FB2024_03 , released April 23, 2024
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Citation
Hartig, J.V., Esslinger, S., Böttcher, R., Saito, K., Förstemann, K. (2009). Endo-siRNAs depend on a new isoform of loquacious and target artificially introduced, high-copy sequences.  EMBO J. 28(19): 2932--2944.
FlyBase ID
FBrf0209063
Publication Type
Research paper
Abstract
Colonization of genomes by a new selfish genetic element is detrimental to the host species and must lead to an efficient, repressive response. In vertebrates as well as in Drosophila, piRNAs repress transposons in the germ line, whereas endogenous siRNAs take on this role in somatic cells. We show that their biogenesis depends on a new isoform of the Drosophila TRBP homologue loquacious, which arises by alternative polyadenylation and is distinct from the one that functions during the biogenesis of miRNAs. For endo-siRNAs and piRNAs, it is unclear how an efficient response can be initiated de novo. Our experiments establish that the endo-siRNA pathway will target artificially introduced sequences without the need for a pre-existing template in the genome. This response is also triggered in transiently transfected cells, thus genomic integration is not essential. Deep sequencing showed that corresponding endo-siRNAs are generated throughout the sequence, but preferentially from transcribed regions. One strand of the dsRNA precursor can come from spliced mRNA, whereas the opposite strand derives from independent transcripts in antisense orientation.
PubMed ID
PubMed Central ID
PMC2760103 (PMC) (EuropePMC)
Related Publication(s)
Personal communication to FlyBase

Lai lab miRNA expression and conservation data for Drosophila.
Mohammed and Lai, 2016.2.8, Lai lab miRNA expression and conservation data for Drosophila. [FBrf0230987]

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Secondary IDs
    Language of Publication
    English
    Additional Languages of Abstract
    Parent Publication
    Publication Type
    Journal
    Abbreviation
    EMBO J.
    Title
    The EMBO Journal
    Publication Year
    1982-
    ISBN/ISSN
    0261-4189
    Data From Reference
    Genes (14)
    Physical Interactions (3)
    Cell Lines (1)
    Natural transposons (2)