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STEM CELLS AND REGENERATION
I-KCKT allows dissection-free RNA profiling of adult Drosophila intestinal progenitor cells
Kasun Buddika, Jingjing Xu, Ishara S. Ariyapala, Nicholas S. Sokol
Development 2021 148: dev196568 doi: 10.1242/dev.196568 Published 7 January 2021
Kasun Buddika
Department of Biology, Indiana University, Bloomington, IN 47405, USA
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Jingjing Xu
Department of Biology, Indiana University, Bloomington, IN 47405, USA
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Ishara S. Ariyapala
Department of Biology, Indiana University, Bloomington, IN 47405, USA
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Nicholas S. Sokol
Department of Biology, Indiana University, Bloomington, IN 47405, USA
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  • For correspondence: nsokol@indiana.edu

Handling Editor: Irene Miguel-Aliaga

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ABSTRACT

The adult Drosophila intestinal epithelium is a model system for stem cell biology, but its utility is limited by current biochemical methods that lack cell type resolution. Here, we describe a new proximity-based profiling method that relies upon a GAL4 driver, termed intestinal-kickout-GAL4 (I-KCKT-GAL4), that is exclusively expressed in intestinal progenitor cells. This method uses UV crosslinked whole animal frozen powder as its starting material to immunoprecipitate the RNA cargoes of transgenic epitope-tagged RNA binding proteins driven by I-KCKT-GAL4. When applied to the general mRNA-binder, poly(A)-binding protein, the RNA profile obtained by this method identifies 98.8% of transcripts found after progenitor cell sorting, and has low background noise despite being derived from whole animal lysate. We also mapped the targets of the more selective RNA binder, Fragile X mental retardation protein (FMRP), using enhanced crosslinking and immunoprecipitation (eCLIP), and report for the first time its binding motif in Drosophila cells. This method will therefore enable the RNA profiling of wild-type and mutant intestinal progenitor cells from intact flies exposed to normal and altered environments, as well as the identification of RNA-protein interactions crucial for stem cell function.

Footnotes

  • Competing interests

    The authors declare no competing or financial interests.

  • Author contributions

    Conceptualization: N.S.S.; Methodology: N.S.S., K.B., J.X.; Software: K.B.; Validation: I.S.A.; Formal analysis: K.B., I.S.A.; Investigation: K.B., J.X.; Writing - original draft: N.S.S., K.B.; Writing - review & editing: N.S.S., K.B.; Visualization: K.B.; Project administration: N.S.S.; Funding acquisition: N.S.S.

  • Funding

    We thank the National Institute of General Medical Sciences (R01GM124220) for financial support. Deposited in PMC for release after 12 months.

  • Data availability

    The PABP CLIP-seq and FMRP eCLIP-seq datasets from this study have been deposited in GEO under accession number GSE160128.

  • Supplementary information

    Supplementary information available online at https://dev.biologists.org/lookup/doi/10.1242/dev.196568.supplemental

  • Received August 31, 2020.
  • Accepted November 19, 2021.
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Keywords

  • CLIP
  • eCLIP
  • PABP
  • FMRP
  • Intestinal stem cell

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STEM CELLS AND REGENERATION
I-KCKT allows dissection-free RNA profiling of adult Drosophila intestinal progenitor cells
Kasun Buddika, Jingjing Xu, Ishara S. Ariyapala, Nicholas S. Sokol
Development 2021 148: dev196568 doi: 10.1242/dev.196568 Published 7 January 2021
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STEM CELLS AND REGENERATION
I-KCKT allows dissection-free RNA profiling of adult Drosophila intestinal progenitor cells
Kasun Buddika, Jingjing Xu, Ishara S. Ariyapala, Nicholas S. Sokol
Development 2021 148: dev196568 doi: 10.1242/dev.196568 Published 7 January 2021

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