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环孢素A对小鼠高剂量绵羊红细胞迟发型超敏反应的增强作用:药物剂量和给药途径的影响及脾细胞群体分析

Augmentation of delayed-type hypersensitivity to high dose sheep erythrocytes by cyclosporin A in the mouse: influence of drug dosage and route of administration and analysis of spleen cell populations.

作者信息

Webster L M, Thomson A W

机构信息

Department of Pathology, University of Aberdeen, Scotland, UK.

出版信息

Clin Exp Immunol. 1988 Jan;71(1):149-54.

Abstract

When administered by various routes 48 h before a high systemic dose (10 degrees) of sheep red blood cells (SRBC), Cyclosporin A (CsA) prevented the suppression of delayed-type hypersensitivity (DTH) reactions elicited 4 days later. Augmentation of DTH was observed over a wide range (5-200 mg/kg) and with circulating CsA levels ranging below 45 ng/ml at the time of immunization or antigen challenge. Splenic lymphocytes from vehicle- and CsA-treated mice exhibited good proliferative responses to mitogen in vitro, but only those from CsA-treated animals responded to antigen. Expression of DTH was associated with a progressive, 2-fold increase in the absolute numbers of splenic L3T4+ cells, whereas no significant alteration in the number of Lyt-2+ lymphocytes was recorded. B cell and macrophage numbers in the spleen were unaffected by CsA. In contrast to its potentiating effects on cell-mediated immunity, CsA caused profound (up to 100%) suppression of the concomitant production of splenic anti-SRBC IgM-secreting plasma cells. Circulating anti-SRBC antibody levels were also markedly reduced. These data show that CsA can permit induction of TDTH, whilst suppressing T-dependent humoral immunity and without significant change in absolute numbers of Lyt-2+ cells.

摘要

在高全身剂量(10度)的绵羊红细胞(SRBC)注射前48小时,通过各种途径给予环孢素A(CsA),可预防4天后引发的迟发型超敏反应(DTH)的抑制。在广泛的剂量范围(5-200mg/kg)内观察到DTH增强,且在免疫或抗原攻击时循环CsA水平低于45ng/ml。来自载体处理和CsA处理小鼠的脾淋巴细胞在体外对有丝分裂原表现出良好的增殖反应,但只有来自CsA处理动物的淋巴细胞对抗原作出反应。DTH的表达与脾L3T4 +细胞绝对数量的逐渐增加2倍相关,而Lyt-2 +淋巴细胞数量没有显著变化。脾脏中的B细胞和巨噬细胞数量不受CsA影响。与它对细胞介导免疫的增强作用相反,CsA导致脾脏分泌抗SRBC IgM的浆细胞的伴随产生受到深度抑制(高达100%)。循环抗SRBC抗体水平也显著降低。这些数据表明,CsA可以允许诱导迟发型超敏反应性T细胞(TDTH),同时抑制T细胞依赖性体液免疫,并且Lyt-2 +细胞的绝对数量没有显著变化。

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