HMMR has oncoprotein-like properties in neuroblastoma cells and high HMMR expression has independent prognostic potential in neuroblastomas
Christina Karapouliou, Elisyazaviera M. Faizul, Vinothini Rajeeve, Pedro R. Cutillas, Andrew W. Stoker

TL;DR
This study shows that HMMR behaves like an oncoprotein in neuroblastoma cells and that high HMMR levels predict poor survival in patients.
Contribution
The study is the first to demonstrate HMMR's oncoprotein-like properties in neuroblastoma and its potential as an independent prognostic marker.
Findings
High HMMR expression is an independent prognostic indicator of poor survival in neuroblastoma patients.
Loss of HMMR suppresses neuroblastoma cell proliferation, motility, and clonogenic capacity.
HMMR influences MTOR and DDR pathways, as shown by phosphoproteomic analysis.
Abstract
Neuroblastoma (NB) is a devastating childhood cancer where most tumours have no clear oncogenic driver. We aimed to define whether HMMR, an oncogene-like protein in several cancers, harbors similar potential in neuroblastoma cells. HMMR is a hyaluronic acid (HA) receptor and a mitotic microtubule regulator. We show that high HMMR expression does not correlate well with MYCN driver expression and moreover statistically HMMR is an independent prognostic indicator of poor survival in NB patients. In cultured KELLY neuroblastoma cells, removal of the HMMR protein suppresses proliferation, motility and clonogenic capacity, while xenografts of HMMR-deficient cells imparted longer animal survival compared to wild type cells. Loss of motility in culture was compensated by addition of exogenous HA, suggesting that HMMR signaling is at least partly under HA control. Through an unbiased…
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Taxonomy
TopicsNeuroblastoma Research and Treatments · Proteoglycans and glycosaminoglycans research · Glycosylation and Glycoproteins Research
