首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Targeting apoptosis to induce stable mixed hematopoietic chimerism and long-term allograft survival without myelosuppressive conditioning in mice.
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Targeting apoptosis to induce stable mixed hematopoietic chimerism and long-term allograft survival without myelosuppressive conditioning in mice.

机译:靶向细胞凋亡,诱导稳定的混合造血倒塌和长期同种异体移植存活,没有小鼠的骨髓抑制调理。

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摘要

Induction of mixed hematopoietic chimerism results in donor-specific immunological tolerance by apoptosis-mediated deletion of donor-reactive lymphocytes. A broad clinical application of this approach is currently hampered by limited predictability and toxicity of the available conditioning protocols. We developed a new therapeutic approach to induce mixed chimerism and tolerance by a direct pharmacological modulation of the intrinsic apoptosis pathway in peripheral T cells. The proapoptotic small-molecule Bcl-2 inhibitor ABT-737 promoted mixed chimerism induction and reversed the antitolerogenic effect of calcineurin inhibitors by boosting the critical role of the proapoptotic Bcl-2 factor Bim. A short conditioning protocol with ABT-737 in combination with costimulation blockade and low-dose cyclosporine A resulted in a complete deletion of peripheral donor-reactive lymphocytes and was sufficient to induce mixed chimerism and robust systemic tolerance across full major histocompatibility complex barriers, without myelosuppression and by using moderate doses of bone marrow cells. Thus, immunological tolerance can be achieved by direct modulation of the intrinsic apoptosis pathway in peripheral lymphocytes-a new approach to translate immunological tolerance into clinically applicable protocols.
机译:混合造血逆变诱导通过凋亡介导的供体反应性淋巴细胞缺失的供体特异性免疫耐受。这种方法的广泛临床应用目前通过可用护发方案的可预测性和毒性受到阻碍。我们开发了一种新的治疗方法,通过外周T细胞中的内在凋亡途径的直接药理学调节来诱导混合逆向和耐受性。促凋亡小分子Bcl-2抑制剂ABT-737促进混合逆变诱导,并通过促进促凋亡Bcl-2因子Bim的关键作用,逆转钙碱抑制剂的抗动素作用。具有ABT-737的短调节方案与共抑制阻断和低剂量环孢菌素A相结合,得到了外周供体反应性淋巴细胞的完全缺失,并且足以在没有髓抑制的情况下诱导整个主要的组织相容性复杂屏障的混合逆变和鲁棒的全身耐受性并使用中等剂量的骨髓细胞。因此,通过直接调节外周淋巴细胞中的内在凋亡途径来实现免疫耐受 - 一种将免疫耐受转化为临床适用的方案的新方法。

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