AUTHOR=Bhogadia Mohammed , Stone Beth , Del Villar Guerra Rafael , Muskett Frederick W. , Ghosh Sudipta , Taladriz-Sender Andrea , Burley Glenn A. , Eperon Ian C. , Hudson Andrew J. , Dominguez Cyril 

TITLE=Biophysical characterisation of the Bcl-x pre-mRNA and binding specificity of the ellipticine derivative GQC-05: Implication for alternative splicing regulation

JOURNAL=Frontiers in Molecular Biosciences

VOLUME=9

YEAR=2022

URL=https://www.frontiersin.org/journals/molecular-biosciences/articles/10.3389/fmolb.2022.943105

DOI=10.3389/fmolb.2022.943105

ISSN=2296-889X

ABSTRACT=<p>The BCL2L1 gene expresses two isoforms of Bcl-x protein via the use of either of two alternative 5′ splice sites (5′ss) in exon 2. These proteins have antagonistic actions, Bcl-X<sub>L</sub> being anti-apoptotic and Bcl-X<sub>S</sub> pro-apoptotic. In a number of cancers the Bcl-X<sub>L</sub> isoform is over-expressed, resulting in cancer cell survival and growth, so switching splicing to the X<sub>s</sub> isoform could have therapeutic benefits. We have previously proposed that a putative G-quadruplex (G4) exists downstream of the X<sub>S</sub> 5′ss and shown that the ellipticine derivative GQC-05, a previously identified DNA G4-specific ligand, induces an increase in the X<sub>S</sub>/X<sub>L</sub> ratio both <italic>in vitro</italic> and in cells. Here, we demonstrate that this G4 forms <italic>in vitro</italic> and that the structure is stabilised in the presence of GQC-05. We also show that GQC-05 binds RNA non-specifically in buffer conditions, but selectively to the Bcl-x G4 in the presence of nuclear extract, highlighting the limitations of biophysical measurements taken outside of a functional environment. We also demonstrate that GQC-05 is able to shift the equilibrium between competing G4 and duplex structures towards the G4 conformation, leading to an increase in accessibility of the X<sub>S</sub> 5′ss, supporting our previous model on the mechanism of action of GQC-05.</p>