VOLUME REGULATION IN MOUSE PANCREATIC BETA-CELLS IS MEDIATED BY A FUROSEMIDE-SENSITIVE MECHANISM

被引：0

作者：

ENGSTROM, KG ^{[1
]}

SANDSTROM, PE ^{[1
]}

SEHLIN, J ^{[1
]}

机构：

[1] UMEA UNIV,DEPT HISTOL & CELL BIOL,S-90187 UMEA,SWEDEN

来源：

BIOCHIMICA ET BIOPHYSICA ACTA | 1991年 / 1091卷 / 02期

关键词：

BETA-CELL MEMBRANE; VOLUME REGULATION; COTRANSPORT; FUROSEMIDE; RUBIDIUM ION EFFLUX; (MOUSE);

D O I：

暂无

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

A possible role for loop diuretic-sensitive Cl-/cation cotransport in volume regulation in the pancreatic beta-cells was investigated by measuring Rb-86+ efflux from beta-cell-rich pancreatic islets as well as the size of isolated beta-cells under different osmotic conditions. Lowering the osmolarity to 262 mosM (83% of control) resulted in a rapid cell swelling which was followed by regulatory volume decrease (RVD). RVD was completely inhibited by furosemide (1 mM), an inhibitor of Cl-/cation co-transport. The hypotonic medium (262 mosM) induced a rapid and strong increase in Rb-86+ efflux from beta-cell-rich mouse pancreatic islets and the furosemide-sensitive portion of the efflux was significantly increased. A slightly less hypotonic medium (285 mosM, 90% of control) induced only cell swelling and no RVD. With this medium only a marginal increase in Rb-86+ efflux was observed. Increasing the osmolarity by adding 50 mM naCl (final osmolarity: 417 mosM, 132% of control) induced a rapid cell shrinkage but no regulatory volume increase (RVI). When the osmolarity was increased from a slightly hypotonic medium (262 mosM) to an isotonic medium (317 mosM) an initial cell shrinkage was followed by RVI. This RVI was inhibited by 1 mM furosemide. The data suggest that RVD as well as RVI in the beta-cells are mediated by loop diuretic-sensitive cotransport of chloride and cations and that these cells show a threshold for hypotonic stimulation of RVD.

引用

页码：145 / 150

页数：6

共 28 条

[1] EFFECT OF HYPOSMOLARITY ON INSULIN RELEASE INVITRO
BLACKARD, WG
KIKUCHI, M
RABINOVITCH, A
RENOLD, AE
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1975, 228 (03): : 706 - 713
[2] VOLUME REGULATION BY AMPHIUMA RED-BLOOD-CELLS - THE MEMBRANE-POTENTIAL AND ITS IMPLICATIONS REGARDING THE NATURE OF THE ION-FLUX PATHWAYS
CALA, PM
[J]. JOURNAL OF GENERAL PHYSIOLOGY, 1980, 76 (06) : 683 - 708
[3] THE NA+/K+/CL- COTRANSPORT IN C6 GLIOMA-CELLS - PROPERTIES AND ROLE IN VOLUME REGULATION
CHASSANDE, O
FRELIN, C
FARAHIFAR, D
JEAN, T
LAZDUNSKI, M
[J]. EUROPEAN JOURNAL OF BIOCHEMISTRY, 1988, 171 (03): : 425 - 433
[4] VOLUME REGULATION IN MOUSE PANCREATIC-ISLET CELLS AS STUDIED BY A NEW TECHNIQUE OF MICROPERIFUSION
ENGSTROM, KG
SANDSTROM, PE
[J]. ACTA PHYSIOLOGICA SCANDINAVICA, 1989, 137 (03): : 393 - 397
[5] ACTIVATION OF ION-TRANSPORT SYSTEMS DURING CELL-VOLUME REGULATION
EVELOFF, JL
WARNOCK, DG
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1987, 252 (01): : F1 - F10
[6] VOLUME REGULATION BY HUMAN-LYMPHOCYTES - ROLE OF CALCIUM
GRINSTEIN, S
DUPRE, A
ROTHSTEIN, A
[J]. JOURNAL OF GENERAL PHYSIOLOGY, 1982, 79 (05) : 849 - 868
[7] RESPONSES OF LYMPHOCYTES TO ANISOTONIC MEDIA - VOLUME-REGULATING BEHAVIOR
GRINSTEIN, S
ROTHSTEIN, A
SARKADI, B
GELFAND, EW
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1984, 246 (03): : C204 - C215
[8] HAHN HJ, 1974, J BIOL CHEM, V249, P5275
[9] STUDIES IN OBESE-HYPERGLYCEMIC MICE
HELLMAN, B
[J]. ANNALS OF THE NEW YORK ACADEMY OF SCIENCES-SERIES, 1965, 131 (A1): : 541 - +
[10] SEPARATE, CA-2+-ACTIVATED K+ AND CL- TRANSPORT PATHWAYS IN EHRLICH ASCITES TUMOR-CELLS
HOFFMANN, EK
LAMBERT, IH
SIMONSEN, LO
[J]. JOURNAL OF MEMBRANE BIOLOGY, 1986, 91 (03) : 227 - 244

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