27 results on '"Itaru Horiuchi"'
Search Results
2. Lipoprotein Receptors of Liver
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Hitoshi Kurushima, Kozo Hayashi, Eisuke Nishio, Goro Kajiyama, Yasuhiko Hirata, Shinya Dojo, Koichiro Nakashima, Masayumi Saeki, Itaru Horiuchi, and Hiromasa Ohtani
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World Wide Web ,Thesaurus (information retrieval) ,Computer science - Published
- 1991
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3. Accumulation of Cholesteryl Esters in Differentiated Monocyte-Macrophage-Like Cells
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Hiromasa Ohtani, Shinya Dojo, Koichiro Nakashima, Eisuke Nishio, Hitoshi Kurushima, Itaru Horiuchi, Masayumi Saeki, Yasuhiko Hirata, Kozo Hayashi, and Goro Kajiyama
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chemistry.chemical_compound ,chemistry ,Biochemistry ,Cholesterol ,Sterol O-acyltransferase ,Reverse cholesterol transport ,Monocytes macrophages ,Cholesterol acyltransferase activity ,Acyl coenzyme A - Published
- 1991
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4. Probucol Promotes Hepatic Uptake of High Density Lipoprotein in Rats
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Itaru Horiuchi, Makato Okahashi, Goro Kajiyama, Koki Takata, Hironori Tokumo, Toshio Kawamoto, Yasuhiko Hirata, and Kazunori Koide
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medicine.medical_specialty ,Apolipoprotein AI ,Reduced high-density lipoprotein ,Cholesterol ,Probucol ,Hepatic cholesterol ,General Medicine ,chemistry.chemical_compound ,Endocrinology ,High-density lipoprotein ,chemistry ,In vivo ,Internal medicine ,Rat liver ,medicine ,lipids (amino acids, peptides, and proteins) ,Pharmacology (medical) ,medicine.drug - Abstract
Probucol significantly reduced high density lipoprotein (HDL)-cholesterol and apolipoprotein AI in rats. Hepatic uptake of radiolabelled human HDL3 increased significantly in vivo and in the isolated perfused rat liver preparation. In vivo, uptake of HDL3 by the adrenal glands also increased significantly. Hepatic cholesterol content in probucol-treated rats tended to increase, whereas newly synthesised cholesterol decreased significantly. The results of the present study suggest that enhanced uptake of HDL is one of the mechanisms of lowering serum HDL with probucol treatment.
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- 1990
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5. Form Cell Formation of Macrophages and Lipoprotein Receptors A Contribution of LDL Receptor and Scavenger Receptor
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Hiromasa Ohtani, Goro Kajiyama, Hitoshi Kurushima, Yasuhiko Hirata, Eisuke Nishio, Itaru Horiuchi, Koichiro Nakashima, Kozo Hayashi, Shinya Dojo, and Masayumi Saeki
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Apolipoprotein E ,Low-density lipoprotein receptor gene family ,Chemistry ,LDL receptor ,Cell formation ,Scavenger receptor ,Receptor ,Lipoprotein ,Cell biology - Published
- 1990
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6. Analysis of neutral amino acid transport systems in the small intestine: a study of brush border membrane vesicles
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Hiromasa Ohtani, Shinya Dojo, Masaki Ito, Masayumi Saeki, Hiroshi Amioka, Hitoshi Kurushima, Eisuke Nishio, Yasuhiko Hirata, Koichiro Nakashima, Goro Kajiyama, Masataka Hiraoka, Kozo Hayashi, and Itaru Horiuchi
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medicine.medical_specialty ,Brush border ,Proline ,Guinea Pigs ,Ileum ,In Vitro Techniques ,Leucine ,Internal medicine ,Neutral amino acid transport ,medicine ,Serine ,Animals ,Cysteine ,Amino Acids ,Alanine ,chemistry.chemical_classification ,System L ,Microvilli ,business.industry ,Vesicle ,Gastroenterology ,Biological Transport ,Small intestine ,Amino acid ,Culture Media ,medicine.anatomical_structure ,Biochemistry ,chemistry ,Biophysics ,business - Abstract
Transport of L-proline, L-leucine and L-cysteine was studied in brush border membrane vesicles prepared from guinea pig ileum. Concentrative transport of L-proline, L-leucine and L-cysteine was obtained in the presence of an Na+ gradient from, outside to inside of the vesicles, which indicated contribution of either system A (alanine-preferring) or system ASC (alanine-, serine- and cysteine-preferring) to the transport. When Na+ was replaced by Li+, L-leucine and L-cysteine maintained the same concentrative transport. However, the concentrative transport of L-proline was markedly decreased by Li+ -for-Na+ substitution. Strong exchange properties of L-leucine transport via system L (leucine-preferring) was observed with brush border membrane vesicles, in which preloaded L-methionine could be exchanged with labeled L-leucine added outside the vesicles. These results suggest that the small intestine of the guinea pig possesses classical neutral amino acid transport systems such as systems A, ASC and L.
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- 1991
7. Effects of pravastatin (CS-514) on biliary lipid metabolism in patients with hyperlipidemia
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Itsuo Takizawa, Toshiyuki Mizuno, Itaru Horiuchi, Toshihide Ohya, Susumu Tazuma, and Goro Kajiyama
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Adult ,Male ,medicine.medical_specialty ,Endocrinology, Diabetes and Metabolism ,Hyperlipidemias ,Naphthalenes ,Bile Acids and Salts ,chemistry.chemical_compound ,Endocrinology ,Internal medicine ,Hyperlipidemia ,medicine ,Bile ,Humans ,Aged ,Pravastatin ,biology ,Triglyceride ,Cholesterol ,business.industry ,Anticholesteremic Agents ,Fatty Acids ,nutritional and metabolic diseases ,Metabolism ,Middle Aged ,medicine.disease ,Lipid Metabolism ,Hydroxymethylglutaryl-CoA reductase ,Lipids ,chemistry ,Enzyme inhibitor ,Heptanoic Acids ,biology.protein ,lipids (amino acids, peptides, and proteins) ,Female ,business ,Lipoprotein ,medicine.drug - Abstract
Pravastatin was administered to 20 patients with hyperlipidemia type IIa and IIb, for a period of 8 to 16 weeks at a daily dose of 10 to 20 mg, to investigate the effects on serum and biliary lipids. At the end of the treatment with pravastatin, the serum cholesterol level was significantly reduced, by 20%, compared with the control level. On the other hand, no significant differences were observed in serum high-density lipoprotein (HDL) cholesterol and triglyceride levels. Additionally, the administration of pravastatin did not change mole % compositions of biliary lipids, such as cholesterol, phospholipids, and total bile acids, as well as individual biliary bile acids. Consequently, there was not any significant change of the cholesterol saturation index. Based on the above results, our findings suggest that, for the treatment of hyperlipidemia, pravastatin is a highly effective cholesterol-lowering drug that does not affect biliary lipid metabolism.
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- 1991
8. Effect of Clinofibrate on Hyperlipidemia
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Takashi Mizuno, Nobue Hirakawa, Toshiyuki Mizuno, Seiji Nakao, Itaru Horiuchi, Takao Yamasaki, Goro Kajiyama, Shizuteru Usui, and Masamichi Fujiyama
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medicine.medical_specialty ,Endocrinology ,business.industry ,Internal medicine ,Hyperlipidemia ,medicine ,Clinofibrate ,medicine.disease ,business ,medicine.drug - Published
- 1984
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9. Proceedings of the 27th Annual Meeting Matsuyama, Japan, November 7–9, 1985
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C. E. Rogler, Yoshihiro Muto, Masayuki Uchimura, Hiroshi Kijima, Hidenobu Watanabe, A. Kakita, M. Kambayashi, T. Takahashi, Y. Saji, T. Tsuburaya, J. Uchino, Yoshifumi Ogura, Hiroshi Yamagiwa, Y. Takehara, K. Yamashita, Seikoh Shimaguchi, Joe Ariyama, Sei Tomatsu, Itaru Oi, Tadasu Fuji, Takayoshi Noguchi, Kenji Yamao, Saburo Nakazawa, H. Suzuki, R. Mizumoto, Masamitu Kumon, Takuro Ogata, Kenichi Yamamoto, Kenichi Sasaki, Hideo Kida, Yuji Nimura, Naokazu Hayakawa, Junichi Kamiya, Shigehiko Shionoya, Yoshinobu Hata, Jun-Ichi Uchino, Takaaki Yamane, Katsutaka Mori, Hiroaki Kinoshita, Tadashi Inoue, Kenichi Takayasu, Noriyuki Moriyama, Masatoshi Makuuchi, Ken Takasaki, Seiichi Tanaka, K. Shirakawa, F. Misaki, Tadashi Shibue, Keizo Tanaka, Masahiro Asaka, Masao Saito, Susumu Yamagata, Yasuo Utiyama, K. Kobayashi, T. Arakawa, Kei Matsueda, Akira Muraoka, Noritsugu Umeda, Shyuzi Mizumachi, Kiwamu Okita, Hiroshi Sakaue, Kouichi Akamatsu, Teruaki Aoki, Fusahiro Nagao, Yozo Watanabe, Tsutomu Kidokoro, Satoshi Nakano, Takashi Kumada, Takaharu Kondo, Tetsuo Hayakawa, Michio Ogawa, Yasuki Matsuda, Takesada Mori, Hideki Yasuda, Yutaka Atomi, Norihito Ohnishi, Akira Kuroda, Yasuhiko Morioka, Katsusuke Satake, Ryoichi Tsuchiya, Shuji Isaji, Ryuji Mizumoto, Masahiro Yamamoto, Yoichi Saitoh, Kazunori Takeda, Susumu Taguchi, Hitoshi Funatomi, Yoshio Hatta, Mikiko Ono, Tatsuya Itoshima, Ryoji Tanaka, Shunichi Sato, Hitoshi Sugaya, Shunji Futagawa, Kenichi Kobayashi, Hironaka Kawasaki, Hirotada Ohkubo, Yoshifumi Kawarada, Hiroyuki Hirasawa, Michio Odaka, Kaichi Isono, Soichiro Miura, Yoshiki Hamada, Tadao Bamba, Nobuo Chikamochi, R. Nezu, A. Okada, Masahiro Okuno, Kaoru Umeyama, Nobuo Hiwatashi, Kazuyuki Nakajima, Tadahiko Fuchigami, Tsuneyoshi Yao, Masakazu Takazoe, Ryosuke Shoda, T. Fukushima, M. Kawamoto, Kenji Mizutani, Katsuhiko Nakai, Katsunori Aoki, Satoru Morioka, Shozo Baba, Akio Sakamoto, Sadahito Usui, Yoshihiro Fukuda, Kazutami Tamura, Hikaru Watanabe, Takato Ueno, Kyuichi Tanikawa, Masaya Oda, Toshio Morizane, Hiroyuki Hashimoto, Ichiro Shimizu, Kenji Shima, Kohsuke Sasaki, Toshimitsu Suzuki, Yoshifumi Seto, Toshiaki Nakashima, Kendo Kiyosawa, Haruhiko Imai, Yukihiro Shimizu, Hiroshi Sasaki, Teruo Mori, Yoshio Mori, Makoto Ogawa, Masafumi Wakashin, Kunio Okuda, Chiaki Kawamoto, Kenichi Ido, Kiyotaka Fujise, Seishi Nagamori, Shinichiro Fujikura, Kazuhiko Shimada, Kazuhito Yamaguchi, Yoshinori Fujimura, Tsuyoshi Kihara, Hironobu Kitamura, Yoshihide Fujiyama, Hitoshi Asakura, Kensuke Kobayashi, Hiroshi Nagura, Takashi Koshikawa, Yuji Murata, Kiyoo Kuroe, H. Kawanishi, K. Koyama, S. Senda, J. Kiely, Kazuo Harima, Masato Furukawa, Toshinori Nakata, Hiroyuki Kawahara, Nobuhiko Komi, Yukio Ishihara, Satoshi Kondo, Koichi Suda, Takeshi Miyano, Kazuo Inui, Toshikazu Ohnuma, Noboru Yamamichi, Fumio Konishi, Nobuto Morita, Yutaka Tanikawa, Eiichi Kitani, Toshikazu Tamura, Tetsuo Ohta, Kohji Konishi, Makoto Utsumi, Noriyuki Ueda, Hideto Sasaki, Toshio Kawamoto, Itaru Horiuchi, Kouji Tada, Teiko Nakai, Katsuko Yamashita, Fuyuhiko Ninomiya, Yasuo Naito, Keiichi Morita, Hitoshi Hachiya, Toshihiko Takeuchi, Keizo Onuki, Toshihiko Ozaki, Y. Tsuchiya, H. Nakamura, Hideyuki Nagashima, Takashi Matsushiro, Masahiro Nakai, K. Takeuchi, G. Watanabe, T. Ito, Y. Idezuki, Masatoshi Isogai, and Kitao Hachisuka
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medicine.medical_specialty ,Surgical oncology ,business.industry ,Internal medicine ,General surgery ,Gastroenterology ,medicine ,Hepatology ,business ,Colorectal surgery ,Abdominal surgery - Published
- 1986
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10. Indices for Prediction of Coronary Sclerosis with Particular Reference to Apo-B/Apo-AI Ratio
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Gen Konemori, Goro Kajiyama, Yuri Kuroki, Hideo Matsuura, Masaki Itoh, Atsuko Nakamoto, Hideyo Amioka, Itaru Horiuchi, Masataka Hiraoka, Kouki Takata, and Masahiro Kawanishi
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medicine.medical_specialty ,Endocrinology ,Apolipoprotein B ,biology ,business.industry ,Internal medicine ,biology.protein ,medicine ,business ,Coronary sclerosis - Published
- 1989
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11. Lipoprotein Components in Bile
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Nobutaka Matsuo, Fumiaki Hind, Shoji Nishimura, Itaru Horiuchi, Masami Ohki, Toshio Kawamoto, Masaharu Yamamoto, Makoto Okahashi, Goro Kajiyama, Tokuo Tsubokura, Ken Oyamada, and Koso Mitsuba
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medicine.medical_specialty ,Very low-density lipoprotein ,Endocrinology ,Chemistry ,Internal medicine ,medicine ,Lipoprotein - Published
- 1984
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12. New Indices of LDL-receptor Activity in Lymphocytes: Using LDL-cholesterol Dependent Proliferation of PHA-stimulated Lymphocytes
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Tetsuhiko Watanabe, Itaru Horiuchi, Hiroshi Kawamura, Koki Takata, Toshihide Ohya, and Goro Kajiyama
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- 1988
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13. Serum Squalene in Patients with Hyperlipoproteinemia
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Goro Kajiyama, Toshihito Hiraoka, Shoji Nishimura, Makoto Okahashi, Nomura Y, Itaru Horiuchi, Toshio Kawamoto, Koki Takata, Hironori Tokumo, and Susumu Tazuma
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medicine.medical_specialty ,Squalene ,chemistry.chemical_compound ,chemistry ,business.industry ,Internal medicine ,medicine ,In patient ,business ,Gastroenterology - Published
- 1986
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14. The Effect of Fatty Acids on Biliary Lipids in the Hamsters
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Kozo Hayashi and Itaru Horiuchi
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- 1987
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15. Effect of Probucol on Biliary Lipids and Fecal Sterol in Hyperlipoproteinemic Patients
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Shoji Nishimura, Goro Kajiyama, Makoto Okahashi, Fumiaki Hino, Toshio Kawamoto, Itaru Horiuchi, and Takashi Nakagawa
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medicine.medical_specialty ,Endocrinology ,Chemistry ,Internal medicine ,medicine ,Probucol ,Sterol ,Feces ,medicine.drug - Published
- 1984
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16. Effect of Hepatic Blood Flow on Serum HDL Level in Rabbits
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Ken Oyamada, Choho Fukuhara, Koki Takata, Masahiro Nakagawa, Hideo Matsuura, Goro Kajiyama, Seiji Nakao, Akima Miyoshi, and Itaru Horiuchi
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medicine.medical_specialty ,Endocrinology ,business.industry ,Internal medicine ,Medicine ,Blood flow ,business - Published
- 1982
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17. The Mechanism of Probucol Lowering Effects of High Density Lipoprotein
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Yasuhiko Hirata, Goro Kajiyama, Toshio Kawamoto, Makoto Okahashi, Hironori Tokumo, Koki Takata, Youko Nomura, Itaru Horiuchi, and Kazunori Koide
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medicine.medical_specialty ,chemistry.chemical_compound ,Endocrinology ,chemistry ,Cholesterol ,Internal medicine ,medicine ,Probucol ,medicine.drug - Published
- 1987
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18. In vitro and in vivo growth characteristics of a new ascites-type neuroblastoma cell from mouse C1300 neuroblastoma
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Itaru Horiuchi, Hiroshi Kato, Hidehiko Tsunooka, Ryo Tanaka, Kuniko Okumura-Noji, Shingi Sasaki, Hiroko Fukami, Akira Masaoka, Kyoko Kano-Tanaka, and Taiji Kato
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Catecholaminergic ,Pathology ,medicine.medical_specialty ,Cell growth ,Cell ,Enolase ,Cell Biology ,Biology ,medicine.disease ,Molecular biology ,In vitro ,Cellular and Molecular Neuroscience ,medicine.anatomical_structure ,Cell culture ,In vivo ,Neuroblastoma ,medicine - Abstract
A clonal ascited type cell, NAs-1, was obtained in culture from a mouse neuroblastoma C1300. The cells were adapted to anchorage-independently grow in the flask by the in vitro-in vivo alternate passage technique, and retained the ability of growing and producing ascites fluid when intraperitoneally injected into mice. Although the majority of growing cells in culture medium showed a small and round cell shape without any neuronal process, occasionally non-specific attachment onto the flask surface was observed, but devoid of the extrusion of processes. Karyotype analysis showed a homogeneous chromosome number, 40, with a marker chromosome [t(13:16)] and a minichromosome. Catecholamines, norepinephrine and dopamine, were found in the cell extracts and the contents of dopamine was particularly high as shown in another catecholaminergic neuroblastoma cell, N1E-115. Neuron specific enolase (γ-subunit) was also detected. The treatment of the cells by dibutyryl cyclic AMP, prostaglandin E1, or BL191 (phosphodiesterase inhibitor) induced the biochemical differentiation in terms of catecholamine and cyclic AMP contents, but failed to promote typical morphological differentiations including the extension of process or the significant promotion of adherence onto the flask surface.
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- 1985
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19. Effect of ursodeoxycholic acid administration on nucleation time in human gallbladder bile
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Itaru Horiuchi, Sumie Hashiba, Shigeki Mizuno, Goro Kajiyama, Sasaki H, Sagawa H, and Susumu Tazuma
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Adult ,medicine.medical_specialty ,Apolipoprotein B ,Nucleation ,Apolipoproteins A ,Gastroenterology ,Preoperative care ,chemistry.chemical_compound ,Cholelithiasis ,Internal medicine ,Preoperative Care ,medicine ,Bile ,Humans ,Aged ,Aged, 80 and over ,Apolipoprotein A-I ,Hepatology ,biology ,Cholesterol ,business.industry ,Ursodeoxycholic Acid ,Deoxycholic acid ,Gallstones ,Middle Aged ,medicine.disease ,Ursodeoxycholic acid ,chemistry ,biology.protein ,Lipoproteins, HDL ,business ,Deoxycholic Acid ,medicine.drug - Abstract
The object of this study was to determine the effects of ursodeoxycholic acid administration on metastability in human gallbladder bile, as reflected by nucleation time. Bile samples from 10 patients with cholesterol gallstones who underwent preoperative ursodeoxycholic acid treatment exhibited a significantly longer median nucleation time (16 days) than those from 11 patients with cholesterol gallstones who received no preoperative treatment (4 days) (p less than 0.01). On the other hand, the median nucleation times of bile samples from 15 patients with noncholesterol gallstones and 24 patients without gallstones were 15 and 14 days, respectively. In addition, 3 mo of treatment with ursodeoxycholic acid significantly elevated the serum concentration of the antinucleating factor apolipoprotein A-I, from 133.3 +/- 12.3 to 148.6 +/- 13.2 mg/dl (p less than 0.05). These findings suggest that ursodeoxycholic acid retards cholesterol crystal nucleation, thereby inhibiting cholesterol gallstone formation. It is also possible that serum apolipoprotein A-I plays a role in this process.
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- 1989
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20. Proceedings of the 26th annual meeting Chiba, Japan, October 18–20, 1984
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Shunsaku Higashi, Yoshio Yamazaki, Junji Tanaka, Kazue Ozawa, Munemasa Ryu, Michio Odaka, Kuniaki Kojima, Takashi Hanzawa, Mitsuo Sugiura, Toru Kanno, Sukeo Yamamoto, Keijiro Ando, Yuji Kado, Morio Sato, Ryusaku Yamada, Masaru Miyazaki, Katsuji Okui, Shingi Imaoka, Yo Sasaki, Yoshiyuki Shimamura, Hisakazu Shimizu, Kiyotaka Tezuka, Ichiya Tsuji, Shoji Kajikawa, Masanori Ishii, Akira Takahashi, Toshinori Kodama, Tomomi Kitatani, Tomoharu Matsuyama, Hiroshi Hasegawa, Hiroaki Kawashima, Katsuyoshi Tabuse, Masaharu Katsumi, Kenji Jinno, Katsuyuki Tokuyama, Yasuo Majima, Yasuhiko Kubo, Atsushi Toyonaga, Satoshi Eguchi, Kenji Hirai, Masahide Abe, Haruki Nakatsuka, Sumio Takashima, Yoshihiro Fukuda, Masahiro Hiraoka, Takatoshi Sasaki, Masakazu Maruyama, Mamoru Nishizawa, Kyoichi Nakamura, N. Saitoh, H. Sarashina, Shinei Kudo, Takeyasu Suda, Shu Kuramoto, Takeshi Oohara, Tomio Narisawa, Makoto Niwa, Nobuaki Kaibara, Shigemasa Koga, S. Takashima, T. Kosaka, Kohi Miura, Norio Nakao, Kunio Ido, Kyoichi Hiramatsu, S. Matsutani, K. Kimura, Akira Sano, Yasumasa Kuroda, Kiyohiro Kawahara, Tomoharu Yoshida, Shuzi Mizumachi, Ken Takeuchi, Yukio Kobayashi, Yasuhiro Takase, Tadasu Fuji, Hideo Amano, Akiyoshi Shu, Eizo Okamoto, Hirokazu Kawata, Tomomitsu Kikuchi, Noburu Sakakibara, Morio Masaki, Reiji Kasukawa, Fumiaki Ikegami, Sachio Takasu, Yoshihisa Tsukada, Fumihiro Ichida, Hiroaki Suzuki, Yoshinori Inagaki, Hideki Yasuda, Tadahiro Takada, Toshikazu Suwa, Yutaka Atomi, Yasuhiko Morioka, Tokuyuki Yokohata, Hisaaki Shimazu, Sadamu Takano, Katsunori Yukimura, S. Shimaguchi, J. Ariyama, Satoshi Sawada, Yoshikuni Okamura, Tomohiko Yoshida, Toshihiko Saito, Okitsugu Nishimura, Haruaki Ogawa, Masahiko Morita, Hiromitsu Saisho, Katsuhide Shimakura, Kazuya Ueno, Susumu Miyata, Tadashi Shibue, Atzumasa Yamaguchi, Seiji Tsunoka, Katsuji Hayashi, Yoshihiko Komatsu, Masakatsu Matsukawa, Yasuso Soejima, Y. Nimura, Toshikazu Ohnuma, Kazuo Inui, Takashi Matsushiro, Hideyuki Nagashima, Hideo Ise, Toshio Sato, Y. Akita, S. Shichino, H. Suzuki, T. Sato, K. Ono, Hideki Fujii, Masayuki Yamamoto, Yoshiro Matsumoto, Katsuhiko Sugahara, Tetsuo Ota, Kohji Konishi, Mikiko Ono, Satoru Sohma, Junji Yoshino, Hirosato Ohta, Hiroshi Obata, Tetsuya Ageta, Sumiaki Tsuru, Yutaka Sasagawa, Koichi Yoshida, Toshiaki Jo, Tsuneo Sasaki, Junichi Ishiwata, Jiro Fujimoto, Takesada Mori, Noboru Azuma, Toshiki Kamano, Akeo Hagiwara, Toshio Takahashi, Y. Sasaki, J. Sasaki, Yasuaki Arai, Choichiro Kido, Kyoichiro Suyama, Masatsugu Kitamura, Yasuyuki Awane, Mishio Maeta, Yuzuru Sugiyama, Hiroki Sohma, Toshiaki Nakashima, Yoshihiro Nakagawa, Kazuo Chijiiwa, Masahiro Yamamoto, Yoichi Saitoh, Itaru Horiuchi, Susumu Fujita, Teruo Nakamura, Isao Marino, Yasushi Matsuzaki, Toshiaki Osuga, Yasutoshi Konno, Nobuo Hiwatashi, Noriaki Tamura, Chisato Hirayama, Naoki Ishiguro, M. Tsuchiya, Masahide Ikeguchi, Susumu Tateno, Toshiaki Setoguchi, Yutaka Shimizu, Masahito Tanaka, Kiyoaki Ouchi, Kenji Koyama, Masayuki Saito, Kunihiko Ohnishi, Fuminori Moriyasu, Motohide Takashi, Shinichi Hino, Toru Kashiwagi, Takeo Koizumi, Kazuo Nagayama, Masaharu Horiguchi, Norio Ueno, Takeo Yamanaka, Akitake Hasumi, Haruo Aoki, Hiroaki Takenaka, Kazuyasu Nakao, Osamu Yamazaki, Hiroaki Kinoshita, H. Komatsu, M. Oda, N. Tsukada, K. Kaneko, Y. Shigeta, K. Funatsu, Akiharu Watanabe, Kazuo Tobe, Akira Matsuo, Yukio Kusumoto, Yukihiko Adachi, Toshio Yamamoto, Chikara Oshio, Hiromasa Ishii, Shigeki Matsuki, Hisao Shibata, Tatsuhiko Kodama, Fumimaro Takaku, Yasuji Miyata, Shigeru Sakamoto, Nobutake Matsuo, Yutaka Tsuchiya, Haruki Nakamura, Toshihiro Maruyama, Tomofumi Morita, Tadasu Tsujii, Masayoshi Kage, Masahiro Arakawa, Nobuyuki Sugiura, Masaaki Ebara, Takashi Kumada, Satoshi Nakano, Hideo Yamazaki, and Sachiko Tanaka
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Gastroenterology - Published
- 1985
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21. Induction of Hepatic LDL Receptor by CS514
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Shinya Dojo, Kazunobu Koide, Tetsuhiko Watanabe, Itaru Horiuchi, Kozo Hayashi, Hiromasa Ohtani, Toshihide Ohya, and Goro Kajiyama
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medicine.medical_specialty ,Endocrinology ,Chemistry ,Internal medicine ,LDL receptor ,medicine - Published
- 1989
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22. Inhibition by neuroblastoma growth inhibitory factor of ascites-type neuroblastoma cell growth in coculture with normal glioblasts
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Takasumi Kato, Hidehiko Tsunooka, Jin-ichi Ito, Taiji Kato, Hiroshi Kato, Nobuyuki Naganawa, Shingi Sasaki, Kuniko Okumura-Noji, Ryo Tanaka, Itaru Horiuchi, Akira Masaoka, Kyoko Kano-Tanaka, and Kanefusa Kato
- Subjects
medicine.medical_specialty ,DNA synthesis ,Clone (cell biology) ,Cell Biology ,Biology ,medicine.disease ,Cell biology ,Cellular and Molecular Neuroscience ,Paracrine signalling ,chemistry.chemical_compound ,Endocrinology ,Nerve growth factor ,Glioblast ,chemistry ,Cell culture ,Internal medicine ,Neuroblastoma ,medicine ,Growth inhibition - Abstract
A new ascites type neuroblastoma clone (NAs-1), which is characteristic both in anchorage-independent growth and catecholaminergic functions, attached on the monolayer culture of glioblasts and was subjected to morphological differentiation including the extrusion of neuronal processes. Other conventional neuroblastoma cells (Neuro2a, NS-20Y, and N1E-115) as well as NAs-1 in cocultured with normal glioblasts underwent a decrease in cell growth rates and DNA synthesis under the effect of the neuroblastoma growth inhibitory factor (NGIF) produced by glioblasts. After their NGIF production had been reduced by u.v. irradiation, glioblasts lost the growth-inhibitory and differentiation-promoting effects in coculture with NAs-1. The supplement of NGIF into u.v.-treated glioblasts restored the dose-dependent growth inhibition of NAs-1. The addition of nerve growth factor into the coculture system brought about neither the marked effect on growth inhibition of NAs-1 nor the morphological differentiation. The results imply a direct function of NGIF on the paracrine regulation of neuroblastoma cell growth in the coculture with normal glioblasts.
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- 1984
23. A new case of familial lecithin: cholesterol acyltransferase (LCAT) deficiency--paradoxical findings regarding LCAT mass and activity in 23 members of a family
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Koki Takata, Tetsuhiko Watanabe, Hiroshi Tokumo, Goro Kajiyama, Yasuhiko Hirata, and Itaru Horiuchi
- Subjects
Proband ,Apolipoprotein E ,Adult ,Male ,medicine.medical_specialty ,Apolipoprotein B ,Phosphatidylcholine-Sterol O-Acyltransferase ,chemistry.chemical_compound ,Lecithin Cholesterol Acyltransferase Deficiency ,Internal medicine ,Medicine ,Humans ,Proteinuria ,biology ,Red Cell ,business.industry ,Cholesterol ,General Medicine ,Middle Aged ,Hypolipoproteinemias ,Endocrinology ,LCAT activity ,chemistry ,Lecithin—cholesterol acyltransferase ,biology.protein ,Female ,medicine.symptom ,business - Abstract
LCAT activity and mass were assayed simultaneously in 23 members of a new family case, revealing two homozygotes with a markedly low HDL--cholesterol level and ester cholesterol ratio. The LCAT mass in these patients was only 0.8 and 0.9 micrograms/ml, respectively (normal range 4.4-8.1) and their LCAT activity was 4 and 6 nM/ml/h 37 degrees C (normal range 60-120). Apolipoprotein (Apo) A-I and II levels were significantly low; however, apolipoprotein E tended to be high. In two-dimensional electrophoresis, apo A-I isoform visualized the increase of immature apo A-I; that is, A-I2. One subject showed the clinical characteristics of classic LCAT deficiency; however, the other, who was a vegetarian, showed corneal opacities and red cell deformity, but not proteinuria. This suggests that a low fat diet which decreases the level of atherogenic large LDL, may lead to a more favourable prognosis with a reduced risk for renal insufficiency. There were two different types of LCAT abnormality in this family series. Among the 10 examined paternal kindred of the proband who was one of two homozygotes, seven had a low LCAT mass but normal LCAT activity with the exception of one kindred who had a low mass and low activity. In contrast, among his seven maternal kindred examined, two had a low LCAT activity but normal mass.
- Published
- 1989
24. Effect of CS-514, a competitive inhibitor of hydroxymethylglutaryl coenzyme A reductase, on cholesterol gallstone formation in hamsters
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Kazunobu Koide, Goro Kajiyama, Itaru Horiuchi, and Kozo Hayashi
- Subjects
Male ,medicine.medical_specialty ,Biophysics ,Reductase ,Naphthalenes ,Biochemistry ,Excretion ,Bile Acids and Salts ,chemistry.chemical_compound ,Endocrinology ,Cholelithiasis ,Reference Values ,Internal medicine ,Cricetinae ,Hyperlipidemia ,medicine ,Dietary Carbohydrates ,Animals ,Bile ,Triglycerides ,Pravastatin ,Triglyceride ,biology ,Mesocricetus ,Cholesterol ,Anticholesteremic Agents ,Reverse cholesterol transport ,medicine.disease ,Lipid Metabolism ,Glucose ,chemistry ,Heptanoic Acids ,HMG-CoA reductase ,Microsome ,biology.protein ,Microsomes, Liver ,lipids (amino acids, peptides, and proteins) ,Hydroxymethylglutaryl-CoA Reductase Inhibitors - Abstract
Male golden hamsters fed a glucose diet as a model for cholesterol gallstone formation were used to investigate the effect of CS-514 on the lithogenicity of bile. Treatment with 0.05% (w/w) CS-514 in the diet for 1-4 weeks caused a decrease in plasma cholesterol and triacylglycerol levels. A marked increase in hepatic hydroxymethylglutaryl-CoA reductase activity in vitro and also an increased de novo cholesterol synthesis in the liver were induced by treatment with CS-514 for 1-4 weeks. The concentration of free cholesterol in liver microsomes and the cholesterol 7 alpha-hydroxylase activity were both decreased by treatment with CS-514 for 1 week, but were not affected by treatment for 4 weeks. The cholesterol output into bile and the lithogenic index of bile were double those of the control (glucose diet only) following treatment with CS-514 for 4 weeks, and the subsequent incidence of cholesterol gallstone formation was elevated. The content of free cholesterol and cholesterol ester in the liver was not affected by treatment with CS-514 for 4 weeks. These results suggest that long-term treatment with CS-514 causes a compensatory increase in the synthesis of hydroxymethylglutaryl-CoA reductase which leads to augmented hepatic de novo cholesterol synthesis and subsequent increased cholesterol output followed by an increase in the lithogenicity of bile. CS-514 apparently does not prevent cholesterol gallstone formation in those examples where the mechanism is thought to be due to augmented hepatic de novo cholesterol synthesis (type IV hyperlipidemia).
- Published
- 1989
25. [The effect of smoking habit on aortic pulse wave velocity using a new method for data analysis]
- Author
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Gen Konemori, Masaki Itoh, Itaru Horiuchi, Goro Kajiyama, Yuri Kuroki, Shigenobu Matsuoka, Masataka Hiraoka, Atsuko Nakamoto, and Masahiro Kawanishi
- Subjects
Adult ,Male ,Smoking habit ,Arteriosclerosis ,medicine.artery ,Statistics ,Medicine ,Humans ,cardiovascular diseases ,Pulse ,Pulse wave velocity ,Aorta ,Aged ,Pulse (signal processing) ,business.industry ,Smoking ,Age Factors ,Regression analysis ,Middle Aged ,medicine.disease ,Regression ,Blood pressure ,cardiovascular system ,Regression Analysis ,Geriatrics and Gerontology ,business ,circulatory and respiratory physiology - Abstract
We measured aortic pulse wave velocity (PWV) in 168 male adult cases of various arteriosclerotic diseases. In order to evaluate the effects of age, smoking habits, alcohol intake, and blood pressure, we applied the least median of squares (LMS) regression which was considered to be very useful for data analysis. The results showed that PWV level increased with age. Furthermore smoking was associated with increasing PWV level and this effect was also related to age. We concluded that the PWV was valuable as an index of arteriosclerosis, and instead of the classical least squares method, LMS regression was very useful for analysis of medical data.
- Published
- 1989
26. Changes in high density lipoproteins in patients with hepatobiliary diseases. Levels and lipid composition of HDL2 and HDL3 and LCAT reaction
- Author
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Akima Miyoshi, Koki Takata, Masaharu Yamamoto, Masahiro Nakagawa, Goro Kajiyama, and Itaru Horiuchi
- Subjects
Adult ,Male ,medicine.medical_specialty ,food.ingredient ,Biliary Tract Diseases ,Sterol O-acyltransferase ,Blood lipids ,Lecithin ,Phosphatidylcholine-Sterol O-Acyltransferase ,chemistry.chemical_compound ,food ,Internal medicine ,medicine ,Choline ,Humans ,Phospholipids ,Triglycerides ,Cholesterol ,business.industry ,Liver Diseases ,Fatty liver ,Cholesterol, HDL ,Gastroenterology ,Albumin ,Hepatology ,medicine.disease ,Endocrinology ,chemistry ,lipids (amino acids, peptides, and proteins) ,Female ,business ,Lipoproteins, HDL - Abstract
Lipids of HDL (high density lipoproteins) and their subfractions (HDL2 and HDL3), and LCAT activity (lecithin: cholesterol acyltransferase) were determined in hepatobiliary diseases without severe hyperbilirubinemia (less than 10 mg/dl). The decrease in major lipid constituents (cholesterol and phospholipids) of HDL was mainly attributable to the decrease in those of HDL3, except in some liver diseases of acute or severe stage (acute hepatitis in an acute stage and hepatoma) which were accompanied with a simultaneous moderate decrease in those of HDL2 and in fatty liver which showed a preferential decrease in those of HDL2. The LCAT activity also decreased in several diseases. Some of the hepatobiliary diseases, on the contrary, showed an increase in HDL-triglycerides (mostly in HDL3 and in some diseases also in HDL2) which might participate to some extent in secondary hyperlipidemia in the liver parenchymal diseases, although they were the minor lipid constituents of HDL. From results that HDL3- but not HDL2-cholesterol levels significantly correlated with serum total protein, albumin and choline esterase, it was suggested that the decrease in large constituents of HDL, particularly of HDL3, is caused by hepatocellular dysfunction which causes inhibition of protein and lipid syntheses in the liver in most of the hepatobiliary diseases except for fatty liver which has a preferential decrease in HDL2 lipids.
- Published
- 1983
27. ASSAY OF GALACTOSE OR N-ACETYLNEURAMINIC ACID-GALACTOSE TERMINATED GLYCOPROTEIN IN THE SERUM OF COLORECTAL CANCER PATIENTS
- Author
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Keiji Nishida, Yohichi Nagamura, Hiroshi Ito, Isao Ishiguro, Itaru Horiuchi, Hiroaki Naruse, Masahiko Yamazaki, Mitsushi Sakagami, and Hidekuni Honda
- Subjects
chemistry.chemical_classification ,chemistry.chemical_compound ,chemistry ,Biochemistry ,Colorectal cancer ,Galactose ,Gastroenterology ,medicine ,Surgery ,medicine.disease ,Glycoprotein ,N-Acetylneuraminic acid - Published
- 1988
- Full Text
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