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1988 Fiscal Year Final Research Report Summary

ULTRAMICRO METHODS FOR DETERMINING ENZYME ACTIVITIES AND SUBSTRATES USING COMBINED BIOLUMINESCENT ASSAY WITH ENZYMATIC CYCLING

Research Project

Project/Area Number 62870009
Research Category

Grant-in-Aid for Developmental Scientific Research

Allocation TypeSingle-year Grants
Research Field General pharmacology
Research InstitutionUNIVERSITY OF TOKYO

Principal Investigator

ENDOU Hitoshi  , 医学部・薬理学, 助教授 (20101115)

Project Period (FY) 1987 – 1988
KeywordsBioluminescence / Enzymatic cycling / Ultramicro analysis / ATP / NADH / Na^+,K^+-ATPase / Isolated nephron segment / 単離ネフロン分節 / NADPH
Research Abstract

To investigate metabolic and pharmacological properties in individual cells constituting heterogenous organs or tissues, ultramicro analysis sensitive enough to be applicable to a single cell should be required. In this project, combined bioluminescent assays with enzymatic cycling methods gave been established.
1) Automatic analysis of bioluminescence. An automatic analysising system has been established by comining a luminometer (LKB-1251) and personal computer (PC 8201) with a recorder or a printer.
2) Micromethod of ATP determination. Extraction of cellular ATP by 10 % trichloroacetic acid has been found to be the best. A tiny amount of ATP less than 10^<-12> mol could be assayed with firefly luciferin and luciferase using the luminometer. By this analytical procedrue, substrate specificity to maintain cellular ATP was clarified in various mouse nephron sehments.
3) Ultramicro analyses of of Na^+,K^+-ATPase activities and fmolar orders of ammonia. Using HADH: FMN oxidoreductase and luciferase, Na^+,K^+-ATPase activity could be quantified by determining pyruvate coverted from phosphoeno lpyruvate in the presence of ADP (a metabolyte of ATP splitted by ATPase) and pyruvate kinase. When enzymatic cycling of NAD was compined with bioluminescent assay, 10^<-16> mol ADP could be determined. This ultramicro method can be applied for the determination of ATPase activity in a single cell. Similarly, fmol ammonia could be analized. These methods were successfully applied for the study of intranephron ammoniagenesis.
4) Ultramicro assay of glucose. Tiny amounts of glucose (less than 10^<-15> mol) could be quantified using combined bioluminesxent assay of NADPH with NADP/NADPH enzymatic cycling method. This analytical procedure has been applied to intrenephron gluconeogenesis study.
5) Real time analysis of superoxide. Using luminol, superoxide stimulated by phorbol ester in isolated glomeruli could be successfully monitored.

  • Research Products

    (47 results)

All Other

All Publications (47 results)

  • [Publications] Endou,H.: Molecular Nephrology. 347-352 (1987)

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  • [Publications] Oka,Y.: Renal Physiol. 10. 283-288 (1987)

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  • [Publications] Oka,Y.: Pediatric Nephrol.2. 124-128 (1988)

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  • [Publications] Koseki,C.: Kidney Int. 33. 543-554 (1988)

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  • [Publications] Endou,H.: Contr.Nehrol.63. 86-90 (1988)

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  • [Publications] Oka,Y.: Biochem.Int.16. 941-948 (1988)

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  • [Publications] Tazawa,J.: Biochem.Int.16. 1127-1135 (1988)

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  • [Publications] Uchida,S.: Am.J.Physiol.255. F977-F983 (1988)

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  • [Publications] Tamura,K.: Am.J.Physiol.255. F1122-F1127 (1988)

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  • [Publications] Endou,H.: Proc.Jap.Acad.

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  • [Publications] Endou,H.: Kidney Int.

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  • [Publications] Jung,K.Y.: Toxicol.Appl.Pharmacol.

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  • [Publications] Jung,K.Y.: Toxicol.Appl.Pharmacol.

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  • [Publications] Takemoto,F.: Pflugers Arch.

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  • [Publications] 伊藤進: 臨床化学. 16. 136-141 (1987)

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  • [Publications] 遠藤仁: 小児科診察. 50. 1321-1327 (1987)

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  • [Publications] 遠藤仁: 日本臨床. 夏季増刊. 290-309 (1987)

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  • [Publications] 遠藤仁: 臨床水電解質. 7. 589-590 (1987)

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  • [Publications] 高橋剛: 腎と透析. 24. 181-187 (1988)

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  • [Publications] 角野勝彦: 腎と透析. 24(5). 743-748 (1988)

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  • [Publications] 内田信一: 腎と透析. 臨時増刊. 55-61 (1988)

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  • [Publications] Endou,H.: "International Forum on Research and Development for Procedure Involving Risk Assessment of Toxic Chemicals" Ed.by Korean society of Toxicology,157 (1987)

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  • [Publications] 遠藤仁: "尿細管異常の検査と臨床" 宇宙堂八木書店, 28 (1987)

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  • [Publications] 遠藤仁: "Annual Review 腎臓 1987" 中外医学社, 52 (1987)

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  • [Publications] 遠藤仁: "医薬品有害作用の予測" R&Dプランニング, 407 (1987)

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  • [Publications] 遠藤仁: "臨床薬物治療学大系 9 老年者" 情報開発研究所, 71 (1987)

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  • [Publications] 遠藤仁: "図解 食道静脈瘤硬化療法" 医学書院, 36 (1988)

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  • [Publications] 遠藤仁: "講座プロスタグランジン 6.腎と硬組織" 東京化学同人, 219 (1988)

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  • [Publications] 遠藤仁: "臨床産業医学全書2-2 産業内科学" 医歯薬出版, 375 (1988)

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  • [Publications] Endou. H.; Yamada, H.; Takahashi, T.; Tamura, K.; Ito, S.: "Intranephron distribution and properties of xanthine oxidase, superoxide dismutase and guanase activities in control and nephrotic rats." Molecular Nephrology. 347-352 (1987)

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  • [Publications] Oka, Y.; Fujiwara, K.; Endou, H.: "Intranephron distribution of EGF immunoreactivity in the mouse." Renal Physiol. 10. 283-288 (1987)

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  • [Publications] Oka, Y.; Fujiwara, K.; Endou, H.: "Epidermal growth factor in the mouse kidney: developmental changes and intranephron localizations." Pediatric Nephrol.2. 124-128 (1988)

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  • [Publications] Koseki, C.; Yamaguchi, Y.; Furusawa, M.; Endou, H.: "Isolation by monoclonal antubody of intercalated cells of rabbit kidney" Kidney Int. 33. 543-554 (1988)

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  • [Publications] Endou, H.; Tamura, S.; Saka, S.; Nishio, Y.; Takemoto, F.; Takahashi, T.: "Intranephron ammoniagenesis and its regulation by PGE_2 in rats and mice." Contr. Nehrol.63. 86-90 (1988)

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  • [Publications] Oka, Y.; Sakamoto, K.; Ikeda, H.; Nagoshi, S.; Tsukagoshi, S.; Aburada,M.; Endou, H.; Fujiwara, K.: "A two-site solid phase enzyme immunoassay foe rat epidermal growth factor." Biochem. Int.16. 941-948 (1988)

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  • [Publications] Tazawa, J.; Endou, H.; Sato, A.; Hasumura, Y.; Takeuchi, J.: "Functional heterogeneity of rat hepatocytes: predominance of aryl hydrocarbon hydroxylase activity in perivenular zone." Biochem. Int.16. 1127-1135 (1988)

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  • [Publications] Uchida, S.; Endou, H.: "Substrate specificity to maintain cellular ATP along the mouse nephron." Am. J. Physiol.255. 977-983 (1988)

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  • [Publications] Tamura, K.; Endou, H.: "Contribution of the purine nucleotide cycle to intranephron ammoniagenesis in rats." Am. J. Physiol.255. 1122-1127 (1988)

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  • [Publications] Endou, H.; Miyanoshita, A.; Jung, K. Y.: "Intranephron distribution of insulin binding in Wistar Kyoto and Spontaneously Hypertensive Rats." Proc. Jap. Acad.

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  • [Publications] Endou, H.; Obara, T.; Ueno, Y.: "Mechanism of ochratoxcity A nephrotoxicity in rats." Kidney Int.

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  • [Publications] Jung, K.Y.; Uchida S.; Endou, H.: "Nephrotoxicity assessment by measuring cellular ATP content. I. Substrate specificities in the maintenance of ATP content in isolated rat nephron segnents." Toxicol. Appl. Pharmacol.

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  • [Publications] Jung, K.Y; Endou, H.: "Nephrotoxicity assessment by measuring cellular ATP content. II. Intranephron site and mechanism of ochratoxin A nephrotoxicity." Toxicol. Appl. Pharmacol.

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  • [Publications] Takemoto, F.; Miyanoshita, A.; Shimamura, K.; Sunano, S.; Endou, H.: "Intranephron PGE_2 production in stroke-prone SHR and WKY." Pflugers Arch.

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  • [Publications] Nosaka, K.; Nakada, J.; Endou, H.: "Cisplation-induced alterations in renal structure, ammoniagenesis and gluconeogenesis of rats." Kidney Int.

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  • [Publications] Endou, H.: Proc. JSPS-NRCT Workshop, Clinical Pharmacology & Pharmacokinetics of Cardiovascular and Renal Drugs.I.C.M.R. Kobe., 119-126 (1987)

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  • [Publications] Endou, H.: International Forum on Research and Development for Procedure Involving Risk Assessment of Toxic Chemicals.Korean Society of Toxicology, 157-174 (1987)

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  • [Publications] Endou, H.: Proceedings of the First Korea-Japan Toxicology Symposium, Safety Assessment of Chemicals in Vitro.Korean Society of Toxicology, 57-66 (1987)

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Published: 1990-12-19  

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