Von hippel-lindau disease: a genetic and clinical review.

[von hippel-lindau disease]

Von Hippel-Lindau Disease (VHL ) is an autosomal dominant inherited systemic cancer syndrome that gives rise to cystic and highly vascularized tumors in many organs , including the eye . Recent studies have contributed to the understanding of VHL pathophysiology , genetics , and the role of the VHL protein . This article reviews recent studies on VHL clinical findings , genetics and tumorigenesis .Literature review of articles on VHL genetics with correlation to clinical findings .Genotype-phenotype correlation studies show that patients with a complete deletion mutation of the VHL gene , relative to participants with a missense or protein-truncating mutation , had better visual acuity and decreased tumorigenesis incidence of retinal hemangioblastomas . It has also been documented that higher levels of vascular endothelial growth factor (VEGF ), hypoxia induced factor (HIF ), and ubiquitin are found in ocular hemangioblastomas . The stromal foamy vacuolated cells seem to be the true tumor cells of the disease acting on the surrounding endothelial cells in ocular hemangioblastomas . Tumor cells and ocular lesions have shown increased levels of Erythropoietin (Epo ), Epo receptor (EpoR ), and CD 133 . Also , CXCR 4 , a CXC chemokine receptor , is expressed in retinal VHL hemangioblastomas . Recent studies suggest that the VHL mutation alone may not be sufficient to develop VHL -associated neoplasms . Studies suggest that targeting various proteins along with anti-angiogenesis molecules may be a better therapeutic approach than targeting VEGF alone .Understanding of the mechanisms and genetics underlying VHL and its associated retinal hemangioblastomas has increased substantially in recent years . This knowledge suggests that future advances may include better identification of individuals at higher risk of vision loss and the development of novel individualized therapies .