Hudlická O, Garnham A, Shiner R, Egginton S
Department of Physiology, University of Birmingham Medical School, Birmingham, UK.
J Physiol. 2008 Oct 15;586(20):4961-75. doi: 10.1113/jphysiol.2008.158055. Epub 2008 Aug 28.
Acute ischaemia-reperfusion disrupts capillary fine structure and increases leukocyte adhesion in postcapillary venules. We determined whether chronic muscle ischaemia has similar consequences, and whether it is possible to ameliorate its effect on muscle performance. Following ischaemia (unilateral ligation, common iliac artery) rat hindlimb muscles were examined without other intervention or following treatment with an xanthine oxidase inhibitor (allopurinol), a Na(+)/H(+) exchange blocker (amiloride), or an oxygen free radical scavenger (vitamin E). No significant leukocyte adhesion or rolling, nor changes in capillary fine structure were observed 3 days postsurgery, when limb use was limited. However, leukocyte rolling and adhesion almost trebled by 7 days (P < 0.001), when normal gait was largely restored. Capillary fine structure was disturbed over a similar time course, e.g. relative endothelial volume (control 46%, 7 days 61%; P < 0.05), that resolved by 5 weeks. Where activity was increased by mild electrical stimulation 3 days after ligation muscles showed enhanced capillary swelling (endothelial volume 66% versus 50%, P < 0.005), but improved fatigue index (52% versus 16%, P < 0.001) as a result of greater blood flow. Muscle fatigue after ligation was related to the extent of contraction-induced hyperaemia (R(2) = 0.725), but not capillary swelling. Amiloride, and to a lesser extent allopurinol but not vitamin E, significantly decreased leukocyte rolling and adhesion, as well as capillary endothelial swelling. We conclude that increased activity of ischaemic muscles on recovery is likely to accentuate acidosis accompanying changes in microcirculation and contribute to enhanced muscle fatigue, whereas formation of oxygen free radicals may be attenuated by endogenous protective mechanisms.
急性缺血再灌注会破坏毛细血管的精细结构,并增加毛细血管后微静脉中的白细胞黏附。我们确定慢性肌肉缺血是否有类似后果,以及是否有可能改善其对肌肉性能的影响。在缺血(单侧结扎,髂总动脉)后,对大鼠后肢肌肉进行检查,未进行其他干预,或用黄嘌呤氧化酶抑制剂(别嘌呤醇)、钠/氢交换阻滞剂(阿米洛利)或氧自由基清除剂(维生素E)进行治疗。在术后3天,当肢体活动受限时,未观察到明显的白细胞黏附或滚动,也未观察到毛细血管精细结构的变化。然而,在术后7天,当正常步态基本恢复时,白细胞滚动和黏附几乎增加了两倍(P<0.001)。毛细血管精细结构在类似的时间进程中受到干扰,例如相对内皮体积(对照组46%,7天61%;P<0.05),在5周时恢复。在结扎后3天通过轻度电刺激增加活动的情况下,肌肉显示出毛细血管肿胀增强(内皮体积66%对50%,P<0.005),但由于血流量增加,疲劳指数得到改善(52%对16%,P<0.001)。结扎后肌肉疲劳与收缩诱导的充血程度有关(R²=0.725),但与毛细血管肿胀无关。阿米洛利以及在较小程度上别嘌呤醇而非维生素E,显著降低了白细胞滚动和黏附以及毛细血管内皮肿胀。我们得出结论,缺血肌肉恢复时活动增加可能会加剧伴随微循环变化的酸中毒,并导致肌肉疲劳增强,而氧自由基的形成可能会被内源性保护机制减弱。