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研究用羧酰胺取代羧酸盐以调节铂(II)硫醚氰化物清除剂的安全性和有效性。

Investigating the Replacement of Carboxylates with Carboxamides to Modulate the Safety and Efficacy of Platinum(II) Thioether Cyanide Scavengers.

作者信息

Behymer Matthew M, Mo Huaping, Fujii Naoaki, Suresh Vallabh, Arzumanian Ari S, Chan Adriano, Nath Anjali K, McCain Robyn, MacRae Calum A, Peterson Randall, Boss Gerry R, Davisson Vincent Jo, Knipp Gregory T

机构信息

Department of Industrial and Molecular Pharmaceutics, Purdue University, 575 Stadium Mall Drive, West Lafayette, Indiana 47907, USA.

Department of Medicinal Chemistry and Molecular Pharmacology, Purdue University, 575 Stadium Mall Drive, West Lafayette, Indiana 47907, USA.

出版信息

Toxicol Sci. 2023 Nov 11;197(2):197-210. doi: 10.1093/toxsci/kfad119.

Abstract

Cyanide represents a persistent threat for accidental or malicious misuse due to easy conversion into a toxic gas and access to large quantities through several industries. The high safety index of hydroxocobalamin is a cornerstone quality as a cyanide scavenger. Unfortunately, intravenous infusion of hydroxocobalamin limits the utility in a mass casualty setting. We previously reported platinum(II) [Pt(II)] complexes with trans-directing sulfur ligands as an efficacious alternative to hydroxocobalamin when delivered by a bolus intramuscular injection in mice and rabbits. Thus, to enable Pt(II) as an alternative to hydroxocobalamin, a high safety factor is needed. The objective is to maintain efficacy and mitigate the risk for nephrotoxicity. Platinum amino acid complexes with the ability to form five- or six-membered rings and possessing either carboxylates or carboxamides are evaluated in vitro for cyanide scavenging. In vivo efficacy was evaulated in the zebrafish and mice cyanide exposure models. In addition, Pt(II) complex toxicity and pharmacokinetics were evaluated in a cyanide naive Sprague-Dawley model. Doses for toxicity are escalated to 5x from the efficacious dose in mice using a body surface area adjustment. The results show the carboxamide ligands display a time and pH dependence on cyanide scavenging in vitro and efficacy in vivo. Additionally, exchanging the carboxylate for carboxamide showed reduced indications of renal injury. A pharmacokinetic analysis of the larger bidentate complexes displayed rapid absorption by intramuscular administration and having similar plasma exposure. These findings point to the importance of pH and ligand structures for methionine carboxamide complexes with Pt(II).

摘要

由于氰化物易于转化为有毒气体,且可通过多个行业获取大量氰化物,因此它对意外或恶意滥用构成持续威胁。羟钴胺素的高安全指数是其作为氰化物清除剂的一项关键品质。不幸的是,静脉输注羟钴胺素限制了其在大规模伤亡情况下的应用。我们之前报道过,带有反式导向硫配体的铂(II)[Pt(II)]配合物,在小鼠和兔子中通过大剂量肌肉注射给药时,是羟钴胺素的一种有效替代品。因此,要使Pt(II)成为羟钴胺素的替代品,就需要一个高安全系数。目标是保持疗效并降低肾毒性风险。对具有形成五元或六元环能力且含有羧酸盐或羧酰胺的铂氨基酸配合物进行体外氰化物清除评估。在斑马鱼和小鼠氰化物暴露模型中评估体内疗效。此外,在未接触氰化物的斯普拉格 - 道利模型中评估Pt(II)配合物的毒性和药代动力学。使用体表面积调整方法,将小鼠毒性剂量从有效剂量逐步提高到5倍。结果表明,羧酰胺配体在体外对氰化物清除呈现时间和pH依赖性,在体内具有疗效。此外,将羧酸盐换成羧酰胺显示肾损伤迹象减少。对较大的双齿配合物进行的药代动力学分析表明,肌肉注射给药后吸收迅速,且血浆暴露情况相似。这些发现表明pH和配体结构对于Pt(II)的甲硫氨酸羧酰胺配合物很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c93c/10823771/0606f6af0e01/kfad119f9.jpg

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