Mutations in XPR1 cause primary familial brain calcification associated with altered phosphate export

Legati, Andrea; Giovannini, Donatella; Nicolas, Gaël; López-Sánchez, Uriel; Quintáns, Beatriz; Oliveira, João Ricardo Mendes de; Sears, Renee L.; Ramos, Eliana Marisa; Spiteri, Elizabeth; Sobrido, María Jesús; Carracedo, Ángel; Castro-Fernández, C.; Cubizolle, Stéphanie; Fogel, Brent L.; Goizet, Cyril; Jen, Joanna C.; Kirdlarp, Suppachok; Lang, Anthony E.; Miedzybrodzka, Zosia; Mitarnun, Witoon; Paucar, Martin; Paulson, Henry L.; Pariente, Jérémie; Richard, Anne; Salins, Naomi; Simpson, Sheila A; Striano, Pasquale; Svenningsson, Per; Tison, François; Unni, Vivek K.; Vanakker, Olivier; Wessels, Marja W.; Wetchaphanphesat, Suppachok; Yang, Michele; Boller, François; Campion, Dominique; Hannequin, Didier; Sitbon, Marc; Geschwind, Daniel H.; Battini, Jean-Luc; Coppola, Giovanni

doi:10.1038/ng.3289

Cited by 249 publications

(222 citation statements)

References 28 publications

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“…Inorganic phosphate transport is crucial to cellular calcium and phosphate homeostasis and the impairment in the function of PiT2 [17] can contribute to the deposition of calcium phosphate in the vascular extracellular matrix [18]. Although calcification is limited to brain in cases reported with SLC20A2, its role of in homeostasis for inorganic phosphate is evident in several other tissues around the body including bone, parathyroid, and kidneys [19,20].…”

Section: Pathophysiology Of Genetically Determined Brain Calcificationmentioning

confidence: 99%

Deconstructing Fahr's disease/syndrome of brain calcification in the era of new genes

Batla

Tai

Schottlaender

et al. 2017

Parkinsonism & Related Disorders

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Section: Pathophysiology Of Genetically Determined Brain Calcificationmentioning

confidence: 99%

Deconstructing Fahr's disease/syndrome of brain calcification in the era of new genes

Batla

Tai

Schottlaender

et al. 2017

Parkinsonism & Related Disorders

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“…(Figure 1), originally identified as the Xenotropic and Polytropic Retrovirus Receptor 1, which is localised on the surface of many cell types [30]. While an initial overexpression study suggested that the SPX domain is not required for Xpr1's phosphate export function [16], a recent human genetic study revealed that several mutations localised within the SPX domain of Xpr1 are responsible for primary familial brain calcification (PFBC), a disease characterized by calcium phosphate deposits in the basal ganglia [33,34]. Biochemical analysis of SPX-mutated Xpr1 proteins revealed that these mutations do reduce phosphate export, demonstrating a regulatory role for the SPX domain in controlling phosphate efflux activity.…”

Section: The Association Between Spx Domains and Phosphate Metabolismmentioning

confidence: 99%

Eukaryotic Phosphate Homeostasis: The Inositol Pyrophosphate Perspective

Azevedo

Saiardi

2017

Trends in Biochemical Sciences

133

129

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“…Phosphate overload induces vascular calcification via phenotypic change of vascular smooth muscle cells into osteoblast-like cells, apoptosis of vascular smooth muscle cells, degradation of extracellular matrix in the arterial wall, and release of matrix vesicles. [31][32][33] Furthermore, clinical studies indicated that deposition of vascular calcification in the artery in a spotty pattern enhanced wall stress and promoted wall rupture. 34 These results collectively suggest that high phosphate-induced small-vessel calcification in the brain may lead to rupture of the vessels after exposure to a multitude of arteriosclerotic risk factors in the uremic milieu.…”

Section: September 2016mentioning

confidence: 99%

Association Between Serum Phosphate Levels and Stroke Risk in Patients Undergoing Hemodialysis

Yamada¹,

Tsuruya

Taniguchi³

et al. 2016

Stroke

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Background and Purpose-The contribution of serum phosphate levels to stroke risk in dialysis patients remains unclear.The present study aimed to elucidate the respective association between serum phosphate levels and the risk of brain hemorrhage or infarction in patients undergoing hemodialysis. Methods-A total of 3437 patients undergoing hemodialysis were followed up for a median of 3.9 years. The primary outcome was the occurrence of brain hemorrhage or infarction. Patients were divided into 4 groups based on their baseline serum phosphate levels (Q1-Q4). Stroke risk was estimated using a Cox proportional hazards model. Results-During the follow-up period, 75 patients experienced brain hemorrhage and 139 experienced brain infarction.The risk of brain hemorrhage was significantly higher in the highest (Q4)

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Mutations in XPR1 cause primary familial brain calcification associated with altered phosphate export

Cited by 249 publications

References 28 publications

Deconstructing Fahr's disease/syndrome of brain calcification in the era of new genes

Deconstructing Fahr's disease/syndrome of brain calcification in the era of new genes

Eukaryotic Phosphate Homeostasis: The Inositol Pyrophosphate Perspective

Association Between Serum Phosphate Levels and Stroke Risk in Patients Undergoing Hemodialysis

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