Bartlett Iain S, Marshall Janice M
Department of Physiology, The Medical School, University of Birmingham, Birmingham B15 2TT, UK.
Exp Physiol. 2002 Mar;87(2):171-84. doi: 10.1113/eph8702341.
In rings of rat iliac artery, contractions were evoked by noradrenaline (NA), the selective alpha(1) adrenoceptor agonist phenylephrine (PE), and K(+), which causes depolarisation-induced contraction. There was no evidence of alpha(2) adrenoceptor-evoked contraction. Hypoxia, induced by reducing P(O(2)) in the bath from 100 mmHg to 70, 55 or 40 mmHg, had similar effects on rings with (E+) and without (E-) endothelium. In E- rings, the NA concentration-response curve was biphasic, whereas that for PE was monophasic. Hypoxia reduced maximum contractions in response to NA and PE (NA(max) and PE(max), respectively) without affecting the concentrations that evoked 50 % of maximum contraction (EC(50)). At P(O(2)) of 70 mmHg, NA(max) of the high affinity alpha(1) receptor for NA (NA(maxh)) and PE(max) were reduced by approximately 15 %, but at P(O(2)) of 55 and 40 mmHg, NA(maxh) was severely attenuated while PE(max) fell by 45 and 75 %, respectively. Similarly, the Ca(2+) channel blocker nicardipine depressed NA(maxh) and PE(max), but P(O(2)) of 55 mmHg further reduced NA(max) and PE(max). Hypoxia also reduced contractions evoked by NA, PE or K(+) at the concentrations required to produce 80 % of the maximum contraction (EC(80)), receptor-mediated contractions being more affected. Ca(2+)-free conditions reduced the contractions evoked by NA and PE, at the EC(80), to approximately 10 % of control. The K(+) channel inhibitors glibenclamide and tetraethylammonium did not prevent hypoxia-induced depression of PE-evoked contraction. Thus, contractions evoked in iliac artery by the high affinity subtype of alpha(1) adrenoceptor for NA, which may respond to circulating levels of NA, and by the single alpha(1) adrenoceptor subtype for PE, are especially vulnerable to P(O(2)) levels less-than-or-equal 55 mmHg. We propose that this reflects hypoxia-induced inhibition of Ca(2+) influx through L-type and receptor-operated Ca(2+) channels; K(+) channel opening makes little contribution.
在大鼠髂动脉环中,去甲肾上腺素(NA)、选择性α(1)肾上腺素能受体激动剂苯肾上腺素(PE)以及可引起去极化诱导收缩的K⁺均可诱发收缩。没有证据表明存在α(2)肾上腺素能受体诱发的收缩。通过将浴槽中的P(O₂)从100 mmHg降至70、55或40 mmHg诱导的缺氧,对有内皮(E+)和无内皮(E-)的血管环有相似的影响。在E-血管环中,NA浓度-反应曲线呈双相,而PE的曲线呈单相。缺氧降低了对NA和PE的最大收缩反应(分别为NA(max)和PE(max)),但不影响引起50%最大收缩的浓度(EC(50))。在P(O₂)为70 mmHg时,NA高亲和力α(1)受体的NA(max)(NA(maxh))和PE(max)降低了约15%,但在P(O₂)为55和40 mmHg时,NA(maxh)严重减弱,而PE(max)分别下降了45%和75%。同样,钙通道阻滞剂尼卡地平降低了NA(maxh)和PE(max),但55 mmHg的P(O₂)进一步降低了NA(max)和PE(max)。缺氧还降低了在产生80%最大收缩所需浓度(EC(80))下由NA、PE或K⁺诱发的收缩,受体介导的收缩受影响更大。无钙条件下,在EC(80)时,NA和PE诱发的收缩降至对照的约10%。钾通道抑制剂格列本脲和四乙铵不能阻止缺氧诱导的PE诱发收缩的抑制。因此,NA的高亲和力α(1)肾上腺素能受体亚型(可能对循环中的NA水平有反应)以及PE的单一α(1)肾上腺素能受体亚型在髂动脉中诱发的收缩,对小于或等于55 mmHg的P(O₂)水平特别敏感。我们认为,这反映了缺氧诱导的通过L型和受体操纵性钙通道的钙内流抑制;钾通道开放的作用不大。
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