"The project has been marked by a combination of meaningful advances, a spinoff publication of partial results, and methodological pitfalls.
In regard to aim (1), I have exceeded my ambitious goals, and already nearly completed Next-Generation Sequencing (NGS) data acquisition from a vast collection of experimental populations for the population genomics analysis. Similarly, I have re-generated high-coverage NGS data for the founder parental lines of the experimental populations; something not originally envisioned at the beginning of the project, but became necessary for a proper analysis of low-frequency rDNA variants. An analysis of genetic variation in 5S rDNAs in Arabidopsis 1001 genomes spun into a collaboration with the group of Dr. Aline Probst from the ""Genetic Development and Reproduction” (GReD) research unit in Clermont-Ferrand (France), and has been recently published in the journal Nucleic Acids Research (Simon et al., 2018; doi: 10.1093/nar/gky163).
In regard to the methodological aim (2), the work has been postponed, because new, optimized vectors have been assembled by the host lab for CRISPR-Cas9 induced-mutations, to streamline the isolation of transgene-free events. In parallel, an amplicon NGS based pipeline for rapid identification of mutations in hundreds of lines has been built. Both are now fully operational, and I can start with the proposed mutagenesis scheme.
In regard to aim (3), I am only waiting for the conclusions derived from the analysis in aim 1 to select a subset of strains for the experimental evolution study.
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