SCI

5 October 2024

Hematopoietic aging promotes cancer by fueling IL-1⍺–driven emergency myelopoiesis

(Science;IF:44.7)

  • Park MD, Le Berichel J, Hamon P, Wilk CM, Belabed M, Yatim N et al. Hematopoietic aging promotes cancer by fueling IL-1⍺-driven emergency myelopoiesis. Science 2024:eadn0327.

  • Correspondence to: miriam.merad@mssm.edu

Abstract: 摘要

Age is a major risk factor for cancer, but how aging impacts tumor control remains unclear. Here, we establish that aging of the immune system, regardless of the age of the stroma and tumor, drives lung cancer progression. Hematopoietic aging enhances emergency myelopoiesis, resulting in the local accumulation of myeloid progenitor-like cells in lung tumors. These cells are a major source of IL-1⍺ that drives the enhanced myeloid response. The age-associated decline of DNMT3A enhances IL-1⍺ production, and disrupting IL-1R1 signaling early during tumor development normalized myelopoiesis and slowed the growth of lung, colonic, and pancreatic tumors. In human tumors, we identified an enrichment for IL-1⍺-expressing monocyte-derived macrophages linked to age, poorer survival, and recurrence, unraveling how aging promotes cancer and offering actionable therapeutic strategies.

年龄是癌症的主要危险因素,但衰老如何影响肿瘤尚不清楚。在这里,我们确定了免疫系统的老化,而不考虑基质和肿瘤的年龄,会驱动肺癌的进展。造血老化增强了紧急髓细胞生成,导致髓系祖细胞样细胞在肺部肿瘤中的局部积累。这些细胞是驱动增强骨髓反应的IL-1⍺的主要来源。DNMT3A的年龄相关性下降增强了IL-1⍺的产生,并在肿瘤发展早期破坏了IL-1R1信号传导,使骨髓生成正常化,减缓了肺、结肠和胰腺肿瘤的生长。在人类肿瘤中,我们发现IL-1⍺表达的单核细胞源性巨噬细胞的富集与年龄、较差的生存率和复发有关,揭示了衰老如何促进癌症,并提供了可操作的治疗策略。

 

AI全文解析
这篇文章探讨了衰老如何通过促进白细胞介素-1α(IL-1α)驱动的应急髓系细胞生成来推动癌症的发展。研究表明,衰老的免疫系统(尤其是造血系统)会加剧髓系细胞生成,从而导致在肺癌等肿瘤的微环境中积累髓系祖细胞。IL-1α的增加刺激了免疫抑制的发生,使得肿瘤更容易生长。研究团队使用小鼠模型和单细胞RNA测序揭示,阻断IL-1α通路(例如使用IL-1R1拮抗剂Anakinra)可以减缓肿瘤的生长,并增强抗肿瘤免疫反应。

 

此外,文章发现衰老导致的DNA甲基转移酶3ADNMT3A)的下调会增强IL-1α和IL-1β的产生,这种变化也在人体的非小细胞肺癌(NSCLC)患者中得到了验证。研究还发现,这一机制可能在结肠癌和胰腺癌等其他实体瘤中也起作用,表明IL-1α/IL-1R1通路的阻断可能具有广泛的癌症治疗潜力。这一发现为衰老与癌症的关系提供了新的免疫学视角,同时提出了