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首页> 外文期刊>Tissue antigens. >Adoptive immunotherapy for cancer: the next generation of gene-engineered immune cells.
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Adoptive immunotherapy for cancer: the next generation of gene-engineered immune cells.

机译:癌症的过继免疫疗法:下一代基因工程免疫细胞。

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摘要

Adoptive cellular immunotherapy involving transfer of tumor-reactive T cells has shown some notable antitumor responses in a minority of cancer patients. In particular, transfer of tumor-infiltrating lymphocytes has resulted in long-term objective responses in patients with advanced melanoma. However, the inability to isolate sufficient numbers of tumor-specific T cells from most malignancies has restricted the broad utility of this approach. An emerging approach to circumvent this limitation involves the genetic modification of effector cells with T cell receptor (TCR) transgenes or chimeric single-chain variable fragment (scFv) receptors that can specifically redirect T cells to tumor. There has been much progress in the design of TCR and scFv receptors to enhance the antigen-specific activation of effector cells and their trafficking and persistence in vivo. Considerable effort has been directed toward improving the safety of this approach and reducing the immunogenicity of the receptor. This review discusses the latest developments in the field of adoptive immunotherapy using genetically modified immune cells that have been transduced with either TCR or scFv receptor transgenes and used in preclinical and clinical settings as anticancer agents.
机译:在少数癌症患者中,涉及转移肿瘤反应性T细胞的过继细胞免疫疗法已显示出一些显着的抗肿瘤反应。特别是,肿瘤浸润淋巴细胞的转移已导致晚期黑色素瘤患者产生长期的客观反应。然而,无法从大多数恶性肿瘤中分离出足够数量的肿瘤特异性T细胞限制了该方法的广泛应用。克服这种局限性的新兴方法涉及用T细胞受体(TCR)转基因或嵌合单链可变片段(scFv)受体对效应细胞进行遗传修饰,该受体可以特异性地将T细胞重定向至肿瘤。在TCR和scFv受体的设计中,在增强效应细胞的抗原特异性活化及其在体内的转运和持久性方面,已经取得了很大进展。已经进行了相当大的努力以提高该方法的安全性并降低受体的免疫原性。这篇综述讨论了采用基因修饰的免疫细胞在过继免疫疗法领域的最新进展,这些免疫细胞已被TCR或scFv受体转基因转导,并在临床前和临床中用作抗癌剂。

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