Methotrexate, but not narrowband ultraviolet B radiation, suppresses interleukin-33 mRNA levels in psoriatic plaques and protein levels in serum of patients with psoriasis
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Meephansan, Jitlada
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Subpayasarn, Urairack
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Ponnikorn, Saranyoo
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Chakkavittumrong, Panlop
[3
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Juntongjin, Premjit
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Komine, Mayumi
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Jichi Med Univ, Dept Dermatol, Shimotsuke, JapanThammasat Univ, Div Dermatol, Chulabhorn Int Coll Med, Rangsit Campus,99 Moo 18 Phahonyothin Rd, Klongluang 12120, Pathum Thani, Thailand
Komine, Mayumi
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Ohtsuki, Mamitaro
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Jichi Med Univ, Dept Dermatol, Shimotsuke, JapanThammasat Univ, Div Dermatol, Chulabhorn Int Coll Med, Rangsit Campus,99 Moo 18 Phahonyothin Rd, Klongluang 12120, Pathum Thani, Thailand
Interleukin (IL)-33 can function both as a conventional cytokine and as a nuclear factor regulating gene transcription. IL-33 expression is strongly upregulated in the nucleus of keratinocytes and serum of patients with psoriasis. However, the role of IL-33 in psoriasis is unclear, and IL-33 expression in the lesional psoriatic skin after conventional systemic treatments has not been investigated. In this study, we aimed to compare IL-33 mRNA in patients' lesional skin samples and IL-33 protein expression in patients' serum before and after treatment with methotrexate (MTX) and narrowband ultraviolet B (NB-UVB). IL-33 mRNA levels in lesional skin and IL-33 protein levels in serum were downregulated after treatment with MTX. Results revealed a significant decrease in IL-33 protein expression (P=0.028). IL-33 expression increased after NB-UVB treatment. IL-33 production is associated with inflammatory skin in psoriasis, possibly through its cytokine function. However, high expression of IL-33 after NB-UVB treatment suggests the occurrence of unknown functions to alleviate psoriatic lesions without IL-33 involvement.