CD38 disruption impairs glucose-induced increases in cyclic ADP-ribose, [Ca2+]i, and insulin secretion

被引：192

作者：

Kato, I ^{[1
]}

Yamamoto, Y ^{[1
]}

Fujimura, M ^{[1
]}

Noguchi, N ^{[1
]}

Takasawa, S ^{[1
]}

Okamoto, H ^{[1
]}

机构：

[1] Tohoku Univ, Sch Med, Dept Biochem, Aoba Ku, Sendai, Miyagi 9808575, Japan

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1999年 / 274卷 / 04期

关键词：

D O I：

10.1074/jbc.274.4.1869

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：

Increases in [Ca2+](i) in pancreatic beta cells, resulting from Ca2+ mobilization from intracellular stores as well as Ca2+ influx from extracellular sources, are important in insulin secretion by glucose. Cyclic ADP-ribose (cADPR), accumulated in beta cells by glucose stimulation, has been postulated to serve as a second messenger for intracellular Ca2+ mobilization for insulin secretion, and CD38 is thought to be involved in the cADPR accumulation (Takasawa, S,, Tohgo, k, Noguchi, N,, Koguma, T,, Nata, K,, Sugimoto, T,, Yonekura, H.,, and Okamoto, H, (1993) J. Biol. Chem, 268, 26052-26054), Here we created "knockout" (CD38(-/-)) mice by homologous recombination, CD38(-/-) mice developed normally but showed no increase in their glucose-induced production of cADPR in pancreatic islets, The glucose-induced [Ca2+](i) rise and insulin secretion were both severely impaired in CD38(-/-) islets, whereas CD38(-/-) islets responded normally to the extracellular Ca2+ influx stimulants tolbutamide and KCl, CD38(-/-) mice showed impaired glucose tolerance, and the serum insulin level was lower than control, and these impaired phenotypes were rescued by beta cell-specific expression of CD38 cDNA These results indicate that CD38 plays an essential role in intracellular Ca2+ mobilization by cADPR for insulin secretion.

引用

页码：1869 / 1872

页数：4

共 37 条

[1] SITE-SPECIFIC RECOMBINATION OF A TRANSGENE IN FERTILIZED-EGGS BY TRANSIENT EXPRESSION OF CRE RECOMBINASE [J].

ARAKI, K ;

ARAKI, M ;

MIYAZAKI, J ;

VASSALLI, P .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (01) :160-164

[2]

ASHCROFT FM, 1992, INSULIN MOL BIOL PAT, P97

[3] POLYMORPHISMS IN THE CODING AND NONCODING REGIONS OF MURINE PGK-1 ALLELES [J].

BOER, PH ;

POTTEN, H ;

ADRA, CN ;

JARDINE, K ;

MULLHOFER, G ;

MCBURNEY, MW .

BIOCHEMICAL GENETICS, 1990, 28 (5-6) :299-308

[4] Mice deficient for the ecto-nicotinamide adenine dinucleotide glycohydrolase CD38 exhibit altered humoral immune responses [J].

Cockayne, DA ;

Muchamuel, T ;

Grimaldi, JC ;

Muller-Steffner, H ;

Randall, TD ;

Lund, FE ;

Murray, R ;

Schuber, F ;

Howard, MC .

BLOOD, 1998, 92 (04) :1324-1333

[5] CA2+-INDUCED CA2+ RELEASE IN SEA-URCHIN EGG HOMOGENATES - MODULATION BY CYCLIC ADP-RIBOSE [J].

GALIONE, A ;

LEE, HC ;

BUSA, WB .

SCIENCE, 1991, 253 (5024) :1143-1146

[6] SPONTANEOUS DIABETES PRODUCED BY SELECTIVE BREEDING OF NORMAL WISTAR RATS [J].

GOTO, Y ;

KAKIZAKI, M ;

MASAKI, N .

PROCEEDINGS OF THE JAPAN ACADEMY, 1975, 51 (01) :80-85

[7] DELETION OF A DNA-POLYMERASE-BETA GENE SEGMENT IN T-CELLS USING CELL-TYPE-SPECIFIC GENE TARGETING [J].

GU, H ;

MARTH, JD ;

ORBAN, PC ;

MOSSMANN, H ;

RAJEWSKY, K .

SCIENCE, 1994, 265 (5168) :103-106

[8]

HARADA N, 1993, J IMMUNOL, V151, P3111

[9]

HERMANS MP, 1987, DIABETOLOGIA, V30, P659

[10] ADP RIBOSYL CYCLASE ACTIVITY OF A NOVEL BONE-MARROW STROMAL CELL-SURFACE MOLECULE, BST-1 [J].

HIRATA, Y ;

KIMURA, N ;

SATO, K ;

OHSUGI, Y ;

TAKASAWA, S ;

OKAMOTO, H ;

ISHIKAWA, J ;

KAISHO, T ;

ISHIHARA, K ;

HIRANO, T .

FEBS LETTERS, 1994, 356 (2-3) :244-248

← 1 2 3 4 →