Westlin W, Mullane K
Department of Pharmacology, New York Medical College, Valhalla.
Circulation. 1988 Jun;77(6 Pt 2):I30-9.
The abilities of angiotensin converting-enzyme (ACE) inhibitors to suppress superoxide anion formation in vitro and to improve postischemic cardiac function in vivo were examined. Three sulfhydryl-containing ACE inhibitors, captopril, its stereoisomer SQ 14,534, and an analog, zofenopril (SQ 26,703) were compared with enalaprilat and teprotide, which lack the sulfhydryl group but inhibit ACE, and two compounds, N-2-mercaptopropionylglycine (MPG) and N-acetylcysteine (NAC), which contain a thiol moiety but are not ACE inhibitors, for suppression of free radical formation in vitro. The autooxidation of epinephrine to adrenochrome is mediated by superoxide anions and inhibited by captopril, SQ 14,534, and zofenopril, with similar IC50 values of 8 to 10 microM, but not by enalaprilat or teprotide (IC50 greater than 1000 microM). This reaction is also inhibited by MPG and NAC with IC50 values of 19 and 17 microM, respectively. In addition, captopril, MPG, or NAC, but not teprotide or enalaprilat, scavenge superoxide anion production by the purine-xanthine oxidase reaction and by canine neutrophils activated with phorbol myristate acetate. These results indicate that captopril scavenges superoxide anions in vitro independent of an action on ACE, which is probably related to the presence of a sulfhydryl moiety. Myocardial segmental function in the anesthetized, open-chest dog is altered during ischemia from active shortening to passive lengthening. Reperfusion after 15 min of ischemia does not restore active shortening within a 3 hr experimental period. Pretreatment of dogs with captopril intravenously (5 mg/kg) results in a 40% to 60% return to active shortening within 60 min of reperfusion. In contrast, equihypotensive doses of enalaprilat do not improve segmental function during reperfusion. Dogs given captopril immediately before restoring coronary blood flow show a similar return of function as that observed in animals treated with the drug before occlusion. SQ 14,534, the isomer of captopril, which is 100-fold less potent as an ACE inhibitor but equipotent in scavenging superoxide anions, also improves reperfusion-induced cardiac dysfunction when administered at reperfusion (5 mg/kg). Thus captopril improves postischemic contractile derangements by a mechanism independent of ACE inhibition. Restoration of blood supply to the ischemic myocardium provokes ventricular fibrillation in 37.5% of control dogs but in only 9% of those administered enalaprilat and 0% of captopril-treated animals. SQ 14,534 does not reduce the incidence of ventricular fibrillation (40%), indicating that the antifibrillatory actions may be related to ACE inhibition.(ABSTRACT TRUNCATED AT 400 WORDS)
研究了血管紧张素转换酶(ACE)抑制剂在体外抑制超氧阴离子形成以及在体内改善缺血后心脏功能的能力。将三种含巯基的ACE抑制剂卡托普利、其立体异构体SQ 14,534和类似物佐芬普利(SQ 26,703)与不含巯基但能抑制ACE的依那普利拉和替普罗肽进行比较,并将两种含有硫醇部分但不是ACE抑制剂的化合物N-2-巯基丙酰甘氨酸(MPG)和N-乙酰半胱氨酸(NAC)用于体外抑制自由基形成。肾上腺素自氧化生成肾上腺色素的过程由超氧阴离子介导,卡托普利、SQ 14,534和佐芬普利可抑制该过程,其半数抑制浓度(IC50)相似,为8至10微摩尔/升,但依那普利拉或替普罗肽无此作用(IC50大于1000微摩尔/升)。该反应也被MPG和NAC抑制,IC50分别为19和17微摩尔/升。此外,卡托普利、MPG或NAC可清除嘌呤 - 黄嘌呤氧化酶反应以及佛波酯肉豆蔻酸酯激活的犬中性粒细胞产生的超氧阴离子,而替普罗肽或依那普利拉则无此作用。这些结果表明,卡托普利在体外清除超氧阴离子的作用独立于其对ACE的作用,这可能与巯基部分的存在有关。在麻醉、开胸犬中,缺血期间心肌节段功能从主动收缩转变为被动拉长。缺血15分钟后再灌注,在3小时的实验期内不能恢复主动收缩。静脉注射卡托普利(5毫克/千克)预处理犬,在再灌注60分钟内可使40%至60%的心肌恢复主动收缩。相比之下,等降压剂量的依那普利拉在再灌注期间不能改善节段功能。在恢复冠状动脉血流前立即给予卡托普利的犬,其功能恢复情况与闭塞前用药的动物相似。卡托普利的异构体SQ 14,534作为ACE抑制剂的效力低100倍,但清除超氧阴离子的能力相当,在再灌注时给予(5毫克/千克)也可改善再灌注诱导的心脏功能障碍。因此,卡托普利通过独立于ACE抑制的机制改善缺血后收缩紊乱。恢复缺血心肌的血液供应会使37.5%的对照犬发生心室颤动,但依那普利拉处理的犬中仅9%发生,卡托普利处理的动物中无此情况。SQ 14,534不能降低心室颤动的发生率(40%),表明抗颤动作用可能与ACE抑制有关。(摘要截短至400字)
