Stabilization of the B-type natriuretic peptide mRNA in cardiac myocytes by α-adrenergic receptor activation: Potential roles for protein kinase C and mitogen-activated protein kinase

Deanna S. Hanford; Christopher C. Glembotski

doi:10.1210/me.10.12.1719

Stabilization of the B-type natriuretic peptide mRNA in cardiac myocytes by α-adrenergic receptor activation: Potential roles for protein kinase C and mitogen-activated protein kinase

Deanna S. Hanford
, Christopher C. Glembotski

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

41 Scopus citations

Abstract

In cardiac myocytes, B-type natriuretic peptide (BNP) expression is induced with the rapid kinetics of a primary response gene. Like many other primary response gene transcripts, the BNP mRNA possesses destabilizing elements and is believed to be short-lived. The rapid induction of a short- lived transcript could be achieved partly by agonist-mediated increases in mRNA t( 1/4 ). Accordingly, the present study was undertaken to evaluate whether the α₁-adrenergic receptor agonist, phenylephrine (PE), a known inducer of BNP expression, could stabilize the BNP mRNA and, if so, what signaling pathways might be involved. In primary myocardial cells treated with a transcription inhibitor, the t( 1/4 ) of the BNP mRNA was found to be about 1 h in the absence of PE; however, in the presence of PE, the t( 1/4 ) increased to 5 h. It was shown that neither the calmodulin kinase inhibitor, KN-62, nor the protein tyrosine kinase inhibitor, tyrphostin, blocked PE-mediated stabilization of the BNP mRNA. However, either the protein kinase C (PKC) inhibitor, GF 109203X, or the mitogen-activated protein kinase kinase (MAPKK) inhibitor, PD 098059, effected some blockade of the stabilizing effects of PE. While maximal doses of PD 098059 nearly completely blocked PE-activated MAPK, stabilization was only partially inhibited. Moreover, maximal doses of GF 109203X, which only partially blocked PE-activated MAPK, nearly completely inhibited stabilization. Thus, while MAPK appears to be required for maximal agonist-mediated stabilization, PKC seems to play a dominant role, participating through both MAPK-dependent and -independent pathways. These results establish roles for both the PKC and MAPK families in α₁-adrenergic receptor-mediated stabilization of the BNP mRNA, suggesting that the rapid induction of BNP expression might be due, in part, to this agonist-mediated increase in mRNA t( 1/4 ).

Original language	English (US)
Pages (from-to)	1719-1727
Number of pages	9
Journal	Molecular Endocrinology
Volume	10
Issue number	12
DOIs	https://doi.org/10.1210/me.10.12.1719
State	Published - 1996
Externally published	Yes

ASJC Scopus subject areas

Molecular Biology
Endocrinology

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@article{6504023d574945ab866d09f8b77a6cb5,

title = "Stabilization of the B-type natriuretic peptide mRNA in cardiac myocytes by α-adrenergic receptor activation: Potential roles for protein kinase C and mitogen-activated protein kinase",

abstract = "In cardiac myocytes, B-type natriuretic peptide (BNP) expression is induced with the rapid kinetics of a primary response gene. Like many other primary response gene transcripts, the BNP mRNA possesses destabilizing elements and is believed to be short-lived. The rapid induction of a short- lived transcript could be achieved partly by agonist-mediated increases in mRNA t( 1/4 ). Accordingly, the present study was undertaken to evaluate whether the α1-adrenergic receptor agonist, phenylephrine (PE), a known inducer of BNP expression, could stabilize the BNP mRNA and, if so, what signaling pathways might be involved. In primary myocardial cells treated with a transcription inhibitor, the t( 1/4 ) of the BNP mRNA was found to be about 1 h in the absence of PE; however, in the presence of PE, the t( 1/4 ) increased to 5 h. It was shown that neither the calmodulin kinase inhibitor, KN-62, nor the protein tyrosine kinase inhibitor, tyrphostin, blocked PE-mediated stabilization of the BNP mRNA. However, either the protein kinase C (PKC) inhibitor, GF 109203X, or the mitogen-activated protein kinase kinase (MAPKK) inhibitor, PD 098059, effected some blockade of the stabilizing effects of PE. While maximal doses of PD 098059 nearly completely blocked PE-activated MAPK, stabilization was only partially inhibited. Moreover, maximal doses of GF 109203X, which only partially blocked PE-activated MAPK, nearly completely inhibited stabilization. Thus, while MAPK appears to be required for maximal agonist-mediated stabilization, PKC seems to play a dominant role, participating through both MAPK-dependent and -independent pathways. These results establish roles for both the PKC and MAPK families in α1-adrenergic receptor-mediated stabilization of the BNP mRNA, suggesting that the rapid induction of BNP expression might be due, in part, to this agonist-mediated increase in mRNA t( 1/4 ).",

author = "Hanford, \{Deanna S.\} and Glembotski, \{Christopher C.\}",

year = "1996",

doi = "10.1210/me.10.12.1719",

language = "English (US)",

volume = "10",

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journal = "Molecular Endocrinology",

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T1 - Stabilization of the B-type natriuretic peptide mRNA in cardiac myocytes by α-adrenergic receptor activation

T2 - Potential roles for protein kinase C and mitogen-activated protein kinase

AU - Hanford, Deanna S.

AU - Glembotski, Christopher C.

PY - 1996

Y1 - 1996

N2 - In cardiac myocytes, B-type natriuretic peptide (BNP) expression is induced with the rapid kinetics of a primary response gene. Like many other primary response gene transcripts, the BNP mRNA possesses destabilizing elements and is believed to be short-lived. The rapid induction of a short- lived transcript could be achieved partly by agonist-mediated increases in mRNA t( 1/4 ). Accordingly, the present study was undertaken to evaluate whether the α1-adrenergic receptor agonist, phenylephrine (PE), a known inducer of BNP expression, could stabilize the BNP mRNA and, if so, what signaling pathways might be involved. In primary myocardial cells treated with a transcription inhibitor, the t( 1/4 ) of the BNP mRNA was found to be about 1 h in the absence of PE; however, in the presence of PE, the t( 1/4 ) increased to 5 h. It was shown that neither the calmodulin kinase inhibitor, KN-62, nor the protein tyrosine kinase inhibitor, tyrphostin, blocked PE-mediated stabilization of the BNP mRNA. However, either the protein kinase C (PKC) inhibitor, GF 109203X, or the mitogen-activated protein kinase kinase (MAPKK) inhibitor, PD 098059, effected some blockade of the stabilizing effects of PE. While maximal doses of PD 098059 nearly completely blocked PE-activated MAPK, stabilization was only partially inhibited. Moreover, maximal doses of GF 109203X, which only partially blocked PE-activated MAPK, nearly completely inhibited stabilization. Thus, while MAPK appears to be required for maximal agonist-mediated stabilization, PKC seems to play a dominant role, participating through both MAPK-dependent and -independent pathways. These results establish roles for both the PKC and MAPK families in α1-adrenergic receptor-mediated stabilization of the BNP mRNA, suggesting that the rapid induction of BNP expression might be due, in part, to this agonist-mediated increase in mRNA t( 1/4 ).

AB - In cardiac myocytes, B-type natriuretic peptide (BNP) expression is induced with the rapid kinetics of a primary response gene. Like many other primary response gene transcripts, the BNP mRNA possesses destabilizing elements and is believed to be short-lived. The rapid induction of a short- lived transcript could be achieved partly by agonist-mediated increases in mRNA t( 1/4 ). Accordingly, the present study was undertaken to evaluate whether the α1-adrenergic receptor agonist, phenylephrine (PE), a known inducer of BNP expression, could stabilize the BNP mRNA and, if so, what signaling pathways might be involved. In primary myocardial cells treated with a transcription inhibitor, the t( 1/4 ) of the BNP mRNA was found to be about 1 h in the absence of PE; however, in the presence of PE, the t( 1/4 ) increased to 5 h. It was shown that neither the calmodulin kinase inhibitor, KN-62, nor the protein tyrosine kinase inhibitor, tyrphostin, blocked PE-mediated stabilization of the BNP mRNA. However, either the protein kinase C (PKC) inhibitor, GF 109203X, or the mitogen-activated protein kinase kinase (MAPKK) inhibitor, PD 098059, effected some blockade of the stabilizing effects of PE. While maximal doses of PD 098059 nearly completely blocked PE-activated MAPK, stabilization was only partially inhibited. Moreover, maximal doses of GF 109203X, which only partially blocked PE-activated MAPK, nearly completely inhibited stabilization. Thus, while MAPK appears to be required for maximal agonist-mediated stabilization, PKC seems to play a dominant role, participating through both MAPK-dependent and -independent pathways. These results establish roles for both the PKC and MAPK families in α1-adrenergic receptor-mediated stabilization of the BNP mRNA, suggesting that the rapid induction of BNP expression might be due, in part, to this agonist-mediated increase in mRNA t( 1/4 ).

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DO - 10.1210/me.10.12.1719

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SN - 0888-8809

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EP - 1727

JO - Molecular Endocrinology

JF - Molecular Endocrinology

IS - 12

ER -

Stabilization of the B-type natriuretic peptide mRNA in cardiac myocytes by α-adrenergic receptor activation: Potential roles for protein kinase C and mitogen-activated protein kinase

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