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P2RY12抑制剂可减少胰腺癌中的癌症相关血栓形成和肿瘤生长。

P2RY12-Inhibitors Reduce Cancer-Associated Thrombosis and Tumor Growth in Pancreatic Cancers.

作者信息

Palacios-Acedo Ana Luisa, Mezouar Soraya, Mège Diane, Crescence Lydie, Dubois Christophe, Panicot-Dubois Laurence

机构信息

Aix Marseille Univ, INSERM 1263, INRA 1260, Center for Cardiovascular and Nutrition Research (C2VN), Marseille, France.

Department of Digestive Surgery, Timone University Hospital, Marseille, France.

出版信息

Front Oncol. 2021 Sep 13;11:704945. doi: 10.3389/fonc.2021.704945. eCollection 2021.

Abstract

Platelet function can be modified by cancer cells to support tumor growth, causing alterations in the delicate hemostatic equilibrium. Cancer-cell and platelet interactions are one of the main pillars of Trousseau's syndrome: a paraneoplastic syndrome with recurring and migrating episodes of thrombophlebitis. Altogether, this leads to a four-fold risk of thrombotic events in cancer patients, which in turn, portend a poor prognosis. We previously demonstrated that anti-P2RY12 drugs inhibit cancer-associated-thrombosis and formation of tumor metastasis in pancreatic cancer models. Here, we aimed to (1) compare the effects of aspirin and clopidogrel on pancreatic cancer prevention, (2) characterize the effects of clopidogrel (platelet P2RY12 inhibitor) on cancer-associated thrombosis and cancer growth , (3) determine the effect of P2RY12 across different digestive-tract cancers , and (4) analyze the expression pattern of P2RY12 in two different cancer types affecting the digestive system. Clopidogrel treatment resulted in better survival rates with smaller primary tumors and less metastasis than aspirin treatment. Clopidogrel was also more effective than aspirin at dissolving spontaneous endogenous thrombi in our orthotopic advanced cancer mouse model. P2RY12 expression gives pancreatic adenocarcinomas proliferative advantages. In conclusion, we propose the hypothesis that clopidogrel should be further studied to target and prevent Trousseau's syndrome; as well as diminish cancer growth and spread. However, more studies are required to determine the implicated pathways and effects of these drugs on cancer development.

摘要

癌细胞可改变血小板功能以支持肿瘤生长,从而导致微妙的止血平衡发生改变。癌细胞与血小板的相互作用是Trousseau综合征的主要支柱之一,Trousseau综合征是一种伴有反复发作和迁移性血栓性静脉炎的副肿瘤综合征。总体而言,这导致癌症患者发生血栓事件的风险增加四倍,进而预示着预后不良。我们之前证明,抗P2RY12药物可抑制胰腺癌模型中与癌症相关的血栓形成和肿瘤转移。在此,我们旨在:(1)比较阿司匹林和氯吡格雷对胰腺癌预防的效果;(2)描述氯吡格雷(血小板P2RY12抑制剂)对癌症相关血栓形成和癌症生长的影响;(3)确定P2RY12在不同消化道癌症中的作用;(4)分析P2RY12在影响消化系统的两种不同癌症类型中的表达模式。与阿司匹林治疗相比,氯吡格雷治疗可提高生存率,使原发性肿瘤更小且转移更少。在我们的原位晚期癌症小鼠模型中,氯吡格雷在溶解自发性内源性血栓方面也比阿司匹林更有效。P2RY12表达赋予胰腺腺癌增殖优势。总之,我们提出以下假设:应进一步研究氯吡格雷以靶向和预防Trousseau综合征,以及减少癌症生长和扩散。然而,需要更多研究来确定这些药物在癌症发展中的相关途径和作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6d1/8475274/9baa9491b2a1/fonc-11-704945-g001.jpg

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