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一种用于万古霉素治疗药物监测的荧光生物传感器,采用体内微透析技术。

A fluorescence biosensor for therapeutic drug monitoring of vancomycin using in vivo microdialysis.

作者信息

Mu Fangya, Zhou Xinguang, Fan Fang, Chen Zhiyu, Shi Guoyue

机构信息

Department of Chemistry, School of Chemistry and Molecular Engineering, East China Normal University, Dongchuan Road 500, Shanghai, 200241, China.

Department of Anesthesiology and Intensive Care Medicine, Xinhua Hospital, College of Medicine, Shanghai Jiaotong University, Kongjiang Road 1665, Shanghai, 200092, China.

出版信息

Anal Chim Acta. 2021 Mar 22;1151:338250. doi: 10.1016/j.aca.2021.338250. Epub 2021 Jan 24.

Abstract

Clinical vancomycin (Van) treatment is administered over a prolonged period to achieve a sustained therapeutic effect. Accurate, rapid, and continuous Van detection is an unmet medical monitoring need that can provide data-based guidance for doctors to adjust the dosage and treatment plan in real-world settings. In this study, we created a Van-specific, fluorescent biosensor that was combined with a microdialysis sampling technique to develop a rapid, simple, accurate, and sensitive detection method, which was validated for Van in vivo. A Van-specific probe was created by separately conjugating each of the two peptide chains of a dimeric derivative of the Van binding peptide L-Lys-D-Ala-D-Ala to a fluorescent dansyl chloride group. Subject-specific pharmacokinetics of Van was recorded in normal rabbits and rabbits with adenine-induced chronic renal failure (CRF), which indicated the feasibility of therapeutic drug monitoring in vivo. The area under the concentration-time curve (AUC) was 10,715 min μg mL (95% CI = 8,892 to 12,538) in the normal rabbits, and 14,822 and 19,025 min μg mL in two selected CRF rabbits. Furthermore, using pharmacokinetic dosing of Van in a rabbit study, we designed the dosage and drug administration interval to achieve a sustained therapeutic effect. The normal rabbits received three Van doses, 20, 5, and 5 mg kg, administered at 0, 500, and 900 min, respectively. The CRF rabbits received two Van doses, 20 and 5 mg kg, administered at 0 and 600 min, respectively. Thus, we established an effective method for the continuous monitoring of Van. This method facilitates the detection of Van in clinical treatment and provides the scientific basis for an effective approach to monitor blood drug levels during the clinical treatment of various diseases.

摘要

临床使用万古霉素(Van)时需长期给药以达到持续的治疗效果。准确、快速且连续地检测Van是一项尚未满足的医学监测需求,可为医生在实际临床环境中调整剂量和治疗方案提供基于数据的指导。在本研究中,我们创建了一种针对Van的荧光生物传感器,并将其与微透析采样技术相结合,开发出一种快速、简单、准确且灵敏的检测方法,该方法已在体内对Van进行了验证。通过将Van结合肽L-Lys-D-Ala-D-Ala的二聚体衍生物的两条肽链分别与荧光丹磺酰氯基团偶联,创建了一种针对Van的探针。记录了正常兔和腺嘌呤诱导的慢性肾衰竭(CRF)兔体内Van的个体特异性药代动力学,这表明了体内治疗药物监测的可行性。正常兔的浓度-时间曲线下面积(AUC)为10,715 min μg/mL(95%置信区间=8,892至12,538),在两只选定的CRF兔中分别为14,822和19,025 min μg/mL。此外,在兔研究中使用Van的药代动力学给药方法,我们设计了剂量和给药间隔以实现持续的治疗效果。正常兔接受三次Van剂量,分别为20、5和5 mg/kg,在0、500和900分钟给药。CRF兔接受两次Van剂量,分别为20和5 mg/kg,在0和600分钟给药。因此,我们建立了一种连续监测Van的有效方法。该方法有助于临床治疗中Van的检测,并为在各种疾病的临床治疗过程中监测血药水平的有效方法提供科学依据。

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