Among the various clay minerals, sepiolite, which is a natural fibrous silicate, isa potential promising nanocarrier for the non-viral transfer of bio-molecules. Indeed,sepiolite has been shown to interact with biological molecules such as lipids,polysaccharides and proteins. Here, we show that sepiolite efficiently binds differenttypes of DNA molecules (genomic, plasmid, single strand and double strandoligonucleotides), introducing the first detailed study on the interaction mechanismsbetween sepiolite and DNA, as well as the physicochemical characterization of theresulting DNA-sepiolite bionanocomposites. The interaction mechanisms aresuggested to be electrostatic interactions, van der Waals forces, cation bridges, andhydrogen bonding. Spectroscopy analysis showed that the binding of DNA to sepiolitewas increased by polycations with valence dependent efficiency, and the DNApreviously adsorbed could be recovered with an efficiency that could be modulatedusing a chelating agent (EDTA), preserving the DNA structure and biological activity.Fourier-transform infrared spectroscopy identified the external silanol groups as themain sites of interaction with the DNA. It was proved that it is possible to use sepiolitefor extracting DNA from bacteria, for DNA purification and for purification from bacterialcontamination. By combining fluorescence microscopy, transmission electronmicroscopy (TEM), time-lapse video microscopy and flow cytometry analysis (FACS),we show that sepiolite can be spontaneously internalized into mammalian cells throughboth endocytic and non-endocytic pathways. As a proof of concept, we show thatsepiolite is able to stably transfer plasmid DNA into bacteria and mammalian cells. Itwas also proved that with the incubation of bacteria with the Sep/DNAbionanocomposite initially prepared in the presence of a low concentration of divalentcation, and using sonicated sepiolite (sSep), it is possible to increase the bacterialtransformation efficiency from 20 to 30-fold compared to previously reported methodswhich are based in the “Yoshida effect”. Additionally, we show that the efficiency ofsepiolite-mediated gene transfer can be optimized: the use of sSep and the exposureto the endosome disrupter chloroquine 100-fold and 2-fold stimulated DNA transfectionefficiency, respectively. These results open the way to the use of sepiolite-basedbionanocomposites as a novel class of hybrid nanocarriers for both potential genetherapy and the development of novel biological models of interest for academic andapplied sciences.