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The roles of adenosine in regulating the respiratory and cardiovascular systems in chronically hypoxic, adult rats.

机译:腺苷在慢性缺氧成年大鼠调节呼吸和心血管系统中的作用。

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1. We have investigated the roles of adenosine in regulating the respiratory and cardiovascular systems of rats that were made chronically hypoxic for 3-4 weeks from 6 weeks of age (CH rats) in an hypoxic chamber at 12% O2. They were studied under anaesthesia while breathing 12% O2 and during acute hypoxia (breathing 8% O2 for 5 min) before and after addition of the adenosine receptor antagonist 8-phenyltheophylline (8-PT, 10 mg kg-1). The results were compared with those obtained from normoxic (N) rats in a previous study. 2. CH rats breathing 12% O2 had greater minute ventilation (VP) than N rats breathing air, but their levels of arterial blood pressure (ABP), heart rate (HR), femoral vascular conductance (FVC) and cerebral vascular conductance (CVC) were fully comparable. 8-PT increased tidal volume (VT) in CH rats indicating a greater tonic central inhibitory influence of adenosine on VT than in N rats. However, 8-PT had no effect on cardiovascular variables, indicating no tonic cardioinhibitory or vasodilator influence of adenosine in CH rats. 3. Acute hypoxia in CH rats increased VE such that at the 5th minute of 8% O2 absolute VE was comparable to that of N rats breathing 8% O2. Moreover, in CH rats 8-PT increased VT at the 5th minute of 8% O2 indicating that the central inhibitory influence of adenosine limits the ability to maintain VT in acute hypoxia as it does in N rats. 4. Eight per cent O2 also produced a full in ABP in CH rats that was comparable to that induced in N rats by the larger change from air to 8% O2. However, the changes in HR were similar in CH and N rats while the increases in FVC and CVC were smaller in CH rats. This suggests that the ability of the secondary effects of hyperventilation and of the baroreceptor reflex to maintain cardiac output and thereby ABP is reduced in CH rats. 5. Whereas 8-PT substantially reduced the hypoxia-induced increases in FVC and CVC in N rats, it had a small effect in CH rats (P = 0.054 and 0.06, respectively). Further, acute hypoxia in CH rats had no effect on the K+ concentration in the venous efflux of hindlimb K+ (KV+) before or after 8-PT treatment. We suggest that in CH rats, the dilator influence of adenosine in acute hypoxia occurs via actions on the blood vessel walls: there was no evidence that adenosine can release dilator concentrations of K+ from skeletal muscle fibres in CH rats as proposed for N rats.
机译:1.我们研究了腺苷在调节从6周龄开始慢性缺氧3-4周的大鼠(CH大鼠)在12%O2的低氧室内对腺苷酸的调节作用。在添加腺苷受体拮抗剂8-phenyltheophylline(8-PT,10 mg kg-1)之前和之后,在麻醉期间分别呼吸12%O2和急性缺氧(呼吸8%O2 5分钟)进行研究。将结果与先前研究中从常氧(N)大鼠获得的结果进行比较。 2.吸入12%O2的CH大鼠的分钟通气量(VP)大于N呼吸空气的分钟通气量,但它们的动脉血压(ABP),心率(HR),股血管电导(FVC)和脑血管电导(CVC) )完全可比。 CH大鼠的8-PT潮气量(VT)增加,表明腺苷对VT的强直中枢抑制作用比N大鼠更大。但是,8-PT对心血管变量无影响,表明腺苷对CH大鼠无强直性心脏抑制或血管扩张作用。 3. CH大鼠的急性缺氧增加了VE,因此在5%O2的第5分钟时,绝对VE与呼吸8%O2的N只大鼠相当。此外,在CH大鼠中,8-PT在5%O2的第5分钟增加了VT,这表明腺苷的中央抑制作用限制了急性缺氧时VT的维持能力,就像N大鼠一样。 4. 8%的O2还在CH大鼠中产生了完全的ABP,这与N大鼠中从空气到8%的较大变化相比可产生的ABP完全相同。但是,CH和N大鼠的HR变化相似,而CH大鼠的FVC和CVC升高较小。这表明在CH大鼠中,过度换气和压力感受器反射的继发作用维持心排血并由此维持ABP的能力降低。 5.尽管8-PT实质上减少了缺氧诱导的N大鼠FVC和CVC升高,但对CH大鼠的影响很小(分别为P = 0.054和0.06)。此外,CH大鼠的急性缺氧对8-PT治疗之前或之后的后肢K +(KV +)的静脉外排中K +浓度没有影响。我们建议在CH大鼠中,腺苷在急性低氧中的扩张作用是通过对血管壁的作用而发生的:没有证据表明腺苷可以像在N大鼠中那样从CH大鼠骨骼肌纤维中释放K +的扩张剂浓度。

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