ALTERED LEVELS OF PHOSPHATIDYLINOSITOL PHOSPHOLIPASE-C ACTIVITY IN RAT-LIVER CELLS IN RESPONSE TO INSULIN, EPINEPHRINE, ACETYLCHOLINE AND BACTERIAL PHOSPHOLIPASE-C

被引：1

作者：

KAMBEROV, ES

TRIFONOV, B

机构：

[1] PAISIJ HILENDARSKI UNIV PLOVDIV,DEPT BIOCHEM & MICROBIOL,PLOVDIV,BULGARIA

[2] MED UNIV PLOVDIV,DEPT PHYSIOL,PLOVDIV,BULGARIA

来源：

REGULATORY PEPTIDES | 1993年 / 44卷 / 03期

关键词：

COMBINED EFFECT; FLUORIDE; INHIBITION; MEMBRANE PREPARATION; SOLUBLE FACTOR;

D O I：

10.1016/0167-0115(93)90135-U

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Rat liver cells were homogenized and subsequently fractionated by a simplified method based on microfiltration, which proved to give a high recovery of membrane-bound phosphatidylinositol phospholipase C (PI-PLC) activity. The effects of insulin, acetylcholine (AC). epinephrine (EN) and bacterial phopsholipase C (bPLC) on the PI-PLC activity were studied after in vitro treatment of isolated membranes or after in situ application in rat liver. A dose-dependent increase of membranous PI-PLC (up to 3-fold) and corresponding 36 to 72% decline of the cytosolic activity were established upon treatment with supraphysiological doses of insulin or with bPLC, respectively. AC induced a biphasic response with a maximal stimulation in the micromolar range. On the other hand EN promoted a slight but significant dose-dependent inhibition of PI-PLC in both cytosol and membranes. Sodium fluoride was also a potent inhibitor of the membrane-associated PI-PLC with an EC50 value of about 5 mM. The combined assay with NaF and EN revealed no additivity between their inhibitory effects, suggesting a common step in the mechanism(s) of inhibition caused by the two agents. The stimulatory effects of insulin and AC were partially reduced by soluble cytosolic factors, which still remain to be identified. When insulin and AC were applied in combination in the presence of cytosol, this resulted in a 56% inhibition of PI-PLC below the control level.

引用

页码：257 / 267

页数：11

共 50 条

[31] DESENSITIZATION OF VASCULAR PHOSPHOLIPASE-C ACTIVITY
SEASHOLTZ, TM
GURDAL, H
WANG, HY
FRIEDMAN, E
JOHNSON, MD
FASEB JOURNAL, 1995, 9 (04): : A950 - A950
[32] PHOSPHOLIPASE-C ACTIVITY IN CARDIOMYOPHATIC HAMSTER
KAWAGUCHI, H
OKAMOTO, H
SANO, H
SHOKI, M
YASUDA, H
KITABATAKE, A
JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY, 1992, 24 : S45 - S45
[33] GLYCAN REQUIREMENTS OF GLYCOSYLPHOSPHATIDYLINOSITOL PHOSPHOLIPASE-C FROM TRYPANOSOMA-BRUCEI - GLUCOSAMINYLINOSITOL DERIVATIVES INHIBIT PHOSPHATIDYLINOSITOL PHOSPHOLIPASE-C
MORRIS, JC
LEI, PS
SHEN, TY
MENSAWILMOT, K
JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (06) : 2517 - 2524
[34] ASSAY OF A PHOSPHATIDYLINOSITOL BISPHOSPHATE PHOSPHOLIPASE-C ACTIVITY IN POSTMORTEM HUMAN BRAIN
ONEILL, C
FOWLER, CJ
WIEHAGER, B
ALAFUZOFF, I
WINBLAD, B
BRAIN RESEARCH, 1991, 543 (02) : 307 - 314
[35] PHOSPHATIDYLINOSITOL-SPECIFIC PHOSPHOLIPASE-C OF MURINE LYMPHOCYTES
KAMISAKA, Y
TOYOSHIMA, S
OSAWA, T
ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1986, 249 (02) : 569 - 578
[36] INHIBITION OF BACTERIAL PHOSPHOLIPASE-C PRODUCTION BY CLINDAMYCIN
BULKACZ, J
SUTTER, VL
NEWMAN, MG
JOURNAL OF DENTAL RESEARCH, 1983, 62 : 290 - 290
[37] HUMAN-PLATELET ACTIVATION BY BACTERIAL PHOSPHOLIPASE-C IS MEDIATED BY PHOSPHATIDYLINOSITOL HYDROLYSIS BUT NOT GENERATION OF PHOSPHATIDIC-ACID - INHIBITION BY A SELECTIVE INHIBITOR OF PHOSPHOLIPASE-C
NAVRAN, SS
ROMSTEDT, K
CHANG, J
MILLER, DD
FELLER, DR
HUZOORAKBAR
THROMBOSIS RESEARCH, 1984, 33 (05) : 499 - 510
[38] PHOSPHOLIPASE-A AND PHOSPHOLIPASE-C ACTIVITY IN UREAPLASMA-UREALYTICUM
DESILVA, NS
QUINN, PA
PEDIATRIC INFECTIOUS DISEASE JOURNAL, 1986, 5 (06) : S350 - S350
[39] HETEROGENEITY OF PHOSPHOLIPASE-C IN RAT-BRAIN
TAKENAWA, T
HOMMA, Y
NAKANISHI, O
PHYSIOLOGY AND PHARMACOLOGY OF TRANSMEMBRANE SIGNALLING, 1989, 811 : 207 - 215
[40] IMIPRAMINE STIMULATES PHOSPHOLIPASE-C ACTIVITY IN RAT-BRAIN
FUKUDA, H
NISHIDA, A
SAITO, H
SHIMIZU, M
YAMAWAKI, S
NEUROCHEMISTRY INTERNATIONAL, 1994, 25 (06) : 567 - 571

← 1 2 3 4 5 →