Changes in cyclic AMP dependent protein kinase and active stiffness in the rat volume overload model of heart hypertrophy

Sergio Lavandero; Gastón Cartagena; Eduardo Guarda; Ramón Corbalán; Iván Godoy; Mario Sapag-Hagar; Jorge E. Jalil

doi:10.1093/cvr/27.9.1634

Changes in cyclic AMP dependent protein kinase and active stiffness in the rat volume overload model of heart hypertrophy

Sergio Lavandero, Gastón Cartagena, Eduardo Guarda, Ramón Corbalán, Iván Godoy, Mario Sapag-Hagar, Jorge E. Jalil

Universidad de Chile

Research output: Contribution to journal › Article › peer-review

28 Citations (Scopus)

Abstract

Objective: The aim was to clarify the role of cyclic AMP dependent protein kinase (PKA) and changes in mechanical heart function during development of cardiac hypertrophy induced by volume overload. Methods: Protein and DNA contents, PKA activity, and peak systolic stress-strain relationships in hearts from animals submitted to aortocaval shunt were assessed as a function of time. Sham operated (control) rats were used as controls. Results: Heart weight to body weight ratio and cardiac protein content per heart increased from d 7 (p < 0.005 and p < 0.01, respectively) reaching their highest values by d 56; the same occurred with cardiac DNA content. PKA activity·g^-1 tissue in soluble extracts of hearts from rats with aortocaval shunt increased by 2.7-fold on d 2 (p < 0.005), reached a ninefold peak increase by d 7 (p < 0.0001) and declined to fourfold by d 56 with respect to control values. The end peak systolic stress-strain relation slopes were: control, 368(SEM 14) g·cm^-2 (n=16); aortocaval shunt values: 2 d, 514(28) g·cm^-2 (n=6); 7 d, 579(10) g·cm^-2 (n=7); and 56 d, 554(28) g·cm^-2 (n=7). The force generating capacity at 0% strain was also significantly higher in the shunt groups as compared to sham operated controls (p < 0.01). Early activation of PKA was also confirmed through endogenous cardiac protein phosphorylation. SDS-PAGE gel electrophoretogram and autoradiography showed more heavily phosphorylated bands in aortocaval shunt hearts than in the control group. Conclusions: PKA activity and the slope of systolic stress-strain regression line followed a similar trend throughout the study, with an early increase in both variables by d 2 in the shunt group, reaching a peak at d 7, and decreasing thereafter but remaining higher than in controls. PKA activity appears to be related to increased force generating capacity rather than to hypertrophy or increased cardiac protein content. Thus PKA activation is an early biochemical event after aortocaval shunt, followed later by cardiac hypertrophy. Changes in PKA activity showed a similar trend to mechanical heart function over time. These findings help to explain the changes in the mechanical properties of the heart preceding the development of cardiac hypertrophy in the rat model of volume overload.Cardiovascular Research 1993;27:1634-1638.

Original language	English
Pages (from-to)	1634-1638
Number of pages	5
Journal	Cardiovascular Research
Volume	27
Issue number	9
DOIs	https://doi.org/10.1093/cvr/27.9.1634
Publication status	Published - Sept 1993

Bibliographical note

Funding Information:
SL is the recipient of a fellowship from Fundaci6n Andes. Chile. We thank Dr CI Pogson for critical review of the manuscript. This work was supported in part by Grants FONDECYT 90-0712. 90-0722 and 92-0738.

Funding

SL is the recipient of a fellowship from Fundaci6n Andes. Chile. We thank Dr CI Pogson for critical review of the manuscript. This work was supported in part by Grants FONDECYT 90-0712. 90-0722 and 92-0738.

Funders	Funder number
Fundaci6n Andes
Fondo Nacional de Desarrollo Científico y Tecnológico	90-0722, 90-0712, 92-0738

ASJC Scopus Subject Areas

General Medicine

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10.1093/cvr/27.9.1634

Cite this

Lavandero, S., Cartagena, G., Guarda, E., Corbalán, R., Godoy, I., Sapag-Hagar, M., & Jalil, J. E. (1993). Changes in cyclic AMP dependent protein kinase and active stiffness in the rat volume overload model of heart hypertrophy. Cardiovascular Research, 27(9), 1634-1638. https://doi.org/10.1093/cvr/27.9.1634

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title = "Changes in cyclic AMP dependent protein kinase and active stiffness in the rat volume overload model of heart hypertrophy",

abstract = "Objective: The aim was to clarify the role of cyclic AMP dependent protein kinase (PKA) and changes in mechanical heart function during development of cardiac hypertrophy induced by volume overload. Methods: Protein and DNA contents, PKA activity, and peak systolic stress-strain relationships in hearts from animals submitted to aortocaval shunt were assessed as a function of time. Sham operated (control) rats were used as controls. Results: Heart weight to body weight ratio and cardiac protein content per heart increased from d 7 (p < 0.005 and p < 0.01, respectively) reaching their highest values by d 56; the same occurred with cardiac DNA content. PKA activity·g-1 tissue in soluble extracts of hearts from rats with aortocaval shunt increased by 2.7-fold on d 2 (p < 0.005), reached a ninefold peak increase by d 7 (p < 0.0001) and declined to fourfold by d 56 with respect to control values. The end peak systolic stress-strain relation slopes were: control, 368(SEM 14) g·cm-2 (n=16); aortocaval shunt values: 2 d, 514(28) g·cm-2 (n=6); 7 d, 579(10) g·cm-2 (n=7); and 56 d, 554(28) g·cm-2 (n=7). The force generating capacity at 0% strain was also significantly higher in the shunt groups as compared to sham operated controls (p < 0.01). Early activation of PKA was also confirmed through endogenous cardiac protein phosphorylation. SDS-PAGE gel electrophoretogram and autoradiography showed more heavily phosphorylated bands in aortocaval shunt hearts than in the control group. Conclusions: PKA activity and the slope of systolic stress-strain regression line followed a similar trend throughout the study, with an early increase in both variables by d 2 in the shunt group, reaching a peak at d 7, and decreasing thereafter but remaining higher than in controls. PKA activity appears to be related to increased force generating capacity rather than to hypertrophy or increased cardiac protein content. Thus PKA activation is an early biochemical event after aortocaval shunt, followed later by cardiac hypertrophy. Changes in PKA activity showed a similar trend to mechanical heart function over time. These findings help to explain the changes in the mechanical properties of the heart preceding the development of cardiac hypertrophy in the rat model of volume overload.Cardiovascular Research 1993;27:1634-1638.",

author = "Sergio Lavandero and Gast{\'o}n Cartagena and Eduardo Guarda and Ram{\'o}n Corbal{\'a}n and Iv{\'a}n Godoy and Mario Sapag-Hagar and Jalil, {Jorge E.}",

note = "Funding Information: SL is the recipient of a fellowship from Fundaci6n Andes. Chile. We thank Dr CI Pogson for critical review of the manuscript. This work was supported in part by Grants FONDECYT 90-0712. 90-0722 and 92-0738.",

year = "1993",

month = sep,

doi = "10.1093/cvr/27.9.1634",

language = "English",

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T1 - Changes in cyclic AMP dependent protein kinase and active stiffness in the rat volume overload model of heart hypertrophy

AU - Lavandero, Sergio

AU - Cartagena, Gastón

AU - Guarda, Eduardo

AU - Corbalán, Ramón

AU - Godoy, Iván

AU - Sapag-Hagar, Mario

AU - Jalil, Jorge E.

N1 - Funding Information: SL is the recipient of a fellowship from Fundaci6n Andes. Chile. We thank Dr CI Pogson for critical review of the manuscript. This work was supported in part by Grants FONDECYT 90-0712. 90-0722 and 92-0738.

PY - 1993/9

Y1 - 1993/9

N2 - Objective: The aim was to clarify the role of cyclic AMP dependent protein kinase (PKA) and changes in mechanical heart function during development of cardiac hypertrophy induced by volume overload. Methods: Protein and DNA contents, PKA activity, and peak systolic stress-strain relationships in hearts from animals submitted to aortocaval shunt were assessed as a function of time. Sham operated (control) rats were used as controls. Results: Heart weight to body weight ratio and cardiac protein content per heart increased from d 7 (p < 0.005 and p < 0.01, respectively) reaching their highest values by d 56; the same occurred with cardiac DNA content. PKA activity·g-1 tissue in soluble extracts of hearts from rats with aortocaval shunt increased by 2.7-fold on d 2 (p < 0.005), reached a ninefold peak increase by d 7 (p < 0.0001) and declined to fourfold by d 56 with respect to control values. The end peak systolic stress-strain relation slopes were: control, 368(SEM 14) g·cm-2 (n=16); aortocaval shunt values: 2 d, 514(28) g·cm-2 (n=6); 7 d, 579(10) g·cm-2 (n=7); and 56 d, 554(28) g·cm-2 (n=7). The force generating capacity at 0% strain was also significantly higher in the shunt groups as compared to sham operated controls (p < 0.01). Early activation of PKA was also confirmed through endogenous cardiac protein phosphorylation. SDS-PAGE gel electrophoretogram and autoradiography showed more heavily phosphorylated bands in aortocaval shunt hearts than in the control group. Conclusions: PKA activity and the slope of systolic stress-strain regression line followed a similar trend throughout the study, with an early increase in both variables by d 2 in the shunt group, reaching a peak at d 7, and decreasing thereafter but remaining higher than in controls. PKA activity appears to be related to increased force generating capacity rather than to hypertrophy or increased cardiac protein content. Thus PKA activation is an early biochemical event after aortocaval shunt, followed later by cardiac hypertrophy. Changes in PKA activity showed a similar trend to mechanical heart function over time. These findings help to explain the changes in the mechanical properties of the heart preceding the development of cardiac hypertrophy in the rat model of volume overload.Cardiovascular Research 1993;27:1634-1638.

AB - Objective: The aim was to clarify the role of cyclic AMP dependent protein kinase (PKA) and changes in mechanical heart function during development of cardiac hypertrophy induced by volume overload. Methods: Protein and DNA contents, PKA activity, and peak systolic stress-strain relationships in hearts from animals submitted to aortocaval shunt were assessed as a function of time. Sham operated (control) rats were used as controls. Results: Heart weight to body weight ratio and cardiac protein content per heart increased from d 7 (p < 0.005 and p < 0.01, respectively) reaching their highest values by d 56; the same occurred with cardiac DNA content. PKA activity·g-1 tissue in soluble extracts of hearts from rats with aortocaval shunt increased by 2.7-fold on d 2 (p < 0.005), reached a ninefold peak increase by d 7 (p < 0.0001) and declined to fourfold by d 56 with respect to control values. The end peak systolic stress-strain relation slopes were: control, 368(SEM 14) g·cm-2 (n=16); aortocaval shunt values: 2 d, 514(28) g·cm-2 (n=6); 7 d, 579(10) g·cm-2 (n=7); and 56 d, 554(28) g·cm-2 (n=7). The force generating capacity at 0% strain was also significantly higher in the shunt groups as compared to sham operated controls (p < 0.01). Early activation of PKA was also confirmed through endogenous cardiac protein phosphorylation. SDS-PAGE gel electrophoretogram and autoradiography showed more heavily phosphorylated bands in aortocaval shunt hearts than in the control group. Conclusions: PKA activity and the slope of systolic stress-strain regression line followed a similar trend throughout the study, with an early increase in both variables by d 2 in the shunt group, reaching a peak at d 7, and decreasing thereafter but remaining higher than in controls. PKA activity appears to be related to increased force generating capacity rather than to hypertrophy or increased cardiac protein content. Thus PKA activation is an early biochemical event after aortocaval shunt, followed later by cardiac hypertrophy. Changes in PKA activity showed a similar trend to mechanical heart function over time. These findings help to explain the changes in the mechanical properties of the heart preceding the development of cardiac hypertrophy in the rat model of volume overload.Cardiovascular Research 1993;27:1634-1638.

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Changes in cyclic AMP dependent protein kinase and active stiffness in the rat volume overload model of heart hypertrophy

Abstract

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ASJC Scopus Subject Areas

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