Julio S M, Heithoff D M, Mahan M J
Department of Molecular, Cellular, and Developmental Biology, University of California, Santa Barbara, California 93106, USA.
J Bacteriol. 2000 Mar;182(6):1558-63. doi: 10.1128/JB.182.6.1558-1563.2000.
Escherichia coli ssrA encodes a small stable RNA molecule, tmRNA, that has many diverse functions, including tagging abnormal proteins for degradation, supporting phage growth, and modulating the activity of DNA binding proteins. Here we show that ssrA plays a role in Salmonella enterica serovar Typhimurium pathogenesis and in the expression of several genes known to be induced during infection. Moreover, the phage-like attachment site, attL, encoded within ssrA, serves as the site of integration of a region of Salmonella-specific sequence; adjacent to the 5' end of ssrA is another region of Salmonella-specific sequence with extensive homology to predicted proteins encoded within the unlinked Salmonella pathogenicity island SPI4. S. enterica serovar Typhimurium ssrA mutants fail to support the growth of phage P22 and are delayed in their ability to form viable phage particles following induction of a phage P22 lysogen. These data indicate that ssrA plays a role in the pathogenesis of Salmonella, serves as an attachment site for Salmonella-specific sequences, and is required for the growth of phage P22.
大肠杆菌的ssrA编码一种小的稳定RNA分子,即转运信使RNA(tmRNA),它具有多种不同功能,包括标记异常蛋白质以便降解、支持噬菌体生长以及调节DNA结合蛋白的活性。在此我们表明,ssrA在鼠伤寒沙门氏菌致病过程中发挥作用,并且在感染期间已知被诱导表达的几个基因的表达中也起作用。此外,ssrA内编码的类噬菌体附着位点attL,是一段沙门氏菌特异性序列区域的整合位点;在ssrA的5'端相邻处是另一段沙门氏菌特异性序列区域,它与未连锁的沙门氏菌致病岛SPI4内预测的蛋白质具有广泛的同源性。鼠伤寒沙门氏菌的ssrA突变体无法支持噬菌体P22的生长,并且在诱导噬菌体P22溶原菌后,其形成有活力噬菌体颗粒的能力会延迟。这些数据表明,ssrA在沙门氏菌的致病过程中发挥作用,作为沙门氏菌特异性序列的附着位点,并且是噬菌体P22生长所必需的。