Ravins M, Jaffe J, Hanski E, Shetzigovski I, Natanson-Yaron S, Moses A E
Department of Clinical Microbiology, Hebrew University-Hadassah Medical School, Jerusalem, Israel.
J Infect Dis. 2000 Dec;182(6):1702-11. doi: 10.1086/317635. Epub 2000 Oct 18.
JRS4(HE), a highly encapsulated, mouse-passaged variant of group A streptococcal strain JRS4, was characterized. The mucoid phenotype of JRS4(HE) was preserved after extensive passage in vitro. The level and size of csrRS transcript in JRS4(HE) was similar to that of JRS4, yet JRS4(HE) expressed high levels of has and sagA and exhibited an increased activity of streptolysin S. These findings indicate that the CsrRS repressor system was inactive in JRS4(HE). JRS4(HE) adhered to HEp-2 cells at the stationary phase but did not internalize these cells. At midlogarithmic phase, JRS4(HE) neither adhered to nor internalized cells, because of an increased amount of hyaluronic acid. Mice injected subcutaneously with JRS4(HE) developed large, deep necrotic lesions. In contrast, mice challenged with JRS4 developed small, superficial lesions. Despite the use of a high inoculum, mice challenged with JRS4(HE) did not develop a lethal bacteremic infection. It is concluded that inactivation of CsrRS in vivo is insufficient to cause a spreading necrotic disease.
对A组链球菌菌株JRS4经小鼠传代后的高度荚膜化变体JRS4(HE)进行了特性分析。JRS4(HE)的黏液样表型在体外多次传代后得以保留。JRS4(HE)中csrRS转录本的水平和大小与JRS4相似,但JRS4(HE)表达高水平的has和sagA,且表现出更高的链球菌溶血素S活性。这些发现表明CsrRS阻遏系统在JRS4(HE)中无活性。JRS4(HE)在稳定期可黏附于HEp-2细胞,但不内化这些细胞。在对数中期,由于透明质酸量增加,JRS4(HE)既不黏附也不内化细胞。皮下注射JRS4(HE)的小鼠会出现大而深的坏死性病变。相比之下,用JRS4攻击的小鼠出现小而表浅的病变。尽管使用了高接种量,但用JRS4(HE)攻击的小鼠并未发生致死性菌血症感染。结论是体内CsrRS失活不足以导致扩展性坏死性疾病。
