期刊
CELL STRESS & CHAPERONES
卷 15, 期 6, 页码 819-826出版社
SPRINGER
DOI: 10.1007/s12192-010-0190-1
关键词
CCT; CCT-eta; Chaperonin; Wound healing; Alpha smooth muscle actin
类别
资金
- Allegheny Singer Research Institute, Allegheny General Hospital
- Pittsburgh Tissue Engineering Institute (PTEI)
- AFIRM [DE014780]
- 3M Fellowship
- [DC 05659]
- [DC 04173]
We have previously identified the CCT subunit eta as specifically reduced in healing fetal skin wounds by differential display, and observed that this reduction is not seen with any other CCT subunit. We now report the cloning and characterization of the cDNAs for rabbit CCT-eta and its closest evolutionary homolog, CCT-beta. Quantitative examination of CCT-eta and -beta message expression in healing fetal and adult wounds at 12 h post-injury confirms that CCT-eta mRNA is decreased in fetal wound tissues, but actually elevated in adult wound tissues. CCT-beta mRNA, in contrast, remains unchanged in both fetal and adult wound tissues. CCT-eta mRNA remains persistently elevated in healing adult wounds for 28 days following injury, whereas CCT-beta mRNA remains invariant throughout. CCT-eta protein is similarly increased, whereas CCT-beta protein remains unchanged. proportional to-smooth muscle actin (proportional to-SMA), a recognized substrate of CCT known to be important in integumentary wound healing, was also measured over the course of wound healing, and both mRNA and protein levels were elevated throughout the 28 days.
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