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未经编辑的同种异体 iNKT 细胞在 MHC 错配的犬受体内具有延长的持久性。

Unedited allogeneic iNKT cells show extended persistence in MHC-mismatched canine recipients.

机构信息

Department of Pathobiology, School of Veterinary Medicine, University of Pennsylvania, Philadelphia, PA 19104, USA.

Department of Biomedical Sciences, School of Veterinary Medicine, University of Pennsylvania, Philadelphia, PA 19104, USA.

出版信息

Cell Rep Med. 2023 Oct 17;4(10):101241. doi: 10.1016/j.xcrm.2023.101241.

Abstract

Allogeneic invariant natural killer T cells (allo-iNKTs) induce clinical remission in patients with otherwise incurable cancers and COVID-19-related acute respiratory failure. However, their functionality is inconsistent among individuals, and they become rapidly undetectable after infusion, raising concerns over rejection and limited therapeutic potential. We validate a strategy to promote allo-iNKT persistence in dogs, an established large-animal model for novel cellular therapies. We identify donor-specific iNKT biomarkers of survival and sustained functionality, conserved in dogs and humans and retained upon chimeric antigen receptor engineering. We reason that infusing optimal allo-iNKTs enriched in these biomarkers will prolong their persistence without requiring MHC ablation, high-intensity chemotherapy, or cytokine supplementation. Optimal allo-iNKTs transferred into MHC-mismatched dogs remain detectable for at least 78 days, exhibiting sustained immunomodulatory effects. Our canine model will accelerate biomarker discovery of optimal allo-iNKT products, furthering application of MHC-unedited allo-iNKTs as a readily accessible universal platform to treat incurable conditions worldwide.

摘要

同种异体不变自然杀伤 T 细胞 (allo-iNKTs) 可诱导无法治愈的癌症和 COVID-19 相关急性呼吸衰竭患者临床缓解。然而,它们在个体之间的功能不一致,并且在输注后很快就无法检测到,这引起了对排斥和有限治疗潜力的担忧。我们验证了一种在狗中促进 allo-iNKT 持久性的策略,狗是一种用于新型细胞治疗的成熟大型动物模型。我们确定了供体特异性 iNKT 存活和持续功能的生物标志物,这些标志物在狗和人类中是保守的,并在嵌合抗原受体工程中保留。我们推断,输注富含这些生物标志物的最佳 allo-iNKT 将延长其持久性,而无需 MHC 消融、高强度化疗或细胞因子补充。输注到 MHC 不匹配的狗体内的最佳 allo-iNKT 可至少检测到 78 天,表现出持续的免疫调节作用。我们的犬模型将加速最佳 allo-iNKT 产品的生物标志物发现,进一步将未经 MHC 编辑的 allo-iNKT 作为一种易于获得的通用平台,在全球范围内用于治疗无法治愈的疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1403/10591065/24f57a5f88f5/fx1.jpg

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