B-Type Natriuretic Peptide Exerts Broad Functional Opposition to Transforming Growth Factor-β in Primary Human Cardiac Fibroblasts

Kapoun, Ann M.; Liang, Faquan; O’Young, Gilbert; Damm, D; Quon, Diana; White, Roger; Munson, Kimberly; Lam, Andrew; Schreiner, George F.; Protter, Andrew A.

doi:10.1161/01.res.0000117070.86556.9f

Cited by 268 publications

(182 citation statements)

References 49 publications

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“…TGF-␤ treatment is known to enhance the profibrotic state by altering expression of proteins such as plasminogen activator inhibitor (PAI-1) and IL-6 (28,29). Consistent with the ability of increased AC expression to blunt collagen synthesis, overexpression of AC6 decreased basal and TGF-␤-regulated expression of PAI-1 by 89 Ϯ 3% and 59 Ϯ 8%, respectively, and IL-6 by 81 Ϯ 2% and 92 Ϯ 3%, respectively.…”

Section: Ac6 Overexpression Enhances Forskolin-and Adrenomedullin-stimentioning

confidence: 78%

Inhibition of cardiac myofibroblast formation and collagen synthesis by activation and overexpression of adenylyl cyclase

Swaney

Roth

Olson

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

192

179

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Transformation of fibroblasts to myofibroblasts, characterized by expression of ␣-smooth muscle actin (␣-SMA) and production of extracellular matrix (ECM) components, is a key event in connective tissue remodeling. Approaches to inhibit this transformation are needed in tissues, such as the heart, where excessive ECM production by cardiac fibroblasts (CFs) causes fibrosis, myocardial stiffening, and cardiac dysfunction. We tested whether adenylyl cyclase (AC) activation (increased cAMP levels) modulates the transformation of adult rat CF to myofibroblasts, as assessed by immunofluorescent microscopy, immunoblotting, and collagen synthesis. A 24-h incubation of CF with TGF-␤ or angiotensin II increased ␣-SMA expression, which was inhibited by the AC agonist forskolin and a cAMP analog that activates protein kinase A. Treatment with forskolin blunted serum-, TGF-␤-, and angiotensin II-stimulated collagen synthesis. CFs engineered to overexpress type 6 AC had enhanced forskolin-promoted cAMP formation, greater inhibition by forskolin of TGF-␤-stimulated ␣-SMA expression, and a decrease in the EC 50 of forskolin to reduce serum-stimulated collagen synthesis. The AC stimulatory agonist adrenomedullin inhibited collagen synthesis in CF that overexpressed AC6 but not in controls. Thus, AC stimulation blunts collagen synthesis and, in parallel, the transformation of adult rat CF to myofibroblasts. AC overexpression enhances these effects, ''uncovering'' an inhibition by adrenomedullin. These findings implicate cAMP as an inhibitor of ECM formation by means of blockade of the transformation of CF to myofibroblasts and suggest that increasing AC expression, thereby enhancing cAMP generation through stimulation of receptors expressed on CF, could provide a means to attenuate and prevent cardiac fibrosis and its sequelae.cardiac fibroblast ͉ cyclic AMP ͉ extracellular matrix ͉ fibrosis ͉ heart failure

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Section: Ac6 Overexpression Enhances Forskolin-and Adrenomedullin-stimentioning

confidence: 78%

Inhibition of cardiac myofibroblast formation and collagen synthesis by activation and overexpression of adenylyl cyclase

Swaney

Roth

Olson

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

192

179

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“…Furthermore, lysyl oxidase (LOX) is also instrumental during collagen biogenesis that catalyzes lysine-derived cross-bridges between two or more lysine residues of nascent procollagen peptides during their maturation into collagen molecules (5, 7). Altered and deregulated expression of these factors has been demonstrated in failing myocardium (5).Involvement of various neurohumoral and growth factors has also been illustrated in the development of cardiac fibrosis both in vitro and in vivo (3,8). Cellular cross-talk between AngII-treated cardiomyocytes and fibroblasts has been shown to play an important role during collagen up-regulation with involvement of IL-6 during fibrosis (8 -10).…”

mentioning

confidence: 99%

“…Involvement of various neurohumoral and growth factors has also been illustrated in the development of cardiac fibrosis both in vitro and in vivo (3,8). Cellular cross-talk between AngII-treated cardiomyocytes and fibroblasts has been shown to play an important role during collagen up-regulation with involvement of IL-6 during fibrosis (8 -10).…”

mentioning

confidence: 99%

Inhibition of Signal Transducer and Activator of Transcription 3 (STAT3) Attenuates Interleukin-6 (IL-6)-induced Collagen Synthesis and Resultant Hypertrophy in Rat Heart

Mir

Chatterjee

Mitra

et al. 2012

Journal of Biological Chemistry

123

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IL-6 has been shown to play a major role in collagen up-regulation process during cardiac hypertrophy, although the precise mechanism is still not known. In this study we have analyzed the mechanism by which IL-6 modulates cardiac hypertrophy. For the in vitro model, IL-6-treated cultured cardiac fibroblasts were used, whereas the in vivo cardiac hypertrophy model was generated by renal artery ligation in adult male Wistar rats (Rattus norvegicus). During induction of hypertrophy, increased phosphorylation of STAT1, STAT3, MAPK, and ERK proteins was observed both in vitro and in vivo. Treatment of fibroblasts with specific inhibitors for STAT1 (fludarabine, 50 M), STAT3 (S31-201, 10 M), p38 MAPK (SB203580, 10 M), and ERK1/2 (U0126, 10 M) resulted in down-regulation of IL-6-induced phosphorylation of specific proteins; however, only S31-201 and SB203580 inhibited collagen biosynthesis. In ligated rats in vivo, only STAT3 inhibitors resulted in significant decrease in collagen synthesis and hypertrophy markers such as atrial natriuretic factor and ␤-myosin heavy chain. In addition, decreased heart weight to body weight ratio and improved cardiac function as measured by echocardiography was evident in animals treated with STAT3 inhibitor or siRNA. Compared with IL-6 neutralization, more pronounced down-regulation of collagen synthesis and regression of hypertrophy was observed with STAT3 inhibition, suggesting that STAT3 is the major downstream signaling molecule and a potential therapeutic target for cardiac hypertrophy.Cardiac fibrosis is considered to be a major player during hypertrophy, where excess synthesis and a disproportionate accumulation of extracellular matrix proteins in the myocardium leads to its stiffness and diastolic dysfunction, leading to heart failure (1-3). Fibrillar collagen 1 and collagen 3 are the most abundant extracellular matrix proteins in the myocardium that maintain myocardial structural integrity (4). Collagen biosynthesis process is mainly compartmentalized in cardiac fibroblasts with a continuous turnover of newly synthesized collagen and degradation of old existing collagen, which involves post-transcriptional as well as post translational events. A physiological balance exists between collagen synthesis and degradation that is necessary to maintain tissue integrity of the myocardium. Extracellular catalytic cleavage of collagen is mediated by matrix metalloproteinases (MMPs) 2 that are eventually regulated by their naturally occurring endogenous inhibitors, i.e. tissue inhibitors of metalloproteinases (TIMPs) (1, 5).The fine balance between MMPs and TIMPs plays a crucial role in regulation of cardiac collagen turnover (5, 6). Furthermore, lysyl oxidase (LOX) is also instrumental during collagen biogenesis that catalyzes lysine-derived cross-bridges between two or more lysine residues of nascent procollagen peptides during their maturation into collagen molecules (5, 7). Altered and deregulated expression of these factors has been demonstrated in failing myocardium (5).Involvem...

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“…It was of interest that transforming growth factor-β (TGF-β) was under-expressed in young HHR. A recent study has shown that human B-type natriuretic peptide (BNP) inhibits TGF-β-induced effects on primary human cardiac fibroblasts, including down-regulating TGF-β-regulated genes related to fibrosis, myofibroblast conversion, proliferation, and inflammation (33). The mouse homologue to the polypeptide hormone BNP, natriuretic peptide precursor type B (Nppb), was over-expressed in both young and old HHR, and several matrix/structural protein-related genes (β-actin, Actb; procollagen-5, Col5a1; cartilage associated protein, Crtap) were under-expressed in young HHR.…”

Section: Discussionmentioning

confidence: 99%

Myocardial Gene Expression Associated with Genetic Cardiac Hypertrophy in the Absence of Hypertension

et al. 2008

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B-Type Natriuretic Peptide Exerts Broad Functional Opposition to Transforming Growth Factor-β in Primary Human Cardiac Fibroblasts

Cited by 268 publications

References 49 publications

Inhibition of cardiac myofibroblast formation and collagen synthesis by activation and overexpression of adenylyl cyclase

Inhibition of cardiac myofibroblast formation and collagen synthesis by activation and overexpression of adenylyl cyclase

Inhibition of Signal Transducer and Activator of Transcription 3 (STAT3) Attenuates Interleukin-6 (IL-6)-induced Collagen Synthesis and Resultant Hypertrophy in Rat Heart

Myocardial Gene Expression Associated with Genetic Cardiac Hypertrophy in the Absence of Hypertension

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