Machine learning points out why antibodies fail to stay on target, binding to molecules that aren’t markers of disease—and suggests better antibody designs.
Antibody treatments may be able to activate the immune system to fight diseases like Parkinson’s, Alzheimer’s, and colorectal cancer, but they are less effective when they bind with themselves and other molecules that aren’t markers of disease.
Peter Tessier (left) and Tiexin Wang (right) prepare antibodies to test how they bind to themselves and other molecules. The machine learning model developed by Tessier’s team could help drug developers design better antibody medicines. Image credit: Hye Jin Lee, Tessier Lab, University of Michigan
New machine-learning algorithms developed at the University of Michigan can highlight problem areas in antibodies that make them prone to binding non-target molecules.
“We can use the models to pinpoint the positions in antibodies that are causing trouble and change those positions to correct the problem without causing new ones,” said Peter Tessier, the Albert M. Mattocks Professor of Pharmaceutical Sciences at U-M and corresponding author of the study in Nature Biomedical Engineering.
“The models are useful because they can be used on existing antibodies, brand new antibodies in development, and even antibodies that haven’t been made yet.”
Working with medical devices – illustrative photo. Image credit: NCI
Antibodies fight disease by binding specific molecules called antigens on disease-causing agents—such as the spike protein on the virus that causes COVID-19. Once bound, the antibody either directly inactivates the harmful viruses or cells or signals the body’s immune cells to do so.
Unfortunately, antibodies designed to bind their specific antigens very strongly and quickly can also bind non-antigen molecules, which removes the antibodies before they target a disease.
Such antibodies are also prone to binding with other antibodies of the same type and, in the process, forming thick solutions that don’t flow easily through the needles that deliver antibody drugs.
“The ideal antibodies should do three things at once: bind tightly to what they’re supposed to, repel each other and ignore other things in the body,” Tessier said.
An antibody that doesn’t check all three boxes is unlikely to become a successful drug, but many clinical-stage antibodies can’t. In their new study, Tessier’s team measured the activity of 80 clinical-stage antibodies in the lab and found that 75% of the antibodies interacted with the wrong molecules, to one another, or both.
Changing the amino acids that comprise an antibody and in turn, the antibody’s 3D structure could prevent antibodies from misbehaving because an antibody’s structure determines what it can bind.
However, some changes could cause more problems than they fix, and the average antibody has hundreds of different amino acid positions that could be changed.
“Exploring all the changes for a single antibody takes about two workdays with our models, which is substantially shorter compared to experimentally measuring each modified antibody—which would take months, at best,” said Emily Makowski, a recent Ph.D. graduate in pharmaceutical sciences and the study’s first author.
The team’s models, trained on the experimental data they collected from clinical-stage antibodies, can identify how to change antibodies so they check all three boxes with 78% to 88% accuracy. This narrows down the number of antibody changes that chemical and biomedical engineers need to manufacture and test in the lab.
“Machine learning is key for accelerating drug development,” said Tiexin Wang, a doctoral student in chemical engineering and study co-author.
Biotech companies are already beginning to recognize machine learning’s potential to optimize the next generation of therapeutic antibodies.
“Some companies have developed antibodies that they are excited about because they have a desired biological activity, but they know they are going to have problems when they try to use these antibodies as drugs,” Tessier said.
“That’s where we come in and show them the specific spots in their antibodies that need to be fixed, and we are already helping some companies do this.”
Source: University of Michigan