛋白酶的毒力。另一方面,我们研究了宿主细胞衍生的蛋白酶在牙周组织破坏中的作用。通过活性测量和灵敏的免疫测定法,测定了牙周炎患者和实验性牙龈炎受试者牙龈沟液中溶酶体蛋白酶(如组织蛋白酶B、H、L、G和髓质素)的水平。结果表明,所有这些酶都与牙龈炎和牙周炎的发展有关。

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