AI Article Synopsis
- A novel syndrome was identified in patients featuring paraganglioma, somatostatinoma, and polycythemia, with polycythemia appearing prior to any tumor formation.
- Genetic mutations affecting HIF2α were determined to be the underlying cause, prompting research to confirm their role in the syndrome's symptoms.
- Transgenic mice with these mutations showed increased erythropoietin levels and continued polycythemia even after treatment with a HIF2α inhibitor, indicating other mechanisms at play and highlighting the potential for this model in studying the syndrome's pathogenesis and treatment.
Article Abstract
We previously identified a novel syndrome in patients characterized by paraganglioma, somatostatinoma, and polycythemia. In these patients, polycythemia occurs long before any tumor develops, and tumor removal only partially corrects polycythemia, with recurrence occurring shortly after surgery. Genetic mosaicism of gain-of-function mutations of the gene (encoding HIF2α) located in the oxygen degradation domain (ODD), typically p.530-532, was shown as the etiology of this syndrome. The aim of the present investigation was to demonstrate that these mutations are necessary and sufficient for the development of the symptoms. We developed transgenic mice with a gain-of-function mutation (corresponding to human ), which demonstrated elevated levels of erythropoietin and polycythemia, a decreased urinary metanephrine-to-normetanephrine ratio, and increased expression of somatostatin in the ampullary region of duodenum. Further, inhibition of HIF2α with its specific inhibitor PT2385 significantly reduced erythropoietin levels in the mutant mice. However, polycythemia persisted after PT2385 treatment, suggesting an alternative erythropoietin-independent mechanism of polycythemia. These findings demonstrate the vital roles of mutations in the syndrome development and the great potential of the animal model for further pathogenesis and therapeutics studies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6562734 | PMC |
| http://dx.doi.org/10.3390/cancers11050667 | DOI Listing |
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