Increased expression of uPA, uPAR, and PAI-1 in psoriatic skin and in basal cell carcinomas

Рубина, К. А.; Sysoeva, Veronika; Zagorujko, E. I.; Цоколаева, З. И.; Курдина, М. И.; Parfyonova, Y.; Ткачук, В. А.

doi:10.1007/s00403-017-1738-z

Cited by 35 publications

(35 citation statements)

References 69 publications

(81 reference statements)

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“…SuPAR was highly expressed in the dermis of patients with psoriasis, yet its serum levels failed to correlate with disease severity. Nonetheless, suPAR’s value needs to be better studied in patients with various stages of psoriasis to confirm these findings 45. SLE is another dermatological autoinflammatory disease, characterised by systemic inflammation that involves nearly all the vital organs.…”

Section: Dermatology and Rheumatologymentioning

confidence: 99%

“…The serine protease activity of plasmin has been found to be involved in inflammatory reactions, tissue remodelling and degradation of matrix proteins in several immune-mediated dermatological and rheumatological diseases 45. Such conditions are characterised by multifactorial pathways leading to systemic inflammation with end-organ damage.…”

Section: Dermatology and Rheumatologymentioning

confidence: 99%

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SuPAR, an emerging biomarker in kidney and inflammatory diseases

Hamie

Daoud

Nemer

et al. 2018

Postgraduate Medical Journal

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Soluble urokinase plasminogen activator receptor (suPAR) is a circulating form of a physiological and pathophysiological important cell surface receptor, implicated in inflammation. Recent studies showed that suPAR is a promising biomarker, useful for diagnosis, assessment and prognosis of several diseases. This review summarises the majority of preliminary studies and analyses the significance and the clinical application of suPAR in various clinical conditions. SuPAR seems to have a significant value in the diagnosis as well as prognosis of many diseases; nonetheless, it merits large-scale studies to set cut-off values that help physicians in following up their patients and accordingly tailor their treatment plans.

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Section: Dermatology and Rheumatologymentioning

confidence: 99%

Section: Dermatology and Rheumatologymentioning

confidence: 99%

SuPAR, an emerging biomarker in kidney and inflammatory diseases

Hamie

Daoud

Nemer

et al. 2018

Postgraduate Medical Journal

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“…The conditioned medium from an epidermal model cultured at low humidity enhanced MMP-1 secretion by normal human dermal fibroblasts [7]. DPP4, EMMPRIN, GDF-15, HGF, uPAR, MIP-3α, ST2 and leptin, which were regulated at reduced humidity in our experiment, are known to have functions in skin remodeling and inflammation [18][19][20][21][22][23][24].…”

Section: Discussionmentioning

confidence: 58%

Reduced humidity induces skin barrier dysfunction and secretion of dipeptidyl peptidase-4 (DPP-4) in a skin-equivalent model

Lee

Bae

Marinho

et al. 2019

ARCH BIOL SCI BELGRA

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Seasonal changes can affect the physiological condition of the skin and cause various cutaneous disorders. The skin barrier function tends to worsen during winter when humidity is lower compared to other seasons. To determine the influence of relative humidity (RH) on the function of the skin barrier, we performed biological and histological assays using skin equivalents that were cultured under reduced humidity in an environmental humidity chamber. We found that reduced humidity led to decreased epidermal thickness and disruption of the skin barrier. Reduced humidity induced the decrease of filaggrin, loricrin and damage to tight junction. In addition, dipeptidyl peptidase-4 (DPP4), which has roles in the immunological process, was upregulated in a skin-equivalent model under reduced humidity. These results suggest that reduced humidity affects the skin barrier function and regulates the secretion of DPP4 in a skin-equivalent model.

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“…In addition to their expression changes associated with wound repair [63], the cohort of SERPINE (plasminogen activator inhibitor 1), PLAUR (plasminogen activator, urokinase receptor), and PLAU (plasminogen activator, urokinase) are upregulated in psoriasis compared to amounts beneath the limits of detection or at very low levels in healthy epidermis [64]. As compared to HaCaT keratinocytes with usual levels of TNIP1 protein under poly (I:C) conditions, TNIP1-deficient cells exposed to this DAMP/PAMP had increased expression of each of the following: SERPINE, 9-fold; PLAUR,~3-fold; and PLAU,~2-fold.…”

Section: Discussionmentioning

confidence: 99%

Enhanced Wound Healing- and Inflammasome-Associated Gene Expression in TNFAIP3-Interacting Protein 1- (TNIP1-) Deficient HaCaT Keratinocytes Parallels Reduced Reepithelialization

Shamilov

Ackley

Aneskievich

2020

Mediators of Inflammation

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TNIP1 protein is a widely expressed, cytoplasmic inhibitor of inflammatory signaling initiated by membrane receptors such as TLRs which recognize pathogen-associated and damage-associated molecular patterns (PAMPs and DAMPs). Keratinocyte TNIP1 deficiency sensitizes cells to PAMPs and DAMPs promoting hyperresponsive expression and secretion of cytokine markers (e.g., IL-8 and IL-6) relevant to cases of chronic inflammation, like psoriasis, where TNIP1 deficiency has been reported. Here, we examined the impact of TNIP1 deficiency on gene expression and cellular responses (migration and viability) relevant to acute inflammation as typically occurs in wound healing. Using siRNA-mediated TNIP1 expression knockdown in cultured HaCaT keratinocytes, we investigated TNIP1 deficiency effects on signaling downstream of TLR3 agonism with low-concentration poly (I:C), a representative PAMP/DAMP. The combination of TNIP1 knockdown and PAMP/DAMP signaling disrupted expression of specific keratinocyte differentiation markers (e.g., transglutaminase 1 and involucrin). These same conditions promoted synergistically increased expression of wound-associated markers (e.g., S100A8, TGFβ, and CCN2) suggesting potential benefit of increased inflammatory response from reduced TNIP1 protein. Unexpectedly, poly (I:C) challenge of TNIP1-deficient cells restricted reepithelialization and reduced cell viability. In these cells, there was not only increased expression for genes associated with inflammasome assembly (e.g., ASC, procaspase 1) but also for A20, a TNIP1 partner protein that represses cell-death signaling. Despite this possibly compensatory increase in A20 mRNA, there was a decrease in phospho-A20 protein, the form necessary for quenching inflammation. Hyperresponsiveness to poly (I:C) in TNIP1-deficient keratinocytes was in part mediated through p38 and JNK pathways. Taken together, we conclude that TNIP1 deficiency promotes enhanced expression of factors associated with promoting wound healing. However, the coupled, increased potential priming of the inflammasome and reduced compensatory activity of A20 has a net negative effect on overall cell recovery potential manifested by poor reepithelialization and viability. These findings suggest a previously unrecognized role for TNIP1 protein in limiting inflammation during successful progression through early wound healing stages.

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Increased expression of uPA, uPAR, and PAI-1 in psoriatic skin and in basal cell carcinomas

Cited by 35 publications

References 69 publications

SuPAR, an emerging biomarker in kidney and inflammatory diseases

SuPAR, an emerging biomarker in kidney and inflammatory diseases

Reduced humidity induces skin barrier dysfunction and secretion of dipeptidyl peptidase-4 (DPP-4) in a skin-equivalent model

Enhanced Wound Healing- and Inflammasome-Associated Gene Expression in TNFAIP3-Interacting Protein 1- (TNIP1-) Deficient HaCaT Keratinocytes Parallels Reduced Reepithelialization

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