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人类对多次注射鼠源单克隆IgG的免疫反应。

Human immune response to multiple injections of murine monoclonal IgG.

作者信息

Shawler D L, Bartholomew R M, Smith L M, Dillman R O

出版信息

J Immunol. 1985 Aug;135(2):1530-5.

PMID:3874237
Abstract

Murine monoclonal antibody infusions in humans should induce a human anti-mouse immunoglobulin (mIgG) immune response, especially if multiple infusions over an extended period of time are necessary for therapeutic efficacy. We have administered multiple infusions of the murine monoclonal antibody T101 to patients with cutaneous T cell lymphoma (CTCL) or chronic lymphocytic leukemia (CLL). Five of 10 CTCL patients, compared with zero of six CLL patients, developed antibodies to mIgG. In those CTCL patients who did not demonstrate anti-mIgG antibodies, we were unable to correlate the lack of response to any of a large number of clinical parameters. Anti-mIgG antibodies were of both the mu and gamma isotypes and were detectable 14 days after the first infusion. Multiple infusions were associated with elevated titers. The anti-idiotypic portion of the anti-mIgG titer steadily increased with each infusion until eventually, in one patient receiving eight weekly infusions, well over one-half the serum anti-mIgG recognized only T101 and not four other murine IgG2AK antibodies tested. To increase our confidence in these findings, four separate assay systems were used to make these determinations. The identification of anti-idiotype antibodies as the dominant species of the immune response to multiple infusions of murine monoclonal antibody has major implications for future work with monoclonal antibodies. Although it has been suggested that human monoclonal antibodies would obviate an immune response, our work implies that such antibodies might still induce anti-idiotype antibodies if multiple infusions are administered.

摘要

在人体中输注鼠单克隆抗体应会引发人抗小鼠免疫球蛋白(mIgG)免疫反应,特别是如果为达到治疗效果需要在较长时间内进行多次输注。我们已对皮肤T细胞淋巴瘤(CTCL)或慢性淋巴细胞白血病(CLL)患者多次输注鼠单克隆抗体T101。10例CTCL患者中有5例产生了抗mIgG抗体,而6例CLL患者中无一例产生。在那些未表现出抗mIgG抗体的CTCL患者中,我们无法将无反应与大量临床参数中的任何一项相关联。抗mIgG抗体既有μ型也有γ型,在首次输注后14天即可检测到。多次输注与滴度升高相关。抗mIgG滴度的抗独特型部分随着每次输注稳步增加,直到最终,在一名每周接受8次输注的患者中,超过一半的血清抗mIgG仅识别T101,而不识别另外四种测试的鼠IgG2AK抗体。为了增强我们对这些发现的信心,使用了四个独立的检测系统进行这些测定。将抗独特型抗体鉴定为对多次输注鼠单克隆抗体免疫反应的主要类型,对未来单克隆抗体的研究工作具有重要意义。尽管有人提出人单克隆抗体可避免免疫反应,但我们的研究表明,如果进行多次输注,此类抗体仍可能诱导抗独特型抗体。

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