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Microbial Genomics
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DOE Microbial Genome Program Awards 2001

Since its beginning in 1994, the DOE Microbial Genome Program has sparked a revolution in microbiology. From the publication by Craig Venter's group (then at The Institute for Genomic Research, TIGR) of the complete genome sequence of Haemophilus influenza, completed genome sequences of some 51 microbes have been published; sequencing of at least a dozen more are known to be complete but not yet published and sequencing projects of approximately 140 additional microbes are presently known to be in varying stages of progress. Activity in the private sector has also been intense. Sequencing technologies have progressed to the point where a high-throughput facility such as the DOE Joint Genome Institute can draft the sequence of a 2.5 Mb microbe in one day and draft about 65 Mb of microbial sequence (about 17-20 microbes) in one month.

These sequences are enabling a variety of new discoveries. These include new genes and pathways, as well as the insight that the horizontal transfer of genetic information may have been remarkably frequent in microbial evolution. An additional discovery is that even in the 470 gene sequence of the smallest known free-living microbe, Mycoplasma genitalium, perhaps as many as 100 - 150 of those genes are not required for life. One of the most repeatable and astonishing results is that even with numerous microbial genomes finished or nearly finished (and thus sufficient for gene analyses), about 50% of each genome characteristically is comprised of genes of unknown function. Microbes have been isolated (and their genomes sequenced) from environments characterized by extremely low pH, temperatures above boiling water, pressures greater than 200 atmospheres, highly toxic metal concentrations, high radiation fluxes, high salinity, and just about every other inhospitable condition imaginable. It is worth noting that most microbes do not cause diseases and, in fact, their important roles in maintaining the ecology of Earth are becoming clearer.

A completed microbial (or any other) genome represents the source code for life. More tangibly, it represents a list of the parts, working and structural, that a cell (or a multicellular organism) requires to exist and to function. For this reason, closely linked to the Microbial Genome Program, OBER has just launched the Microbial Cell Project. With the assistance of DOE's Offices of Basic Energy Sciences (BES) and Advanced Scientific Computing Research (ASCR), awards have been made initiating research into how microbial cells work and how high-throughput computational technologies can be exploited to model their functioning (see next story). OBER will support research to provide the fundamental understanding that will allow the use of these microbes to address the challenges of carbon sequestration, bioremediation, cellulose degradation, energy production, and biotechnology.

These new Microbial Genome awards represent a departure from the past. Instead of focusing on the high throughput production of new microbial genome sequence data, a mission now given over to the DOE Joint Genome Institute, the foci of the MGP has evolved towards post-genomic analyses. The five thrusts are: A) functional analyses of microbial genomes; B) bioinformatic tools for microbial genome analyses; C) studies of lateral gene transfers, including their frequency and biological constraints; D) novel technologies for genomic characterization; and E) studies of microbial consortia and communities. Of more than 70 applications to the program, 28 awards have been made.

In the area of functional studies, the new awards include:

In the area of bioinformatics tools, resources, and activities, the new projects include:

In the area of studies of horizontal gene transfers, the new projects include:

In the area of novel technologies, the new projects include:

In the area of studies of microbial consortia and hard-to-culture species, the new projects include:

The impact of the DOE Microbial Genome Program has been great. Genome sequencing projects are multiplying, not least because, with the approaching conclusion of the Human Genome Project, the US has considerable sequencing capacity that provides an immense opportunity for biology. In fact, our capacity to sequence outstrips our capacity to understand all the information in the sequences we have acquired. This is no reason to stop however; as the sequence database grows, so does its utility for comparative genomic purposes, for gene discovery, for understanding the biology of our environment, and perhaps most powerfully, for fueling the engine of biological science by generating testable hypotheses that will keep biologists busy for years to come.

Daniel Drell with contributions from John Houghton and Anna Palmisano (October, 2001).