Toxicity of antimony and its compounds.

K A Winship
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Abstract

Experimental and clinical experience with compounds containing antimony have shown that the trivalent compounds are generally more toxic than the pentavalent ones. APT can cause severe pain and tissue necrosis and is therefore not given by intramuscular or subcutaneous injection. APT has the actions and uses of AST, but it is less soluble and more irritating than the sodium salt which is therefore more suitable for intravenous use. Trivalent antimony compounds are toxic when used topically. Adverse effects are similar for all trivalent compounds, and include nausea, vomiting, weakness and myalgia, abdominal colic, diarrhoea, and skin rashes, including pustular eruptions. Hypersensitivity reactions also occur. Respiratory symptoms include cough, dyspnoea, and chronic lung changes. Cardiotoxicity is the most important and may produce arrhythmias, myocardial depression and damage, Stokes-Adams attacks, heart failure, and cardiac arrest. Hepatic damage and necrosis, as well as blood dyscrasias, may occur. Toxic effects on the kidney may follow chronic use. Continuous treatment with small doses of antimony may give rise to symptoms of subacute poisoning, similar to those of chronic arsenic poisoning, due to accumulation of antimony in the body, especially if trivalent compounds are used, because of their long biological half-lives. Reproductive disorders and chromosome damage have been reported; antimony compounds are, therefore, potentially toxic to reproduction and have mutagenic, and oncogenic potential. Antimony compounds should, therefore, not be used during pregnancy or in the presence of hepatic, renal, or heart disease. Pentavalent antimony preparations especially the organic compounds, together with non-metallic synthetic preparations, such as the diamidines, have now replaced APT for use in leishmaniasis. Because of the toxicity of antimony compounds, investigations have been undertaken to reduce their adverse effects by combining them with chelating agents. These preparations appear to have reduced the toxic effects of antimony without affecting the efficacy of the preparations. Liposome-encapsulated antimony products have, more recently, been shown to be much less toxic because of the reduced dose of the antimony compound required for effective therapy. The historical uses of antimony were based on the belief that the topical and systemic adverse effects, for example, skin eruptions and diarrhoea and vomiting, were signs that the condition being treated was responding by being brought to the surface to relieve congestion at the diseased area. There is no evidence in topical use, but there is evidence that such use can cause severe reactions.(ABSTRACT TRUNCATED AT 400 WORDS)

锑及其化合物的毒性。
含锑化合物的实验和临床经验表明,三价化合物通常比五价化合物毒性更大。APT可引起剧烈疼痛和组织坏死,因此不能通过肌内或皮下注射给予。APT具有AST的作用和用途,但它比钠盐可溶性更低,刺激性更强,因此更适合静脉注射。三价锑化合物局部使用时是有毒的。所有三价化合物的不良反应相似,包括恶心、呕吐、虚弱和肌痛、腹绞痛、腹泻和皮疹,包括脓疱疹。过敏反应也会发生。呼吸道症状包括咳嗽、呼吸困难和慢性肺部病变。心脏毒性是最重要的,可能导致心律失常、心肌抑制和损害、斯托克斯-亚当斯发作、心力衰竭和心脏骤停。可能发生肝损伤和坏死,以及血液紊乱。长期使用可能对肾脏产生毒性作用。持续用小剂量锑治疗可能引起亚急性中毒症状,类似于慢性砷中毒症状,这是由于锑在体内的积累,特别是如果使用三价化合物,因为它们的生物半衰期很长。生殖障碍和染色体损伤已被报道;因此,锑化合物对生殖有潜在毒性,并具有致突变和致癌的潜力。因此,在怀孕期间或存在肝、肾或心脏疾病时,不应使用锑化合物。五价锑制剂,特别是有机化合物,连同非金属合成制剂,如二胺类,现已取代APT用于利什曼病。由于锑化合物的毒性,已经进行了研究,通过将它们与螯合剂结合来减少它们的不良影响。这些制剂似乎降低了锑的毒性作用,而不影响制剂的功效。最近,由于有效治疗所需的锑化合物剂量减少,脂质体封装的锑产品毒性小得多。锑的历史用途是基于这样一种信念,即局部和全身的不良反应,例如皮肤爆发、腹泻和呕吐,是被治疗的病症通过被带到表面来缓解患病区域的充血而起作用的迹象。没有证据表明局部使用,但有证据表明这种使用会引起严重的反应。(摘要删节为400字)
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