Dipartimento di Medicina e Scienze dell'Invecchiamento, Università degli Studi "G. d'Annunzio" di Chieti-Pescara, Chieti, Italy.
Center for Advanced Studies and Technology (CAST), Università degli Studi "G. d'Annunzio" di Chieti-Pescara, Chieti, Italy.
J Immunother Cancer. 2023 Mar;11(3). doi: 10.1136/jitc-2022-006056.
Progression of colorectal cancer (CRC), a leading cause of cancer-related death worldwide, is driven by colorectal cancer stem cells (CR-CSCs), which are regulated by endogenous and microenvironmental signals. Interleukin (IL)-30 has proven to be crucial for CSC viability and tumor progression. Whether it is involved in CRC tumorigenesis and impacts clinical behavior is unknown.
IL30 production and functions, in stem and non-stem CRC cells, were determined by western blot, immunoelectron microscopy, flow cytometry, cell viability and sphere formation assays. CRISPR/Cas9-mediated deletion of the gene, RNA-Seq and implantation of gene transfected or deleted CR-CSCs in NSG mice allowed to investigate IL30's role in CRC oncogenesis. Bioinformatics and immunopathology of CRC samples highlighted the clinical implications.
We demonstrated that both CR-CSCs and CRC cells express membrane-anchored IL30 that regulates their self-renewal, via WNT5A and RAB33A, and/or proliferation and migration, primarily by upregulating CXCR4 STAT3, which are suppressed by IL30 gene deletion, along with WNT and RAS pathways. Deletion of gene downregulates the expression of proteases, such as MMP2 and MMP13, chemokine receptors, mostly CCR7, CCR3 and CXCR4, and growth and inflammatory mediators, including ANGPT2, CXCL10, EPO, IGF1 and EGF. These factors contribute to IL30-driven CR-CSC and CRC cell expansion, which is abrogated by their selective blockade. gene deleted CR-CSCs displayed reduced tumorigenicity and gave rise to slow-growing and low metastatic tumors in 80% of mice, which survived much longer than controls. Bioinformatics and CIBERSORTx of the '' collection, and morphometric assessment of IL30 expression in clinical CRC samples revealed that the lack of IL30 in CRC and infiltrating leucocytes correlates with prolonged overall survival.
IL30 is a new CRC driver, since its inactivation, which disables oncogenic pathways and multiple autocrine loops, inhibits CR-CSC tumorigenicity and metastatic ability. The development of CRISPR/Cas9-mediated targeting of IL30 could improve the current therapeutic landscape of CRC.
结直肠癌(CRC)是全球癌症相关死亡的主要原因,其进展是由结直肠癌症干细胞(CR-CSCs)驱动的,这些干细胞受到内源性和微环境信号的调节。白细胞介素(IL)-30 已被证明对 CSC 活力和肿瘤进展至关重要。然而,它是否参与 CRC 肿瘤发生以及对临床行为的影响尚不清楚。
通过 Western blot、免疫电子显微镜、流式细胞术、细胞活力和球体形成试验,确定了 IL30 在干细胞和非干细胞 CRC 细胞中的产生和功能。通过 CRISPR/Cas9 介导的基因缺失、RNA-Seq 以及将转染或缺失基因的基因的 CR-CSCs 植入 NSG 小鼠中,研究了 IL30 在 CRC 癌变中的作用。CRC 样本的生物信息学和免疫病理学突出了其临床意义。
我们证明了 CR-CSCs 和 CRC 细胞都表达膜结合的 IL30,该因子通过 WNT5A 和 RAB33A 调节其自我更新,或者通过上调 CXCR4 和 STAT3 促进增殖和迁移,这些作用可被基因缺失抑制,同时抑制 WNT 和 RAS 通路。基因缺失会下调蛋白酶(如 MMP2 和 MMP13)、趋化因子受体(主要是 CCR7、CCR3 和 CXCR4)以及生长和炎症介质(包括 ANGPT2、CXCL10、EPO、IGF1 和 EGF)的表达。这些因素有助于 IL30 驱动的 CR-CSC 和 CRC 细胞扩增,而这些扩增可被其选择性阻断。缺失基因的 CR-CSCs 显示出降低的致瘤性,并在 80%的小鼠中导致生长缓慢和低转移性肿瘤,这些小鼠的存活时间明显长于对照组。对“”集合的生物信息学和 CIBERSORTx 分析,以及对临床 CRC 样本中 IL30 表达的形态计量学评估表明,CRC 和浸润性白细胞中缺乏 IL30 与总生存期延长相关。
IL30 是一种新的 CRC 驱动因子,因为其失活可抑制致癌途径和多种自分泌环,从而抑制 CR-CSC 的致瘤性和转移能力。开发基于 CRISPR/Cas9 的 IL30 靶向治疗方法可能会改善 CRC 的当前治疗格局。
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