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Dive into the research topics where Hiroki Aizawa is active.

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Featured researches published by Hiroki Aizawa.


Nature | 1997

Mutation of the mouse klotho gene leads to a syndrome resembling ageing.

Makoto Kuro-o; Yutaka Matsumura; Hiroki Aizawa; Hiroshi Kawaguchi; Tatsuo Suga; Toshihiro Utsugi; Yoshio Ohyama; Masahiko Kurabayashi; Tadashi Kaname; Eisuke Kume; Hitoshi Iwasaki; Akihiro Iida; Takako Shiraki-Iida; Satoshi Nishikawa; Ryozo Nagai; Yo-ichi Nabeshima

A new gene, termed klotho, has been identified that is involved in the suppression of several ageing phenotypes. A defect in klotho gene expression in the mouse results in a syndrome that resembles human ageing, including a short lifespan, infertility, arteriosclerosis, skin atrophy, osteoporosis and emphysema. The gene encodes a membrane protein that shares sequence similarity with the β-glucosidase enzymes. The klotho gene product may function as part of a signalling pathway that regulates ageing in vivo and morbidity in age-related diseases.


FEBS Letters | 1998

Structure of the mouse klotho gene and its two transcripts encoding membrane and secreted protein

Takako Shiraki-Iida; Hiroki Aizawa; Yutaka Matsumura; Susumu Sekine; Akihiro Iida; Hideharu Anazawa; Ryozo Nagai; Makoto Kuro-o; Yo-ichi Nabeshima

We previously established a novel mouse model for human aging and identified the genetic foundation responsible for it. A defect in expression of a novel gene, termed klotho (kl), leads to a syndrome resembling human aging in mice. The kl gene encodes a single‐pass membrane protein whose extracellular domain carries homology to β‐glucosidases. In this report, we present the entire mouse kl gene organization. The mouse kl gene spans about 50 kilobases and consists of five exons. The promoter region lacks a TATA‐box and contains four potential binding sites for SP1. We further show that two kl gene transcripts encoding membrane or secreted protein are generated through alternative transcriptional termination. These findings provide fundamental information for further study of the kl gene which may regulate aging in vivo.


Cellular and Molecular Life Sciences | 2000

Endothelial dysfunction in the klotho mouse and downregulation of klotho gene expression in various animal models of vascular and metabolic diseases.

Ryozo Nagai; Yuichiro Saito; Yoshio Ohyama; Hiroki Aizawa; Tatsuo Suga; Tetsuya Nakamura; Masahiko Kurabayashi; Makoto Kuro-o

Abstract. The human aging process is associated with vascular endothelial dysfunction. However, humoral factors which might protect against endothelial dysfucntion during aging have not yet been identified. We recently identified the klotho gene as a possible regulator of human aging. In the present study using the klotho-deficient heterozygous mouse, we examined whether the Klotho protein is a humoral factor protecting against endothelial dysfunction. We further cloned rat klotho cDNA and investigated whether klotho mRNA expression in rat kidney is altered under pathological conditions such as hypertension, hyperlipidemia, renal failure, and inflammatory stress. The Klotho protein itself, or its metabolites, promotes endothelial NO production in aorta as well as arterioles, and klotho mRNA in kidney is downregulated under sustained circulatory stress.


Biochemical and Biophysical Research Communications | 1998

Identification of the human klotho gene and its two transcripts encoding membrane and secreted klotho protein.

Yutaka Matsumura; Hiroki Aizawa; Takako Shiraki-Iida; Ryozo Nagai; Makoto Kuro-o; Yo-ichi Nabeshima


Biochemical and Biophysical Research Communications | 1998

Klotho Protein Protects against Endothelial Dysfunction

Yuichiro Saito; Takahiro Yamagishi; Tetsuya Nakamura; Yoshio Ohyama; Hiroki Aizawa; Tatsuo Suga; Yutaka Matsumura; Hiroaki Masuda; Masahiko Kurabayashi; Makoto Kuro-o; Yo-ichi Nabeshima; Ryozo Nagai


American Journal of Respiratory Cell and Molecular Biology | 2000

Disruption of the klotho gene causes pulmonary emphysema in mice. Defect in maintenance of pulmonary integrity during postnatal life.

Tatsuo Suga; Masahiko Kurabayashi; Yoshichika Sando; Yoshio Ohyama; Toshitaka Maeno; Yuri Maeno; Hiroki Aizawa; Yutaka Matsumura; Tomoyuki Kuwaki; Makoto Kuro-o; Yo-ichi Nabeshima; Ryozo Nagai


Biochemical and Biophysical Research Communications | 1998

Molecular cloning of rat klotho cDNA: markedly decreased expression of klotho by acute inflammatory stress.

Yoshio Ohyama; Masahiko Kurabayashi; Hiroaki Masuda; Tetsuya Nakamura; Yasushi Aihara; Tadashi Kaname; Tatsuo Suga; Masashi Arai; Hiroki Aizawa; Yutaka Matsumura; Makoto Kuro-o; Yo-ichi Nabeshima; Ryozo Nagail


Biochemical and Biophysical Research Communications | 1998

Downregulation of the klotho gene in the kidney under sustained circulatory stress in rats

Hiroki Aizawa; Yuichiro Saito; Tetsuya Nakamura; Masahiro Inoue; Tetsuro Imanari; Yoshio Ohyama; Yutaka Matsumura; Hiroaki Masuda; Shigenori Oba; Naobumi Mise; Kenjiro Kimura; Akira Hasegawa; Masahiko Kurabayashi; Makoto Kuro-o; Yo-ichi Nabeshima; Ryozo Nagai


Internal Medicine | 1998

Bilateral Coronary Ostial Stenosis and Aortic Regurgitation due to Syphilitic Aortitis

Hiroki Aizawa; Akira Hasegawa; Masashi Arai; Fumio Naganuma; Masako Hatori; Tsugiyasu Kanda; Tadashi Suzuki; Kazuhiko Murata; Yasushi Satoh; Susumu Ishikawa; Yasuo Morishita; Ryozo Nagai


Hypertension Research | 1998

ETA Receptor Antagonist Ameliorates Nephrosclerosis and Left Ventricular Hypertrophy Induced in Rat by Prolonged Inhibition of Nitric Oxide Synthesis

Tetsuya Nakamura; Toshiaki Kurashina; Yuichiro Saito; Hiroyuki Sumino; Nobuhiro Akuzawa; Hiroki Aizawa; Hironosuke Sakamoto; Zenpei Ono; Ryozo Nagai

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Makoto Kuro-o

Jichi Medical University

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Ryozo Nagai

Jichi Medical University

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Yo-ichi Nabeshima

Foundation for Biomedical Research

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Tetsuya Nakamura

Tokyo Medical and Dental University

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