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首页> 外文期刊>Infection and immunity >Arthropathic properties of gonococcal peptidoglycan fragments: implications for the pathogenesis of disseminated gonococcal disease.
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Arthropathic properties of gonococcal peptidoglycan fragments: implications for the pathogenesis of disseminated gonococcal disease.

机译:淋病球菌肽聚糖片段的关节病理特性:对传播性淋病球菌疾病的发病机制的影响。

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We examined the arthropathic activity of purified peptidoglycan (PG) fragments derived from (i) lysozyme-resistant, extensively O-acetylated PG from Neisseria gonorrhoeae FA19 (O-PG), and (ii) lysozyme-sensitive, O-acetyl-deficient PG from N. gonorrhoeae RD5 (non-O-PG). Male Lewis rats were injected intradermally in the tail with 200 micrograms of PG emulsified in mineral oil and water (1:1) or with the oil and water emulsion alone (controls). Quantitation of hind paw size indicated that macromolecular PG of various chemical and physical forms induced paw swelling (P versus controls, less than 0.01) that was evident at about day 14 and that reached a maximum at about day 24. PG-mediated paw swelling was accompanied by intense synovitis with some cartilage and bone involvement. The minimal arthropathic dose of soluble macromolecular PG was 20 micrograms per rat. Of particular interest was that macromolecular O-PGs from strain FA19 caused considerably more extensive swelling than did either their RD5 non-O-PG counterparts or the homologous FA19 PG that had been de-O-acetylated by mild alkali treatment. This suggested that the persistence of hydrolase-resistant high-molecular-weight fragments, afforded by extensive O-acetylation, may be important for optimal expression of arthropathic activity. However, oligomeric PG was not an absolute requirement, since even low-molecular-weight fragments, including the anhydro-muramyl-containing disaccharide peptide monomer released by growing gonococci, were also arthritogenic. Experiments employing purified gonococcal lipopolysaccharide indicated that the arthropathic activity of PG preparations was not due to contaminating lipopolysaccharide. Based on the arthritogenicity of gonococcal PG in this model system, we suggest that PG may play a role in the pathogenesis of gonococcal arthritis, and that such an activity might be potentiated by the persistence of hydrolase-resistant O-PG.
机译:我们检查了从(i)淋病奈瑟氏球菌FA19(O-PG)的耐溶菌酶的,广泛O-乙酰化的PG和(ii)溶菌酶敏感的,O-乙酰基缺乏的PG衍生的纯化肽聚糖(PG)片段的关节活性来自淋病奈瑟氏球菌RD5(非O-PG)。在雄性Lewis大鼠的尾巴内皮内注射200微克在矿物油和水中乳化的PG(1:1)或仅在油和水乳化液中(对照组)注射。后足大小的定量表明,各种化学和物理形式的大分子PG引起足爪肿胀(P与对照组相比,小于0.01),在第14天时明显,在第24天达到最大。伴有严重的滑膜炎,伴有软骨和骨受累。可溶性大分子PG的最小关节病剂量为每只大鼠20微克。特别令人感兴趣的是,菌株FA19的大分子O-PG引起的溶胀比其RD5非O-PG对应物或已通过轻度碱处理脱O-乙酰化的同源FA19 PG引起的膨胀要大得多。这表明由广泛的O-乙酰化提供的耐水解酶的高分子量片段的持久性对于关节活性的最佳表达可能是重要的。然而,寡聚PG不是绝对必要的,因为即使低分子量的片段,包括通过生长的球菌而释放的含脱水基-山m基的二糖肽单体,也是致关节炎的。使用纯化的淋球菌脂多糖的实验表明,PG制剂的关节病活性不是由于污染脂多糖引起的。基于该模型系统中淋球菌PG的致关节炎性,我们认为PG可能在淋球菌性关节炎的发病机理中起作用,并且这种活性可能会因耐水解酶的O-PG的持续存在而增强。

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