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Differential expression of chaperonin containing T-complex polypeptide (CCT) subunits during fetal and adult skin wound healing

机译:胎儿和成人皮肤伤口愈合过程中含有伴侣蛋白的T复合多肽(CCT)亚基的差异表达

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摘要

Integumentary wound healing in early fetal life is regenerative and proceeds without scar formation. Expressomic analysis of this phenomenon by differential display has previously determined that the eta subunit of the cytosolic chaperonin containing T-complex polypeptide (CCT) is downregulated in the healing fetal wound milieu. We now report that no other CCT subunit shares this distinct pattern of gene regulation as determined by limiting dilution reverse transcriptase polymerase chain reaction (RT-PCR); all seven of the remaining CCT subunits demonstrate no change in messenger RNA (mRNA) expression in healing fetal wounds compared to unwounded control tissue. The alpha subunit, however, did evidence reduced message levels in healing adult wound tissue. We herein report on the cloning and sequence of the complementary DNA (cDNA) for rabbit CCT-alpha and confirm its wound specific decrease in adult tissues through quantitative real-time RT-PCR assay. We also confirm that quantitative evaluation of CCT-alpha and CCT-zeta mRNA expression shows no change in healing fetal wounds.
机译:胎儿早期的皮肤外伤口愈合是可再生的,并且不会形成疤痕。通过差异显示对该现象的表达组学分析先前已经确定,在愈合的胎儿伤口环境中,含有胞质伴侣蛋白的T-复合多肽(CCT)的eta亚基被下调。我们现在报道,没有其他CCT亚基通过限制稀释的逆转录酶聚合酶链反应(RT-PCR)来确定这种独特的基因调控模式。与未受伤的对照组织相比,所有剩余的7个CCT亚基在愈合的胎儿伤口中均未显示信使RNA(mRNA)表达变化。但是,α亚基确实证明了在成人伤口愈合组织中信息水平降低。我们在此报告了兔CCT-α的互补DNA(cDNA)的克隆和序列,并通过定量实时RT-PCR测定证实其在成人组织中的伤口特异性降低。我们还证实,定量评估CCT-alpha和CCT-zeta mRNA的表达表明愈合的胎儿伤口没有变化。

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