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Simultaneous Detection of Changes in Protein Expression and Oxidative Modification as a Function of Age andAPOEGenotype

Acceso Cerrado
ID Minciencias: ART-0000243728-6
Ranking: ART-ART_A1

Abstract:

To better elucidate temporal changes in protein oxidation resulting from aging and the Alzheimer's disease-associated Apolipoprotein E (ApoE), we developed a 2D-DIGE-based method for simultaneously detecting differential expression and carbonyl oxidation of proteins. Specifically, we examined changes in the levels of oxidation and total protein expression in hippocampi from young-adult (25−30 weeks) and old (76−97 weeks) mice transgenic for the human Apolipoprotein E gene (APOE, APOE3, APOE4) isoforms, APOE3 or APOE4. Protein samples were labeled with either a fluorescent aminooxyacetamide (Alexa Fluor 488) to detect carbonyl modifications or with NHS-Cy3 to detect total protein expression. A protein sample used as an internal control was labeled with NHS-Cy5 and run on each gel. DIGE analysis revealed 38 differentially oxidized and 100 differentially expressed protein spots with significantly different levels (P < 0.05). For oxidized proteins, principal component analysis revealed two distinct clusters: one in which oxidation increased with age independent of APOE genotype, and the second in which oxidation was dependent on APOE genotype. For total protein expression, principal component analysis revealed a large overlap between changes with overall aging and between APOE genotypes. The use of a fluorescent tag to label oxidized proteins, in combination with a NHS-Cy3 to label total protein, makes it possible to determine changes in both protein oxidation and protein expression levels in a single experiment. These studies reveal that the expression levels of peroxiredoxin protein family members Prdx2, 3, and 6 are modified by age, APOE genotype, or both.

Tópico:

Mitochondrial Function and Pathology

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Citations: 21
21

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Información de la Fuente:

SCImago Journal & Country Rank
FuenteJournal of Proteome Research
Cuartil año de publicaciónNo disponible
Volumen10
Issue4
Páginas1632 - 1644
pISSNNo disponible
ISSN1535-3907

Enlaces e Identificadores:

Minciencias IDART-0000243728-6Scienti ID0000243728-6Pmid URLhttps://pubmed.ncbi.nlm.nih.gov/21210719
Openalex URLhttps://openalex.org/W2317956471Doi URLhttps://doi.org/10.1021/pr1009788
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