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使用抗CD30单克隆抗体HeFi-1对人间变性大细胞淋巴瘤小鼠模型进行有效治疗并不需要激活Fc受体。

Effective therapy for a murine model of human anaplastic large-cell lymphoma with the anti-CD30 monoclonal antibody, HeFi-1, does not require activating Fc receptors.

作者信息

Zhang Meili, Yao Zhengsheng, Zhang Zhuo, Garmestani Kayhan, Goldman Carolyn K, Ravetch Jeffrey V, Janik John, Brechbiel Martin W, Waldmann Thomas A

机构信息

Metabolism Branch, Radiation Oncology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Blood. 2006 Jul 15;108(2):705-10. doi: 10.1182/blood-2005-11-4607. Epub 2006 Mar 21.

DOI:10.1182/blood-2005-11-4607
PMID:16551968
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1895489/
Abstract

CD30 is a member of the tumor necrosis factor receptor family. Overexpression of CD30 on some neoplasms versus its limited expression on normal tissues makes this receptor a promising target for antibody-based therapy. Anaplastic large-cell lymphoma (ALCL) represents a heterogeneous group of aggressive non-Hodgkin lymphomas characterized by the strong expression of CD30. We investigated the therapeutic efficacy of HeFi-1, a mouse IgG1 monoclonal antibody, which recognizes the ligand-binding site on CD30, and humanized anti-Tac antibody (daclizumab), which recognizes CD25, in a murine model of human ALCL. The ALCL model was established by intravenous injection of karpas299 cells into nonobese diabetic/severe combined immuno-deficient (SCID/NOD) wild-type or SCID/NOD Fc receptor common gamma chain-deficient (FcRgamma(-/-)) mice. HeFi-1, given at a dose of 100 microg weekly for 4 weeks, significantly prolonged survival of the ALCL-bearing SCID/NOD wild-type and SCID/NOD FcRgamma(-/-) mice (P < .01) as compared with the control groups. In vitro studies showed that HeFi-1 inhibited the proliferation of karpas299 cells, whereas daclizumab did not inhibit cell proliferation. We demonstrated that the expression of FcRgamma on polymorphonuclear leukocytes and monocytes was not required for HeFi-1-mediated tumor growth inhibition in vivo, although it was required for daclizumab.

摘要

CD30是肿瘤坏死因子受体家族的成员。与CD30在正常组织中的有限表达相比,其在某些肿瘤上的过表达使得该受体成为基于抗体治疗的一个有前景的靶点。间变性大细胞淋巴瘤(ALCL)是一组异质性侵袭性非霍奇金淋巴瘤,其特征是CD30的强表达。我们在人ALCL的小鼠模型中研究了HeFi-1(一种识别CD30上配体结合位点的小鼠IgG1单克隆抗体)和人源化抗Tac抗体(达利珠单抗,识别CD25)的治疗效果。通过将karpas299细胞静脉注射到非肥胖糖尿病/重症联合免疫缺陷(SCID/NOD)野生型或SCID/NOD Fc受体共同γ链缺陷(FcRγ(-/-))小鼠中建立ALCL模型。HeFi-1以每周100μg的剂量给药4周,与对照组相比,显著延长了携带ALCL的SCID/NOD野生型和SCID/NOD FcRγ(-/-)小鼠的生存期(P <.01)。体外研究表明,HeFi-1抑制karpas299细胞的增殖,而达利珠单抗不抑制细胞增殖。我们证明,体内HeFi-1介导的肿瘤生长抑制不需要多形核白细胞和单核细胞上FcRγ的表达,尽管达利珠单抗需要。