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Tumor immunotherapy across MHC barriers using allogeneic T-cell precursors
Authors: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
Institution:Department Immunology, Memorial Sloan-Kettering Cancer Center, 1275 York Avenue, New York, New York 10021, USA.
Abstract: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.
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