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Dive into the research topics where Tetsuhiko Toyoshima is active.

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Featured researches published by Tetsuhiko Toyoshima.


Connective Tissue Research | 2001

Collagen-Binding Domain of a Clostridium Histolyticum Collagenase Exhibits a Broad Substrate Spectrum Both in Vitro and in Vivo

Tetsuhiko Toyoshima; Osamu Matsushita; Junzaburo Minami; Nozomu Nishi; Akinobu Okabe; Toshifumi Itano

The substrate spectrum of the tandem collagen-binding domain (CBD) of Clostridium histolyticum class I collagenase (Co1G) was examined both in vitro and in vivo. CBD bound to insoluble type I, II, III and IV collagens in vitro, and to skin, aorta, tendon, kidney. trachea and corneal tissues containing various types of collagen fibrils or sheets. CBD hound to all kinds of collagen fibrils regardless of their diameters and also bound to sheet-forming collagen in the glomerular basal lamina or Descemets membrane of the cornea. This wide substrate spectrum expands possible applications of the drug delivery system we proposed previously (PNAS 95:7018-7023, 1998). Therapeutic agents fused with CBD will hind not only to subcutaneous tissues, but also to other tissues containing non-type I collagen.


Brain Research | 1987

The fibers which leave the Probst's longitudinal bundle seen in the brain of an acallosal mouse: a study with the horseradish peroxidase technique

Hiroki S. Ozaki; Tetuhide H. Murakami; Tetsuhiko Toyoshima; Masahisa Shimada

The congenital absence of the corpus callosum, a brain anomaly frequently noted in humans, has been recently found to occur in some mice of the ddN strain in our laboratory. In the brains of these mice, the Probsts longitudinal bundle is always present on both cerebral hemispheres and gives rise to some aberrant fibers toward the midline. In this research, the neuroanatomical features of these fibers were studied by iontophoretical injections of horseradish peroxidase (HRP) into the neocortex of acallosal mouse brains. The results revealed that the fibers which leave the Probsts longitudinal bundle are, at least, of 3 kinds: namely, the fibers that run out from the anterior portion of the bundle and take a U-turn ipsilaterally without crossing the midline through the septal tissue to go back again into the longitudinal bundle at the level where they have left it; the commissural fibers that leave the bundle from its middle portion and cross through a tiny bridge of tissue associated with the ventral hippocampal commissure to the opposite hemisphere; and the fibers that arise from the posterior portion of the bundle and accumulate as an anomalous fascicle below the cingulum. The observation that no labeled fibers were seen within the anterior commissure in the present HRP materials suggests that the axons from neocortex which are prevented from crossing the midline in mice with congenital absence of the corpus callosum cannot find an alternative pathway via the anterior commissure.


Neuroreport | 1999

Re-evaluation of sexual dimorphism in human corpus callosum

Saeko Oka; Osamu Miyamoto; Najma A. Janjua; Naomi Honjo-Fujiwara; Motoomi Ohkawa; Seigo Nagao; Hiroko Kondo; Taeko Minami; Tetsuhiko Toyoshima; Toshifumi Itano

To study the sexual dimorphism of human corpus cauosum (CC), we analyzed the midsaggital magnetic resonance imaging (MRI) morphometry in 67 adults aged (mean+/-s.d.) 36.82+/-9.35 years. Four specific angles of the CC were determined. All four angles in 34 females and 33 age-matched males showed a significant difference between females and males. These morphometric findings confirm a gender difference in the orientation of corpus callosum.


Journal of Histochemistry and Cytochemistry | 1999

Ultrastructural distribution of 36-kD microfibril-associated glycoprotein (MAGP-36) in human and bovine tissues.

Tetsuhiko Toyoshima; Kayoko Yamashita; Hiromi Furuichi; Tsuyoshi Shishibori; Toshifumi Itano; Ryoji Kobayashi

We observed the ultrastructural distribution of MAGP-36 by immunoelectron microscopy in human and bovine tissues. MAGP-36 was present in microfibrils associated with tropoelastin in skin, aorta, and spleen. It was not detected in microfibrils from the ocular zonule and kidney mesangium that were not associated with tropoelastin. In skin, MAGP-36 was present in both early immature elastic fibers and mature elastic fibers. In mature elastic fibers, MAGP-36 was localized around amorphous elastic cores at the elastin-microfibril interface and in electron-dense bundles. Localization of MAGP-36 in elastic fibers coincided with the distribution of lysyl oxidase, an enzyme that plays a pivotal role in the deposition of tropoelastin. These findings suggest that MAGP-36 may be involved in elastogenesis. (J Histochem Cytochem 47:1049–1056, 1999)


Neuroreport | 1996

Expression of calbindin-D28K by reactive astrocytes in gerbil hippocampus after ischaemia

Tetsuhiko Toyoshima; Shin-ichi Yamagami; Bushra Y. Ahmed; Li Jin; Osamu Miyamoto; Toshifumi Itano; Masaaki Tokuda; Hideki Matsui; Osamu Hatase

Calbindin-D28K (calbindin) is a member of the superfamily of calcium-binding proteins that is implicated in the regulation of intracellular calcium. In the adult mammalian brain, calbindin was thought to be present only in neurones, where it is believed to serve a neuroprotective role. We now report the expression of calbindin after ischaemia in reactive astrocytes in the CA1 subfield of the hippocampus. Since other calcium-binding proteins, such as S-100 and calmodulin, which induce transformation or proliferation of glia, occur in astrocytes, it is conceivable that the expression of calbindin after ischaemia might be an important part of the process of gliosis.


Acta Neurochirurgica | 1999

The chronic cell death with DNA fragmentation after post-ischaemic hypothermia in the gerbil hippocampus.

Takehiro Nakamura; Osamu Miyamoto; Shin-ichi Yamagami; Tetsuhiko Toyoshima; Tetsuro Negi; Toshifumi Itano; Seigo Nagao

Summary The long-term effects of post-ischaemic hypothermia are controversial. The purpose of this study was to examine the long-term effects of post-ischaemic hypothermia on neuronal survival in gerbils in terms of morphology and function. Hypothermia was induced at 32° C for 4 h immediately after ischaemia. Examination was performed at 1 week and at 1 month after ischaemia. Post-ischaemic hypothermia prevented CA1 neuronal damage 1 week after ischaemia. At 1 month after ischaemic insult, however, the degree of the protective effect of post-ischaemic hypothermia was reduced in the lateral and medial CA1 areas. DNA fragmentation was also observed at 1 month. The errors in the 8-arm radial maze trial were increased at 1 month. These data may indicate that cells in the CA1 area are very vulnerable to ischaemia and die after post-ischaemic hypothermia, and that their death is associated with apoptosis.


Neuroscience Research | 1984

Agenesis of the corpus callosum in ddN strain mouse associated with unusual facial appearance (flat-face)

Hiroki S. Ozaki; Tetuhide H. Murakami; Tetsuhiko Toyoshima; Masahisa Shimada

In the course of an experiment involving brother-sister matings between ddN strain mice, mice occurred with an unusual facial appearance (flat-face). Subsequently, 4 mice with flat-face were bred from the litters of the second birth (ca. 10% frequency). This flat-face was assumed to be the result of a malformed short nose, hypoplastic maxilla and mandible, and hypertelorism. These 4 flat-face mice exhibited no significant delays in growth, motor ability or the development of learning ability. Histologically, they were all characterized by an almost total absence of callosal fibers and the presence of abnormal longitudinal neuromatous bundles. Therefore, the flat-face mice may be useful as experimental animals for brain research, as one can easily judge that they lack the corpus callosum from the facial appearance.


Cell and Tissue Research | 2008

Differential gene expression of 36-kDa microfibril-associated glycoprotein (MAGP-36/MFAP4) in rat organs

Tetsuhiko Toyoshima; Tetsuya Ishida; Nozomu Nishi; Ryoji Kobayashi; Takehiro Nakamura; Toshifumi Itano

By using quantitative Western blot analysis and the real time polymerase chain reaction technique, we investigated the differential gene expression of microfibril-associated glycoprotein (MAGP-36) in rat organs. The gene was expressed highly in sites rich in elastic fibers, such as aorta, skin, and esophagus. However, MAGP-36 was also expressed highly in some other sites containing no elastic fibers. In lung and trachea, the expression levels of MAGP-36 mRNA were about seven times higher than those in other elastic tissues, although the protein abundances were almost at the same levels as other elastic tissues. MAGP-36 seemed to be secreted outside these organs. In brain, kidney, and spleen, although the expression levels of MAGP-36 mRNA were low, substantial amounts of MAGP-36 protein were detected. An immunohistochemical study revealed that MAGP-36 was present at the brush border of the S3 segment of proximal tubules in kidney. Since MAGP-36 is known to bind to mannan, MAGP-36 might be involved in mannose transport in the S3 segment. Thus, MAGP-36 might be multifunctional and present in a wide variety of sites in various organs.


Brain Research | 2014

Ameliorative effects of yokukansan on behavioral deficits in a gerbil model of global cerebral ischemia

Yanan Liu; Takehiro Nakamura; Tetsuhiko Toyoshima; Feng Lu; Kazunori Sumitani; Aya Shinomiya; Richad F. Keep; Tohru Yamamoto; Takashi Tamiya; Toshifumi Itano

The aim of this study was to investigate the neuroprotective effects of yokukansan, a traditional Kampo medicine, on the behavioral dysfunction induced by cerebral ischemia/reperfusion injury in gerbils. Gerbils were treated with yokukasan by oral gavage for 30 days, once per day, until the day before induction of ischemia, which was induced by occluding the bilateral common carotid artery for 5 min. The effects of yokukansan (50, 100 and 300 mg/kg) were examined by measuring neuronal damage and behavioral deficits (locomotor activity, 8-arm radial maze task). The anti-inflammatory and anti-oxidant properties of yokukansan were also examined. Administration of yokukansan at 300 mg/kg significantly reduced hippocampal neuronal death after brain ischemia, inhibited the ischemia-induced inflammatory response and DNA oxidative damage. Yokukansan also reduced ischemia-induced locomotor hyperactivity and improved memory impairment. These findings suggest that yokukansan can inhibit the inflammatory response, oxidative damage and subsequent neuronal death induced by cerebral ischemia/reperfusion injury, and also can contribute to improvement in neurological deficits following such injury.


Acta Medica Okayama | 2001

The contribution of low affinity NGF receptor (p75NGFR) to delayed neuronal death after ischemia in the gerbil hippocampus.

Mossa Arujuma Bagum; Osamu Miyamoto; Tetsuya Masada; Shun-ichirou Nagahata; Tetsuhiko Toyoshima

The implication of low affinity nerve growth factor receptor (p75NGFR), which is believed to play a pro-apoptotic role, in delayed neuronal death (DND) after ischemia in the gerbil hippocampus was investigated. Immunohistochemistry and Western blot analysis revealed that the presence of p75 NGFR immunoreactivity (IR) was negligible in the hippocampus of the sham control gerbil but appeared clearly in CA1 neurons 3 and 4 days after 5-min transient ischemia. Terminal deoxynucleotidyl transferase-mediated UTP nick end labeling (TUNEL) positive nuclei appeared when the level of p75NGFR IR increased. Furthermore, almost all TUNEL-positive CA1 neurons also costained for p75NGFR. These results suggest that p75NGFR contributes to DND after ischemia by an apoptotic mechanism.

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