2007
DOI: 10.1152/physiolgenomics.00060.2007
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Global expression profiles from C57BL/6J and DBA/2J mouse lungs to determine aging-related genes

Abstract: This study identified gene expression profiles that provided evidence for genomic mechanisms underlying the pathophysiology of aging lung. Aging lungs from C57BL/6 (B6) and DBA/2 (D2) mouse strains differ in physiology and morphometry. Lungs were harvested from B6 mice at 2, 18, and 26 mo and from D2 mice at 2 and 18 mo of age. Purified RNA was subjected to oligonucleotide microarray analyses, and differential expression analyses were performed for comparison of various data sets. A significant majority of dif… Show more

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Cited by 48 publications
(52 citation statements)
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“…These age-related impairments in respiratory mechanics were associated with progressively reduced expression of Hhip in Hhip +/+ murine lungs and even greater reductions in Hhip expression in Hhip +/− lungs during aging (Fig. S1) (23), supporting protective roles of Hhip during aging.…”
Section: Resultsmentioning
confidence: 64%
See 1 more Smart Citation
“…These age-related impairments in respiratory mechanics were associated with progressively reduced expression of Hhip in Hhip +/+ murine lungs and even greater reductions in Hhip expression in Hhip +/− lungs during aging (Fig. S1) (23), supporting protective roles of Hhip during aging.…”
Section: Resultsmentioning
confidence: 64%
“…Motivated by human GWAS studies showing that HHIP is associated with both COPD affection status in case-control studies and FEV 1 levels in general population samples (12,13), we demonstrate that HHIP protects aging-related airspace enlargement and increases in lung compliance in mice. Reduction in HHIP expression in COPD lungs (16), as well as in lungs of aging rodents (23), increases susceptibility to develop emphysema during aging. Furthermore, reduced antioxidant capacity and increased oxidant levels in Hhip +/− mice preceded emphysema development.…”
Section: Hhip Interacts With Gstp1 and Enhances Glutathione-conjugatingmentioning
confidence: 99%
“…An absolute fold change (FC) of Ն1.5 was also used as a criterion to select noteworthy genes. These criteria were consistent with the bioinformatics techniques used in previous mouse studies (11,14,31). NetAffx (26) was used to extract gene ontology information for the gene expression profiles.…”
Section: Animalsmentioning
confidence: 95%
“…Aging and longevity studies were also compared to a number of studies which examined gender-dependent gene changes in the mouse liver (Amador-Noguez et al, 2005;Guo et al, 2009). In addition, profiles from aged livers were compared to heart, gastrocnemius muscle and brain neocortex from 30-month versus 5-month-old mice (Barger et al, 2008), lungs from 26-month versus 2-month-old mice (Misra et al, 2007), hematopoietic stem cells from 22 to 23-month versus 2 to 3-month-old mice (Rossi et al, 2005) and brain neocortex from 30-month versus 5-month-old mice (Oberdoerffer et al, 2008). Files (.cel) from all studies and raw gene expression values from the AGEMAP study were uploaded to Rosetta Resolver (Seattle, WA) for analysis.…”
Section: Meta-analysismentioning
confidence: 99%
“…The expression of the genes identified in the mouse liver was compared to that in a number of other aging studies. From left to right, these included heart, gastrocnemius muscle and neocortex from 30-month versus 5-month-old mice (Barger et al, 2008), lungs from 26-month versus 2-month-old mice (Misra et al, 2007), hematopoietic stem cells from 22 to 23-month versus 2 to 3-month-old mice (Rossi et al, 2005) and brain neocortex from 30-month versus 5-month-old mice (Oberdoerffer et al, 2008). The genes are presented in the same order as in Fig.…”
Section: Independent Aging Studies Validate the Hepatic Genes Of Agingmentioning
confidence: 99%