Yuan Zhou scite author profile

The diverse biological functions of RNA are determined by the complex structures of RNA stabilized by both secondary and tertiary interactions. An RNA triplex is an important tertiary structure motif that is found in many pseudoknots and other structured RNAs. A triplex structure usually forms through tertiary interactions in the major or minor groove of a Watson-Crick base-paired stem. A major-groove RNA triplex structure is stable in isolation by forming consecutive major-groove base triples such as U·A-U and C(+) ·G-C. Minor-groove RNA triplexes, e.g., A-minor motif triplexes, are found in almost all large structured RNAs. As double-stranded RNA stem regions are often involved in biologically important tertiary triplex structure formation and protein binding, the ability to sequence specifically target any desired RNA duplexes by triplex formation would have great potential for biomedical applications. Programmable chemically modified triplex-forming oligonucleotides (TFOs) and triplex-forming peptide nucleic acids (PNAs) have been developed to form TFO·RNA2 and PNA·RNA2 triplexes, respectively, with enhanced binding affinity and sequence specificity at physiological conditions. Here, we (1) provide an overview of naturally occurring RNA triplexes, (2) summarize the experimental methods for studying triplexes, and (3) review the development of TFOs and triplex-forming PNAs for targeting an HIV-1 ribosomal frameshift-inducing RNA, a bacterial ribosomal A-site RNA, and a human microRNA hairpin precursor, and for inhibiting the RNA-protein interactions involving human RNA-dependent protein kinase and HIV-1 viral protein Rev.

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Enhancing Spin-Phonon and Spin-Spin Interactions Using Linear Resources in a Hybrid Quantum System

Zhou

Gao

et al. 2020

Phys. Rev. Lett.

104

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Hybrid spin-mechanical setups offer a versatile platform for quantum science and technology, but improving the spin-phonon as well as the spin-spin couplings of such systems remains a crucial challenge.Here, we propose and analyze an experimentally feasible and simple method for exponentially enhancing the spin-phonon and the phonon-mediated spin-spin interactions in a hybrid spin-mechanical setup, using only linear resources. Through modulating the spring constant of the mechanical cantilever with a time-dependent pump, we can acquire a tunable and nonlinear (two-phonon) drive to the mechanical mode, thus amplifying the mechanical zero-point fluctuations and directly enhancing the spin-phonon coupling. This method allows the spin-mechanical system to be driven from the weak-coupling regime to the strong-coupling regime, and even the ultrastrong coupling regime. In the dispersive regime, this method gives rise to a large enhancement of the phonon-mediated spin-spin interactions between distant solid-state spins, typically two orders of magnitude larger than that without modulation. As an example, we show that the proposed scheme can apply to generating entangled states of multiple spins with high fidelities even in the presence of large dissipations.

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Recognition of RNA duplexes by chemically modified triplex-forming oligonucleotides

Zhou

Kierzek

Loo

et al. 2013

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Triplex is emerging as an important RNA tertiary structure motif, in which consecutive non-canonical base pairs form between a duplex and a third strand. RNA duplex region is also often functionally important site for protein binding. Thus, triplex-forming oligonucleotides (TFOs) may be developed to regulate various biological functions involving RNA, such as viral ribosomal frameshifting and reverse transcription. How chemical modification in TFOs affects RNA triplex stability, however, is not well understood. Here, we incorporated locked nucleic acid, 2-thio U- and 2′-O methyl-modified residues in a series of all pyrimidine RNA TFOs, and we studied the binding to two RNA hairpin structures. The 12-base-triple major-groove pyrimidine–purine–pyrimidine triplex structures form between the duplex regions of RNA/DNA hairpins and the complementary RNA TFOs. Ultraviolet-absorbance-detected thermal melting studies reveal that the locked nucleic acid and 2-thio U modifications in TFOs strongly enhance triplex formation with both parental RNA and DNA duplex regions. In addition, we found that incorporation of 2′-O methyl-modified residues in a TFO destabilizes and stabilizes triplex formation with RNA and DNA duplex regions, respectively. The (de)stabilization of RNA triplex formation may be facilitated through modulation of van der Waals contact, base stacking, hydrogen bonding, backbone pre-organization, geometric compatibility and/or dehydration energy. Better understanding of the molecular determinants of RNA triplex structure stability lays the foundation for designing and discovering novel sequence-specific duplex-binding ligands as diagnostic and therapeutic agents targeting RNA.

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Yuan Zhou

RNA triplexes: from structural principles to biological and biotech applications

Enhancing Spin-Phonon and Spin-Spin Interactions Using Linear Resources in a Hybrid Quantum System

Recognition of RNA duplexes by chemically modified triplex-forming oligonucleotides

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