Biphasic Increase in Chamiluminescence of Lymphokine-Treated
スポンサーリンク
概要
- 論文の詳細を見る
The effect of incubation time with lymphokines on macrophage activities was studied by use of the phorbol myristate acetate-induced luminol-dependent chemiluminescence method and cytotoxicity test. When thioglycollate-elicited ICR mouse peritoneal macrophages were incubated with lymphokines, their ability to generate chemiluminescence increased biphasically during incubation. That is, within one day, it reached a maximal level at about 4 h (early response), and then progressively decreased to the control level. However, when the incubation time was further prolonged, it began to increase again, and reached about 2-fold the control level after 3 d (late response). The increase in the chemiluminescence of lymphokine-treated macrophages with increasing incubation time is not due to the increase in the macrophage cell numbers. In contrast to the clear biphasic increase in chemiluminescence, there was no clear biphasic increase in cytotoxicity in lymphokine-treated macrophages. The activities in the lymphokine supernatants to induce the early and the late chemiluminescent response in macrophages disappeared together with the activity to induce cytotoxicity, on dialysis at pH 2 for 24 h or on heating at 80℃ for 30 min, but not at 56℃ for 30 min. Although the lymphokines increasing macrophage chemiluminescence were separated into two fractions in Sephadex G-100 gel filtration, each fraction had both activities to induce the early and the late chemiluminescent response, and the major fraction largely corresponded to that of the activity to induce cytotoxicity. These results suggested that there is a lymphokine which alters macrophage chemiluminescence biphasically by itself, and it may be interferon-γ.
- 公益社団法人日本薬学会の論文
- 1988-01-25
著者
-
松本 優子
Department Of Clinical Chemistry School Of Pharmaceutical Science Toho University
-
松本 優子
Department Of Biology Faculty Of Education Gunma University
-
武藤 里志
Department Of Clinical Chemistry School Of Pharmaceutical Science Toho University
-
由岐 英剛
Department of Clinical Chemistry, School of Pharmaceutical Science, Toho University
-
荻野 秀敏
Department of Clinical Chemistry, School of Pharmaceutical Science, Toho University
-
五十嵐 かおる
Department of Clinical Chemistry, School of Pharmaceutical Science, Toho University
-
由岐 英剛
Faculty Of Pharmaceutical Sciences Osaka University
-
由岐 英剛
Department Of Clinical Chemistry School Of Pharmaceutical Science Toho University
-
五十嵐 かおる
Department Of Clinical Chemistry School Of Pharmaceutical Science Toho University
-
荻野 秀敏
Department Of Clinical Chemistry School Of Pharmaceutical Science Toho University
関連論文
- Studies of Oligosaccharides. XV. Syntheses of Hydroquinone Glycosides of Gentio Oligosaccharides
- Studies of Oligosaccharides. XII. Hydrophilization of Glycyrrhetinic Acid by Coupling to Gentio Oligosaccharides
- A Simple Fluorescent Post-labeling Technique with o-Phthalaldehyde for the Analysis of Proteins by Polyacrylamide Gel Electrophoresis
- Determination of Cytosine, 3-Methylcytosine, and 5-Methylcytosine in Nucleic Acids by High Performance Liquid Chromatography
- Rapid Effect of Interferon-γ on Human Monocyte Chemiluminescence
- Biphasic Increase in Chamiluminescence of Lymphokine-Treated
- Rapid Effect of Lymphokines on Macrophage Activities Determined by Measuring Chemiluminescence
- Effect of Light on Nonphotosynthetic Microorganisms. IV. Photoinduced Carotenogenesis in Mycobacterium smegmatis
- Field and Laboratory Studies on the Growth of Pectinatella gelatinosa OKA, a Freshwater Bryozoan
- Study on Some Factors Affecting the Precision of Luminescence Analyses
- Studies on Antiviral Agents. V. Synthesis and Antiviral Activity of N-Chloro Compounds.
- Studies on Antiviral Agents. IV. Biological Activity of Tenuazonic Acid Derivatives.
- Studies on Antiviral Agents. I. Relationship between Chemical Reactivity of Sulfhydryl Reagents and Their Inactivating Activity of Adenovirus Type 5
- Synthesis and Anti-tumor Activity of Tenuazonic Acid Analogues
- Computerized Analyzing System for Chemiluminescence
- Trisulfation of Hexoses by Means of Concentrated Sulfuric Acid
- Studies on Antiviral Agents. III. Synthesis of Tenuazonic Acid Derivatives.
- Studies on Antiviral Agents. II. Synthesis and Biological Activity of Maleimide Derivatives.
- Synthesis of Purine and Pyrimidine Derivatives of Arsonic Acid.
- Studies on Chemotherapeutic Agents.III. A Synthesis of 3-Phenylpurine Derivatives
- Studies on Chemotherapeutic Agents.II. A Synthesis of Purine Nucleosides of _D-Glucuronic Acid
- Studies on Chemotherapeutic Agents.I. A Synthesis of Pyrimidine Nucleosides of D-glucuronic Acid and Its Derivatives
- A Synthesis of Uracil and Cytosine Nucleosides containing D-Glucuronic Acid and its Derivatives as the Sugar Component
- Rearrangement Reaction of 7-Mercaptooxazolo[5,4-d]pyrimidine to 7-Hydroxythiazolo[5,4-d]pyrimidine
- Syntheses of Thiazolo-[5,4-d]pyrimidine Derivatives and Related Compounds.
- The Synthesis of 8-Substituted Purine Derivatives. II. Some 8-Substituted 6-Mercaptopurines.
- Studies of Oligosaccharides. XIV. Structure-Activity Relationship of Variations in the Sugar Moiety of Digitoxin
- The Synthesis of 8-Substituted Purine Derivatives. I. Some 8-Substituted Derivatives of Hypoxanthine.