Prieto D, García-Sacristán A, Simonsen U
Departamento de Fisiologia, Facultad de Veterinaria, Universidad Complutense, Madrid, Spain.
Regul Pept. 1998 Sep 25;75-76:155-60. doi: 10.1016/s0167-0115(98)00063-9.
In vitro experiments in a microvascular myograph were designed in order to characterize the receptor subtypes and the mechanisms underlying the contractions induced by neuropeptide Y (NPY) in rat coronary small arteries. The rank order of potency for NPY-receptor agonist-induced increases in tension in endothelium-intact preparations was polypeptide Y (PYY)> NPY > or = [Leu31Pro34]NPY, while NPY(13-36) only induced small contractions at the highest concentration applied. The selective neuropeptide Y1 receptor antagonist, BIBP 3226, caused rightward shifts in the concentration-response curves for NPY and the slope of the Schild plot was not significantly different from unity. The pA2 value for BIBP 3226 against NPY was 7.88+/-0.15 (n = 6). We have earlier shown that endothelial cell removal does not change the contractile responses induced by NPY, but indomethacin (3 x 10(-6) M) significantly reduced the contractions induced by the peptide. In contrast, the thromboxane receptor antagonist, SQ29548, which abolished the contractions induced by the thromboxane analogue, U46619, did not change the concentration-response curves for NPY. In conclusion, the present study suggests that Y1 receptors mediate NPY-induced contractions in rat coronary resistance arteries, and that a non-thromboxane prostanoid is involved in the contractile mechanism.
为了确定大鼠冠状动脉小动脉中神经肽 Y(NPY)诱导收缩的受体亚型及潜在机制,我们设计了微血管肌动描记器的体外实验。在内皮完整的标本中,NPY 受体激动剂诱导张力增加的效力排序为多肽 Y(PYY)> NPY > 或 = [Leu31Pro34]NPY,而 NPY(13 - 36)仅在应用的最高浓度时诱导微小收缩。选择性神经肽 Y1 受体拮抗剂 BIBP 3226 使 NPY 的浓度 - 反应曲线右移,且 Schild 图的斜率与 1 无显著差异。BIBP 3226 对 NPY 的 pA2 值为 7.88 ± 0.15(n = 6)。我们先前已表明,去除内皮细胞不会改变 NPY 诱导的收缩反应,但吲哚美辛(3×10⁻⁶ M)显著降低了该肽诱导的收缩。相反,血栓素受体拮抗剂 SQ29548 消除了血栓素类似物 U46619 诱导的收缩,但并未改变 NPY 的浓度 - 反应曲线。总之,本研究表明 Y1 受体介导大鼠冠状动脉阻力动脉中 NPY 诱导的收缩,且一种非血栓素类前列腺素参与了收缩机制。
