| Literature DB >> 29167025 |
Zhen-Rui Shi1, Guo-Zhen Tan1, Cui-Xiang Cao2, Yan-Fang Han1, Zhen Meng1, Xiao-Yong Man3, Ze-Xin Jiang1, Yu-Ping Zhang1, Ning-Ning Dang4, Kai-Hua Wei5, Ding-Fang Bu6, Fu-Tong Liu7, Liangchun Wang8.
Abstract
Psoriasis-specific proteins dysregulated in keratinocytes and involved in the pathophysiological process of psoriasis remains elusive. We report here that epidermal galectin-3 expression is significantly downregulated in lesional skin, but not in non-lesional skin in psoriasis patients, nor in a group of diseases known as psoriasiform dermatitis clinically and histologically similar to psoriasis. The deficiency of epidermal galectin-3 is sufficient to promote development of psoriatic lesions, as evidenced by more severe skin inflammation in galectin-3 knockout (gal3-/-) mice, compared to wild-type mice, after imiquimod treatment, and in skin from gal3-/- mice grafted onto wildtype mice. The development of psoriatic-like lesions is attributable to 1) the spontaneously tuning up of psoriasis signatures in keratinocytes through JNK pathway; and 2) neutrophil accumulation caused by the enhanced leukocyte-recruiting capacity associated with overexpression of S100A7-9 and CXCL-1, 8 in keratinocytes with impaired galectin-3 expression. Psoriasis-like skin inflammation is significantly improved in gal-3-/- mice both by inhibition of neutrophils accumulation with a selective CXCR2 antagonist of SB225002, and by intracutaneous injection of recombinant galectin-3. Overall, these findings offer promising galectin-3-related diagnostic and therapeutic resolutions of psoriasis.Entities:
Keywords: Galectin-3; Keratinocyte; Neutrophil; Pathogenesis; Psoriasis
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Year: 2017 PMID: 29167025 DOI: 10.1016/j.jaut.2017.11.002
Source DB: PubMed Journal: J Autoimmun ISSN: 0896-8411 Impact factor: 7.094