Abstract
Over the past decade, about one-fifth of FDA-approved drugs each year involve novel mechanism-of-action human targets. Although riskier than modulating well-known targets, these therapies address unmet needs and strengthen sector innovation. The Open Targets Platform is a valuable open resource for identifying novel targets, integrating diverse datasets with regular updates and a user-friendly interface. To expand its capabilities, we implement comprehensive timestamping across millions of biomedical data points and introduce a target novelty metric for disease contexts, enabling discovery of novel targets within the ecosystem. We also present a retrospective analysis of novel drug target approvals over two decades, revealing a shift around 2015: supportive biomedical evidence (e.g., human genetics, literature-derived insights, differential expression, and pathway data) increasingly appears before rather than after the approval year. These findings underscore the importance of time-based evidence assessments for earlier identification of novel clinical opportunities and offer guidance for future target selection trends.