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G-quadruplex formation enhances splicing efficiency of PAX9 intron 1

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Abstract

G-quadruplexes are secondary structures present in DNA and RNA molecules, which are formed by stacking of G-quartets (i.e., interaction of four guanines (G-tracts) bounded by Hoogsteen hydrogen bonding). Human PAX9 intron 1 has a putative G-quadruplex-forming region located near exon 1, which is present in all known sequenced placental mammals. Using circular dichroism (CD) analysis and CD melting, we showed that these sequences are able to form highly stable quadruplex structures. Due to the proximity of the quadruplex structure to exon–intron boundary, we used a validated double-reporter splicing assay and qPCR to analyze its role on splicing efficiency. The human quadruplex was shown to have a key role on splicing efficiency of PAX9 intron 1, as a mutation that abolished quadruplex formation decreased dramatically the splicing efficiency of human PAX9 intron 1. The less stable, rat quadruplex had a less efficient splicing when compared to human sequences. Additionally, the treatment with 360A, a strong ligand that stabilizes quadruplex structures, further increased splicing efficiency of human PAX9 intron 1. Altogether, these results provide evidences that G-quadruplex structures are involved in splicing efficiency of PAX9 intron 1.

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Acknowledgments

The authors thank Dr Nilva Cervigne for helpful discussions. Also, thank Dr Ana Carolina Migliorini Figueira and Spectroscopy and Calorimetry Facility at Brazilian Biosciences National Laboratory (LNBio), CNPEM, Campinas, Brazil for their support with the use of Jasco J-810 spectropolarimeter (Easton, MD, USA) and GloMax® 96 Microplate Luminometer. This work was supported by Conselho Nacional de Desenvolvimento Científico e Tecnológico, CNPq.

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Correspondence to Mariana Martins Ribeiro or Sergio Roberto Peres Line.

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Ribeiro, M.M., Teixeira, G.S., Martins, L. et al. G-quadruplex formation enhances splicing efficiency of PAX9 intron 1. Hum Genet 134, 37–44 (2015). https://doi.org/10.1007/s00439-014-1485-6

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  • DOI: https://doi.org/10.1007/s00439-014-1485-6

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