Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model

[Image: see text] Nominal concentrations (C(Nom)) in cell culture media are routinely used to define concentration–effect relationships in the in vitro toxicology. The actual concentration in the medium (C(Medium)) can be affected by adsorption processes, evaporation, or degradation of chemicals. Th...

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Autores principales: Dimitrijevic, Dunja, Fabian, Eric, Nicol, Beate, Funk-Weyer, Dorothee, Landsiedel, Robert
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9682521/
https://www.ncbi.nlm.nih.gov/pubmed/36264934
http://dx.doi.org/10.1021/acs.chemrestox.2c00128
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author Dimitrijevic, Dunja
Fabian, Eric
Nicol, Beate
Funk-Weyer, Dorothee
Landsiedel, Robert
author_facet Dimitrijevic, Dunja
Fabian, Eric
Nicol, Beate
Funk-Weyer, Dorothee
Landsiedel, Robert
author_sort Dimitrijevic, Dunja
collection PubMed
description [Image: see text] Nominal concentrations (C(Nom)) in cell culture media are routinely used to define concentration–effect relationships in the in vitro toxicology. The actual concentration in the medium (C(Medium)) can be affected by adsorption processes, evaporation, or degradation of chemicals. Therefore, we measured the total and free concentration of 12 chemicals, covering a wide range of lipophilicity (log K(OW) −0.07–6.84), in the culture medium (C(Medium)) and cells (C(Cell)) after incubation with Balb/c 3T3 cells for up to 48 h. Measured values were compared to predictions using an as yet unpublished in silico mass balance model that combined relevant equations from similar models published by others. The total C(Medium) for all chemicals except tamoxifen (TAM) were similar to the C(Nom). This was attributed to the cellular uptake of TAM and accumulation into lysosomes. The free (i.e., unbound) C(Medium) for the low/no protein binding chemicals were similar to the C(Nom), whereas values of all moderately to highly protein-bound chemicals were less than 30% of the C(Nom). Of the 12 chemicals, the two most hydrophilic chemicals, acetaminophen (APAP) and caffeine (CAF), were the only ones for which the C(Cell) was the same as the C(Nom). The C(Cell) for all other chemicals tended to increase over time and were all 2- to 274-fold higher than C(Nom). Measurements of C(Cytosol), using a digitonin method to release cytosol, compared well with C(Cell) (using a freeze–thaw method) for four chemicals (CAF, APAP, FLU, and KET), indicating that both methods could be used. The mass balance model predicted the total C(Medium) within 30% of the measured values for 11 chemicals. The free C(Medium) of all 12 chemicals were predicted within 3-fold of the measured values. There was a poorer prediction of C(Cell) values, with a median overprediction of 3- to 4-fold. In conclusion, while the number of chemicals in the study is limited, it demonstrates the large differences between C(Nom) and total and free C(Medium) and C(Cell), which were also relatively well predicted by the mass balance model.
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spelling pubmed-96825212022-11-24 Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model Dimitrijevic, Dunja Fabian, Eric Nicol, Beate Funk-Weyer, Dorothee Landsiedel, Robert Chem Res Toxicol [Image: see text] Nominal concentrations (C(Nom)) in cell culture media are routinely used to define concentration–effect relationships in the in vitro toxicology. The actual concentration in the medium (C(Medium)) can be affected by adsorption processes, evaporation, or degradation of chemicals. Therefore, we measured the total and free concentration of 12 chemicals, covering a wide range of lipophilicity (log K(OW) −0.07–6.84), in the culture medium (C(Medium)) and cells (C(Cell)) after incubation with Balb/c 3T3 cells for up to 48 h. Measured values were compared to predictions using an as yet unpublished in silico mass balance model that combined relevant equations from similar models published by others. The total C(Medium) for all chemicals except tamoxifen (TAM) were similar to the C(Nom). This was attributed to the cellular uptake of TAM and accumulation into lysosomes. The free (i.e., unbound) C(Medium) for the low/no protein binding chemicals were similar to the C(Nom), whereas values of all moderately to highly protein-bound chemicals were less than 30% of the C(Nom). Of the 12 chemicals, the two most hydrophilic chemicals, acetaminophen (APAP) and caffeine (CAF), were the only ones for which the C(Cell) was the same as the C(Nom). The C(Cell) for all other chemicals tended to increase over time and were all 2- to 274-fold higher than C(Nom). Measurements of C(Cytosol), using a digitonin method to release cytosol, compared well with C(Cell) (using a freeze–thaw method) for four chemicals (CAF, APAP, FLU, and KET), indicating that both methods could be used. The mass balance model predicted the total C(Medium) within 30% of the measured values for 11 chemicals. The free C(Medium) of all 12 chemicals were predicted within 3-fold of the measured values. There was a poorer prediction of C(Cell) values, with a median overprediction of 3- to 4-fold. In conclusion, while the number of chemicals in the study is limited, it demonstrates the large differences between C(Nom) and total and free C(Medium) and C(Cell), which were also relatively well predicted by the mass balance model. American Chemical Society 2022-10-20 2022-11-21 /pmc/articles/PMC9682521/ /pubmed/36264934 http://dx.doi.org/10.1021/acs.chemrestox.2c00128 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by-nc-nd/4.0/Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Dimitrijevic, Dunja
Fabian, Eric
Nicol, Beate
Funk-Weyer, Dorothee
Landsiedel, Robert
Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model
title Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model
title_full Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model
title_fullStr Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model
title_full_unstemmed Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model
title_short Toward Realistic Dosimetry In Vitro: Determining Effective Concentrations of Test Substances in Cell Culture and Their Prediction by an In Silico Mass Balance Model
title_sort toward realistic dosimetry in vitro: determining effective concentrations of test substances in cell culture and their prediction by an in silico mass balance model
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9682521/
https://www.ncbi.nlm.nih.gov/pubmed/36264934
http://dx.doi.org/10.1021/acs.chemrestox.2c00128
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