Endothelin converting enzyme (ECE) activity in human vascular smooth muscle

1. We have characterized the human smooth muscle endothelin converting enzyme (ECE) present in the media of the endothelium-denuded human umbilical vein preparation.
2. Endothelin-1 (ET-1) and ET-2 were potent constrictors of umbilical vein with EC₅₀ values of 9.2 nM and 29.6 nM, respectively. ET-1 was at least 30 times more potent than ET-3 suggesting the presence of constrictor ET_A receptors. Little or no response was obtained to the ET_B-selective agonist sarafotoxin 6c. These data suggest that endothelin-mediated vasoconstriction is via ET_A receptors in this preparation.
3. Autoradiographical visualization of endothelin receptors with subtype selective ligands confirmed the predominance of the ET_A receptor in the media of umbilical vein. High density of binding was obtained with the ET_A selective [¹²⁵I]-PD151242, with much lower levels detected with the ET_B selective [¹²⁵I]-BQ3020.
4. Big ET-1 (EC₅₀=42.7 nM) and big ET-2_(1-38) (EC₅₀=99.0 nM) were less potent than ET-1 and ET-2, respectively. Big ET-2_(1-38) was more potent than its isoform big ET-2_(1-37) with concentration–response curves to big ET-2_(1-37) incomplete at 300 nM. No response was obtained to big ET-3 at concentrations up to 700 nM. The C-terminal fragments, big ET-1_(22-38) and big ET-2_(22-38) were inactive.
5. Responses to ET-1 were unaffected by either the neutral endopeptidase (NEP) inhibitor thiorphan (10⁻⁵ M) or by the dual NEP/ECE inhibitor phosphoramidon (10⁻⁵ M). Big ET-1 was also unaffected by thiorphan but antagonized in a concentration-dependent manner by phosphoramidon (10⁻⁵ M and 10⁻⁴ M).
6. Addition of all four big endothelin peptides to human umbilical vein preparations resulted in detectable amounts of ET-IR in the bathing medium. Therefore, although big ET-3 was functionally inactive this reflects the low potency of ET-3 at the ET_A receptor rather than the lack of ability of this smooth muscle ECE to convert big ET-3 to ET-3.
7. To conclude we have demonstrated the presence of a phosphoramidon-sensitive ECE on the smooth muscle layer of the human umbilical vein which can convert big ET-1, big ET-2_(1-37), big ET-2_(1-38) and big ET-3 to their mature biologically active forms. The precise subcellular localization of this enzyme and its physiological relevance remains to be determined.