Comparison of pharmacokinetic study profiles of insulin in rat plasma through conventional sampling and microsampling by micro-LC-MS/MS

Gaudry Bruno Troche; Tue Søeborg; Thóra Brynja Bödvarsdottir; Mads Bjelke; Nikoline Juul Nielsen

doi:10.4155/bio-2023-0006

Comparison of pharmacokinetic study profiles of insulin in rat plasma through conventional sampling and microsampling by micro-LC-MS/MS

Gaudry Bruno Troche^*, Tue Søeborg, Thóra Brynja Bödvarsdottir, Mads Bjelke, Nikoline Juul Nielsen

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

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Abstract

Aim: With microsamples of blood, full pharmacokinetic profiles from individual animals can be obtained as an alternative to the sparse-sampling approach, where conventional volume samples from several animals are required. However, microsamples require assays that are more sensitive. Methods: The sensitivity of the LC-MS assay was increased 47-fold using microflow LC-MS. Results & conclusion: By analyzing both microsamples and conventional samples from the same animals, it is demonstrated that sparse-sampling profiles can be nonrepresentative of the full profiles. This bias can affect the tested treatment by increasing or reducing its apparent effect. Microsampling enables unbiased results compared with sparse-sampling. An increase in assay sensitivity to balance the low sample volumes was achievable by microflow LC-MS.

Originalsprog	Engelsk
Tidsskrift	Bioanalysis
Vol/bind	15
Udgave nummer	5
Sider (fra-til)	283-294
Antal sider	12
ISSN	1757-6180
DOI	https://doi.org/10.4155/bio-2023-0006
Status	Udgivet - 2023

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10.4155/bio-2023-0006

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Citationsformater

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title = "Comparison of pharmacokinetic study profiles of insulin in rat plasma through conventional sampling and microsampling by micro-LC-MS/MS",

abstract = "Aim: With microsamples of blood, full pharmacokinetic profiles from individual animals can be obtained as an alternative to the sparse-sampling approach, where conventional volume samples from several animals are required. However, microsamples require assays that are more sensitive. Methods: The sensitivity of the LC-MS assay was increased 47-fold using microflow LC-MS. Results & conclusion: By analyzing both microsamples and conventional samples from the same animals, it is demonstrated that sparse-sampling profiles can be nonrepresentative of the full profiles. This bias can affect the tested treatment by increasing or reducing its apparent effect. Microsampling enables unbiased results compared with sparse-sampling. An increase in assay sensitivity to balance the low sample volumes was achievable by microflow LC-MS.",

keywords = "insulins, microflow liquid chromatography, microsampling, pharmacokinetics, DOPING CONTROL ANALYSIS, LIQUID-CHROMATOGRAPHY, MASS-SPECTROMETRY, WHOLE-BLOOD, PROTEINS, PEPTIDES, ANALOGS, QUANTIFICATION, URINE",

author = "Troche, {Gaudry Bruno} and Tue S{\o}eborg and B{\"o}dvarsdottir, {Th{\'o}ra Brynja} and Mads Bjelke and Nielsen, {Nikoline Juul}",

year = "2023",

doi = "10.4155/bio-2023-0006",

language = "English",

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journal = "Bioanalysis",

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TY - JOUR

T1 - Comparison of pharmacokinetic study profiles of insulin in rat plasma through conventional sampling and microsampling by micro-LC-MS/MS

AU - Troche, Gaudry Bruno

AU - Søeborg, Tue

AU - Bödvarsdottir, Thóra Brynja

AU - Bjelke, Mads

AU - Nielsen, Nikoline Juul

PY - 2023

Y1 - 2023

N2 - Aim: With microsamples of blood, full pharmacokinetic profiles from individual animals can be obtained as an alternative to the sparse-sampling approach, where conventional volume samples from several animals are required. However, microsamples require assays that are more sensitive. Methods: The sensitivity of the LC-MS assay was increased 47-fold using microflow LC-MS. Results & conclusion: By analyzing both microsamples and conventional samples from the same animals, it is demonstrated that sparse-sampling profiles can be nonrepresentative of the full profiles. This bias can affect the tested treatment by increasing or reducing its apparent effect. Microsampling enables unbiased results compared with sparse-sampling. An increase in assay sensitivity to balance the low sample volumes was achievable by microflow LC-MS.

AB - Aim: With microsamples of blood, full pharmacokinetic profiles from individual animals can be obtained as an alternative to the sparse-sampling approach, where conventional volume samples from several animals are required. However, microsamples require assays that are more sensitive. Methods: The sensitivity of the LC-MS assay was increased 47-fold using microflow LC-MS. Results & conclusion: By analyzing both microsamples and conventional samples from the same animals, it is demonstrated that sparse-sampling profiles can be nonrepresentative of the full profiles. This bias can affect the tested treatment by increasing or reducing its apparent effect. Microsampling enables unbiased results compared with sparse-sampling. An increase in assay sensitivity to balance the low sample volumes was achievable by microflow LC-MS.

KW - insulins

KW - microflow liquid chromatography

KW - microsampling

KW - pharmacokinetics

KW - DOPING CONTROL ANALYSIS

KW - LIQUID-CHROMATOGRAPHY

KW - MASS-SPECTROMETRY

KW - WHOLE-BLOOD

KW - PROTEINS

KW - PEPTIDES

KW - ANALOGS

KW - QUANTIFICATION

KW - URINE

U2 - 10.4155/bio-2023-0006

DO - 10.4155/bio-2023-0006

M3 - Journal article

C2 - 37058314

SN - 1757-6180

VL - 15

SP - 283

EP - 294

JO - Bioanalysis

JF - Bioanalysis

IS - 5

ER -