Rendell M S, Shehan M A, Kahler K, Bailey K L, Eckermann A J
Creighton Diabetes Center, Omaha, Nebraska, USA.
Angiology. 1997 Mar;48(3):203-13. doi: 10.1177/000331979704800302.
In previous studies, using laser Doppler techniques, the authors have demonstrated a duration-dependent reduction in skin blood flow reserve at sites of nutritive (NUTR) perfusion that occurs in diabetes and correlates with the presence of diabetic retinopathy and proteinuria. They speculated that it might be possible to reverse this decrease in blood flow by using agents with peripheral vasodilating properties. They chose the calcium channel blocking agent isradipine as a prototype. As a contrast agent, they chose atenolol, which has an equivalent antihypertensive effect but minimal peripheral vasodilating properties. They studied 24 diabetic hypertensive patients in a randomized, two-way crossover design. They assigned patients randomly to one or the other active drug and titrated to a maximum tolerated maintenance dose. Skin blood flow was measured at the end of the titration and maintenance phases. Patients then entered a four-week washout period, followed by crossover to the alternative drug, and measurements were repeated. At baseline, the twenty-four-hour mean ambulatory systolic blood pressure was 150 +/- 2 mm Hg with a twenty-four-hour mean diastolic blood pressure of 93 +/- 1 mm Hg. Thermally stimulated skin blood flow reserve was about 50% lower in these patients as compared with an age-, sex-, and weight-matched group of 28 nondiabetic, nonhypertensive patients. There was no difference in skin blood flow between the two groups at basal skin temperature or at a controlled temperature of 35 degrees C. Both atenolol and isradipine successfully lowered blood pressure in the study patients. There was a slightly greater decrease in systolic blood pressure with isradipine and a greater decrease in heart rate with atenolol. Neither isradipine nor atenolol treatment affected skin blood flow values at the maximal 44 degrees C temperature. However, at basal skin temperature and at 35 degrees C, isradipine-treated patients had substantial increases in skin blood flow at NUTR sites. For example, skin blood flow at the knee at 35 degrees C with isradipine treatment was 3.1 +/- 0.4 mL/min/100 g compared with 1.1 +/- 0.2 with atenolol, 1.3 +/- 0.1 with placebo, and 0.9 +/- 0.1 for the nondiabetic controls (all P < 0.01). The authors found a twofold to threefold increase in basal skin blood flow at NUTR sites with isradipine treatment. This degree of increase is substantially greater than that previously demonstrated by their group using pentoxifylline. Locally reduced skin blood flow is a factor in promoting skin breakdown and delayed healing. Further study is needed to explore the possibility that isradipine treatment may enhance healing of diabetic skin ulcers.
在以往的研究中,作者使用激光多普勒技术,在糖尿病患者营养性(NUTR)灌注部位证实了皮肤血流储备随病程延长而减少,这种减少与糖尿病视网膜病变和蛋白尿的存在相关。他们推测,使用具有外周血管舒张特性的药物可能逆转这种血流减少的情况。他们选择钙通道阻滞剂伊拉地平作为原型药物。作为对照药物,他们选择了阿替洛尔,其具有同等的降压效果,但外周血管舒张特性极小。他们采用随机、双向交叉设计对24例糖尿病高血压患者进行了研究。将患者随机分配至两种活性药物中的一种,并滴定至最大耐受维持剂量。在滴定期和维持期结束时测量皮肤血流。然后患者进入为期四周的洗脱期,之后交叉使用另一种药物,并重复测量。基线时,24小时平均动态收缩压为150±2 mmHg,24小时平均动态舒张压为93±1 mmHg。与28例年龄、性别和体重匹配的非糖尿病、非高血压患者相比,这些患者热刺激后的皮肤血流储备降低了约50%。在基础皮肤温度或35℃的受控温度下,两组之间的皮肤血流无差异。阿替洛尔和伊拉地平均成功降低了研究患者的血压。伊拉地平使收缩压降低幅度略大,阿替洛尔使心率降低幅度更大。伊拉地平和阿替洛尔治疗均未影响44℃最高温度时的皮肤血流值。然而,在基础皮肤温度和35℃时,伊拉地平治疗的患者在NUTR部位的皮肤血流有显著增加。例如,在35℃时,伊拉地平治疗的患者膝部皮肤血流为3.1±0.4 mL/min/100 g,而阿替洛尔治疗者为1.1±0.2 mL/min/100 g,安慰剂组为1.3±0.1 mL/min/100 g,非糖尿病对照组为0.9±0.1 mL/min/100 g(所有P<0.01)。作者发现伊拉地平治疗使NUTR部位的基础皮肤血流增加了2至3倍。这种增加程度明显大于他们的研究小组先前使用己酮可可碱所证实的程度。局部皮肤血流减少是促进皮肤破损和愈合延迟的一个因素。需要进一步研究以探索伊拉地平治疗可能促进糖尿病皮肤溃疡愈合的可能性。
