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工程化小鼠分泌白细胞介素 21 的白血病细胞诱导颗粒酶 B T 细胞和 CD4+CD44+CD62L+效应记忆细胞,同时抑制调节性 T 细胞,从而导致长期存活。

Engineered murine IL-21-secreting leukemia cells induce granzyme B T cells and CD4CD44CD62L effector memory cells while suppressing regulatory T cells, leading to long-term survival.

机构信息

Princess Margaret Cancer Centre, University Health Network, Room 8-105, Toronto, ON, M5G 2M9, Canada.

Department of Immunology, Temerty Faculty of Medicine, University of Toronto, Toronto, Canada.

出版信息

Cancer Immunol Immunother. 2023 Aug;72(8):2597-2612. doi: 10.1007/s00262-023-03442-2. Epub 2023 Apr 15.

Abstract

We have explored the use of an IL-21 cell-based anti-leukemia treatment in a mouse model of acute lymphoblastic leukemia. 70Z/3 leukemia cells, engineered to secrete IL-21 and injected into the peritoneum of syngeneic mice, induced a strong anti-leukemia response resulting in 100% survival. Mice that mounted an IL-21-induced anti-leukemia immune response were immune to the parent cell line (no IL-21) when rechallenged.Above a certain threshold, IL-21 secretion correlated with improved survival compared to mice injected with parent 70Z/3 cells. IL-21 was detected in serum with peak levels on day 7, correlating with the maximum expansion of IL-21-secreting 70Z/3 cells which subsequently were eliminated. Mice injected with IL-21-secreting leukemia cells had elevated numbers of granzyme B CD4 and CD8 T cells in the peritoneum, compared to mice injected with the parent cell line. Regulatory T cells, which increased greatly in 70Z/3-injected mice, failed to do so in mice injected with IL-21-secreting cells. Upon rechallenge, IL-21-primed mice went through a secondary immune response, primarily requiring CD4 T cells, triggering a significant increase of CD4CD44CD62L effector memory T cells. Adoptive transfer of T cells from IL21-primed/rechallenged hosts into naïve mice was successful, indicating that IL-21-primed antigen-experienced T cells convey immunity to naïve mice.Our study shows that delivery of IL-21 in a cell-based anti-leukemia protocol has the potential to induce a potent immune response leading to cancer elimination and long-term immunity-properties which make IL-21 an attractive candidate for cancer immunotherapy. Protecting against tumor antigens as well as improving cancer immunity is justified, as current strategies are limited.

摘要

我们研究了在急性淋巴细胞白血病小鼠模型中使用 IL-21 细胞为基础的抗白血病治疗方法。将分泌 IL-21 的 70Z/3 白血病细胞注入同基因小鼠的腹腔中,引发了强烈的抗白血病反应,导致 100%的存活率。产生 IL-21 诱导的抗白血病免疫反应的小鼠在再次受到亲本细胞系(无 IL-21)的攻击时具有免疫力。超过一定的阈值,与注射亲本 70Z/3 细胞的小鼠相比,IL-21 的分泌与改善的存活率相关。在第 7 天检测到血清中的 IL-21,与 IL-21 分泌的 70Z/3 细胞的最大扩张相关,随后这些细胞被消除。与注射亲本细胞系的小鼠相比,注射 IL-21 分泌白血病细胞的小鼠的腹腔中具有更高数量的颗粒酶 B CD4 和 CD8 T 细胞。在 70Z/3 注射的小鼠中大量增加的调节性 T 细胞在注射 IL-21 分泌细胞的小鼠中没有增加。在再次挑战时,IL-21 引发的小鼠经历了二次免疫反应,主要需要 CD4 T 细胞,引发 CD4CD44CD62L 效应记忆 T 细胞的显著增加。从 IL21 引发/再挑战的宿主中转移 T 细胞到幼稚小鼠中是成功的,这表明 IL-21 引发的抗原经验 T 细胞将免疫力传递给幼稚小鼠。我们的研究表明,在基于细胞的抗白血病方案中递送 IL-21 有可能诱导强大的免疫反应,从而导致癌症消除和长期免疫特性,使 IL-21 成为癌症免疫治疗的有吸引力的候选物。保护肿瘤抗原以及改善癌症免疫是合理的,因为当前的策略是有限的。

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