Rhaponticin suppresses the stemness phenotype of gastric cancer stem-like cells CD133+/CD166 + by inhibiting programmed death-ligand 1.

IF 2.5 3区医学 Q2 GASTROENTEROLOGY & HEPATOLOGY

BMC Gastroenterology Pub Date : 2024-11-21 DOI:10.1186/s12876-024-03512-4

Yulong Li, Yu Zhang, Jialin Tang

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引用次数: 0

Abstract

Background: Gastric cancer stem cells (GCSCs) are key contributors to tumorigenesis, recurrence and metastasis, complicating gastric cancer (GC) treatment. Rhaponticin (RA), a potential novel anticancer drug, has unexplored effects on GCSCs.

Methods: GCSCs were isolated using CD133 and CD166 markers with magnetic bead separation method and then evaluated their response to the IC50 concentrations of RA (16.90 µg/mL for BGC-823 and 22.18 µg/mL for SGC-7901), and effects on cell proliferation, migration, invasion, and stemness were measured. We analyzed the GCSC-related microarray dataset GSE111556 and explored RA's role in restoring programmed cell death ligand 1 (PD-L1) function in CD133+/CD166 + cells post-PD-L1 knockdown. RA's impact on tumour growth and immune microenvironment was assessed in a xenograft mouse model.

Results: The CD133+/CD166 + subpopulation exhibited stem-like characteristics, with the highest proportion in BGC-823 (38.85%) and SGC-7901 (43.81%) cells. These cells formed tumour spheres and had increased expression of stemness markers Sox2 and Oct-4 (compared to the parental cell line, P < 0.001). RA treatment showed no toxicity to normal GES-1 cells but reduced the viability of CD133+/CD166 + cells in a dose-dependent manner, with IC50 values of 16.90 µg/ml for BGC-823 and 22.18 µg/ml for SGC-7901. RA also decreased the proportion of CD133+/CD166 + cells and their stem-like properties (P < 0.001). Analysis of the GEO database identified PD-L1 as a key target gene of RA, with high expression in GC tissues. Knocking down PD-L1 in CD133+/CD166 + cells and introducing RA did not significantly change PD-L1 expression (P>0.05), suggesting RA's effect may be PD-L1 dependent. In a xenograft mouse model, the tumour size in the RA treatment group was approximately one-sixth that of the CD133+/CD166 + group (P < 0.001). Post-RA treatment, there was an elevation in the expression levels of CD4 and CD8, alongside a reduction in PD-L1 expression (P < 0.001).

Conclusions: RA suppresses GCSC stem - like phenotype by inhibiting PD - L1 and enhancing T cell tumour infiltration in the studied models. These findings suggest that RA may have potential for further exploration as a candidate for GC treatment, but extensive preclinical and clinical studies are required to determine its true therapeutic value.

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皂苷通过抑制程序性死亡配体1抑制胃癌干样细胞CD133+/CD166+的干表型

背景：胃癌干细胞（GCSCs）是肿瘤发生、复发和转移的关键因素，使胃癌（GC）治疗变得复杂。皂苷（RA）是一种潜在的新型抗癌药物，但其对胃癌干细胞的作用尚未被探索：方法：利用磁珠分离法，使用CD133和CD166标记物分离GCSCs，然后评估它们对IC50浓度RA（BGC-823为16.90 µg/mL，SGC-7901为22.18 µg/mL）的反应，并测量其对细胞增殖、迁移、侵袭和干性的影响。我们分析了与 GCSC 相关的微阵列数据集 GSE111556，并探讨了 RA 在 CD133+/CD166 + 细胞中恢复程序性细胞死亡配体 1（PD-L1）功能的作用。在异种移植小鼠模型中评估了RA对肿瘤生长和免疫微环境的影响：结果：CD133+/CD166+亚群表现出干细胞的特征，在BGC-823（38.85%）和SGC-7901（43.81%）细胞中比例最高。这些细胞形成肿瘤球，干性标志物Sox2和Oct-4的表达增加（与亲代细胞系相比，P 0.05），表明RA的作用可能依赖于PD-L1。在异种移植小鼠模型中，RA治疗组的肿瘤大小约为CD133+/CD166 +组的六分之一（P 结论：RA抑制了GCSC干细胞的表达：在所研究的模型中，RA通过抑制PD-L1和增强T细胞肿瘤浸润来抑制GCSC干样表型。这些研究结果表明，RA可能有潜力作为GC治疗的候选药物进行进一步探索，但要确定其真正的治疗价值，还需要进行广泛的临床前和临床研究。

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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来源期刊

BMC Gastroenterology 医学-胃肠肝病学

CiteScore

4.20

自引率

0.00%

发文量

465

审稿时长

6 months

期刊介绍： BMC Gastroenterology is an open access, peer-reviewed journal that considers articles on all aspects of the prevention, diagnosis and management of gastrointestinal and hepatobiliary disorders, as well as related molecular genetics, pathophysiology, and epidemiology.