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Therapeutic effect of novel anti-human Fas antibody HFE7a on graft-versus-host disease model.

机译:新型抗人Fas抗体HFE7a对移植物抗宿主疾病模型的治疗作用。

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In order to evaluate anti-human Fas antibody, we have established a new graft-versus-host disease (GVHD) model wherein splenocytes of human Fas transgenic mice (hFas-TgM) were transferred to immune-deficient SCID mice. In this model, although host SCID cells are not activated by or responsive to graft hFas-TgM cells, graft hFas-TgM cells are activated by and responsive to host SCID cells and thus cause GVHD symptoms. SCID mice that received hFas-TgM splenocytes had increased human Fas-positive lymphocytes in lymph nodes, decreased in body weight, and developed skin diseases, including rash and alopecia. Administration of novel anti-human Fas antibody HFE7A, which did not induce liver toxicity after administration to mice, decreased the level of the human Fas-positive lymphocytes, blocked the decrease of body weight, and suppressed development of skin diseases in this model. These results indicate that induction of apoptosis to activated graft cells with nontoxic anti-Fas antibody could reduce GVHD symptoms. Copyright 2001 Academic Press.
机译:为了评估抗人Fas抗体,我们建立了一种新的移植物抗宿主病(GVHD)模型,其中将人Fas转基因小鼠(hFas-TgM)的脾细胞转移到免疫缺陷的SCID小鼠中。在此模型中,尽管宿主SCID细胞未被移植hFas-TgM细胞激活或未响应,但移植hFas-TgM细胞却被宿主SCID细胞激活并响应,因此引起了GVHD症状。接受hFas-TgM脾细胞的SCID小鼠的淋巴结中人类Fas阳性淋巴细胞增加,体重下降,并发展了包括皮疹和脱发在内的皮肤疾病。在该模型中,新型抗人Fas抗体HFE7A的施用在小鼠中不会引起肝毒性,降低了人类Fas阳性淋巴细胞的水平,阻止了体重的减少,并抑制了皮肤疾病的发展。这些结果表明用无毒抗Fas抗体诱导活化的移植细胞凋亡可以减轻GVHD症状。版权所有2001,学术出版社。

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