Thrombospondin-1 过度表达刺激 Smad4 缺失，并通过 TGF-β 信号激活加速胰腺导管腺癌的恶性行为,Translational Oncology

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Thrombospondin-1 过度表达刺激 Smad4 缺失，并通过 TGF-β 信号激活加速胰腺导管腺癌的恶性行为
Translational Oncology ( IF 4.5 ) Pub Date : 2022-09-15 , DOI: 10.1016/j.tranon.2022.101533
Kazuki Matsumura ₁ , Hiromitsu Hayashi ₁ , Norio Uemura ₁ , Yoko Ogata ₁ , Liu Zhao ₁ , Hiroki Sato ₁ , Yuta Shiraishi ₁ , Hideyuki Kuroki ₁ , Fumimasa Kitamura ₁ , Takayoshi Kaida ₁ , Takaaki Higashi ₁ , Shigeki Nakagawa ₁ , Kosuke Mima ₁ , Katsunori Imai ₁ , Yo-Ichi Yamashita ₁ , Hideo Baba ₁

Affiliation

介绍

胰腺导管腺癌（PDAC）的特点是丰富的基质和癌症相关成纤维细胞（CAF）提供了有利的肿瘤微环境。Smad4 被认为是包括 PDAC 在内的多种癌症的肿瘤抑制因子，Smad4 的缺失会加速细胞侵袭性和转移潜力。血小板反应蛋白-1 (TSP-1) 可作为体内潜在转化生长因子-β (TGF-β) 的主要激活剂。然而，TSP-1 以及 PDAC 进展过程中 Smad4 丢失和 TGF-β 信号激活的介质的作用尚未得到解决。目的是阐明 TSP-1 在 PDAC 进展中的生物学作用。

方法和结果

高基质硬度刺激 CAF 中的 TSP-1 表达，TSP-1敲除可抑制细胞增殖，抑制 CAF 中促纤维化和激活基质相关基因的表达。PDAC 细胞的旁分泌 TSP-1 处理通过激活 TGF-β 信号（例如磷酸化 Akt 和 Smad2/3 表达）促进细胞增殖和上皮间质转化 (EMT)。令人惊讶的是， DPC4 （Smad4 基因）的敲除可诱导 PDAC 细胞中 TSP-1 过度表达并激活 TGF-β 信号。有趣的是，TSP-1 过表达还诱导 Smad4 表达下调，并增强体外和体内细胞增殖。LSKL 肽可拮抗 TSP-1 介导的潜在 TGF-β 激活，可减弱细胞增殖、迁移和化疗耐药性，并增强 PDAC 细胞的凋亡。

结论

源自 CAF 的 TSP-1 会刺激癌细胞中 Smad4 表达的丧失，并通过 PDAC 中的 TGF-β 信号激活加速恶性行为。TSP-1 可能是一个新的治疗靶点，不仅适用于僵硬基质中的 CAF，也适用于 PDAC 微环境中的癌细胞。

"点击查看英文标题和摘要"

Thrombospondin-1 overexpression stimulates loss of Smad4 and accelerates malignant behavior via TGF-β signal activation in pancreatic ductal adenocarcinoma

Introduction

Pancreatic ductal adenocarcinoma (PDAC) is characterized by abundant stroma and cancer-associated fibroblasts (CAFs) provide a favorable tumor microenvironment. Smad4 is known as tumor suppressor in several types of cancers including PDAC, and loss of Smad4 triggers accelerated cell invasiveness and metastatic potential. The thrombospondin-1 (TSP-1) can act as a major activator of latent transforming growth factor-β (TGF-β) in vivo. However, the roles of TSP-1 and the mediator of Smad4 loss and TGF-β signal activation during PDAC progression have not yet been addressed. The aim is to elucidate the biological role of TSP-1 in PDAC progression.

Methods and results

High substrate stiffness stimulated TSP-1 expression in CAFs, and TSP-1 knockdown inhibited cell proliferation with suppressed profibrogenic and activated stroma-related gene expressions in CAFs. Paracrine TSP-1 treatment for PDAC cells promoted cell proliferation and epithelial mesenchymal transition (EMT) with activated TGF-β signals such as phosphorylated Akt and Smad2/3 expressions. Surprisingly, knockdown of DPC4 (Smad4 gene) induced TSP-1 overexpression with TGF-β signal activation in PDAC cells. Interestingly, TSP-1 overexpression also induced downregulation of Smad4 expression and enhanced cell proliferation in vitro and in vivo. Treatment with LSKL peptide, which antagonizes TSP-1-mediated latent TGF-β activation, attenuated cell proliferation, migration and chemoresistance with enhanced apoptosis in PDAC cells.

Conclusions

TSP-1 derived from CAFs stimulates loss of Smad4 expression in cancer cells and accelerates malignant behavior by TGF-β signal activation in PDAC. TSP-1 could be a novel therapeutic target, not only for CAFs in stiff stroma, but also for cancer cells in the PDAC microenvironment.

更新日期：2022-09-16

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