Research and Development, Bellicum Pharmaceuticals, 2710 Reed Road, Suite 160, Houston, TX 77030, USA.
Research and Development, Bellicum Pharmaceuticals, 2710 Reed Road, Suite 160, Houston, TX 77030, USA.
Mol Ther. 2021 Feb 3;29(2):718-733. doi: 10.1016/j.ymthe.2020.10.019. Epub 2020 Oct 22.
Allogeneic, off-the-shelf (OTS) chimeric antigen receptor (CAR) cell therapies have the potential to reduce manufacturing costs and variability while providing broader accessibility to cancer patients and those with other diseases. However, host-versus-graft reactivity can limit the durability and efficacy of OTS cell therapies requiring new strategies to evade adaptive and innate-immune responses. Human herpes virus-8 (HHV8) maintains infection, in part, by evading host T and natural killer (NK) cell attack. The viral K3 gene encodes a membrane-tethered E3 ubiquitin ligase that discretely targets major histocompatibility complex (MHC) class I components, whereas K5 encodes a similar E3 ligase with broader specificity, including MHC-II and the MHC-like MHC class I polypeptide-related sequence A (MIC-A)- and sequence B (MIC-B)-activating ligands of NK cells. We created γ-retroviruses encoding K3 and/or K5 transgenes that efficiently transduce primary human T cells. Expression of K3 or K5 resulted in dramatic downregulation of MHC-IA (human leukocyte antigen [HLA]-A, -B, and -C) and MHC class II (HLA-DR) cell-surface expression. K3 expression was sufficient for T cells to resist exogenously loaded peptide-MHC-specific cytotoxicity, as well as recognition in one-way allogeneic mixed lymphocyte reactions. Further, in immunodeficient mice engrafted with allogeneic T cells, K3-transduced T cells selectively expanded in vivo. Ectopic K5 expression in MHC class I, MIC-A/B K562 cells also reduced targeting by primary NK cells. Coexpression of K3 in prostate stem cell antigen (PSCA)-directed, inducible MyD88/CD40 (iMC)-enhanced CAR-T cells did not impact cytotoxicity, T cell growth, or cytokine production against HPAC pancreatic tumor target cells, whereas K5-expressing cells showed a modest reduction in interleukin (IL)-2 production without effect on cytotoxicity. Together, these results support application of these E3 ligases to advance development of OTS CAR-T cell products.
同种异体、现成的(OTS)嵌合抗原受体(CAR)细胞疗法有可能降低制造成本和变异性,同时为癌症患者和其他疾病患者提供更广泛的治疗机会。然而,宿主对移植物的反应性可能会限制 OTS 细胞疗法的持久性和疗效,这需要新的策略来逃避适应性和固有免疫反应。人类疱疹病毒 8(HHV8)通过逃避宿主 T 细胞和自然杀伤(NK)细胞的攻击,部分维持感染。病毒的 K3 基因编码一种膜结合的 E3 泛素连接酶,可特异性靶向主要组织相容性复合体(MHC)I 类成分,而 K5 编码一种具有更广泛特异性的类似 E3 连接酶,包括 MHC-II 和 MHC 样 MHC Ⅰ类多肽相关序列 A(MIC-A)和序列 B(MIC-B)激活 NK 细胞的配体。我们创建了编码 K3 和/或 K5 转基因的γ逆转录病毒,这些病毒可有效地转导原代人 T 细胞。K3 或 K5 的表达导致 MHC-I(人白细胞抗原 [HLA]-A、-B 和 -C)和 MHC Ⅱ类(HLA-DR)细胞表面表达的显著下调。K3 的表达足以使 T 细胞抵抗外源性加载的肽-MHC 特异性细胞毒性,以及在单向同种异体混合淋巴细胞反应中的识别。此外,在植入同种异体 T 细胞的免疫缺陷小鼠中,K3 转导的 T 细胞在体内选择性扩增。MHC I 类、MIC-A/B K562 细胞中 K5 的异位表达也降低了初级 NK 细胞的靶向性。在前列腺干细胞抗原(PSCA)定向的、诱导型 MyD88/CD40(iMC)增强的 CAR-T 细胞中共同表达 K3 并不影响针对 HPAC 胰腺肿瘤靶细胞的细胞毒性、T 细胞生长或细胞因子产生,而表达 K5 的细胞则表现出白细胞介素(IL)-2 产生的适度减少,而对细胞毒性没有影响。总之,这些结果支持应用这些 E3 连接酶来推进 OTS CAR-T 细胞产品的开发。
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