AI Article Synopsis

  • Various missense mutations in the VHL gene are linked to familial bilateral pheochromocytoma, with the p.Arg82Leu mutation being newly identified in a germline context among these patients.
  • Long-term follow-up showed that the mutation has not led to any symptoms, suggesting it may not significantly disrupt VHL gene function.
  • In silico analyses and molecular dynamics simulations suggest a potential pathogenic effect of the mutation, but the long-term outcomes for these patients remain uncertain.

Article Abstract

Various missense mutations in the VHL gene have been reported among patients with familial bilateral pheochromocytoma. However, the p.Arg82Leu mutation in the VHL gene described here among patients with familial bilateral pheochromocytoma, has never been reported previously in a germline configuration. Interestingly, long-term follow-up of these patients indicated that the mutation might have had little impact on the normal function of the VHL gene, since all of them have remained asymptomatic. We further attempted to correlate this information with the results obtained by in silico analysis of this mutation using SIFT, PhD-SNP SVM profile, MutPred, PolyPhen2, and SNPs&GO prediction tools. To gain, new mechanistic insight into the structural effect, we mapped the mutation on to 3D structure (PDB ID 1LM8). Further, we analyzed the structural level changes in time scale level with respect to native and mutant protein complexes by using 12 ns molecular dynamics simulation method. Though these methods predict the mutation to have a pathogenic potential, it remains to be seen if these patients will eventually develop symptomatic disease.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3633967PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0061908PLOS

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