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author:

Liao, C. (Liao, C..) [1] | Xie, G. (Xie, G..) [2] | Zhu, L. (Zhu, L..) [3] | Chen, X. (Chen, X..) [4] | Li, X. (Li, X..) [5] | Lu, H. (Lu, H..) [6] | Xu, B. (Xu, B..) [7] | Ramot, Y. (Ramot, Y..) [8] | Paus, R. (Paus, R..) [9] | Yue, Z. (Yue, Z..) [10]

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Scopus

Abstract:

The intermediate filament protein keratin 17 (Krt17) shows highly dynamic and inducible expression in skin physiology and pathology. Because Krt17 exerts physiologically important functions beyond providing structural stability to keratinocytes whereas abnormal Krt17 expression is a key feature of dermatoses such as psoriasis and pachyonychia congenita, the currently unclear regulation of Krt17 expression needs to be better understood. Using a rat model of radiation dermatitis, we report here that Krt17 expression initially is down-regulated but later is strongly up-regulated by ionizing radiation. The early down-regulation correlates with the activation of p53 signaling. Deletion of p53 abolishes the initial down-regulation but not its subsequent up-regulation, suggesting that p53 represses Krt17 transcription. Because previous work reported up-regulation of Krt17 by ultraviolet irradiation, which also activates p53 signaling, the effect of ultraviolet radiation was reexamined. This revealed that the initial down-regulation of Krt17 is conserved, but the up-regulation comes much faster. Chromatin immunoprecipitation analysis in vivo and electromobility shift assay in vitro identified two p53-binding sites in the promoter region of Krt17. Thus, p53 operates as a direct Krt17 repressor, which invites therapeutic targeting in dermatoses characterized by excessive Krt17 expression. © 2015 The Authors

Keyword:

Community:

  • [ 1 ] [Liao, C.]Institute of Life Sciences, Fuzhou University, Fuzhou, Fujian, China
  • [ 2 ] [Xie, G.]Institute of Life Sciences, Fuzhou University, Fuzhou, Fujian, China
  • [ 3 ] [Zhu, L.]Institute of Life Sciences, Fuzhou University, Fuzhou, Fujian, China
  • [ 4 ] [Chen, X.]Institute of Life Sciences, Fuzhou University, Fuzhou, Fujian, China
  • [ 5 ] [Li, X.]Department of Radiation Oncology, Union Hospital of Fujian Medical University, Fuzhou, Fujian, China
  • [ 6 ] [Lu, H.]Department of Radiation Oncology, Union Hospital of Fujian Medical University, Fuzhou, Fujian, China
  • [ 7 ] [Xu, B.]Department of Radiation Oncology, Union Hospital of Fujian Medical University, Fuzhou, Fujian, China
  • [ 8 ] [Ramot, Y.]Department of Dermatology, Hadassah-Hebrew University Medical Center, Jerusalem, Israel
  • [ 9 ] [Paus, R.]Dermatology Research Centre, Institute of Inflammation and Repair, University of Manchester, Manchester, United Kingdom
  • [ 10 ] [Paus, R.]Department of Dermatology, University of Muenster, Muenster, Germany
  • [ 11 ] [Yue, Z.]Institute of Life Sciences, Fuzhou University, Fuzhou, Fujian, China

Reprint 's Address:

  • [Yue, Z.]Institute of Life Sciences, Fuzhou UniversityChina

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Source :

Journal of Investigative Dermatology

ISSN: 0022-202X

Year: 2016

Issue: 3

Volume: 136

Page: 680-689

6 . 2 8 7

JCR@2016

5 . 9 0 0

JCR@2023

ESI HC Threshold:215

JCR Journal Grade:1

CAS Journal Grade:1

Cited Count:

WoS CC Cited Count:

SCOPUS Cited Count: 20

ESI Highly Cited Papers on the List: 0 Unfold All

WanFang Cited Count:

Chinese Cited Count:

30 Days PV: 1

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