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Insights into ribosomal DNA dominance and magnification through characterization of isogenic deletion alleles. | LitMetric

AI Article Synopsis

  • The primary ribosomal RNA (rRNA) genes are found in large tandem repeats across all organisms, causing instability that can affect gene copy numbers, but the specific conditions influencing this remain unclear.
  • Targeted damage to the rRNA genes on the Y chromosome revealed that complete loss of rDNA results in lethal effects in Drosophila after embryogenesis, hindering larval development.
  • The study also explored how the presence of retrotransposons-R1 and R2 is linked to rDNA copy number, revealing a complex relationship between X- and Y-linked rDNA and suggesting a connection between nucleolar dominance and amplification of rDNA in Drosophila.

Article Abstract

The major loci for the large primary ribosomal RNA (rRNA) genes (35S rRNAs) exist as hundreds to thousands of tandem repeats in all organisms and dozens to hundreds in Drosophila. The highly repetitive nature of the ribosomal DNA (rDNA) makes it intrinsically unstable, and many conditions arise from the reduction in or magnification of copy number, but the conditions under which it does so remain unknown. By targeted DNA damage to the rDNA of the Y chromosome, we created and investigated a series of rDNA alleles. We found that complete loss of rDNA leads to lethality after the completion of embryogenesis, blocking larval molting and metamorphosis. We find that the resident retrotransposons-R1 and R2-are regulated by active rDNA such that reduction in copy number derepresses these elements. Their expression is highest during the early first instar, when loss of rDNA is lethal. Regulation of R1 and R2 may be related to their structural arrangement within the rDNA, as we find they are clustered in the flanks of the nucleolus organizing region (NOR; the cytological appearance of the rDNA). We assessed the complex nucleolar dominance relationship between X- and Y-linked rDNA using a histone H3.3-GFP reporter construct and incorporation at the NOR and found that dominance is controlled by rDNA copy number as at high multiplicity the Y-linked array is dominant, but at low multiplicity the X-linked array becomes derepressed. Finally, we found that multiple conditions that disrupt nucleolar dominance lead to increased rDNA magnification, suggesting that the phenomena of dominance and magnification are related, and a single mechanism may underlie and unify these two longstanding observations in Drosophila.

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Source
http://dx.doi.org/10.1093/genetics/iyae063DOI Listing

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