Association of the fibronectin type III domain–containing protein 5 rs1746661 single nucleotide polymorphism with reduced brain glucose metabolism in elderly humans

Lima Filho, Ricardo André Santana; Benedet, Andréa L.; De Bastiani, Marco Antônio; Povala, Guilherme; Ferreira, Danielle Cozachenco; Ferreira, Sérgio Teixeira; De Felice, Fernanda Guarino; Rosa Neto, Pedro; Zimmer, Eduardo Rigon; Lourenço, Mychael Vinícius da Costa

dc.contributor.author	Lima Filho, Ricardo André Santana	pt_BR
dc.contributor.author	Benedet, Andréa L.	pt_BR
dc.contributor.author	De Bastiani, Marco Antônio	pt_BR
dc.contributor.author	Povala, Guilherme	pt_BR
dc.contributor.author	Ferreira, Danielle Cozachenco	pt_BR
dc.contributor.author	Ferreira, Sérgio Teixeira	pt_BR
dc.contributor.author	De Felice, Fernanda Guarino	pt_BR
dc.contributor.author	Rosa Neto, Pedro	pt_BR
dc.contributor.author	Zimmer, Eduardo Rigon	pt_BR
dc.contributor.author	Lourenço, Mychael Vinícius da Costa	pt_BR
dc.contributor.other	Alzheimer’s Disease Neuroimaging Initiative	pt_BR
dc.date.accessioned	2023-09-23T03:38:54Z	pt_BR
dc.date.issued	2023	pt_BR
dc.identifier.issn	2632-1297	pt_BR
dc.identifier.uri	http://hdl.handle.net/10183/265162	pt_BR
dc.description.abstract	Fibronectin type III domain–containing protein 5 (FNDC5) and its derived hormone, irisin, have been associated with metabolic control in humans, with described FNDC5 single nucleotide polymorphisms being linked to obesity and metabolic syndrome. Decreased brain FNDC5/irisin has been reported in subjects with dementia due to Alzheimer’s disease. Since impaired brain glucose metabolism develops in ageing and is prominent in Alzheimer’s disease, here, we examined associations of a single nucleotide polymorphism in the FNDC5 gene (rs1746661) with brain glucose metabolism and amyloid-β deposition in a cohort of 240 cognitively unimpaired and 485 cognitively impaired elderly individuals from the Alzheimer’s Disease Neuroimaging Initiative. In cognitively unimpaired elderly individuals harbouring the FNDC5 rs1746661(T) allele, we observed a regional reduction in low glucose metabolism in memory-linked brain regions and increased brain amyloid-β PET load. No differences in cognition or levels of cerebrospinal fluid amyloid-β42, phosphorylated tau and total tau were observed between FNDC5 rs1746661(T) allele carriers and non-carriers. Our results indicate that a genetic variant of FNDC5 is associated with low brain glucose metabolism in elderly individuals and suggest that FNDC5 may participate in the regulation of brain metabolism in brain regions vulnerable to Alzheimer’s disease pathophysiology. Understanding the associations between genetic variants in metabolism-linked genes and metabolic brain signatures may contribute to elucidating genetic modulators of brain metabolism in humans.	en
dc.format.mimetype	application/pdf	pt_BR
dc.language.iso	eng	pt_BR
dc.relation.ispartof	Brain communications. Oxford. Vol. 5, no. 4 (Aug. 2023), fcad216, 10 p.	pt_BR
dc.rights	Open Access	en
dc.subject	Doenças neurodegenerativas	pt_BR
dc.subject	Alzheimer’s disease	en
dc.subject	Doença de Alzheimer	pt_BR
dc.subject	FNDC5/irisin	en
dc.subject	PET-FDG	en
dc.subject	Transtornos do metabolismo de glucose	pt_BR
dc.subject	Polimorfismo de nucleotídeo único	pt_BR
dc.subject	Glucose metabolism	en
dc.subject	Single nucleotide polymorphism	en
dc.title	Association of the fibronectin type III domain–containing protein 5 rs1746661 single nucleotide polymorphism with reduced brain glucose metabolism in elderly humans	pt_BR
dc.type	Artigo de periódico	pt_BR
dc.identifier.nrb	001177151	pt_BR
dc.type.origin	Estrangeiro	pt_BR

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