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血管紧张素转换酶(ACE)抑制剂的不良反应。

Adverse reactions with angiotensin converting enzyme (ACE) inhibitors.

作者信息

DiBianco R

出版信息

Med Toxicol. 1986 Mar-Apr;1(2):122-41. doi: 10.1007/BF03259832.

DOI:10.1007/BF03259832
PMID:3023783
Abstract

Teprotide, a nonapeptide isolated from the venom of a Brazilian pit viper, Bothrops jararaca, was the first angiotensin converting enzyme (ACE) inhibitor to be discovered and tested. It was found to be an effective, non-toxic antihypertensive agent as well as an afterload-reducing agent for patients with congestive heart failure (CHF). The primary activity of teprotide resulted from blockade of the angiotensin I converting enzyme--the pivotal step in the renin-angiotensin-aldosterone system (RAAS), and consequent reductions in angiotensin II levels. There was limited clinical testing for teprotide because of: its scarcity; the need for parenteral administration; and the subsequent discovery and synthesis of captopril, the first orally active angiotensin converting enzyme inhibitor. Captopril is the prototype oral angiotensin converting enzyme inhibitor and has been extensively studied since the initiation of formal studies in 1976. Perhaps one of the most closely researched drugs in modern times, the experience with captopril now includes more than 12,000 patients studied in formalized trials and over 4,000,000 patients treated world-wide by physicians for hypertension and congestive heart failure. Enalapril (MK421) is the first of what appears to be a growing number of analogues which are structurally and pharmacodynamically different from captopril; yet, they possess the same capacity for inhibiting the activity of angiotensin converting enzyme. The side effect profile of enalapril (and presumably future) angiotensin converting enzyme inhibitors appears to be similar to captopril, though clearly more experience is needed with newer agents. The initial use of captopril was troubled by a relatively high incidence of side effects which will form the focus of this discussion. Partially the result of incomplete pharmacokinetic information, captopril was administered in early studies at dosages now recognised to be far in excess of those necessary for drug action. In addition, dosages were given without regard for deficiencies of renal function, now known to be the main excretory route of captopril. The population of those patients studied frequently had chronic, treatment-resistant hypertension, often associated with concomitant end-organ disease (especially renal disease); and many additional factors further complicating the clinical setting, e.g. a relatively high incidence of collagen vascular disease and immunosuppressive treatments.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

替普罗肽是从巴西蝮蛇(Bothrops jararaca)毒液中分离出的一种九肽,是首个被发现并进行测试的血管紧张素转换酶(ACE)抑制剂。它被发现是一种有效的、无毒的抗高血压药物,也是用于充血性心力衰竭(CHF)患者的降低后负荷药物。替普罗肽的主要活性源于对血管紧张素I转换酶的阻断——这是肾素-血管紧张素-醛固酮系统(RAAS)中的关键步骤,并随之降低血管紧张素II水平。替普罗肽的临床试验有限,原因如下:其稀缺性;需要肠胃外给药;以及随后卡托普利的发现与合成,卡托普利是首个口服活性血管紧张素转换酶抑制剂。卡托普利是口服血管紧张素转换酶抑制剂的原型,自1976年开始正式研究以来已得到广泛研究。卡托普利或许是现代研究最深入的药物之一,目前其相关经验包括在正式试验中研究的超过12000名患者,以及全球范围内医生为治疗高血压和充血性心力衰竭而治疗的超过400万名患者。依那普利(MK421)是众多类似物中的首个,这些类似物在结构和药效学上与卡托普利不同;然而,它们具有相同的抑制血管紧张素转换酶活性的能力。依那普利(以及可能未来的)血管紧张素转换酶抑制剂的副作用谱似乎与卡托普利相似,不过显然对于新药物还需要更多经验。卡托普利最初的使用因相对较高的副作用发生率而受到困扰,这将成为本次讨论的焦点。部分原因是药代动力学信息不完整,在早期研究中卡托普利的给药剂量现在被认为远远超过药物作用所需剂量。此外,给药时没有考虑到肾功能不足,而现在已知肾功能是卡托普利的主要排泄途径。所研究的患者群体经常患有慢性、难治性高血压,通常伴有终末器官疾病(尤其是肾脏疾病);还有许多其他因素使临床情况更加复杂,例如胶原血管疾病的发生率相对较高以及免疫抑制治疗。(摘要截选至400字)

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本文引用的文献

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A BRADYKININ-POTENTIATING FACTOR (BPF) PRESENT IN THE VENOM OF BOTHROPS JARARCA.存在于矛头蝮蛇毒液中的一种缓激肽增强因子(BPF)。
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青蒿琥酯和卡托普利在体内外协同抑制血管生成。
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Lisinopril-induced isolated visceral angioedema: review of ACE-inhibitor-induced small bowel angioedema.赖诺普利引起的孤立性内脏血管性水肿:血管紧张素转换酶抑制剂引起的小肠血管性水肿综述
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ACE-inhibitor-induced cough, an adverse drug reaction unrecognised for several years: studies in prescription-event monitoring.血管紧张素转换酶抑制剂所致咳嗽,一种多年来未被认识的药物不良反应:处方事件监测研究
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ACE inhibitors. Drug interactions of clinical significance.血管紧张素转换酶抑制剂。具有临床意义的药物相互作用。
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Captopril in the management of hypertension with renal artery stenosis: its long-term effect as a predictor of surgical outcome.卡托普利在肾动脉狭窄性高血压治疗中的应用:其作为手术结果预测指标的长期效果
Am J Cardiol. 1982 Apr 21;49(6):1460-6. doi: 10.1016/0002-9149(82)90361-7.
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Effect of food on the bioavailability of captopril in healthy subjects.食物对健康受试者中卡托普利生物利用度的影响。
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Pityriasis rosea-like rash from captopril.卡托普利引起的玫瑰糠疹样皮疹。
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Transient anuria following administration of angiotensin I-converting enzyme inhibitor (SQ 14225) in a patient with renal artery stenosis of the solitary kidney successfully treated with renal autotransplantation.
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Drug therapy. Captopril.药物治疗。卡托普利。
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Fetal abnormality associated with the use of captopril during pregnancy.孕期使用卡托普利与胎儿异常相关。
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