Akt/mTOR 和 MNK/eIF4E 通路重塑前列腺癌翻译组以分泌 HGF、SPP1 和 BGN 并募集抑制性髓样细胞。
The Akt/mTOR and MNK/eIF4E pathways rewire the prostate cancer translatome to secrete HGF, SPP1 and BGN and recruit suppressive myeloid cells.
机构信息
Institute of Oncology Research, Oncology Institute of Southern Switzerland, Bellinzona, Switzerland.
Ima Biotech, Lille, France.
出版信息
Nat Cancer. 2023 Aug;4(8):1102-1121. doi: 10.1038/s43018-023-00594-z. Epub 2023 Jul 17.
Abstract
Cancer is highly infiltrated by myeloid-derived suppressor cells (MDSCs). Currently available immunotherapies do not completely eradicate MDSCs. Through a genome-wide analysis of the translatome of prostate cancers driven by different genetic alterations, we demonstrate that prostate cancer rewires its secretome at the translational level to recruit MDSCs. Among different secreted proteins released by prostate tumor cells, we identified Hgf, Spp1 and Bgn as the key factors that regulate MDSC migration. Mechanistically, we found that the coordinated loss of Pdcd4 and activation of the MNK/eIF4E pathways regulate the mRNAs translation of Hgf, Spp1 and Bgn. MDSC infiltration and tumor growth were dampened in prostate cancer treated with the MNK1/2 inhibitor eFT508 and/or the AKT inhibitor ipatasertib, either alone or in combination with a clinically available MDSC-targeting immunotherapy. This work provides a therapeutic strategy that combines translation inhibition with available immunotherapies to restore immune surveillance in prostate cancer.
摘要
癌症高度浸润髓系来源的抑制性细胞(MDSCs)。目前可用的免疫疗法并不能完全清除 MDSCs。通过对不同遗传改变驱动的前列腺癌的翻译组进行全基因组分析,我们证明前列腺癌在翻译水平上重新编程其分泌组以招募 MDSCs。在前列腺肿瘤细胞释放的不同分泌蛋白中,我们鉴定出 Hgf、Spp1 和 Bgn 是调节 MDSC 迁移的关键因素。从机制上讲,我们发现 Pdcd4 的协调缺失和 MNK/eIF4E 途径的激活调节了 Hgf、Spp1 和 Bgn 的 mRNA 翻译。在单独或与一种临床可用的 MDSC 靶向免疫疗法联合使用 MNK1/2 抑制剂 eFT508 和/或 AKT 抑制剂 ipatasertib 治疗的前列腺癌中,MDSC 浸润和肿瘤生长受到抑制。这项工作提供了一种治疗策略,将翻译抑制与现有免疫疗法相结合,以恢复前列腺癌的免疫监视。
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