IUCRP UC Discovery Gr ant success story UC Discovery Gr Fighting Malaria: Creating cheap, simple microbial drug factories Worldwide, nearly two million people die of
this same drug production method can be used
malaria every year. Unfortunately, the most widely
to manufacture many other compounds from
available, affordable anti-malarial drugs are based
the isoprenoid family, including terpene-based
on chloroquine, and the Plasmodium parasite that
fragrances and flavors. Steve del Cardayre is
causes malaria has developed resistance to it.
Product Manager-Fermentation at Codexis the
Drugs based on an ancient Chinese extract of the
spinoff of Maxygen that is pursuing the research
plant Sweet Wormwood, or Artemisia annua, are
with Keasling. He says that the UC Discovery
more effective, but they are too expensive for
Grant gave the company a valuable opportunity to
undertake exploratory and fairly high risk research
and validate their approach to producing these
value-added products. According to del Cardayre,
the product lines “looked good on paper” but
the science was at such an early stage it was not
possible for the firm to make an informed decision
about investing in an all-out R&D program.
Keasling’s work showed that the science works
but alerted Codexis to the substantial additional
investment required to actually develop and
commercialize fragrance and flavor products.
They decided not to pursue in-house development
of the products and redirected their efforts to
marketing the tools developed in their research
Dr. Jay Keasling
partnership with Keasling as part of their
gen, a California-based biotechnology company,
have come up with a way to do just that. Through
Del Cardayre emphasizes that the UC Discovery
a research partnership funded by a UC Discovery
Grant gave them a valuable opportunity to
Grant, Keasling and Maxygen modified the bacteri-
undertake the exploratory research that both
um Escherichia coli to produce complex chemicals
validated the approach and showed the expense
with medicinal qualities. The bacterium can now
to be prohibitive. It saved them from making
produce amorphadiene, a precursor to the anti-
substantial investment in something that
malaria drug artemisinin — the active ingredient in
ultimately would prove to expensive to pursue.
Sweet Wormwood extracts— and the most difficult
In addition to substantial cost savings that freed
up internal R&D resources for other strategic
targetes, the project added a new technology to
To produce amorphadiene in E. coli, Keasling and
his research team inserted a combination of genes
from E. coli, yeast, and Sweet Wormwood into
the host bacterium to construct an entirely new
metabolic pathway. The modified bacterium now
converts inexpensive sugars into large quantities of
amorphadiene. By cloning one or two more genes Industry Sponsor: Maxygen, Inc. (later acquired by Codexis, Inc.)
from Sweet Wormwood, it will be possible to produce
large quantities of artemisinin inexpensively.
Prof. Jay Keasling, Chemical Engineering, UC Berkeley
Title: Metabolic Engineering of Microorganisms for Sesquiterpene
What’s in it for the California economy? Well,
Grant #: (Bio99-10044) Grant Period: 9/1/2000-8/31/2002
Grant #: (biostar 01-10223) Grant Period: 8/13/2002-8/12/2003
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