Understanding the paradoxical mechanical response of in-phase A-tracts at different force regimes

Abstract A-tracts are A:T rich DNA sequences that exhibit unique structural and mechanical properties associated with several functions in vivo. The crystallographic structure of A-tracts has been well characterized. However, the mechanical properties of these sequences is controversial and their re...

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Veröffentlicht in:Nucleic acids research 2020-05, Vol.48 (9), p.5024-5036
Hauptverfasser: Marin-Gonzalez, Alberto, Pastrana, Cesar L, Bocanegra, Rebeca, Martín-González, Alejandro, Vilhena, J G, Pérez, Rubén, Ibarra, Borja, Aicart-Ramos, Clara, Moreno-Herrero, Fernando
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Sprache:eng
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Zusammenfassung:Abstract A-tracts are A:T rich DNA sequences that exhibit unique structural and mechanical properties associated with several functions in vivo. The crystallographic structure of A-tracts has been well characterized. However, the mechanical properties of these sequences is controversial and their response to force remains unexplored. Here, we rationalize the mechanical properties of in-phase A-tracts present in the Caenorhabditis elegans genome over a wide range of external forces, using single-molecule experiments and theoretical polymer models. Atomic Force Microscopy imaging shows that A-tracts induce long-range (∼200 nm) bending, which originates from an intrinsically bent structure rather than from larger bending flexibility. These data are well described with a theoretical model based on the worm-like chain model that includes intrinsic bending. Magnetic tweezers experiments show that the mechanical response of A-tracts and arbitrary DNA sequences have a similar dependence with monovalent salt supporting that the observed A-tract bend is intrinsic to the sequence. Optical tweezers experiments reveal a high stretch modulus of the A-tract sequences in the enthalpic regime. Our work rationalizes the complex multiscale flexibility of A-tracts, providing a physical basis for the versatile character of these sequences inside the cell.
ISSN:0305-1048
1362-4962
DOI:10.1093/nar/gkaa225