Contrary to the popular belief that antibody development is a bespoke craft, modern methods enable a reproducible, systematic engineering process. This allows for predictable creation of antibodies with specific properties, such as matching affinity for human and animal targets, a feat once considered a "flight of fancy."
Related Insights
AI modeling transforms drug development from a numbers game of screening millions of compounds to an engineering discipline. Researchers can model molecular systems upfront, understand key parameters, and design solutions for a specific problem, turning a costly screening process into a rapid, targeted design cycle.
Breakthrough drugs aren't always driven by novel biological targets. Major successes like Humira or GLP-1s often succeeded through a superior modality (a humanized antibody) or a contrarian bet on a market (obesity). This shows that business and technical execution can be more critical than being the first to discover a biological mechanism.
The relationship between a multi-specific antibody's design and its function is often non-intuitive. LabGenius's ML platform excels by exploring this complex "fitness landscape" without human bias, identifying high-performing molecules that a rational designer would deem too unconventional or "crazy."
To overcome on-target, off-tumor toxicity, LabGenius designs antibodies that act like biological computers. These molecules "sample" the density of target receptors on a cell's surface and are engineered to activate and kill only when a specific threshold is met, distinguishing high-expression cancer cells from low-expression healthy cells.
Traditional antibody optimization is a slow, iterative process of improving one property at a time, taking 1-3 years. By using high-throughput data to train machine learning models, companies like A-AlphaBio can now simultaneously optimize for multiple characteristics like affinity, stability, and developability in a single three-month process.
Profluent CEO Ali Madani frames the history of medicine (like penicillin) as one of random discovery—finding useful molecules in nature. His company uses AI language models to move beyond this "caveman-like" approach. By designing novel proteins from scratch, they are shifting the paradigm from finding a needle in a haystack to engineering the exact needle required.
Many innovative drug designs fail because they are difficult to manufacture. LabGenius's ML platform avoids this by simultaneously optimizing for both biological function (e.g., potency) and "developability." This allows them to explore unconventional molecular designs without hitting a production wall later.
A significant, often overlooked, hurdle in drug development is that therapeutic antibodies bind differently to animal targets than human ones. This discrepancy can force excessively high doses in animal studies, leading to toxicity issues and causing promising drugs to fail before ever reaching human trials.
The future of biotech moves beyond single drugs. It lies in integrated systems where the 'platform is the product.' This model combines diagnostics, AI, and manufacturing to deliver personalized therapies like cancer vaccines. It breaks the traditional drug development paradigm by creating a generative, pan-indication capability rather than a single molecule.
Titus believes a key area for AI's impact is in bringing a "design for manufacturing" approach to therapeutics. Currently, manufacturability is an afterthought. Integrating it early into the discovery process, using AI to predict toxicity and scalability, can prevent costly rework.
