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用于保护人类免受有机磷毒性侵害的生物清除剂。

Bioscavengers for the protection of humans against organophosphate toxicity.

作者信息

Doctor Bhupendra P, Saxena Ashima

机构信息

Division of Biochemistry, Walter Reed Army Institute of Research, 503 Robert Grant Road, Silver Spring, MD 20910, USA.

出版信息

Chem Biol Interact. 2005 Dec 15;157-158:167-71. doi: 10.1016/j.cbi.2005.10.024. Epub 2005 Nov 15.

Abstract

Current antidotes for organophosphorus compounds (OP) poisoning consist of a combination of pretreatment with carbamates (pyridostigmine bromide), to protect acetylcholinesterase (AChE) from irreversible inhibition by OP compounds, and post-exposure therapy with anti-cholinergic drugs (atropine sulfate) to counteract the effects of excess acetylcholine and oximes (e.g., 2-PAM chloride) to reactivate OP-inhibited AChE. These antidotes are effective in preventing lethality from OP poisoning, but they do not prevent post-exposure incapacitation, convulsions, seizures, performance decrements, or in many cases permanent brain damage. These symptoms are commonly observed in experimental animals and are likely to occur in humans. The problems intrinsic to these antidotes stimulated attempts to develop a single protective drug, itself devoid of pharmacological effects, which would provide protection against the lethality of OP compounds and prevent post-exposure incapacitation. One approach is the use of enzymes such as cholinesterases (ChEs), beta-esterases in general, as single pretreatment drugs to sequester highly toxic OP anti-ChEs before they reach their physiological targets. This approach turns the irreversible nature of the OP: ChE interaction from disadvantage to an advantage; instead of focusing on OP as an anti-ChE, one can use ChE as an anti-OP. Using this approach, it was shown that administration of fetal bovine serum AChE (FBSAChE) or equine serum butyrylcholinesterase (EqBChE) or human serum BChE (HuBChE) protected the animals from multiple LD50s of a variety of highly toxic OPs without any toxic effects or performance decrements. The bioscavengers that have been explored to date for the detoxification of OPs fall into three categories: (A) those that can catalytically hydrolyze OPs and thus render them non-toxic, such as OP hydrolase and OP anhydrase; (B) those that stoichiometrically bind to OPs, that is, 1 mol of enzyme neutralizes one or 2 mol of OP inactivating both, such as ChEs and related enzymes; and (C) and those generally termed as "pseudo catalytic", e.g., a combination of ChE and an oxime pre-treatment such that the catalytic activity of OP-inhibited ChE can rapidly and continuously be restored in the presence of an oxime. Since the biochemical mechanism underlying prophylaxis by exogenous esterases such as ChEs is established and tested in several animal species, including non-human primates, this concept should allow a reliable extrapolation of results from animal experiments to human application. Having being extensively investigated by several groups, plasma derived HuBChE is judged to be the most suitable bioscavenger for its advancement for human use. The program is being developed at the present time for conducting a safety clinical trial in human volunteers. Several other candidate bioscavengers will follow; e.g., recombinant HuBChE expressed in the milk of transgenic goats, pseudo catalytic scavenger(s), e.g., a combination of ChE and oxime, and possibly PON 1 as a catalytic scavenger in the future.

摘要

目前用于有机磷化合物(OP)中毒的解毒剂包括用氨基甲酸盐(溴吡斯的明)进行预处理,以保护乙酰胆碱酯酶(AChE)免受OP化合物的不可逆抑制,以及暴露后用抗胆碱能药物(硫酸阿托品)进行治疗,以对抗过量乙酰胆碱的作用,并用肟类药物(如氯解磷定)使被OP抑制的AChE重新活化。这些解毒剂在预防OP中毒致死方面有效,但不能预防暴露后失能、惊厥、癫痫发作、性能下降,在许多情况下也不能预防永久性脑损伤。这些症状在实验动物中很常见,在人类中也可能发生。这些解毒剂固有的问题促使人们尝试开发一种单一的保护性药物,这种药物本身没有药理作用,既能预防OP化合物的致死性,又能防止暴露后失能。一种方法是使用诸如胆碱酯酶(ChEs)、一般的β-酯酶等酶作为单一的预处理药物,在剧毒的OP抗胆碱酯酶到达其生理靶点之前将其隔离。这种方法将OP与ChE相互作用的不可逆性质从劣势转化为优势;与其将OP视为抗胆碱酯酶,不如将ChE用作抗OP。使用这种方法表明,给予胎牛血清AChE(FBSAChE)、马血清丁酰胆碱酯酶(EqBChE)或人血清BChE(HuBChE)可保护动物免受多种剧毒OP的多个半数致死量的影响,且无任何毒性作用或性能下降。迄今为止探索的用于OP解毒的生物清除剂可分为三类:(A)能够催化水解OP从而使其无毒的物质,如OP水解酶和OP脱水酶;(B)化学计量地与OP结合的物质,即1摩尔酶中和1或2摩尔OP从而使两者均失活的物质,如ChEs和相关酶;(C)通常被称为“假催化”的物质,例如ChE和肟预处理的组合,使得在存在肟的情况下被OP抑制的ChE的催化活性能够快速且持续地恢复。由于外源性酯酶(如ChEs)预防的生化机制已在包括非人灵长类动物在内的几种动物物种中得到确立和测试,这一概念应能使动物实验结果可靠地外推至人类应用。经过多个研究小组的广泛研究,血浆来源 HuBChE 被认为是最适合推进人类使用的生物清除剂。目前正在开展一项针对人类志愿者的安全性临床试验。随后还会有其他几种候选生物清除剂;例如,在转基因山羊乳汁中表达的重组 HuBChE、假催化清除剂(如 ChE 和肟的组合),未来可能还有对氧磷酶 1 作为催化清除剂。

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