追求极致:艾哈迈达巴德迈向移植耐受的初始征程。
In pursuit of the ultimate: the initial Ahmedabad journey toward transplantation tolerance.
作者信息
Trivedi H L, Vanikar A V, Modi P R, Shah P R, Shah V R, Trivedi V B
机构信息
Department of Nephrology and Transplantation Medicine, Institute of Transplantation Sciences, Gulabben Rasiklal Doshi and Kamlaben Mafatlal Mehta Institute of Kidney Diseases and Research Centre, Ahmedabad, Gujarat, India.
出版信息
Transplant Proc. 2007 Apr;39(3):653-7. doi: 10.1016/j.transproceed.2007.01.064.
We designed a prospective clinical trial of 357 patients divided in two groups--treated (n = 201) and controls (n = 156)--to evaluate effects of donor hematopoietic stem cell transplantation (HSCT) with minimal nonmyeloablative conditioning for tolerance induction in living related donor renal allograft recipients. Conditioning included donor leukocyte infusions, target-specific irradiation, anti-T-cell antibody, cyclophosphamide, cyclosporine (CsA), followed by bone marrow (BM)-derived and peripheral blood stem cell (PBSC) infusion into thymus, liver, BM, and periphery, with mean total dose of 20 x 10(8) nucleated cells/kg body weight (BW) (mean CD34(+) count: 0.9%) pretransplantation. CsA (3 mg/kg BW/d) and prednisolone (10 mg/d) were used for immunosuppression. Azathioprine/mycophenolate mofetil were added in the event of an acute rejection episode. The controls underwent transplantation with three drug immunosuppression. With a mean follow-up of 21.5 months, the treated cohort showed better allograft function with mean serum creatinine (SCr), 1.42 +/- 0.31 mg% in contrast with the controls mean SCr, 1.61 +/- 0.52 mg% (P < .0001) at 23.9 months follow-up. One-year allograft/patient survival was 95%/96.7% versus 89%/93.4%, respectively. Peripheral blood chimerism by fluorescent in situ hybridization was 0.8% +/- 0.2% in the subset of treated patients with gender-mismatched donors. No graft-versus-host disease was noted. Nine patients with donor-specific cytotoxic alloantibodies pretransplantation showed a decrease in positivity to <15% post-HSCT and were transplanted safely. A transient rise in donor-specific cytotoxic alloantibodies was noted in 19 treated patients post-HSCT, 14 of whom returned to the transplantable range within 2 weeks and five required a desensitization protocol. "Prope" tolerance may be induced in living related donor renal transplantation across major histocompatability complex barriers using HSCT with minimal nonmyeloablative conditioning.
我们设计了一项针对357例患者的前瞻性临床试验,将其分为两组——治疗组(n = 201)和对照组(n = 156),以评估在活体亲属供肾移植受者中采用最小化非清髓性预处理的供体造血干细胞移植(HSCT)诱导免疫耐受的效果。预处理包括供体白细胞输注、靶向照射、抗T细胞抗体、环磷酰胺、环孢素(CsA),随后将骨髓(BM)来源的和外周血干细胞(PBSC)输注到胸腺、肝脏、BM和外周,移植前平均总剂量为20×10⁸有核细胞/千克体重(BW)(平均CD34⁺细胞计数:0.9%)。使用CsA(3毫克/千克BW/天)和泼尼松龙(10毫克/天)进行免疫抑制。在发生急性排斥反应时添加硫唑嘌呤/霉酚酸酯。对照组采用三联药物免疫抑制进行移植。平均随访21.5个月,治疗组的移植肾功能更好,平均血清肌酐(SCr)为1.42±0.31毫克%,而对照组在随访23.9个月时的平均SCr为1.61±0.52毫克%(P < 0.0001)。1年移植肾/患者生存率分别为95%/96.7%和89%/93.4%。在接受性别不匹配供体治疗的患者亚组中,通过荧光原位杂交检测的外周血嵌合率为0.8%±0.2%。未观察到移植物抗宿主病。9例移植前有供体特异性细胞毒性同种抗体的患者在HSCT后阳性率降至<15%并安全接受移植。19例接受治疗的患者在HSCT后出现供体特异性细胞毒性同种抗体短暂升高,其中14例在2周内恢复到可移植范围,5例需要脱敏方案。使用最小化非清髓性预处理的HSCT,可能在跨越主要组织相容性复合体屏障的活体亲属供肾移植中诱导“前体”耐受。
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