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July 11, 2011 - Volume 89, Number 28
- p. 8
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Forensic Chemistry: A new method could increase the number of explosives detected by airport screeners.
Trade: U.S. companies complain of market dumping by China.
Layoffs follow similar moves by Amgen, AstraZeneca.
Environment: Ban to halt export of hazardous waste to developing world.
Penrose (Parney) Albright will direct DOE national lab.
Toxic Exposure: Mercury isotopes in human hair illuminate dietary and industrial sources.
Cancer Biochemistry: Mass spectrometry follows the metabolism of very long fatty acids in cancer cells.
In a major step toward achieving one of the key unsolved problems of structural biochemistry, the crystal structure of a large part of the yeast Mediator protein complex has been determined.
Found in eukaryotes from yeast to humans, Mediator plays a role in the expression of genes and their transcription into mRNA. The structure will help researchers learn more about how it assembles from constituent proteins and how it works at a molecular level, which has been largely unknown. The work could also aid discovery of drugs that control gene expression by targeting Mediator, just as some antibiotics target the ribosome.
Transcription factors known as activators regulate gene expression by binding to gene-promoter regions and encouraging RNA polymerase II-catalyzed transcription of the genetic code into mRNA. In 1990, a group led by Roger D. Kornberg of Stanford University School of Medicine found that an enormous protein complex they called Mediator was responsible for passing instructions from activators to RNA polymerase II.
Scientists have chased Mediator’s makeup ever since, but the best structures to date have included only two or three subunits; whereas yeast Mediator has 21 and those of higher eukaryotes have more. Now, biochemist Yuichiro Takagi of Indiana University School of Medicine and coworkers have crystallized and structurally analyzed yeast Mediator’s seven-subunit “head,” a component essential to its activity (Nature, DOI: 10.1038/nature10162).
A surprising revelation is that 10 α-helices are shared by five of the head’s subunits—the first such bundle found to originate from so many proteins, the researchers note. The structure provides clues about how Mediator assembles, how it’s stabilized, and how it works.
“Mediator function is central to all or most RNA polymerase II transcriptional regulation, but its mechanisms are only just being worked out,” comments RNA polymerase II expert Joan Conaway of Stowers Institute for Medical Research, Kansas City. “This structure is a really big deal because it should enable and guide the rational design of experiments to discover possible mechanisms.”
Challenges remain: Mediator’s “middle” and “tail” have yet to be determined, the structure’s 4.3-Å resolution isn’t sufficient to resolve atoms, and parts of the head aren’t included in the model.
But the structure is a major achievement “because Takagi and coworkers had to express the subunits, assemble the head module, and then get crystals that would diffract,” says Mediator specialist Michel Werner of the Institute of Biology & Technology, in Saclay, France. “It shows how the subunits are arranged and helps in interpreting how Mediator recruits transcription factors to activate polymerase.” The work suggests it will eventually be possible to get a complete picture of the Mediator complex, he says.
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