Modeling of free fatty acid dynamics: insulin and nicotinic acid resistance under acute and chronic treatments

Andersson, Robert; Kroon, Tobias; Almquist, Joachim; Jirstrand, Mats; Oakes, Nicholas D.; Evans, Neil D.; Chappel, Michael J.; Gabrielsson, Johan

doi:10.1007/s10928-017-9512-6

Cited by 9 publications

(15 citation statements)

References 39 publications

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“…The standard pharmacological approach of activating a target around the clock often fails because of time-dependent loss of drug efficacy and postdosing rebound above predose baseline levels. This case study presents data that originally explored the idea that a more comprehensive understanding of the relationship between plasma exposure and a pharmacological response combined with knowledge of the physiologic regulation of metabolism (i.e., simultaneously analyzed considering the effect of key biomarkers) can be used to mitigate these barriers, allowing the invention of new pharmacostrategies (Andersson et al, 2017;Kroon et al, 2017). The metaanalysis aimed at investigating in what way our inference about the system is changed when all drug exposure data are removed.…”

Section: Results and Conclusion Withmentioning

confidence: 99%

“…A well defined dosing regimen, rate, extent, and timing of drug intervention were designed sequentially across several studies. This resulted in suppression of tolerance and rebound and, most importantly, in profound improvements of the metabolic profile of a preclinical disease model (Andersson et al, 2017;Kroon et al, 2017). In turn, this information may provide vital input to projects aimed at discovery and development of novel drugs for metabolic disorder.…”

Section: Results and Conclusion Withmentioning

confidence: 99%

“…The raw data for case studies 1-7 are available in a spreadsheet format (Gabrielsson and Weiner, 2010). The eighth case study is aimed at demonstrating how data from several studies in a drug discovery project can be merged and analyzed simultaneously (Andersson et al, 2017). This latter meta-analysis utilizes data from multiple dose provocations with nicotinic acid (NiAc; dose, route, rate, and mode), as well as two intertwined biomarkers (plasma fatty acids and insulin) in a large population of control and disease model rats.…”

Section: Dose-response-time Data Analysismentioning

confidence: 99%

“…These case studies were selected to demonstrate how to tackle baseline/no baseline, time delays, peak shifts, saturation, cell growth/kill data, functional adaptation, rebound, multiple sources of drug provocations and biomarkers, and rapid exposure-response data ( Table 2). Isaksson et al (2009) and Andersson et al (2016Andersson et al ( , 2017 successfully performed meta-analyses on preclinical data on NiAc (nonlinear absorption and elimination)-induced fatty acid lowering, with accurate and precise parameter estimates. The kinetic nonlinearities were well separated from the pharmacodynamic nonlinearities.…”

Section: A Backgroundmentioning

confidence: 99%

“…These studies cover a large range of therapeutic and experimental areas. Some of the preclinical studies use two or more modes of administration and are more experimental in nature (Schoenwald and Smolen, 1971;Smolen, 1971aSmolen, ,b, 1976aSmolen, ,b, 1978Smolen et al, 1972;Smolen and Weigand, 1973;Isaksson et al, 2009;Andersson et al, 2017). Other studies are performed in critically ill patients (Salem et al, 2016), in neonates (Trefz et al, 2015), under disease progression (Musuamba et al, 2015), for postoperative pain management (Abou Hammoud et al, 2009), in drug interaction studies (Gruwez et al, 2005(Gruwez et al, , 2007, and in metabolic systems (Fasanmade and Jusko, 1995;Hamberg et al, 2010;Ternant et al, 2014;Saffian et al, 2016), to mention just a few.…”

Section: A Backgroundmentioning

confidence: 99%

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Dose-Response-Time Data Analysis: An Underexploited Trinity

et al. 2018

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Section: Results and Conclusion Withmentioning

confidence: 99%

Section: Results and Conclusion Withmentioning

confidence: 99%

Section: Dose-response-time Data Analysismentioning

confidence: 99%

Section: A Backgroundmentioning

confidence: 99%

Section: A Backgroundmentioning

confidence: 99%

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Dose-Response-Time Data Analysis: An Underexploited Trinity

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Challenge model of TNFα turnover at varying LPS and drug provocations

Held

Hoppe

Cvijović

et al. 2019

J Pharmacokinet Pharmacodyn

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A mechanism-based biomarker model of TNF α -response, including different external provocations of LPS challenge and test compound intervention, was developed. The model contained system properties (such as k t , k out ), challenge characteristics (such as k s , k LPS , K m, LPS , S max , SC 50 ) and test-compound-related parameters ( I max , IC 50 ). The exposure to test compound was modelled by means of first-order input and Michaelis–Menten type of nonlinear elimination. Test compound potency was estimated to 20 nM with a 70% partial reduction in TNF α -response at the highest dose of 30 mg·kg −1 . Future selection of drug candidates may focus the estimation on potency and efficacy by applying the selected structure consisting of TNF α system and LPS challenge characteristics. A related aim was to demonstrate how an exploratory (graphical) analysis may guide us to a tentative model structure, which enables us to better understand target biology. The analysis demonstrated how to tackle a biomarker with a baseline below the limit of detection. Repeated LPS-challenges may also reveal how the rate and extent of replenishment of TNF α pools occur. Lack of LPS exposure-time courses was solved by including a biophase model, with the underlying assumption that TNF α -response time courses, as such, contain kinetic information. A transduction type of model with non-linear stimulation of TNF α release was finally selected. Typical features of a challenge experiment were shown by means of model simulations. Experimental shortcomings of present and published designs are identified and discussed. The final model coupled to suggested guidance rules may serve as a general basis for the collection and analysis of pharmacological challenge data of future studies. Electronic supplementary material The online version of this article (10.1007/s10928-019-09622-x) contains supplementary material, which is available to authorized users.

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