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免疫缺陷小鼠脾脏中人类B细胞的生长与分化

Human B cell growth and differentiation in the spleen of immunodeficient mice.

作者信息

Depraetere S, Verhoye L, Leclercq G, Leroux-Roels G

机构信息

Innogenetics N.V., Ghent-Zwijnaarde, Belgium.

出版信息

J Immunol. 2001 Mar 1;166(5):2929-36. doi: 10.4049/jimmunol.166.5.2929.

DOI:10.4049/jimmunol.166.5.2929
PMID:11207241
Abstract

Human mAbs (HumAbs) have therapeutic potential against infectious diseases and cancer. Heretofore, their production has been hampered by ethical constraints preventing the isolation of Ag-specific activated B cells by in vivo immunization. Alternatively, severe combined immune deficient (SCID) mice, transplanted i.p. with human (Hu)-PBLs, allow the in vivo stimulation of human Ab responses without the usual constraints. Unfortunately, human B cells only represent a minor fraction of the surviving graft, they are scattered all over the animal body, and thus are hard to isolate for subsequent immortalization procedures. To prevent this dispersion and to provide the human B cells with a niche for expansion and maturation, SCID mice were engrafted with Hu-PBL directly into the spleen. Simultaneously endogenous murine NK cell activity was depleted by treatment with an anti-mouse IL-2 receptor beta-chain Ab. During engraftment, human B lymphocytes became activated, divided intensely, and differentiated into plasmacytoid cells. In vivo exposure to a recall Ag after cell transfer induced expansion of Ag-specific B cell clones. One week after inoculation, human B cells were abundant in the spleen and could easily be recovered for fusion with a heteromyeloma line. This resulted in the formation of stable hybridoma cell lines that secreted Ag-specific HumAbs. Thus transplantation of human lymphoid cells in the spleens of immune deficient mice represents a model for the study of human T cell-dependent B cell activation and proves to be an excellent tool for the successful production of HumAbs.

摘要

人源单克隆抗体(HumAbs)对传染病和癌症具有治疗潜力。在此之前,其生产受到伦理限制的阻碍,这种限制使得无法通过体内免疫来分离抗原特异性活化B细胞。另外,严重联合免疫缺陷(SCID)小鼠经腹腔移植人外周血淋巴细胞(Hu-PBLs)后,可在无常规限制的情况下在体内刺激人源抗体反应。不幸的是,人B细胞仅占存活移植物的一小部分,它们分散在动物全身,因此很难分离出来用于后续的永生化程序。为防止这种分散,并为人类B细胞提供一个扩增和成熟的微环境,将Hu-PBL直接植入SCID小鼠的脾脏。同时,用抗小鼠IL-2受体β链抗体处理来耗尽内源性小鼠NK细胞活性。在植入过程中,人B淋巴细胞被激活,强烈分裂,并分化为浆细胞样细胞。细胞转移后在体内接触回忆抗原可诱导抗原特异性B细胞克隆的扩增。接种一周后,脾脏中富含人B细胞,可轻松回收用于与异源骨髓瘤细胞系融合。这导致形成了分泌抗原特异性HumAbs的稳定杂交瘤细胞系。因此,在免疫缺陷小鼠脾脏中移植人淋巴细胞代表了一种研究人T细胞依赖性B细胞活化的模型,并被证明是成功生产HumAbs的一种优秀工具。

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