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Supplementation of l‐arginine boosts the therapeutic efficacy of anticancer chemoimmunotherapy

机译:L-精氨酸的补充促进了抗癌化疗的治疗疗效

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摘要

Myeloid‐derived suppressor cells (MDSCs) play a crucial role in immunosuppression in tumor‐bearing hosts. MDSCs express arginase‐I and indoleamine 2,3‐dioxygenase; they suppress T‐cell function by reducing the levels of l‐arginine and l‐tryptophan, respectively. We examined the anticancer effects of supplementation of these amino acids in CT26 colon carcinoma‐bearing mice. Oral supplementation of l‐arginine or l‐tryptophan (30 mg/mouse) did not affect tumor growth, whereas oral supplementation of d‐arginine was lethal. Supplementation of l‐arginine showed a tendency to augment the efficacy of cyclophosphamide (CP). CP reduced the proportions of granulocytic MDSCs and increased the proportions of monocytic MDSCs in the spleen and tumor tissues of CT26‐bearing mice. l‐Arginine supplementation alone did not affect the MDSC subsets. CP treatment tended to reduce the plasma levels of l‐arginine in CT26‐bearing mice and significantly increased the number of tumor‐infiltrating CD8+ T cells. In addition, l‐arginine supplementation significantly increased the proportions of tumor peptide‐specific CD8+ T cells in draining lymph nodes. Importantly, additional supplementation of l‐arginine significantly increased the number of cured mice that were treated with CP and anti‐PD‐1 antibody. Totally, l‐arginine supplementation shows promise for boosting the therapeutic efficacy of chemoimmunotherapy.
机译:粘骨衍生的抑制细胞(MDSC)在携带肿瘤宿主中的免疫抑制中起至关重要的作用。 MDSCs表达氨基酶-I和吲哚胺2,3-二氧化根酶;它们通过降低L-精氨酸和L-色氨酸的水平来抑制T细胞功能。我们检查了补充这些氨基酸在CT26结肠癌癌小鼠中的抗癌效果。 L-精氨酸或L-色氨酸(30mg /小鼠)的口服补充不影响肿瘤生长,而D-精氨酸的口服补充是致命的。 L-精氨酸的补充表明,增强环磷酰胺(CP)的功效的趋势。 CP减少了粒细胞MDSC的比例,并增加了CT26轴承小鼠脾组和肿瘤组织中单核细胞MDSC的比例。单独的L-精氨酸补充不会影响MDSC子集。 CP治疗倾向于降低CT26轴承小鼠中L-精氨酸的血浆水平,并显着增加了肿瘤渗透CD8 + T细胞的数量。此外,L-精氨酸补充剂显着增加了肿瘤肽特异性CD8 + T细胞在排水淋巴结中的比例。重要的是,额外的L-精氨酸的补充显着增加了CP和抗PD-1抗体处理的固化小鼠的数量。完全,L-精氨酸补充剂展示了提高化疗治疗的治疗效果的承诺。

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