翻译合成DNA聚合酶基因表达受年龄和IGF-1的影响

Stanley D. Rider Jr. , Madison S. Owens , Craig A. Rohan , Jeffrey B. Travers , Michael G. Kemp
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摘要

在老年人中,暴露在阳光下的皮肤区域容易发生癌变,并且从DNA中去除诱变紫外线光产物的能力降低。为了确定老年皮肤是否更依赖于翻译合成(TLS) DNA聚合酶来复制未修复的紫外线光产物,我们检测了年轻人和老年人表皮中TLS聚合酶的表达。虽然在这两个年龄组之间没有观察到显著差异,但在老年个体中发现TLS聚合酶基因POLH、POLI、POLK、REV1和REV7的表达与皮肤衰老生物标志物基因COL1A1呈负相关,而与S100A7不相关。我们进一步研究了UVB暴露对TLS聚合酶表达的影响,发现与年轻成人皮肤相比,UVB照射的老年人皮肤中POLI、POLK和REV1的mRNA水平升高。先前的研究将胰岛素样生长因子-1的产生和信号传导减少与UVB反应改变联系起来,与此一致的是,对培养的角质形成细胞和老年皮肤的研究表明,缺乏胰岛素样生长因子-1信号传导与更强的UVB依赖性诱导REV1相关。总之,这项工作表明,在未来的人类皮肤癌研究中,应该考虑uvb照射下老年皮肤中TLS聚合酶基因表达的改变。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Translesion Synthesis DNA Polymerase Gene Expression Is Impacted by Age and IGF-1 in Epidermal Human Skin
Regions of sun-exposed skin are prone to carcinogenesis in geriatric individuals and exhibit a reduced ability to remove mutagenic UV photoproducts from DNA. To determine whether geriatric skin may be more reliant on translesion synthesis (TLS) DNA polymerases to replicate unrepaired UV photoproducts, we examined the expression of TLS polymerases in the epidermis of young and geriatric individuals. Although significant differences were not observed between these 2 age groups, the expression of the TLS polymerase genes POLH, POLI, POLK, REV1, and REV7 were found to be inversely correlated with the skin aging biomarker gene COL1A1 but not with S100A7 among geriatric individuals. We further examined the effect of UVB exposure on TLS polymerase expression and found that mRNA levels of POLI, POLK, and REV1 were elevated in UVB-irradiated geriatric skin relative to those in young adult skin. Consistent with prior studies linking reduced insulin-like growth factor-1 production and signaling with altered UVB responses, studies with cultured keratinocytes and geriatric skin indicated that deficient insulin-like growth factor-1 signaling is associated with a stronger UVB-dependent induction of REV1. In summary, this work suggests that alterations to TLS polymerase gene expression in UVB-irradiated geriatric skin should be considered in future studies of skin cancer in human subjects.
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