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小鼠对淋巴细胞性脉络丛脑膜炎病毒的免疫反应。V. 急性感染期间脾脏中产生大量细胞毒性T淋巴细胞。

The immune response of the mouse to lymphocytic choriomeningitis virus. V. High numbers of cytolytic T lymphocytes are generated in the spleen during acute infection.

作者信息

Moskophidis D, Assmann-Wischer U, Simon M M, Lehmann-Grube F

出版信息

Eur J Immunol. 1987 Jul;17(7):937-42. doi: 10.1002/eji.1830170707.

Abstract

In the spleens of C57BL/6J (B6) and CBA/J (CBA) mice undergoing acute infection with lymphocytic choriomeningitis (LCM) virus, lymphocytes with the ability to develop in vitro into LCM virus-specific cytolytic clones were enumerated by use of the limiting dilution method. At intervals after virus inoculation, defined numbers of cells were cultivated with virus-infected syngeneic stimulator cells and T cell growth factor in multiple wells of microculture plates. After 7 days, individual cell cultures were tested for their ability to cause release of 51Cr from infected and uninfected syngeneic target cells. In cultures seeded with spleen cells from uninfected mice or from mice infected 3 days previously, no cytolytic activity was observed. On day 5, cells developing into LCM virus-specific cytolytic effector cells were detected. They rose in numbers, and on days 8 to 9 after infection, values of approximately 1/10 and 1/200 in B6 and CBA mice, respectively, were calculated. A low proportion of microcultures proved cytolytic also for noninfected syngeneic target cells, but the counts thus released were consistently much lower than the counts set free from infected targets, and no regular dose-response relationships existed between seeded cells and positive cultures. Determination of cell surface antigens of responder cells by negative and positive selection procedures disclosed that they were predominantly T lymphocytes and expressed Lyt-2 but not L3T4 surface markers. Lysis by the great majority of LCM virus-specific clones was restricted by products of the major histocompatibility gene complex (MHC), but a few lysed, in addition, allogeneic infected or uninfected targets; however, a consistent pattern of alloreactivity was not observed. Furthermore, cells of a proportion of the cultures also lysed uninfected YAC cells. Probably this natural killer-like activity was acquired by T lymphocytes during prolonged cultivation. We conclude that most spleen cells that during acute infection with LCM virus attained the ability to develop in vitro into LCM virus-specific cytolytic clones were derived from MHC-restricted Lyt-2+, L3T4- antigen-specific cytolytic T lymphocytes and their activated precursors.

摘要

在感染淋巴细胞性脉络丛脑膜炎(LCM)病毒的C57BL/6J(B6)和CBA/J(CBA)小鼠的脾脏中,运用极限稀释法对具有在体外发育成LCM病毒特异性溶细胞克隆能力的淋巴细胞进行计数。在病毒接种后的不同时间间隔,将一定数量的细胞与病毒感染的同基因刺激细胞以及T细胞生长因子一起在微量培养板的多个孔中培养。7天后,检测各个细胞培养物使感染和未感染的同基因靶细胞释放51Cr的能力。在用未感染小鼠或3天前感染小鼠的脾细胞接种的培养物中,未观察到溶细胞活性。在第5天,检测到发育成LCM病毒特异性溶细胞效应细胞的细胞。它们的数量增加,在感染后的第8至9天,B6和CBA小鼠中的值分别计算为约1/10和1/200。低比例的微量培养物对未感染的同基因靶细胞也显示出溶细胞作用,但由此释放的计数始终远低于从感染靶细胞释放的计数,并且接种细胞与阳性培养物之间不存在常规的剂量反应关系。通过阴性和阳性选择程序对反应细胞的细胞表面抗原进行测定,结果显示它们主要是T淋巴细胞,表达Lyt-2但不表达L3T4表面标志物。绝大多数LCM病毒特异性克隆的裂解受主要组织相容性基因复合体(MHC)产物的限制,但少数克隆除了裂解同基因感染或未感染的靶细胞外,还裂解异基因感染或未感染的靶细胞;然而,未观察到一致的同种异体反应模式。此外,一部分培养物的细胞也裂解未感染的YAC细胞。可能这种自然杀伤样活性是T淋巴细胞在长时间培养过程中获得的。我们得出结论,在急性感染LCM病毒期间获得在体外发育成LCM病毒特异性溶细胞克隆能力的大多数脾细胞源自MHC限制的Lyt-2 +、L3T4 - 抗原特异性溶细胞T淋巴细胞及其活化前体。

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