The clinical and biochemical hallmarks generally associated with GLUT1DS may be caused by defects in genes other than SLC2A1

Sánchez Lijarcio, Obdulia; Yubero, Delia; Leal, Fátima; Couce, María L.; González Gutiérrez-Solana, Luis; López Laso, Eduardo; García Cazorla, Ángels; Pías Peleteiro, Leticia; Azua Brea, Begoña de; Ibáñez Mico, Salvador; Mateo-Martínez, Gonzalo; Troncoso Schifferli, Lucy; Witting Enríquez, Scarlet; Ugarte, Magdalena; Artuch, Rafael; Pérez, Belén

Author	dc.contributor.author	Sánchez Lijarcio, Obdulia
Author	dc.contributor.author	Yubero, Delia
Author	dc.contributor.author	Leal, Fátima
Author	dc.contributor.author	Couce, María L.
Author	dc.contributor.author	González Gutiérrez-Solana, Luis
Author	dc.contributor.author	López Laso, Eduardo
Author	dc.contributor.author	García Cazorla, Ángels
Author	dc.contributor.author	Pías Peleteiro, Leticia
Author	dc.contributor.author	Azua Brea, Begoña de
Author	dc.contributor.author	Ibáñez Mico, Salvador
Author	dc.contributor.author	Mateo-Martínez, Gonzalo
Author	dc.contributor.author	Troncoso Schifferli, Lucy
Author	dc.contributor.author	Witting Enríquez, Scarlet
Author	dc.contributor.author	Ugarte, Magdalena
Author	dc.contributor.author	Artuch, Rafael
Author	dc.contributor.author	Pérez, Belén
Admission date	dc.date.accessioned	2022-07-05T15:12:27Z
Available date	dc.date.available	2022-07-05T15:12:27Z
Publication date	dc.date.issued	2022
Cita de ítem	dc.identifier.citation	Clinical Genetics. 2022;102:40–55	es_ES
Identifier	dc.identifier.other	10.1111/cge.14138
Identifier	dc.identifier.uri	https://repositorio.uchile.cl/handle/2250/186465
Abstract	dc.description.abstract	Glucose transporter 1 deficiency syndrome (GLUT1DS) is a neurometabolic disorder caused by haploinsufficiency of the GLUT1 glucose transporter (encoded by SLC2A1) leading to defective glucose transport across the blood-brain barrier. This work describes the genetic analysis of 56 patients with clinical or biochemical GLUT1DS hallmarks. 55.4% of these patients had a pathogenic variant of SLC2A1, and 23.2% had a variant in one of 13 different genes. No pathogenic variant was identified for the remaining patients. Expression analysis of SLC2A1 indicated a reduction in SLC2A1 mRNA in patients with pathogenic variants of this gene, as well as in one patient with a pathogenic variant in SLC9A6, and in three for whom no candidate variant was identified. Thus, the clinical and biochemical hallmarks generally associated with GLUT1DS may be caused by defects in genes other than SLC2A1.	es_ES
Patrocinador	dc.description.sponsorship	Carlos III Institute (ISCIII) European Commission PI19/01155 CIBERER ERTRLE0I1 Consejeria de Educacion, Juventud y Deporte, Comunidad de Madrid B2017/BMD3721 Fundacion Isabel Gemio La Caixa Foundation LCF/PR/PR16/11110018	es_ES
Lenguage	dc.language.iso	en	es_ES
Publisher	dc.publisher	Wiley	es_ES
Type of license	dc.rights	Attribution-NonCommercial-NoDerivs 3.0 United States	*
Link to License	dc.rights.uri	http://creativecommons.org/licenses/by-nc-nd/3.0/us/	*
Source	dc.source	Clinical Genetics	es_ES
Keywords	dc.subject	GLUT1	es_ES
Keywords	dc.subject	GLUT1DS	es_ES
Keywords	dc.subject	Hypoglycorrhachia	es_ES
Título	dc.title	The clinical and biochemical hallmarks generally associated with GLUT1DS may be caused by defects in genes other than SLC2A1	es_ES
Document type	dc.type	Artículo de revista	es_ES
dc.description.version	dc.description.version	Versión publicada - versión final del editor	es_ES
dcterms.accessRights	dcterms.accessRights	Acceso abierto	es_ES
Cataloguer	uchile.catalogador	apc	es_ES
Indexation	uchile.index	Artículo de publícación WoS	es_ES

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