AUTHOR=Moreau Marjory , Simms Liam , Andersen Melvin E. , Trelles Sticken Edgar , Wieczorek Roman , Pour Sarah Jean , Chapman Fiona , Roewer Karin , Otte Sandra , Fisher Jeffrey , Stevenson Matthew 

TITLE=Use of quantitative in vitro to in vivo extrapolation (QIVIVE) for the assessment of non-combustible next-generation product aerosols

JOURNAL=Frontiers in Toxicology

VOLUME=6

YEAR=2024

URL=https://www.frontiersin.org/journals/toxicology/articles/10.3389/ftox.2024.1373325

DOI=10.3389/ftox.2024.1373325

ISSN=2673-3080

ABSTRACT=<p>With the use of <italic>in vitro</italic> new approach methodologies (NAMs) for the assessment of non-combustible next-generation nicotine delivery products, new extrapolation methods will also be required to interpret and contextualize the physiological relevance of these results. Quantitative <italic>in vitro</italic> to <italic>in vivo</italic> extrapolation (QIVIVE) can translate <italic>in vitro</italic> concentrations into in-life exposures with physiologically-based pharmacokinetic (PBPK) modelling and provide estimates of the likelihood of harmful effects from expected exposures. A major challenge for evaluating inhalation toxicology is an accurate assessment of the delivered dose to the surface of the cells and the internalized dose. To estimate this, we ran the multiple-path particle dosimetry (MPPD) model to characterize particle deposition in the respiratory tract and developed a PBPK model for nicotine that was validated with human clinical trial data for cigarettes. Finally, we estimated a Human Equivalent Concentration (HEC) and predicted plasma concentrations based on the minimum effective concentration (MEC) derived after acute exposure of BEAS-2B cells to cigarette smoke (1R6F), or heated tobacco product (HTP) aerosol at the air liquid interface (ALI). The MPPD-PBPK model predicted the <italic>in vivo</italic> data from clinical studies within a factor of two, indicating good agreement as noted by WHO International Programme on Chemical Safety (2010) guidance. We then used QIVIVE to derive the exposure concentration (HEC) that matched the estimated <italic>in vitro</italic> deposition point of departure (POD) (MEC cigarette = 0.38 puffs or 11.6 µg nicotine, HTP = 22.9 puffs or 125.6 µg nicotine) and subsequently derived the equivalent human plasma concentrations. Results indicate that for the 1R6F cigarette, inhaling 1/6th of a stick would be required to induce the same effects observed <italic>in vitro</italic>, <italic>in vivo</italic>. Whereas, for HTP it would be necessary to consume 3 sticks simultaneously to induce <italic>in vivo</italic> the effects observed <italic>in vitro</italic>. This data further demonstrates the reduced physiological potency potential of HTP aerosol compared to cigarette smoke. The QIVIVE approach demonstrates great promise in assisting human health risk assessments, however, further optimization and standardization are required for the substantiation of a meaningful contribution to tobacco harm reduction by alternative nicotine delivery products.</p>