研究者業績

杉浦 一充

スギウラ カズミツ  (Kazumitsu Sugiura)

基本情報

所属
藤田医科大学 医学部皮膚科学 教授
学位
医学(博士)(名古屋大学)

研究者番号
70335032
J-GLOBAL ID
200901045673927248
researchmap会員ID
6000004452

外部リンク

学歴

 2

委員歴

 15

主要な論文

 268
  • Yurie Hasegawa, Yohei Iwata, Hidehiko Fukushima, Yoshihito Tanaka, Soichiro Watanabe, Kenta Saito, Hiroyuki Ito, Mizuki Sugiura, Masashi Akiyama, Kazumitsu Sugiura
    Scientific reports 12(1) 13384-13384 2022年8月4日  査読有り最終著者責任著者
    Loss-of-function homozygous or compound heterozygous mutations in IL36RN, which encodes interleukin-36 receptor antagonist (IL-36Ra), have been implicated in the pathogenesis of skin disorders. We previously reported that Il36rn-/- mice exhibit an enhanced contact hypersensitivity (CHS) response through increased neutrophil recruitment. In addition, Il36rn-/- mice show severe imiquimod-induced psoriatic skin lesions and enhanced neutrophil extracellular trap (NET) formation. We hypothesized that NETs may play an important role in the CHS response. To confirm this, we examined the CHS response and NET formation in Il36rn-/- mice. Il36rn-/- mice showed enhanced CHS responses, increased infiltration of inflammatory cells, including neutrophils, CD4+ T cells, and CD8+ T cells, NET formation, and enhanced mRNA expression of cytokines and chemokines, including IL-1β, C-X-C motif chemokine ligand (CXCL)1, CXCL2, and IL-36γ. Furthermore, NET formation blockade improved the CHS response, which consequently decreased inflammatory cell infiltration and NET formation. Consistently, we observed decreased expression of these cytokines and chemokines. These findings indicate that IL-36Ra deficiency aggravates the CHS response caused by excessive inflammatory cell recruitment, NET formation, and cytokine and chemokine production, and that NET formation blockade alleviates the CHS response. Thus, NET formation may play a prominent role in the CHS response.
  • Hideaki Uchida, Masahiro Kamata, Shota Egawa, Mayumi Nagata, Saki Fukaya, Kotaro Hayashi, Atsuko Fukuyasu, Takamitsu Tanaka, Takeko Ishikawa, Takamitsu Ohnishi, Kazumitsu Sugiura, Yayoi Tada
    Journal of the American Academy of Dermatology 87(5) 1181-1184 2022年3月8日  査読有り
  • Y Tanaka, Y Iwata, K Saito, H Fukushima, S Watanabe, Y Hasegawa, M Akiyama, K Sugiura
    Journal of the European Academy of Dermatology and Venereology : JEADV 36(2) 295-304 2022年2月  査読有り最終著者責任著者
    BACKGROUND: Loss-of-function homozygous or compound heterozygous mutations in IL36RN, which encodes interleukin-36 receptor antagonist (IL-36Ra), has been implicated in the pathogenesis of skin disorders. However, the pathogenic role of IL-36Ra in cutaneous ischemia-reperfusion (I/R) injury remains unclear. OBJECTIVES: We investigated the role of IL36Ra in cutaneous I/R injury. METHODS: We examined I/R injury in Il36rn-/- mice. The area of wounds, numbers of infiltrated cells, apoptotic cells and neutrophil extracellular trap (NET) formation were assessed. The expression levels of various genes were analysed using real-time RT-PCR. The expression of high mobility group box 1 (HMGB1), an endogenous toll-like receptor (TLR) 4 ligand, was confirmed using immunohistology, and serum HMGB1 levels were measured by ELISA. Cytokine production by stimulated cultured J774A.1 and HaCaT cells was examined. RESULTS: IL-36Ra deficiency resulted in significantly delayed wound healing and increased neutrophil and macrophage infiltration into the wound tissues. Il36rn-/- mice had increased mRNA expression levels of CXCL1, CXCL2, CCL4, TNF-α, TGF-β, IL-1β, IL-6 and IL-36γ relative to wild-type mice. Apoptosis was identified in keratinocytes by TUNEL assay. HMGB1 expression in the I/R site was decreased in both keratinocytes and adnexal cells, while serum HMGB1 levels were significantly elevated after reperfusion. The mRNA levels of various cytokines, including IL-1β, were elevated in J774A.1 cells through TLR4 signalling by HMGB1 stimulation. In addition, HaCaT cells stimulated with IL-1β showed significantly increased CXCL1, TNF-α, IL-6, IL-36β and IL-36γ mRNA expression. Furthermore, NET formation was increased by IL-36Ra deficiency. Finally, either the blockade of TLR4 signalling by TAK-242 or inhibition of NET formation by Cl-amidine normalized exacerbated I/R injury in Il36rn-/- mice. CONCLUSIONS: This study indicated that IL-36Ra deficiency exacerbates cutaneous I/R injury due to excessive inflammatory cell recruitment, NET formation, and excessive cytokine and chemokine production via the TLR4 pathway by HMGB1 released from epidermal apoptotic cells.
  • Kazumitsu Sugiura
    Dermatology and therapy 12(2) 315-328 2022年2月  査読有り筆頭著者責任著者
    Generalised pustular psoriasis (GPP), a severe neutrophilic skin disease characterised by the sudden and widespread eruption of superficial sterile pustules, remains a challenging disease with limited treatment options. The recent discovery of genetic mutations associated with GPP and advances in understanding of the molecular mechanisms of autoinflammation have resulted in identification of key cytokines that drive the development and progression of GPP. Accumulating evidence demonstrates that interleukin (IL)-36 acts as a central node cytokine by orchestrating the hyperactivation of key pro-inflammatory cytokines and stimulating immune cells, including neutrophilic accumulations, a unique feature of GPP skin lesions. These findings are paving the way for the discovery and development of novel targeted GPP therapeutics that block the IL-36 pathway and neutralise the pathogenic immunologic mechanisms and pro-inflammatory cytokines. This article provides an overview of the current evidence that supports the role of IL-36 as a central node cytokine in GPP pathogenesis.
  • Takuya Takeichi, John Y W Lee, Yusuke Okuno, Yuki Miyasaka, Yuya Murase, Takenori Yoshikawa, Kana Tanahashi, Emi Nishida, Tatsuya Okamoto, Komei Ito, Yoshinao Muro, Kazumitsu Sugiura, Tamio Ohno, John A McGrath, Masashi Akiyama
    Frontiers in immunology 12 737747-737747 2021年  査読有り
    Heterozygous mutations in JAK1 which result in JAK-STAT hyperactivity have been implicated in an autosomal dominant disorder that features multi-organ immune dysregulation. This study identifies another previously unreported heterozygous missense JAK1 mutation, H596D, in an individual with a unique autoinflammatory keratinization disease associated with early-onset liver dysfunction and autism. Using CRISPR-Cas9 gene targeting, we generated mice with an identical Jak1 knock-in missense mutation (Jak1 H595D/+;I596I/+;Y597Y/+ mice) that recapitulated key aspects of the human phenotype. RNA sequencing of samples isolated from the Jak1 H595D/+;I596I/+;Y597Y/+ mice revealed the upregulation of genes associated with the hyperactivation of tyrosine kinases and NF-κB signaling. Interestingly, there was a strong correlation between genes downregulated in Jak1 H595D/+;I596I/+;Y597Y/+ mice and those downregulated in the brain of model mice with 22q11.2 deletion syndrome that showed cognitive and behavioral deficits, such as autism spectrum disorders. Our findings expand the phenotypic spectrum of JAK1-associated disease and underscore how JAK1 dysfunction contributes to this autoinflammatory disorder.
  • Soichiro Watanabe, Yohei Iwata, Hidehiko Fukushima, Kenta Saito, Yoshihito Tanaka, Yurie Hasegawa, Masashi Akiyama, Kazumitsu Sugiura
    Scientific reports 10(1) 20149-20149 2020年11月19日  査読有り最終著者責任著者
    Loss-of-function mutations in the interleukin (IL)-36 gene IL36RN are associated with psoriasis. The importance of neutrophil extracellular traps (NETs), web-like structures composed of neutrophil DNA, in the pathogenesis of psoriasis has been unclear. Here, we aimed to clarify the role of NET signaling in the deficiency of IL36 receptor antagonist (DITRA). We evaluated the severity of psoriasis-like lesions induced by imiquimod cream treatment in Il36rn-/- mice. The mRNA levels of psoriasis-related cytokines were measured via real-time reverse transcription polymerase chain reaction, and the effects of Cl-amidine, a peptidyl arginine deiminase 4 (PAD4) inhibitor, on psoriasis-like lesions were evaluated. PAD4 is a histone-modifying enzyme that is involved in NET formation. Psoriasis area and severity index scores, epidermal thickness, and infiltrated neutrophil counts were significantly increased in Il36rn-/- mice; NET formation was confirmed pathologically. Several cytokines and chemokines were upregulated in the skin lesions of Il36rn-/- mice and Cl-amidine treatment improved these psoriasis-like lesions. These results suggest that NET formation plays an important role in the pathology of psoriasis-like lesions in these mice and might represent a promising therapeutic target for DITRA.
  • Kenta Saito, Yohei Iwata, Hidehiko Fukushima, Soichiro Watanabe, Yoshihito Tanaka, Yurie Hasegawa, Masashi Akiyama, Kazumitsu Sugiura
    Scientific reports 10(1) 14772-14772 2020年9月8日  査読有り最終著者責任著者
    Loss-of-function homozygous or compound heterozygous mutations in IL36RN, which encodes interleukin-36 receptor antagonist (IL-36Ra), have been implicated in the pathogenesis of various skin disorders. Previous findings showed that IL-36γ promoted wound healing in mice; however, the pathogenic role of IL-36Ra in wound healing remains unclear. We elucidated the role of IL-36Ra, a regulator of IL-36 in tissue repair by investigating the recruitment of inflammatory cells and cytokine production in the absence of IL-36Ra. Full-thickness excisional wounds were made on the back of Il36rn-/- mice and healing was assessed by monitoring macroscopic wound sizes, numbers of infiltrated cells, and gene expression of inflammatory cytokines. Macroscopic wound healing, re-epithelialization, and granulation tissue formation were delayed by 3 days post-injury in Il36rn-/- mice. This delay was associated with increased infiltrations of neutrophils and macrophages, and increased expression of cytokines, such as IL-36γ, C-X-C motif chemokine ligand 1 (CXCL1), and transforming growth factor (TGF)-β. Importantly, administration of TAK-242, a toll-like receptor 4 (TLR4) inhibitor, caused normalization of wound healing in Il36rn-/- mice, abrogating the initial delay in tissue repair. These results showed that targeting TLR4- mediated infiltrations of immune cells and cytokine production could be beneficial in regulating wound healing in IL-36Ra-deficient skin disorders.
  • Tomoki Taki, Kana Tanahashi, Takuya Takeichi, Takenori Yoshikawa, Yuya Murase, Kazumitsu Sugiura, Masashi Akiyama
    JAMA dermatology 156(10) 1030-1032 2020年7月15日  査読有り
    This nonrandomized clinical trial evaluates the association of topical minoxidil with hypotrichosis in patients with autosomal recessive woolly hair/hypotrichosis carrying LIPH pathogenic variants.
  • Mayumi Nagata, Masahiro Kamata, Saki Fukaya, Kotaro Hayashi, Atsuko Fukuyasu, Takamitsu Tanaka, Takeko Ishikawa, Takamitsu Ohnishi, Kazumitsu Sugiura, Yayoi Tada
    Journal of the American Academy of Dermatology 82(3) 758-761 2020年3月  査読有り
  • Hidehiko Fukushima, Yohei Iwata, Soichiro Watanabe, Kenta Saito, Yoshihito Tanaka, Yurie Hasegawa, Masashi Akiyama, Kazumitsu Sugiura
    Scientific reports 10(1) 734-734 2020年1月20日  査読有り最終著者責任著者
    Loss-of-function mutations in IL36RN cause generalized pustular psoriasis (GPP), which is characterized by neutrophil-infiltrated lesions. Neutrophils are important during contact hypersensitivity in mice. However, it has never been determined whether interleukin-36 receptor antagonist (IL-36Ra) deficiency is an exacerbating factor in contact dermatitis. We examined whether a loss-of-function IL36RN mutation exacerbates contact dermatitis and evaluated the changes in contact dermatitis-related cytokines. Wild-type and Il36rn-/- mice were treated with 1-fluoro-2,4-dinitorobenzene (DNFB) and evaluated for ear thickness, histopathological features, numbers of infiltrated neutrophils, and numbers of CD4 + and CD8 + T cells. Furthermore, mRNA levels of contact dermatitis-related cytokines were measured by real-time polymerase chain reaction, and effects of TAK-242, a toll-like receptor 4 (TLR4) inhibitor, on the contact hypersensitivity (CHS) response were evaluated. We found that the ear thickness, cytokine expression, and neutrophil infiltration significantly increased in Il36rn-/- mice compared with that in wild-type mice. TAK-242 alleviated CHS and prevented neutrophil infiltration, cytokine expression, and ear thickening in Il36rn-/- mice. These data indicate that Il36rn-/- mutations are an exacerbating factor for CHS and that TAK-242 can reduce the inflammatory responses that are associated with the CHS response.
  • Masashi Akiyama, Valerio De Vita, Kazumitsu Sugiura
    Frontiers in immunology 11 1753-1753 2020年  査読有り最終著者
  • Fukushima H, Iwata Y, Numata S, Saito K, Watanabe S, Kobayashi T, Sugiura K
    The Journal of dermatology 46(8) e301-e302 2019年3月  査読有り最終著者
  • T Takeichi, K Sugiura, K Tanahashi, K Noda, M Kono, M Akiyama
    The British journal of dermatology 179(5) 1210-1211 2018年11月  査読有り
  • M Kono, M Akiyama, Y Inoue, T Nomura, A Hata, Y Okamoto, T Takeichi, Y Muro, W H I McLean, H Shimizu, K Sugiura, Y Suzuki, N Shimojo
    The British journal of dermatology 179(1) 190-191 2018年7月  査読有り
  • Masashi Akiyama, Takuya Takeichi, John A McGrath, Kazumitsu Sugiura
    Journal of dermatological science 90(2) 105-111 2018年5月  査読有り最終著者
    Classifying inflammatory skin diseases is challenging, especially for the expanding group of disorders triggered by genetic factors resulting in hyperactivated innate immunity that result in overlapping patterns of dermal and epidermal inflammation with hyperkeratosis. For such conditions, the umbrella term "autoinflammatory keratinization diseases" (AIKD) has been proposed. AIKD encompasses diseases with mixed pathomechanisms of autoinflammation and autoimmunity, and includes IL-36 receptor antagonist (IL-36Ra)-related pustulosis, CARD14-mediated pustular psoriasis, pityriasis rubra pilaris (PRP) type V, and familial keratosis lichenoides chronica (KLC). Mechanistically, the entities include generalized pustular psoriasis (GPP) without psoriasis vulgaris, impetigo herpetiformis and acrodermatitis continua, which are IL-36Ra-related pustuloses caused by loss-of-function mutations in IL36RN; GPP with psoriasis vulgaris and palmoplantar pustular psoriasis which are CARD14-mediated pustular psoriasiform dermatoses with gain-of-function variants of CARD14; PRP type V which is caused by gain-of-function mutations in CARD14; and, familial KLC in which mutations in NLRP1, an inflammasome sensor protein predominantly expressed in skin, have been identified. It is likely that further inflammatory keratinization disorders will also fall within the concept of AIKD, as elucidation of novel pathogenic mechanisms of inflammatory keratinization diseases emerges. A better understanding of the pathophysiology of AIKD is likely to lead to innovative, targeted therapies that benefit patients.
  • Masashi Akiyama, Takuya Takeichi, John A. McGrath, Kazumitsu Sugiura
    JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY 140(6) 1545-1547 2017年12月  査読有り最終著者
  • T. Takeichi, A. Kobayashi, E. Ogawa, Y. Okuno, S. Kataoka, M. Kono, K. Sugiura, R. Okuyama, M. Akiyama
    BRITISH JOURNAL OF DERMATOLOGY 177(4) E133-E135 2017年10月  査読有り
  • T. Takeichi, T. Nomura, H. Takama, M. Kono, K. Sugiura, D. Watanabe, H. Shimizu, M. A. Simpson, J. A. McGrath, M. Akiyama
    BRITISH JOURNAL OF DERMATOLOGY 177(3) E62-E64 2017年9月  査読有り
  • Akitaka Shibata, Kazumitsu Sugiura, Yasuhide Furuta, Yoshiko Mukumoto, Osamu Kaminuma, Masashi Akiyama
    JOURNAL OF AUTOIMMUNITY 80 28-38 2017年6月  査読有り責任著者
    Background: IL36RN encodes the IL-36 receptor antagonist (IL-36Ra), and loss-of-function mutations in IL36RN define a recessively inherited autoinflammatory disease named "deficiency of IL-36Ra" (DITRA). DITRA causes systemic autoinflammatory diseases, including generalized pustular psoriasis (GPP), an occasionally life-threatening disease that is characterized by widespread sterile pustules on the skin, fever and other systemic symptoms. GPP can present at any age, and provocative factors include various infections, medicines and pregnancy. Objective: We aimed to elucidate the role of toll-like receptor 4 (TLR4) signaling in DITRA and to innovate an efficient treatment for DITRA. Methods: We generated Il36rn(-/-) mice and treated them with TLR4 agonist to establish DITRA model mice. Furthermore, we administrated TLR4 antagonist TAK-242 to the model mice to inhibit the DITRA symptoms. Result: II36rn-1 mice treated by TLR4 agonist showed autoinflammatory symptoms in skin, articulation and liver. Thus, we established model mice for DITRA or GPP that show cutaneous, articular, and hepatic autoinflammatory symptoms typical of DITRA or GPP: sterile pustules on the skin, liver abscesses and enthesitis of the hind paws. Additionally, these symptoms were canceled by TAK-242 administration. We demonstrated the inhibitory effects of the TLR4 antagonist TAK-242 on the autoinflammatory symptoms exhibited by the DITRA models. Conclusion: We suggested that blockage of TLR4 signaling is a promising treatment for DITRA and GPP. (C) 2017 Elsevier Ltd. All rights reserved.
  • Takuya Takeichi, Kazumitsu Sugiura, Toshifumi Nomura, Taiko Sakamoto, Yasushi Ogawa, Naoki Oiso, Yuko Futei, Aki Fujisaki, Akiko Koizumi, Yumi Aoyama, Kimiko Nakajima, Yutaka Hatano, Kei Hayashi, Akemi Ishida-Yamamoto, Sakuhei Fujiwara, Shigetoshi Sano, Keiji Iwatsuki, Akira Kawada, Yasushi Suga, Hiroshi Shimizu, John A. McGrath, Masashi Akiyama
    JAMA DERMATOLOGY 153(1) 66-70 2017年1月  査読有り
    IMPORTANCE We found CARD14 mutations (2 de novo novel mutations and another previously reported mutation) in 3 of 3 patients with pityriasis rubra pilaris (PRP) type V, but not in patients with PRP of other types. Our findings, combined with the published literature, suggest that type V PRP, both familial and sporadic, can be caused by CARD14 mutations. Detailed clinical observation revealed that all 3 patients displayed unique patchy macular brown hyperpigmentation. OBJECTIVE To further determine how often patients with PRP have pathogenic mutations in CARD14 and to elucidate which clinical subtype of PRP is caused by CARD14 mutations. DESIGN, SETTING, AND PARTICIPANTS We sequenced the entire coding regions of CARD14 in genomic DNA from patients with 5 clinical subtypes of PRP. The detailed clinical features were analyzed in all the patients. The pathogenicity of each mutation was evaluated by several computational predictions. PRP was classified into 6 subgroups, types I to VI, based on clinical criteria. We categorized all the patients with PRP into the clinical subtypes using the classic PRP classification; 22 cases of PRP with varying subtypes were studied. MAIN OUTCOMES AND MEASURES The prevalence of CARD14 mutations in each subtype of PRP was evaluated. Clinical features and characteristics of patients with PRP with CARD14 mutations were analyzed. RESULTS Overall 22 patients with PRP were included in our study (12 men, 10 women; mean [SD] age, 26 [18] years). Among 3 patients with PRP type V, all were found to have CARD14 mutations: 2 de novo novel mutations (p. Cys127Ser and p. Gln136Leu), and another previously reported mutation (p. Gly117Ser). All were close to the reported pathogenic domains. In silico analysis of all 3 mutations suggested that they are functionally relevant to pathogenesis. All 3 patients displayed unique patchy macular brown hyperpigmentation additionally to other typical features of PRP. Patients with PRP type I and type IV, 1 patient each, had the rare variants in CARD14. CONCLUSIONS AND RELEVANCE Pityriasis rubra pilaris type V is a distinct variant of PRP that is caused by CARD14 mutations. In addition, a rare variant of CARD14 might also be implicated in the pathophysiology of other forms of PRP.
  • Takuya Takeichi, Yaei Togawa, Yusuke Okuno, Rieko Taniguchi, Michihiro Kono, Hiroyuki Matsue, Kazumitsu Sugiura, Masashi Akiyama
    JOURNAL OF DERMATOLOGICAL SCIENCE 85(1) 58-60 2017年1月  査読有り
  • K. Sugiura, K. Endo, T. Akasaka, M. Akiyama
    JOURNAL OF THE EUROPEAN ACADEMY OF DERMATOLOGY AND VENEREOLOGY 29(10) 2054-2056 2015年10月  査読有り筆頭著者責任著者
  • K. Tanahashi, K. Sugiura, M. Akiyama
    BRITISH JOURNAL OF DERMATOLOGY 173(3) 865-866 2015年9月  査読有り
  • Kazumitsu Sugiura, Ayaka Nakasuka, Hiroaki Kono, Michihiro Kono, Masashi Akiyama
    JOURNAL OF DERMATOLOGICAL SCIENCE 79(3) 319-320 2015年9月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Masashi Akiyama
    JOURNAL OF DERMATOLOGICAL SCIENCE 79(1) 4-9 2015年7月  査読有り筆頭著者
    Research on the molecular genetics and pathomechanisms of autosomal recessive congenital ichthyosis (ARCI) has advanced considerably and several causative genes and molecules underlying the disease have been identified. Three major ARCI phenotypes are harlequin ichthyosis (HI), lamellar ichthyosis (LI), and congenital ichthyosiform erythroderma (CIE): Skin barrier defects are involved in the pathogenesis of ARCI. In this review, the causative genes of ARCI and its phenotypes as well as recent advances in the field are summarized. The known causative molecules underlying ARCI include ABCA12, TGM1, ALOXE3, ALOX12B, NIPAL4, CYP4F22, PNPLA1, CERS3, and LIPN. It is important to examine genetic associations and to elucidate the pathomechanisms of ARCI to establish effective therapies and beneficial genetic counseling. Next-generation sequencing is a promising method that enables the detection of causative disease mutations, even in cases of unexpected concomitant genetic diseases. For genetic diagnosis, obtaining mRNA from hair follicle epithelial cells, which are analogous to keratinocytes in the interfollicular epidermis, is convenient and minimally invasive in patients with ARCI. We confirmed that our mRNA analysis method using hair follicle samples can be applied not only to keratinization disorders, but also to other genetic diseases in the dermatology field. Studies that suggest potential next-generation therapies using ARCI model mice are also reviewed. (C) 2015 Japanese Society for Investigative Dermatology. Published by Elsevier Ireland Ltd. All rights reserved.
  • K. Sugiura, M. Arima, K. Matsunaga, M. Akiyama
    BRITISH JOURNAL OF DERMATOLOGY 173(1) 309-311 2015年7月  査読有り
  • Kazumitsu Sugiura, Toshiyuki Kitoh, Daisuke Watanabe, Masahiko Muto, Masashi Akiyama
    RHEUMATOLOGY 54(1) 197-199 2015年1月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Masashi Akiyama
    ACTA DERMATO-VENEREOLOGICA 95(7) 858-859 2015年  査読有り筆頭著者
  • K. Sugiura, K. Haruna, Y. Suga, M. Akiyama
    JOURNAL OF THE EUROPEAN ACADEMY OF DERMATOLOGY AND VENEREOLOGY 28(12) 1835-1836 2014年12月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Ryuhei Uchiyama, Ryuhei Okuyama, Masashi Akiyama
    JOURNAL OF THE AMERICAN ACADEMY OF DERMATOLOGY 71(5) E216-E218 2014年11月  査読有り
  • Kazumitsu Sugiura, Naoki Oiso, Shin Iinuma, Hiromasa Matsuda, Masako Minami-Hori, Akemi Ishida-Yamamoto, Akira Kawada, Hajime Iizuka, Masashi Akiyama
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 134(9) 2472-2474 2014年9月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Yasushi Suga, Masashi Akiyama
    JOURNAL OF DERMATOLOGICAL SCIENCE 75(3) 199-201 2014年9月  査読有り筆頭著者
  • Kazumitsu Sugiura, Yoshinao Muro, Masashi Akiyama
    ARTHRITIS & RHEUMATOLOGY 66(9) 2648-2648 2014年9月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Masahiko Muto, Masashi Akiyama
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 134(6) 1755-1757 2014年6月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura
    JOURNAL OF DERMATOLOGICAL SCIENCE 74(3) 187-192 2014年6月  査読有り筆頭著者責任著者
    Generalized pustular psoriasis (GPP) is often present in patients with existing or prior psoriasis vulgaris (PV; "GPP with PV"). However, cases of GPP have been known to arise without a history of PV ("GPP alone"). There has long been debate over whether GPP alone and GPP with PV are distinct subtypes that are etiologically different from each other. We recently reported that the majority of GPP alone cases is caused by recessive mutations of IL36RN. In contrast, only a few exceptional cases of GPP with PV were found to have recessive IL36RN mutations. Very recently, we also reported that CARD14 p.Asp176His, a gain-of-function variant, is a predisposing factor for GPP with PV; in contrast, the variant is not associated with GPP alone in the Japanese population. These results suggest that GPP alone is genetically different from GPP with PV. IL36RN mutations are also found in some patients with severe acute generalized exanthematous pustulosis, palmar-plantar pustulosis, and acrodermatitis continua of hallopeau. CARD14 mutations and variants are causal or disease susceptibility factors of PV, GPP, or pityriasis rubra pilaris, depending on the mutation or variant position of CARD14. It is clinically important to analyze IL36RN mutations in patients with sterile pustulosis. For example, identifying recessive IL36RN mutations leads to early diagnosis of GPP, even at the first episode of pustulosis. In addition, individuals with IL36RN mutations are very susceptible to GPP or GPP-related generalized pustulosis induced by drugs (e.g., amoxicillin), infections, pregnancy, or menstruation. (C) 2014 Japanese Society for Investigative Dermatology. Published by Elsevier Ireland Ltd. All rights reserved.
  • Kazumitsu Sugiura, Naoki Oiso, Akira Kawada, Masashi Akiyama
    JOURNAL OF THE AMERICAN ACADEMY OF DERMATOLOGY 70(3) E51-E52 2014年3月  査読有り筆頭著者
  • Kazumitsu Sugiura, Yukiko Shoda, Masashi Akiyama
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 134(2) 578-579 2014年2月  査読有り筆頭著者責任著者
  • Kayo Yasuda, Kazumitsu Sugiura, Takuya Takeichi, Yasushi Ogawa, Yoshinao Muro, Masashi Akiyama
    EXPERIMENTAL DERMATOLOGY 23(2) 119-124 2014年2月  査読有り責任著者
    The nuclear localization signal (NLS)-containing proteins LEDGF and STAT3 localize to the nucleus in both the spinous and basal layers of the epidermis in psoriatic skin, where they function as transcription factors or co-factors to activate epidermal keratinocytes (KCs). However, the mechanism underlying the localization of these proteins remains to be elucidated. We investigated the differential nucleocytoplasmic transport of NLS-containing proteins as a potential pathogenic mechanism for psoriasis vulgaris. Nucleoporins play an important role in the Ran-GTP-dependent nucleocytoplasmic transport of NLS-containing proteins. We showed, using immunohistochemical staining, that the nucleoporins Ran-binding protein 2 (RanBP2) and Ran-GTPase-activating protein 1 (RanGAP1) have greater expression on the nuclear envelope in psoriatic epidermal KCs than in KCs from healthy controls. We then studied the signalling pathways involved in the regulation of these proteins in HaCaT cells. The two major downstream pathways of epidermal growth factor receptor (EGFR) signalling activated in psoriatic KCs are the MAPK/Erk/1/2 and the phosphatidylinositol-3-kinase/Akt pathways. Therefore, we treated HaCaT cells with inhibitors to disrupt the MAP kinase kinase 1 (MEK1), PI3-kinase, or mTOR pathways. RanBP2 and RanGAP1 protein expression levels were significantly greater in the nuclear envelope of HaCaT cells that were not treated with inhibitors than in cells treated with a combination of PI3-kinase and MEK1 inhibitors or mTOR and MEK1 inhibitors. These results suggest that adequate nuclear envelope expression of RanBP2 and RanGAP1 could be a prerequisite for nucleocytoplasmic transport in KCs in psoriatic epidermis.
  • Kana Tanahashi, Kazumitsu Sugiura, Michihiro Kono, Hiromichi Takama, Nobuyuki Hamajima, Masashi Akiyama
    PLOS ONE 9(2) e89261 2014年2月  査読有り
    Mutations in LIPH cause of autosomal recessive woolly hair/hypotrichosis (ARWH), and the 2 missense mutations c.736T>A (p.Cys246Ser) and c.742C>A (p.His248Asn) are considered prevalent founder mutations for ARWH in the Japanese population. To reveal genotype/phenotype correlations in ARWH cases in Japan and the haplotypes in 14 Japanese patients from 14 unrelated Japanese families. 13 patients had woolly hair, and 1 patient had complete baldness since birth. An LIPH mutation search revealed homozygous c.736T>A mutations in 10 of the patients. Compound heterozygous c.736T>A and c.742C>A mutations were found in 3 of the patients, and homozygous c.742C>A mutation in 1 patient. The phenotype of mild hypotrichosis with woolly hair was restricted to the patients with the homozygous c.736T>A mutation. The severe phenotype of complete baldness was seen in only 1 patient with homozygous c.742C>A. Haplotype analysis revealed that the alleles containing the LIPH c.736T>A mutation had a haplotype identical to that reported previously, although 4 alleles out of 5 chromosomes containing the LIPH c.742C>A mutation had a different haplotype from the previously reported founder allele. These alleles with c.742C>A are thought to be the third founder LIPH mutation causing ARWH. To accurately determine the prevalence of the founder mutations, we investigated allele frequencies of those mutations in 819 Japanese controls. Heterozygous c.736T>A mutations were found in 13 controls (allele frequency: 0.0079; carrier rate: 0.016), and heterozygous c.742C>A mutations were found in 2 controls (allele frequency: 0.0012; carrier rate: 0.0024). In conclusion, this study confirms the more accurate allele frequencies of the pathogenic founder mutations of LIPH and shows that there is a third founder mutation in Japan. In addition, the present findings suggest that the mutation patterns of LIPH might be associated with hypotrichosis severity in ARWH.
  • Kazumitsu Sugiura, Yoshinao Muro, Masashi Akiyama
    Acta Dermato-Venereologica 94(4) 470-471 2014年  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Akemi Takemoto, Michiya Yamaguchi, Hidetoshi Takahashi, Yukiko Shoda, Teruyuki Mitsuma, Kenshiro Tsuda, Emi Nishida, Yaei Togawa, Kimiko Nakajima, Akihiro Sakakibara, Shigeo Kawachi, Makoto Shimizu, Yasutomo Ito, Takuya Takeichi, Michihiro Kono, Yasushi Ogawa, Yoshinao Muro, Akemi Ishida-Yamamoto, Shigetoshi Sano, Hiroyuki Matsue, Akimichi Morita, Hitoshi Mizutani, Hajime Iizuka, Masahiko Muto, Masashi Akiyama
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 133(11) 2514-2521 2013年11月  査読有り筆頭著者責任著者
    Generalized pustular psoriasis (GPP) is a rare inflammatory skin disease that can be life-threatening. Recently, it has been reported that familial GPP is caused by homozygous or compound heterozygous mutations of IL36RN. However, the majority of GPP cases are sporadic and it is controversial whether IL36RN mutations are a causative/predisposing factor for sporadic GPP. We searched for IL36RN mutations in two groups of GPP patients in the Japanese population in this study: GPP without psoriasis vulgaris (PV), and GPP with PV. Eleven cases of GPP without PV (GPP alone) and 20 cases of GPP accompanied by PV (GPP with PV) were analyzed. Surprisingly, 9 out of 11 cases of GPP alone had homozygous or compound heterozygous mutations in IL36RN. In contrast, only 2 of 20 cases of GPP with PV had compound heterozygous mutations in IL36RN. The two cases of GPP with PV who had compound heterozygous mutations in IL36RN are siblings, and both cases had PV-susceptible HLA-A*0206. We determined that GPP alone is a distinct subtype of GPP and is etiologically distinguished from GPP with PV, and that the majority of GPP alone is caused by deficiency of the interleukin-36 receptor antagonist due to IL36RN mutations.
  • Kazumitsu Sugiura, Yasushi Suga, Masashi Akiyama
    JOURNAL OF DERMATOLOGICAL SCIENCE 72(2) 197-199 2013年11月  査読有り筆頭著者
  • Kazumitsu Sugiura, Masaaki Teranishi, Yoshinari Matsumoto, Masashi Akiyama
    JAMA DERMATOLOGY 149(11) 1350-1351 2013年11月  査読有り筆頭著者
  • Kazumitsu Sugiura, Takaaki Matsumoto, Yoshinao Muro, Masashi Akiyama
    Journal of the American Academy of Dermatology 69(5) e269-e270 2013年11月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Takuya Takeichi, Kana Tanahashi, Yasutomo Ito, Tomoki Kosho, Ken Saida, Hisashi Uhara, Ryuhei Okuyama, Masashi Akiyama
    Journal of dermatological science 72(2) 193-5 2013年11月  査読有り筆頭著者
  • Kazumitsu Sugiura, Takuya Takeichi, Masashi Akiyama
    EUROPEAN JOURNAL OF DERMATOLOGY 23(6) 899-900 2013年11月  査読有り筆頭著者責任著者
  • T. Kobayashi, K. Sugiura, T. Takeichi, T. Takeichi, M. Akiyama
    British Journal of Dermatology 169(4) 948-950 2013年10月  査読有り責任著者
  • Kazumitsu Sugiura, Kana Tanahashi, Yoshinao Muro, Masashi Akiyama
    Journal of the American Academy of Dermatology 69(4) e200-e202 2013年10月  査読有り
  • Michihiro Kono, Kazumitsu Sugiura, Mutsumi Suganuma, Masahiro Hayashi, Hiromichi Takama, Tamio Suzuki, Kayoko Matsunaga, Yasushi Tomita, Masashi Akiyama
    HUMAN MOLECULAR GENETICS 22(17) 3524-3533 2013年9月  査読有り
    Reticulate acropigmentation of Kitamura (RAK) is a rare genetic disorder of cutaneous pigmentation with an autosomal dominant pattern of inheritance and a high penetration rate. The characteristic skin lesions are reticulate, slightly depressed pigmented macules mainly affecting the dorsa of the hands and feet, which first appear before puberty and subsequently expand to the proximal limb and the trunk. To identify mutations that cause RAK, we performed exome sequencing of four family members in a pedigree with RAK. Fifty-three SNV/Indels were considered as candidate mutations after some condition narrowing. We confirmed the mutation status in each candidate gene of four other members in the same pedigree to find the gene that matched the mutation status and phenotype of each member. A mutation in ADAM10 encoding a zinc metalloprotease, a disintegrin and metalloprotease domain-containing protein 10 (ADAM10), was identified in the RAK family. ADAM10 is known to be involved in the ectodomain shedding of various substrates in the skin. Sanger sequencing of four additional unrelated RAK patients revealed four additional ADAM10 mutations. We identified a total of three truncating mutations, a splice site mutation and a missense mutation in ADAM10. We searched for mutations in the KRT5 gene, a causative gene for the similar pigmentation disorder Dowling-Degos disease (DDD), in all the patients and found no KRT5 mutation. These results reveal that mutations in ADAM10 are a cause of RAK and that RAK is an independent clinical entity distinct from DDD.
  • Hiroyuki Takama, Kazumitsu Sugiura, Yasushi Ogawa, Yoshinao Muro, Masashi Akiyama
    JOURNAL OF DERMATOLOGICAL SCIENCE 71(2) 100-106 2013年8月  査読有り責任著者
    Background: Barrier-to-autointegration factor 1 (BANF1) is an essential component of the nuclear lamina. Recent studies have clarified that BANF1 is a causative molecule of Nestor-Guillermo progeria syndrome. Despite recent progress in studies on BANF1, the role of BANF1 in keratinocytes has not been addressed at all. Objective: This study aims to determine the localization of BANF1 in psoriatic epidermal keratinocytes as well as in normal keratinocytes and to clarify its possible function in those keratinocytes. Methods: Immunohistochemistry of BANF1 was performed on 10 cases of psoriasis and 10 healthy control individuals. Expression of molecules associated with inflammation of the skin by HSC-1, a human skin squamous cell carcinoma cell line, stimulated by TPA and treated with siRNA to BANF1 were analyzed with quantitative PCR and Western blot. Results: Strong nuclear-dominant immunostaining of BANF1 was seen in the epidermal keratinocytes of psoriatic lesions, although in the normal epidermis, all the KCs in the upper epidermis showed cytoplasmic-dominant staining of BANF1. By BANF1 knockdown in TPA-stimulated HSC-1 cells, the mRNA levels of S100A9 were significantly elevated compared with those of control HSC-1 cells treated with siRNA to CD4. The protein expression level of S100A9 and phosphorylated c-Jun was elevated by BANF1 knockdown. Conclusion: BANF1 is translocated onto the nuclear envelope in the psoriatic epidermal keratinocytes, suggesting that BANF1 is associated with upregulated proliferation of keratinocytes in psoriatic lesions. Activation of BANF1 possibly suppresses S100A9 expression and inactivates c-Jun, resulting in suppression of cutaneous inflammation. (C) 2013 Japanese Society for Investigative Dermatology. Published by Elsevier Ireland Ltd. All rights reserved.
  • Kazumitsu Sugiura, Nana Sugiura, Tetsuya Yagi, Mitsutaka Iguchi, Hideaki Ohno, Yoshitsugu Miyazaki, Masashi Akiyama
    Acta Dermato-Venereologica 93(2) 187-188 2013年3月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Hiroshi Koga, Riho Ishikawa, Takaaki Matsumoto, Mika Matsubara, Rika Hagiwara, Yoshinao Muro, Takashi Hashimoto, Masashi Akiyama
    JAMA DERMATOLOGY 149(1) 111-113 2013年1月  査読有り筆頭著者責任著者
  • Kazumitsu Sugiura, Takuya Takeichi, Michihiro Kono, Yasuki Ito, Yasushi Ogawa, Yoshinao Muro, Masashi Akiyama
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 132(12) 2855-2857 2012年12月  査読有り筆頭著者責任著者
  • K. Sugiura, T. Takeichi, M. Kono, Y. Ogawa, Y. Shimoyama, Y. Muro, M. Akiyama
    BRITISH JOURNAL OF DERMATOLOGY 167(3) 699-701 2012年9月  査読有り筆頭著者責任著者
  • Yoshinao Muro, Kazumitsu Sugiura, Kei Hoshino, Masashi Akiyama
    RHEUMATOLOGY 51(5) 800-804 2012年5月  査読有り
    Objective. Autoantibodies against melanoma differentiation-associated gene 5 (MDA-5) are one of the serological markers for DM. Anti-MDA-5 antibodies are especially associated with rapidly progressive interstitial lung disease (ILD) in amyopathic DM (ADM). It is known that the antibody status of anti-ENAs does not generally change significantly with disease course. For anti-MDA-5 antibodies, however, few longitudinal studies have investigated such changes. This study aimed to establish a quantitative assay for anti-MDA-5 antibodies towards assessing the long-term outcome of ADM patients who had anti-MDA-5 antibodies. Methods. We established ELISA for measuring anti-MDA-5 antibody levels using in vitro transcription and translation recombinant protein. The antibody levels were measured at different time points in 11 clinically ADM patients who tested positive for the anti-MDA-5 antibody on their first visit (range of follow-up 3 months to 16 years). Results. At the stage of clinical remission, six patients received no medication and the four others received low-dose CS. ELISA showed that anti-MDA-5 antibodies disappeared in nine of the patients and fell to just above the cut-off in one patient; in the patient who died, the antibodies remained. Conclusion. Our results suggest that anti-MDA-5 antibodies may be useful as a marker for monitoring disease activity in ILD complicated with ADM. Serial monitoring at short intervals is required to evaluate whether anti-MDA-5 antibody levels correlate with ADM disease activity.
  • Takuya Takeichi, Kazumitsu Sugiura, Yoshinao Muro, Kenji Matsumoto, Yasushi Ogawa, Kyoko Futamura, Osamu Kaminuma, Noriko Hashimoto, Yoshie Shimoyama, Hirohisa Saito, Yasushi Tomita
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 130(12) 2760-2767 2010年12月  査読有り責任著者
    Lens epithelium-derived growth factor (LEDGF)/dense fine speckles 70 kDa protein (DFS70) is a transcription cofactor that enhances growth and is overexpressed in various cancers. In the epidermis, LEDGF/DFS70 localizes to the nucleus of keratinocytes (KCs) in the basal layers and to the cytoplasm of cells in the upper layers. However, the biological and pathological relevance of LEDGF/DFS70 in the epidermis is virtually unknown. Compared with normal epidermis, we detected strong nuclear staining of LEDGF/DFS70 in both the spinous and basal layers of the epidermis of psoriatic skin. To investigate the roles of LEDGF/DFS70 in the epidermis of psoriatic skin, we generated HaCaT cells that constitutively express enhanced green fluorescence protein (EGFP)-LEDGF (EGFP-LEDGF-HaCaT) or EGFP alone (EGFP-HaCaT) as a control. EGFP-LEDGF-HaCaT cells had increased expression of IL-6, which was attenuated by LEDGF-specific RNA interference and the p38-specific inhibitors SB-239063 and SB-203580. Furthermore, EGFP-LEDGF-HaCaT cells had increased expression of S100A7 and S100A9 and decreased expression of filaggrin. These findings are compatible with the expression pattern in psoriatic tissues. Taken together, these results strongly suggest that ectopic expression of LEDGF/DFS70 in KCs could be involved in the pathology of psoriasis vulgaris.
  • Kei Hoshino, Yoshinao Muro, Kazumitsu Sugiura, Yasushi Tomita, Ran Nakashima, Tsuneyo Mimori
    Rheumatology 49(9) 1726-1733 2010年9月  査読有り
    Objectives. Myositis-specific autoantibodies are useful for diagnosing PM/DM. Recently, two new myositis-specific autoantibodies against melanoma differentiation-associated gene 5 (MDA5) and transcriptional intermediary factor 1-γ (TIF1-γ) were identified in DM. Here, we detected these autoantibodies in patient sera using new assays with recombinant MDA5 and TIF1-γ, and associated clinical features with the presence of anti-MDA5 or anti-TIF1-γ antibodies. Methods. We screened 135 Japanese patients with various CTDs, including 82 with DM. DM patients were classified as clinically amyopathic DM (CADM), cancer-associated DM or classical DM without cancer. Anti-MDA5 and anti-TIF1-γ antibodies were detected by their ability to immunoprecipitate biotinylated recombinant proteins.Results. Sera from 21 (26%) of 82 DM patients immunoprecipitated MDA5, and every anti-MDA5-positive patient had DM (except one patient with SSc). Sera from 20 (65%) of 31 CADM patients reacted with MDA5. Notably, anti-MDA5-positive DM patients had significantly more interstitial lung disease than anti-MDA5-negative DM patients (95 vs 32%, P < 0.001). Sera from 12 (15%) of 82 DM patients immunoprecipitated TIF1-γ, and anti-TIF1-γ antibodies were only detected in DM patients. Strikingly, 7 (58%) of 12 patients with cancer-associated DM had sera that reacted with TIF1-γ. Anti-TIF1-γ-positive DM patients had significantly more internal malignancies than anti-TIF1-γ-negative DM patients (58 vs 9%, P < 0.001).Conclusions. Anti-MDA5 and anti-TIF1-γ antibodies were confirmed to be serological DM subset markers. Anti-MDA5 and anti-TIF1-γ antibodies were detected based on their ability to immunoprecipitate biotinylated recombinant MDA5 and TIF1-γ, and were closely associated with life-threatening complications in DM. © The Author 2010. Published by Oxford University Press on behalf of the British Society for Rheumatology. All rights reserved.
  • Mayuko Yamaki, Kazumitsu Sugiura, Yoshinao Muro, Yoshie Shimoyama, Yasushi Tomita
    EXPERIMENTAL DERMATOLOGY 19(8) 730-735 2010年8月  査読有り責任著者
    Epidermal growth factor receptor tyrosine kinase (EGFR-TK) is a transducer of mitogenic signals, and is involved in the pathogenesis and progression of a number of cancers, including non-small cell lung cancer (NSCLC). Gefitinib is an EGFR-TK inhibitor that is clinically used to treat NSCLC; however, this drug frequently causes adverse effects, including skin eruptions. The mechanism underlying these skin reactions is elusive, although it is assumed that they are caused by the inhibition of EGFR-TK signalling in epidermal and adnexal cells. In this article, we demonstrate by immunocytochemistry that the skin lesions of patients treated with oral gefitinib had higher expression of CCL2 and CCL5 compared to normal human epidermis. Further, PD153035, a gefitinib prototype, induced CCL2 and CCL5 mRNA and protein expression in HaCaT and HSC-1 keratinocyte cell lines with or without interleukin-1 (IL-1) treatment in vitro. PD153035 also reduced the levels of interleukin-1 receptor 2 (IL-1R2), an IL-1 decoy receptor. Moreover, we demonstrate that reduction in IL-1R2 by RNA interference increased IL-1-mediated CCL2 and CCL5 mRNA and protein expression. Taken together, our data strongly suggest that IL-1-mediated signalling is activated to induce the high expression of CCL2 and CCL5 via reduction in IL-1R2 in the skin lesions caused by gefitinib.
  • Kazumitsu Sugiura, Yoshinao Muro, Kyoko Futamura, Kenji Matsumoto, Noriko Hashimoto, Yuji Nishizawa, Tetsuro Nagasaka, Hirohisa Saito, Yasushi Tomita, Jiro Usukura
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 129(9) 2126-2135 2009年9月  査読有り筆頭著者責任著者
    The unfolded protein response (UPR), which is induced by stress to the endoplasmic reticulum (ER), is involved in the functional alteration of certain cells, such as the differentiation of B cells to plasma cells. The aim of this study is to determine whether the UPR is activated during epidermal keratinocyte (KC) differentiation. Here, we show that the expression of the UPR-induced proteins Bip/GRP78 and HRD1 was increased in cells in the suprabasal layers of normal human epidermis that contain KCs undergoing differentiation as well as in skin-equivalent cultured KCs. However, Bip/GRP78 and HRD1 were poorly expressed in proliferating KCs in squamous cell carcinoma and psoriasis vulgaris tissues. The epidermal growth factor receptor tyrosine kinase inhibitor, PD153035, which induces KC differentiation, upregulated UPR-induced marker mRNAs and proteins. Furthermore, microarray analyses and quantitative PCR revealed that ER stress-inducing reagents, tunicamycin (TU), thapsigargin, and brefeldin A, altered the expression of genes essential for human epidermal KC differentiation, including C/EBP beta, KLF4, and ABCA12 in vitro. However, ABCA12 and KLF4 mRNA did not increase with TU treatment after siRNA-mediated knockdown of XBP-1. Taken together, our findings strongly suggest that the UPR is activated during normal epidermal KC differentiation and induces C/EBP beta, KLF4, and ABCA12 mRNAs.
  • Y. Muro, K. Sugiura, Y. Morita, Y. Tomita
    LUPUS 17(3) 171-176 2008年  査読有り
    Autoantibodies against dense fine speckles 70 (DFS70) are found in 10% of healthy individuals, but only in a tiny population of patients with autoimmune rheumatic disease. The antibody may thus be a marker of autoimmune rheumatic disease negativity. To investigate this possibility, we examined the presence of various disease-marker autoantibodies in anti-DFS70 antibody-positive patients with autoimmune rheumatic disease. Serum samples from 500 patients with various types of autoimmune rheumatic disease were examined for anti-DFS70 antibodies by indirect immunofluorescence and immunoblotting. Various disease-marker autoantibodies were measured by enzyme-linked immunosorbent assay. Twenty-two patients were positive for anti-DFS70 antibodies. Eighteen patients also had disease-marker autoantibodies including anti-double stranded DNA, anti-cardiolipin, anti-SS-A, or other antibodies. In one patient with Sjogren syndrome and two patients with dermatomyositis, no disease-marker antibodies were found; however, one patient with dermatomyositis had a concomitant anti-cytoplasmic antibody. All seven systemic lupus erythematosus patients fulfilled the classification criteria for this disease even if anti-nuclear antibody-positive findings were excluded. One patient with morphea had high-titer anti-single stranded DNA antibody. According to this and previous studies, patients with only anti-DFS70 antibody are rarely diagnosed as having autoimmune rheumatic disease. Recognizing dense fine speckle patterns in anti-nuclear antibodies tests is, thus, very important for analysis of laboratory results in rheumatology clinics.
  • M Okamoto, Y Ogawa, A Watanabe, K Sugiura, Y Shimomura, N Aoki, T Nagasaka, Y Tomita, Y Muro
    JOURNAL OF AUTOIMMUNITY 23(3) 257-266 2004年11月  査読有り
    Alopecia areata (AA) has been suspected to be an autoimmune disease, although there is no distinct evidence, we investigated the relationship between AA and autoantibodies against dense fine speckles 70, kDa (DFS70) in 111 patients with alopecia and 105 healthy controls. The sera from 59 out of 111 (53%) Japanese alopecia patients were positive for anti-nuclear antibody (ANA), as compared to the sera of 16 out of 1:05 (15%) healthy controls (p < 0.001). Twenty percent (22/111) of the alopecia patients were shown to be positive for the prevalence of anti-DFS70 antibodies, as compared to 8% (8/105) of the healthy controls (P < 0.01). IgG subclass analysis by ELISA showed that IgG1 and IgG2-anti-DFS70 antibodies were dominant in alopecia patients. The DFS70 gene expression in the hair structures was clearly detected in both those with and those without the anti-DFS70 antibody by RTPCR. immunohistochemical techniques showed that the DFS70 was localized predominantly in the outer root sheath (ORS) cells. The elevated anti-DFS70 antibodies in alopecia patients and the localization of the DFS70 in the ORS suggest that autoantibodies against the DFS70 are related to the etiology in a certain population of AA. (C) 2004 Elsevier Ltd. All rights reserved.
  • Y Ogawa, K Sugiura, A Watanabe, M Kunimatsu, M Mishima, Y Tomita, Y Muro
    JOURNAL OF AUTOIMMUNITY 23(3) 221-231 2004年11月  査読有り
    Autoantibodies against DFS70 (Dense Fine Speckles 70) are found in 30% of Japanese atopic dermatitis patients, and less frequently in patients with other diseases. We have recently reported that they are also seen in 11% of hospital workers, but in only similar to2% of patients with systemic rheumatic disease. In this study, in order to investigate the possible pathological role of anti-DFS70 antibodies, fine epitope mapping was carried out using 93 anti-DFS70 autoantibody-positive sera. Immunoblotting using overlapping peptides failed to reveal major linear epitopes. Western blotting using various truncated proteins showed a strikingly uniform epitope distribution on a suspected tertiary structure expressed by DFS70(349-435). Some sera showed reactivity only in an immunoprecipitation assay using an in vitro translated DFS70. Circular dichroism analysis revealed that DFS349-435 contains an approximately 40% alpha-helical conformation, while an overlapping, non-antigenic peptide is composed of random coiled structures. The skewed single major epitope enabled us to establish a highly quantitative ELISA for the epitope region. Antibody titers showed no significant differences between the diseased group and healthy individuals. We propose that anti-DFS70 antibody may be a natural autoantibody, which might modify or reflect the inflammatory process of various disorders. (C) 2004 Elsevier Ltd. All rights reserved.
  • K Higashimoto, T Urano, K Sugiura, H Yatsuki, K Joh, W Zhao, M Iwakawa, H Ohashi, M Oshimura, N Niikawa, T Mukai, H Soejima
    AMERICAN JOURNAL OF HUMAN GENETICS 73(4) 948-956 2003年10月  査読有り
    To clarify the chromatin-based imprinting mechanism of the p57(KIP2)/LIT1 subdomain at chromosome 11p15.5 and the mouse ortholog at chromosome 7F5, we investigated the histone-modification status at a differentially CpG methylated region of Lit1/LIT1 (DMR-Lit1/LIT1), which is an imprinting control region for the subdomain and is demethylated in half of patients with Beckwith-Wiedemann syndrome (BWS). Chromatin-immunoprecipitation assays revealed that, in both species, DMR-Lit1/LIT1 with the CpG-methylated, maternally derived inactive allele showed histone H3 Lys9 methylation, whereas the CpG-unmethylated, paternally active allele was acetylated on histone H3/H4 and methylated on H3 Lys4. We have also investigated the relationship between CpG methylation and histone H3 Lys9 methylation at DMR-LIT1 in patients with BWS. In a normal individual and in patients with BWS with normal DMR-LIT1 methylation, histone H3 Lys9 methylation was detected on the maternal allele; however, it disappeared completely in the patients with the DMR-LIT1 imprinting defect. These findings suggest that the histone-modification status at DMR-Lit1/LIT1 plays an important role in imprinting control within the subdomain and that loss of histone H3 Lys9 methylation, together with CpG demethylation on the maternal allele, may lead to the BWS phenotype.
  • K Sugiura, Y Muro
    JOURNAL OF RHEUMATOLOGY 26(10) 2168-2172 1999年10月  査読有り筆頭著者
    Objective. To elucidate the frequency and clinical significance of anti-annexin V antibodies in patients with scleroderma. Methods. The study population consisted of 66 patients with scleroderma. Their sera were examined for IgG anti-annexin V antibodies by ELISA and immunoblotting. Results. IgG anti-annexin V antibodies were detected by ELISA in 12 patients (18.2%) with scleroderma. Anti-annexin V antibodies were associated with digital ischemia in the patients with scleroderma. Only one patient of the 12 had anticardiolipin antibodies. Although 6 patients with anti-annexin V antibodies were also examined for activated partial thromboplastin time (APTT), none showed prolonged APTT. No IgG anti-annexin V antibodies were detected by immunoblotting. Conclusion. Anti-annexin V antibodies in scleroderma are related to digital ischemia. These antibodies may be associated with the pathogenesis of vascular involvement in scleroderma.
  • K. Sugiura, Y. Muro, M. A. Mont, L. C. Jones, M. Petri
    Journal of Rheumatology 25(12) 2477-2478 1998年  査読有り筆頭著者
  • K Sugiura, Y Muro, Y Nagai, T Kamimoto, T Wakabayashi, M Ohashi, M Hagiwara
    BIOCHIMICA ET BIOPHYSICA ACTA-GENE STRUCTURE AND EXPRESSION 1352(1) 23-26 1997年5月  査読有り筆頭著者
    We isolated a cDNA encoding a human homologue of ZF5 (hZF5), which has five Kruppel-like C2H2 type zinc fingers at carboxyl terminus and the BTB/POZ (poxvirus and zinc finger) at the amino terminus, using autoimmune sera from a patient with overlap syndrome (dermatomyositis and scleroderma). Sequencing of the entire cDNA revealed an open reading frame (ORF) of 1349 bp with a deduced protein sequence of 449 amino acid residues and a calculated molecular weight of 51.3 kDa. The deduced amino acid sequence of hZF5 is highly homologous to mouse ZF5 (99.3% identity). Immunofluorescence studies revealed that HA-tagged hZF5 transiently expressed in COS-7 cells showed the nuclear dot pattern in the BTB/POZ domain-dependent manner.

MISC

 142
  • 杉浦 一充
    皮膚科 4(2) 146-154 2023年8月  
  • 桜 莉唯心, 杉山 由華, 杉浦 一充, 戸倉 新樹
    臨床皮膚科 77(4) 317-321 2023年4月  
    <文献概要>72歳,女性.40歳頃より全身に皮疹が出現し,近医で入院加療をしたが,確定診断に至ることなく,症状の出現と消退を繰り返していた.71歳時に心筋梗塞で当院入院中に同皮疹が出現し当科を紹介された.初診時,背部や側腹部,両上肢に一部膿疱を伴い落屑を付着した紅斑を認めた.左上腕の紅斑からの生検標本では,角層下に大型の好中球性膿疱がみられ,真皮上層の血管周囲性に炎症性細胞が浸潤し,また膿疱辺縁に多房性のKogoj海綿状膿疱もみられた.遺伝子検索では,IL36RN c. 115+6T>C heterozygoteの変異を認め,IL-36受容体拮抗因子欠損症(deficiency of interleukin-36 receptor antagonist: DITRA)と診断された.グセルクマブ投与を開始し,紅斑や膿疱は消退した.DITRAはIL36RN遺伝子変異によるIL-36受容体拮抗因子機能不全を背景とした疾患である.DITRAは疾患概念が最近確立した病態であり,自験例のように膿疱性乾癬とすら診断されることなく,症状出現から約30年を経過して診断に至る症例もあるため,尋常性乾癬を伴わないGPPやその類縁疾患を診察する際に遺伝子検索を行う重要性を実感した.
  • 安田 澪奈, 岩月 啓氏, 鈴木 究, 中川 満, 黒田 誠, 杉浦 一充
    皮膚病診療 45(4) 342-345 2023年4月  
    <文献概要>症例のポイント ・小児の限局性リンパ腫様丘疹症(lymphomatoid papulosis:LyP)を経験した.・病理組織学的所見では,急性痘瘡状苔癬状粃糠疹(pityriasis lichenoides et varioliformis acuta:PLEVA)が鑑別にあがったが,再検の結果,CD8陽性LyPと診断した.・腫瘍性リンパ球は,血管中心性および汗器官と末梢神経向性浸潤を認めていた.・LyPは病理組織学的所見と遺伝子表現型からサブタイプ分類が提唱されているが,所見の重複などで分類不能な場合がある.
  • 前田 珠希, 住友 千穂, 犬塚 雄貴, 有馬 豪, 杉浦 一充
    皮膚科の臨床 64(13) 2115-2118 2022年12月  
    <文献概要>27歳,女性。初診5ヵ月前から口腔内に広域な白苔,リンパ節腫脹を認め前医を受診した。血液検査で単純ヘルペスウイルスIgM抗体陽性であり,ヘルペスウイルス性咽頭炎と診断された。1ヵ月前より口腔内潰瘍が悪化し経口摂取困難となったため,精査目的に当院耳鼻咽喉科へ紹介となり,口腔内潰瘍の精査目的で当科を受診した。口腔内潰瘍とざ瘡様皮疹を認め,遺伝子検索を行ったところHLA-B51陽性でありBehcet病疑いと診断した。また抗SS-A抗体陽性,下口唇生検の結果よりSjoegren症候群と診断した。Behcet病とSjoegren症候群の併発はまれであるため,軽度の症状でも見逃さずに両者が併発している可能性を考える必要がある。
  • 杉浦 美月, 岩田 洋平, 齋藤 健太, 山田 友菜, 塚本 徹哉, 杉浦 一充
    Skin Surgery 31(2) 41-45 2022年10月  
    症例1 70歳日本人男性,左鼻翼部の8mm大の常色腫瘍.症例2 43歳日本人女性,右鼻翼部の7mm大の常色腫瘍.ダーモスコピーで2症例ともarborizing vessels,shiny white areasを認めた.切除範囲は腫瘍辺縁をダーモスコピーで確認することで決定した.全摘標本のHE染色では,柵状配列を示す基底細胞様細胞が胞巣状に深部に増殖する所見を認めた.免疫染色では,Melan-A染色で腫瘍胞巣内にメラノサイトが確認されたがFontana-Masson染色でメラニン顆粒は認められなかった.以上の所見より無色素性基底細胞癌と診断した.無色素性基底細胞癌は,肉眼所見のみでは診断に苦慮することがあるので,ダーモスコピーを積極的に用いることで正確な診断や適切な切除範囲の決定に結び付けることができると考えられる.(著者抄録)
  • 福田 晃洋, 有馬 豪, 岩田 洋平, 杉浦 一充
    Skin Cancer 37(2) 150-155 2022年10月  
    症例1:79歳,男性。初診の1年前より左肩甲骨部に腫瘤を認めた。近医の皮膚生検で平滑筋肉腫と診断され当科へ紹介。初診時,左肩甲骨部に40×35mmの腫瘤を認めた。MRIで腫瘍が皮下脂肪織内まであり,水平マージンは3cm,深部マージンは筋膜を含めて切除し,遊離分層植皮術を施行した。症例2:67歳,男性。初診の4ヵ月前より右大腿後面に腫瘤を認めた。近医の皮膚生検で平滑筋肉腫を疑われ当科へ紹介。初診時,右大腿後面に45×25mmの腫瘤を認めた。MRIで腫瘍は真皮内に限局しており,水平マージンは5mm,深部マージンは筋膜上で切除した。2症例とも皮膚型平滑筋肉腫と診断した。症例1では免疫組織学的検査で腫瘍結節部のSMAが陰性,desminが弱陽性であった。悪性度が高く脱分化している可能性があり,通常の皮膚型平滑筋肉腫と異なっていた。症例1は術後1年2ヵ月,症例2は術後7年経過したが再発や転移を認めていない。(著者抄録)
  • 杉浦 一充
    小児内科 54(8) 1265-1268 2022年8月  
    <Key Points>(1)乳児期の接触皮膚炎としては、口周囲の接触皮膚炎やおむつ皮膚炎があり、学童期の接触皮膚炎としては金属、植物による接触皮膚炎がみられる。(2)接触皮膚炎は刺激性接触皮膚炎、アレルギー性接触皮膚炎、光毒性接触皮膚炎、光アレルギー性接触皮膚炎、非アレルギー性接触蕁麻疹、アレルギー性接触蕁麻疹の6つに分類される。(3)問診と皮膚テストで原因物質を同定する。(4)原因物質の含まれる日常品への接触を避けるための細やかな患者指導が重要である。(著者抄録)
  • 伊藤 靖敏, 武市 拓也, 棚橋 華奈, 吉川 剛典, 村瀬 友哉, 室 慶直, 秋山 真志, 池田 賢太, 森実 真, 川上 佳夫, 中村 保夫, 武藤 潤, 大磯 直毅, 清島 真理子, 川田 暁, 杉浦 一充, 須賀 康, 荻 朋男
    角化症研究会記録集 36 45-48 2022年6月  
  • 杉浦 一充
    皮膚科 1(2) 225-232 2022年2月  
  • 前田 珠希, 秋田 浩孝, 福島 英彦, 栃井 大輔, 杉浦 一充
    皮膚の科学 20(4) 349-353 2021年12月  
    53歳女性。8歳時に左鎖骨部皮下腫瘤を切除した。43歳頃より左鎖骨近傍に皮下腫瘤が出現した。CTにて左鎖骨近位部と縦隔に腫瘤病変を認めたため当科紹介となった。左鎖骨部皮下血管腫と縦隔血管腫を考え,全摘術を施行した。病理学的検討では皮下腫瘤は海綿状血管腫,縦隔病変は縦隔血管腫と診断した。皮下に発症した海綿状血管腫の中で縦隔血管腫と合併した報告は自験例のみであった。海綿状血管腫は他臓器に血管腫を伴う報告があり,随伴症状を有することもあるため内臓血管腫の合併の有無の検索も必要である。(著者抄録)
  • 杉浦 一充
    現代医学 68(2) 97-98 2021年12月  
  • 横井 聡美, 有馬 豪, 杉浦 一充
    皮膚病診療 43(10) 900-902 2021年10月  
    <文献概要>ポイント ・先天性乏毛症とは遺伝子異常によって,生下時や幼少時より乏毛を呈する疾患の総称である.本邦ではLIPH遺伝子に共通の創始者変異を高頻度で認める.・自験例でもLIPH遺伝子にc.736T>A(p.Cys246Ser)のミスセンス変異をホモ接合型に有していた.・本邦におけるLIPH遺伝子の創始者変異の保有率は約2%とされている.・先天性乏毛症の治療として,ミノキシジル外用液の有効性が報告されている.
  • 杉浦 一充
    Pharma Medica 39(10) 23-27 2021年10月  
    <文献概要>膿疱性乾癬(generalized pustular psoriasis:GPP)はオーストリア人のLeo von Zumbuschが1910年に初めての報告をした。初めての報告は姉弟例であったが,長らく孤発性の疾患と考えられており,2011年までの約100年間,病因は不明であった。2011年にGPPの病因の1つがIL36RN遺伝子の変異によることが明らかにされてから,GPPの病態解明の研究は発展を遂げ,IL36RN遺伝子の他にCARD14遺伝子,AP1S3遺伝子,SERPINA3遺伝子,MPO遺伝子が病因遺伝子として報告されてきている。本稿では,自然免疫に関連する遺伝子の異常による自己炎症という側面をもつGPPの病態について,これまでの知見をまとめる。
  • 稲葉 弥寿子, 伊佐見 真実子, 鶴田 京子, 杉浦 一充
    臨床皮膚科 75(9) 707-711 2021年8月  
    <文献概要>左上肢に数珠様結節を呈した60歳,男性の皮膚リンパ型ノカルジア症を報告した.左手関節皮膚潰瘍と左前腕と上腕の数珠様結節を認めメロペネムで軽快した.上腕結節部の膿など4ヶ所11条件で培養し1ヶ所のみ小さなコロニーを認めマトリックス支援レーザー脱離イオン化飛行時間型質量分析でNocardia brasiliensisが同定された.培養提出から結果判明まで18日間を要した.数珠様結節を呈する疾患は他にもスポロトリコーシス,Mycobacterium marinum,皮膚クリプトコッカス症の報告がある.いずれも一般的な条件では培養されない可能性が高い.数珠様結節を呈する疾患において培養を提出する際に設定したほうがよい条件を文献的考察を交えて検討した.具体的には,(1)1週間以上培養をする,(2)室温培養も追加する,(3)抗酸菌は30℃設定も追加する,(4)シクロヘキシミドを加えないサブロー・ブドウ糖寒天培地を使用するなどを考慮したほうがよいと考えらえた.
  • 杉浦 一充
    Derma. (312) 45-52 2021年8月  
    自己炎症性角化症とは、表皮角化細胞における自然免疫に関連したタンパク質を遺伝子産物とする1遺伝子の変異ないし多型を病因とした、炎症性角化症を発症する疾患群である。一方、自己炎症性疾患では蕁麻疹様皮疹などをきたす。皮膚所見が異なるという観点から、自己炎症性疾患の亜型として秋山らにより2017年に提唱された。当初、自己炎症性角化症にはIL-36受容体拮抗因子欠損症、CARD14関連乾癬、NLRP1関連異常症のうちfamilial keratosis lichenoides chronicaが含まれていたが、遺伝性皮膚疾患の研究の進展により、自己炎症性角化症に含まれる疾患は拡大しつつある。(著者抄録)
  • 杉浦 一充
    生体の科学 71(6) 555-560 2020年12月  
    <文献概要>自己炎症性角化症とは,表皮角化細胞に存在する自然免疫に関連するタンパク質をコードする,1遺伝子の変異ないし多型を病因とする,炎症性角化症を発症する疾患群である。蕁麻疹様皮疹を来す自己炎症性疾患とは皮膚所見が異なるという観点から,2017年に提唱された。当初,自己炎症性角化症にはIL-36受容体拮抗因子欠損症(deficiency of interleukin-thirty six receptor antagonist;DITRA),CARD14関連乾癬(CARD14 mediated psoriasis;CAMPS),familial keratosis lichenoides chronica(FKLC)が含まれていたが,遺伝性皮膚疾患の研究の進展により,自己炎症性角化症に含まれる疾患も拡大しつつある。
  • 熊野 友華, 永井 晶代, 鈴木 加余子, 岡部 光邦, 杉浦 一充
    日本皮膚免疫アレルギー学会雑誌 3(3) 420-424 2020年10月  
    症例は41歳男性で、歯髄炎の治療を受けた2時間後に蕁麻疹を生じ、ステロイド薬・抗ヒスタミン薬で一旦消退傾向であったが、数時間後にアナフィラキシーショックとなりアドレナリンにより改善した。歯根管消毒薬を使用後に蕁麻疹を生じた既往があり、局所麻酔薬のみの処置の際には蕁麻疹は生じなかったことから、パラホルムアルデヒド・ジブカイン塩酸塩パスタを原因として疑った。特異的IgE抗体はホルマリンに陽性であった。プリックテストはすべて陰性で、スクラッチテストはホルムアルデヒド、パラホルムアルデヒド・ジブカイン塩酸塩パスタに1+であった。歯根管消毒薬であるパラホルムアルデヒド・ジブカイン塩酸塩パスタに含まれたホルムアルデヒドによるアナフィラキシーショックと診断した。
  • 熊野 友華, 岩田 洋平, 山北 高志, 室 慶直, 久保 良二, 杉浦 一充
    臨床皮膚科 74(8) 579-582 2020年7月  
    <文献概要>38歳,女性.抗菌薬不応性の発熱,全身の紅斑,両前腕の筋痛,関節痛があり,初診1ヵ月前に近医を受診した.蕁麻疹様血管炎を疑われプレドニゾロンの内服が開始され,一旦皮疹は消退したが減量に伴い再燃したため当院へ紹介となった.初診時は胸部,上背部,腰部に網目状色素沈着を認め,皮膚筋炎や成人Still病が疑われた.皮膚筋炎の各種特異抗体は陰性であり,成人Still病の診断基準を満たし,非定型疹を呈した成人Still病と確定診断した.成人Still病は典型的なサーモンピンク疹だけでなく,多彩な非定型疹を呈することがあり,診断に難渋することもある.自験例のように色素性痒疹様皮疹を認め,発熱や関節痛などを生じていたときは,成人Still病も鑑別する必要がある.
  • 杉浦 一充
    現代医学 67(1) 75-77 2020年6月  
  • 良元 のぞみ, 永井 晶代, 鈴木 加余子, 杉浦 一充
    日本皮膚免疫アレルギー学会雑誌 3(2) 355-361 2020年4月  
    症例1(42歳男性)、症例2(26歳女性)、症例3(37歳女性)。いずれも外痔核に対するトリベノシド・リドカイン軟膏の使用開始1〜2週間後に臀部の浮腫性紅斑が出現した。全例にトリベノシド・リドカイン軟膏および成分のパッチテストを試行した結果、同軟膏およびトリベノシドに陽性反応を示した。症例1はトリベノシドによるアレルギー性接触皮膚炎、症例2と症例3はトリベノシドによる接触皮膚炎症候群と診断された。3症例ともトリベノシドを含む薬剤の服用および外用を禁止したところ、皮疹の再燃はみられなぃなった。
  • 杉浦 一充
    内科 125(3) 427-429 2020年3月  
    <文献概要>▼紅皮症とは単一の疾患名ではなく,症候名である.▼紅皮症では皮膚毛細血管が著しく拡張するため,体温調節,水や電解質の代謝,循環などにも影響を及ぼす.▼紅皮症の原疾患は湿疹・皮膚炎,水疱症・膿疱症,炎症性角化症,膠原病および類縁疾患,薬疹と移植片対宿主病(GVHD),感染症,腫瘍などである.▼内臓悪性腫瘍のデルマドロームとして紅皮症をきたすこともある.▼治療方針決定のためには,原疾患の診断が重要である.▼脱水・感染などで全身状態が急速に増悪する場合があるので,入院による全身管理が望ましい.
  • 福島 英彦, 沼田 茂樹, 岩田 洋平, 杉浦 一充
    皮膚科の臨床 62(2) 225-228 2020年2月  
    <文献概要>79歳,女性。右鼠径部の発赤・腫脹を主訴に救急外来を受診した。腹部単純CTで右鼠径から右大陰唇にかけて皮下にガス像を伴う液体貯留が確認されたため,外陰部ガス壊疽と診断し,緊急でデブリードマンを施行した。術後13日目より右鼠径部から持続的な排液を認めたため,腹部単純CTや腹部超音波検査を行ったが診断には至らず,右鼠径部より瘻孔造影を施行し,腸管皮膚瘻と診断した。1年前の腹部単純CTで同部位に大腿ヘルニアを認めたことから,大腿ヘルニア嵌頓より腸管穿孔を引き起こしガス壊疽に至ったと考えた。まれではあるが腸管の嵌頓から腸管皮膚瘻が生じ,壊死性軟部組織感染症を引き起こすことがあり,その診断に瘻孔造影が有用である。
  • 臼田 千穂, 岩田 洋平, 秋田 浩孝, 黒田 誠, 杉浦 一充
    西日本皮膚科 81(6) 500-503 2019年12月  
    IgG4関連疾患は,血中IgG4上昇及び組織へのIgG4陽性形質細胞浸潤を特徴とした疾患概念である。IgG4関連疾患は膵臓,腎臓,涙腺,唾液腺など全身臓器の肥厚や腫大を来す。IgG4関連疾患に伴う皮膚病変は多岐にわたり,そのなかに偽リンパ腫に似た臨床症状および病理所見を示すものがある。自験例では,鼻根部に出現した紅色腫瘤が急速に増大し,病理組織学的に真皮全層性に稠密な形質細胞浸潤とリンパ濾胞形成を認め,偽リンパ腫に合致した所見を呈していた。免疫グロブリンH鎖の遺伝子再構成バンドは検出されず,免疫組織化学染色でIgG4陽性形質細胞浸潤を認め,IgG4/IgG陽性形質細胞比は30%であった。血中IgG4値の上昇は認められたが皮膚以外の臓器病変はなく,IgG4関連偽リンパ腫と診断した。これまで原因不明の良性リンパ増殖性疾患と定義される偽リンパ腫の中にも,IgG4が病態に関与するものが混在すると推測される。IgG4関連皮膚疾患に関して文献的考察を含めて報告する。(著者抄録)
  • 福島 英彦, 有馬 豪, 小林 束, 鈴木 明子, 岩田 貴子, 杉浦 一充
    皮膚病診療 41(12) 1125-1128 2019年12月  
    <文献概要>症例のポイント ・高圧酸素療法が著効し,下肢温存できた壊死性軟部組織感染症を経験した.・高圧酸素療法は壊死性軟部組織感染症において有効な治療法である可能性を示した.
  • 榊原 潤, 沼田 茂樹, 岩田 洋平, 村手 健一郎, 武藤 多津郎, 渡邉 宏久, 山北 高志, 渡邊 薫, 杉浦 一充
    皮膚科の臨床 61(13) 2007-2010 2019年12月  
    <文献概要>68歳,男性。10日前に発症した左上肢帯状疱疹に対してバラシクロビルの内服で治療開始した。5日前より左上肢挙上困難となり,当科を紹介受診した。左上肢の筋力低下があり,MRIで脳・脊髄炎の所見はなかったが,髄液を用いたRT-PCR法によりvaricella-zoster virus(VZV)-DNAが検出された。以上の所見より帯状疱疹による運動神経障害と診断し,ステロイドパルス療法とアシクロビル20mg/kg/日の点滴静注を行い,治療2週間後には髄液中VZV-DNAが陰性化し,症状も徐々に改善,48週で完治した。自験例の経験より,運動神経障害を伴う重症な帯状疱疹においては,早期に診断し抗ウイルス薬の点滴投与で治療することが重要と考えた。
  • 臼田 千穂, 岩田 洋平, 秋田 浩孝, 黒田 誠, 杉浦 一充
    西日本皮膚科 81(6) 500-503 2019年12月  
    IgG4関連疾患は,血中IgG4上昇及び組織へのIgG4陽性形質細胞浸潤を特徴とした疾患概念である。IgG4関連疾患は膵臓,腎臓,涙腺,唾液腺など全身臓器の肥厚や腫大を来す。IgG4関連疾患に伴う皮膚病変は多岐にわたり,そのなかに偽リンパ腫に似た臨床症状および病理所見を示すものがある。自験例では,鼻根部に出現した紅色腫瘤が急速に増大し,病理組織学的に真皮全層性に稠密な形質細胞浸潤とリンパ濾胞形成を認め,偽リンパ腫に合致した所見を呈していた。免疫グロブリンH鎖の遺伝子再構成バンドは検出されず,免疫組織化学染色でIgG4陽性形質細胞浸潤を認め,IgG4/IgG陽性形質細胞比は30%であった。血中IgG4値の上昇は認められたが皮膚以外の臓器病変はなく,IgG4関連偽リンパ腫と診断した。これまで原因不明の良性リンパ増殖性疾患と定義される偽リンパ腫の中にも,IgG4が病態に関与するものが混在すると推測される。IgG4関連皮膚疾患に関して文献的考察を含めて報告する。(著者抄録)
  • 前田 珠希, 小林 束, 岩田 洋平, 山北 高志, 奥井 太郎, 杉浦 一充
    皮膚病診療 41(11) 1049-1052 2019年11月  
    <文献概要>症例のポイント ・Zinsser-Cole-Engman症候群,別名の先天性角化不全症(dyskeratosis congenita:DKC)は合併症により若年で死亡する可能性があるため,定期的な血液検査および画像検査,悪性腫瘍の検索を継続していく必要がある・皮膚科医の役割としては,とくに皮膚有棘細胞癌の発生に注意して経過観察することである.・比較的生存期間の長いDKCの1例を経験した.
  • 吉田 美沙子, 秋田 浩孝, 杉浦 一充
    Skin Surgery 28(3) 194-197 2019年10月  
    症例は42歳女性で、4歳頃より両頬部に自覚症状のない紅色小結節が出現した。近医を受診するも診断を告げられず放置していたが次第に症状が顕著となり、加療目的に当科を受診した。顔面線維腫および左足趾2ヶ所の爪囲線維腫の症状から、診断基準の大症状の2項目を満たし、結節性硬化症と診断した。ダイレーザーを10回、炭酸ガスレーザーを5回数ヵ月間隔で施行したところ、ダイレーザーにて血管病変が少し縮小し、炭酸ガスレーザーにて血管線維腫の線維性隆起性病変が若干平坦化したが、改善は乏しく再発もみられた。その後、結節性硬化症の顔面血管線維腫の治療薬として上市されたシロリムスゲルを顔面血管線維腫と頭部線維性局面および左足趾爪囲線維腫に1日2回、1日0.8g外用する治療を開始した。その結果、20週間使用した時点で顔面血管線維腫の隆起がかなり平坦化し、両頬部の色素性病変が縮小した。頭部線維性局面は色調、隆起とも改善がみられた。足趾爪囲線維腫は変化がなかった。
  • 高向 梨沙, 神崎 美玲, 杉浦 一充
    皮膚病診療 41(8) 761-764 2019年8月  
    <文献概要>症例のポイント ・小児汎発性膿疱性乾癬の3歳男児例を経験し,遺伝子解析によりCARD14(caspase recruitment domain-containing protein 14)遺伝子に疾患感受性多型が検出された.・自験例はCARD14遺伝子多型を背景として発症したと考えられ,自己炎症性角化症のひとつであるCARD14関連乾癬に分類される.・小児期発症の汎発性膿疱性乾癬においては,IL36RN遺伝子およびCARD14遺伝子の解析が早期診断に有用である.・小児汎発性膿疱性乾癬に対する全身療法の選択肢はいまだ限られており,有効かつ安全に使用できる治療薬の開発が望まれる.
  • 杉浦 一充
    皮膚病診療 41(7) 602-607 2019年7月  
    <文献概要>はじめに 好中球の機能亢進が病態に関与している皮膚疾患は多数ある.たとえば,膿疱性乾癬,化膿性汗腺炎,壊疽性膿皮症,Behcet病などでは,病変部に好中球の浸潤がみられるのが特徴である.従来,機能亢進している好中球は通常の細胞の形態を保っていると考えられていたが,必ずしもそうでないということが明らかになってきた.近年,好中球細胞外トラップ(neutrophil extracellulartraps:NETs)という好中球の新たな形態・機能が明らかにされた(図1).NETsは微生物に対する生体防御のみならず,さまざまな疾患の病態に関与していることが注目されている.皮膚疾患も例外でないことも明らかにされてきた.本稿では,NETsと各種皮膚疾患との関係について概説する.
  • 臼田 千穂, 永井 晶代, 小林 束, 杉浦 一充
    日本皮膚科学会雑誌 129(8) 1633-1638 2019年7月  
    75歳、男性。水疱性類天疱瘡(BP)と診断しプレドニゾロン(PSL)60mg/日で治療を開始した。しかし水疱の新生が続いたため、免疫グロブリン大量療法(IVIG)を施行したところ、皮膚状態は改善傾向となった。IVIG投与開始から数日後より血小板減少がみられたが、自然軽快した。その後再燃し、さらに3回のIVIGを実施し、同時に血小板輸血を行った2回目を除いて、実施する度に血小板減少をきたしたが、いずれも自然軽快した。IVIGによる血小板減少のリスクを念頭に置いて、実施前後で定期的な採血による確認が必要である。(著者抄録)
  • 杉浦 一充
    現代医学 66(1) 49-52 2019年6月  
    膿胞性乾癬(汎発型)(generalized pustular psoriasis:GPP)は急激な発熱とともに全身の皮膚が潮紅し、無菌性膿疱が多発する。病理組織学的に角層下の表皮の海綿状態に好中球性の膿瘍からなる。Kogoj海綿状膿疱を特徴とする角層下膿疱を形成する。上気道感染、抗生剤などの薬剤、妊娠、全身のステロイド投与などにより誘発され、再発を繰り返すことが本症の特徴である。GPPは多数の症例が、1つの遺伝子変異を病因とする。病因遺伝子はIL36RN遺伝子あるいはCARD14遺伝子である。IL36RN遺伝子変異では遺伝子産物のIL-36受容体拮抗因子(IL-36Ra)機能欠損を引き起こす。IL-36Ra欠損症としての膿疱形成のメカニズムに基づいた新規治療法の開発が期待されている。(著者抄録)
  • 杉浦 一充
    Derma. (284) 59-64 2019年6月  
    炎症性角化症は皮膚の炎症と表皮肥厚と過角化が同時に起こる疾患群である。代表的な疾患は乾癬である。紅皮症では湿疹・皮膚炎群以外の原因の半分を乾癬性紅皮症が占める。毛孔性紅色粃糠疹と扁平苔癬も紅皮症をきたしうる炎症性角化症である。遺伝性角化症で紅皮症を呈しうる疾患としては、先天性魚鱗癬紅皮症、表皮融解性魚鱗癬、シェーグレン・ラルソン症候群、ネザートン症候群、ラッド症候群、KID症候群がある。紅皮症でしばしば遭遇する乾癬性紅皮症の病態と治療に日頃より習熟しておくとともに、頻度の低い炎症性角化症、遺伝性角化症も鑑別として挙げることができるようにしておきたい。(著者抄録)
  • 杉浦 一充
    日本皮膚科学会雑誌 129(6) 1311-1315 2019年5月  
    最近、筆者らは自然免疫に関与する1つの遺伝子の変異が病因で炎症性角化症をひきおこす疾患群「自己炎症性角化症」を提唱した。膿胞性乾癬(汎発型)はしばしばこの自己炎症性角化症に含まれる。病因遺伝子はIL36RN遺伝子あるいはCARD14遺伝子である。IL36RN遺伝子変異により遺伝子産物のIL-36受容体拮抗因子(IL-36Ra)機能欠損を引き起こす。IL-36Ra欠損症の膿疱形成のメカニズムは以下のとおりである。最初にTLR-4リガンド、TNF-α、IL-1β、IL-17A等によりIL-36α、IL-36β、IL-36γの前駆体が誘導される。第二にIL-36α、IL-36β、IL-36γの前駆体が好中球由来のプロテアーゼでN末端が切断されて活性化する。第三にIL-36Raが機能欠損しているので、IL-36受容体以下のシグナルが持続して活性化される。最後にCXCL1やIL-8などの好中球を遊走させるケモカインが放出され、膿疱を形成されると考えられる。(著者抄録)
  • 臼田 千穂, 小林 束, 永井 晶代, 吉川 哲史, 杉浦 一充
    皮膚病診療 41(3) 221-224 2019年3月  
    <文献概要>症例のポイント ●薬剤性過敏症症候群(drug-induced hypersensitivity syndrome:DIHS)は再燃しやすく遅発性臓器障害も問題となるため,確実に診断することが望ましい.●しかし臨床的にDIHSを強く疑っても,ヒトヘルペスウイルス6(human herpesvirus:HHV-6)を同定することができずDIHSの診断にまで至らないことも少なくない.●HHV-6Bの再活性化をウイルス分離培養で同定し,DIHSを早期に診断した1例を経験した.
  • 永野 佳那, 金子 栄, 小山 千草, 杉浦 一充, 秋山 真志, 森田 栄伸
    皮膚病診療 41(1) 41-44 2019年1月  
    <文献概要>症例のポイント ・C1q腎症によるネフローゼ症候群を合併した先天性魚鱗癬様紅皮症の1例を経験した.・adenosine triphosphate-binding cassette,subfamily A,member 12 (ABCA12)の遺伝子異常が判明しており,病態との関連が疑われている.
  • 近藤 まや, 有馬 豪, 良元 のぞみ, 渡邊 総一郎, 杉浦 一充
    皮膚科の臨床 60(13) 2019-2022 2018年12月  
    <文献概要>43歳,男性。20年前より前医で尋常性乾癬に対しvery strongクラスのステロイド外用剤で治療されていた。3年前よりクロベタゾールプロピオン酸エステル(デルモベート)軟膏へ変更され,徐々に外用量が増加し,2ヵ月前より高血圧,肥満,糖尿病が増悪した。血清ACTH,コルチゾールの日内変動消失より薬剤性クッシング症候群と診断し,同薬を中止し,ステロイド内服補充を開始し,その後,尋常性乾癬に対しブロダルマブを導入した。ステロイドは外用剤であっても重大な全身性副作用をきたすことがあり,使用には細心の注意が必要である。同薬を扱うすべての医師が本疾患について熟知すべきと考える。
  • 有馬 豪, 岩田 洋平, 渡邊 総一郎, 杉浦 一充
    日本皮膚科学会雑誌 128(9) 1971-1971 2018年8月  

書籍等出版物

 15

講演・口頭発表等

 97

担当経験のある科目(授業)

 4

共同研究・競争的資金等の研究課題

 35

産業財産権

 3

その他

 1
  • 2020年2月 - 現在
    膿疱性乾癬と関節症性乾癬のモデルマウス(膿疱性乾癬と関節症性乾癬の病態を細胞・組織レベルで再現。名古屋大との共同研究で作成。Shibata A, et al. J Autoimmun 2017;80:28-38.特許第6654773号 インターロイキン36受容体アンタゴニスト欠損症の治療薬) *本研究シーズに関する産学共同研究の問い合わせは藤田医科大学産学連携推進センター(fuji-san@fujita-hu.ac.jp)まで