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抗肿瘤药物米托蒽醌的选择性免疫调节作用。I. B淋巴细胞功能的抑制

Selective immunomodulation by the antineoplastic agent mitoxantrone. I. Suppression of B lymphocyte function.

作者信息

Fidler J M, DeJoy S Q, Gibbons J J

出版信息

J Immunol. 1986 Jul 15;137(2):727-32.

PMID:3487580
Abstract

Novantrone mitoxantrone, an antineoplastic agent with antiproliferative properties, is under investigation as an immunomodulating agent. The impact of mitoxantrone treatment on B lymphocyte reactivity is presented here. Administered i.p. in H2O at a dose of 0.5 mg/kg, daily for 14 days, mitoxantrone abrogated both the in vivo antibody response (to ovalbumin) and the in vitro plaque-forming cell (PFC) response (to SRC). In addition to the effects on thymus-dependent reactivity, PFC responses to the thymus-independent antigens TNP-LPS and TNP-Ficoll were also inhibited when tested in vivo or in vitro. B cells were identified as a target for the suppressive activity of mitoxantrone by using T cell-replacing factor to reconstitute the in vitro anti-SRC PFC response of a T lymphocyte-depleted spleen cell preparation. LPS-induced B cell mitogenesis was largely inhibited by mitoxantrone treatment. However, depletion of Sephadex G-10-adherent cells significantly restored the proliferative response. Flow cytometric analysis revealed a dramatic decrease in splenic B lymphocyte content. Therefore, mitoxantrone exerted a potent suppressive influence on the humoral immune system through a direct reduction in B cell number augmented by macrophage-mediated inhibition of B cell proliferation.

摘要

诺维本(米托蒽醌)是一种具有抗增殖特性的抗肿瘤药物,目前正作为一种免疫调节剂进行研究。本文介绍了米托蒽醌治疗对B淋巴细胞反应性的影响。米托蒽醌以0.5毫克/千克的剂量溶于水中,腹腔注射,每日一次,共14天,它消除了体内抗体反应(针对卵清蛋白)和体外空斑形成细胞(PFC)反应(针对SRC)。除了对胸腺依赖性反应的影响外,在体内或体外检测时,对胸腺非依赖性抗原TNP-LPS和TNP-Ficoll的PFC反应也受到抑制。通过使用T细胞替代因子来重建T淋巴细胞耗竭的脾细胞制剂的体外抗SRC PFC反应,确定B细胞是米托蒽醌抑制活性的靶点。米托蒽醌治疗在很大程度上抑制了LPS诱导的B细胞有丝分裂。然而,去除葡聚糖G-10黏附细胞可显著恢复增殖反应。流式细胞术分析显示脾B淋巴细胞含量显著下降。因此,米托蒽醌通过直接减少B细胞数量,并增强巨噬细胞介导的对B细胞增殖的抑制作用,对体液免疫系统产生了强大的抑制影响。

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