Angiotensin II Type 1 and 2 Receptors in Conduit Arteries of Normal Developing Microswine

S. Bagby, Linda S. LeBard, Zaiming Luo, R. Speth, B. Ogden, C. Corless
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引用次数: 16

Abstract

Objective—To identify vascular cells capable of responding to angiotensin II (Ang II) generated in conduit arteries, we examined the Ang II type 1 receptor (AT1R) and Ang II type 2 receptor (AT2R) in the thoracic aorta (TA) and abdominal aorta (AA) and branches in 90-day fetal, 3-week postnatal, and 6-month adult microswine. Methods and Results—By autoradiography (125I-[Sar1Ile8]-Ang II with or without AT1R- or AT2R-selective analogues or 125I - CGP 42112), there were striking rostrocaudal differences in (1) AT2R binding at all ages (prominent in AA wall and branches, sparse in TA wall and branches) and (2) a non-AT2R binding site for CGP 42112 (consistently evident in postnatal TA and branches but absent in AA and branches). Furthermore, patterns of AT2R distribution in infradiaphragmatic arteries were developmentally distinct. In fetal AAs, high-density AT2Rs occupied the inner 60% of the medial-endothelial wall. In postnatal AAs, AT2Rs were sparse in the medial-endothelial wall but prominent in a circumferential smooth muscle &agr;-actin–negative cell layer at the medial-adventitial border, occupying ≈20% to 25% of the AA cross-sectional area. AT1R density in the TA and AA medial-endothelial wall increased with age, whereas AT2R density decreased after birth. Conclusions—A novel AT2R-positive cell layer confined to postnatal infradiaphragmatic arteries physically links adventitial and medial layers, appears optimally positioned to transduce AT2R-dependent functions of local Ang II, and suggests that adventitial Ang II may elicit regionally distinct vascular responses.
正常发育微猪导管动脉血管紧张素II型1和2型受体
目的:为了鉴定能够对导管动脉血管紧张素II (Ang II)产生反应的血管细胞,我们检测了90天胎儿、出生后3周和6个月成年微猪胸主动脉(TA)和腹主动脉(AA)及其分支中的Ang II 1型受体(AT1R)和Ang II 2型受体(AT2R)。方法和结果:通过放射自显影(125I-[Sar1Ile8]- ang II伴或不伴AT1R或AT2R选择性类似物或125I- CGP 42112),发现(1)AT2R结合在所有年龄段(在AA壁和分支中突出,在TA壁和分支中稀疏)和(2)CGP 42112的非AT2R结合位点(在出生后的TA和分支中一致明显,但在AA和分支中不存在)存在显著的直立性差异。此外,AT2R在膈下动脉的分布模式在发育过程中是不同的。在胎儿AAs中,高密度的AT2Rs占据了内内皮壁的60%。在出生后的AAs中,AT2Rs在内侧内皮壁稀疏,但在内侧外边界的平滑肌-肌动蛋白阴性细胞层中突出,占AA横截面面积的约20%至25%。TA和AA内侧内皮壁的AT1R密度随年龄增长而增加,而出生后AT2R密度下降。结论:一种新的at2r阳性细胞层局限于出生后的膈下动脉,将外膜层和内膜层物理连接起来,似乎是传导at2r依赖局部Ang II功能的最佳位置,并表明外膜Ang II可能引发区域不同的血管反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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