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血小板和细胞外囊泡及其与癌症的相互作用。

Platelets and extracellular vesicles and their cross talk with cancer.

机构信息

Cardeza Foundation for Hematologic Research, Department of Medicine, Thomas Jefferson University, Philadelphia, PA.

出版信息

Blood. 2021 Jun 10;137(23):3192-3200. doi: 10.1182/blood.2019004119.

Abstract

Platelets play significant and varied roles in cancer progression, as detailed throughout this review series, via direct interactions with cancer cells and by long-range indirect interactions mediated by platelet releasates. Microvesicles (MVs; also referred to as microparticles) released from activated platelets have emerged as major contributors to the platelet-cancer nexus. Interactions of platelet-derived MVs (PMVs) with cancer cells can promote disease progression through multiple mechanisms, but PMVs also harbor antitumor functions. This complex relationship derives from PMVs' binding to both cancer cells and nontransformed cells in the tumor microenvironment and transferring platelet-derived contents to the target cell, each of which can have stimulatory or modulatory effects. MVs are extracellular vesicles of heterogeneous size, ranging from 100 nm to 1 µm in diameter, shed by living cells during the outward budding of the plasma membrane, entrapping local cytosolic contents in an apparently stochastic manner. Hence, PMVs are encapsulated by a lipid bilayer harboring surface proteins and lipids mirroring the platelet exterior, with internal components including platelet-derived mature messenger RNAs, pre-mRNAs, microRNAs, and other noncoding RNAs, proteins, second messengers, and mitochondria. Each of these elements engages in established and putative PMV functions in cancer. In addition, PMVs contribute to cancer comorbidities because of their roles in coagulation and thrombosis and via interactions with inflammatory cells. However, separating the effects of PMVs from those of platelets in cancer contexts continues to be a major hurdle. This review summarizes our emerging understanding of the complex roles of PMVs in the development and progression of cancer and cancer comorbidities.

摘要

血小板在癌症进展中发挥着重要且多样化的作用,正如本综述系列所述,通过与癌细胞的直接相互作用以及血小板释放物介导的长程间接相互作用来实现。从活化的血小板释放的微泡(MV;也称为微颗粒)已成为血小板-癌症连接的主要贡献者。血小板衍生的 MV(PMV)与癌细胞的相互作用可以通过多种机制促进疾病进展,但 PMV 也具有抗肿瘤功能。这种复杂的关系源于 PMV 与肿瘤微环境中的癌细胞和非转化细胞的结合,并将血小板衍生的内容物转移到靶细胞,其中每一种都可以具有刺激或调节作用。MV 是大小不均一的细胞外囊泡,直径从 100nm 到 1µm 不等,在质膜向外出芽的过程中由活细胞释放,以一种明显随机的方式将局部胞质内容物包裹在内。因此,PMV 被一个脂质双层包裹,该双层含有表面蛋白和脂质,反映了血小板的外部,内部成分包括血小板衍生的成熟信使 RNA、前体 RNA、microRNA 和其他非编码 RNA、蛋白质、第二信使和线粒体。这些元素中的每一个都参与了癌症中已建立和推测的 PMV 功能。此外,由于 PMV 在凝血和血栓形成中的作用以及与炎症细胞的相互作用,PMV 也有助于癌症合并症的发生。然而,在癌症背景下将 PMV 的作用与血小板的作用分开仍然是一个主要障碍。本综述总结了我们对 PMV 在癌症发展和进展以及癌症合并症中的复杂作用的最新认识。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3073/8351904/6bc939667d81/bloodBLD2019004119Cabsf1.jpg

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