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Featured researches published by Atsushi Shiga.


Toxicologic Pathology | 2009

Spontaneous Ganglioneuroma Possibly Originating from the Trigeminal Ganglion in a B6C3F1 Mouse

Yuzo Yasui; Yasufumi Ohta; Yoshihide Ueda; Kazushige Hasegawa; Tohru Kihara; Masayo Hosoi; Rumiko Miyajima; Atsushi Shiga; Kiyoshi Imai; Kazuhiro Toyoda

In a carcinogenicity study, a neuronal tumor in the cranial cavity was observed in a 110-week-old female B6C3F1 mouse. At necropsy, the tumor was seen at the site of the pituitary gland. Histologically, the tumor consisted of well-differentiated ganglion cells, nerve fiber/neuropil-like elements and ganglion-like cells. The tumor was composed mainly of ganglion-like cells, which were arranged in solid sheets interspersed with thin fibrovascular stroma. Nissl substance was detected at the margin in the cytoplasm of well-differentiated ganglion cells, and nerve fibers were identified by the Kluever-Barrera method. Immunohistochemically, the well-differentiated ganglion cells were positive for S-100, neurofilament protein (NF), neuron-specific enolase (NSE), synaptophysin, and chromogranin A. The nerve fiber/neuropil-like elements were positive for S-100, NF, NSE, and glial fibrillary acidic protein (GFAP), and the ganglion-like cells were strongly positive only for NSE and synaptophysin. On the other hand, there were no pituitary cells, such as prolactin-positive or adrenocorticotropic hormone (ACTH)-positive cells in the tumor tissue. Detailed histopathological examination suggested that the tumor might be a ganglioneuroma arising from the trigeminal ganglion. This report provides additional histopathological evidence of peripheral nerve neoplasms in mice.


Toxicologic Pathology | 2015

Hepatic Lesions Caused by Large Granular Lymphocyte Leukemia in Fischer 344 Rats Similar Morphologic Features and Morphogenesis to Those of Nodular Regenerative Hyperplasia (NRH) in the Human Liver

Atsushi Shiga; Isao Narama

To characterize the hepatic lesions in Fischer 344 (F344) rats afflicted with large granular lymphocyte (LGL) leukemia, the livers of rats with LGL leukemia at various stages were examined histopathologically and immunohistochemically. The morphologic features in the livers of rats afflicted with LGL leukemia were diffuse, uniform-sized, granular, or micronodular lesions consisting of hepatocytes showing centrilobular atrophy and perilobular hypertrophy (CAPH) without fibrosis. With progression in the stage of the LGL leukemia, the severity of the CAPH of hepatocytes increased resulting in fatty change and/or single-cell necrosis, along with compensatory hyperplasia of the hepatocytes, finally resulting in lesions similar to those seen in nodular regenerative hyperplasia (NRH) in the human liver. The CAPH of hepatocytes was a nonspecific tissue adaptation against ischemia or hypoxemia and/or imbalance in blood supply due to disturbance in the portal circulation and hemolytic anemia induced by the leukemia cells. In addition, direct and/or indirect hepatocellular injuries by leukemia cells were considered to be necessary for the formation of human NRH-like lesions. Morphogenetic investigation of the livers of rats afflicted with LGL leukemia may be helpful to clarify the pathogenesis of NRH in the human liver.


Journal of Toxicologic Pathology | 2010

Study on the pathogenesis of foreign body granulomatous inflammation in the livers of sprague-dawley rats.

Atsushi Shiga; Yasufumi Ota; Yoshihide Ueda; Masayo Hosoi; Rumiko Miyajima; Kazushige Hasegawa; Fukutaro Mizuhashi

Focal granulomatous inflammation developed in the livers of five 10-week-old male Sprague-Dawley rats. The characteristic features of this lesion were the presence of foreign body multinucleated giant cells engulfing calcium deposits and site-specific development in a fissure formed in a sub-lobation in the left lobe or interlobar fissure of the medial lobe of the liver. To clarify the pathogenesis of this lesion, rat livers showing abnormal sub-lobation or lobar atrophy, rat livers in an acute dermal toxicity study and guinea pig livers in a skin sensitization test were also examined histologically. Consequently, the present lesion was considered to be a reactive change against calcium that was dystrophically deposited in the area of hepatocellular necrosis due to delayed circulatory disturbance caused by external pressure or extension force. Granulomatous lesions like in the present cases should be differentiated from those caused by evident exogenous pathogens such as chemicals or microorganisms.


Journal of Toxicologic Pathology | 2017

A spontaneous myoepithelial carcinoma in the mammary gland of an aged female ICR (CD-1) mouse

Tsuyoshi Ito; Toshinori Yoshida; Katsumi Soma; Yoshitaka Katoh; Yuko Shimada; Aya Ohnuma-Koyama; Naofumi Takahashi; Yoshimasa Okazaki; Atsushi Shiga; Maki Kuwahara; Takanori Harada

We report a female Crlj:CD1(ICR) mouse with a spontaneous mammary gland tumor composed of biphasic tumor cells, i.e., epithelioid and spindle-shaped myoepithelial cells. Macroscopically, a subcutaneous mass, approximately 3 cm in diameter was found in the lumbodorsal region. Histopathologically, the epithelioid cells proliferated in an alveolar or nest-like growth pattern, occasionally forming glandular-like structures. On the other hand, the spindle-shaped cells proliferated in a sarcomatous pattern. Normal mammary gland was observed in the vicinity of the tumor. Both types of tumor cells showed immunoreactivity for cytokeratin (wide spectrum screening), vimentin, S100, and p63. In addition, the epithelioid cells and spindle-shaped cells were immunopositive for glial fibrillary acidic protein and smooth muscle actin, respectively. Moderate atypia, high proliferative activity, massive necrosis, and partial infiltration to the surrounding tissues were also observed. We made a diagnosis of myoepithelial carcinoma, which is extremely rare in ICR mice.


Journal of Toxicologic Pathology | 2017

Spontaneous malignant myoid thymoma in an aged female Fischer 344 rat

Yoshitaka Katoh; Tsuyoshi Ito; Yuko Shimada; Aya Ohnuma-Koyama; Naofumi Takahashi; Yoshimasa Okazaki; Atsushi Shiga; Maki Kuwahara; Toshinori Yoshida; Takanori Harada

A whitish mass approximately 30 mm in diameter was noted in the anterior mediastinum of a 67-week-old female Fischer 344 rat. Histopathologically, two types of tumor cells were identified on the basis of morphologic features: epithelial tumor cells with a tubular or cord-like growth pattern and rhabdomyosarcomatous tumor cells characterized by the presence of cross-striations. Immunohistochemically, the epithelial tumor cells reacted positively for cytokeratin AE1/AE3, and some reacted positively for p63, which is expressed in normal thymic epithelial cells. The rhabdomyosarcomatous tumor cells stained positively for desmin, sarcomeric actin, and S-100 protein, which coincides with the stainability of normal thymic myoid cells. Since the tumor was also found to have malignant features such as high proliferative activity, cytologic atypia, and necrotic behavior, it was diagnosed as a malignant myoid thymoma. We believe that this is the first case report of such a tumor in a rodent.


Journal of Veterinary Medical Science | 1994

Lymphangiosarcoma in a Dog

Atsushi Shiga; Kinji Shirota; Yumi Une; Yasuo Nomura


Experimental Animals | 1993

Historical control data of organ weight and gross findings in F344/DuCrj rats and B6C3F1 mice.

Hijiri Iwata; Takashi Hagiwara; Mutsumi Katoh; Sanae Yamamoto; Seiki Yamakawa; Atsushi Shiga; Yasuhiko Hirouchi; Kazuo Kobayashi; Hiroyuki Inoue; Makoto Enomoto


Journal of Veterinary Medical Science | 2001

Combined hepatocellular and cholangiocellular carcinoma in a dog.

Atsushi Shiga; Kinji Shirota; Makoto Enomoto


Journal of Veterinary Medical Science | 1997

HEPATOBLASTOMA IN A DOG

Atsushi Shiga; Kinji Shirota; Takuo Shida; Takatsugu Yamada; Yasuo Nomura


Journal of Veterinary Medical Science | 1997

Morphological and Immunohistochemical Studies on Porcine Serum-Induced Rat Liver Fibrosis

Atsushi Shiga; Kinji Shirota; Teruo Ikeda; Yasuo Nomura

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Shinichi Mikami

Dainippon Sumitomo Pharma Co.

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