Tohru Yoshizumi
Osaka University
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Featured researches published by Tohru Yoshizumi.
Molecular and Cellular Biochemistry | 1999
Shuichi Nozaki; Takao Tanaka; Shizuya Yamashita; Koichi Sohmiya; Tohru Yoshizumi; Fumio Okamoto; Yasushi Kitaura; Chikao Kotake; Hiroyuki Nishida; Atsuyuki Nakata; Tsutomu Nakagawa; Kengo Matsumoto; Kaoru Kameda-Takemura; Seiji Tadokoro; Yoshiyuki Kurata; Yoshiaki Tomiyama; Keishiro Kawamura; Yuji Matsuzawa
Long-chain fatty acids (LCFA) are the major energy substrate for heart and their oxidation is important for achieving maximal cardiac work. However, the mechanism of uptake of LCFA by myocardium has not been clarified. We previously reported that bovine myocardial LCFA transporter has a sequence homology to human CD36. Clinically, total defect of myocardial uptake of radiolabeled long-chain fatty acid analog [123I-BMIPP: Iodine-123 15-(p-iodophenyl)-(R,S)-methylpentadecanoic acid] has been reported in some restricted cases, but the etiology has not been clarified. In the present study, we analyzed CD36 expression and CD36 gene in subjects who showed total lack of myocardial 123I-BMIPP accumulation, and, vice versa, evaluated myocardial 123I-BMIPP uptake in subjects with CD36 deficiency. Four unrelated subjects were evaluated; Two were found to have negative myocardial LCFA accumulation by 123I-BMIPP scintigraphy, after which the expression of CD36 on their platelets and monocytes was analyzed. Remaining two subjects were identified as CD36 deficiency by screening, then 123I-BMIPP scintigraphy was performed. Expression of CD36 on platelets and monocytes was measured by flow cytometric analysis. The molecular defects responsible for CD36 deficiency was detected by allele-specific restriction enzyme analysis. CD36 expression was totally deficient in all 4 subjects on both platelets and monocytes. Two subjects were homozygous for a 478C→T mutation. One was heterozygous for the dinucleotide deletion of exon V and single nucleotide insertion of exon X, and remaining one was considered to be heterozygous for the dinucleotide deletion of exon V and an unknown gene abnormality. All cases demonstrated a completely negative accumulation of myocardial LCFA despite of normal myocardial perfusion, which was evaluated by thallium scintigraphy. In addition, all cases demonstrated apparently normal hepatic LCFA accumulation Thus, these findings suggested that CD36 acts as a major myocardial specific LCFA transporter in humans.
Annals of Medicine | 2012
Aki Hiuge-Shimizu; Ken Kishida; Tohru Funahashi; Yuko Ishizaka; Rie Oka; Minoru Okada; Shizu Suzuki; Norihide Takaya; Tohru Nakagawa; Toshiki Fukui; Hiroshi Fukuda; Naoya Watanabe; Tohru Yoshizumi; Tadashi Nakamura; Yuji Matsuzawa; Minoru Yamakado; Iichiro Shimomura
Abstract Background. The management of cardiovascular risk factors is important for prevention of atherosclerotic cardiovascular diseases (ACVD). Visceral fat accumulation plays an important role in the clustering of cardiovascular risk factors, leading to ACVD. The present study investigated the gender- and age-specific relationship between obesity-related cardiovascular risk factor accumulation and computed tomography (CT)-measured fat distribution in a large-scale Japanese general population. Methods and results. Fat distribution was measured on CT scans in 12,443 subjects (males/females = 10,080/2,363), who underwent medical health check-up at 9 centers in Japan. The investigated obesity-related cardiovascular risk factors were hyperglycemia, dyslipidemia, and elevated blood pressure. Visceral fat area (VFA) for all males and old females showed almost symmetric distribution, while that of young females showed skewed distribution with a marked left shift. Only a small proportion of young females had large visceral fat and cardiovascular risk accumulation. The mean number of risk factors exceeded 1.0 at around 100 cm2 for VFA in all groups, irrespective of gender, age (cut-off age 55), and BMI (cut-off BMI 25 kg/m2). Conclusions. In this large-scale Japan-wide general population study, an absolute VFA value of about 100 cm2 equated with obesity-related cardiovascular risk factor accumulation, irrespective of gender, age, and BMI. Clinical trial registration information. https://upload.umin.ac.jp/cgi-open-bin/ctr/ctr.cgi?function=brows&action=brows&type=summary&recptno=R000002780&language=E.
Radiology | 1999
Tohru Yoshizumi; Tadashi Nakamura; Mitsukazu Yamane; Abdul Hasan M. Waliul Islam; Masakazu Menju; Kouichi Yamasaki; Takeshi Arai; Kazuaki Kotani; Tohru Funahashi; Shizuya Yamashita; Yuji Matsuzawa
Journal of the American College of Cardiology | 2008
Takao Maruyama; Masanori Takada; Toshiaki Hasuike; Atsushi Yoshikawa; Eiji Namimatsu; Tohru Yoshizumi
American Journal of Cardiology | 2004
Takao Maruyama; Tohru Yoshizumi; Ritsu Tamura; Shigekazu Takashima; Hiroyuki Toyoshima; Ichiro Konishi; Shizuya Yamashita; Kouichi Yamasaki
The Journal of Nuclear Medicine | 1999
Kazuki Fukuchi; Shuichi Nozaki; Tohru Yoshizumi; Shinji Hasegawa; Uehara T; Tsutomu Nakagawa; Tohru Kobayashi; Yoshiaki Tomiyama; Shizuya Yamashita; Yuji Matsuzawa; Tsunehiko Nishimura
The Journal of Nuclear Medicine | 2000
Tohru Yoshizumi; Shuichi Nozaki; Kazuki Fukuchi; Koichi Yamasaki; Takahiro Fukuchi; Takao Maruyama; Yoshiaki Tomiyama; Shizuya Yamashita; Tsunehiko Nishimura; Yuji Matsuzawa
Journal of Atherosclerosis and Thrombosis | 2012
Aki Hiuge-Shimizu; Ken Kishida; Tohru Funahashi; Yuko Ishizaka; Rie Oka; Minoru Okada; Shizu Suzuki; Norihide Takaya; Tohru Nakagawa; Toshiki Fukui; Hiroshi Fukuda; Naoya Watanabe; Tohru Yoshizumi; Tetsuya Ohira; Tadashi Nakamura; Yuji Matsuzawa; Minoru Yamakado; Iichiro Shimomura
World Journal of Radiology | 2014
Miwa Ryo; Ken Kishida; Tadashi Nakamura; Tohru Yoshizumi; Tohru Funahashi; Iichiro Shimomura
Journal of Atherosclerosis and Thrombosis | 2012
Aki Hiuge-Shimizu; Ken Kishida; Tohru Funahashi; Masaaki Okutsu; Ryosuke Kametani; Hiroshi Kobayashi; Yoichi Nozaki; Akihiro Nomura; Hiroyoshi Yokoi; Tohru Yoshizumi; Tetsuya Ohira; Tadashi Nakamura; Yuji Matsuzawa; Satoru Sumitsuji; Iichiro Shimomura