Hypoxia inhibits TNF-α-induced TSLP expression in keratinocytes

Tashiro, Naoyuki; Segawa, Ryosuke; Tobita, Ryozo; Asakawa, Shuichi; Mizuno, Natsumi; Hiratsuka, Masahiro; Hirasawa, Noriyasu

doi:10.1371/journal.pone.0224705

Cited by 17 publications

(14 citation statements)

References 26 publications

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“…Furthermore, the results showed that the longer the prenatal hypoxia is, the higher the TNF value will be. It aligns with the previous research [19], [20], [21], revealing that hypoxia causes an increase in TNF [22], [23]. TNF-α is produced from various cells such as lymphoid cells, cardiac myocytes, activated macrophages, endothelial cells, mast cells, fibroblasts, neurons, and adipose tissue.…”

Section: Discussionsupporting

confidence: 91%

An Increase in TNF-α Levels in Fetus due to Prenatal Ischemic Hypoxia

Indriawati

Risdiana

Wibowo

2021

Open Access Maced J Med Sci

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BACKGROUND: Prenatal ischemic hypoxia can increase mortality and morbidity and affect the immune system. One of the immune responses is tumor necrosis factor-α (TNF-α) levels. However, the cellular mechanism of immune response abnormalities due to prenatal hypoxia remains unclear. An 11–17-day-old fetus is a sensitive period of neural development. Brain ischemia will cause cell dysfunction and can even affect TNF-α levels. Thus, how prenatal ischemic hypoxia increases TNF-α levels in the fetus remains unclear. AIM: This study aims to examine the effect of the onset and duration of prenatal ischemic hypoxia on TNF-α levels. METHODOLOGY: An experimental study with a post-test control design was conducted. Thirty Rattus norvegicus were induced with prenatal ischemic hypoxia (embryos aged 7, 12, and 17 days). The independent variable was prenatal ischemic hypoxia, while the dependent variable was TNF-α levels. TNF-α was measured using the ELISA technique and was carried out when the fetus was 19 days old (E19). The TNF-α was analyzed using ANOVA, and the limit of significance was set at p < 0.05. RESULTS: The TNF-α levels in the prenatal ischemic hypoxia group were statistically higher than in the control group (p < 0.05). The more the onset and the longer the ischemic hypoxia is, the higher the TNF-level (p < 0.05). CONCLUSION: The prenatal ischemic hypoxia increased TNF-α levels in the fetus.

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Section: Discussionsupporting

confidence: 91%

An Increase in TNF-α Levels in Fetus due to Prenatal Ischemic Hypoxia

Indriawati

Risdiana

Wibowo

2021

Open Access Maced J Med Sci

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“…This finding is unusual, considering that, at least some cytokines, appear to be more prominently represented in the acute phase of Pso rather than AD [ 34 ]., AD has been thoroughly studied in relation to both types of dermatoses, but Pso might represent an interesting field of study. In particular, the role of TNF-alpha should be evaluated, since TSLP appears to be conducive to an increase in TNF-alpha activity [ 35 , 37 ] and several molecules have been used so far to treat Pso by targeting TNF-alpha [ 63 ]. It is plausible to suggest that, since TNF-alpha treatments could lead to several side effects, including the development of new Pso lesions [ 64 ], targeting a molecule down the same pathway, in this case TSLP, could lead to better results in terms of skin clearance and less side effects.…”

Section: Discussionmentioning

confidence: 99%

“…Tashiro et al, using cultures of HaCaT cells (immortalized keratinocytes), found that TSLP, in hypoxic conditions, presents reduced levels via the inactivation of its production stimulated by TNF-alpha, via HIF2 and HRE mechanisms (two products involved in the skin response to hypoxemia). It is the authors’ suggestion that targeting these two molecules could lead to lower levels of TSLP and the resolution of lesions both in Pso and AD [ 37 ]. Schaper et al correlated the levels of TSLP from human skin samples derived from healthy controls, Pso patients and AD patients, noticing that both Pso and AD patients, but mostly Pso patients, presented higher levels of TSLP, especially the inflammation-related isoform rather than the basal one, via histamine release by hyper-active Th2 cells [ 34 ].…”

Section: Psoriasis: Role Of Epithelium Derived Cytokines In Skin Damagementioning

confidence: 99%

Role of Epithelium-Derived Cytokines in Atopic Dermatitis and Psoriasis: Evidence and Therapeutic Perspectives

et al. 2021

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Atopic dermatitis and psoriasis are two of the most common chronic skin conditions. Current target therapies represent viable and safe solutions for the most severe cases of these two dermatoses but, presently, several limitations exist in terms of efficacy and side effects. A new class of products, epithelium-derived cytokines (TSLP, IL-25, IL-33), show an increasing potential for use in target therapy for these patients, and demonstrate a direct link between a generalized inflammatory and oxidative stress status and the human skin. A review was conducted to better understand their role in the aforementioned conditions. Of these three molecules, TSLP led has been most often considered in studies regarding target therapies, and most of the results in the literature are related to this cytokine. These three cytokines share common stimuli and are linked to each other in both acute and chronic phases of these diseases, and have been challenged as target therapies or biomarkers of disease activity. The results lead to the conclusion that epithelium-derived cytokines could represent a therapeutic opportunity for these patients, especially in itch control. Furthermore, they might work better when paired together with currently available therapies or in combination with in-development treatments. Further studies are needed in order to verify the efficacy and safety of the biologic treatments currently under development.

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“…HIF‐1α potentiates macrophage‐mediated immunity against L major and L amazonensis 89,90 . Hypoxia suppresses the expression of TSLP (a TH2 cell enhancer) in keratinocytes 91 . The wound healing is impaired in aged mice losing HIF‐1α in their keratinocytes 87 .…”

Section: Discussionmentioning

confidence: 99%

Immunological role of keratinocytes in leishmaniasis

Jafarzadeh

Nair²,

Jafarzadeh

et al. 2021

Parasite Immunology

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Following inoculation of Leishmania, a protozoan parasite, into the skin of a mammal, the epidermal keratinocytes recognize the parasite and influence the local immune response that can give rise to different outcomes of leishmaniasis. The early keratinocyte‐derived cytokines and keratinocytes‐T cells interactions shape the anti‐leishmanial immune responses that contribute to the resistance or susceptibility to leishmaniasis. The keratinocyte‐derived cytokines can directly potentiate the leishmanicidal activity of monocytes and macrophages. As keratinocytes express MHC‐II and enhance the expression of costimulatory molecules, these cells act as antigen‐presenting cells (APCs) in cutaneous leishmaniasis (CL). Depending on the epidermal microenvironment, the keratinocytes induce various types of effector CD4+ T cells. Keratinocyte apoptosis and necrosis have been also implicated in ulceration in CL. Further, keratinocytes contribute to the healing of Leishmania‐related cutaneous wounds. However, keratinocyte‐derived IL‐10 may play a key role in the development of post‐kala‐azar dermal leishmaniasis (PKDL). In this review, a comprehensive discussion regarding the multiple roles played by keratinocytes during leishmaniasis was provided, while highlighting novel insights concerning the immunological and pathological roles of these cells.

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Hypoxia inhibits TNF-α-induced TSLP expression in keratinocytes

Cited by 17 publications

References 26 publications

An Increase in TNF-α Levels in Fetus due to Prenatal Ischemic Hypoxia

An Increase in TNF-α Levels in Fetus due to Prenatal Ischemic Hypoxia

Role of Epithelium-Derived Cytokines in Atopic Dermatitis and Psoriasis: Evidence and Therapeutic Perspectives

Immunological role of keratinocytes in leishmaniasis

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