Atrial and C-type natriuretic peptides amplify growth factor activity in primary aortic smooth muscle cells

doi:10.1016/S0008-6363(95)00148-4

Cardiovascular Research 1996 31(1):37-47; doi:10.1016/S0008-6363(95)00148-4
© 1996 by European Society of Cardiology

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Atrial and C-type natriuretic peptides amplify growth factor activity in primary aortic smooth muscle cells

Gursev S. Dhaunsi and Aviv Hassid^*

Department of Physiology and Biophysics, University of Tennessee, 894 Union Avenue, Memphis, TN 38163, USA

^* Corresponding author. Tel. (+1-901) 448-8304; Fax (+1-901) 448-7126. ahassid{at}physiol.utmem.edu

Objectives: The objective of the current study was to determinewhether atrial natriuretic peptides enhance the mitogenic effectof FGF-2, based on a previous study showing that NO enhancesthe mitogenic effect of FGF-2. Methods: Primary rat aortic smoothmuscle cells were used for all experiments. Mitogenic activitywas determined by (³H)thymidine incorporation and cell counting.Cyclic GMP was measured by radioimmunoassay. Messenger RNA wasmeasured by Northern blotting. FGFR-1 receptor protein was measuredby Western blotting. Results: ANP and CNP had no consistentmitogenic effect of their own but they both enhanced FGF-2-inducedDNA synthesis and/or cell proliferation by 2–3 fold. ANPenhanced the increase of c-fos mRNA induced by FGF-2. ANP, aloneor in combination with FGF-2, had no effect on FGF receptorprotein levels. HS-142-1, a specific antagonist of guanylylcyclase-linked A- or B-type ANP receptors, inhibited the co-mitogeniceffect of ANP. Exogenous cGMP was also co-mitogenic, whereastwo peptides that bind selectively to the ANF C-receptor, cANFand des[Cys¹⁰⁵,Cys¹²¹]rANF_104–126, had no mitogenic orco-mitogenic effect. The co-mitogenic effect of ANP graduallydisappeared as the subculture number of the cells was increased,indicating that it was selective for primary cells. ANP enhancedthe mitogenic response of primary aortic smooth muscle cellsto EGF whereas that to IGF-1 and PDGF was either not increased,or increased modestly. Conclusions: ANP enhances the mitogeniceffect of FGF-2, via a mechanism that may involve elevationof immediate early gene expression but not enhancement of FGFreceptor protein levels. We speculate that ANP and CNP releasedfrom macrophages and endothelial cells could enhance the mitogeniceffect of FGF-2 or EGF in vivo.

KEYWORDS cGMP; Mitogenesis; ANF; Growth factors; Smooth muscle cell proliferation

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