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Regulatory Action of ß-adrenergic Agonist and 8-bromocyclic AMP on Calcium Currents in the Unfertilized Mouse Eggs
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  • Regulatory Action of ß-adrenergic Agonist and 8-bromocyclic AMP on Calcium Currents in the Unfertilized Mouse Eggs
저자명
Haan, Jae-Hee,Cheong, Seung-Jin,Kim, Yang-Mi,Park, Choon-Ok,Hong, Seong-Geun
간행물명
대한생리학회지
권/호정보
1993년|27권 2호(통권52호)|pp.175-184 (10 pages)
발행정보
대한생리학회|한국
파일정보
정기간행물|ENG|
PDF텍스트(0.21MB)
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영문초록

There are many report suggesting that influx and intracellular calcium concentration ([Ca2+]i) are related to cell signalling in various cells. However, it has not been reported that calcium channel activation is affected by the substances involved in signal transduction pathways in the mouse eggs. In this study, the effects of isoprenaline (ISP) and cyclic AMP on calcium influx through calcium channels were investigated to show their relationship with the signal transduction process in unfertilized mouse eggs. Using whole cell voltage clamp techniques, calcium currents, elicited by the depolarizing pulses of 300 ms duration (from -50 mV to 50 mV in 10 mV increments) from a holding potential of -80 mV, were recorded. The current-voltage (I-V) relation of calcium currents was shown to be bell-shaped; the current began to activate at -50 mV and reached its maximum (-1.33±0.16 nA: mean±S.E., n=7) at -10 mV, then decayed at around 50 mV. Calcium currents were fully activated within 7 ms ~ 20 ms and completely inactivated 200 ms after onset of the step pulse. ISP within the concentration ranges of 10-8 M ~ 10-4 M dose-dependently increased the amplitude calcium current. The permeable cyclic AMP analogue,8-bromocyclic AMP, also increased its maximal amplitude by 46ft at 10-5 M, while protein kinase inhibitor (PKI), which is known to inhibit 0.02 phosphorylating units of cyclic AMP-dependent protein kinase (PKA) per microgram decreased calcium currents. Currents recorded in the presence of PKI were resistant to increase by the application of 10-5 M. Also, PKI inhibited the calcium current increase elicited by ISP treatment. These results suggest that β-adrenergic regulation of the calcium channel is mediated by the cAMP-dependent protein kinase. This signal transduction pathway might play a role in regulating [Ca2+]i, level due to the increase of calcium influx in mouse eggs.

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