|
|
 |
NEWS
INDEX
Archives
2005
April
By creating molecular 'bridge,'
scientists change function of a protein
Jim Barlow,
Life Sciences Editor
217-333-5802;jebarlow@uiuc.edu
 |
| Click
photo to enlarge |
| Photo
by Kwame Ross |
| Huimin
Zhao, left, a professor of chemical and biomedical
engineering, and graduate student Zhilei Chen have
changed the function of a protein using a co-evolution
approach. |
|
|
5/5/05
CHAMPAIGN, Ill. —
By designing a molecular bridge, scientists at the University of Illinois
at Urbana-Champaign have forged a successful pathway through a complex
ocean of barriers: They’ve changed the function of a protein using
a co-evolution approach.
In a study to be published in the Journal of Molecular Biology, doctoral
student Zhilei Chen and Huimin Zhao, a professor of chemical and biomolecular
engineering, describe what they call a “simple and efficient method
for creation of novel protein functions in an existing protein scaffold.”
In doing so, Zhao and Chen skirted the two time-and-labor-consuming
approaches tried repeatedly in the past decade: rational design, which
requires extensive knowledge of protein folding, structure, function
and dynamics; and directed evolution that mimics natural evolution in
a test tube but may require the screening of an astronomical number
of mutants for the creation of new protein functions.
“We now provide one possible solution to a long-lasting barrier
that is important in the protein engineering area – that is the
creation of the new protein functions,” Zhao said. “Our
approach is to build a bridge between the existing protein function
to the target new function by adding some intermediate functions followed
by stepwise directed evolution of these intermediate functions. If done,
it gives you the ability to create protein functions for any purpose
you want – as a catalyst to create new chemicals that might be
useful in such things as therapeutics, for example.”
By way of in-vitro co-evolution, the researchers gradually changed the
function of the human estrogen receptor alpha, a nuclear hormone receptor
mostly expressed in the prostate, ovary and urinary tract. What they
did was modify the estrogen receptor in a step-wise fashion, Zhao said.
They used testosterone and progesterone to build the bridge.
The receptor was gradually altered to accept one steroid, then another,
until accepting the desired one – corticosterone, a potent glucocoticoid.
In total, Zhao and Chen did four rounds of random mutagenesis and screened
about 1 million mutants before they found two estrogen receptor mutants
that can be activated by corticosterone. The whole process was done
in a couple of months.
The authors conclude that their new method may provide “a general
approach to engineering biomolecules and biosystems such as receptors,
enzymes, antibodies, ribosymes, DNAzymes and viruses with novel functions.”
Zhao is a member of the Institute for Genomic Biology and the Center
for Biophysics and Computational Biology at Illinois. He also is an
affiliate in the chemistry and bioengineering departments.
The National Science Foundation CAREER Award to Zhao helped to fund
the research.
|
|
|
|
