首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Influence of dimethyl myleran on tolerance induction and immune function in major histocompatibility complex-haploidentical murine bone-marrow transplantation.
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Influence of dimethyl myleran on tolerance induction and immune function in major histocompatibility complex-haploidentical murine bone-marrow transplantation.

机译:二甲基髓磷脂对主要组织相容性复合物-单倍体鼠骨髓移植中耐受耐受和免疫功能的影响。

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摘要

To study murine major histocompatibility complex (MHC)-haploidentical bone-marrow transplantation (BMT), B6C3F1 mice (H-2b/k) underwent BMT using syngeneic [B6C3F1 (H-2b/k)], haploidentical [CB6F1 (H-2d/b)], or fully allogeneic [DBA/2 (H-2d)] donor mice. As pretreatment, dimethyl myleran (DMM), an alkylating agent that produces effective myeloablation but little immunosuppression, was used with total body irradiation (TBI). Four conditioning regimens were studied: TBI 800 rads (1 rad = 0.01 Gy), TBI 950 rads, TBI 800 rads plus DMM (0.2 mg per mouse), and TBI 950 rads plus DMM. Survival rates, chimerism, proliferative responses in mixed-lymphocyte culture, specific cell-mediated lympholysis, and in vivo plaque-forming cell responses to several antigens were compared. TBI 800 rads plus DMM was maximally effective. Haploidentical BMT was as successful in inducing long-term survival and immune and hematologic reconstitution as was syngeneic BMT. This regimen plus haploidentical BMT of T-cell-purged marrow yielded survivors tolerant of donor and recipient major histocompatibility complex. Such myeloablation and immunosuppression prevented graft rejection, immunodeficiency due to histoincompatibility, and damage to a radiosensitive cell population. A microenvironmental influence crucial to some antibody responses was thus revealed. Delayed recovery of antibody production after BMT in humans may be due partly to suboptimal myeloablation or excess irradiation.
机译:为了研究鼠类主要组织相容性复合物(MHC)-单倍体骨髓移植(BMT),使用同系[B6C3F1(H-2b / k)],单倍体[CB6F1(H-2d)对B6C3F1小鼠(H-2b / k)进行了BMT / b)]或完全同种异体[DBA / 2(H-2d)]供体小鼠。作为预处理,将二甲基myleran(DMM)(一种可产生有效的髓鞘消融但几乎没有免疫抑制作用的烷基化剂)与全身照射(TBI)一起使用。研究了四种调节方案:TBI 800 rads(1 rad = 0.01 Gy),TBI 950 rads,TBI 800 rads加DMM(每只小鼠0.2 mg)和TBI 950 rads加DMM。比较了存活率,嵌合体,混合淋巴细胞培养物中的增殖反应,特异性细胞介导的淋巴细胞溶解以及体内对几种抗原的噬菌斑形成细胞反应。 TBI 800 rads加DMM的效果最佳。单倍型BMT与同质BMT一样成功地诱导了长期生存以及免疫和血液学重建。这种方案加上T细胞净化的骨髓的单倍BMT产生了能够耐受供体和受体主要组织相容性复合物的幸存者。这种骨髓消融和免疫抑制作用防止了移植排斥,由于组织相容性引起的免疫缺陷和对放射敏感性细胞群的损害。因此揭示了对某些抗体应答至关重要的微环境影响。人类BMT后抗体生产的恢复延迟可能部分归因于次优的骨髓消融或过度照射。

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