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新型氰化物解毒剂二甲基三硫醚制剂的血脑屏障穿透及药代动力学研究

Investigation of blood-brain barrier penetration and pharmacokinetics of a new formulation of cyanide antidote dimethyl trisulfide.

作者信息

Kiss Lóránd, Walter Fruzsina R, Katona Gábor, Santa-Maria Ana Raquel, Whiteman Ashley C, Rios Christian T, Kelley Kyler D, Nelson Breanna, Thompson David E, Csóka Ildikó, Szabó-Révész Piroska, Deli Mária A, Petrikovics Ilona

机构信息

Department of Chemistry, Sam Houston State University, 1003 Bowers Blvd, Huntsville, TX 77341 USA.

Department of Pathophysiology, University of Szeged, Szőkevalfi-Nagy Béla U. 6., Szeged, Hungary 6720.

出版信息

Toxicol Environ Health Sci. 2025;17(2):313-323. doi: 10.1007/s13530-025-00257-9. Epub 2025 Apr 29.

Abstract

OBJECTIVE

During cyanide poisoning, the rescue of vital organs like the brain is urgent. However, due to the presence of the blood-brain barrier (BBB), the currently available cyanide antidotes cannot reach the brain. Dimethyl trisulfide (DMTS) is a potent cyanide antidote and has excellent BBB permeability. Nonetheless, its formulation and application are challenging due to its highly lipophilic profile. In this work, a novel DMTS formulation, called FF-DMTS, was investigated. Its effect on in vitro DMTS permeability through BBB models, cellular viability, and in vivo absorption were tested.

METHODS

The particle size was measured in FF-DMTS formulation. The permeability of DMTS in this new formulation was tested in BBB-PAMPA and in primary triple co-culture models of BBB. The effect of FF-DMTS on cellular viability was determined. To test the membrane and barrier integrity transendothelial electrical resistance (TEER) and cell layer impedance measurements, immunofluorescent stainings and the fluorescein permeability technique were applied. The pharmacokinetics of DMTS were revealed in blood and brain tissue.

RESULTS

The average size of micelles in FF-DMTS was 16 nm. The permeability of DMTS through BBB-PAMPA and cell culture model was 7.68 × 10 and 23.81 × 10 cm/s, respectively. The FF-DMTS disturbed the barrier integrity of brain endothelial cells without causing any alteration in cellular viability until 300 µg/ml DMTS concentration. After administration of 150 mg/kg DMTS to mice, its absorption into the blood was rapid (5 min) and the plasma concentration of DMTS reached 5.2 µg/ml. The DMTS was also detected in brain, where its peak concentration was 495 ng/g brain tissue after 10 min of intramuscular administration. Furthermore, even 2 h later, DMTS was detected in brain.

CONCLUSIONS

Here, we showed that the novel FF-DMTS formulation has good permeability through BBB and a remarkable pharmacokinetic profile. Therefore, further investigation of the efficacy of FF-DMTS for treating cyanide intoxication is important.

摘要

目的

在氰化物中毒期间,抢救大脑等重要器官刻不容缓。然而,由于血脑屏障(BBB)的存在,目前可用的氰化物解毒剂无法到达大脑。二甲基三硫醚(DMTS)是一种有效的氰化物解毒剂,具有出色的血脑屏障通透性。尽管如此,由于其高度亲脂性,其制剂和应用具有挑战性。在这项研究中,研究了一种名为FF-DMTS的新型DMTS制剂。测试了其对通过血脑屏障模型的体外DMTS通透性、细胞活力和体内吸收的影响。

方法

测量FF-DMTS制剂的粒径。在BBB-PAMPA和血脑屏障的原代三重共培养模型中测试了该新制剂中DMTS的通透性。确定了FF-DMTS对细胞活力的影响。为了测试膜和屏障完整性,应用了跨内皮电阻(TEER)和细胞层阻抗测量、免疫荧光染色和荧光素通透性技术。揭示了DMTS在血液和脑组织中的药代动力学。

结果

FF-DMTS中胶束的平均尺寸为16纳米。DMTS通过BBB-PAMPA和细胞培养模型的通透性分别为7.68×10和23.81×10厘米/秒。在DMTS浓度达到300微克/毫升之前,FF-DMTS扰乱了脑内皮细胞的屏障完整性,但未引起细胞活力的任何改变。给小鼠注射150毫克/千克DMTS后,其吸收进入血液很快(5分钟),DMTS的血浆浓度达到5.2微克/毫升。在脑中也检测到了DMTS,肌肉注射10分钟后其峰值浓度为495纳克/克脑组织。此外,即使在2小时后,脑中仍检测到DMTS。

结论

在此,我们表明新型FF-DMTS制剂具有良好的血脑屏障通透性和显著的药代动力学特征。因此,进一步研究FF-DMTS治疗氰化物中毒的疗效具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2617/12379708/8ddf8aa53c29/13530_2025_257_Fig1_HTML.jpg

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