AI Article Synopsis
- Aberrant expression of Tn antigen, associated with cancer progression, is linked to the enzyme GALNT2, which plays a role in O-glycosylation.
- Increased GALNT2 expression in neuroblastoma (NB) tumors correlates with factors such as better differentiation, younger age at diagnosis, and favorable survival outcomes.
- GALNT2 modifies O-glycans on IGF-1R, inhibiting IGF-1-induced growth and invasion of NB cells, indicating its critical role in NB pathogenesis.
Article Abstract
Aberrant expression of the simple mucin-type carbohydrate antigens such as Tn antigen is associated with malignant transformation and cancer progression. N-acetylgalactosaminyltransferase 2 (GALNT2), one of the enzymes that mediate the initial step of mucin-type O-glycosylation, is responsible for forming Tn antigen. GALNT2 is expressed differentially in nervous tissues during mouse embryogenesis; however, the role of GALNT2 in neuroblastoma (NB) remains unclear. Here we showed that increased GALNT2 expression evaluated using immunohistochemistry in NB tumor tissues correlated well with the histological grade of differentiation as well as younger age at diagnosis, early clinical stage, primary tumor originated from the extra-adrenal site, favorable INPC histology, and MYCN non-amplification. Multivariate analysis showed that GALNT2 expression is an independent prognostic factor for better survival for NB patients. GALNT2 overexpression suppressed IGF-1-induced cell growth, migration, and invasion of NB cells, whereas GALNT2 knockdown enhanced these NB phenotypes. Mechanistic investigations demonstrated that GALNT2 overexpression modified O-glycans on IGF-1R, which suppressed IGF-1-triggered IGF-1R dimerization and subsequent downstream signaling events. Conversely, these properties were reversed by GALNT2 knockdown in NB cells. Our findings suggest that GALNT2 regulates malignant phenotypes of NB cells through the IGF-1R signaling pathway, suggesting a critical role for GALNT2 in the pathogenesis of NB.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4322969 | PMC |
| http://dx.doi.org/10.18632/oncotarget.2627 | DOI Listing |
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