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噬菌体展示工程化T细胞受体作为研究肿瘤肽-MHC相互作用的工具

Phage Display Engineered T Cell Receptors as Tools for the Study of Tumor Peptide-MHC Interactions.

作者信息

Løset Geir Åge, Berntzen Gøril, Frigstad Terje, Pollmann Sylvie, Gunnarsen Kristin S, Sandlie Inger

机构信息

Nextera AS , Oslo , Norway ; Centre for Immune Regulation, Oslo University Hospital, University of Oslo , Oslo , Norway ; Department of Biosciences, University of Oslo , Oslo , Norway.

Nextera AS , Oslo , Norway.

出版信息

Front Oncol. 2015 Jan 12;4:378. doi: 10.3389/fonc.2014.00378. eCollection 2014.

Abstract

Cancer immunotherapy has finally come of age, demonstrated by recent progress in strategies that engage the endogenous adaptive immune response in tumor killing. Occasionally, significant and durable tumor regression has been achieved. A giant leap forward was the demonstration that the pre-existing polyclonal T cell repertoire could be re-directed by use of cloned T cell receptors (TCRs), to obtain a defined tumor-specific pool of T cells. However, the procedure must be performed with caution to avoid deleterious cross-reactivity. Here, the use of engineered soluble TCRs may represent a safer, yet powerful, alternative. There is also a need for deeper understanding of the processes that underlie antigen presentation in disease and homeostasis, how tumor-specific peptides are generated, and how epitope spreading evolves during tumor development. Due to its plasticity, the pivotal interaction where a TCR engages a peptide/MHC (pMHC) also requires closer attention. For this purpose, phage display as a tool to evolve cloned TCRs represents an attractive avenue to generate suitable reagents allowing the study of defined pMHC presentation, TCR engagement, as well as for the discovery of novel therapeutic leads. Here, we highlight important aspects of the current status in this field.

摘要

癌症免疫疗法终于走向成熟,这一点从最近在肿瘤杀伤中激活内源性适应性免疫反应的策略所取得的进展中得到了证明。偶尔也会实现显著且持久的肿瘤消退。一个巨大的飞跃是证明了可以通过使用克隆的T细胞受体(TCR)来重新定向预先存在的多克隆T细胞库,以获得特定的肿瘤特异性T细胞池。然而,必须谨慎进行该操作以避免有害的交叉反应。在此,使用工程化可溶性TCR可能是一种更安全但同样强大的替代方法。还需要更深入地了解疾病和体内平衡中抗原呈递的基础过程、肿瘤特异性肽是如何产生的,以及在肿瘤发展过程中表位扩展是如何演变的。由于其可塑性,TCR与肽/MHC(pMHC)之间的关键相互作用也需要更密切的关注。为此,噬菌体展示作为一种进化克隆TCR的工具,是生成合适试剂的一个有吸引力的途径,这些试剂可用于研究特定的pMHC呈递、TCR结合,以及发现新的治疗线索。在此,我们强调该领域当前状况的重要方面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c513/4290511/4f1a8d77cb33/fonc-04-00378-g001.jpg

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