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揭示受过癌症教育的血小板及其促进免疫治疗发展的因素。

Revealing profile of cancer-educated platelets and their factors to foster immunotherapy development.

作者信息

Trivanović Drenka, Mojsilović Slavko, Bogosavljević Nikola, Jurišić Vladimir, Jauković Aleksandra

机构信息

Group for Hematology and Stem Cells, Institute for Medical Research, National Institute of Republic of Serbia, University of Belgrade, Dr. Subotica 4, PBOX 102, 11129, Belgrade 11000, Serbia.

Group for Hematology and Stem Cells, Institute for Medical Research, National Institute of Republic of Serbia, University of Belgrade, Dr. Subotica 4, PBOX 102, 11129, Belgrade 11000, Serbia.

出版信息

Transl Oncol. 2024 Feb;40:101871. doi: 10.1016/j.tranon.2023.101871. Epub 2023 Dec 21.

Abstract

Among multiple hemostasis components, platelets hyperactivity plays major roles in cancer progression by providing surface and internal components for intercellular crosstalk as well as by behaving like immune cells. Since platelets participate and regulate immunity in homeostatic and disease states, we assumed that revealing platelets profile might help in conceiving novel anti-cancer immune-based strategies. The goal of this review is to compile and discuss the most recent reports on the nature of cancer-associated platelets and their interference with immunotherapy. An increasing number of studies have emphasized active communication between cancer cells and platelets, with platelets promoting cancer cell survival, growth, and metastasis. The anti-cancer potential of platelet-directed therapy has been intensively investigated, and anti-platelet agents may prevent cancer progression and improve the survival of cancer patients. Platelets can (i) reduce antitumor activity; (ii) support immunoregulatory cells and factors generation; (iii) underpin metastasis and, (iv) interfere with immunotherapy by expressing ligands of immune checkpoint receptors. Mediators produced by tumor cell-induced platelet activation support vein thrombosis, constrain anti-tumor T- and natural killer cell response, while contributing to extravasation of tumor cells, metastatic potential, and neovascularization within the tumor. Recent studies showed that attenuation of immunothrombosis, modulation of platelets and their factors have a good perspective in immunotherapy optimization. Particularly, blockade of intra-tumoral platelet-associated programmed death-ligand 1 might promote anti-tumor T cell-induced cytotoxicity. Collectively, these findings suggest that platelets might represent the source of relevant cancer staging biomarkers, as well as promising targets and carriers in immunotherapeutic approaches for combating cancer.

摘要

在多种止血成分中,血小板的过度活跃通过为细胞间串扰提供表面和内部成分以及表现得像免疫细胞,在癌症进展中起主要作用。由于血小板在稳态和疾病状态下参与并调节免疫,我们推测揭示血小板特征可能有助于构思基于免疫的新型抗癌策略。本综述的目的是汇编和讨论关于癌症相关血小板的性质及其对免疫治疗干扰的最新报告。越来越多的研究强调癌细胞与血小板之间的活跃通讯,血小板促进癌细胞的存活、生长和转移。针对血小板的治疗的抗癌潜力已得到深入研究,抗血小板药物可能预防癌症进展并提高癌症患者的生存率。血小板可以(i)降低抗肿瘤活性;(ii)支持免疫调节细胞和因子的产生;(iii)促进转移,以及(iv)通过表达免疫检查点受体的配体干扰免疫治疗。肿瘤细胞诱导的血小板活化产生的介质支持静脉血栓形成,抑制抗肿瘤T细胞和自然杀伤细胞反应,同时促进肿瘤细胞的外渗、转移潜力和肿瘤内的新血管形成。最近的研究表明,免疫血栓形成的减弱、血小板及其因子的调节在免疫治疗优化方面具有良好的前景。特别是,阻断肿瘤内血小板相关的程序性死亡配体1可能促进抗肿瘤T细胞诱导的细胞毒性。总的来说,这些发现表明血小板可能代表相关癌症分期生物标志物的来源,以及在对抗癌症的免疫治疗方法中作为有前景的靶点和载体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bcbf/10776659/bf66f316590f/ga1.jpg

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