دورية أكاديمية
أعرض في EDS

The phenotype of polycythemia due to Croatian homozygous VHL (571C>G:H191D) mutation is different from that of Chuvash polycythemia (VHL 598C>T:R200W)

التفاصيل البيبلوغرافية
العنوان: The phenotype of polycythemia due to Croatian homozygous VHL (571C>G:H191D) mutation is different from that of Chuvash polycythemia (VHL 598C>T:R200W)
المؤلفون: Tomasic, Nikica Ljubas, Piterkova, Lucie, Huff, Chad, Bilic, Ernest, Yoon, Donghoon, Miasnikova, Galina Y., Sergueeva, Adelina I., Niu, Xiaomei, Nekhai, Sergei, Gordeuk, Victor, Prchal, Josef T.
المصدر: The Center For Sickle Cell Disease Faculty Publications
بيانات النشر: Digital Howard @ Howard University
سنة النشر: 2013
المجموعة: Howard University: Digital Howard
الوصف: Mutations of VHL (a negative regulator of hypoxia-inducible factors) have position-dependent distinct cancer phenotypes. Only two known inherited homozygous VHL mutations exist and they cause polycythemia: Chuvash R200W and Croatian H191D. We report a second polycythemic Croatian H191D homozygote distantly related to the first propositus. Three generations of both families were genotyped for analysis of shared ancestry. Biochemical and molecular tests were performed to better define their phenotypes, with an emphasis on a comparison with Chuvash polycythemia. The VHL H191D mutation did not segregate in the family defined by the known common ancestors of the two subjects, suggesting a high prevalence in Croatians, but haplotype analysis indicated an undocumented common ancestor ~six generations ago as the founder of this mutation. We show that erythropoietin levels in homozygous VHL H191D individuals are higher than in VHL R200W patients of similar ages, and their native erythroid progenitors, unlike Chuvash R200W, are not hypersensitive to erythropoietin. This observation contrasts with a report suggesting that polycythemia in VHL R200W and H191D homozygotes is due to the loss of JAK2 regulation from VHL R200W and H191D binding to SOCS1. In conclusion, our studies further define the hematologic phenotype of VHL H191D and provide additional evidence for phenotypic heterogeneity associated with the positional effects of VHL mutations. © 2013 Ferrata Storti Foundation.
نوع الوثيقة: text
اللغة: unknown
العلاقة: https://dh.howard.edu/sicklecell_fac/71Test
الإتاحة: https://dh.howard.edu/sicklecell_fac/71Test
رقم الانضمام: edsbas.1B8D5EC2
قاعدة البيانات: BASE
الوصف
الوصف غير متاح.