CAR-T细胞双重靶向CD123和NKG2DL以根除AML细胞并选择性靶向免疫抑制细胞。

IF 7.2 2区 医学
Oncoimmunology Pub Date : 2023-08-26 eCollection Date: 2023-01-01 DOI:10.1080/2162402X.2023.2248826
Xin Jin, Danni Xie, Rui Sun, Wenyi Lu, Xia Xiao, Yibing Yu, Juanxia Meng, Mingfeng Zhao
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引用次数: 1

摘要

嵌合抗原受体(CAR)-T细胞在治疗急性粒细胞白血病(AML)的早期临床研究中尚未取得显著进展。这种缺乏进展的部分原因可能是AML的免疫抑制微环境,如单核细胞样骨髓来源的抑制细胞(M-MDSCs)和选择性活化的巨噬细胞(M2细胞),它们可以抑制CAR-T细胞的抗肿瘤活性。此外,AML细胞通常是异质性的,单靶CAR-T细胞可能无法消除所有AML细胞,导致疾病复发。CD123和NKG2D配体(NKG2DL)是CAR-T治疗AML的常用靶点,并且M-MDSCs和M2细胞表达这两种抗原。我们通过各种结构优化筛选开发了靶向CD123和NKG2DL的双靶向CAR-T(123NL CAR-T)细胞。我们的研究表明,123NL CAR-T细胞可以根除AML细胞并选择性靶向免疫抑制细胞。结合CD34和CD20抗原的靶向表位的高度紧凑的标记物/自杀基因RQR8也结合在CAR结构的前面。利妥昔单抗与RQR8的结合导致123NL CAR-T细胞的消除并停止其细胞毒性。总之,我们成功开发了123NL CAR-T细胞对肿瘤细胞和免疫抑制细胞的双重作用,可以避免靶点逃逸并抵抗免疫抑制微环境的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

CAR-T cells dual-target CD123 and NKG2DLs to eradicate AML cells and selectively target immunosuppressive cells.

CAR-T cells dual-target CD123 and NKG2DLs to eradicate AML cells and selectively target immunosuppressive cells.

CAR-T cells dual-target CD123 and NKG2DLs to eradicate AML cells and selectively target immunosuppressive cells.

CAR-T cells dual-target CD123 and NKG2DLs to eradicate AML cells and selectively target immunosuppressive cells.

Chimeric antigen receptor (CAR)-T cells have not made significant progress in the treatment of acute myeloid leukemia (AML) in earlyclinical studies. This lack of progress could be attributed in part to the immunosuppressive microenvironment of AML, such as monocyte-like myeloid-derived suppressor cells (M-MDSCs) and alternatively activated macrophages (M2 cells), which can inhibit the antitumor activity of CAR-T cells. Furthermore, AML cells are usually heterogeneous, and single-target CAR-T cells may not be able to eliminate all AML cells, leading to disease relapse. CD123 and NKG2D ligands (NKG2DLs) are commonly used targets for CAR-T therapy of AML, and M-MDSCs and M2 cells express both antigens. We developed dual-targeted CAR-T (123NL CAR-T) cells targeting CD123 and NKG2DL by various structural optimization screens. Our study reveals that 123NL CAR-T cells eradicate AML cells and selectively target immunosuppressive cells. A highly compact marker/suicide gene, RQR8, which binds targeting epitopes of CD34 and CD20 antigens, was also incorporated in front of the CAR structure. The binding of Rituximab to RQR8 leads to the elimination of 123NL CAR-T cells and cessation of their cytotoxicity. In conclusion, we successfully developed dual effects of 123NL CAR-T cells against tumor cells and immunosuppressive cells, which can avoid target escape and resist the effects of immunosuppressive microenvironment.

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来源期刊
Oncoimmunology
Oncoimmunology ONCOLOGY-IMMUNOLOGY
CiteScore
12.80
自引率
2.80%
发文量
276
期刊介绍: Tumor immunology explores the natural and therapy-induced recognition of cancers, along with the complex interplay between oncogenesis, inflammation, and immunosurveillance. In response to recent advancements, a new journal, OncoImmunology, is being launched to specifically address tumor immunology. The field has seen significant progress with the clinical demonstration and FDA approval of anticancer immunotherapies. There's also growing evidence suggesting that many current chemotherapeutic agents rely on immune effectors for their efficacy. While oncologists have historically utilized chemotherapeutic and radiotherapeutic regimens successfully, they may have unwittingly leveraged the immune system's ability to recognize tumor-specific antigens and control cancer growth. Consequently, immunological biomarkers are increasingly crucial for cancer prognosis and predicting chemotherapy efficacy. There's strong support for combining conventional anticancer therapies with immunotherapies. OncoImmunology will welcome high-profile submissions spanning fundamental, translational, and clinical aspects of tumor immunology, including solid and hematological cancers, inflammation, and both innate and acquired immune responses.
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