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IP3 receptor types 2 and 3 mediate exocrine secretion underlying energy metabolism
Authors:Futatsugi Akira  Nakamura Takeshi  Yamada Maki K  Ebisui Etsuko  Nakamura Kyoko  Uchida Keiko  Kitaguchi Tetsuya  Takahashi-Iwanaga Hiromi  Noda Tetsuo  Aruga Jun  Mikoshiba Katsuhiko
Institution:Calcium Oscillation, International Cooperative Research Project, Japan Science and Technology Agency, Tokyo 108-0071, Japan. afutatsu@brain.riken.jp
Abstract:Type 2 and type 3 inositol 1,4,5-trisphosphate receptors (IP3R2 and IP3R3) are intracellular calcium-release channels whose physiological roles are unknown. We show exocrine dysfunction in IP3R2 and IP3R3 double knock-out mice, which caused difficulties in nutrient digestion. Severely impaired calcium signaling in acinar cells of the salivary glands and the pancreas in the double mutants ascribed the secretion deficits to a lack of intracellular calcium release. Despite a normal caloric intake, the double mutants were hypoglycemic and lean. These results reveal IP3R2 and IP3R3 as key molecules in exocrine physiology underlying energy metabolism and animal growth.
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