EBioMedicine (Nov 2016)

Prokineticin 2 Plays a Pivotal Role in Psoriasis

  • Xiaoqin He,
  • Chuanbin Shen,
  • Qiumin Lu,
  • Jiong Li,
  • Yuquan Wei,
  • Li He,
  • Ruizhen Bai,
  • Jie Zheng,
  • Ning Luan,
  • Zhiye Zhang,
  • Mingqiang Rong,
  • Ren Lai

DOI
https://doi.org/10.1016/j.ebiom.2016.10.022
Journal volume & issue
Vol. 13, no. C
pp. 248 – 261

Abstract

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Psoriasis is histologically characterized by keratinocytes (KC) hyperproliferation, inflammation, and increased angiogenesis, but the pathological factor responsible for these symptoms is unknown. Here, a neuroendocrine peptide (prokineticin 2, PK2), is highly expressed in human and mouse psoriatic skins but no significant change in other autoimmune diseases, suggesting that PK2 is a psoriasis-specific factor. Bacterial products significantly up-regulated PK2, implying that infection induces PK2 over-expression. PK2 promoted KC and macrophage to produce interleukin-1 (IL-1), the central player of inflammation and psoriasis, which acts on adjacent fibroblast to induce inflammatory cascades and KC hyperproliferation. IL-1 feeds back on macrophages to induce PK2 production to perpetuate PK2-IL-1 positive feedback loop. PK2 also promoted angiogenesis, another psoriatic symptom. In mouse models, PK2 over-expression aggravated psoriasis while its knock-down inhibited pathological development. The results indicate that PK2 over-production perpetuates psoriatic symptoms by creating PK-2-IL-1 vicious loop. PK2 is a central player in psoriasis and a promising psoriasis-specific target.

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