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Jennifer DoudnaJennifer Doudna

PBD Faculty Scientist, Howard Hughes Investigator
Professor of Biochemistry & Molecular Biology, University of California, Berkeley

Contact info:

Lawrence Berkeley National Laboratory
Physical Biosciences Division
One Cyclotron Road
Mailstop: 305 Hildebrand Hall
Berkeley, California 94720
USA

Location: Building 11- room 0310  
Phone: (510) 643-0225
Fax: (510) 643-0080 
Email: JDoudna@lbl.gov

Research Emphasis

RNA forms a variety of complex globular structures, some of which function like enzymes or form functional complexes with proteins. There are three major areas of focus in the lab: catalytic RNA, the function of RNA in the signal recognition particle and the mechanism of RNA-mediated internal initiation of protein synthesis. We are interested in understanding and comparing catalytic strategies used by RNA to those of protein enzymes, focusing on intron splicing and the self-cleaving RNA from hepatitis delta virus (HDV), a human pathogen. We are also investigating RNA-mediated initiation of protein synthesis, focusing on the internal ribosome entry site (IRES) RNA from Hepatitis C virus. Cryo-EM, x-ray crystallography and biochemical experiments are focused on understanding the structure and mechanism of the IRES and its amazing ability to hijack the mammalian ribosome and associated translation factors. A third area of focus in the lab is the signal recognition particle, which contains a highly conserved RNA required for targeting proteins for export out of cells. Each of these projects seeks to understand the molecular basis for RNA function, using a combination of structural, biophysical and biochemical approaches.

Publications