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MRL/I小鼠和类风湿性关节炎患者滑膜细胞中胶原分解性及Ras诱导的半胱氨酸蛋白酶组织蛋白酶L与增殖相关癌基因的表达

Expression of the collagenolytic and Ras-induced cysteine proteinase cathepsin L and proliferation-associated oncogenes in synovial cells of MRL/I mice and patients with rheumatoid arthritis.

作者信息

Trabandt A, Aicher W K, Gay R E, Sukhatme V P, Nilson-Hamilton M, Hamilton R T, McGhee J R, Fassbender H G, Gay S

机构信息

Department of Medicine, University of Alabama, Birmingham 35294.

出版信息

Matrix. 1990 Dec;10(6):349-61. doi: 10.1016/s0934-8832(11)80142-3.

Abstract

Based on the observation that rheumatoid joint destruction is related to the presence of transformed-appearing proliferating synovial lining cells attached to cartilage and bone at the site of early destruction, we searched for the expression of proliferation- and transformation-associated oncoproteins in synovial tissues from patients with early destructive rheumatoid arthritis (RA). Immunolocalization of Ras and Myc proteins was found in about 70% of the RA cases and was restricted to the proliferating synovial lining cells. The cysteine proteinase, cathepsin L, which has been shown to be the major ras-induced protein in ras-transformed murine NIH 3T3 cells, was detected in 50% of the RA cases, predominantly in synovial cells attached to cartilage and bone at the site of joint destruction. Moreover, utilizing cytoplastic dot hybridization analysis, we demonstrated the presence of RNA sequences complementary to human cathepsin L in primary cultures of human synovial cells from RA joints and complementary to murine cathepsin L in synovial lining cells derived from MRL/l mice developing spontaneously a RA-like disease. Significant levels of ras oncogene transcripts and products in human RA synovial cells associated with an increased expression of the cathepsin L gene indicate that this collagen-degrading enzyme may contribute to the destruction of cartilage and bone in RA.

摘要

基于类风湿性关节破坏与早期破坏部位附着于软骨和骨的形态转化的增殖性滑膜衬里细胞的存在有关这一观察结果,我们在早期破坏性类风湿性关节炎(RA)患者的滑膜组织中寻找增殖和转化相关癌蛋白的表达。在约70%的RA病例中发现了Ras和Myc蛋白的免疫定位,且局限于增殖的滑膜衬里细胞。半胱氨酸蛋白酶组织蛋白酶L,已被证明是ras转化的小鼠NIH 3T3细胞中主要的ras诱导蛋白,在50%的RA病例中被检测到,主要存在于关节破坏部位附着于软骨和骨的滑膜细胞中。此外,利用细胞质斑点杂交分析,我们在来自RA关节的人滑膜细胞原代培养物中证明了与人类组织蛋白酶L互补的RNA序列的存在,以及在自发发展为类RA疾病的MRL/l小鼠的滑膜衬里细胞中与小鼠组织蛋白酶L互补的RNA序列的存在。人类RA滑膜细胞中ras癌基因转录本和产物的显著水平与组织蛋白酶L基因表达的增加相关,表明这种胶原降解酶可能促成了RA中软骨和骨的破坏。

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