In silico approaches in carcinogenicity hazard assessment: case study of pregabalin, a nongenotoxic mouse carcinogen

Douglas A Keller; Arianna Bassan; Alexander Amberg; Leigh Ann Burns Naas; Jon Chambers; Kevin Cross; Frances Hall; Gloria D Jahnke; Amarjit Luniwal; Serena Manganelli; Jordi Mestres; Amy L Mihalchik-Burhans; David Woolley; Raymond R Tice

doi:10.3389/ftox.2023.1234498

In silico approaches in carcinogenicity hazard assessment: case study of pregabalin, a nongenotoxic mouse carcinogen

Front Toxicol. 2023 Nov 13:5:1234498. doi: 10.3389/ftox.2023.1234498. eCollection 2023.

Authors

Affiliations

¹ Independent Consultant, Kennett Square, PA, United States.
² Innovatune, Padova, Italy.
³ Sanofi Preclinical Safety, Frankfurt, Germany.
⁴ Magnolia Toxicology Consulting, Traverse City, MI, United States.
⁵ Instem, Cambridge, United Kingdom.
⁶ Instem, Columbus, OH, United States.
⁷ Independent Consultant, Chapel Hill, NC, United States.
⁸ Medline Industries, Northfield, IL, United States.
⁹ Nestlé Research, Lausanne, Switzerland.
¹⁰ Chemotargets SL, Parc Científic de Barcelona, Barcelona, Spain.
¹¹ ToxStrategies LLC, Asheville, NC, United States.
¹² ForthTox, Linlithgow, United Kingdom.
¹³ RTice Consulting, Hillsborough, NC, United States.

Abstract

In silico toxicology protocols are meant to support computationally-based assessments using principles that ensure that results can be generated, recorded, communicated, archived, and then evaluated in a uniform, consistent, and reproducible manner. We investigated the availability of in silico models to predict the carcinogenic potential of pregabalin using the ten key characteristics of carcinogens as a framework for organizing mechanistic studies. Pregabalin is a single-species carcinogen producing only one type of tumor, hemangiosarcomas in mice via a nongenotoxic mechanism. The overall goal of this exercise is to test the ability of in silico models to predict nongenotoxic carcinogenicity with pregabalin as a case study. The established mode of action (MOA) of pregabalin is triggered by tissue hypoxia, leading to oxidative stress (KC5), chronic inflammation (KC6), and increased cell proliferation (KC10) of endothelial cells. Of these KCs, in silico models are available only for selected endpoints in KC5, limiting the usefulness of computational tools in prediction of pregabalin carcinogenicity. KC1 (electrophilicity), KC2 (genotoxicity), and KC8 (receptor-mediated effects), for which predictive in silico models exist, do not play a role in this mode of action. Confidence in the overall assessments is considered to be medium to high for KCs 1, 2, 5, 6, 7 (immune system effects), 8, and 10 (cell proliferation), largely due to the high-quality experimental data. In order to move away from dependence on animal data, development of reliable in silico models for prediction of oxidative stress, chronic inflammation, immunosuppression, and cell proliferation will be critical for the ability to predict nongenotoxic compound carcinogenicity.

Keywords: In silico toxicology protocol; cell proliferation; chronic inflammation; mode of action; non-genotoxic carcinogen; oxidative stress; pregabalin.