Thomas E, Starzl Transplantation Institute, University of Pittsburgh Medical Center, Pittsburgh, PA 15260, USA.
BMC Mol Biol. 2012 Jun 25;13:20. doi: 10.1186/1471-2199-13-20.
Small proline rich protein (SPRR) 2A is one of 14 SPRR genes that encodes for a skin cross-linking protein, which confers structural integrity to the cornified keratinocyte cell envelope. New evidence, however, shows that SPRR2A is also a critical stress and wound repair modulator: it enables a variety of barrier epithelia to transiently acquire mesenchymal characteristics (EMT) and simultaneously quench reactive oxygen species during wound repair responses. p53 is also widely recognized as the node in cellular stress responses that inhibits EMT and triggers cell-cycle arrest, apoptosis, and cellular senescence. Since some p53-directed processes would seem to impede wound repair of barrier epithelia, we hypothesized that SPRR2A up regulation might counteract these effects and enable/promote wound repair under stressful environmental conditions.
Using a well characterized cholangiocarcinoma cell line we show that levels of SPRR2A expression, similar to that seen during stressful biliary wound repair responses, disrupts acetylation and subsequent p53 transcriptional activity. p53 deacetylation is accomplished via two distinct, but possibly related, mechanisms: 1) a reduction of p300 acetylation, thereby interfering with p300-p53 binding and subsequent p300 acetylation of K382 in p53; and 2) an increase in histone deacetylase 1 (HDAC1) mRNA and protein expression. The p300 CH3 domain is essential for both the autoacetylation of p300 and transference of the acetyl group to p53 and HDAC1 is a component of several non-p300 complexes that enhance p53 deacetylation, ubiquitination, and proteosomal degradation. HDAC1 can also bind the p300-CH3 domain, regulating p300 acetylation and interfering with p300 mediated p53 acetylation. The importance of this pathway is illustrated by showing complete restoration of p53 acetylation and partial restoration of p300 acetylation by treating SPRR2A expressing cells with HDAC1 siRNA.
Up-regulation of SPRR2A, similar to that seen during barrier epithelia wound repair responses reduces p53 acetylation by interfering with p300-p53 interactions and by increasing HDAC1 expression. SPRR2A, therefore, functions as a suppressor of p53-dependent transcriptional activity, which otherwise might impede cellular processes needed for epithelial wound repair responses such as EMT.
小富含脯氨酸蛋白 (SPRR) 2A 是编码皮肤交联蛋白的 14 个 SPRR 基因之一,该蛋白赋予角蛋白细胞包膜结构完整性。然而,新的证据表明,SPRR2A 也是一种关键的应激和伤口修复调节剂:它使各种屏障上皮细胞能够暂时获得间充质特征 (EMT),并在伤口修复反应中同时清除活性氧。p53 也被广泛认为是细胞应激反应中的节点,它抑制 EMT 并触发细胞周期停滞、细胞凋亡和细胞衰老。由于一些 p53 导向的过程似乎会阻碍屏障上皮的伤口修复,我们假设 SPRR2A 的上调可能会抵消这些影响,并在应激环境条件下促进/促进伤口修复。
使用经过充分表征的胆管癌细胞系,我们表明,与应激性胆管伤口修复反应中观察到的水平相似的 SPRR2A 表达水平会破坏乙酰化和随后的 p53 转录活性。p53 的去乙酰化是通过两种不同但可能相关的机制实现的:1) 降低 p300 的乙酰化,从而干扰 p300-p53 结合以及随后 p300 对 p53 中 K382 的乙酰化;和 2) 组蛋白去乙酰化酶 1 (HDAC1) mRNA 和蛋白表达增加。p300 CH3 结构域对于 p300 的自身乙酰化和乙酰基转移到 p53 至关重要,HDAC1 是几种非 p300 复合物的组成部分,这些复合物增强了 p53 的去乙酰化、泛素化和蛋白酶体降解。HDAC1 还可以结合 p300-CH3 结构域,调节 p300 的乙酰化并干扰 p300 介导的 p53 乙酰化。通过用 HDAC1 siRNA 处理表达 SPRR2A 的细胞,完全恢复 p53 的乙酰化并部分恢复 p300 的乙酰化,说明了该途径的重要性。
与屏障上皮伤口修复反应中观察到的相似,SPRR2A 的上调通过干扰 p300-p53 相互作用和增加 HDAC1 表达来减少 p53 的乙酰化。因此,SPRR2A 作为 p53 依赖性转录活性的抑制剂发挥作用,否则可能会阻碍上皮细胞伤口修复反应所需的细胞过程,例如 EMT。
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