Dua Ashok K, Dua Nickesh, Murrant Coral L
Department of Human Health and Nutritional Science, University of Guelph, Guelph, Ontario, Canada.
Am J Physiol Heart Circ Physiol. 2009 Jul;297(1):H433-42. doi: 10.1152/ajpheart.00216.2009. Epub 2009 May 22.
To test the hypothesis that the vasodilator complement that produces arteriolar vasodilation during muscle contraction depends on both stimulus and contraction frequency, we stimulated four to five skeletal muscle fibers in the anesthetized hamster cremaster preparation in situ and measured the change in diameter of arterioles at a site of overlap with the stimulated muscle fibers. Diameter was measured before, during, and after 2 min of skeletal muscle contraction stimulated over a range of stimulus frequencies [4, 20, and 40 Hz; 15 contractions/min (cpm), 250 ms train duration] and a range of contraction frequencies (6, 15, and 60 cpm; 20 Hz stimulus frequency, 250 ms train duration). Muscle fibers were stimulated in the absence and presence of an inhibitor of adenosine receptors [10(-6) M xanthine amine congener (XAC)], an ATP-dependent potassium (K(+)) channel inhibitor (10(-5) M glibenclamide), an inhibitor of a source of K(+) by inhibition of voltage-dependent K(+) channels [3 x 10(-4) M 3,4-diaminopyridine (DAP)], and an inhibitor of nitric oxide synthase [10(-6) M N(G)-nitro-l-arginine methyl ester (l-NAME) + 10(-7) S-nitroso-N-acetylpenicillamine (a nitric oxide donor)]. L-NAME inhibited the dilations at all stimulus frequencies and contraction frequencies except 60 cpm. XAC inhibited the dilations at all contraction frequencies and stimulus frequencies except 40 Hz. Glibenclamide inhibited all dilations at all stimulus and contraction frequencies, and DAP did not inhibit dilations at any stimulus frequencies while attenuating dilation at a contraction frequency of 60 cpm only. Our data show that the complement of dilators responsible for the vasodilations induced by skeletal muscle contraction differed depending on the stimulus and contraction frequency; therefore, both are important determinants of the dilators involved in the processes of arteriolar vasodilation associated with active hyperemia.
为了验证肌肉收缩期间产生小动脉血管舒张的血管舒张成分取决于刺激和收缩频率这一假设,我们在麻醉的仓鼠提睾肌原位制备中刺激四到五条骨骼肌纤维,并测量与受刺激肌肉纤维重叠部位小动脉直径的变化。在一系列刺激频率[4、20和40Hz;15次收缩/分钟(cpm),250ms串刺激持续时间]和一系列收缩频率(6、15和60cpm;20Hz刺激频率,250ms串刺激持续时间)下刺激骨骼肌收缩2分钟,分别在收缩前、收缩期间和收缩后测量小动脉直径。在存在和不存在腺苷受体抑制剂[10(-6)M黄嘌呤胺同类物(XAC)]、ATP依赖性钾(K(+))通道抑制剂(10(-5)M格列本脲)、通过抑制电压依赖性K(+)通道抑制K(+)来源的抑制剂[3×10(-4)M 3,4-二氨基吡啶(DAP)]以及一氧化氮合酶抑制剂[10(-6)M N(G)-硝基-L-精氨酸甲酯(L-NAME)+10(-7)S-亚硝基-N-乙酰青霉胺(一氧化氮供体)]的情况下刺激肌肉纤维。L-NAME除了在60cpm时外,在所有刺激频率和收缩频率下均抑制血管舒张。XAC除了在40Hz时外,在所有收缩频率和刺激频率下均抑制血管舒张。格列本脲在所有刺激和收缩频率下均抑制所有血管舒张,而DAP在任何刺激频率下均不抑制血管舒张,仅在收缩频率为60cpm时减弱血管舒张。我们的数据表明,负责骨骼肌收缩诱导的血管舒张的舒张成分因刺激和收缩频率而异;因此,两者都是参与与活跃性充血相关的小动脉血管舒张过程的舒张因子的重要决定因素。
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