Two compound heterozygous variants in the CLN8 gene are responsible for neuronal cereidolipofuscinoses disorder in a child: a case report

Baltar, Federico; Simoes, Camila; Garagorry, Francisco; Graña, Martín; Rodríguez, Soledad; Aunchayna, María Haydée; Tapié, Alejandra; Cerisola, Alfredo; González, Gabriel; Naya, Hugo; Spangenberg, Lucía; Raggio, Víctor

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Campo DC	Valor	Lengua/Idioma
dc.rights.license	Reconocimiento 4.0 Internacional. (CC BY)	-
dc.contributor.author	Baltar, Federico	es
dc.contributor.author	Simoes, Camila	es
dc.contributor.author	Garagorry, Francisco	es
dc.contributor.author	Graña, Martín	es
dc.contributor.author	Rodríguez, Soledad	es
dc.contributor.author	Aunchayna, María Haydée	es
dc.contributor.author	Tapié, Alejandra	es
dc.contributor.author	Cerisola, Alfredo	es
dc.contributor.author	González, Gabriel	es
dc.contributor.author	Naya, Hugo	es
dc.contributor.author	Spangenberg, Lucía	es
dc.contributor.author	Raggio, Víctor	es
dc.date.accessioned	2025-06-11T17:49:58Z	-
dc.date.available	2025-06-11T17:49:58Z	-
dc.date.issued	2024-05-01	-
dc.identifier.uri	https://hdl.handle.net/20.500.12381/4062	-
dc.description.abstract	Background Neuronal Ceroid Lipofuscinosis (NCL) disorders, recognized as the primary cause of childhood dementia globally, constitute a spectrum of genetic abnormalities. CLN8, a subtype within NCL, is characterized by cognitive decline, motor impairment, and visual deterioration. This study focuses on an atypical case with congenital onset and a remarkably slow disease progression. Methods Whole-genome sequencing at 30× coverage was employed as part of a national genomics program to investigate the genetic underpinnings of rare diseases. This genomic approach aimed to challenge established classifications (vLINCL and EPMR) and explore the presence of a continuous phenotypic spectrum associated with CLN8. Results The whole-genome sequencing revealed two novel likely pathogenic mutations in the CLN8 gene on chromosome 8p23.3. These mutations were not previously associated with CLN8-related NCL. Contrary to established classifications (vLINCL and EPMR), our findings suggest a continuous phenotypic spectrum associated with CLN8. Pathological subcellular markers further validated the genomic insights. Discussion The identification of two previously undescribed likely pathogenic CLN8 gene mutations challenges traditional classifications and highlights a more nuanced phenotypic spectrum associated with CLN8. Our findings underscore the significance of genetic modifiers and interactions with unrelated genes in shaping variable phenotypic outcomes. The inclusion of pathological subcellular markers further strengthens the validity of our genomic insights. This research enhances our understanding of CLN8 disorders, emphasizing the need for comprehensive genomic analyses to elucidate the complexity of phenotypic presentations and guide tailored therapeutic strategies. The identification of new likely pathogenic mutations underscores the dynamic nature of CLN8-related NCL and the importance of individualized approaches to patient management.	es
dc.description.sponsorship	Banco Iberomericano de Desarrollo	es
dc.description.sponsorship	Fondo para la Convergencia Estructural del Mercosur	es
dc.description.sponsorship	Agencia Nacional de Investigación e Innovación	es
dc.language.iso	eng	es
dc.publisher	Frontiers	es
dc.rights	Acceso abierto	*
dc.source	Frontiers in Pediatrics	es
dc.subject	genómica médica	es
dc.title	Two compound heterozygous variants in the CLN8 gene are responsible for neuronal cereidolipofuscinoses disorder in a child: a case report	es
dc.type	Artículo	es
dc.subject.anii	Ciencias Naturales y Exactas
dc.subject.anii	Ciencias de la Computación e Información
dc.subject.anii	Ciencias de la Información y Bioinformática
dc.subject.anii	Ciencias Médicas y de la Salud
dc.subject.anii	Medicina Básica
dc.subject.anii	Genética Humana
dc.identifier.anii	FSS_X_2022_1_173209	es
dc.type.version	Publicado	es
dc.identifier.doi	10.3389/fped.2024.1379254	-
dc.anii.institucionresponsable	Facultad de Medicina, Universidad de la República, Montevideo, Uruguay	es
dc.anii.institucionresponsable	Institut Pasteur de Montevideo, Montevideo, Uruguay	es
dc.anii.institucionresponsable	Hospital de Clínicas, Facultad de Medicina, Universidad de la República, Montevideo, Uruguay	es
dc.anii.institucionresponsable	Facultad de Agronomía, Universidad de la República, Montevideo, Uruguay	es
dc.anii.subjectcompleto	//Ciencias Naturales y Exactas/Ciencias de la Computación e Información/Ciencias de la Información y Bioinformática	es
dc.anii.subjectcompleto	//Ciencias Médicas y de la Salud/Medicina Básica/Genética Humana	es
Aparece en las colecciones:	Institut Pasteur de Montevideo

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