Zakrzewski Johannes L, Suh David, Markley John C, Smith Odette M, King Christopher, Goldberg Gabrielle L, Jenq Robert, Holland Amanda M, Grubin Jeremy, Cabrera-Perez Javier, Brentjens Renier J, Lu Sydney X, Rizzuto Gabrielle, Sant'Angelo Derek B, Riviere Isabelle, Sadelain Michel, Heller Glenn, Zúñiga-Pflücker Juan Carlos, Lu Chen, van den Brink Marcel R M
Department Immunology, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, New York, New York 10021, USA.
Nat Biotechnol. 2008 Apr;26(4):453-61. doi: 10.1038/nbt1395. Epub 2008 Mar 30.
We present a strategy for adoptive immunotherapy using T-lineage committed lymphoid precursor cells generated by Notch1-based culture. We found that allogeneic T-cell precursors can be transferred to irradiated individuals irrespective of major histocompatibility complex (MHC) disparities and give rise to host-MHC restricted and host-tolerant functional allogeneic T cells, improving survival in irradiated recipients as well as enhancing anti-tumor responses. T-cell precursors transduced to express a chimeric receptor targeting hCD19 resulted in significant additional anti-tumor activity, demonstrating the feasibility of genetic engineering of these cells. We conclude that ex vivo generated MHC-disparate T-cell precursors from any donor can be used universally for 'off-the-shelf' immunotherapy, and can be further enhanced by genetic engineering for targeted immunotherapy.
我们提出了一种采用基于Notch1培养产生的T系定向淋巴前体细胞进行过继性免疫治疗的策略。我们发现,同种异体T细胞前体可转移至经辐照的个体,而不论主要组织相容性复合体(MHC)差异如何,并产生宿主MHC限制且宿主耐受的功能性同种异体T细胞,从而提高经辐照受体的存活率并增强抗肿瘤反应。转导以表达靶向hCD19的嵌合受体的T细胞前体产生了显著的额外抗肿瘤活性,证明了对这些细胞进行基因工程改造的可行性。我们得出结论,从任何供体体外产生的MHC不相合T细胞前体可普遍用于“现成可用”的免疫治疗,并且可通过基因工程进一步增强以进行靶向免疫治疗。
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