Article (Scientific journals)
Overexpression of the sarcolemmal calcium pump in the myocardium of transgenic rats.
Hammes, A.; Oberdorf-Maass, S.; Rother, T. et al.
1998In Circulation Research, 83 (9), p. 877-88
Peer reviewed
 

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Keywords :
Animals; Animals, Genetically Modified; Calcium/metabolism; Calcium-Transporting ATPases/analysis/genetics/physiology; Heart/physiology; Hemodynamics; Humans; Immunoblotting; Myocardium/enzymology; Rats; Sarcolemma/enzymology
Abstract :
[en] The plasma membrane calmodulin-dependent calcium ATPase (PMCA) is a calcium-extruding enzyme controlling Ca2+ homeostasis in nonexcitable cells. However, its function in the myocardium is unclear because of the presence of the Na+/Ca2+ exchanger. We approached the question of the physiological function of the calcium pump using a transgenic "gain of function" model. Transgenic rat lines carrying the human PMCA 4 cDNA under control of the ventricle-specific myosin light chain-2 promoter were established, and expression in the myocardium was ascertained at the mRNA, protein, and functional levels. In vivo hemodynamic measurements in adult homozygous animals showed no differences in baseline and increased cardiac performance recruited by volume overload compared with controls. No differences between transgenic and control cardiomyocytes were found in patch clamp voltage dependence, activation/inactivation behavior of the L-type Ca2+ current, or fast [Ca2+]i transients (assessed by the Fura-2 method). To test whether the PMCA might be involved in processes other than beat-to-beat regulation of contraction/relaxation, we compared growth processes of neonatal transgenic and control cardiomyocytes. A 1.6- and 2.3-fold higher synthesis rate of total protein was seen in cells from transgenic animals compared with controls on incubation with 2% FCS for 24 hours and 36 hours, respectively. An effect of similar magnitude was observed using 20 micromol/L phenylephrine. A 1.4-fold- and 2.0-fold-higher protein synthesis peak was seen in PMCA-overexpressing cardiomyocytes after stimulation with isoproterenol for 12 hours and 24 hours, respectively. Because pivotal parts of the alpha- and beta-adrenergic signal transduction pathways recently have been localized to caveolae, we tested the hypothesis that the PMCA might alter the amplitude of alpha- and beta-adrenergic growth signals by virtue of its localization in caveolae. Biochemical as well as immunocytochemical studies suggested that the PMCA in large part was colocalized with caveolin 3 in caveolae of cardiomyocytes. These results indicate that the sarcolemmal Ca2+-pump has little relevance for beat-to-beat regulation of contraction/relaxation in adult animals but likely plays a role in regulating myocardial growth, possibly through modulation of caveolar signal transduction.
Disciplines :
Cardiovascular & respiratory systems
Author, co-author :
Hammes, A.
Oberdorf-Maass, S.
Rother, T.
Nething, K.
Gollnick, F.
Linz, K. W.
Meyer, R.
Hu, K.
Han, H.
Gaudron, P.
Ertl, G.
Hoffmann, S.
Ganten, U.
Vetter, R.
Schuh, K.
Benkwitz, C.
Zimmer, H. G.
Neyses, Ludwig ;  University of Luxembourg > Research Office
More authors (8 more) Less
Language :
English
Title :
Overexpression of the sarcolemmal calcium pump in the myocardium of transgenic rats.
Publication date :
1998
Journal title :
Circulation Research
ISSN :
0009-7330
Volume :
83
Issue :
9
Pages :
877-88
Peer reviewed :
Peer reviewed
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