Neuroendocrine properties of intrinsic cardiac adrenergic cells in fetal rat heart

Abstract

Intrinsic cardiac adrenergic (ICA) cells in developing rat heart constitute a novel adrenergic signaling system involved in cardiac regulation. Regulatory mechanisms of ICA cells remain to be defined. Immunohistochemical study of fetal rat hearts demonstrated ICA cells with catecholamine biosynthetic enzyme tyrosine hydroxylase (TH) and phenylethanolamine N-methyltransferase (PNMT). The mRNA of TH and PNMP was also detected in fetal rat hearts before sympathetic innervation. Immunoreactivity of norepinephrine transporter (NET) was localized to ICA cells in rat heart tissue and primary cell culture. For the functional study, the activity of intracellular Ca²⁺concentration ([Ca²⁺]_i) transients was quantified by a ratio fluorescent spectrometer in cultured ICA cells and myocytes. ICA cells generated spontaneous [Ca²⁺]_itransients that were eliminated by tetrodotoxin or Ca²⁺-free solutions and showed greatly reduced amplitude with the addition of L-type Ca²⁺channel blocker nifedipine. [³H]norepinephrine studies demonstrate release and uptake of norepinephrine. Functional interaction between catecholamines produced by the ICA cells and cocultured myocytes was evident by the effect of the β-adrenergic blocker atenolol eliciting a dose-dependent reduction in the amplitude and frequency of [Ca²⁺]_itransients of beating myocytes. Hypoxia inhibited [Ca²⁺]_itransient activity of ICA cells, which subsequently produced a reoxygenation-mediated rebound augmentation of [Ca²⁺]_itransients. We conclude that ICA cells are capable of catecholamine synthesis, release, and uptake. They generate spontaneous [Ca²⁺]_itransient activity that can be regulated by oxygen tension. ICA cells may provide an alternative adrenergic supply to maintain cardiac contractile and pacemaker function at rest and during stress in the absence of sympathetic innervation.