将 NK-92 细胞开发为有效的通用现成细胞疗法所面临的挑战。

Zhiyuan Niu,Mengjun Wang,Yangchun Yan,Xinru Jin,Linwei Ning,Bingqian Xu,Yanfeng Wang,Yuekai Hao,Zhixia Luo,Changjiang Guo,Lingtong Zhi,Wuling Zhu
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摘要

基于人源 NK-92 细胞的 CAR-NK 疗法表现出不一致性,总体疗效不理想,而且癌症患者体内的 CAR-NK92 细胞会被迅速清除。分析表明,虽然健康人(n = 10)体内原有的 IgM 能强烈识别 NK-92 和 CAR-NK92 细胞,但 IgG 和 IgE 却不能。然而,只有一部分癌症患者(3/8)对这些细胞表现出强烈的 IgM 识别,还有一部分患者(2/8)表现出预先存在的 IgG 识别。这些结果表明,NK-92 和 CAR-NK92 细胞与已有的人类抗体之间存在天然免疫反应。此外,CAR-NK92 细胞注入后的 IgG 和 IgM 识别增强也证明了该疗法的免疫原性。我们还证实,补体抑制剂会降低健康血浆对这些细胞的细胞毒性,这表明抗体可通过补体依赖性细胞毒性促进 CAR-NK92 细胞的快速清除。鉴于 NK-92 细胞缺乏已知的 IgG 和 IgM 受体,识别和修改 NK-92 和 CAR-NK92 细胞上这些 Abs 的识别靶点可能会改善临床疗效。此外,我们发现 NK-92 细胞上 NKG2D 受体的第 72 个氨基酸是丙氨酸。以前的研究表明,人类 NK 细胞上的 NKG2D 第 72 个氨基酸存在多态性,与 NKG2D72Ala 相比,NKG2D72Thr 对 NK 细胞的激活效果更好。我们通过体外细胞毒性实验证实了这一结论也适用于 NK-92 细胞。因此,降低 CAR-NK92 的免疫活性和免疫原性以及将携带 NKG2D72Ala 的 NK-92 直接转换为 NKG2D72Thr 是实现 NK-92 细胞成为合格的通用现成细胞疗法的迫切挑战。
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Challenges in the Development of NK-92 Cells as an Effective Universal Off-the-Shelf Cellular Therapeutic.
The human-derived NK-92 cell-based CAR-NK therapy exhibits inconsistency with overall suboptimal efficacy and rapid in vivo clearance of CAR-NK92 cells in cancer patients. Analysis indicates that although pre-existing IgM in healthy individuals (n = 10) strongly recognizes both NK-92 and CAR-NK92 cells, IgG and IgE do not. However, only a subset of cancer patients (3/8) exhibit strong IgM recognition of these cells, with some (2/8) showing pre-existing IgG recognition. These results suggest a natural immunoreactivity between NK-92 and CAR-NK92 cells and pre-existing human Abs. Furthermore, the therapy's immunogenicity is evidenced by enhanced IgG and IgM recognition postinfusion of CAR-NK92 cells. We also confirmed that healthy plasma's cytotoxicity toward these cells is reduced by complement inhibitors, suggesting that Abs may facilitate the rapid clearance of CAR-NK92 cells through complement-dependent cytotoxicity. Given that NK-92 cells lack known receptors for IgG and IgM, identifying and modifying the recognition targets for these Abs on NK-92 and CAR-NK92 cells may improve clinical outcomes. Moreover, we discovered that the 72nd amino acid of the NKG2D receptor on NK-92 cells is alanine. Previous studies have demonstrated polymorphism at the 72nd amino acid of the NKG2D on human NK cells, with NKG2D72Thr exhibiting a superior activation effect on NK cells compared with NKG2D72Ala. We confirmed this conclusion also applies to NK-92 cells by in vitro cytotoxicity experiments. Therefore, reducing the immunoreactivity and immunogenicity of CAR-NK92 and directly switching NK-92 bearing NKG2D72Ala to NKG2D72Thr represent pressing challenges in realizing NK-92 cells as qualified universal off-the-shelf cellular therapeutics.
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