Published August 29, 2006
| Version v1
Journal article
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Macronuclear genome sequence of the ciliate Tetrahymena thermophila, a model eukaryote
Creators
- Eisen, Jonathan A.1
- Coyne, Robert S.2
- Wu, Martin2
- Wu, Dongying2
- Thiagarajan, Mathangi2
- Wortman, Jennifer R.2
- Badger, Jonathan H.2
- Ren, Qinghu2
- Amedeo, Paolo2
- Jones, Kristie M.2
- Tallon, Luke J.2
- Delcher, Arthur L.3
- Salzberg, Steven L.3
- Silva, Joana C.2
- Haas, Brian J.2
- Majoros, William H.4
- Farzad, Maryam2
- Carlton, Jane M.5
- Smith Jr., Roger K.2
- Garg, Jyoti6
- Pearlman, Ronald E.6
- Elde, Nels C.7
- Turkewitz, Aaron P.7
- 1. University of California Davis
- 2. The Institute for Genomic Research
- 3. University of Maryland
- 4. Duke University
- 5. New York University
- 6. York University
- 7. University of Chicago
Description
The ciliate Tetrahymena thermophila is a model organism for molecular and cellular biology. Like other ciliates, this species has separate germline and soma functions that are embodied by distinct nuclei within a single cell. The germline-like micronucleus (MIC) has its genome held in reserve for sexual reproduction. The soma-like macronucleus (MAC), which possesses a genome processed from that of the MIC, is the center of gene expression and does not directly contribute DNA to sexual progeny. We report here the shotgun sequencing, assembly, and analysis of the MAC genome of T. thermophila, which is approximately 104 Mb in length and composed of approximately 225 chromosomes. Overall, the gene set is robust, with more than 27,000 predicted protein-coding genes, 15,000 of which have strong matches to genes in other organisms. The functional diversity encoded by these genes is substantial and reflects the complexity of processes required for a free-living, predatory, single-celled organism. This is highlighted by the abundance of lineage-specific duplications of genes with predicted roles in sensing and responding to environmental conditions (e.g., kinases), using diverse resources (e.g., proteases and transporters), and generating structural complexity (e.g., kinesins and dyneins). In contrast to the other lineages of alveolates (apicomplexans and dinoflagellates), no compelling evidence could be found for plastid-derived genes in the genome. UGA, the only T. thermophila stop codon, is used in some genes to encode selenocysteine, thus making this organism the first known with the potential to translate all 64 codons in nuclear genes into amino acids. We present genomic evidence supporting the hypothesis that the excision of DNA from the MIC to generate the MAC specifically targets foreign DNA as a form of genome self-defense. The combination of the genome sequence, the functional diversity encoded therein, and the presence of some pathways missing from other model organisms makes T. thermophila an ideal model for functional genomic studies to address biological, biomedical, and biotechnological questions of fundamental importance. © 2006 Eisen et al.
Notes
Due to the large number of authors, only the first 20 and the University of Chicago authors are included on the above author list. Please download the article for the complete list of authors.
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Additional details
Identifiers
- DOI
- 10.1371/journal.pbio.0040286
- Other
- oai:uchicago.tind.io:10903
Funding
- National Science Foundation
- Microbial Genome Sequencing Program
- National Institute of General Medical Sciences
- R01 GM067012–03
- National Center for Research Resources
- Protist EST Project and grant
- National Science Foundation
- MCB-0132675