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CD44 Glycoprotein in Cancer: a Molecular Conundrum Hampering Clinical Applications

Overview
Journal Clin Proteomics
Publisher Biomed Central
Date 2018 Jul 10
PMID 29983670
Citations 27
Authors
Rita Azevedo
Cristiana Gaiteiro
Andreia Peixoto
Marta Relvas-Santos
Luis Lima
Lucio Lara Santos
Jose Alexandre Ferreira
Affiliations
Soon will be listed here.
Abstract

CD44 is a heavily glycosylated membrane receptor playing a key role in cell adhesion, signal transduction and cytoskeleton remodelling. It is also one of the most studied glycoproteins in cancer, frequently explored for stem cell identification, and associated with chemoresistance and metastasis. However, CD44 is a general designation for a large family of splicing variants exhibiting different degrees of glycosylation and, potentially, functionally distinct roles. Moreover, structural diversity associated with ambiguous nomenclature has delayed clinical developments. Herein, we attempt to comprehensively address these aspects and systematize CD44 nomenclature, setting milestones for biomarker discovery. In addition, we support that CD44 may be an important source of cancer neoantigens, most likely resulting from altered splicing and/or glycosylation. The discovery of potentially targetable CD44 (glyco)isoforms will require the combination of glycomics with proteogenomics approaches, exploring customized protein sequence databases generated using genomics and transcriptomics. Nevertheless, the necessary high-throughput analytical and bioinformatics tools are now available to address CD44 role in health and disease.

Citing Articles

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Aguilar-Chaparro M, Rivera-Pineda S, Hernandez-Galdamez H, Rios-Castro E, Garibay-Cerdenares O, Pina-Vazquez C J Cell Biochem. 2025; 126(2):e70003.

PMID: 39943801 PMC: 11833284. DOI: 10.1002/jcb.70003.

Proteogenomic Approaches for Diseasome Studies.

Pokhriyall M, Shukla N, Singh T, Suravajhala P Methods Mol Biol. 2024; 2859:253-264.

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Basal endothelial glycocalyx's response to shear stress: a review of structure, function, and clinical implications.

Vittum Z, Cocchiaro S, Mensah S Front Cell Dev Biol. 2024; 12:1371769.

PMID: 38562144 PMC: 10982814. DOI: 10.3389/fcell.2024.1371769.

CD44 in Bladder Cancer.

Duex J, Theodorescu D Cancers (Basel). 2024; 16(6).

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RNA-binding proteins regulating the CD44 alternative splicing.

Maltseva D, Tonevitsky A Front Mol Biosci. 2023; 10:1326148.

PMID: 38106992 PMC: 10722200. DOI: 10.3389/fmolb.2023.1326148.

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