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首页> 外文期刊>Xenotransplantation >Xenotransplantation of purified pre-natal porcine beta cells in mice normalizes diabetes when a short anti-CD4-CD8 antibody treatment is combined with transient insulin injections.
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Xenotransplantation of purified pre-natal porcine beta cells in mice normalizes diabetes when a short anti-CD4-CD8 antibody treatment is combined with transient insulin injections.

机译:当短暂的抗CD4-CD8抗体治疗与短暂胰岛素注射结合时,小鼠中纯化的产前猪β细胞的异种移植可使糖尿病正常化。

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BACKGROUND: Pre-natal porcine endocrine islet cell grafts were recently shown to contain immature beta cells with a marked potential for growth and differentiation following transplantation, and hence for a progressive and long-term correction of diabetes in immune-incompetent mice. The present study investigates whether these grafts are also capable of correcting hyperglycemia in immune-competent mice receiving a short treatment with anti-CD4-CD8 antibodies. METHODS: Pure endocrine islet cell grafts with 0.5 to 1.0 million beta cells were prepared from pre-natal pigs and transplanted under the kidney capsule of alloxan-diabetic CBA/Ca mice. Survival, growth and function of implanted beta cells were followed by measuring plasma porcine C-peptide and glucose, and graft insulin content at start and at post-transplant (PT) week 35. The effect was studied of a 5-day treatment with non-depleting anti-CD4 YTS177 and depleting anti-CD8 YTS169 antibody, either without or with transient insulin injections. RESULTS: Without antibody treatment, all graft recipients remained porcine C-peptide negative and died. Antibody treatment decreased CD4-expression and percentage CD8 cells for 10 and 18 weeks respectively. It resulted in a 30 week-survival of nine out of 14 graft recipients; all nine had progressively become C-peptide positive but only one proceeded to normoglycemia. When antibody treatment was combined with transient insulin injections, 11 out of 14 graft recipients survived long-term, eight became C-peptide positive and six were normoglycemic at PT week 30. In both groups, surviving recipients exhibited a graft insulin content that was 6- to 9-fold higher than at implantation. CONCLUSIONS: Pre-natal porcine beta cells grow and differentiate when transplanted in diabetic immune-competent mice that have been transiently immune suppressed with anti-CD4 and anti-CD8 monoclonal antibodies. They develop metabolic control when recipients are also transiently treated with insulin injections.
机译:背景:最近显示,产前猪内分泌胰岛细胞移植物中含有未成熟的β细胞,在移植后具有明显的生长和分化潜能,因此可以逐步和长期纠正免疫功能低下的小鼠中的糖尿病。本研究调查这些移植物是否还能够纠正接受抗CD4-CD8抗体短期治疗的具有免疫能力的小鼠的高血糖症。方法:从产前猪中制备具有0.5至100万个β细胞的纯内分泌胰岛细胞移植物,并将其移植到四氧嘧啶糖尿病CBA / Ca小鼠的肾囊下。在测量第35周开始和移植后(PT)的血浆猪C肽和葡萄糖以及移植胰岛素含量后,观察植入的β细胞的存活,生长和功能。在没有或有短暂胰岛素注射的情况下使抗CD4 YTS177抗体和抗CD8 YTS169抗体消耗。结果:未经抗体处理,所有移植受体均保持猪C肽阴性并死亡。抗体治疗分别降低了10周和18周的CD4表达和CD8细胞百分比。结果导致14个移植受者中有9个接受了30周的生存;所有九种已逐渐变为C肽阳性,但只有一种进展为血糖正常。当抗体治疗与短暂胰岛素注射结合时,14位移植受者中的11位可以长期存活,八位成为C肽阳性,六位在PT周30降糖。两组中,存活的接受者的移植胰岛素含量为6 -比植入时高9倍。结论:将产前猪β细胞移植到已经被抗CD4和抗CD8单克隆抗体暂时免疫抑制的糖尿病免疫小鼠中后,它们会生长并分化。当接受者也接受胰岛素注射短暂治疗时,它们就可以控制新陈代谢。

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