Calpastatin Domain L Is Involved in the Regulation of L-Type Ca Channels in Guinea Pig Cardiac Myocytes

We have found previously that L-type Ca super(2+) channel run-down in cell-free patches is partially (10-28%) reversed by calpastatin (CS) and have suggested that CS, an endogenous inhibitor of calpain, has a Ca super(2+)-channel-regulating function. CS is composed of repetitive domains 1-4 (calpain...

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Veröffentlicht in:Biochemical and biophysical research communications 2000-12, Vol.279 (3), p.756-761
Hauptverfasser: Hao, L, Kameyama, A, Kuroki, S, Takano, J, Takano, E, Maki, M, Kameyama, M
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Sprache:eng
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Zusammenfassung:We have found previously that L-type Ca super(2+) channel run-down in cell-free patches is partially (10-28%) reversed by calpastatin (CS) and have suggested that CS, an endogenous inhibitor of calpain, has a Ca super(2+)-channel-regulating function. CS is composed of repetitive domains 1-4 (calpain-inhibitory domain) and domain L (a domain whose function is unknown). We therefore investigated which domain of CS was involved in the regulation of Ca super(2+) channel activity in guinea pig cardiac myocytes using the patch-clamp technique. After the patches were excised into inside-out mode in basic internal solution, the Ca super(2+) channel activity ran down to 0.45% of the control level recorded in the cell-attached mode. Application of human recombinant full-length CS (25 mu M) and domain L (25 mu M) restored the Ca super(2+) channel activity to 13 and 19% of the control level, respectively, while the channel activity was not restored by CS domain 1 (25 mu M) (0.66%). Mouse CS domain XLL (25 mu M), a complex of domain XL and domain L, restored the calcium channel activity to 11% of the control level. These results suggested that the Ca super(2+)-channel-regulating function of CS is located in domain L. This study is the first description of the function of CS domain L. Copyright 2000 Academic Press.
ISSN:0006-291X
DOI:10.1006/bbrc.2000.4040