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Rejection of an MHC class II negative tumor following induction of murine syngeneic graft-versus-host disease.

机译:在诱导鼠同胞移植物与宿主疾病之后,抑制MHC类II阴性肿瘤。

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Cyclosporin A (CsA) has been used clinically to induce graft-versus-host disease following autologous bone marrow transplantation in an attempt to destroy residual leukemia cells and reduce relapse. To analyze the antitumor potential of murine syngeneic graft-versus-host disease (SGVHD), C3H/HeN mice were lethally irradiated, reconstituted with T cell-depleted syngeneic bone marrow (ATBM) and treated with CsA for 21 days. Graft-versus-leukemia activity was assessed by challenging groups of olive oil-treated control ATBM (OO-ATBM) and CsA-treated (CsA-ATBM) mice 1 week after CsA therapy with graded doses of the syngeneic 38C13 B cell lymphoma. Following CsA treatment, up to 70% of CsA-ATBM developed SGVHD and more than 70% of the animals injected with 500 38C13 cells exhibited long-term survival (MST >80 days). In contrast, none of the OO-ATBM control mice developed SGVHD, and more than 75% of these mice died following injection of 500 38C13 tumor cells (MST = 34 days). Long-term survivors were not resistant to tumor challenge suggesting that tumor-specific immunity did not develop. Finally, class II negative 38C13 cells cultured in IL-4 or IL-10 were not inducible for MHC class II molecules, demonstrating that class II-independent antitumor mechanisms exist in SGVHD mice.
机译:临床上使用环孢菌素A(CSA)临床上诱导自体骨髓移植后诱导移植物与宿主疾病,以破坏残留的白血病细胞并减少复发。为了分析鼠同胞移植物与宿主疾病(SGVHD)的抗肿瘤潜力,致死地照射C3H /母鸡小鼠,用T细胞耗尽的同工骨髓(ATBM)重构,并用CSA处理21天。通过在CSA治疗后1周与Syngeneic 38C13b细胞淋巴瘤的渐变剂量持续剂量的橄榄油处理的对照ATBM(OO-ATBM)和CSA治疗(CSA-ATBM)小鼠组进行橄榄油处理的对照组(CSA-ATBM)小鼠的群体,评估移植物与白血病活性。在CSA治疗之后,高达70%的CSA-ATBM开发了SGVHD,超过70%的动物注射了5008C13细胞,表现出长期存活(MST> 80天)。相反,OO-ATBM对照小鼠均未开发SGVHD,并且超过75%的这些小鼠在注射5008C13肿瘤细胞(MST = 34天)后死亡。长期幸存者对肿瘤攻击不具有抗性,表明肿瘤特异性免疫没有发展。最后,在IL-4或IL-10中培养的II类阴性38C13细胞对MHC II类分子诱导,证明了在SGVHD小鼠中存在II独立的抗肿瘤机制。

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