Pharmaceutical companies like Pfizer have vast amounts of human genetic data (GWAS hits) linked to diseases but struggle to determine which are viable drug targets. Gordian's high-throughput in vivo screening directly tests the causal effects of hundreds of these targets, rapidly identifying the most promising candidates.
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Gordian Biotechnology embeds unique genetic "barcodes" into hundreds of different gene therapies. This transforms gene therapy from a treatment modality into a high-throughput screening tool, allowing them to test many potential drugs simultaneously inside a single living animal and trace which ones worked.
Instead of testing a single drug candidate in cheap models before moving to expensive ones, Gordian's parallel testing platform makes it cost-effective to use clinically relevant large animals, like horses, at the very beginning of the discovery process. This flips the traditional R&D funnel on its head.
Genomics (DNA/RNA) only provides the 'sheet music' for cancer. Functional Precision Medicine acts as the orchestra, testing how live tumor cells respond to drugs in real time. AI serves as the conductor, optimizing the 'performance' for superior outcomes.
Inspired by the broad benefits of drugs like GLP-1s, Gordian is proactively creating "atlases" of target effects across multiple organs (heart, kidney, liver). This strategy positions them to discover the next class of drugs that treat multiple related conditions simultaneously, a key focus for their internal pipeline.
While AI excels where large, clean datasets exist (like protein folding), it struggles with modeling slow, progressive diseases like Alzheimer's or obesity. These are organ-level phenomena, and the necessary data doesn't exist yet. In vivo platforms are critical for generating this required foundational data.
With over 5,000 oncology drugs in development and a 9-out-of-10 failure rate, the current model of running large, sequential clinical trials is not viable. New diagnostic platforms are essential to select drugs and patient populations more intelligently and much earlier in the process.
Unlike using genetically identical mice, Gordian tests therapies in large, genetically varied animals. This variation mimics human patient diversity, helping identify drugs that are effective across different biological profiles and addressing patient heterogeneity, a primary cause of clinical trial failure.
Traditional methods like crystallography are slow and analyze purified proteins outside their native environment. A-muto's platform uses proteomics and AI to analyze thousands of protein conformations in living disease models, capturing a more accurate picture of disease biology and identifying novel targets.
The company intentionally makes its early research "harder in the short term" by using complex, long-term animal models. This counterintuitive strategy is designed to generate highly predictive data early, thereby reducing the massive financial risk and high failure rate of the later-stage clinical trials.
Gordian uses AAV vectors to create a "mosaic" tissue where different cells receive different genetic perturbations. Single-cell transcriptomics then reveals the causal effects of each target in a complex, living environment, a massive speed advantage over traditional, single-target animal studies.