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CD19嵌合抗原受体不变自然杀伤T细胞激活自然杀伤细胞并降低同种异体反应性。

CD19-chimeric antigen receptor-invariant natural killer T cells transactivate NK cells and reduce alloreactivity.

作者信息

Wesle Anton, Moraes Ribeiro Emmanuelle, Schairer Rebekka, Keppeler Hildegard, Korkmaz Fulya, Radszuweit Pia, Bieber Kristin, Lengerke Claudia, Schneidawind Dominik, Schneidawind Corina

机构信息

Department of Hematology, Oncology, Clinical Immunology and Rheumatology, University Hospital Tübingen, Tübingen, Germany.

Department of Hematology, Oncology, Clinical Immunology and Rheumatology, University Hospital Tübingen, Tübingen, Germany; Department of Medical Oncology and Hematology, University Hospital Zürich, Zürich, Switzerland.

出版信息

Cytotherapy. 2025 Jan;27(1):7-15. doi: 10.1016/j.jcyt.2024.08.004. Epub 2024 Aug 10.

Abstract

Invariant natural killer T (iNKT) cells are a small fraction of T lymphocytes with strong cytotoxic and immunoregulatory properties. We previously showed that human culture-expanded iNKT cells prevent alloreactivity and lyse primary leukemia blasts. Here, iNKT cells have several advantages over T cells based on their immunoregulatory capabilities. Since chimeric antigen receptors (CARs) increase the benefit of immune effector cells, they play a crucial role in improvement of cytotoxic abilities of novel cellular therapeutics such as iNKT cells. In the present study, we investigated transactivation of NK cells and prevention of alloreactivity through iNKT cells transduced with a CD19-directed CAR. iNKT cells were isolated by magnetic cell separation from peripheral blood mononuclear cells and transduced with a CD19-CAR retrovirus. Transduction efficiency, purity and cell subsets were measured by flow cytometry. Transactivation and cytotoxicity assays have been established to investigate the ability of CD19-CAR-iNKT cells to transactivate primary NK cells. A mixed lymphocyte reaction (MLR) was performed to explore the inhibition of alloreactive CD3+ T cells by CD19-CAR-iNKT cells. CD19-CAR-iNKT cells are able to transactivate NK cells independent of cell contact: The expression of activation marker CD69 was significantly increased and also production of the proinflammatory cytokine interferon-gamma was higher in NK cells pretreated with CD19-CAR-iNKT cells. Consequently, the cytotoxic activity of such NK cells was significantly increased being able to lyse leukemia cells more effectively than without prior transactivation. Adding CD19-CAR-iNKT cells to an MLR resulted in a decreased expression of the T cell activation marker CD25 on alloreactive CD3+ T lymphocytes stimulated with HLA mismatched dendritic cells. Also, the proliferation of alloreactive CD3+ T lymphocytes was significantly reduced in this setting. We demonstrate that CD19-CAR-iNKT cells keep their immunoregulatory properties despite transduction with a CAR making them an attractive effector cell population for application after allogeneic hematopoietic cell transplantation. By transactivating NK cells, increasing their cytotoxic activity and suppressing alloreactive T cells, they might further improve outcomes through prevention of both relapse and graft-versus-host disease.

摘要

不变自然杀伤T(iNKT)细胞是一小部分具有强大细胞毒性和免疫调节特性的T淋巴细胞。我们之前表明,人类培养扩增的iNKT细胞可预防同种异体反应并裂解原发性白血病母细胞。在此,基于其免疫调节能力,iNKT细胞相对于T细胞具有若干优势。由于嵌合抗原受体(CAR)增加了免疫效应细胞的益处,它们在改善诸如iNKT细胞等新型细胞疗法的细胞毒性能力方面发挥着关键作用。在本研究中,我们研究了通过用CD19导向的CAR转导的iNKT细胞对NK细胞的反式激活以及对同种异体反应的预防。通过磁珠细胞分选从外周血单个核细胞中分离iNKT细胞,并用CD19-CAR逆转录病毒进行转导。通过流式细胞术测量转导效率、纯度和细胞亚群。已建立反式激活和细胞毒性测定以研究CD19-CAR-iNKT细胞反式激活原发性NK细胞的能力。进行混合淋巴细胞反应(MLR)以探索CD19-CAR-iNKT细胞对同种异体反应性CD3 + T细胞的抑制作用。CD19-CAR-iNKT细胞能够独立于细胞接触反式激活NK细胞:在用CD19-CAR-iNKT细胞预处理的NK细胞中,激活标志物CD69的表达显著增加,促炎细胞因子干扰素-γ的产生也更高。因此,此类NK细胞的细胞毒性活性显著增加,能够比未预先反式激活时更有效地裂解白血病细胞。将CD19-CAR-iNKT细胞添加到MLR中导致在用HLA不匹配的树突状细胞刺激的同种异体反应性CD3 + T淋巴细胞上T细胞激活标志物CD25的表达降低。此外,在这种情况下,同种异体反应性CD3 + T淋巴细胞的增殖显著减少。我们证明CD19-CAR-iNKT细胞尽管用CAR进行了转导,但仍保持其免疫调节特性,使其成为异基因造血细胞移植后应用的有吸引力的效应细胞群体。通过反式激活NK细胞、增加其细胞毒性活性并抑制同种异体反应性T细胞,它们可能通过预防复发和移植物抗宿主病进一步改善治疗结果。

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