Programmed Chromosome Deletion in the Ciliate .

G3 (Bethesda)

Departments of Biochemistry and Molecular Biophysics and Biological Sciences, Columbia University, New York, NY and

Published: October 2019

AI Article Synopsis

  • The ciliate organism has two types of nuclei: a germline micronucleus with about 100 large chromosomes and a somatic macronucleus with numerous smaller "nanochromosomes."
  • During sexual reproduction, the micronucleus transforms into a macronucleus through a complex DNA rearrangement process, which is influenced by RNA-based pathways that govern epigenetic inheritance.
  • Introducing synthetic DNA that matches a native nanochromosome leads to its deletion and the loss of associated gene expression, revealing remnants with telomeres; these changes can be inherited and suggest a novel method for studying genome rearrangement and gene knockouts.

Article Abstract

The ciliate contains two nuclei: a germline micronucleus and a somatic macronucleus. These two nuclei diverge significantly in genomic structure. The micronucleus contains approximately 100 chromosomes of megabase scale, while the macronucleus contains 16,000 gene-sized, high ploidy "nanochromosomes." During its sexual cycle, a copy of the zygotic germline micronucleus develops into a somatic macronucleus via DNA excision and rearrangement. The rearrangement process is guided by multiple RNA-based pathways that program the epigenetic inheritance of sequences in the parental macronucleus of the subsequent generation. Here, we show that the introduction of synthetic DNA molecules homologous to a complete native nanochromosome during the rearrangement process results in either loss or heavy copy number reduction of the targeted nanochromosome in the macronucleus of the subsequent generation. This phenomenon was tested on a variety of nanochromosomes with different micronuclear structures, with deletions resulting in all cases. Deletion of the targeted nanochromosome results in the loss of expression of the targeted genes, including gene knockout phenotypes that were phenocopied using alternative knockdown approaches. Further investigation of the chromosome deletion showed that, although the full length nanochromosome was lost, remnants of the targeted chromosome remain. We were also able to detect the presence of telomeres on these remnants. The chromosome deletions and remnants are epigenetically inherited when backcrossed to wild type strains, suggesting that an undiscovered mechanism programs DNA elimination and cytoplasmically transfers to both daughter cells during conjugation. Programmed deletion of targeted chromosomes provides a novel approach to investigate genome rearrangement and expands the available strategies for gene knockout in .

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6778801PMC
http://dx.doi.org/10.1534/g3.118.200930DOI Listing

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