Your search keyword '"Jun-ichi Kawano"' showing total 39 results

1. Periosteal Myxoid Leiomyosarcoma Histologically Mimicking Extraskeletal Myxoid Chondrosarcoma: Report of a Case with Histopathological and Cytopathological Comparison with Extraskeletal Myxoid Chondrosarcoma

Author

Tatsuya Aso, Masanobu Eguchi, Kazuhiko Yuzawa, Jun-ichi Kawano, Wataru Fujinuma, Tsuyoshi Ishida, Toru Motoi, Yoshinao Kikuchi, Asako Yamamoto, Shiori Watabe, Hiroshi Uozaki, and Kenji Sato

Subjects

Leiomyosarcoma, Pathology, medicine.medical_specialty, Histology, medicine.diagnostic_test, business.industry, Soft tissue, Chromogenic in situ hybridization, General Medicine, Extraskeletal Myxoid Chondrosarcoma, medicine.disease, Pathology and Forensic Medicine, Cytopathology, Biopsy, medicine, Immunohistochemistry, business, Myxoid Leiomyosarcoma

Abstract

Myxoid leiomyosarcoma (MLS) is a rare variant of leiomyosarcoma, with most cases occurring in the uterus. A case of MLS arising in the periosteal region of the tibia, mimicking extraskeletal myxoid chondrosarcoma (EMC), is described. The evaluation included histological and cytological comparison with EMC. The patient was a 77-year-old man with a palpable mass at the anterior aspect of the right lower leg. After diagnosis by cytopathology and biopsy examination, a wide resection was performed. The resulting cytological smears were composed primarily of spindle-shaped tumor cells in a myxoid and hemorrhagic background. Histologically, the tumor showed abundant myxoid matrix and tumor cells proliferating in a cord-like to reticular pattern, exhibiting a lace-like arrangement that mimicked EMC. Although immunohistochemical findings suggested leiomyosarcoma, a diagnosis of EMC eventually was excluded by the lack of a split signal when assessed for a rearrangement of NR4A3 by chromogenic in situ hybridization. Despite histological similarity to EMC, characteristic cytological findings of EMC such as epithelioid structures with a cord-like pattern and chondroblast-like lacunar structures were not observed in the smears of this patient’s MLS. We propose that cytopathological examination of bone and soft tissue lesions is useful as a diagnostic tool in similar cases. A total diagnostic workup, including clinical, radiographic, cytopathological, histopathological, and molecular findings, is needed to ensure an accurate final diagnosis and to reduce diagnostic error.

Published

2021

2. Usefulness of Distributing an Occluder to Be Used in a Primary Vision Screening in 3-Year-Old Children

Author

Yoshitake Shigenori, Onituka Shin, Yoshikazu Uchikawa, Jun-ichi Kawano, Kai Sayuri, Mayumi Okano, and Shogo Tamura

Subjects

Pediatrics, medicine.medical_specialty, Primary (chemistry), business.industry, medicine, General Medicine, business

Published

2017

3. Distribution and morphological changes of the Golgi apparatus duringDrosophilaspermatogenesis

Author

Masa-Toshi Yamamoto, Yoshihiro H. Inoue, Jun-ichi Kawano, and Yusaku Yasuno

Subjects

Male, Spermatid, urogenital system, Golgi Apparatus, Cell Biology, Golgi apparatus, Biology, Cell biology, symbols.namesake, medicine.anatomical_structure, Microscopy, Electron, Transmission, Meiosis, Cytoplasm, symbols, medicine, Animals, Drosophila, Telophase, Spermatogenesis, Acrosome, Developmental Biology, Anaphase

Abstract

In spermatogenesis, the Golgi apparatus is important for the formation of the acrosome, which is a sperm-specific organelle essential for fertilization. Comprehensive examinations of the spatiotemporal distribution and morphological characterizations of the Golgi in various cells during spermatogenesis are necessary for functional analyses and mutant screenings in the model eukaryote Drosophila. Here, we examined the distribution and morphology of the Golgi during Drosophila spermatogenesis with immunofluorescence and electron microscopy. In pre-meiotic germ cells, the Golgi apparatuses were distributed evenly in the cytoplasm. In contrast, they were located exclusively in two regions near the poles during the meiotic metaphase, where they were segregated prior to the chromosomes. In cells in anaphase to telophase, the Golgi were predominantly left behind in the equatorial region between the separating daughter nuclei. After completion of meiosis, the dispersed Golgi were assembled at the apical side of the spermatid nucleus to form the acrosome. Further investigation of the Golgi distribution in β2-tubulin mutants showed aberrant and uneven distributions of the Golgi among sister cells in the meiotic spermatocytes and in the post-meiotic spermatids. At the ultrastructural level, the Golgi apparatus in pre-meiotic spermatocytes comprised a pair of stacks. The two stacks were situated adjacent to each other, as if they had duplicated before entering into meiotic division. These results highlight the dynamic nature of the Golgi during spermatogenesis and provide a framework for analyzing the correlations between the dynamics of the Golgi and its function in sperm development.

Published

2013

4. 眼瞼閉鎖ラットの形態学 2. 無眼球症

Author

Soutarou, IWAMOTO, Tohru, SONODA, Jun-ichi, KAWANO, Taiki, IBUKI, 九州保健福祉大学 作業療法学科, 九州保健福祉大学 視機能療法学科, 佐藤焼酎製造場(株), Department of Occupational Therapy School of Health Science, Kyushu University of Health and Welfare, Department of Orthoptics and Visual Sciencies School of Health Science, Kyushu University of Health and Welfare, and Sato-shouchu-seizojou co.ltd.

Subjects

genetic structures, 小眼球症, ラット, 無眼球症, rat, sense organs, eye diseases, anophthalmos, microphthalmos

Abstract

Many anomalies of the visual system, bilateral anophthalmos, unilateral anophthalmos and optic nerve degeneration seem to be closely related to microphthalmos were found in KUHW-rats derived from a Wistar strain inbred colony. Nevertheless the rats have no recognizable eye and optic nerve in both sides were completely missing, their eyelids and optic tracts were present in anophthalmos rats. Diffuse axonal degeneration of the optic nerve on the affected side and contra-lateral optic tract were observed in microphthalmos rats. Breeding and morphological studies were undertaken to determine the nature of the ocular defect, as well as its cause and pathogenesis. These anomalies were found to be inherited as an autosomal recessive trait with variable expressivity. The studies of the prenatal morphogenesis of the microphthalmos suggested that the primary disorder reflects a disturbance of the neuroepithelium of the retinal anlage and results in defective early formation of the optic cup. Microphthalmos and anophthalmos are congenital ocular malformations that may create eyelid malformations because of the absence of the globe's trophic effects on the growth of the lids and orbit. It is particularly relevant in understanding the pathogenesis of microphthalmos in the human eye.

Published

2006

5. A case of parathyroid tumor arising from autotransplanted hyperplastic nodule

Author

Takashi Kojima, Mikiko Ishii, Kana Miyata, Jun-ichi Kawano, Fumihiko Tanaka, Tohru Akamine, Mamoru Kozakai, and Tomoko Shimada

Subjects

Nodule (geology), Pathology, medicine.medical_specialty, medicine, engineering, engineering.material, Biology

Abstract

背景:日常的には鏡検する機会の少ない副甲状腺腫瘍の細胞診を経験したので, 副甲状腺過形成および他に鑑別を要する甲状腺疾患の細胞像との比較検討を試みた.症例:49歳, 女性.46歳時に人工透析に伴う腎性副甲状腺機能亢進症を指摘され, 副甲状腺全摘が行われた際, その一部が甲状腺周囲筋肉内に自家移植された.3年後, 甲状腺右葉から峡部にかけて鶏卵大の低エコー領域を認めたため穿刺吸引細胞診を施行, 小型円形核に粗顆粒状の核クロマチンを有する細胞のシート状または重積性のある集塊が得られた.既往所見等から副甲状腺関連病変の再発を疑ったが, 細胞像のみからは良悪性の鑑別は困難であり, 手術材料の組織学的所見および免疫染色所見より, 自家移植された過形成組織を母地として発生した副甲状腺腫瘍と考えられた.結論:副甲状腺疾患の良悪性の細胞診での判定は困難であるが, 副甲状腺疾患の既往や甲状腺疾患細胞の鑑別点に注意することにより診断が可能と思われた.

Published

2006

6. Regeneration of gastric mucosa during ulcer healing follows pathways that correspond to the ontogenetic course of rat fundic glands

Author

Ryoko Nagaike, Akira Sawaguchi, Fumiyo Aoyama, Jun-ichi Kawano, Tsutomu Oinuma, and Tatsuo Suganuma

Subjects

Male, Pathology, medicine.medical_specialty, Biology, Pathology and Forensic Medicine, Basal (phylogenetics), Gastric glands, Gastric mucosa, medicine, Animals, Gastric Fundus, Stomach Ulcer, Rats, Wistar, Molecular Biology, Wound Healing, Regeneration (biology), Griffonia simplicifolia, Stomach, Fundic Gland, Cell Biology, General Medicine, biology.organism_classification, Immunohistochemistry, digestive system diseases, Rats, medicine.anatomical_structure, Bromodeoxyuridine, Gastric Mucosa, Glycoconjugates

Abstract

Gastric ulcers in humans are notoriously chronic and recurring lesions. Although the average individual who undergoes no treatments requires many years for healing, most studies on the healing process of the experimentally induced ulcers have mainly focused on the early stages. Natural history of the ulcer healing has not been completely revealed. We have undertaken long-term investigation up to the 150th day after the cryo-injury to shed light on the natural history of the ulcer healing process compared with developmental changes of postnatal fundic glands. By the 30th day, restitutive gastric glands were mostly seen to cover the ulcer lesions, where well-developed gland-type mucous cells, showing Griffonia simplicifolia agglutinin (GSA)-II labeling, appeared to occupy the basal portion. Most of the bromodeoxyuridine-labeled cells were superimposed on the GSA-II-positive cell zone, forming the proliferative zone. By the 150th day, the restitutive glands were complete, with all epithelial components and topology of the normal fundic glands. The process of the ulcer healing was quite compatible with the developmental changes of the postnatal fundic glands. These results imply that the regeneration of gastric epithelium during the ulcer healing follows pathways linked to the ontogenetic course of the fundic gland.

Published

2004

7. ラットの角膜と網膜における steroid sulfatase の分布

Author

Jun-ichi, KAWANO, Tatsuo, SUGANUMA, 九州保健福祉大学保健科学部視機能療法学科, 宮崎大学医学部医学科解剖学第2講座, Department of Orthoptics and Visual Sciences, School of Health Sciences, Kyushu University of Health and Welfare, and Department of Anatomy, Miyazaki Medical College, University of Miyazaki

Subjects

retina, 免疫組織化学, 角膜, ステロイドスルファターゼ, 網膜, immunohistochemistry, 酵素組織化学, steroid sulfatase, enzyme-histochemistry, sense organs, sornea, eye diseases

Abstract

Distribution of steroid sulfatase was studied immunohistochemically as well as enzyme-histochemically in rat cornea and retina. The immunostaining with a monoclonal antibody specific to the enzyme revealed that the enzyme protein was abundantly distributed in inner segments of photoreceptor cells and in retinal pigment epithelial cells. Other parts of the retina contained less amounts of the enzyme. The cornea showed no specific immunostaining. Electron microscopic immunohistochemical studies revealed that the enzyme molecules were localized in endoplasmic reticula and nuclear envelopes of the retinal cells. Distribution patterns resulted from the enzyme-histochemical studies were comparable to the immunohistochemical ones. The enzyme activity, however, was detected not only in these retinal cells, but also in corneal cells, including corneal epithelial, stroma, and endothelial cells. No regional difference on the enzyme activity was shown in the cornea.

Published

2004

8. Partial iodide organification defect caused by a novel mutation of the thyroid peroxidase gene in three siblings

Author

Tomio Kotani, Tatsuo Suganuma, Akira Hishinuma, Kazumi Umeki, Jun–ichi Kawano, Shohei Harada, and Tamio Ieiri

Subjects

endocrine system, medicine.medical_specialty, Mutation, biology, Endocrinology, Diabetes and Metabolism, Endoplasmic reticulum, Thyroid, food and beverages, Apical membrane, Compound heterozygosity, medicine.disease_cause, Exon, Endocrinology, medicine.anatomical_structure, Thyroid peroxidase, Internal medicine, embryonic structures, biology.protein, medicine, Hormone

Abstract

BACKGROUND: Three siblings with goitre and latent to mild hypothyroidism were suspected of having thyroid peroxidase (TPO) abnormality. Direct sequencing of their genomic DNAs showed two novel mutations of the TPO gene, one of which was G1687T (Gly533Cys; exon 9) and the other 1808-13del (Asp574/Leu575del; exon 10). The two mutations were compound heterozygous, as the former was found in their father's DNA as heterozygous, and the latter was found in DNA from their mother, also as heterozygous. As Gly533 and Asp574/Leu575 were well-conserved amino acids in the peroxidase superfamily, Gly533Cys- and Asp574/Leu575del-TPOs were thought to be affected structurally or functionally. In expression studies using CHO-Kl cells and mRNAs introduced with individual mutations, both mutated TPO proteins were expressed at the same molecular size as wild-type TPO and had enzyme activity, although Gly533Cys-TPO was slightly lower in efficiency of expression and more degenerative than wild-type TPO. METHODS: We examined the localization of both mutated TPOs. Gly533Cys-TPO was located on the endoplasmic reticulum (ER) and nuclear envelope but not on the plasma membrane, whereas Asp574/Leu575del-TPO was located not only on the ER and nuclear envelope but also on the plasma membrane, as wild-type TPO. Nevertheless, only one point differed between Asp574/Leu575del- and wild-type TPOs: the mutated TPO was expressed on the plasma membrane surface at less than half the rate of wild-type TPO. RESULTS: Gly533Cys-TPO synthesized almost no thyroid hormone because of its defective localization on the apical membrane surface of thyrocytes, whereas Asp574/Leu575del-TPO performed thyroid hormone synthesis at a rate of less half that of wild-type TPO. In cotransfection experiments using three combinations of wild-type and G1687T-mRNAs, wild-type and 1808-13del-mRNAs, and G1687T-, 1808-13del-mRNAs, the three kinds of mRNAs were considered to have no influence on cell surface TPO expression of another mRNA when a 50%-maximal amount of each mRNA was transfected. When a larger amount of each mRNA was transfected, the former two combinations showed the level of cell surface TPO expression obtained from the saturating amount of wild-type mRNA, whereas the last combination of mutated mRNAs covered only about half of the expression level. CONCLUSION: Defective thyroid hormone production resulting from the abnormal TPOs was at a level that caused latent hypothyroidism when the patients were born. With their growth, thyroid hormone volume gradually became inadequate and their thyroid gland enlarged compensatorily.

Published

2003

9. Cytological features and diagnostic problems of well differentiated liposarcoma

Author

Tohru Akamine, Takashi Kojima, Mikiko Ishii, Jun-ichi Kawano, Fumihiko Tanaka, and Tomoko Shimada

Subjects

Pathology, medicine.medical_specialty, Well Differentiated Liposarcoma, medicine, Biology

Abstract

目的:高分化型脂肪肉腫の細胞学的特徴を明らかにし, さらに脱分化型脂肪肉腫の細胞像および脂肪腫との鑑別点についても検討した.方法:穿刺吸引細胞診を行った高分化型脂肪肉腫 (脂肪腫類似型) 5例, 脱分化型脂肪肉腫2例, 大型の脂肪腫6例について, Papanicolaou染色およびMay-GrUenwald Giemsa染色標本を用いて, 細胞学的特徴を検討した.成績:脂肪肉腫7例すべてに, 2核の異型細胞が出現しており, 高分化型脂肪肉腫の細胞学的特徴と考えられた. May-Gruenwald Giemsa染色標本では, この2核細胞は裸核状を呈することが多いが, ときに細胞質内に空胞を認めた. 一方, 大型の異型多核細胞が高分化型3例, 脱分化型2例にみられた. 脂肪腫6例中2例にも少数の異型多核細胞を認めたが, 高分化型脂肪肉腫にみられるものに比べ異型性の程度はより軽微であった.結論:高分化型脂肪肉腫および脱分化型脂肪肉腫7例すべてにみられた2核細胞は, これらの細胞学的診断に有用な所見であると思われた. しかし, 脂肪腫の2例にもわずかに出現しており, 組織学的にも同様の所見であったこの2例は厳重なfollow upを必要とすると考えられる.細胞診断において, 2核および大型多核異型細胞の有無のみで高分化型脂肪肉腫と診断するのではなく, 脂肪腫においても出現する可能性を考慮に入れて診断することが重要である.

Published

2003

10. A case of 'adenoid cystic' carcinoma of the uterine cervix. Cytological and histological comparison with adenoid cystic carcinoma of the salivary gland

Author

Jun-ichi Kawano, Fumihiko Tanaka, Tomoko Shimada, Takashi Kojima, Tohru Akamine, and Mikiko Ishii

Subjects

Pathology, medicine.medical_specialty, Uterine cervix, medicine.anatomical_structure, Salivary gland, business.industry, Adenoid cystic carcinoma, Medicine, business, medicine.disease

Published

2003

11. Multistratified Expression of Polysialic Acid and Its Relationship to VAChT-containing Neurons in the Inner Plexiform Layer of Adult Rat Retina

Author

Soyuki Ide, Ryoko Nagaike, Tsutomu Oinuma, Yoshiko Idate, Jun-ichi Kawano, Akira Sawaguchi, and Tatsuo Suganuma

Subjects

Male, 0301 basic medicine, Histology, Vesicular Acetylcholine Transport Proteins, Blotting, Western, Vesicular Transport Proteins, Biology, urologic and male genital diseases, Immunofluorescence, Retina, 03 medical and health sciences, Immunolabeling, Vesicular acetylcholine transporter, medicine, Animals, Rats, Wistar, Fluorescent Antibody Technique, Indirect, Microscopy, Immunoelectron, Neural Cell Adhesion Molecules, Neurons, Microscopy, Confocal, 030102 biochemistry & molecular biology, medicine.diagnostic_test, Polysialic acid, Membrane Transport Proteins, Inner plexiform layer, Molecular biology, Rats, 030104 developmental biology, medicine.anatomical_structure, nervous system, Sialic Acids, Neural cell adhesion molecule, Synaptic Vesicles, sense organs, Anatomy, Carrier Proteins, Immunostaining

Abstract

We investigated the localization of polysialic acid (PSA), neural cell adhesion molecule (NCAM), and vesicular acetylcholine transporter (VAChT) in adult rat retina by using immunofluorescence with a confocal laser scanning microscope. Western blot analysis showed a typical broad smear of PSA and isoforms of NCAM (120, 140, and 180 kD). PSA immunofluorescence revealed multistratification in the inner plexiform layer (IPL). Dual immunostaining for PSA and NCAM exhibited the selective co-expression of PSA and NCAM on Müller cells. Moreover, dual immunolabeling for PSA and VAChT completely separated the five strata in the IPL. Strata 1, 3, and 5 were immunoreactive for PSA and Strata 2 and 4 for VAChT. These results suggest the possibility that PSA molecules on Müller cells are spatially related to ON and OFF retinal channels in the IPL.

Published

1999

12. Abstracts

Author

Liliam Pineda, Takayuki Harada, Akinobu Nakano, Yoshitaka Ohsugi, Akira Matsuno, Tadashi Nagashima, Susumu Takekoshi, R.Yoshiyuki Osamura, Keiichi Watanabe, Hideki Mori, Takako Nomura, Junzo Sasaki, Naritaka HEIJI, Toru KAMEYA, Ikuo KOBAYASHI, Yuichi SATO, Takeshi KAWASE, Yasuko Kato, Takeshi Baba, Nobuo Terada, Hideho Ueda, Ichiro Takayama, Yasuhisa Fujii, Shinichi Ohno, Takumi Tamayama, Masahito Watanabe, Jun Watanabe, Yasuharu Takamori, Hiroko Mondo, Shinsuke Kanamura, Hirohiko IWATSUKI, Masumi SUDA, Ichiro KUMANO, Chizuru OGAWA, Satoko Inoue, Ichiro Naito, Toshiyuki MATSUZAKI, Takeshi SUZUKI, Kuniaki TAKATA, Motohiro TAKEYA, Ryu-ichiro TOMOKIYO, Katsunori JINNOUCHI, Kiyoshi TAKAHASHI, Naoko UDAKA, Takaaki ITO, Hitoshi KITAMURA, Ryoichiro KAGEYAMA, Norimichi Nemoto, Taku Honma, Hitohiko Murakami, Wei Lu, Hisashi Ushiyama, Yoshikatsu Kanai, Wei LU, Norimichi NEMOTO, Hisashi USHIYAMA, Naohiko KOSHIKAWA, Hiroto MIZUSHIMA, Kaoru MIYAZAKI, Makoto Sano, Akihiro Umezawa, Atsushi Suzuki, Takahiro Honda, Kouji Shimoda, Jun-ichi Hata, Hirotsugu IMAEDA, Atsushi TAKAKI, Hiroshi YAMAMOTO, Naoki HAYASHI, Takaaki NAKAMURA, Mineko FUJIMIYA, Runa MASAKI, Ritsuko OHTANI-KANEKO, Kayoko YAMASHITA, Tare SAITO, Kyoji YAMADA, Susumu YAMAGUCHI, Kazuaki HIRATA, Kensuke CHIKAMORI, Keiji Suzuki, Kyoumi Nakazato, Tomomi Yoshida, Katsuyuki Nakajima, Jun-ichi Kawano, Akira Sawaguchi, Ryoko Nagaike, Tsutomu Oinuma, Tatsuo Suganuma, Hideaki TAMAKI, Shohei YAMASHINA, Ayami NAKAZAWA, Nobuteru USUDA, Yuxiu SHI, Haiping LU, Cangxia XIE, Mitsuhiro KAWATA, Hiroshi OGAWA, Mayumi NISHI, Yimu Yang, Hitoshi Ozawa, Kazunari Yuri, Mituhiro Kawata, Hitoshi OZAWA, Yimu YANG, Kazunori Ishimura, Toshiko Suzuki-Yamamoto, Kazunori Toida, Yoshihiro Tsuruo, Kikuko Watanabe, Akiko SETO-OHSHIMA, Shuichi UEDA, Yuri HAGIWARA, Atsuko ISHIZUYA-OKA, Junichiro HAMADA, Ichiro YAMAZOE, Yoshihiro TAKEUCHI, Hiroko MATSUSHITA, Hisahiro SAKAI, Hisashi KAWANO, Tadashi SAWADA, Nobuyuki KARASAWA, Ryohachi ARAI, Ikuko NAGATSU, Keiko IKEMOTO, Hiroshi SHIMODA, Yoshiaki TAKAHASHI, Seiji KATO, Satoshi Iino, and Yoshiaki Nojyo

Subjects

Histology, Physiology, Cell Biology, Biochemistry, Pathology and Forensic Medicine

Published

1999

13. Abstracts

Author

Mamoru Nagano, Atuko Fujioka, Koh Shinoda, Maki YOSHIDA, Mayumi NISHI, Zenro KIZAKI, Tadashi SAWADA, Mitsuhiro KAWATA, Kiyoshi KUROKAWA, Maki MURATA, Hisao YAMADA, Motoi KUDO, Nobuteru USUDA, Keiju KAMIJO, Ayami NAKAZAWA, Naoko OGIWARA, Masashi YAMADA, Kohei JOHKURA, Johbu ITOH, Kenji KAWAI, Akihiko SEARIZAWA, Kazuhiko YASUMURA, Kenji OGAWA, R. Yoshiyuki OSAMURA, Yawara SUMI, Masanori T. ITOH, Minoru YOSHIDA, Sadaki Yokota, Akira Sawaguchi, Jun-ichi Kawano, Ryoko Nagaike, Tsutomu Oinuma, Tatsuo Suganuma, Tsuyoshi IWATA, Hitoshi OZAWA, Emi INUI, Osamu UKIMURA, Munekado KOJIMA, Tsuneharu MIKI, Tomomi YAMAMOTO, Yasuaki SHIBATA, Masashi SHIN, Yoshitaka HISHIKAWA, Akira YAMAGUCHI, Toshimitsu KOBAYASHI, Takehiko KOJI, Norifumi FUTAGAWA, Hiroshi TAKANO, Tetsuji NAGATA, Kizashi NAGATA, Shigeru TAKETANI, Masasuke ARAKI, M. Araki, Y. Isobe, Y. Nakane, M. Tudsuki, Nobuaki SHIKATA, Airo TSUBURA, Nobukazu ARAKI, Teruhiko Okada, Vadim S. Zinchuk, Toshihiro Kobayashi, Harumichi Seguchi, Yuko Ito, Yoshinori Otsuki, Xin Li, Yutaka Yatomi, Yoshie Miura, Ryohei Katoh, Yukio Ozaki, Akira Kawaoi, Takao SENDA, Mayumi Matsuta, Morimasa Matsuta, Toshihide Akasaka, Hidehiko Suzuki, Naoya Yamazaki, Kazuhiro Yagila, Hitoshi Okamura, Akiko Ogawa, Katutosi Ito, Masako Maeda, Hirokazu Ohtaki, Hisayuki Funahashi, Seiji Shioda, Mayuko Ikebe, Hiroaki Matsumoto, Katsutoshi Ito, TOMOYUKI MATSUDA, KENSHI KAKIHARA, MASASHI UEDA, YOSHITAKA TAMADA, SEIJI HAYASHI, NORIO IIJIMA, MASAKI TANAKA, YASUHIKO IBATA, H. NAGATA, S. TAKEKOSHI, T. OHNISHI, J. ITOH, H. HASEGAWA, Y. YAMAMOTO, S. OHNO, K. WATANABE, Y Kataoka, N Iijima, K Kakihara, Y Tamada, S Hayashi, M Tanaka, S Hinuma, H Matsumoto, C Kitada, H Onda, H Honjo, Y Ibata, Keisuke INOUE, Yoshitaka TAMADA, Norio IIJIMA, Seiji HAYASHI, Masaki TANAKA, Akihiko ISHIHARA, Yasuhiko IBATA, Ikuko NAGATSU, Nobuyuki KARASAWA, Keiki YAMADA, Mikihiro Shirasu, Kazushi Kimura, Akira Mizoguchi, Chizuka Ide, Naoya Matsumoto, Masaaki Kitada, Shushovan Chakrabortty, Hideho Ueda, Takeshi Baba, Yasuko Kato, Ichiro Takayama, Yasuhisa Fujii, Nobuo Terada, and Shinichi Ohno

Subjects

Histology, Physiology, Cell Biology, Biochemistry, Pathology and Forensic Medicine

Published

1999

14. Myxoid liposarcoma and round cell liposarcoma-Cytological and morphometric study

Author

Tohru Akamine, Fumihiko Tanaka, Takashi Kojima, Jun-ichi Kawano, Tsuyoshi Ishida, Mikiko Ishii, and Tomoko Shimada

Subjects

Myxoid liposarcoma, Pathology, medicine.medical_specialty, medicine, Round Cell Liposarcoma, Biology, medicine.disease

Published

1999

15. Abstracts

Author

Xinhua Zhou, Akihiko Kudo, Hayato Kawakami, Hiroshi Hirano, M.H. FAYED, T. MAKITA, Etsuko SUZAKI, Katsuko KATAOKA, Osamu Katsumata, Kazushi Fujimoto, Shohei Yamashina, Nobuteru USUDA, Kohhei JOHKURA, Tatsuo SUGANUMA, Akira SAWAGUCHI, Ryoko NAGAIKE, Jun-ichi KAWANO, Tsutomu OINUMA, Shin-ichi Izumi, Michiko Iwamoto, Masashi Shin, Paul K. Nakano, Tadashi Ueda, Yoshimaro Ishikawa, Eri Kubo, Norio Miyoshi, Masaru Fukuda, Yoshio Akagi, H. Miki, M. Nakajima, K. Yuge, M. Taomoto, A. Tsubura, N. Shikata, H. Senzaki, Atsushi MASUDA, Takanori NAGAOKA, Masahito OYAMADA, Tetsuro TAKAMATSU, Hirokazu Furuta, Yoshinobu Hata, Keiichi Yokoyama, Tetsuro Takamatsu, J. Itoh, I. Takumi, K. Kawai, A. Serizawa, N. Sanno, A. Teramoto, R.Y. Osamura, Morimasa MATSUTA, Mayumi MATSUTA, Nishiya I, Satoru TAKAHASHI, Kazuki KAWABE, Michael M. LIEBER, Robert B JENKINS, HIRONOBU SASANO, KAZUMI IINO, TAKASHI SUZUKI, HIROSHI NAGURA, Y-B Ge, J. Ohmori, S. Tsuyama, D-H Yang, F. Murata, Kohei JOHKURA, Yan LIANG, Toshifumi MATSUI, Ayami NAKAZAWA, Susumu HIGUCHI, Yukio MATSUSHITA, Heiji Naritaka, Toru Kameya, Yuichi Sato, Hiroshi Inoue, Mitsuhiro Otani, Takeshi Kawase, Yuji KUROOKA, Kimio NASU, Shuji KAMEYAMA, Nobuo MORIYAMA, Junichi YANO, Gozo TSUJIMOTO, Tsutomu Matsushita, Masahito Oyamada, Hitoshi YAMAMOTO, Junko MATSUURA, Takako NOMURA, Junzo SASAKI, Tokio NAWA, Riko KITAZAWA, Sohei KITAZAWA, Hideyoshi KASIMOTO, Sakan MAEDA, Jun WATANABE, Kazuto Mino, Kazumasa KONDO, Shinsuke KANAMURA, Tetsuo Ueki, Takumi Takeuchi, Hiroaki Nishimatsu, Takahiro Kajiwara, Nobuo Moriyama, Kazuki Kawabe, Takashi Tominaga, Ken-ichiro Kobayashi, Sadatugu Minei, Yasuhiro Okada, Yataro Yamanaka, Taketo Ichinose, Takahiko Hachiya, Daisaku Hirano, Hajime Ishida, Kiyoki Okada, Hideaki HASEGAWA, Keiichi WATANABE, J. ITOH, H. HASEGAWA, S. UMEMURA, M. YASUDA, S. TAKEKOSHI, R.Y. OSAMURA, K. WATANABE, Kazuo TAKEDA, Tatsuya HOSHI, Katsuaki KATO, Shuichi OHARA, Ryo KONNO, Shigeru ASAKI, Takayoshi TOYOTA, Hiroo TATENO, Sumio NISHIKAWA, Fumie SASAKI, Yuko Ito, Kenji Matsumoto, Eriko Daikoku, Yoshinori Otsuki, Makoto SANO, Akihiro UMEZAWA, Hitoshi ABE, Mariko FUKUMA, Atsushi SUZUKI, Takashi ANDO, and Jun-ichi HATA

Subjects

Histology, Physiology, Cell Biology, Biochemistry, Pathology and Forensic Medicine

Published

1998

16. A protein-specific monoclonal antibody to rat liver beta 1-->4 galactosyltransferase and its application to immunohistochemistry

Author

Tsutomu Oinuma, Jun-ichi Kawano, Tatsuo Suganuma, and Soyuki Ide

Subjects

Male, Histology, medicine.drug_class, Immunoblotting, Golgi Apparatus, Biology, Monoclonal antibody, Salivary Glands, law.invention, Immunoenzyme Techniques, Mice, symbols.namesake, Antigen, Antibody Specificity, law, N-Acetyllactosamine Synthase, medicine, Animals, Rats, Wistar, Microscopy, Immunoelectron, Epididymis, Galactosyltransferase, Mice, Inbred BALB C, Antibodies, Monoclonal, Golgi apparatus, Rats, Staining, medicine.anatomical_structure, Biochemistry, Microsomes, Liver, symbols, Recombinant DNA, Immunohistochemistry, Electrophoresis, Polyacrylamide Gel, Anatomy

Abstract

We have produced a new protein-specific monoclonal antibody (MAb) to rat liver beta 1-->4 galactosyltransferase. This MAb, GTL2, was selected as the most reactive IgG to a periodate-treated antigen. Antigen and protein specificities of GTL2 were verified by immunoblotting of a non-glycosylated recombinant protein of human galactosyltransferase and enzymatically deglycosylated rat galactosyltransferase. Using GTL2, an immunohistochemical study was done in rat liver, epididymis, and salivary glands. Intense staining was observed in Golgi areas of epididymal duct epithelial cells, and submandibular and sublingual acinar cells. Hepatocytes showed weaker staining. Immunoelectron microscopic observation revealed that the staining was exclusively localized in trans-Golgi membranes of these cells.

Published

1994

17. Sialomucin in Middle Ear Cholesteatoma Perimatrix

Author

Jun-ichi Kawano, Tomoyuki Nagai, and Tatsuo Suganuma

Subjects

Pathology, medicine.medical_specialty, Tympanic Membrane, Sialomucins, Guinea Pigs, Ear, Middle, Biology, Guinea pig, Dermis, otorhinolaryngologic diseases, medicine, Animals, Humans, Middle Ear Cholesteatoma, Ear canal, Cholesteatoma, Ear Diseases, Serum Albumin, Lamina propria, Mucin, Mucins, General Medicine, Anatomy, medicine.disease, Fetuin, medicine.anatomical_structure, Otorhinolaryngology, alpha-Fetoproteins, Epidermis

Abstract

Mucosubstance histochemistry of human middle ear cholesteatoma revealed that sialomucins are abundant and sulfomucins present in small amounts in the glandlike structures of the cholesteatoma perimatrix. Based on the study, various glycoproteins were injected into the dermis of the external ear canal and infiltrated into the tympanic membranes of guinea pigs. Tympanic membranes were obtained 7 days later and light- and electron-microscopically studied. Injection of a sialomucin from bovine submaxillary gland resulted in marked proliferation of epidermis and degeneration of the lamina propria. Asialomucin prepared from sialomucin by hydrolysis produced mild thickening of the epidermis but the lamina propria was not degenerated. Fetuin and bovine serum albumin did not cause proliferation of the epidermis. Cholesterol granuloma formed in some of the specimens injected with sialomucin. The presence of sialomucin in cholesteatoma perimatrix and these experimental studies using tympanic membranes of guinea pigs suggests that sialomucins participate in the proliferation of epidermis and degeneration of subepidermal connective tissue in human middle ear cholesteatoma.

Published

1992

18. Ultracytochemichal Study of Glucose-6-Phosphate Dehydrogenase Activity

Author

Toshihisa Lee, Tetsuji Nagata, Motohiro Takeya, Takumi Imahori, Tatsuo Suganuma, K. Ito, Da Silva, Katsuhiko Mikoshiba, Masao Iwamori, Noriyoshi Nagamoto, Kinji Itow, Yasutaka Ishii, Nobuo Moriyama, Sayami Kobayashi, Ryohei Katoh, Masaki Iwai, Takuma Saito, Kazuo Chihara, Megumi Iwano, Shuii Hamazaki, Yasuhiro Kaji, Yoshiro Ebihara, Toshihiro Takizawa, Tomoko Takeshita, Noriyuki Komatsu, T. Kobayashi, Hitoshi Ishigooka, Yongli Kong, Yoichiro Takashima, Chihiro Kawasaki, Kanji Tanaka, Riko Kitazawa, Takeshi Okanoue, Yohei Hosokawa, Hitoshi Sakakibara, Shinnichi Sai, Hiroshi Kawanishi, Ken-ichi Iyama, Kaori Ihida, Yoshirou Hori, Tsunao Oh-I, Atsuko Itoh, Masahiko Mori, Mitsuhiro Kawata, Yoshihiko Kobayashi, Setsuya Fujita, Tateo Daimon, Mayuko Kunikata, Akiko Miyake, Masahiko Akai, Masahiro Koshiba, Yoshihiro Kitagawa, Shigeharu Kurimoto, Shinichiro Tsuyama, Kozo Ito, Akira Kawaoi, Shirou Nozawa, Mika Morita, Hiroshi Hirano, Yasuaki Tokuda, Kei Kashima, Satoshi Katagiri, Nobuyuki Kashio, Masaaki Fukase, Nobuaki Ito, Yoshio Aso, Michinori Mano, Joubu Itoh, Kyotaro Kanazawa, Mitsuhiko Kitaoka, Yoshihiko Iwama, Masaru Kimura, Kazuhiro Iyonaga, Shigeki Matsubara, Mitsuoki Eguchi, Masamichi Itoh, Tetsuhiro Minamikawa, Noriko Yamasaki, Yoshinari Hirano, Takayuki Harada, Koshiro Hioki, Mitsuyasu Toyoda, H. Seguchi, Takanori Hattori, K. Watanabe, Shingo Kawahara, Taketoshi Sugiyama, Ryoji Kushima, Manabu Mukobayashi, Tadaomi Hirota, Akihiro Hemmi, Toshio Yamashita, Nobukazu Araki, Koichi Suzuki, Yong-Xi Cui, Tetsuro Takamatu, J. Figueredo, Motomu Kashiwadani, Shigeo Mori, Fusayoshi Murata, Robert Yoshiyuki Osamura, Masayuki Andoh, Shigeru Morikawa, Kazuya Uri, Takashi Kitaoka, Kiyoshi Takahashi, Kuniaki Takata, Jun-ichi Kawano, Utsunomiya H, Keiji Kawamoto, E-iti Yokomura, Yasuhiko Ibata, Harubumi Kasai, Sohei Kitazawa, Taiji Katoh, Toshimitsu Ishibashi, Tsutomu Oinuma, Hirobumi Kumazawa, Kazuhiro Kawai, Jun Kita, K. Uchida, Taro Tamada, Yasuhiro Wada, Yoshiko Itoh, Sakan Maeda, Yoshio Ooi, and Tadami Kumazawa

Subjects

Pyruvate dehydrogenase lipoamide kinase isozyme 1, Glucose-6-phosphate dehydrogenase activity, Histology, Biochemistry, Physiology, Chemistry, Cell Biology, Pyruvate dehydrogenase phosphatase, Branched-chain alpha-keto acid dehydrogenase complex, Pathology and Forensic Medicine

Published

1992

19. Subcellular localization of N-acetylglucosaminide beta 1----4 galactosyltransferase revealed by immunoelectron microscopy

Author

Tatsuo Suganuma, Hisako Muramatsu, Kaori Ihida, Takashi Muramatsu, Fusayoshi Murata, and Jun-ichi Kawano

Subjects

Male, Histology, Nuclear Envelope, medicine.drug_class, Immunoelectron microscopy, Cell, Golgi Apparatus, Monoclonal antibody, Epithelium, Mice, N-Acetyllactosamine Synthase, Testis, Tumor Cells, Cultured, medicine, Animals, Microscopy, Immunoelectron, Epididymis, Galactosyltransferase, Sertoli Cells, Chemistry, Stomach, Teratoma, Antibodies, Monoclonal, Leydig Cells, Rats, Inbred Strains, Seminiferous Tubules, Subcellular localization, Sertoli cell, Spermatozoa, Molecular biology, Rats, Foveolar cell, Jejunum, Seminiferous tubule, medicine.anatomical_structure, Anatomy, Subcellular Fractions

Abstract

We prepared a monoclonal antibody (MAb) against N-acetylglucosaminide beta 1----4 galactosyltransferase purified from F9 embryonal carcinoma cells. The MAb recognized the protein portion of the enzyme, since it inhibited galactosyltransferase activity, reacted with the enzyme both from F9 cells and from bovine milk, and did not exhibit anti-carbohydrate activity. Using this MAb, we studied the subcellular localization of the enzyme by immunoelectron microscopy. Intense staining was observed in trans-Golgi stacks within testicular interstitial cells and mucous neck cells, confirming the specificity of the immunological reaction. Cell surface galactosyltransferase was detected in the following regions: cultured cells such as F9 embryonal carcinoma cells, testicular interstitial cells, seminiferous tubule epithelial cells, Sertoli cells, the head of the epididymal sperm, epididymal epithelial cells, and apical surfaces of epithelial cells in the fundic gland and of intestinal goblet cells. The use of Triton X-100 intensified the cell surface immunoreactivity, and in certain cases the mode of distribution of the cell surface enzyme was different from that described in previous reports. In addition, nuclear envelopes of cultured cells were distinctly stained. The possible significance of the latter finding is discussed in relation to recent advances in nuclear localization of glycoproteins.

Published

1991

20. Regional distribution of steroid sulfatase in the rat epididymal duct. Enzyme-histochemical, immuno-histochemical and biochemical studies

Author

Tsutomu Oinuma, Eizo Aikawa, Jun-ichi Kawano, and Tatsuo Suganuma

Subjects

chemistry.chemical_classification, endocrine system, Histology, urogenital system, Physiology, medicine.medical_treatment, Cell Biology, Estradiol binding, Epididymis, Biochemistry, Epithelium, Pathology and Forensic Medicine, Steroid hormone, medicine.anatomical_structure, Enzyme, chemistry, medicine, Steroid sulfatase, Immunohistochemistry, Binding site

Abstract

Regional distribution of steroid sulfatase was studied in the rat epididymal duct by enzyme-histochemical, immuno-histochemical and biochemical methods. A large amount of the enzyme was localized in the proximal part of the caput. This specific localization resulted from regional differences in the amount of the enzyme in principal cells, major constituents of the epithelium. In principal cells the amount of the enzyme, largest in the proximal part of the caput, drastically decreased caudally. In the corpus and cauda, principal cells possessed trace amounts of the enzyme, while clear cells had a large amount. Distribution of the enzyme generally agreed with that of estradiol binding sites.

Published

1991

21. Beyond vasodilation: the antioxidant effect of adrenomedullin in Dahl salt-sensitive rat aorta

Author

Toshihiko Yanagita, Jun-ichi Kawano, Tanenao Eto, Alex F. Chen, Toshihiro Tsuruda, Yuan-Ning Cao, Tatsuo Suganuma, Kazuo Kitamura, Yasuko Nagoshi, Kenji Kuwasako, Akihiko Wada, and Johji Kato

Subjects

medicine.medical_specialty, Antioxidant, Endothelium, Nitric Oxide Synthase Type III, medicine.medical_treatment, Biophysics, Vasodilation, Aorta, Thoracic, Blood Pressure, In Vitro Techniques, Biochemistry, Antioxidants, Adrenomedullin, Enos, Superoxides, medicine.artery, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Molecular Biology, Saline, Aorta, Rats, Inbred Dahl, biology, Chemistry, Cell Biology, biology.organism_classification, Recombinant Proteins, Rats, Nitric oxide synthase, Endocrinology, medicine.anatomical_structure, biology.protein, Endothelium, Vascular, Nitric Oxide Synthase, Peptides

Abstract

We have investigated the antioxidant effect of adrenomedullin (AM) on endothelial function in the Dahl salt-sensitive (DS) rat hypertension model. Dahl salt-resistant (DR) and DS rats were fed an 8% NaCl diet. In addition, the DS rats were subcutaneously infused with either saline or recombinant human AM for 4 weeks. Although systolic blood pressures measured weekly in AM- and saline-infused rats did not significantly differ, aortic O2*- levels were significantly (P0.01) higher in the latter. Likewise, both endothelial nitric oxide synthase (eNOS) mRNA and protein were significantly higher in saline-infused DS rats. Infusion of AM reduced both O2*- and eNOS expression to levels comparable to those seen in DR rats. AM infusion also upregulated the gene expression of guanosine-5'-triphosphate cyclohydrolase I and downregulated the expression of p22(phox), suggesting that AM increased the NOS coupling and bioavailability of NO. AM possesses significant antioxidant properties that improve endothelial function.

Published

2005

22. Comparative analysis and characterization of mutated thyroid peroxidases with disturbance expressed on the cell surface

Author

Tomio Kotani, Ikuo Yamamoto, Jun-ichi Kawano, Yatsuki Aratake, and Kazumi Umeki

Subjects

Protein Folding, Immunoprecipitation, Calnexin, Cell, CHO Cells, medicine.disease_cause, Biochemistry, Iodide Peroxidase, Endocrinology, Cricetulus, Cricetinae, medicine, Animals, Humans, Point Mutation, RNA, Messenger, Molecular Biology, Messenger RNA, Mutation, biology, Cell Membrane, Transfection, Molecular biology, medicine.anatomical_structure, biology.protein, Antibody, Intracellular

Abstract

Five mutated thyroid peroxidases (TPO) with varying degrees of disturbance in cell surface expression, probably owing to misfolding, were comparatively analyzed. CHO-K1 cells transfected with these mutated mRNAs expressed TPO protein in 65.6–82.1% of cells in antibody staining, and the TPOs were located in intracellular structures like the nuclear envelope and ER as well as cytoplasmically like wild-type TPO. When cell surface expression was examined, three mutated TPOs, G533C-, D574/L575del-, and G771R-TPOs, were expressed to varying degrees. In contrast, R175Q- and R665W-TPOs were thought not to be expressed on the cell surface, although a vague increment in R175Q-TPO was observed with increasing amounts of mRNA. In the kinetic study, three mutated TPOs having insufficient expression on the cell surface showed delays in decrease at 4 and 8 h after chase, although between 8 and 24 h after chase they decreased rapidly, as did the two other mutated TPOs. In immunoprecipitation by anti-TPO antibody, G533C-, D574/L575del-, and G771R-TPOs exhibited increasing interaction with calnexin. The combined evidence suggested that some of the mutated TPOs with disturbance in cell surface expression, probably owing to misfolding, exhibited the delay in kinetics of newly synthesized protein as a result of increasing interaction with calnexin and that such TPOs could be expressed to some extent on the cell surface.

Published

2004

23. A Novel Missense Mutation in the Thyroid Peroxidase Gene, R175Q, Resulting in Insufficient Cell Surface Enzyme in Two Siblings

Author

Ikuo Yamamoto, Yozo Ichiba, Yatsuki Aratake, Kazumi Umeki, Mahoko Furujo, Tatsuo Suganuma, Jun-ichi Kawano, and Tomio Kotani

Subjects

medicine.medical_specialty, endocrine system, Goiter, TPO gene, Original, Endocrinology, Diabetes and Metabolism, Cell, medicine.disease_cause, Compound heterozygosity, Endocrinology, fluids and secretions, Thyroid peroxidase, Internal medicine, medicine, Missense mutation, Gene, Mutation, goiter, biology, business.industry, missense mutation, food and beverages, congenital hypothyroidism, hemic and immune systems, medicine.disease, Congenital hypothyroidism, medicine.anatomical_structure, Pediatrics, Perinatology and Child Health, embryonic structures, biology.protein, business

Abstract

Thyroid peroxidase (TPO) abnormality is one of the causes of congenital hypothyroidism. Two missense mutations were found as a compound heterozygous mutation in two siblings with congenital goitrous hypothyroidism. One of these mutations, G614A (R175Q), was a novel mutation. Characterization of the novel mutation and a cotransfection experiment with two mutated TPO mRNAs were carried out. G614A-mRNA introduced into CHO-K1 cells expressed TPO protein with the same molecular weight as that of wild-type mRNA. The R175Q-TPO was thought to possess enzyme activity. In terms of localization, a very small amount of mutated TPO was expressed on the plasma membrane of CHO-K1 cells. This plasma membrane expression of R175Q-TPO was insufficient to perform thyroid hormone synthesis, but was markedly different from R665W-TPO. When G614A- and C2083T-mRNAs were cotransfected, cell surface TPO-positive cells were only 13.1% in contrast to 54.4% for wild-type mRNA. The low positivity and intensity of cell surface TPO suggested that in the patients' thyroids thyroid hormone synthesis was hardly performed. The congenital hypothyroidism of the patients was thought to be a result of the mutations of the TPO gene (G614A/C2083T).

Published

2003

24. Cryofixation processing is an excellent method to improve the retention of adrenomedullin antigenicity

Author

Jun-ichi Kawano, Toshihiro Aoki, Tanenao Eto, Akira Sawaguchi, Tatsuo Suganuma, Soyuki Ide, Hiroaki Yuchi, and Kazuo Kitamura

Subjects

Male, Pathology, medicine.medical_specialty, Histology, Cryofixation, law.invention, Adrenomedullin, law, Adrenal Glands, medicine, Animals, Rats, Wistar, Microscopy, Immunoelectron, Molecular Biology, Cryopreservation, Chemistry, Myocardium, Cardiac muscle, Cell Biology, Immunogold labelling, Immunohistochemistry, Rats, Medical Laboratory Technology, medicine.anatomical_structure, Freeze substitution, Electron microscope, Adrenal medulla, Peptides, Immunostaining

Abstract

We reappraised the precise immunohistochemical localization of adrenomedullin (AM) by means of the combined use of the catalyzed signal amplification (CSA) system and plunge freezing (PF)/freeze substitution (FS) for light microscopy or high-pressure freezing (HPF)/FS for electron microscopy, focusing on the rat adrenal gland and heart. In the case of adrenal glands, the PF processing showed that almost all medullary cells were intensively immunoreactive, while the cortical cells showed weak immunoreaction. In the heart, almost all cardiac muscle cells of the atria were also vividly stained with the PF/FS and the CSA enhancement. On the contrary, traces of immunoreactions were seen in most of the ventricular cells. These results are consistent with the previous reports of AM radioimmunoassays and the expression of AM mRNA. However, the chemical fixation processing revealed heterogeneous immunostaining in the atrial and ventricular myocardium as well as the adrenal medulla. Intensity of the immunostaining in the chemically fixed tissues was not likely to correspond with that of AM radioimmunoassays. The HPF/FS processing clearly demonstrated the immunogold labeling on secretory granules of adrenal medullary cells as well as cardiac muscle cells of the right auricles. Immunogold labeling intensity of the cryofixed specimens was 3- to 25-fold higher than that of the chemically fixed ones.

Published

2002

25. Identification and characterization of an insect homologue of the vertebrate Golgi apparatus protein 1 (MG-160/cysteine-rich fibroblast growth factor receptor/E-selectin ligand-1/latent transforming growth factor-beta complex protein-1) with a Golgi-specific monoclonal antibody

Author

Tomio Kotani, Tatsuo Nakayama, Jun-ichi Kawano, Tatsuo Suganuma, Masa-Toshi Yamamoto, and Hiroshi Matsubayashi

Subjects

Histology, Sialoglycoproteins, Golgi apparatus protein 1, Molecular Sequence Data, Fluorescent Antibody Technique, Golgi Apparatus, Receptors, Cell Surface, Biology, Spodoptera, Cell Line, symbols.namesake, Animals, Drosophila Proteins, Amino Acid Sequence, Molecular Biology, Peptide sequence, FGF10, Membrane Glycoproteins, Sequence Homology, Amino Acid, Insulin-like growth factor 2 receptor, Antibodies, Monoclonal, Cell Biology, Fibroblast growth factor receptor 4, Golgi apparatus, Immunohistochemistry, Receptors, Fibroblast Growth Factor, Medical Laboratory Technology, Transmembrane domain, Microscopy, Electron, Biochemistry, Latent TGF-beta Binding Proteins, Vertebrates, symbols, Cation-dependent mannose-6-phosphate receptor

Abstract

A monoclonal antibody 14F10 was raised against Golgi fractions from Sf21 cells and selected as Golgi specific. Immunohistochemical stainings with the antibody localized the antigen in Golgi cisterns of the cells. The antigen was purified and shown to be a 130-K membrane protein with N-glycans and intrachain disulfide bonds. Amino acid sequencing of its peptide fragments revealed that the antigen contained homologous sequences to those encoded by CG7190 and CG7193 Drosophila melanogaster genes. No possible transmembrane domain existed in these deduced amino acid sequences, while one did in that encoded by CG7195, an adjacent gene to CG7193. Furthermore, 5' and 3' expression sequence tags of LD19434 had been mapped to CG7190 and a downstream region of CG7195, respectively. These findings supported that all of these genes actually composed a single gene, which encoded an orthologous protein to a vertebrate Golgi-resident protein, Golgi apparatus protein 1, also called cysteine-rich FGF receptor, E-selectin ligand-1, or latent TGF-beta complex protein-1. Our results suggested that the Golgi apparatus protein 1 played a critical role in the Golgi cisterns through the animal kingdom.

Published

2002

26. Fluid dynamics of the excretory flow of zymogenic and mucin contents in rat gastric gland processed by high-pressure freezing/freeze substitution

Author

Kyoko Hotta, Tsutomu Oinuma, Akira Sawaguchi, Jun-ichi Kawano, Kazuhiko Ishihara, and Tatsuo Suganuma

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Histology, Freeze Substitution, 03 medical and health sciences, Potassium Permanganate, Gastric glands, medicine, Organometallic Compounds, Animals, Frozen Sections, Rats, Wistar, Enzyme Precursors, 030102 biochemistry & molecular biology, biology, Staining and Labeling, Chemistry, Griffonia simplicifolia, Mucin, Mucins, Immunogold labelling, biology.organism_classification, Molecular biology, Immunohistochemistry, Staining, Rats, 030104 developmental biology, medicine.anatomical_structure, Freeze substitution, Lead, Excretory system, Gastric Mucosa, Ultrastructure, Anatomy

Abstract

The high-pressure freezing/freeze substitution technique followed by Lowi-cryl K4M embedding provided an excellent ultrastructure and retention of antigenicity of rat gastric glands as well as the intraluminal fluid contents. By taking this advantage, we histochemically investigated the excretory flow of the zymogenic and mucin contents in rat gastric glandular lumen at the ultrastructural level. The combination of KMnO4-UA/Pb staining for zymogenic contents and Griffonia simplicifolia agglutinin-II (GSA-II) labeling for mucous neck cell (MNC) mucin distinguished the exocytosed zymogenic contents from the MNC mucin in the glandular lumen. Interestingly, at the base and neck regions, the zymogenic contents showed a droplet-like appearance, forming a distinct interface with the MNC mucin. At the pit region, the GSA-II labeling demonstrated restricted paths, designated as MNC mucous channels, which flowed into the surface mucous gel layer. It should be noted that the interface between exocytosed zymogenic contents and MNC mucin disappeared, and that the zymogenic contents merged into the MNC mucous channels. At the top pit region, the surface mucous gel layer showed laminated arrays of three types of gastric mucins. On the basis of these ultrastructural findings, we propose a model of the excretory flow in rat gastric gland.

Published

2002

27. A monoclonal antibody against insect CALNUC recognizes the prooncoprotein EWS specifically in mammalian cells. Immunohistochemical and biochemical studies of the antigen in rat tissues

Author

Ryoko Nagaike, Akira Sawaguchi, Tatsuo Nakayama, Tatsuo Suganuma, Tomio Kotani, Tsutomu Oinuma, Yasunari Takami, and Jun-ichi Kawano

Subjects

Male, Histology, Tissue Fixation, medicine.drug_class, Nerve Tissue Proteins, Monoclonal antibody, Heterogeneous-Nuclear Ribonucleoproteins, chemistry.chemical_compound, Epitopes, Mice, Antigen, Antibody Specificity, Formaldehyde, medicine, Tumor Cells, Cultured, Animals, Humans, Nucleobindins, Tissue Distribution, Nuclear protein, Rats, Wistar, Paraformaldehyde, Growth Substances, Molecular Biology, Mammals, biology, Calcium-Binding Proteins, Antibodies, Monoclonal, Cell Biology, Molecular biology, Immunohistochemistry, Staining, Rats, Blot, DNA-Binding Proteins, Medical Laboratory Technology, chemistry, Ribonucleoproteins, Organ Specificity, biology.protein, Insect Proteins, Calcium, Antibody, RNA-Binding Protein EWS

Abstract

A monoclonal antibody against insect CALNUC was shown to recognize an 85-kDa nuclear protein specifically in mammalian cells. Amino acid sequencing of the protein purified from rat liver revealed it to be EWS, a prooncoprotein for Ewing sarcomas and related tumors. Using the antibody, distribution of EWS was studied in rat tissues fixed with 4% paraformaldehyde by immunohistochemical methods. On thaw-fixed cryosections or those of perfusion-fixed tissues, almost all cell nuclei showed the specific staining. In immersion-fixed tissues, the staining unexpectedly disappeared in particular tissues (kidney cortex, liver, etc.), although it was recovered by autoclaving the cryosections. Western blotting also demonstrated the ubiquitous expression of EWS in the tissues. In extracts from the liver, the 85-kDa band rapidly disappeared in a Ca(2+)-dependent manner, but never in the testis. The antigen was very labile in kidney homogenates even without Ca2+. Biochemical studies with digoxigenin-labeled EWS showed that the Ca(2+)-dependent disappearance was associated with upward mobility shifts of EWS. These suggested that EWS was ubiquitously expressed in rat tissues, and that the antigen was masked in particular tissues during the immersion fixation.

Published

2001

28. A simple contrast enhancement by potassium permanganate oxidation for Lowicryl K4M ultrathin sections prepared by high pressure freezing/freeze substitution

Author

Jun-ichi Kawano, Akira Sawaguchi, Tsutomu Oinuma, Y. Goto, Tatsuo Suganuma, and Soyuki Ide

Subjects

Histology, Duodenum, Analytical chemistry, Acrylic Resins, Uranyl acetate, Citric Acid, Pathology and Forensic Medicine, law.invention, chemistry.chemical_compound, Potassium Permanganate, law, Freezing, Organometallic Compounds, Pressure, Animals, Rats, Wistar, Staining and Labeling, Tissue Embedding, Histocytochemistry, Stomach, Epithelial Cells, Immunogold labelling, Image Enhancement, Staining, Rats, Potassium permanganate, Microscopy, Electron, Membrane, Jejunum, chemistry, Freeze substitution, Lead, Colloidal gold, Electron microscope, Oxidation-Reduction, Nuclear chemistry, Electron Probe Microanalysis

Abstract

A simple contrast enhancement method is presented for Lowicryl K4M ultrathin sections prepared by high pressure freezing/freeze substitution. The sections were treated with an acidified potassium permanganate oxidizing solution followed by uranyl acetate and lead citrate staining. The method, designated KMnO4–UA/Pb staining, provided a much greater contrast in electron microscopy than conventional UA/Pb staining. In detail, the visibility of plasma membrane was especially improved and the nuclear heterochromatin, mitochondria and cytoplasmic ribosomes showed an adequate increase in electron density. In the mucous cells of rat Brunner's glands, the Golgi cisternae were well defined with the KMnO4–UA/Pb staining. Interestingly, the membranes of the intermediate compartments were moderately reactive to the KMnO4–UA/Pb staining, whereas the cis and the trans compartments were only faintly stained. It should be emphasized that the KMnO4 oxidation following colloidal gold labelling did not cause a remarkable reduction of immunogold labelling and the enhanced contrast helped us to examine the gold particles with high accuracy. This contrast enhancement method is highly promising, with the potential to become a useful tool for histochemical investigation, including immunocytochemistry with the Lowicryl K4M ultrathin sections prepared by high pressure freezing/freeze substitution techniques.

Published

2001

29. Reappraisal of potassium permanganate oxidation applied to Lowicryl K4M embedded tissues processed by high pressure freezing/freeze substitution, with special reference to differential staining of the zymogen granules of rat gastric chief cells

Author

Hiromasa Tojo, Ryoko Nagaike, Tsutomu Oinuma, Tatsuo Suganuma, Akira Sawaguchi, Jun-ichi Kawano, Mitsuhiro Okamoto, and Soyuki Ide

Subjects

Male, Histology, Freeze Substitution, Acrylic Resins, Cytoplasmic Granules, Phospholipases A, Cryofixation, Fixatives, Potassium Permanganate, Gastric glands, medicine, Organometallic Compounds, Pressure, Animals, Tissue Embedding, Citrates, Rats, Wistar, Coloring Agents, Chief Cells, Gastric, Enzyme Precursors, Staining and Labeling, Chemistry, Differential staining, Zymogen granule, Staining, Rats, Gastric chief cell, Microscopy, Electron, Phospholipases A2, medicine.anatomical_structure, Freeze substitution, Biochemistry, Lead, Oxidation-Reduction, Electron Probe Microanalysis

Abstract

The high pressure freezing/freeze substitution technique is known to yield a deep vitreous freezing of tissues. Combination of this technique with Lowicryl K4M embedding allows us histochemical studies of dynamic cellular processes with improved structural preservation. The disadvantage of Lowicryl K4M embedding is its poor electron density in electron microscopy. To address this problem, we examined the effects of KMnO4 oxidation applied to Lowicryl K4M embedded rat gastric glands processed by high pressure freezing. The KMnO4 oxidation-uranyl acetate-lead citrate sequence succeeded not only in contrast enhancement of cellular components, but also in differential staining of the zymogen granules of rat gastric chief cells. This technique could be applied to semi-thin sections of Lowicryl K4M embedded rat gastric glands. The KMnO4 oxidation-toluidine blue staining provided sufficient contrast with regard to the zymogen granules. Various experiments used in this study verified that the KMnO4 oxidation plays an essential role in the differential staining of the zymogen granules. Combined use of the KMnO4 oxidation with phospholipase A2-immunostaining demonstrated that gold labeling was localized to the zymogen granules without the loss of immunolabeling. Energy dispersive X-ray microanalysis revealed some manganese depositions on the zymogen granules. It is highly anticipated that the KMnO4 oxidation will become a useful tool for histochemical investigations combined with cryofixation/freeze substitution and low temperature embedding techniques.

Published

2000

30. Human colorectal carcinoma-specific glycoconjugates detected by pokeweed mitogen lectin

Author

Tatsuo Suganuma, Y. Haraguchi, Jun-ichi Kawano, Tsutomu Oinuma, T. Eto, and T. Aoki

Subjects

Adenoma, Adult, Male, Pathology, medicine.medical_specialty, Histology, Glycoconjugate, Lewis X Antigen, Carcinoma, medicine, Humans, Intestinal Mucosa, Aged, chemistry.chemical_classification, Aged, 80 and over, biology, Epithelioma, Histocytochemistry, Pokeweed mitogen, Lectin, Antibodies, Monoclonal, Middle Aged, medicine.disease, Molecular biology, Immunohistochemistry, chemistry, Pokeweed Mitogens, biology.protein, Female, Anatomy, Colorectal Neoplasms, Neuraminidase, Glycoconjugates, Carcinoma in Situ

Abstract

Pokeweed mitogen (PWM) lectin, known to bind branched poly-N-acetyllactosamines, has a highly selective affinity for human colorectal carcinomas. We performed light microscopic (LM) histochemistry with PWM lectin on paraffin sections of human colorectal tissues. In histological sections, normal mucosae and adenomas with mild dysplasia exhibited negative reaction (0/10, 0/13, respectively) with or without neuraminidase pre-digestion, whereas adenomas with moderate dysplasia showed a small increase in PWM lectin reactivity after neuraminidase digestion (4/23). In contrast, we observed a high incidence of positive reactivity in colorectal carcinoma without neuraminidase pre-digestion (38/44). After digestion with neuraminidase, there was increased reactivity of colorectal carcinomas in situ (7/12) and invasive carcinomas (13/32). These results imply that human colorectal carcinomas consistently contain substantial amounts of PWM-reactive branched poly-N-acetyllactosamine glycoconjugates structures. We also compared the staining patterns of PWM lectin and monoclonal antibodies (MAb) directed to Lewis X (LeX) or Lewis Y (LeY) antigen. PWM lectin reactivity was largely confined to the apical membranes of carcinoma tissues. MAb-LeX or MAb-LeY immunoreactivity was seen on the apical membranes and in the cytoplasm of both adenomas and carcinomas. Therefore, histochemical studies with this lectin should be useful for identification of carcinoma tissues and analysis of glycoconjugates associated with colorectal carcinoma.

Published

1993

31. Bromodeoxyuridine-immunohistochemistry on cellular differentiation and migration in the fundic gland of Xenopus laevis during development

Author

Jun-ichi Kawano, Tsutomu Oinuma, and Tatsuo Suganuma

Subjects

medicine.medical_specialty, Histology, Cellular differentiation, Xenopus, Biology, Pathology and Forensic Medicine, chemistry.chemical_compound, Xenopus laevis, Cell Movement, Internal medicine, medicine, Gastric mucosa, Animals, Gastric Fundus, Fundic Gland, Cell Differentiation, Cell Biology, biology.organism_classification, Molecular biology, Immunohistochemistry, Epithelium, Foveolar cell, medicine.anatomical_structure, Endocrinology, chemistry, Bromodeoxyuridine, Gastric Mucosa

Abstract

Cellular differentiation and migration in the fundic glands of adult and larval Xenopus laevis have been examined using bromodeoxyuridine-immunohistochemistry. In the adult fundic gland, cumulative labeling with bromodeoxyuridine revealed a proliferative cell zone between the surface mucous cells and mucous neck cells, in what is referred to as the neck portion of the gland. The labeling-index of mucous neck cells had rapidly increased by week-5. The labeling-index of oxynticopeptic cells showed a more delayed increase until week-7, coincident with the decrease in the labeling of mucous neck cells. In the immature fundic glands of larvae, the labeled proliferating cells were randomly distributed throughout the developing gastric mucosa. During metamorphosis, the labeling-index of immature epithelial cells was highest at stage 63. Following administration of bromodeoxyurdine at this, stage, there was no significant loss of labeled epithelial cells during the metamorphosing period. Furthermore, there was no significant difference in the labeling-indices among the epithelial cells, such as surface mucous cells/generative cells, mucous neck cells, and oxynticopeptic cells, 7 days after administration. Cellular differentiation and migration pathways of epithelial cells in the fundic gland of adult X. laevis and its larvae are discussed.

Published

1992

32. Desulfation of Tyrosine-O-sulfated Peptides by Some Eukaryotic Sulfatases

Author

Masahito Suiko, Jun-ichi Kawano, Yoichi Sakakibara, Ming-Cheh Liu, Tamaki Tojo, and P. H. Prasantha Fernando

Subjects

chemistry.chemical_classification, Tyrosine sulfation, biology, Sulfatase, Organic Chemistry, Peptide, General Medicine, Arylsulfatases, Applied Microbiology and Biotechnology, Biochemistry, Analytical Chemistry, Enzyme, Sulfation, chemistry, Protein Biosynthesis, biology.protein, Tyrosine, Sulfatases, Peptides, Molecular Biology, Arylsulfatase, Biotechnology

Abstract

Three mammalian and eight non-mammalian arylsulfatases were investigated for their activities toward tyrosine-O-sulfate (TyrS) in peptides. None of the mammalian arylsulfatases exhibited detectable activities toward TyrS-containing peptides. Of the non-mammalian arylsulfatases tested, Types VII, VIII, and H-1, 2, and 5 displayed strong activity on endo-TyrS residues. The prokaryotic sulfatase, Type VI, was active only on free TyrS and N-terminal TyrS of Leu-enkephalin. All the sulfatases were active on p-nitrophenyl sulfate and p-nitrocatechol sulfate.

Published

1996

33. Synthesis of New Transition Metal Carbene Complexes from .pi.-Sulfurane Compounds: Reaction of 10-S-3 Tetraazapentalene Derivatives with Pd(PPh3)4 and RhCl(PPh3)3

Author

Fujiko Iwasaki, Jun-ichi Kawano, Masanori Yasui, Hiroo Inoue, Noriki Fukunishi, and Noboru Matsumura

Subjects

chemistry.chemical_compound, Colloid and Surface Chemistry, Transition metal, Chemistry, Pi, Tetraazapentalene, Organic chemistry, General Chemistry, Biochemistry, Medicinal chemistry, Carbene, Catalysis

Published

1995

34. 1P-0073 The antioxidant effect of adrenomedulin in the Dahl salt-sensitive rat

Author

Tatsuo Suganuma, Kazuo Kitamura, Jun-ichi Kawano, A. Chen, Tanenao Eto, Johji Kato, Yasuko Nagoshi, Kenji Kuwasako, and Y. Cao

Subjects

Dahl salt sensitive, Antioxidant, Biochemistry, Chemistry, medicine.medical_treatment, Internal Medicine, medicine, General Medicine, Cardiology and Cardiovascular Medicine

Published

2003

35. Characterization of a Monoclonal Antibody to Hog Thyroid Peroxidase and Its Use for Immunohistochemical Localization of the Peroxidase in the Thyroid Gland1

Author

Sachiya Ohtaki, Seiichi Hashida, Eiji Ishikawa, Masayoshi Imagawa, Eizo Aikawa, Jun-ichi Kawano, Hidehiko Nakagawa, and Tomio Kotani

Subjects

biology, Thyroid, General Medicine, Apical membrane, Immune complex formation, Biochemistry, Follicular cell, Horseradish peroxidase, medicine.anatomical_structure, Thyroid peroxidase, Iodide Peroxidase, medicine, biology.protein, Molecular Biology, Peroxidase

Abstract

A monoclonal antibody (30.1.2) to hog thyroid peroxidase was produced, purified, and characterized. The IgG of 30.1.2 formed an immune complex with the peroxidase in a 1:2 or 1:1 molar ratio depending on the IgG to antigen ratio in the incubation mixture. Immune complex formation did not inhibit the peroxidase activity, which was actually activated 2-fold in the 1:1 complex. Studies of the binding of the conjugate of the IgG or its Fab' with horseradish peroxidase to untreated and acetone-treated thyroid microsomes showed that the IgG conjugate could bind to only a very small portion of the total binding sites (thyroid peroxidase) present in untreated microsomes even after prolonged incubation. The binding of the Fab' conjugate to untreated microsomes, on the other hand, increased as the incubation time was increased, reaching 40% of the total sites after 20 h of incubation. These findings indicated that thyroid peroxidase is localized on the inner surface of the microsomal membranes and that the Fab' conjugate, but not the IgG conjugate, can slowly penetrate through the membrane barrier to reach the peroxidase. Immunohistochemical experiments using the Fab' conjugate as a probe revealed that most thyroid peroxidase in the thyroid gland is located in the endoplasmic reticulum and perinuclear cisternae of the follicular cell, although a small amount could occasionally be detected in the apical membrane including microvilli. In contrast to previous reports, no thyroid peroxidase could be found in other cellular structures such as Golgi apparatus and apical vesicles by the immunohistochemical technique employed.

Published

1985

36. Characterization of rat and human steroid sulfatases

Author

Naoto Minamino, Sachiya Ohtaki, Jun-ichi Kawano, Tomio Kotani, Tsutomu Oinuma, Eizo Aikawa, and Hisayuki Matsuo

Subjects

Macromolecular Substances, Placenta, medicine.medical_treatment, Molecular Sequence Data, Ion chromatography, Biophysics, Fluorescence spectrometry, Antigen-Antibody Complex, Biochemistry, Michaelis–Menten kinetics, Chromatography, Affinity, Substrate Specificity, Steroid, Species Specificity, Affinity chromatography, Pregnancy, Structural Biology, Microsomes, medicine, Animals, Humans, Amino Acid Sequence, Amino Acids, Molecular Biology, Gel electrophoresis, chemistry.chemical_classification, Chromatography, Antibodies, Monoclonal, Rats, Amino acid, Molecular Weight, Kinetics, Enzyme, chemistry, Microsomes, Liver, Female, Sulfatases

Abstract

Rat and human steroid sulfatases were purified from liver and placenta, respectively, by the same procedure. The rat and human enzymes were solubilized with Triton X-100, and purified by immunoaffinity chromatography with a monoclonal antibody showing high binding activities to both the enzymes. They were further purified by high-pressure anion-exchange chromatography to compare their structural and catalytic properties. Sodium dodecyl sulfate-polyacrylamide gel electrophoresis showed that both enzymes had a molecular weight of 62,000. The enzymes had similar amino acid compositions and amino-terminal amino acid sequences. Significant differences of the optimum pH, Michaelis constant and maximum velocity were observed between these enzymes. The optimum pH of each enzyme varied from 6.0 to 8.0, depending on substrates and with or without Triton X-100. In detergent-free media, steroid sulfates competitively inhibited the ability of these enzymes to hydrolyze 4-nitrophenyl sulfate. In media containing Triton X-100, on the other hand, the inhibition types of the steroid sulfates on the hydrolyzing activities of the rat and human enzymes were noncompetitive- and mixed-types, respectively.

Published

1989

37. A monoclonal antibody to rat liver arylsulfatase C and its application in immunohistochemistry

Author

Jun-ichi Kawano, Tomio Kotani, Tsutomu Oinuma, Kazumi Umeki, Sachiya Ohtaki, and Eizo Aikawa

Subjects

Male, Histology, medicine.drug_class, Monoclonal antibody, Kidney, medicine, Animals, Arylsulfatases, chemistry.chemical_classification, biology, Immunoperoxidase, Endoplasmic reticulum, Antibodies, Monoclonal, Rats, Inbred Strains, Molecular biology, Immunohistochemistry, Staining, Rats, Enzyme, Biochemistry, chemistry, Liver, biology.protein, Microsome, Steryl-Sulfatase, Anatomy, Sulfatases, Arylsulfatase

Abstract

We purified arylsulfatase C from rat liver microsomes and prepared a monoclonal antibody (P42C2) to the purified enzyme. By SDS-PAGE and immunoblotting analysis using P42C2, the molecular weight of the purified enzyme and of the enzyme in liver and kidney microsomes were estimated at 62,000 daltons. P42C2 caused little inhibition of arylsulfatase C activity, and was bound only slightly to liver microsomes. Localization of arylsulfatase C was studied at the light and electron microscopic level by the indirect immunoperoxidase method using P42C2. In rat liver, arylsulfatase C was detected mainly in the hepatocytes, and less frequently in endothelial cells, Kupffer's cells, and Ito's cells. In rat kidney, strong staining was observed in the straight portions of the proximal tubules. The podocytes, interstitial cells, endothelial cells, and epithelial cells of Henle's thin limbs were stained faintly. By electron microscopy, arylsulfatase C was found localized on the membranes of the endoplasmic reticulum and nuclear envelopes in these cells. These immunohistochemical findings agree with the localization demonstrated by an enzyme-histochemical method which we had previously developed.

Published

1989

38. Distribution of antibodies against various influenza A viruses in animals

Author

Ryo Yanagawa, Jun-ichi Kawano, Yumiko Matsuoka, Tokio Onta, and Hiroshi Kida

Subjects

Swine, Influenza a, General Medicine, Biology, Antibodies, Viral, H5N1 genetic structure, Virology, Rats, Dogs, Influenza A virus, Mink, biology.protein, Cats, Distribution (pharmacology), Animals, Cattle, Horses, Antibody

Published

1978

39. Regional distribution of arylsulfatase C and estrone-sulfate sulfatase activities in rat brain and hypophysis

Author

Jun-ichi Kawano and Eizo Aikawa

Subjects

Male, endocrine system, medicine.medical_specialty, Pituitary gland, Nuclear Envelope, Endoplasmic Reticulum, Pineal Gland, chemistry.chemical_compound, Pineal gland, Estrone sulfate, Internal medicine, Ependyma, medicine, Animals, Molecular Biology, Arylsulfatases, biology, Histocytochemistry, General Neuroscience, Endoplasmic reticulum, Sulfatase, Brain, Rats, Inbred Strains, Rats, Endocrinology, medicine.anatomical_structure, Biochemistry, chemistry, Pituitary Gland, biology.protein, Choroid plexus, Steryl-Sulfatase, Neurology (clinical), Sulfatases, Arylsulfatase, Developmental Biology

Abstract

Regional distributions of arylsulfatase C and estrone-sulfate sulfatase activities were studied in rat brain and hypophysis by both histochemical and biochemical methods. Both methods showed that high activities of both enzymes were localized in pineal gland, choroid plexus, and adenohypophysis. Ultracytochemical techniques visualized the arylsulfatase C activity in the endoplasmic reticulum and the nuclear envelope of pineal cells, ependymal cells, and some types of cells of the adenohypophysis.

Published

1987