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二巯基丁二酸、二巯基丙磺酸和甲羟孕酮——作为砷解毒剂。

DMSA, DMPS, and DMPA--as arsenic antidotes.

作者信息

Aposhian H V, Carter D E, Hoover T D, Hsu C A, Maiorino R M, Stine E

出版信息

Fundam Appl Toxicol. 1984 Apr;4(2 Pt 2):S58-70. doi: 10.1016/0272-0590(84)90138-6.

DOI:10.1016/0272-0590(84)90138-6
PMID:6327446
Abstract

meso-Dimercaptosuccinic acid (DMSA), 2,3-dimercapto-1-propanesulfonic acid, Na salt (DMPS), and N-(2,3- dimercaptopropyl )- phthalamidic acid (DMPA) are water soluble analogs of 2,3-dimercapto-1-propanol (BAL). The relative effectiveness or therapeutic index of these dimercapto compounds in protecting mice from the lethal effects of an LD99 of sodium arsenite is DMSA greater than DMPS greater than DMPA greater than BAL in the magnitude of 42:14:4:1, respectively. DMPS, DMPA, or DMSA will mobilize tissue arsenic. BAL, however, increases the arsenic content of the brain of rabbits injected with sodium arsenite. These results raise the question as to the appropriateness of BAL as the treatment for systemic arsenic poisoning. Either DMSA or DMPS, when given sc or po, will protect rabbits against the lethal systemic effects of subcutaneously administered Lewisite . DMPS and DMSA have promise as prophylactics for the prevention of the vesicant action of Lewisite . The sodium arsenite inhibition of the pyruvate dehydrogenase (PDH) complex can be prevented and reversed in vitro or in vivo by DMPS, DMSA, DMPA, or BAL. Of them all, DMPS is most potent and BAL appears to be the least potent. The usefulness of all these dimercapto compounds would be enhanced by a careful study of their metabolism and biotransformation. These dimercapto compounds are in a great many respects orphan drugs. At this stage of their development, it is very difficult for the clinician to obtain funds to study them clinically even though they appear to be useful for treatment of poisoning by any one of the heavy metals.

摘要

中-二巯基丁二酸(DMSA)、2,3-二巯基-1-丙烷磺酸钠(DMPS)和N-(2,3-二巯基丙基)邻苯二甲酰胺酸(DMPA)是2,3-二巯基-1-丙醇(BAL)的水溶性类似物。这些二巯基化合物在保护小鼠免受亚砷酸钠LD99致死效应方面的相对效力或治疗指数分别为DMSA大于DMPS大于DMPA大于BAL,其比例为42:14:4:1。DMPS、DMPA或DMSA会促使组织中的砷排出。然而,BAL会增加注射亚砷酸钠的兔子大脑中的砷含量。这些结果引发了关于BAL作为系统性砷中毒治疗药物是否合适的问题。DMSA或DMPS经皮下或口服给药时,可保护兔子免受皮下注射路易氏剂的致死性全身效应。DMPS和DMSA有望作为预防路易氏剂起疱作用的预防药物。在体外或体内,DMPS、DMSA、DMPA或BAL均可预防并逆转亚砷酸钠对丙酮酸脱氢酶(PDH)复合物的抑制作用。在所有这些物质中,DMPS效力最强,而BAL似乎效力最弱。对这些二巯基化合物的代谢和生物转化进行仔细研究,将提高它们的效用。这些二巯基化合物在很多方面都属于孤儿药。在它们的这个研发阶段,临床医生很难获得资金对其进行临床研究,尽管它们似乎对治疗任何一种重金属中毒都有用。

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