Department of Pharmacology, East Tennessee State University, Johnson City, TN, United States.
Auton Neurosci. 2012 Jul 2;169(1):34-42. doi: 10.1016/j.autneu.2012.03.003. Epub 2012 Apr 11.
To evaluate whether cervical spinal neurons can influence cardiac indices and myocyte viability in the acutely ischemic heart, the hearts of anesthetized rabbits subjected to 30 min of LAD coronary arterial occlusion (CAO) were studied 3h after reperfusion. Control animals were compared to those exposed to pre-emptive high cervical cord stimulation (SCS; the dorsal aspect of the C1-C2 spinal cord was stimulated electrically at 50 Hz; 0.2 ms; 90% of motor threshold, starting 15 min prior to and continuing throughout CAO). Four groups of animals were so tested: 1) neuroaxis intact; 2) prior cervical vagotomy; 3) prior transection of the dorsal spinal columns at C6; and 4) following pharmacological treatment [muscarinic (atropine) or adrenergic (atenolol, prazosin or yohimbine) receptor blockade]. Infarct size (IS) was measured by tetrazolium, expressed as percentage of risk zone. C1-C2 SCS reduced acute ischemia induced IS by 43%, without changing the incidence of sudden cardiac death (SCD). While SCS-induced reduction in IS was unaffected by vagotomy, it was no longer evident following transection of C6 dorsal columns or atropinization. Beta-adrenoceptor blockade eliminated ischemia induced SCD, while alpha-receptor blockade doubled its incidence. During SCS, myocardial ischemia induced SCD was eliminated following vagotomy while remaining unaffected by atropinization. These data indicate that, in contrast to thoracic spinal neurons, i) cranial cervical spinal neurons affect both adrenergic and cholinergic motor outflows to the heart such that ii) their activation modifies ventricular infarct size and lethal arrhythmogenesis.
为了评估颈脊髓神经元是否会影响急性缺血心脏的心脏指数和心肌细胞活力,对麻醉兔的心脏进行了研究,这些兔子在左前降支冠状动脉闭塞(CAO)30 分钟后进行了再灌注。将对照动物与预先进行高颈脊髓刺激(SCS;在 C1-C2 脊髓的背侧以 50Hz、0.2ms、90%运动阈进行电刺激,在 CAO 之前 15 分钟开始并持续进行)的动物进行比较。对四组动物进行了测试:1)完整的神经轴;2)预先进行颈迷走神经切断术;3)C6 处的背侧脊髓柱横断;4)进行药物治疗[毒蕈碱(阿托品)或肾上腺素能(阿替洛尔、普萘洛尔或育亨宾)受体阻断]。通过四唑盐测量梗塞面积(IS),表示为危险区的百分比。C1-C2 SCS 将急性缺血引起的 IS 减少了 43%,而不改变心脏性猝死(SCD)的发生率。虽然 SCS 诱导的 IS 减少不受迷走神经切断术的影响,但在 C6 背侧柱横断或阿托品化后,这种影响不再明显。β-肾上腺素能受体阻断消除了缺血诱导的 SCD,而α-受体阻断使 SCD 的发生率增加了一倍。在 SCS 期间,迷走神经切断术后,心肌缺血诱导的 SCD 消除了,而阿托品化对其没有影响。这些数据表明,与胸段脊髓神经元不同,i)颅颈脊髓神经元影响到心脏的肾上腺素能和胆碱能运动输出,ii)它们的激活改变了心室梗塞面积和致命性心律失常的发生。