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Integrin Regulation in Immunological and Cancerous Cells and Exosomes.

TLDR
In this article, integrins represent the biologically and medically significant family of cell adhesion molecules that govern a wide range of normal physiology and are dynamically controlled via activation-dependent conformational changes regulated by the balance of intracellular activators and inactivators, such as Shank-associated RH domain interactor (SHARPIN) and integrin cytoplasmic domain-associated protein 1 (ICAP-1).
Abstract
Integrins represent the biologically and medically significant family of cell adhesion molecules that govern a wide range of normal physiology. The activities of integrins in cells are dynamically controlled via activation-dependent conformational changes regulated by the balance of intracellular activators, such as talin and kindlin, and inactivators, such as Shank-associated RH domain interactor (SHARPIN) and integrin cytoplasmic domain-associated protein 1 (ICAP-1). The activities of integrins are alternatively controlled by homotypic lateral association with themselves to induce integrin clustering and/or by heterotypic lateral engagement with tetraspanin and syndecan in the same cells to modulate integrin adhesiveness. It has recently emerged that integrins are expressed not only in cells but also in exosomes, important entities of extracellular vesicles secreted from cells. Exosomal integrins have received considerable attention in recent years, and they are clearly involved in determining the tissue distribution of exosomes, forming premetastatic niches, supporting internalization of exosomes by target cells and mediating exosome-mediated transfer of the membrane proteins and associated kinases to target cells. A growing body of evidence shows that tumor and immune cell exosomes have the ability to alter endothelial characteristics (proliferation, migration) and gene expression, some of these effects being facilitated by vesicle-bound integrins. As endothelial metabolism is now thought to play a key role in tumor angiogenesis, we also discuss how tumor cells and their exosomes pleiotropically modulate endothelial functions in the tumor microenvironment.

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Prostate Cancer Biomarkers: From diagnosis to prognosis and precision-guided therapeutics.

TL;DR: A recent review as discussed by the authors summarizes the progress that has so far been made in the identification of the genomic events that can be used for the classification, prediction and prognostication of prostate cancer, and as major targets for clinical intervention.
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miRNAs as potential game-changers in bone diseases: Future medicinal and clinical uses.

TL;DR: In this article , the most up-to-date information on the clinical relevance of micro-RNAs in bone disorders was brought together to explore their potential as a therapeutic target.
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Enhanced effect of autologous EVs delivering paclitaxel in pancreatic cancer.

TL;DR: In this article , the functional ligand RGD and magnetic nanoparticles (MNPs) were conjugated onto EV surfaces for pancreatic cancer therapy, which showed a significant reduction in tumor size compared to the free PTX-treated and control groups.
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Pancreatic Cancer Small Extracellular Vesicles (Exosomes): A Tale of Short- and Long-Distance Communication

TL;DR: In this article, small extracellular vesicles (sEVs, exosomes) were used as biomarkers for diagnosis and prognosis of pancreatic ductal adenocarcinoma (PDAC).
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Exosome in Crosstalk between Inflammation and Angiogenesis: A Potential Therapeutic Strategy for Stroke

TL;DR: The exosomes in complex interaction mechanisms of angiogenesis and inflammation following stroke as well as the challenges of exosomal studies such as secretion, uptake, modification, and application are discussed.
References
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Journal ArticleDOI

Interleukin-10 Deficiency Alters Endothelial Progenitor Cell–Derived Exosome Reparative Effect on Myocardial Repair via Integrin-Linked Kinase Enrichment

TL;DR: ILK knockdown in IL-10 knockout EPC-derived exosome significantly rescued their reparative dysfunction in myocardial repair, improved left ventricle cardiac function, reduced MI scar size, and enhanced post-MI neovascularization in MI mouse model.
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Kindling the flame of integrin activation and function with kindlins

TL;DR: The three members of the kindlin family have now been implicated as essential regulators of integrin function in individual cells and in whole organisms.
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ITGB3-mediated uptake of small extracellular vesicles facilitates intercellular communication in breast cancer cells

TL;DR: The authors describe thus far unknown roles of ITGB3 in the uptake of extracellular vesicles, required for colony growth of breast cancer cells.
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ITGB4-mediated metabolic reprogramming of cancer-associated fibroblasts

TL;DR: How TNBC-derived ITGB4 protein triggers glycolysis in CAFs via BNIP3L-dependent mitophagy is presented and the possibility that ITGB 4-inducedMitophagy could be targeted as a cancer therapy is suggested.
Related Papers (5)
Trending Questions (1)
Are integrins have polraized distrubution in endothelial cells?

Integrins exhibit polarized distribution in endothelial cells, influencing functions like proliferation and migration, crucial in tumor angiogenesis and microenvironment modulation by tumor and immune cell exosomes.