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高效液相色谱-质谱联用技术分析药物时血液微量采样技术及采样部位的评估

Evaluation of blood microsampling techniques and sampling sites for the analysis of drugs by HPLC-MS.

作者信息

Smith Christopher, Sykes Angela, Robinson Sally, Thomas Elizabeth

机构信息

Clinical Pharmacology Department, Alderley, AstraZeneca Pharmaceuticals, Mereside, Alderley Park, Macclesfield, Cheshire, SK10 4TG, UK.

出版信息

Bioanalysis. 2011 Jan;3(2):145-56. doi: 10.4155/bio.10.193.

Abstract

BACKGROUND

the potential for whole blood sampling (20 µl) in toxicokinetic studies to reduce the sample volume was investigated. Blood microsamples were collected in three ways, either as a dried blood spot (DBS), a blood sample collected in a micropipette placed in a plastic tube and mixed with water or as plasma in the normal manner.

RESULTS

blood samples on the DBS and the whole blood microtube (WBMT) were compared along with DBS and plasma to determine the toxicokinetic data equivalency. The DBS and WBMT comparison was shown to be equivalent, as demonstrated on a correlation plot with an R(2) value of 0.97 for an x = y plot. The plasma comparison with DBS also gave a good correlation. A correction factor (x(2)) was applied to the blood data to allow for the distribution of the compound between plasma and bloods, and therefore, a direct comparison could be made. The correlation plot derived from the sample data gave an R(2) value 0.98 (x = y plot), indicating dataset equivalency. Sampling sites were evaluated in a dog study. Blood was collected from the peripheral region, in this case the ear, and a venous region of the dog; and spotted onto DBS cards. Comparison of the mean area under the curve data for the sampling sites showed equivalent data: 5095 and 5175 ng.h/ml for the 25 mg/kg dose and 16695 ng.h/ml and 16000 ng.h/ml for the 50 mg/kg dose for the ear and the venous samples, respectively.

CONCLUSION

the DBS cards were shown to be an equivalent microsampling process when compared with WBMT and conventional plasma analysis. With the added benefits of sample storage, shipment and ease of use for DBS, this technology could change the way samples are taken and then analyzed in bioanalysis in the future.

摘要

背景

研究了在毒代动力学研究中采用全血采样(20微升)以减少样本量的可能性。血液微量样本通过三种方式采集,即作为干血斑(DBS)、收集在置于塑料管中的微量移液器中并与水混合的血液样本,或按常规方式采集的血浆。

结果

比较了DBS和全血微量管(WBMT)上的血液样本以及DBS和血浆,以确定毒代动力学数据的等效性。DBS和WBMT的比较显示是等效的,在x = y图的相关图上,R(2)值为0.97就证明了这一点。血浆与DBS的比较也具有良好的相关性。对血液数据应用了一个校正因子(x(2)),以考虑化合物在血浆和血液之间的分布,因此可以进行直接比较。从样本数据得出的相关图给出了R(2)值0.98(x = y图),表明数据集等效。在一项犬类研究中评估了采样部位。从外周区域(在这种情况下是耳朵)和犬的静脉区域采集血液,并点样到DBS卡上。采样部位的曲线下平均面积数据比较显示数据等效:25毫克/千克剂量时,耳朵样本和静脉样本的曲线下平均面积分别为5095和5175纳克·小时/毫升;50毫克/千克剂量时,分别为16695和16000纳克·小时/毫升。

结论

与WBMT和传统血浆分析相比,DBS卡显示是一种等效的微量采样方法。由于DBS具有样本储存、运输和使用方便等额外优点,这项技术可能会改变未来生物分析中样本采集和分析的方式。

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