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Two distinct functional effects of protein phosphatase inhibitors on guinea‐pig cardiac L‐type Ca2+ channels.
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Description
<jats:p>1. The effects of the phosphatase inhibitors okadaic acid and calyculin A on single guinea‐pig ventricular L‐type Ca2+ channels were studied. The inactive derivative norokadaone was used as a negative control. 2. The two known effects of cAMP‐dependent stimulation are mimicked by the phosphatase inhibitors to a varying extent. Only okadaic acid promotes the high‐activity gating mode (‘mode 2’), while calyculin A increases channel availability to a larger extent. As revealed by kinetic analysis of slow gating, the two phosphatase inhibitors retard a slow rate constant, which is assumed to represent exit from the available state by dephosphorylation. Norokadaone was inactive in both regards. 3. Mode 2 gating elicited by very positive prepulses is augmented by okadaic acid, and mode 2 lifetime is prolonged. Calyculin A fails to affect these parameters. Thus, voltage‐facilitated mode 2 gating reveals the same pharmacological properties as the mode 2 sweeps observed using conventional pulse protocols. 4. The results are interpreted in terms of the different sensitivity of protein phosphatase subtypes towards the inhibitors: channel availability appears to be controlled by a phosphorylation site dephosphorylated by a type 1‐like phosphatase, while mode 2 gating is coupled to a distinct site, dephosphorylated by a type 2A‐like phosphatase.</jats:p>
Journal
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- The Journal of Physiology
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The Journal of Physiology 484 (3), 583-592, 1995-05
Wiley
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Details 詳細情報について
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- CRID
- 1360011145719983488
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- ISSN
- 14697793
- 00223751
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- Data Source
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- Crossref