Data di Pubblicazione:
2016
Abstract:
Nuclear aggregates of polyamines (NAPs) are supramolecular compounds generated by the self-assembly of protonated
nuclear polyamines (spermine, spermidine and putrescine) and phosphate ions. In the presence of genomic DNA, the hierarchical
process of self-structuring ultimately produces nanotube-like polymers that envelop the double helix. Because
of their modular nature and their aggregation-disaggregation dynamics, NAPs confer plasticity and flexibility to DNA.
Through the disposition of charges, NAPs also enable a bidirectional stream of information between the genome and interacting
moieties.
High mobility group (HMG) B1 is a non-histone chromosomal protein that binds to DNA and that influences
multiple nuclear processes. Because genomic DNA binds to either NAPs or HMGB1 protein, we explored the ability
of in vitro self-assembled NAPs (ivNAPs) to mediate the DNA-HMGB1 interaction. To this end, we structured
DNA-NAPs-HMGB1 and DNA-HMGB1-NAPs ternary complexes in vitro through opportune sequential incubations.
Mobility shift electrophoresis and atomic force microscopy showed that the DNA-ivNAPs-HGMB1 complex had conformational
assets supposedly more suitable those of the DNA-HGMB1-ivNAPs to comply with the physiological and
functional requirements of DNA. Our findings indicated that ivNAPs act as mediators of the DNA-HMGB1 interaction.
Tipologia CRIS:
01.01 Articolo in rivista
Keywords:
Nuclear aggregates of polyamines; HMGB1; EMSA; Atomic force microscopy; DNA conformational transitions; Supramolecular nanotubes
Elenco autori:
D'Agostino, Luciano; Iacomino, Giuseppe; Picariello, Gianluca
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