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体内启动后反馈抑制性T细胞活性迅速丧失。

Rapid loss of feedback suppressor T-cell activity after priming in vivo.

作者信息

Rothermel A L, Calkins C E

出版信息

Immunology. 1986 Apr;57(4):539-43.

Abstract

T cells from antigen-primed mice have a diminished capacity to mediate feedback suppression when compared to T cells from unprimed mice. This was demonstrated using an in vitro model of B-cell induced feedback suppression in which spleen cells from mice primed with sheep erythrocytes (SRBC) activate feedback suppressor T-cell precursors to mediate suppression of the primed spleen cell response. The addition of splenic T cells from unprimed mice to cultures of spleen cells from SRBC-primed mice resulted in suppression of the secondary IgM and IgG anti-SRBC response. In contrast, no suppression was detected when T cells from mice primed with SRBC were added to the primed spleen cell cultures. The loss of suppression by T cells from primed mice was antigen-specific and was detectable by 24 hr after priming, coinciding with the appearance after priming of T-cell enhancing activity. The reduced suppressive activity could be due to changes in the active T-cell subset itself or to the appearance of cells or factors within the T-cell population that block or mask detection of feedback suppression. In either case, the present finding suggests that priming of a host not only activates feedback suppression induction mechanisms, but also rapidly affects the ability of the T-cell population to develop effective feedback suppression.

摘要

与未致敏小鼠的T细胞相比,来自抗原致敏小鼠的T细胞介导反馈抑制的能力减弱。这是通过B细胞诱导的反馈抑制体外模型证明的,在该模型中,用绵羊红细胞(SRBC)致敏的小鼠的脾细胞激活反馈抑制性T细胞前体,以介导对致敏脾细胞反应的抑制。将未致敏小鼠的脾T细胞添加到SRBC致敏小鼠的脾细胞培养物中,导致二次IgM和IgG抗SRBC反应受到抑制。相反,当将用SRBC致敏的小鼠的T细胞添加到致敏脾细胞培养物中时,未检测到抑制作用。致敏小鼠的T细胞抑制作用的丧失是抗原特异性的,在致敏后24小时即可检测到,这与致敏后T细胞增强活性的出现相一致。抑制活性降低可能是由于活性T细胞亚群本身的变化,或者是由于T细胞群体中出现了阻断或掩盖反馈抑制检测的细胞或因子。无论哪种情况,目前的发现表明,宿主的致敏不仅激活了反馈抑制诱导机制,而且还迅速影响了T细胞群体产生有效反馈抑制的能力。

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