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与链球菌细胞壁肽聚糖 - 多糖聚合物分子量相关的关节病特性。

Arthropathic properties related to the molecular weight of peptidoglycan-polysaccharide polymers of streptococcal cell walls.

作者信息

Fox A, Brown R R, Anderle S K, Chetty C, Cromartie W J, Gooder H, Schwab J H

出版信息

Infect Immun. 1982 Mar;35(3):1003-10. doi: 10.1128/iai.35.3.1003-1010.1982.

Abstract

The covalently bound polymers of peptidoglycan and group-specific polysaccharide (PG-APS) were isolated from the cell walls of group A streptococci. Arthritis was induced in rats with a single intraperitoneal injection of an aqueous suspension of PG-APS fragments derived by sonication. The joint lesions induced with this polydisperse suspension followed a bimodal pattern consisting of an acute phase, which reached a peak 5 days after injection and then receded, followed by a chronic, remittent, erosive arthritis lasting several months. The relative severities of the acute and chronic phases could be manipulated by selection of the size of PG-APS fragments. The fragments of PG-APS obtained by sonic treatment were resolved on the basis of size into three major populations by sucrose gradient or differential centrifugation. Based upon light scattering and gel filtration, the average molecular weight of the largest family of fragments was estimated to be about 500 x 10(6), the intermediate fragments were 50 x 10(6) daltons, and the predominant size in the smallest population was 5.3 x 10(6) daltons. The larger fragments induced negligible acute inflammation, but chronic disease became apparent 5 to 9 weeks after injection. The smallest fragments induced the most severe acute inflammation, with relatively little late, chronic joint disease. The particles of intermediate size induced moderate acute inflammation and the most severe chronic, erosive joint lesions. A single injection of fragments of the isolated peptidoglycan moiety of the PG-APS induced only a moderate acute inflammation of joints, with no apparent capacity to maintain the injury and induce chronic disease.

摘要

从A组链球菌细胞壁中分离出肽聚糖和群特异性多糖(PG-APS)的共价结合聚合物。通过腹腔内单次注射经超声处理得到的PG-APS片段的水悬浮液,在大鼠中诱发关节炎。用这种多分散悬浮液诱发的关节损伤呈现双峰模式,包括急性期,在注射后5天达到峰值,然后消退,随后是持续数月的慢性、缓解性、侵蚀性关节炎。急性期和慢性期的相对严重程度可通过选择PG-APS片段的大小来控制。通过蔗糖梯度或差速离心,根据大小将经超声处理获得的PG-APS片段分为三个主要群体。基于光散射和凝胶过滤,最大片段家族的平均分子量估计约为500×10⁶,中间片段为50×10⁶道尔顿,最小群体中的主要大小为5.3×10⁶道尔顿。较大的片段诱发的急性炎症可忽略不计,但在注射后5至9周出现明显的慢性疾病。最小的片段诱发最严重的急性炎症,后期慢性关节疾病相对较少。中等大小的颗粒诱发中度急性炎症和最严重的慢性侵蚀性关节损伤。单次注射PG-APS分离的肽聚糖部分的片段仅诱发关节中度急性炎症,没有明显的维持损伤和诱发慢性疾病的能力。

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