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Experimental dermatology 34(3) e70074 2025年3月Ikaros, which is encoded by the Ikaros family zinc finger 1 (IKZF1) gene, is a zinc finger transcription factor. We have previously generated K5-Ikzf1-EGFP transgenic mice (Ikzf1 Tg) by introducing the IKZF1 isoform into epithelial cells expressing keratin 5, which develop patchy alopecia. However, there has been no detailed in vivo investigation of the function of IKZF1 in alopecia or of Ikaros expression in hair follicles of alopecia patients. Our aim was to investigate whether IKZF1 overexpression is involved in the pathogenesis of alopecia areata (AA) using Ikzf1 Tg and to examine Ikaros expression in human scalp skin. We grossly and histologically examined the alopecic lesions of Ikzf1 Tg and the skin of wild-type (WT) mice and the associated mRNA expression of inflammatory mediators. We also examined Ikaros' expression in human scalp skin. Grossly and histologically, we found that the Ikzf1 Tg developed AA-like lesions. Immunohistochemically, the hair follicles of the Ikzf1 Tg expressed high levels of the NKG2D ligand H60 and contained infiltrating CD8+NKG2D+ T cells. Interleukin 15, tumour necrosis factor-α, CXC chemokine ligand (Cxcl)1, Cxcl10, Cxcl11, signal transducer and activator of transcription (STAT)1, STAT3, Janus kinase (JAK)1 and JAK3 mRNA expression were significantly higher in the alopecic lesions of the Ikzf1 Tg than in the WT mice. Ikzf1 Tg given corticosteroid injections exhibited hair regrowth. Immunohistochemical analysis of scalp hair follicles showed that Ikaros was more highly expressed in AA patients than in non-AA controls. Our study suggests that IKZF1 and Ikaros are involved in the pathogenesis of AA.
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Experimental dermatology 34(2) e70064 2025年2月Atopic dermatitis (AD) is a common skin disease. Although AD pathogenesis has been widely researched, inhibitory mechanisms in AD are still unclear. Sialic acid-binding immunoglobulin-like lectins (Siglecs) are a family of receptors recognising sialic acids; most Siglecs work as inhibitory receptors. Among Siglecs, Siglec-E is expressed on dendritic cells (DCs) and eosinophils, important immune cells in AD. Although Siglec-E inhibits Type 1 inflammatory diseases, how it influences AD is unknown. Thus, we investigated the role of Siglec-E in AD mouse model by using Siglec-E knockout (KO) mice. We demonstrated that Siglec-E attenuated AD-like inflammation of mice caused by topical application of MC903 on ear skin (MC903-induced AD). To reveal the role of Siglec-E in MC903-induced AD, we focused on Siglec-E on DCs and eosinophils. We first showed that Sigle-E was expressed on cutaneous DCs and migratory DCs of draining lymph nodes. Moreover, OX40L expression on cutaneous DCs was reduced in the presence of Siglec-E. In vitro experiments using cultured spleen DCs (SpDCs), highly expressing Siglec-E, revealed that IL-33 was involved in the induction of Siglec-E and confirmed that Siglec-E inhibited OX40L expression on SpDCs induced by IL-33. Moreover, CD4+ T cell-SpDC coculture revealed that Siglec-E inhibited Th2 polarisation under IL-33 stimulation. We finally revealed that Siglec-E was expressed on eosinophils and reduced the eosinophils infiltration to the MC903-treated ear skin with the suppression of CD49d, a necessary integrin for eosinophil migration to skin tissue [1], expression on eosinophils. These findings elucidated the inhibitory role of Siglec-E in MC903-induced AD.
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The journal of allergy and clinical immunology. Global 3(4) 100317-100317 2024年11月BACKGROUND: Atopic dermatitis (AD) is a common chronic eczematous skin disease with severe pruritus. Several new therapeutic agents for AD such as dupilumab, an anti-IL-4Rα antibody, have been developed in recent years. We need to predict which agent is the best choice for each patient, but this remains difficult. OBJECTIVE: Our aim was to examine clinical background factors and baseline biomarkers that could predict the achievement of improved clinical outcomes in patients with AD treated with dupilumab. METHODS: A multicenter, prospective observational study was conducted on 110 patients with AD. The Eczema Area and Severity Index was used as an objective assessment, and the Patient-Oriented Eczema Measure and Numerical Rating Scale for Pruritus were used as patient-reported outcomes. In addition, some clinical background factors were evaluated. RESULTS: The achievement of an absolute Eczema Area and Severity Index of 7 or less was negatively associated with current comorbidity of food allergy and baseline serum lactate dehydrogenase (LDH) levels. There were negative associations between achievement of a Patient-Oriented Eczema Measure score of 7 or less and duration of severe AD and between achievement of an itching Numerical Rating Scale for Pruritus score of 1 or less and current comorbidity of allergic conjunctivitis or baseline serum periostin level. Furthermore, signal detection analysis showed that a baseline serum LDH level less than 328 U/L could potentially be used as a cutoff value for predicting the efficacy of dupilumab. CONCLUSION: Baseline biomarkers such as LDH and periostin and clinical background factors such as current comorbidity of food allergy and a long period of severe disease may be useful indicators when choosing dupilumab for systemic treatment for AD, as they can predict the efficacy of dupilumab.
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Experimental dermatology 33(11) e70015 2024年11月Platelet-activating factor (PAF) is an important chemical mediator in the field of inflammation, but its function in the skin is unclear. To unravel the role of PAF, we focused on lysophosphatidylcholine acyltransferase 2 (LPCAT2 also called LPLAT9), a biosynthetic enzyme involved in PAF production, and investigated the role of PAF in allergic contact dermatitis (ACD) and irritant contact dermatitis (ICD). We measured the amount of PAF in the skin and investigated the ear swelling responses and leukocyte infiltration into the skin following the application of 2,4,6-trinitro-1-chlorobenzene (TNCB) or croton oil in wild-type (WT) and LPCAT2 knockout (LPCAT2-KO) mice. The amount of PAF was increased in the skin of WT mice after TNCB or croton oil application but not detected in LPCAT2-KO mice. The ear swelling response was decreased in LPCAT2-KO mice compared with that in WT mice. In the ACD model, the numbers of lymphocytes, eosinophils, macrophages, mast cells and neutrophils were smaller in LPCAT2-KO mice than in WT mice. In the ICD model, the ear swelling response was also decreased in LPCAT2-KO mice compared with that in WT mice. When double staining of each inflammatory cell type and LPCAT2 was performed in ACD tissue, marked co-staining of the eosinophil marker and LPCAT2 was observed. In addition, LPCAT2 expression was observed in the epidermis. These results indicate that PAF is involved in the infiltration of several cell types into the sites of allergic and non-allergic skin inflammation. Furthermore, eosinophils and keratinocytes are primarily responsible for PAF production in skin inflammation.
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Contact dermatitis 91(3) 259-260 2024年9月
MISC
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Journal of Environmental Dermatology and Cutaneous Allergology 11(5) 452-452 2017年11月
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Journal of Environmental Dermatology and Cutaneous Allergology 11(5) 460-460 2017年11月
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Journal of Environmental Dermatology and Cutaneous Allergology 11(5) 470-470 2017年11月
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Journal of Environmental Dermatology and Cutaneous Allergology 11(4) 316-321 2017年10月
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皮膚科の臨床 59(9) 1431-1434 2017年8月症例は69歳男性で、皮膚生検で尋常性乾癬と診断され、以後約10年間にわたり近医内科でシクロスポリン250mg/日内服およびステロイド外用の治療を継続していた。特にこの間、シクロスポリンの血中濃度のモニタリングなどはされていなかった。初診の19日前より皮疹の増悪傾向が続くため、当科を受診した。検査所見より腎機能障害を認め、シクロスポリンが原因と考え内服を中止した。中止10日目頃より、全身に紅斑および浮腫が拡大し、緊満性水疱が出現したため、内服中止20日後に入院した。ほぼ全身に浸潤を触れる浮腫性紅斑、上肢に緊満性の水疱を認めた。臨床経過および検査所見より、尋常性乾癬に併発した水疱性類天疱瘡と診断した。入院初日よりプレドニゾロン、ベタメタゾン酪酸エステルプロピオン酸エステル軟膏の外用を開始した。水疱の新生を認め、ドキシサイクリン、ニコチン酸アミドの内服を開始したところ、水疱の新生はなく、皮疹も軽快した。
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アレルギー 66(4-5) 576-576 2017年5月
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皮膚科の臨床 59(1) 26-29 2017年1月26歳男。全身に多発する紅斑、色素沈着を主訴とした。20歳時より市販の頭痛薬を頓服しており、1年前より右上腕に続いて下顎、陰茎、臀部、下肢に赤褐色紅斑が多数出現した。3日前に市販の頭痛薬を内服したところ、服薬4時間後より皮疹の発赤が増強し、市販の頭痛薬による固定薬疹が考えられた。頓服歴のある市販薬とその成分についてオープンテストを行った結果、新セデス錠、ノーシンピュア、イブクイックとその共通成分であるアリルイソプロピルアセチル尿素で紅斑とそう痒が強く出現し、皮疹部のパッチテストでエテンザミドが陽性を示したことから、アリルイソプロピルアセチル尿素とエテンザミドによる固定薬疹と診断した。
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Journal of Environmental Dermatology and Cutaneous Allergology 10(4) 400-400 2016年10月
共同研究・競争的資金等の研究課題
10-
日本学術振興会 科学研究費助成事業 2024年4月 - 2027年3月
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日本学術振興会 科学研究費助成事業 基盤研究(C) 2021年4月 - 2024年3月
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日本学術振興会 科学研究費助成事業 基盤研究(C) 2018年4月 - 2021年3月
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日本学術振興会 科学研究費助成事業 基盤研究(C) 2018年4月 - 2021年3月
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日本学術振興会 科学研究費助成事業 基盤研究(C) 2015年4月 - 2018年3月