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Featured researches published by Jun Utsumi.


Anesthesia & Analgesia | 1999

Xenon has greater inhibitory effects on spinal dorsal horn neurons than nitrous oxide in spinal cord transected cats.

Yoshiya Miyazaki; Takehiko Adachi; Jun Utsumi; Tsutomu Shichino; Hajime Segawa

UNLABELLED Xenon (Xe) suppresses wide dynamic range neurons in cat spinal cord to a similar extent as nitrous oxide (N2O). The antinociceptive action of N2O involves the descending inhibitory system. To clarify whether the descending inhibitory system is also involved in the antinociceptive action of Xe, we compared the effects of Xe on the spinal cord dorsal horn neurons with those of N2O in spinal cord-transected cats anesthetized with alpha-chloralose and urethane. We investigated the change of wide dynamic range neuron responses to touch and pinch by both anesthetics. Seventy percent Xe significantly suppressed both touch- and pinch-evoked responses in all 12 neurons. In contrast, 70% N2O did not show significant suppression in touch- and pinch-evoked responses. These results suggest that the antinociceptive action of Xe might not be mediated by the descending inhibitory system, but instead may be produced by the direct effect on spinal dorsal horn neurons. IMPLICATIONS Xenon (Xe) is an inert gas with anesthetic properties. We examined the antinociceptive effects of Xe and nitrous oxide (N2O) in spinal cord-transected cats. Our studies indicate that Xe has a direct antinociceptive action on the spinal cord that is greater than that of N2O.


Anesthesia & Analgesia | 1997

The effect of xenon on spinal dorsal horn neurons : A comparison with nitrous oxide

Jun Utsumi; Takehiko Adachi; Yoshiya Miyazaki; Jiro Kurata; Masatoshi Shibata; Masahiro Murakawa; Toshiyuki Arai; Kenjiro Mori

We compared the effects of xenon (Xe) on the spinal cord dorsal horn neurons with those of nitrous oxide (N2 O) in cats anesthetized with chrolarose and urethane.We assessed the potency of both anesthetics by the inhibition of wide dynamic range neuron responses evoked by cutaneous noxious (pinch) stimulation to a hindpaw. During 70% Xe inhalation, the responses of 7 of 11 neurons to pinch stimulation were suppressed. N2 O, 70%, suppressed it in 8 of 11 neurons. The potency of Xe and N2 O was compared in six neurons that were suppressed by both anesthetics. After 20 min of Xe inhalation, the response to pinch was suppressed to 49.5% +/- 8.2% (mean +/- SE), while N2 O, 70% in oxygen, suppressed it to 45.9% +/- 7.9%. The difference between N2 O and Xe was not significant. We conclude that Xe and N2 O suppress the spinal cord dorsal horn neurons to a similar degree. (Anesth Analg 1997;84:1372-6)


Molecular Brain | 2011

Copy number loss of (src homology 2 domain containing)-transforming protein 2 (SHC2) gene: discordant loss in monozygotic twins and frequent loss in patients with multiple system atrophy.

Hidenao Sasaki; Mitsuru Emi; Hiroshi Iijima; Noriko Ito; Hidenori Sato; Ichiro Yabe; Takeo Kato; Jun Utsumi; Kenichi Matsubara

BackgroundMultiple system atrophy (MSA) is a sporadic disease. Its pathogenesis may involve multiple genetic and nongenetic factors, but its etiology remains largely unknown. We hypothesized that the genome of a patient with MSA would demonstrate copy number variations (CNVs) in the genes or genomic regions of interest. To identify genomic alterations increasing the risk for MSA, we examined a pair of monozygotic (MZ) twins discordant for the MSA phenotype and 32 patients with MSA.ResultsBy whole-genome CNV analysis using a combination of CNV beadchip and comparative genomic hybridization (CGH)-based CNV microarrays followed by region-targeting, high-density, custom-made oligonucleotide tiling microarray analysis, we identified disease-specific copy number loss of the (Src homology 2 domain containing)-transforming protein 2 (SHC2) gene in the distal 350-kb subtelomeric region of 19p13.3 in the affected MZ twin and 10 of the 31 patients with MSA but not in 2 independent control populations (p = 1.04 × 10-8, odds ratio = 89.8, Pearsons chi-square test).ConclusionsCopy number loss of SHC2 strongly indicates a causal link to MSA. CNV analysis of phenotypically discordant MZ twins is a powerful tool for identifying disease-predisposing loci. Our results would enable the identification of novel diagnostic measure, therapeutic targets and better understanding of the etiology of MSA.


BioMed Research International | 2015

Characteristic Gene Expression Profiles of Human Fibroblasts and Breast Cancer Cells in a Newly Developed Bilateral Coculture System

Takayuki Ueno; Jun Utsumi; Masakazu Toi; Kazuharu Shimizu

The microenvironment of cancer cells has been implicated in cancer development and progression. Cancer-associated fibroblast constitutes a major stromal component of the microenvironment. To analyze interaction between cancer cells and fibroblasts, we have developed a new bilateral coculture system using a two-sided microporous collagen membrane. Human normal skin fibroblasts were cocultured with three different human breast cancer cell lines: MCF-7, SK-BR-3, and HCC1937. After coculture, mRNA was extracted separately from cancer cells and fibroblasts and applied to transcriptomic analysis with microarray. Top 500 commonly up- or downregulated genes were characterized by enrichment functional analysis using MetaCore Functional Analysis. Most of the genes upregulated in cancer cells were downregulated in fibroblasts while most of the genes downregulated in cancer cells were upregulated in fibroblasts, indicating that changing patterns of mRNA expression were reciprocal between cancer cells and fibroblasts. In coculture, breast cancer cells commonly increased genes related to mitotic response and TCA pathway while fibroblasts increased genes related to carbohydrate metabolism including glycolysis, glycogenesis, and glucose transport, indicating that fibroblasts support cancer cell proliferation by supplying energy sources. We propose that the bilateral coculture system using collagen membrane is useful to study interactions between cancer cells and stromal cells by mimicking in vivo tumor microenvironment.


Neuroscience Letters | 1996

Nitrous oxide depresses somatocardiac sympathetic A- and C-reflexes in anesthetized rats

Takehiko Adachi; Yoshiya Miyazaki; Jiro Kurata; Jun Utsumi; Tetsutaro Shinomura; Shin-ichi Nakao; Masahiro Murakawa; Tsutomu Shichino; Kenjiro Mori

Effect of nitrous oxide (N2O) on the somatosympathetic A- and C-reflexes was investigated using artificially ventilated rats anesthetized with alpha-chloralose and urethane. Somatocardiac sympathetic A- and C-reflexes were elicited in the inferior cardiac nerve by electrical stimulation of A and C afferent fibers of the tibial nerve, respectively. Both reflexes were depressed by inhalation of N2O for 20 min. The depression was greater in the C-reflex than in the A-reflex. The depressive effects of N2O on both reflexes were unchanged after pretreatment with intravenous naloxone (0.2 or 2.0 mg/kg) or by prolongation of the inhalation of N2O for 2 h. These results suggest that the opioid receptor is not involved and that acute tolerance is not developed in the depressive action of N2O on the somatosympathetic A- and C-reflexes.


BJA: British Journal of Anaesthesia | 1999

Dexmedetomidine reduces seizure threshold during enflurane anaesthesia in cats.

Yoshiya Miyazaki; Takehiko Adachi; Jiro Kurata; Jun Utsumi; Tsutomu Shichino; Hajime Segawa


BJA: British Journal of Anaesthesia | 1998

Effect of xenon on central nervous system electrical activity during sevoflurane anaesthesia in cats: comparison with nitrous oxide.

Jun Utsumi; Takehiko Adachi; Jiro Kurata; Yoshiya Miyazaki; Masatoshi Shibata; Masahiro Murakawa; Toshiyuki Arai; Keiichiro Mori


The Journal of Japan Society for Clinical Anesthesia | 1991

Coronary artery spasm during abdominal surgery: Two episodes in the same patient

Seigo Mishima; Kyoumi Kasai; Manabu Yamamoto; Kouichi Kitoh; Hisashi Fujita; Jun Utsumi


The Journal of Japan Society for Clinical Anesthesia | 2014

A Successful Case of Percutaneous Cardiac Pacing for Sudden Cardiac Arrest during Emergency Brain Operation

Tatsunori Toyonaga; Machiko Hashimoto; Jun Utsumi; Junichiro Kotani


Archive | 2013

Urinary biomarker for use in test for prostate cancer

Kenji Nakayama; 憲司 中山; Kazuharu Shimizu; 清水 一治; Jun Utsumi; 潤 内海; Takahiro Inoue; 井上 貴博; Osamu Ogawa; 小川 修

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