Literature DB >> 28818035

Comparative analysis of inosine-substituted duplex DNA by circular dichroism and X-ray crystallography.

Justin P Peters1, Ewa A Kowal2, Pradeep S Pallan2, Martin Egli2, L James Maher1.   

Abstract

Leveraging structural biology tools, we report the results of experiments seeking to determine if the different mechanical properties of DNA polymers with base analog substitutions can be attributed, at least in part, to induced changes from classical B-form DNA. The underlying hypothesis is that different inherent bending and twisting flexibilities may characterize non-canonical B-DNA, so that it is inappropriate to interpret mechanical changes caused by base analog substitution as resulting simply from 'electrostatic' or 'base stacking' influences without considering the larger context of altered helical geometry. Circular dichroism spectra of inosine-substituted oligonucleotides and longer base-substituted DNAs in solution indicated non-canonical helical conformations, with the degree of deviation from a standard B-form geometry depending on the number of I⋅C pairs. X-ray diffraction of a highly inosine-substituted DNA decamer crystal (eight I⋅C and two A⋅T pairs) revealed an A-tract-like conformation with a uniformly narrow minor groove, reduced helical rise, and the majority of sugars adopting a C1'-exo (southeastern) conformation. This contrasts with the standard B-DNA geometry with C2'-endo sugar puckers (south conformation). In contrast, the crystal structure of a decamer with only four I⋅C pairs has a geometry similar to that of the reference duplex with eight G⋅C and two A⋅T pairs. The unique crystal geometry of the inosine-rich duplex is noteworthy given its unusual CD signature in solution and the altered mechanical properties of some inosine-containing DNAs.

Entities:  

Keywords:  A-tracts; B-DNA; DNA topology; X-ray crystallography; circular dichroism; inosine; metal ion coordination; sequence-dependent helix geometry

Mesh:

Substances:

Year:  2017        PMID: 28818035      PMCID: PMC6251417          DOI: 10.1080/07391102.2017.1369164

Source DB:  PubMed          Journal:  J Biomol Struct Dyn        ISSN: 0739-1102


  81 in total

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Authors:  Tomáš Dršata; Nada Špačková; Petr Jurečka; Marie Zgarbová; Jiří Šponer; Filip Lankaš
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