Effect of orally administered collagen hydrolysate on gene expression profiles in mouse skin: a DNA microarray analysis.

نویسندگان

  • Chisato Oba
  • Kyoko Ito
  • Satomi Ichikawa
  • Masashi Morifuji
  • Yuji Nakai
  • Tomoko Ishijima
  • Keiko Abe
  • Keiko Kawahata
چکیده

Dietary collagen hydrolysate has been hypothesized to improve skin barrier function. To investigate the effect of long-term collagen hydrolysate administration on the skin, we evaluated stratum corneum water content and skin elasticity in intrinsically aged mice. Female hairless mice were fed a control diet or a collagen hydrolysate-containing diet for 12 wk. Stratum corneum water content and skin elasticity were gradually decreased in chronologically aged control mice. Intake of collagen hydrolysate significantly suppressed such changes. Moreover, we used DNA microarrays to analyze gene expression in the skin of mice that had been administered collagen hydrolysate. Twelve weeks after the start of collagen intake, no significant differences appeared in the gene expression profile compared with the control group. However, 1 wk after administration, 135 genes were upregulated and 448 genes were downregulated in the collagen group. This suggests that gene changes preceded changes of barrier function and elasticity. We focused on several genes correlated with functional changes in the skin. Gene Ontology terms related to epidermal cell development were significantly enriched in upregulated genes. These skin function-related genes had properties that facilitate epidermal production and differentiation while suppressing dermal degradation. In conclusion, our results suggest that altered gene expression at the early stages after collagen administration affects skin barrier function and mechanical properties. Long-term oral intake of collagen hydrolysate improves skin dysfunction by regulating genes related to production and maintenance of skin tissue.

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Effect of orally administered collagen hydrolysate on gene expression profiles in mouse

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عنوان ژورنال:
  • Physiological genomics

دوره 47 8  شماره 

صفحات  -

تاریخ انتشار 2015