Focused on elucidating the mechanisms of evolution at the molecular and population-genetic levels, this project involves an integration of theory development and experimental work performed in a phylogenetic comparative manner. The molecular/cellular level focus is on the rate of error production via DNA replication, mRNA transcription, and protein translation in ~50 bacterial and eukaryotic species. This work seeks to test the drift-barrier hypothesis, which postulates that the level of refinement that natural selection can achieve with any trait is limited by the power of random drift and inversely proportional to the effective population size. Measures of replication-fidelity derive from mutation accumulation in long-term sets of serially bottlenecked replicate lines followed by whole-genome sequencing. Newly developed methods will yield parallel estimates of the much higher rates at which inappropriate ribonucleotides appear in mRNAs and erroneous amino acids are incorporated into proteins, allowing evaluation of whether negative associations exist between error propagation at these two levels. The population-genetic mechanisms of evolution will be clarified via a project to sequence 5000 genomes from geographically widespread isolates of the model microcrustacean Daphnia pulex, as well as from smaller numbers of key outgroup species. Combined with information on the fine-scaled pattern of recombination, this study will reveal the relative magnitudes of drift, mutation, and recombination in a collection of ~60 populations, a survey far beyond that for any other species. This will enable a test of the hypothesis that variation at the level of gene structure and genomic architecture is directly driven by the local population-genetic environment. The D. pulex system also has unique features for gaining insights into two major unsolved mysteries in evolutionary genetics: the origin and long-term effects of introns in protein-coding genes, and the causes and consequences of the loss of meiotic recombination. Relevance to human health. Because mutation is the source of all variation upon which natural selection acts, provides the fuel for the emergence of pathogens, and is the ultimate cause of genetic disorders and cancer, our work on replication fidelity has broad significance for diverse human-health issues. Because transcription and translation errors lead to cellular toxicity and protein aggregation, work at these levels also has significant applied implications. Finally, for the first time, the 5000 Genomes Project will reveal how population evolutionary features are defined by the relative power of drift, mutation and recombination, yielding insight into the factors driving the efficiencies and mechanisms by which all species respond to natural selection. Elucidation of the molecular/cellular mechanisms by which meiotic production of haploid eggs requiring fertilization is converted to ameiotic production of diploid eggs is highly desirable as it would open up possibilities of clonal propagation in diverse species.

Public Health Relevance

This project is focused on the molecular-genetic mechanisms associated with the production of variation in organismal diversity, and the consequences for organismal fitness. The research will generate a comprehensive empirical and theoretical understanding of the rates at which cellular errors arise at the DNA, RNA, and protein levels, and reveal the degree to which heritable mutations of various types and recombination rates have negative vs. positive fitness effects.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Unknown (R35)
Project #
5R35GM122566-04
Application #
9693268
Study Section
Special Emphasis Panel (ZGM1)
Program Officer
Janes, Daniel E
Project Start
2017-05-01
Project End
2022-04-30
Budget Start
2019-05-01
Budget End
2020-04-30
Support Year
4
Fiscal Year
2019
Total Cost
Indirect Cost
Name
Arizona State University-Tempe Campus
Department
Miscellaneous
Type
Organized Research Units
DUNS #
943360412
City
Tempe
State
AZ
Country
United States
Zip Code
85287
Long, Hongan; Doak, Thomas G; Lynch, Michael (2018) Limited Mutation-Rate Variation Within the Paramecium aurelia Species Complex. G3 (Bethesda) 8:2523-2526
Long, Hongan; Miller, Samuel F; Williams, Emily et al. (2018) Specificity of the DNA Mismatch Repair System (MMR) and Mutagenesis Bias in Bacteria. Mol Biol Evol 35:2414-2421
Jiang, Xiaoqian; Tang, Haixu; Mohammed Ismail, Wazim et al. (2018) A Maximum-Likelihood Approach to Estimating the Insertion Frequencies of Transposable Elements from Population Sequencing Data. Mol Biol Evol 35:2560-2571
Long, Hongan; Sung, Way; Kucukyildirim, Sibel et al. (2018) Evolutionary determinants of genome-wide nucleotide composition. Nat Ecol Evol 2:237-240
Lynch, Michael (2018) Phylogenetic divergence of cell biological features. Elife 7:
Ackerman, Matthew S; Johri, Parul; Spitze, Ken et al. (2017) Estimating Seven Coefficients of Pairwise Relatedness Using Population-Genomic Data. Genetics 206:105-118
Dillon, Marcus M; Sung, Way; Sebra, Robert et al. (2017) Genome-Wide Biases in the Rate and Molecular Spectrum of Spontaneous Mutations in Vibrio cholerae and Vibrio fischeri. Mol Biol Evol 34:93-109
Gout, Jean-Francois; Li, Weiyi; Fritsch, Clark et al. (2017) The landscape of transcription errors in eukaryotic cells. Sci Adv 3:e1701484
Tincher, Clayton; Long, Hongan; Behringer, Megan et al. (2017) The Glyphosate-Based Herbicide Roundup Does not Elevate Genome-Wide Mutagenesis of Escherichia coli. G3 (Bethesda) 7:3331-3335
Lynch, Michael; Gutenkunst, Ryan; Ackerman, Matthew et al. (2017) Population Genomics of Daphnia pulex. Genetics 206:315-332

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