Tabi Z, Allan J E, Ceredig R, Doherty P C
Department of Experimental Pathology, John Curtin School of Medical Research, Canberra, Australia.
Immunology. 1988 Mar;63(3):423-9.
Prior treatment of C57BL/6J mice with 300 mg/kg of cyclophosphamide (Cy) converts a subclinical infection with vaccinia virus to a lethal disease. This is accompanied by a loss of more than 80% of spleen cells and a decreased capacity, on a cell-for-cell basis, to develop virus-immune cytotoxic T lymphocytes (CTL), although the frequency of CTL precursors among surviving T cells is not greatly modified. Phenotypically, the surviving T cells express low levels of cell-surface Thy-1, Lyt-2 and L3T4 and, upon stimulation, are less able to produce IL-2 for more than 1 week following Cy treatment. The defect in capacity to generate CTL effectors both in vitro and in vivo can be corrected by providing an exogenous source of IL-2. These experiments indicate that a single dose of Cy induces changes in T cells that persist throughout the development of an immune response. Such effects are in accordance with the known property of Cy to mediate DNA damage.
用300mg/kg环磷酰胺(Cy)预先处理C57BL/6J小鼠,可使亚临床痘苗病毒感染转变为致死性疾病。这伴随着超过80%的脾细胞丢失,并且在逐个细胞基础上,产生病毒免疫细胞毒性T淋巴细胞(CTL)的能力下降,尽管存活T细胞中CTL前体的频率没有太大改变。从表型上看, 存活的T细胞表达低水平的细胞表面Thy-1、Lyt-2和L3T4,并且在受到刺激后,在Cy处理后的1周多时间内产生IL-2的能力较弱。通过提供外源性IL-2可以纠正体外和体内产生CTL效应细胞能力的缺陷。这些实验表明,单剂量的Cy会诱导T细胞发生变化,这些变化在免疫反应的整个发展过程中持续存在。这种效应与Cy介导DNA损伤的已知特性一致。