In Vitro Toxicology Testing: Dismantling the Barriers via Collaboration

Such cross-talk could drive forward the progression of in vitro toxicity analyses. Firstly, tool developers could partner with larger pharmaceutical companies to bear the risks and costs of optimizing a new tool for the market, creating a win-win situation in which pharma obtains a valuable new tool while the tool developer gains a high-value customer. Secondly, upstart Contract Research Organizations (CROs) could partner with tool developers to create sustainable business models that support the larger pharmaceutical companies to drive forward new technologies. Finally, the regulatory agencies must also be engaged and consulted in these efforts.    

Collaboration among these key players could also promote wider adoption of new in vitro assays. When seeking to make their product commercially available, tool developers are typically faced with major commercial competition from established, standardized methods that are at times required by regulatory agencies. In other words, the choice of methods a company uses is in many cases dictated by regulatory expectations. In keeping costs low, many firms are not willing to try anything new and only dedicate resources towards the methods required by regulatory agencies. Therefore, tool developers need to form robust partnerships with both end-users and regulators, so they can share risks and drive the field forward.

The benefits of collaboration

One initiative started in 2013 by the non-profit ILSI Health and Environmental Sciences Institute ran workshops in which attendees from pharmaceutical companies worked independently with tool developers, CROs, and regulatory agencies to replace thorough QT testing with enhanced in vitro methods for assessing cardiovascular toxicity.

Since then, much progress has been made among this multidisciplinary team to develop the Comprehensive in vitro Proarrhythmia Assay (CiPA), which is currently undergoing a validation program and promises to amend regulatory requirements for proarrhythmia assessments.

Another initiative in 2015 reviewed non-animal alternatives for acute systemic toxicity testing and explored ways to facilitate the implementation of in vitro alternatives. Involving input from representatives of international regulatory agencies, academia, nongovernmental organizations, and industry, the resulting strategy to achieve near-term progress was published earlier this year.

Studies have also started to demonstrate the preclinical value of in vitro biomimetic liver models for toxicity testing. For example, induced pluripotent stem cell-derived hepatocyte-like cells (iPSC-derived HLCs) are a few steps away from human clinical application, with great promise for in vitro drug toxicity screening because they have a sufficient metabolic profile and CYP activity. 

The future of in vitro toxicity testing

Promoting the adoption of in vitro toxicity testing is an important undertaking, so we should strive to overcome the barriers preventing its widespread adoption. Already, collaborative efforts have made progress in this regard, and research advances are increasingly demonstrating the potential of in vitro biomimetic liver models. As tool developers work more closely with regulatory authorities and pharmaceutical companies to drive innovation and commercial access, the more likely we will be able to identify ever better ways to protect our health.