Mutations in XPR1 Cause Primary Familial Brain Calcification Associated With Altered Phosphate Export

al., et; Carracedo, Angel; Castro-Fernandez, Cristina; Cubizolle, Stephanie; Fogel, Brent L.; Giovannini, Donatella; Goizet, Cyril; Jen, Joanna C.; Kirdlarp, Suppachok; Lang, Anthony E.; Legati, Andrea; Lopez-Sanchez, Uriel; Nicolas, G.; Oliveira, J. R.; Quintans, Beatriz; Ramos, Eliana Marisa; Salins, Naomi; Sears, Renee L.; Sobrido, M. J.; Spiteri, Elizabeth

Mutations in XPR1 Cause Primary Familial Brain Calcification Associated With Altered Phosphate Export

Authors: et al.
Angel Carracedo
Cristina Castro-Fernandez
Stephanie Cubizolle
Brent L. Fogel
Donatella Giovannini
Cyril Goizet
Joanna C. Jen
Suppachok Kirdlarp
Anthony E. Lang
Andrea Legati
Uriel Lopez-Sanchez
G. Nicolas
J. R. Oliveira
Beatriz Quintans
Eliana Marisa Ramos
Naomi Salins
Renee L. Sears
M. J. Sobrido
Elizabeth Spiteri
Publication date: 1 January 2015
Publisher: Barrow - St. Joseph\u27s Scholarly Commons

Abstract

Primary familial brain calcification (PFBC) is a neurological disease characterized by calcium phosphate deposits in the basal ganglia and other brain regions and has thus far been associated with SLC20A2, PDGFB or PDGFRB mutations. We identified in multiple families with PFBC mutations in XPR1, a gene encoding a retroviral receptor with phosphate export function. These mutations alter phosphate export, implicating XPR1 and phosphate homeostasis in PFBC

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