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小鼠节段性胰腺同种异体移植分泌转基因抗CD4单克隆抗体可促进长期存活。

Transgenic anti-CD4 monoclonal antibody secretion by mouse segmental pancreas allografts promotes long term survival.

作者信息

Mottram P L, Murray-Segal L J, Han W, Zhan Y, Brady J L, Lew A M

机构信息

University of Melbourne, Department of Surgery, and the Walter and Eliza Hall Institute for Medical Research, Royal Melbourne Hospital, Parkville, Australia.

出版信息

Transpl Immunol. 2000 Nov;8(3):203-9. doi: 10.1016/s0966-3274(00)00028-9.

Abstract

To compare the effectiveness of transgenic and systemic monoclonal antibody therapy for pancreas transplantation, vascularised segmental pancreas allografts from wild-type or transgenic pancreatic tissue that secreted monoclonal anti-CD4 were placed in CBA recipients in which diabetes had been induced chemically by streptozotocin (STZ, non-autoimmune diabetes). In untreated CBA recipients, wild-type BALB/c or C57BL/6 bml pancreas transplants were rejected in a mean survival time (MST) of 27 and 30 days, respectively. BALB/c and C57BL/6 graft survival improved when recipients were given a short course of T cell depleting monoclonal anti-CD4 antibody, (GK 1.5, 2 mg total on days -1, 0, 1, 2 with grafting on day 0) with MST +/- S.D. of 71 +/- 29 and 44 +/- 36 days, respectively. Thus, transient depletion of CD4 was effective in delaying pancreas allograft rejection in these strain combinations. The use of C57BL/6 bml mice transgenic for a rat anti-CD4 antibody (GK5 mice) as pancreas donors provided allografts that secreted sufficient anti-CD4 antibody to cause CD4 T cell depletion in the recipients (CD4 cells decreased from 30 to < 5% of small lymphocytes). This degree of depletion was not sustained and the CD4 recovery inversely correlated with graft survival. Mice with > 20% CD4 cells in the splenic lymphocyte population 4 weeks post-transplant rejected their grafts (3 of 10 mice). However, in 7 of 10 mice CD4 cells remained low (< 15%) and allografts survived for > 80 days. The GK5 allografts survived significantly longer than those from non-transgenic bml controls (MST 83 +/- 32 days, compared with 30 days, P < 0.0005). This survival time was similar to that of BALB/c allografts in CBA recipients treated with a high dose of anti-CD4 antibody. Thus, transgenic secretion of anti-CD4 antibody by the pancreas allograft was very effective in prolonging its survival.

摘要

为比较转基因和全身性单克隆抗体疗法对胰腺移植的有效性,将来自分泌单克隆抗CD4的野生型或转基因胰腺组织的血管化节段性胰腺同种异体移植物植入经链脲佐菌素(STZ,非自身免疫性糖尿病)化学诱导糖尿病的CBA受体中。在未经治疗的CBA受体中,野生型BALB/c或C57BL/6 bml胰腺移植的平均存活时间(MST)分别为27天和30天。当受体接受短疗程的T细胞耗竭单克隆抗CD4抗体(GK 1.5,移植当天0、-1、1、2天共2mg)时,BALB/c和C57BL/6移植物的存活情况有所改善,MST±标准差分别为71±29天和44±36天。因此,在这些品系组合中,CD4的短暂耗竭有效地延迟了胰腺同种异体移植的排斥反应。使用转大鼠抗CD4抗体(GK5小鼠)基因的C�7BL/6 bml小鼠作为胰腺供体,所提供的同种异体移植物分泌足够的抗CD4抗体,导致受体中的CD4 T细胞耗竭(CD4细胞从小淋巴细胞的30%降至<5%)。这种耗竭程度并不持久,CD4的恢复与移植物存活呈负相关。移植后4周脾淋巴细胞群体中CD4细胞>20%的小鼠排斥其移植物(10只小鼠中有3只)。然而,10只小鼠中有7只CD4细胞仍保持低水平(<15%),同种异体移植物存活超过80天。GK5同种异体移植物的存活时间明显长于非转基因bml对照(MST 83±32天,而对照为30天,P<0.0005)。这个存活时间与用高剂量抗CD4抗体治疗的CBA受体中BALB/c同种异体移植物的存活时间相似。因此,胰腺同种异体移植物转基因分泌抗CD4抗体在延长其存活时间方面非常有效。

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