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G-Quadruplex Recognition by DARPIns through Epitope/Paratope Analogy**
Authors:Tom Miclot  Dr. Emmanuelle Bignon  Prof. Alessio Terenzi  Prof. Stéphanie Grandemange  Prof. Giampaolo Barone  Prof. Antonio Monari
Affiliation:1. Department of Biological, Chemical and Pharmaceutical Sciences and Technologies, Università degli Studi di Palermo, Viale delle Scienze, 90128 Palermo, Italy;2. Université de Lorraine and CNRS LPCT UMR 7019, 54000 Nancy, France;3. Université de Lorraine and CNRS CRAN UMR 7039, 54000 Nancy, France
Abstract:We investigated the mechanisms leading to the specific recognition of Guanine Guadruplex (G4) by DARPins peptides, which can lead to the design of G4 s specific sensors. To this end we carried out all-atom molecular dynamic simulations to unravel the interactions between specific nucleic acids, including human-telomeric (h-telo), Bcl-2, and c-Myc, with different peptides, forming a DARPin/G4 complex. By comparing the sequences of DARPin with that of a peptide known for its high affinity for c-Myc, we show that the recognition cannot be ascribed to sequence similarity but, instead, depends on the complementarity between the three-dimensional arrangement of the molecular fragments involved: the α-helix/loops domain of DARPin and the G4 backbone. Our results reveal that DARPins tertiary structure presents a charged hollow region in which G4 can be hosted, thus the more complementary the structural shapes, the more stable the interaction.
Keywords:c-Myc promoter  DARPin  epitope/paratope recognition  guanine quadruplex  molecular dynamics
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