2014
DOI: 10.1007/s00018-014-1799-5
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Cancer intelligence acquired (CIA): tumor glycosylation and sialylation codes dismantling antitumor defense

Abstract: 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 imm… Show more

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Cited by 96 publications
(96 citation statements)
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References 166 publications
(272 reference statements)
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“…In normal smooth and skeletal muscle cells, the non-modified CD97 protein core is present, whereas in their malignant counterparts, i.e., in leiomyosarcoma and rhabdomyosarcoma cells, CD97 is found N-glycosylated [66, 67]. It is well known that glycosylation patterns are modified in cancer [88, 89]; therefore, it is important to determine whether such changes are relevant to the tumorigenic process for each individual aGPCR. N-glycosylation of CD97 is mapped to the adhesive EGF-like domains and is needed for the binding of the interaction partner CD55 [67], which is consistent with CD97 and CD55 often being co-expressed in cancer [53, 54, 9093].…”
Section: Alterations In Adhesion Gpcr Expression In Tumors Comparedmentioning
confidence: 99%
“…In normal smooth and skeletal muscle cells, the non-modified CD97 protein core is present, whereas in their malignant counterparts, i.e., in leiomyosarcoma and rhabdomyosarcoma cells, CD97 is found N-glycosylated [66, 67]. It is well known that glycosylation patterns are modified in cancer [88, 89]; therefore, it is important to determine whether such changes are relevant to the tumorigenic process for each individual aGPCR. N-glycosylation of CD97 is mapped to the adhesive EGF-like domains and is needed for the binding of the interaction partner CD55 [67], which is consistent with CD97 and CD55 often being co-expressed in cancer [53, 54, 9093].…”
Section: Alterations In Adhesion Gpcr Expression In Tumors Comparedmentioning
confidence: 99%
“…The "sialome" is a central axis of immune modulation that has not yet been explored in the context of cancer therapy (15)(16)(17). When sufficiently abundant, glycans terminating in sialic acid residues create a signature of healthy self that suppresses immune activation via several pathways (18).…”
mentioning
confidence: 99%
“…An immunosuppressive capacity of NeuGc‐gangliosides is postulated as they exhibit the capacity to downmodulate CD4 molecules on the T lymphocyte surface or to inhibit dendritic cell differentiation and maturation in vitro . This tolerance may be altered by active specific immunotherapy …”
Section: Discussionmentioning
confidence: 99%