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303 results on '"Okiyama N"'

1. Honey and Chamomile Activate Keratinocyte Antioxidative Responses via the KEAP1/NRF2 System

Author

Ogawa T, Ishitsuka Y, Nakamura Y, Okiyama N, Watanabe R, Fujisawa Y, and Fujimoto M

Subjects
nrf2, honey, chamomile, keratinocyte, Dermatology, RL1-803
Abstract

Tatsuya Ogawa, 1 Yosuke Ishitsuka, 1 Yoshiyuki Nakamura, 1 Naoko Okiyama, 1 Rei Watanabe, 1, 2 Yasuhiro Fujisawa, 1 Manabu Fujimoto 1, 2 1Department of Dermatology, Faculty of Medicine, University of Tsukuba, Tsukuba, Ibaraki, Japan; 2Department of Dermatology, Osaka University Graduate School of Medicine, Suita, Osaka, JapanCorrespondence: Yosuke IshitsukaDepartment of Dermatology, Faculty of Medicine, University of Tsukuba, 1-1-1 Tennodai, Tsukuba, Ibaraki 305-8575, JapanTel +81-29-853-3128Fax +81-29-853-3217Email yosuke.ishitsuka@md.tsukuba.ac.jpIntroduction: The stratum corneum protects against the entry of pathogens, allergens, and irritants while preventing dehydration. The Kelch-like erythroid cell-derived protein with cap-n-collar homology-associated protein 1 (KEAP1)/NF-E2-related factor 2 (NRF2) system maintains skin barrier homeostasis. Aggregated evidence suggests that NRF2-mediated antioxidative response is hardwired into the stratified squamous epithelia. Honey and chamomile have long been regarded as natural antioxidants. Nonetheless, it is still unclear whether they activate the KEAP1/NRF2 system in the epidermis and could promote epidermal barrier recovery.Methods: To address the abovementioned issue, we explored the antioxidative property of honey/chamomile extract by using non-cell-based KEAP1-inhibition assay and cultured human epidermal keratinocytes.Results: Herein we report that the extract inhibited KEAP1-NRF2 interaction and induced keratinocyte production of antioxidant small proline-rich protein.Conclusion: Our results may offer an opportunity to develop cosmetic products that boost NRF2-mediated antioxidative/antiaging, epidermis-intrinsic bio-responses.Keywords: NRF2, honey, chamomile, keratinocyte

Published
2020

3. POS0142 THE ASSOCIATION OF AUTOANTIBODIES WITH CLINICAL MANIFESTATIONS AND LONG-TERM REMISSIONS IN COMPARISON WITH JUVENILE- AND ADULT-ONSET IDIOPATHIC INFLAMMATORY MYOPATHIES

Author

Tsuji, H., primary, Nakashima, R., additional, Sasai, T., additional, Shirakashi, M., additional, Onizawa, H., additional, Hiwa, R., additional, Kitagori, K., additional, Akizuki, S., additional, Onishi, A., additional, Yoshifuji, H., additional, Tanaka, M., additional, Yasumi, T., additional, Ichimura, Y., additional, Okiyama, N., additional, and Morinobu, A., additional

Published
2023
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8. AUTOIMMUNE & INFLAMMATORY NMD

Author

Tanboon, J., primary, Inoue, M., additional, Saito, Y., additional, Hayashi, S., additional, Noguchi, S., additional, Okiyama, N., additional, Fujimoto, M., additional, and Nishino, I., additional

Published
2021
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11. Sweat retention anhidrosis associated with tubular aggregate myopathy

Author

Ishitsuka, Y., primary, Inoue, S., additional, Furuta, J., additional, Koguchi‐Yoshioka, H., additional, Nakamura, Y., additional, Watanabe, R., additional, Okiyama, N., additional, Fujisawa, Y., additional, Enokizono, T., additional, Fukushima, H., additional, Suzuki, H., additional, Nishino, I., additional, Kosaki, K., additional, and Fujimoto, M., additional

Published
2019
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19. 抗‐TIF‐1b 抗体与皮肌炎

Author

Ueda‐Hayakawa, I., primary, Hamaguchi, Y., additional, Okiyama, N., additional, Motegi, S., additional, Yamaoka, T., additional, Miyake, S., additional, Higashi, A., additional, Okamoto, H., additional, Takehara, K., additional, and Fujimoto, M., additional

Published
2019
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20. Anti‐TIF‐1β antibody in dermatomyositis

Author

Ueda‐Hayakawa, I., primary, Hamaguchi, Y., additional, Okiyama, N., additional, Motegi, S., additional, Yamaoka, T., additional, Miyake, S., additional, Higashi, A., additional, Okamoto, H., additional, Takehara, K., additional, and Fujimoto, M., additional

Published
2019
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22. 深度学习超越皮肤科医生

Author

Fujisawa, Y., primary, Otomo, Y., additional, Ogata, Y., additional, Nakamura, Y., additional, Fujita, R., additional, Ishitsuka, Y., additional, Watanabe, R., additional, Okiyama, N., additional, Ohara, K., additional, and Fujimoto, M., additional

Published
2019
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23. Deep learning surpasses dermatologists

Author

Fujisawa, Y., primary, Otomo, Y., additional, Ogata, Y., additional, Nakamura, Y., additional, Fujita, R., additional, Ishitsuka, Y., additional, Watanabe, R., additional, Okiyama, N., additional, Ohara, K., additional, and Fujimoto, M., additional

Published
2019
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24. Unusual Bone Lesions with Osteonecrosis Mimicking Bone Metastasis of Squamous Cell Carcinoma in Recessive Dystrophic Epidermolysis Bullosa

Author

Saito, A, primary, Nakamura, Y, additional, Tanaka, R, additional, Inoue, S, additional, Okiyama, N, additional, Ishitsuka, Y, additional, Maruyama, H, additional, Watanabe, R, additional, Yoshida, K, additional, Ishiko, A, additional, Fujimoto, M, additional, Shinkuma, S, additional, and Fujisawa, Y, additional

Published
2019
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28. Autoantibody to transcriptional intermediary factor‐1β as a myositis‐specific antibody: clinical correlation with clinically amyopathic dermatomyositis or dermatomyositis with mild myopathy

Author

Ueda‐Hayakawa, I., primary, Hamaguchi, Y., additional, Okiyama, N., additional, Motegi, S., additional, Yamaoka, T., additional, Miyake, S., additional, Higashi, A., additional, Okamoto, H., additional, Takehara, K., additional, and Fujimoto, M., additional

Published
2018
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29. Diffuse erythema with ‘angel wings’ sign in Japanese patients with anti-small ubiquitin-like modifier activating enzyme antibody-associated dermatomyositis

Author

Inoue, S., primary, Okiyama, N., additional, Shobo, M., additional, Motegi, S., additional, Hirano, H., additional, Nakagawa, Y., additional, Saito, A., additional, Nakamura, Y., additional, Ishitsuka, Y., additional, Fujisawa, Y., additional, Watanabe, R., additional, and Fujimoto, M., additional

Published
2018
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31. 521 DRB1 is the primary genetic locus contributing to susceptibility to dermatomyositis positive for anti-TIF1γ antibody in Japanese

Author

Yamaguchi, Y., primary, Kuwana, M., additional, Kanaoka, M., additional, Watanabe, T., additional, Okiyama, N., additional, Gono, T., additional, Kodera, M., additional, Kambara, T., additional, Hamaguchi, Y., additional, Seishima, M., additional, Takehara, K., additional, Fujimoto, M., additional, and Aihara, M., additional

Published
2018
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39. Autoantibody to transcriptional intermediary factor‐1β as a myositis‐specific antibody: clinical correlation with clinically amyopathic dermatomyositis or dermatomyositis with mild myopathy.

Author

Ueda‐Hayakawa, I., Hamaguchi, Y., Okiyama, N., Motegi, S., Yamaoka, T., Miyake, S., Higashi, A., Okamoto, H., Takehara, K., and Fujimoto, M.

Subjects
MYOSITIS, DERMATOMYOSITIS, MUSCLE weakness, MUSCLE diseases, INTERSTITIAL lung diseases, IMMUNOGLOBULINS, CREATINE kinase
Abstract

Summary: Background: Myositis‐specific autoantibodies (MSAs) are associated with unique clinical subsets in polymyositis/dermatomyositis (PM/DM). Autoantibodies against transcriptional intermediary factor (TIF)‐1γ and TIF‐1α are known to be MSAs. Previously, we reported that TIF‐1β is also targeted in patients with DM with or without concomitant anti‐TIF‐1α/γ antibodies. Objectives: To evaluate the clinical features of seven cases with anti‐TIF‐1β antibodies alone. Methods: Serum autoantibody profiles were determined, and protein and RNA immunoprecipitation studies were conducted. Western blotting was performed to confirm autoantibody reactivity against TIF‐1β. Results: Anti‐TIF‐1β antibody was identified by immunoprecipitation assay in 24 cases. Among them, seven patients were positive for anti‐TIF‐1β antibody alone. Six of the seven patients were classified as having DM. Among the six cases of DM, two patients had no muscle weakness and normal creatine kinase (CK) levels, and were classified as having clinically amyopathic DM. Four patients had muscle weakness, but three of them had normal serum CK levels that responded well to systemic steroids. Characteristic features of DM included skin rashes, such as Gottron sign, periungual erythema, punctate haemorrhage on the perionychium and facial erythema including heliotrope, which were observed in 86%, 57%, 86% and 71% of our cases, respectively. One of the seven patients had appendiceal cancer. None of the patients had interstitial lung disease. Conclusions: Seven patients were confirmed to have anti‐TIF‐1β antibody without any other MSAs, including TIF‐1α/γ antibodies, and six of them were diagnosed with DM. We suggest that anti‐TIF‐1β antibody is an MSA, and that it is associated with clinically amyopathic DM or DM with mild myopathy. What's already known about this topic? Previously we reported that transcriptional intermediary factor (TIF)‐1β is also targeted in patients with dermatomyositis with or without concomitant anti‐TIF‐1α/γ antibodies.Anti‐TIF‐1β antibody could be a myositis‐specific autoantibody. What does this study add? We describe seven patients with anti‐TIF‐1β antibody but without anti‐TIF‐1α/γ reactivity.Anti‐TIF‐1β antibody is possibly associated with clinically amyopathic dermatomyositis or dermatomyositis with mild myopathy. Linked Comment:Fiorentino. Br J Dermatol 2019; 180:709–710. Respond to this article Plain language summary available online [ABSTRACT FROM AUTHOR]

Published
2019
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40. Deep‐learning‐based, computer‐aided classifier developed with a small dataset of clinical images surpasses board‐certified dermatologists in skin tumour diagnosis.

Author

Fujisawa, Y., Otomo, Y., Ogata, Y., Nakamura, Y., Fujita, R., Ishitsuka, Y., Watanabe, R., Okiyama, N., Ohara, K., and Fujimoto, M.

Subjects
SKIN cancer, DIAGNOSTIC imaging, DIAGNOSIS, CANCER, MEDICAL practice, SKIN
Abstract

Summary: Background: Application of deep‐learning technology to skin cancer classification can potentially improve the sensitivity and specificity of skin cancer screening, but the number of training images required for such a system is thought to be extremely large. Objectives: To determine whether deep‐learning technology could be used to develop an efficient skin cancer classification system with a relatively small dataset of clinical images. Methods: A deep convolutional neural network (DCNN) was trained using a dataset of 4867 clinical images obtained from 1842 patients diagnosed with skin tumours at the University of Tsukuba Hospital from 2003 to 2016. The images consisted of 14 diagnoses, including both malignant and benign conditions. Its performance was tested against 13 board‐certified dermatologists and nine dermatology trainees. Results: The overall classification accuracy of the trained DCNN was 76·5%. The DCNN achieved 96·3% sensitivity (correctly classified malignant as malignant) and 89·5% specificity (correctly classified benign as benign). Although the accuracy of malignant or benign classification by the board‐certified dermatologists was statistically higher than that of the dermatology trainees (85·3% ± 3·7% and 74·4% ± 6·8%, P < 0·01), the DCNN achieved even greater accuracy, as high as 92·4% ± 2·1% (P < 0·001). Conclusions: We have developed an efficient skin tumour classifier using a DCNN trained on a relatively small dataset. The DCNN classified images of skin tumours more accurately than board‐certified dermatologists. Collectively, the current system may have capabilities for screening purposes in general medical practice, particularly because it requires only a single clinical image for classification. What's already known about this topic? Several computer‐aided classification systems have been introduced that achieve high sensitivity for melanoma detection; however, low specificity was a trade‐off for high sensitivity.The application of deep‐learning technology to skin cancer classification could potentially improve the sensitivity and specificity of skin cancer screening.The number of training images required for such a system is thought to be extremely large, and compiling large datasets for rare skin conditions is difficult. What does this study add? Our deep convolutional neural network (DCNN), trained on only 4867 images from 1842 patients, classified images of skin tumours into 14 different diagnoses more accurately than board‐certified dermatologists.The fluctuation range was only ± 3·2% by fivefold cross‐validation, showing the robustness of the system.Our DCNN system requires only a single image and provides 96·3% sensitivity and 89·5% specificity in the detection of skin cancer; however, it should be validated in a prospective clinical study before use for screening purposes in general medical practice. Linked Editorial:Janda and Soyer. Br J Dermatol 2019; 180:247–248. Plain language summary available online Respond to this article [ABSTRACT FROM AUTHOR]

Published
2019
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41. CD8 resident memory T cells with interleukin 17A‐producing potential are accumulated in disease‐naïve nonlesional sites of psoriasis possibly in correlation with disease duration.

Author

Vo, S., Watanabe, R., Koguchi‐Yoshioka, H., Matsumura, Y., Ishitsuka, Y., Nakamura, Y., Okiyama, N., Fujisawa, Y., and Fujimoto, M.

Subjects
T cells, DISEASE duration, MEMORY, PSORIASIS, CYTOTOXIC T cells
Abstract

CD8 resident memory T cells with interleukin 17A-producing potential are accumulated in disease-naïve nonlesional sites of psoriasis possibly in correlation with disease duration Although CD103 SP - sp CD8 T cells also showed augmented IL-17A production both in lesional and DN nonlesional skin (lesional skin: 2-7 ± 2-5%; DN nonlesional skin: 5-3 ± 6-3%; normal skin: 0-1 ± 0-1%), the CD103 SP + sp CD8 T SB RM sb fraction was a significantly larger source of IL-17A (Fig. c). In CD8 T cells, this IL-17A/IFN- production ratio in CD103+CD8 TRM (left) and CD103-CD8 T cells (right) from DN nonlesional skin is shown according to disease duration (n = 12). [Extracted from the article]

Published
2019
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45. Antihelix/helix violaceous macules in Japanese patients with anti‐melanoma differentiation‐associated protein 5 (MDA5) antibody‐associated dermatomyositis.

Author

Okiyama, N., Inoue, S., Saito, A., Nakamura, Y., Ishitsuka, Y., Fujisawa, Y., Watanabe, R., and Fujimoto, M.

Subjects
*MYOSITIS, *DERMATOMYOSITIS, *MACULES, *PROTEINS, *EXTRACELLULAR matrix proteins
Abstract

The article present a case study of several patients with anti-melanoma differentiation associated protein 5 (MDA5) antibody associated dermatomyositis. It mentions the diagnosis of clinically amyopathic dermatomyositis (CADM) essentially depends on cutaneous manifestations; and also mentions the recognition of distinctive rashes for anti-MDA5 antibody positive DM can greatly aid in distinguishing from other DM subsets.

Published
2019
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46. Skin resident memory T‐cell population is not constructed effectively in systemic sclerosis.

Author

Koguchi‐Yoshioka, H., Watanabe, R., Fujisawa, Y., Ishitsuka, Y., Nakamura, Y., Okiyama, N., and Fujimoto, M.

Abstract

The article discusses a study to determine the role of skin resident memory T‐cell population in systemic sclerosis (SSc) that is characterized by tissue fibrosis, vascular damage, and dysregulation of the immune system. Topics discussed include dysfunction of regulatory T cells with lower CD69 expression, immunofluorescence analysis of SSc, and humoral factors from the SSc T cells.

Published
2019
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