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  3. Cancer intelligence acquired (CIA): tumor glycosylation and sialylation codes dismantling antitumor defense
 

Cancer intelligence acquired (CIA): tumor glycosylation and sialylation codes dismantling antitumor defense

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BORIS DOI
10.7892/boris.62074
Publisher DOI
10.1007/s00018-014-1799-5
PubMed ID
25487607
Description
Aberrant glycosylation is a key feature of malignant transformation and reflects epigenetic and genetic anomalies among the multitude of molecules involved in glycan biosynthesis. Although glycan biosynthesis is not template bound, altered tumor glycosylation is not random, but associated with common glycosylation patterns. Evidence suggests that acquisition of distinct glycosylation patterns evolves from a ‘microevolutionary’ process conferring advantages in terms of tumor growth, tumor dissemination, and immune escape. Such glycosylation modifications also involve xeno- and hypersialylation. Xeno-autoantigens such as Neu5Gc-gangliosides provide potential targets for immunotherapy. Hypersialylation may display ‘enhanced self’ to escape immunosurveillance and involves several not mutually exclusive inhibitory pathways that all rely on protein–glycan interactions. A better understanding of tumor ‘glycan codes’ as deciphered by lectins, such as siglecs, selectins, C-type lectins and galectins, may lead to novel treatment strategies, not only in cancer, but also in autoimmune disease or transplantation.
Date of Publication
2014-12
Publication Type
Article
Subject(s)
600 - Technology::610 - Medicine & health
Language(s)
en
Contributor(s)
Frias Boligan, Kayluz
Institut für Pharmakologie
Mesa, Circe
Fernandez, Luis Enrique
von Gunten, Stephan
Institut für Pharmakologie
Additional Credits
Institut für Pharmakologie
Series
Cellular and molecular life sciences
Publisher
Springer
ISSN
1420-682X
Access(Rights)
open.access
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