Toehold‐Mediated Strand Displacement in a Triplex Forming Nucleic Acid Clamp for Reversible Regulation of Polymerase Activity and Protein Expression

Herein, we present a generalizable and versatile strategy to engineer synthetic DNA ligand-binding devices that can be programmed to load and release a specific ligand at a defined temperature. We do so by re-engineering two model DNA-based receptors: a triplex-forming bivalent DNA-based receptor that recognizes a specific DNA sequence and an ATPbinding aptamer. The temperature at which these receptors load/release their ligands can be finely modulated by controlling the entropy associated with the linker connecting the two ligand-binding domains. The availability of a set of receptors with tunable and reversible temperature dependence allows achieving complex load/release behavior such as sustained ligand release over a wide temperature range. Similar programmable thermo-responsive synthetic ligand-binding devices can be of utility in applications such as drug delivery and production of smart materials.

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“…Finally, the approach is also relevant for RNA sequences that can form triplex structures in a similar way to DNA sequences (Figure S8). − …”

Section: Resultsmentioning

confidence: 99%

Thermo-Programmed Synthetic DNA-Based Receptors

2023

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“…were the first to report on the synthesis of aTNA and that aTNA forms an antiparallel homo‐duplex of high stability [17, 18] . We have later shown that aTNA forms highly stable sandwich type triplex structures with DNA and RNA and that aTNA is capable of forming i‐motifs and G‐quadruplexes [19–22] . This artificial oligonucleotide furthermore forms parallel duplexes with DNA and RNA, presumably because of an optimal rigidity [17] .…”

Section: Figurementioning

confidence: 95%

Functionalized Acyclic (l)‐Threoninol Nucleic Acid Four‐Way Junction with High Stability In Vitro and In Vivo

et al. 2022

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Oligonucleotides are increasingly being used as a programmable connection material to assemble molecules and proteins in well‐defined structures. For the application of such assemblies for in vivo diagnostics or therapeutics it is crucial that the oligonucleotides form highly stable, non‐toxic, and non‐immunogenic structures. Only few oligonucleotide derivatives fulfil all of these requirements. Here we report on the application of acyclic l‐threoninol nucleic acid (aTNA) to form a four‐way junction (4WJ) that is highly stable and enables facile assembly of components for in vivo treatment and imaging. The aTNA 4WJ is serum‐stable, shows no non‐targeted uptake or cytotoxicity, and invokes no innate immune response. As a proof of concept, we modify the 4WJ with a cancer‐targeting and a serum half‐life extension moiety and show the effect of these functionalized 4WJs in vitro and in vivo, respectively.

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“…The triplex formation phenomenon has been used for reversible regulation of polymerase activity and protein expression [61]. It was found that a construct of two acyclic L-aTNA homopyrimidine segments (linked to a hexaethylene glycol linker) and DNA (directly linked to an L-aTNA segment) can bind DNA and RNA by forming a highly stable triplex structure.…”

Section: Threoninol Nucleic Acids (Tna)mentioning

confidence: 99%

Acyclic Nucleic Acids with Phosphodiester Linkages—Synthesis, Properties and Potential Applications

Tomaszewska-Antczak

Guga

2021

Applied Sciences

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This review summarizes the synthetic efforts on acyclic analogs of nucleic acids and provides information on the most interesting features of selected classes of such compounds. The selection includes the following types of analogs: Flexible (FNA), Unlocked (UNA), Glycol (GNA), Butyl (BuNA), Threoninol (TNA) and Serinol Nucleic Acids (SNA). These classes of analogs are discussed in terms of their synthetic methods, the thermal stability of their homo- and hetero-duplexes and their applicability in biological and biochemical research and nanotechnology.

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Toehold‐Mediated Strand Displacement in a Triplex Forming Nucleic Acid Clamp for Reversible Regulation of Polymerase Activity and Protein Expression

Cited by 11 publications

References 37 publications

Thermo-Programmed Synthetic DNA-Based Receptors

Thermo-Programmed Synthetic DNA-Based Receptors

Functionalized Acyclic (l)‐Threoninol Nucleic Acid Four‐Way Junction with High Stability In Vitro and In Vivo

Acyclic Nucleic Acids with Phosphodiester Linkages—Synthesis, Properties and Potential Applications

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