Yazdanbakhsh K, Park C G, Winslow G M, Choi Y
Howard Hughes Medical Institute, Rockefeller University, New York 10021.
J Exp Med. 1993 Aug 1;178(2):737-41. doi: 10.1084/jem.178.2.737.
It has recently been shown that open reading frames in the 3' long terminal repeats of mouse mammary tumor viruses encode superantigens. These viral superantigens (vSAGs) stimulate most T cells expressing appropriate V beta s almost regardless of the rest of the variable components of the T cell receptors (TCR) expressed by those cells. vSAGs produce a type II integral membrane protein with a nonessential short cytoplasmic domain and a large glycosylated extracellular COOH-terminal domain, which is predicted to interact with major histocompatibility complex class II molecules and the TCR. The transmembrane region of vSAG also has an internal positively charged lysine residue of unknown significance. A set of chimeric and mutant vSAG genes has been used in transfection experiments to show that only the extreme COOH-terminal portion of vSAGs determine their TCR V beta specificities, and to show that the lysine residue in the transmembrane domain is not essential for the function of vSAG.
最近研究表明,小鼠乳腺肿瘤病毒3'长末端重复序列中的开放阅读框编码超抗原。这些病毒超抗原(vSAGs)几乎可以刺激大多数表达合适Vβ的T细胞,而几乎不考虑这些细胞所表达的T细胞受体(TCR)可变成分的其余部分。vSAGs产生一种II型整合膜蛋白,其具有一个非必需的短细胞质结构域和一个大的糖基化细胞外COOH末端结构域,预计该结构域与主要组织相容性复合体II类分子和TCR相互作用。vSAG的跨膜区域还具有一个意义未知的带正电荷的内部赖氨酸残基。一组嵌合和突变的vSAG基因已用于转染实验,以表明只有vSAGs的极端COOH末端部分决定其TCR Vβ特异性,并表明跨膜结构域中的赖氨酸残基对于vSAG的功能不是必需的。
