Department of Medicine and Sciences of Aging, G. d'Annunzio University of Chieti-Pescara, Via L. Polacchi 11, 66100, Chieti, Italy.
Anatomic Pathology and Immuno-Oncology Unit, Center for Advanced Studies and Technology (CAST), G. d'Annunzio University of Chieti-Pescara, Chieti, Italy.
J Immunother Cancer. 2019 Jul 31;7(1):201. doi: 10.1186/s40425-019-0668-z.
Interleukin(IL)-30/IL-27p28 production by Prostate Cancer (PC) Stem-Like Cells (SLCs) has proven, in murine models, to be critical to tumor onset and progression. In PC patients, IL-30 expression by leukocytes infiltrating PC and draining lymph nodes correlates with advanced disease grade and stage. Here, we set out to dissect the role of host immune cell-derived IL-30 in PC growth and patient outcome.
PC-SLCs were implanted in wild type (WT) and IL-30 conditional knockout (IL-30KO) mice. Histopathological and cytofluorimetric analyses of murine tumors and lymphoid tissues prompted analyses of patients' PC samples and follow-ups.
Implantation of PC-SLCs in IL-30KO mice, gave rise to slow growing tumors characterized by apoptotic events associated with CD4T lymphocyte infiltrates and lack of CD4Foxp3 T regulatory cells (Tregs). IL-30 knockdown in PC-SLCs reduced cancer cell proliferation, vascularization and intra-tumoral Indoleamine 2,3-Dioxygenase (IDO)CD11bGr-1 myeloid-derived cells (MDCs) and led to a significant delay in tumor growth and increase in survival. IL-30-silenced tumors developed in IL-30KO mice, IL-30tumors, lacked vascular supply and displayed frequent apoptotic cancer cells entrapped by perforinTRAILCD3Tlymphocytes, most of which had a CD4T phenotype, whereas IL-10TGFβFoxp3Tregs were lacking. IL-30 silencing in PC-SLCs prevented lung metastasis in 73% of tumor-bearing WT mice and up to 80% in tumor-bearing IL-30KO mice. In patients with high-grade and locally advanced PC, those with IL-30tumors, showed distinct intra-tumoral cytotoxic granule-associated RNA binding protein (TIA-1)CD4Tlymphocyte infiltrate, rare Foxp3Tregs and a lower biochemical recurrence rate compared to patients with IL-30tumors in which IL-30 is expressed in both tumor cells and infiltrating leukocytes.
The lack of host leukocyte-derived IL-30 inhibits Tregs expansion, promotes intra-tumoral infiltration of CD4T lymphocytes and cancer cell apoptosis. Concomitant lack of MDC influx, obtained by IL-30 silencing in PC-SLCs, boosts cytotoxic T lymphocyte activation and cancer cell apoptosis resulting in a synergistic tumor suppression with the prospective benefit of better survival for patients with advanced disease.
前列腺癌(PC)干细胞样细胞(SLCs)产生的白细胞介素(IL)-30/IL-27p28 已被证明在小鼠模型中对肿瘤的发生和进展至关重要。在 PC 患者中,浸润 PC 和引流淋巴结的白细胞表达的 IL-30 与晚期疾病分级和分期相关。在这里,我们着手剖析宿主免疫细胞来源的 IL-30 在 PC 生长和患者预后中的作用。
将 PC-SLC 植入野生型(WT)和 IL-30 条件性敲除(IL-30KO)小鼠中。对小鼠肿瘤和淋巴组织的组织病理学和细胞流式分析促使对患者的 PC 样本进行分析和随访。
将 PC-SLC 植入 IL-30KO 小鼠中,导致肿瘤生长缓慢,特征为与 CD4T 淋巴细胞浸润相关的凋亡事件,以及缺乏 CD4Foxp3 T 调节细胞(Tregs)。PC-SLC 中的 IL-30 敲低减少了癌细胞的增殖、血管生成和肿瘤内吲哚胺 2,3-双加氧酶(IDO)CD11bGr-1 髓样来源细胞(MDC),并导致肿瘤生长显著延迟和生存率提高。在缺乏 IL-30 供应的情况下,IL-30 沉默的肿瘤在 IL-30KO 小鼠中形成,并且显示出频繁的凋亡癌细胞被穿孔素 TRAILCD3T 淋巴细胞包围,其中大多数具有 CD4T 表型,而 IL-10TGFβFoxp3Tregs 则缺乏。PC-SLC 中的 IL-30 沉默可防止 73%的荷瘤 WT 小鼠和高达 80%的荷瘤 IL-30KO 小鼠发生肺转移。在高级别和局部晚期 PC 患者中,IL-30 肿瘤患者的肿瘤内存在明显的细胞毒性颗粒相关 RNA 结合蛋白(TIA-1)CD4T 淋巴细胞浸润,罕见的 Foxp3Tregs,以及较低的生化复发率,而 IL-30 肿瘤患者的肿瘤细胞和浸润白细胞均表达 IL-30。
缺乏宿主白细胞来源的 IL-30 可抑制 Tregs 的扩增,促进 CD4T 淋巴细胞在肿瘤内浸润和癌细胞凋亡。同时缺乏 MDC 浸润,这是通过 PC-SLC 中的 IL-30 沉默获得的,可增强细胞毒性 T 淋巴细胞的激活和癌细胞凋亡,从而与晚期疾病患者的更好生存前景产生协同的肿瘤抑制作用。
