Anybody drawing up a list of New England’s biotech companies that really broke through in 2009 would have to consider Forma Therapeutics. The Cambridge, MA-based startup has nailed down a $25.5 million Series B venture round, which means it has now raised a total of more than $50 million this year to support what it hopes will be an efficient new engine for discovering new drugs.
The second-round investment was led by a new backer, Lilly Ventures, and it included a pair of existing investors: the Novartis Option Fund and Bio One Capital of Singapore. Lexington, MA-based Cubist Pharmaceuticals (NASDAQ: [[ticker:CBST]]), a partner of Forma’s, also became a new equity investor by converting some debt it had previously extended to the smaller company.
We first wrote about Forma in January, when Ryan had the story about how its founders, a group of scientists from the Broad Institute of MIT and Harvard, raised $25 million in their first big financing. The company has been on a tear ever since, more than doubling in size to 85 employees, adding research sites in Connecticut and Singapore, clinching five partnerships with organizations interested in its drug discovery engine, and now raking in this latest venture round. The $50 million figure I cited in the first paragraph is actually a bit of an underestimate, because Forma has brought in even more cash from its partners, which isn’t being disclosed.
“It does feel good,” says Steven Tregay, Forma’s CEO. “It’s been a productive year.”
What Forma has that’s different, and which other companies and organizations want a piece of, is its method for discovering drugs against cancer, infections, and potentially a number of other diseases. Forma focuses particularly (though not exclusively) on developing drugs that aim for protein targets that have traditionally eluded the pharmaceutical industry, Tregay says.
The first piece of the system is a screening technology that allows Forma to look at how proteins interact, not just in the isolation of a lab dish, but in the broader and vastly more complicated context of the whole cell, Tregay says. The second element is based on computing models that look for the “hotspots” or binding pockets, on the protein of interest, to see just how realistic it is to make a drug against that target. Based on that information, Forma, has been building up a portfolio of novel compounds that can hit the targets, both to stock its own internal pipeline and for its partners, Tregay says.
If this sort of technology can be proven