Context-dependent roles for autophagy in myeloid cells in tumor progression

bioRxiv Pub Date : 2024-07-16 DOI:10.1101/2024.07.12.603292
Jayoung Choi, Gayoung Park, Steve Seung-Young Lee, Erin M Dominici, Lev Becker, Kay F. Macleod, Stephen J. Kron, Seungmin Hwang
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Abstract

Autophagy is known to suppress tumor initiation by removing genotoxic stresses in normal cells. Conversely, autophagy is also known to support tumor progression by alleviating metabolic stresses in neoplastic cells. Centered on this pro-tumor role of autophagy, there have been many clinical trials to treat cancers through systemic blocking of autophagy. Such systemic inhibition affects both tumor cells and non-tumor cells, and the consequence of blocked autophagy in non-tumor cells in the context of tumor microenvironment is relatively understudied. Here, we examined the effect of autophagy-deficient myeloid cells on the progression of autophagy-competent tumors. We found that blocking autophagy only in myeloid cells modulated tumor progression markedly but such effects were context dependent. In a tumor implantation model, the growth of implanted tumor cells was substantially reduced in mice with autophagy-deficient myeloid cells; T cells infiltrated deeper into the tumors and were responsible for the reduced growth of the implanted tumor cells. In an oncogene-driven tumor induction model, however, tumors grew faster and metastasized more in mice with autophagy- deficient myeloid cells. These data demonstrate that the autophagy status of myeloid cells plays a critical role in tumor progression, promoting or suppressing tumor growth depending on the context of tumor-myeloid cell interactions. This study indicates that systemic use of autophagy inhibitors in cancer therapy may have differential effects on rates of tumor progression in patients due to effects on myeloid cells and that this warrants more targeted use of selective autophagy inhibitors in a cancer therapy in a clinical setting.
髓系细胞自噬在肿瘤进展中的作用与环境有关
众所周知,自噬可消除正常细胞中的基因毒性压力,从而抑制肿瘤的发生。相反,自噬也能减轻肿瘤细胞的代谢压力,从而支持肿瘤的发展。围绕自噬的这种促肿瘤作用,已经有许多临床试验通过全身性阻断自噬来治疗癌症。这种全身性抑制既影响肿瘤细胞,也影响非肿瘤细胞,而在肿瘤微环境中,非肿瘤细胞自噬受阻的后果相对研究较少。在这里,我们研究了自噬缺陷的髓样细胞对自噬能力肿瘤进展的影响。我们发现,仅阻断髓系细胞的自噬功能就能明显调节肿瘤的进展,但这种影响与环境有关。在肿瘤植入模型中,自噬缺陷髓系细胞小鼠植入肿瘤细胞的生长大大减少;T细胞渗入肿瘤更深的部位,是植入肿瘤细胞生长减少的原因。然而,在癌基因驱动的肿瘤诱导模型中,自噬缺陷髓系细胞小鼠的肿瘤生长更快,转移更多。这些数据表明,髓系细胞的自噬状态在肿瘤进展过程中起着至关重要的作用,根据肿瘤与髓系细胞相互作用的具体情况促进或抑制肿瘤生长。这项研究表明,在癌症治疗中全身使用自噬抑制剂可能会由于对髓系细胞的影响而对患者的肿瘤进展率产生不同的影响,这就需要在临床癌症治疗中更有针对性地使用选择性自噬抑制剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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