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18 results on '"Sekine, Yumi"'

1. Candesartan prevents arteriopathy progression in cerebral autosomal recessive arteriopathy with subcortical infarcts and leukoencephalopathy model

Author

Kato, Taisuke, Manabe, Ri-Ichiroh, Igarashi, Hironaka, Kametani, Fuyuki, Hirokawa, Sachiko, Sekine, Yumi, Fujita, Natsumi, Saito, Satoshi, Kawashima, Yusuke, Hatano, Yuya, Ando, Shoichiro, Nozaki, Hiroaki, Sugai, Akihiro, Uemura, Masahiro, Fukunaga, Masaki, Sato, Toshiya, Koyama, Akihide, Saito, Rie, Sugie, Atsushi, Toyoshima, Yasuko, Kawata, Hirotoshi, Murayama, Shigeo, Matsumoto, Masaki, Kakita, Akiyoshi, Hasegawa, Masato, Ihara, Masafumi, Kanazawa, Masato, Nishizawa, Masatoyo, Tsuji, Shoji, and Onodera, Osamu

Subjects
Candesartan -- Testing, CADASIL -- Drug therapy -- Models -- Development and progression, Health care industry
Abstract

Cerebral small vessel disease (CSVD) causes dementia and gait disturbance due to arteriopathy. Cerebral autosomal recessive arteriopathy with subcortical infarcts and leukoencephalopathy (CARASIL) is a hereditary form of CSVD caused by loss of high-temperature requirement A1 (HTRA1) serine protease activity. In CARASIL, arteriopathy causes intimal thickening, smooth muscle cell (SMC) degeneration, elastic lamina splitting, and vasodilation. The molecular mechanisms were proposed to involve the accumulation of matrisome proteins as substrates or abnormalities in transforming growth factor [beta] (TGF-[beta]) signaling. Here, we show that [HTRA1.sup.-/-] mice exhibited features of CARASIL-associated arteriopathy: intimal thickening, abnormal elastic lamina, and vasodilation. In addition, the mice exhibited reduced distensibility of the cerebral arteries and blood flow in the cerebral cortex. In the thickened intima, matrisome proteins, including the hub protein fibronectin (FN) and latent TGF-[beta] binding protein 4 (LTBP-4), which are substrates of HTRA1, accumulated. Candesartan treatment alleviated matrisome protein accumulation and normalized the vascular distensibility and cerebral blood flow. Furthermore, candesartan reduced the mRNA expression of Fn1, Ltbp-4, and Adamtsl2, which are involved in forming the extracellular matrix network. Our results indicate that these accumulated matrisome proteins may be potential therapeutic targets for arteriopathy in CARASIL., Introduction Cerebral small vessel disease (CSVD) is a sporadic and hereditary arteriopathy of the cerebral small vessels that results in dementia and gait disturbance (1). The molecular mechanism of CSVD [...]

Published
2021
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8. Abstract TMP92: Characteristic Brain MRI Features of Manifesting Heterozygotes With Cerebral Autosomal Recessive Arteriopathy With Subcortical Infarcts and Leukoencephalopathy

Author

Uemura, Masahiro, primary, Nozaki, Hiroaki, additional, Sekine, Yumi, additional, Mizuta, Ikuko, additional, Noda, Tomoko, additional, Miyazaki, Kazuhide, additional, Kaito, Muichi, additional, Nishimoto, Yoshinori, additional, Shimoe, Yutaka, additional, Shirata, Akiko, additional, Yamane, Kiyomi, additional, Yanagawa, Sohei, additional, Hirayama, Mikio, additional, Tamura, Masato, additional, Mizuno, Toshiki, additional, Nishizawa, Masatoyo, additional, and Onodera, Osamu, additional

Published
2017
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9. Abstract TP269: Distinct Molecular Mechanisms of Htra1 Mutants in Manifesting Heterozygotes With Carasil

Author

Nozaki, Hiroaki, primary, Kato, Taisuke, additional, Nihonmatsu, Megumi, additional, Saito, Yohei, additional, Mizuta, Ikuko, additional, Noda, Tomoko, additional, Koike, Ryoko, additional, Miyazaki, Kazuhide, additional, Kaito, Muichi, additional, Ito, Shoichi, additional, Makino, Masahiro, additional, Koyama, Akihide, additional, Shiga, Atsushi, additional, Uemura, Masahiro, additional, Sekine, Yumi, additional, Murakami, Ayuka, additional, Moritani, Suzuko, additional, Hara, Kenju, additional, Yokoseki, Akio, additional, Kuwano, Ryozo, additional, Endo, Naoto, additional, Momotsu, Takeshi, additional, Yoshida, Mari, additional, Nishizawa, Masatoyo, additional, Mizuno, Toshiki, additional, and Onodera, Osamu, additional

Published
2017
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10. Distinct molecular mechanisms ofHTRA1mutants in manifesting heterozygotes with CARASIL

Author

Nozaki, Hiroaki, primary, Kato, Taisuke, additional, Nihonmatsu, Megumi, additional, Saito, Yohei, additional, Mizuta, Ikuko, additional, Noda, Tomoko, additional, Koike, Ryoko, additional, Miyazaki, Kazuhide, additional, Kaito, Muichi, additional, Ito, Shoichi, additional, Makino, Masahiro, additional, Koyama, Akihide, additional, Shiga, Atsushi, additional, Uemura, Masahiro, additional, Sekine, Yumi, additional, Murakami, Ayuka, additional, Moritani, Suzuko, additional, Hara, Kenju, additional, Yokoseki, Akio, additional, Kuwano, Ryozo, additional, Endo, Naoto, additional, Momotsu, Takeshi, additional, Yoshida, Mari, additional, Nishizawa, Masatoyo, additional, Mizuno, Toshiki, additional, and Onodera, Osamu, additional

Published
2016
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13. MRI Features of Cerebral Autosomal Recessive Arteriopathy with Subcortical Infarcts and Leukoencephalopathy (S52.006)

Author

Nozaki, Hiroaki, primary, Sekine, Yumi, additional, Fukutake, Toshio, additional, Nishimoto, Yoshinori, additional, Shibata, Mamoru, additional, Yutaka, Shimoe, additional, Shirata, Akiko, additional, Yanagawa, Sohei, additional, Hirayama, Mikio, additional, Yamane, Kiyomi, additional, Nakano, Imaharu, additional, Suzuki, Norihiro, additional, Nishizawa, Masatoyo, additional, and Onodera, Osamu, additional

Published
2013
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17. Distinct molecular mechanisms of HTRA1mutants in manifesting heterozygotes with CARASIL

Author

Nozaki, Hiroaki, Kato, Taisuke, Nihonmatsu, Megumi, Saito, Yohei, Mizuta, Ikuko, Noda, Tomoko, Koike, Ryoko, Miyazaki, Kazuhide, Kaito, Muichi, Ito, Shoichi, Makino, Masahiro, Koyama, Akihide, Shiga, Atsushi, Uemura, Masahiro, Sekine, Yumi, Murakami, Ayuka, Moritani, Suzuko, Hara, Kenju, Yokoseki, Akio, Kuwano, Ryozo, Endo, Naoto, Momotsu, Takeshi, Yoshida, Mari, Nishizawa, Masatoyo, Mizuno, Toshiki, and Onodera, Osamu

Published
2016
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18. [Multimodal imaging of a case of acute syphilitic posterior placoid chorioretinitis].

Author

Sekine Y, Yashiro S, O'hira A, Yoshida N, Morinaga M, Nagashima N, and Katai N

Subjects
Acute Disease, Angiography, Chorioretinitis drug therapy, Humans, Male, Middle Aged, Multimodal Imaging, Ophthalmoscopy, Penicillin G therapeutic use, Syphilis drug therapy, Chorioretinitis diagnosis, Syphilis diagnosis
Abstract

Background: Acute syphilitic posterior placoid chorioretinitis (ASPPC) is a rare manifestation of ocular syphilis. We report on multimodal imaging including ophthalmoscopy, spectral-domain optical coherence tomography (SD-OCT), fluorescein angiography (FA) and indocyanine green angiography (IA) of a case diagnosed with ASPPC., Case: A 45-year-old man who was positive for human immunodeficiency virus presented with a 2-week history of visual loss in the right eye., Clinical Findings: Ophthalmoscopy showed a unilateral yellowish lesion involving the macula. SD-OCT revealed absence of the photoreceptor inner segment ellipsoid as well as an absent external limiting membrane, and nodular elevations of the retinal pigment epithelium layer at the macula. Late IA demonstrated punctate hypofluorescent dots in diffuse hyperfluorescent area corresponding to the macular lesion. Serologic tests were positive for syphilis and the patient was treated with intravenous penicillin G. Visual acuity improved with treatment from 20/100 to 20/16 and the retinal appearance returned to normal. There was completely restored stratification of the outer retina after therapy., Conclusion: In the present case of ASPPC, the SD-OCT imaging demonstrated characteristic abnormalities including RPE nodularity which showed hypofluorescent dots on late IA.

Published
2015

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