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Physiol. Genomics 29: 169-180, 2007; doi:10.1152/physiolgenomics.00229.2006
1094-8341/07 $8.00
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Received 20 October 2006; accepted in final form 5 January 2007.
Physiological Genomics 29:169-180 (2007)
1094-8341/07 $8.00 © 2007 American Physiological Society

Sex-specific regulation of gene expression in the aging monkey aorta

Hongyu Qiu1, Bin Tian2, Ranilo G. Resuello3, Filipinas F. Natividad4, Athanasios Peppas1, You-Tang Shen1, Dorothy E. Vatner1, Stephen F. Vatner1,* and Christophe Depre1,*

1 Cardiovascular Research Institute, Department of Cell Biology and Molecular Medicine, New Jersey Medical School, Newark, New Jersey
2 Department of Biochemistry and Molecular Biology, University of Medicine and Dentistry of New Jersey (UMDNJ), New Jersey Medical School, Newark, New Jersey
3 Simian Conservation Breeding and Research Center (SICONBREC), Incorporated, Philippines
4 St. Luke's Medical Center Quezon City, Philippines

Although increased vascular stiffness is more prominent in aging males than females, and males are more prone to vascular disease with aging, no study has investigated the genes potentially responsible for sex differences in vascular aging. We tested the hypothesis that the transcriptional adaptation to aging differs in males and females using a monkey model, which is not only physiologically and phylogenetically closer to humans than the more commonly studied rodent models but also is not afflicted with the most common forms of vascular disease that accompany the aging process in humans, e.g., atherosclerosis, hypertension, and diabetes. The transcriptional profile of the aorta was compared by high-density microarrays between young and old males or females (n = 6/group). About 600 genes were expressed differentially when comparing old versus young animals. Surprisingly, <5% of these genes were shared between males and females. Radical differences between sexes were especially apparent for genes regulating the extracellular matrix, which relates to stiffness. Aging males were also more prone than females to genes switching smooth muscle cells from the "contractile" to "secretory" phenotype. Other sex differences involved genes participating in DNA repair, stress response, and cell signaling. Therefore, major differences of gene regulation exist between males and females in vascular aging, which may underlie the physiological differences characterizing aging arteries in males and females. Furthermore, the analyses in young monkeys demonstrated differences in genes regulating vascular structure, implying that the sex differences in vascular stiffness that develop with aging are programmed at an early age.

extracellular matrix; gender; vasculature; microarray




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