Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7.
ZAC, an encoding gene mapped at chromosome 6q24-q25 within PSORS1, was previously found over-expressed in the lower compartment of the hyperplastic epidermis in psoriatic lesions. Cytokines produced in the inflammatory dermatoses may drive AP-1 transcription factor to induce responsive gene expressi...
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doaj-b85cdec2b4e84def980326d9ffa5b53f2020-11-24T21:23:16ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-011012e014417510.1371/journal.pone.0144175Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7.Yu-Wen ChuShu-Ting LiuHsiao-Chun ChengShih-Ming HuangYung-Lung ChangChien-Ping ChiangYing-Chun LiuWei-Ming WangZAC, an encoding gene mapped at chromosome 6q24-q25 within PSORS1, was previously found over-expressed in the lower compartment of the hyperplastic epidermis in psoriatic lesions. Cytokines produced in the inflammatory dermatoses may drive AP-1 transcription factor to induce responsive gene expressions. We demonstrated that mZac1 can enhance AP-1-responsive S100A7 expression of which the encoding gene was located in PSORS4 with HaCaT keratinocytes. However, the mZac1-enhanced AP-1 transcriptional activity was suppressed by curcumin, indicating the anti-inflammatory property of this botanical agent and is exhibited by blocking the AP-1-mediated cross-talk between PSORS1 and PSORS4. Two putative AP-1-binding sites were found and demonstrated to be functionally important in the regulation of S100A7 promoter activity. Moreover, we found curcumin reduced the DNA-binding activity of AP-1 to the recognition element located in the S100A7 promoter. The S100A7 expression was found to be upregulated in the lesioned epidermis of atopic dermatitis and psoriasis, which is where this keratinocyte-derived chemoattractant engaged in the pro-inflammatory feedback loop. Understanding the regulatory mechanism of S100A7 expression will be helpful to develop therapeutic strategies for chronic inflammatory dermatoses via blocking the reciprocal stimuli between the inflammatory cells and keratinocytes.http://europepmc.org/articles/PMC4669192?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Yu-Wen Chu Shu-Ting Liu Hsiao-Chun Cheng Shih-Ming Huang Yung-Lung Chang Chien-Ping Chiang Ying-Chun Liu Wei-Ming Wang |
spellingShingle |
Yu-Wen Chu Shu-Ting Liu Hsiao-Chun Cheng Shih-Ming Huang Yung-Lung Chang Chien-Ping Chiang Ying-Chun Liu Wei-Ming Wang Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7. PLoS ONE |
author_facet |
Yu-Wen Chu Shu-Ting Liu Hsiao-Chun Cheng Shih-Ming Huang Yung-Lung Chang Chien-Ping Chiang Ying-Chun Liu Wei-Ming Wang |
author_sort |
Yu-Wen Chu |
title |
Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7. |
title_short |
Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7. |
title_full |
Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7. |
title_fullStr |
Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7. |
title_full_unstemmed |
Opposing Effects of Zac1 and Curcumin on AP-1-Regulated Expressions of S100A7. |
title_sort |
opposing effects of zac1 and curcumin on ap-1-regulated expressions of s100a7. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2015-01-01 |
description |
ZAC, an encoding gene mapped at chromosome 6q24-q25 within PSORS1, was previously found over-expressed in the lower compartment of the hyperplastic epidermis in psoriatic lesions. Cytokines produced in the inflammatory dermatoses may drive AP-1 transcription factor to induce responsive gene expressions. We demonstrated that mZac1 can enhance AP-1-responsive S100A7 expression of which the encoding gene was located in PSORS4 with HaCaT keratinocytes. However, the mZac1-enhanced AP-1 transcriptional activity was suppressed by curcumin, indicating the anti-inflammatory property of this botanical agent and is exhibited by blocking the AP-1-mediated cross-talk between PSORS1 and PSORS4. Two putative AP-1-binding sites were found and demonstrated to be functionally important in the regulation of S100A7 promoter activity. Moreover, we found curcumin reduced the DNA-binding activity of AP-1 to the recognition element located in the S100A7 promoter. The S100A7 expression was found to be upregulated in the lesioned epidermis of atopic dermatitis and psoriasis, which is where this keratinocyte-derived chemoattractant engaged in the pro-inflammatory feedback loop. Understanding the regulatory mechanism of S100A7 expression will be helpful to develop therapeutic strategies for chronic inflammatory dermatoses via blocking the reciprocal stimuli between the inflammatory cells and keratinocytes. |
url |
http://europepmc.org/articles/PMC4669192?pdf=render |
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