Adipocyte‑rich microenvironment promotes chemoresistance via upregulation of peroxisome proliferator‑activated receptor gamma/ABCG2 in epithelial ovarian cancer.

IF 8.3 2区材料科学 Q1 MATERIALS SCIENCE, MULTIDISCIPLINARY

ACS Applied Materials & Interfaces Pub Date : 2024-04-01 Epub Date: 2024-03-01 DOI:10.3892/ijmm.2024.5361

Siqi Chen, Zixuan Liu, Haixia Wu, Bo Wang, Yuqing Ouyang, Junru Liu, Xiaoyan Zheng, Haoke Zhang, Xueying Li, Xiaofan Feng, Yan Li, Yangyang Shen, Hong Zhang, Bo Xiao, Chunyan Yu, Weimin Deng

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引用次数: 0

Abstract

The effects of adipocyte‑rich microenvironment (ARM) on chemoresistance have garnered increasing interest. Ovarian cancer (OVCA) is a representative adipocyte‑rich associated cancer. In the present study, epithelial OVCA (EOC) was used to investigate the influence of ARM on chemoresistance with the aim of identifying novel targets and developing novel strategies to reduce chemoresistance. Bioinformatics analysis was used to explore the effects of ARM‑associated mechanisms contributing to chemoresistance and treated EOC cells, primarily OVCAR3 cells, with human adipose tissue extracts (HATES) from the peritumoral adipose tissue of patients were used to mimic ARM in vitro. Specifically, the peroxisome proliferator‑activated receptor γ (PPARγ) antagonist GW9662 and the ABC transporter G family member 2 (ABCG2) inhibitor KO143, were used to determine the underlying mechanisms. Next, the effect of HATES on the expression of PPARγ and ABCG2 in OVCAR3 cells treated with cisplatin (DDP) and paclitaxel (PTX) was determined. Additionally, the association between PPARγ, ABCG2 and chemoresistance in EOC specimens was assessed. To evaluate the effect of inhibiting PPARγ, using DDP, a nude mouse model injected with OVCAR3‑shPPARγ cells and a C57BL/6 model injected with ID8 cells treated with GW9662 were established. Finally, the factors within ARM that contributed to the mechanism were determined. It was found that HATES promoted chemoresistance by increasing ABCG2 expression via PPARγ. Expression of PPARγ/ABCG2 was related to chemoresistance in EOC clinical specimens. GW9662 or knockdown of PPARγ improved the efficacy of chemotherapy in mice. Finally, angiogenin and oleic acid played key roles in HATES in the upregulation of PPARγ. The present study showed that the introduction of ARM‑educated PPARγ attenuated chemoresistance in EOC, highlighting a potentially novel therapeutic adjuvant to chemotherapy and shedding light on a means of improving the efficacy of chemotherapy from the perspective of ARM.

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富含脂肪细胞的微环境通过上调过氧化物酶体增殖激活受体γ/ABCG2促进上皮性卵巢癌的化疗耐药性

富含脂肪细胞的微环境（ARM）对化疗耐药性的影响越来越受到关注。卵巢癌（OVCA）是一种具有代表性的富含脂肪细胞的相关癌症。本研究以上皮性卵巢癌（EOC）为研究对象，探讨ARM对化疗耐药性的影响，旨在确定新的靶点并开发新的策略来降低化疗耐药性。研究人员利用生物信息学分析探讨了ARM相关机制对化疗耐药性的影响，并用来自患者瘤周脂肪组织的人类脂肪组织提取物（HATES）在体外模拟ARM处理EOC细胞（主要是OVCAR3细胞）。具体来说，我们使用过氧化物酶体增殖激活受体γ（PPARγ）拮抗剂 GW9662 和 ABC 转运体 G 家族成员 2（ABCG2）抑制剂 KO143 来确定其潜在机制。接着，测定了 HATES 对顺铂 (DDP) 和紫杉醇 (PTX) 处理的 OVCAR3 细胞中 PPARγ 和 ABCG2 表达的影响。此外，还评估了 PPARγ、ABCG2 与 EOC 标本化疗耐药性之间的关联。为了评估使用 DDP 抑制 PPARγ 的效果，建立了注射 OVCAR3-shPPARγ 细胞的裸鼠模型和注射经 GW9662 处理的 ID8 细胞的 C57BL/6 模型。最后，确定了促成该机制的 ARM 内部因素。研究发现，HATES通过PPARγ增加ABCG2的表达来促进化疗抗性。PPARγ/ABCG2的表达与EOC临床标本的化疗耐药性有关。GW9662 或敲除 PPARγ 可提高小鼠化疗的疗效。最后，血管生成素和油酸在HATES中对PPARγ的上调起到了关键作用。本研究表明，引入ARM教育的PPARγ可减轻EOC的化疗耐药性，突出了一种潜在的新型化疗辅助手段，并从ARM的角度阐明了一种提高化疗疗效的方法。

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来源期刊

ACS Applied Materials & Interfaces 工程技术-材料科学：综合

CiteScore

16.00

自引率

6.30%

发文量

4978

审稿时长

1.8 months

期刊介绍： ACS Applied Materials & Interfaces is a leading interdisciplinary journal that brings together chemists, engineers, physicists, and biologists to explore the development and utilization of newly-discovered materials and interfacial processes for specific applications. Our journal has experienced remarkable growth since its establishment in 2009, both in terms of the number of articles published and the impact of the research showcased. We are proud to foster a truly global community, with the majority of published articles originating from outside the United States, reflecting the rapid growth of applied research worldwide.