Quasi-two-body decays $$B \rightarrow D K^*(892) \rightarrow D K \pi $$ in the perturbative QCD approach

Ma, Ai-Jun; Wang, Wen-Fei; Li, Ya; Xiao, Z. J.

doi:10.1140/epjc/s10052-019-7055-2

Cited by 35 publications

(42 citation statements)

References 76 publications

(79 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…To strengthen the interaction between the 3′-end of the siRNA, Xu et al [53] designed and synthesized a series of chemically modified nucleotide monomers containing an aromatic hydrophobic structure by applying bioisosterism strategy. Pyrimidine ring was substituted with benzene to enhance the binding between modified motif and hydrophobic residues Phe292, Leu337 and Phe310 in the PAZ domain.…”

mentioning

confidence: 99%

Therapeutic potential of chemically modified siRNA: Recent trends

et al. 2017

View full text Add to dashboard Cite

Small Interfering RNAs (siRNAs) are one of the valuable tools to investigate the functions of genes, and are also used for gene silencing. It has a wide scope in drug discovery through in vivo target validation. siRNA therapeutics are not optimal drug-like molecules due to poor bioavailability, immunogenic and off-target effects. In order to overcome the challenges associated with siRNA therapeutics, identification of appropriate chemical modifications that improves the stability, specificity and potency of siRNA is essential. This review focuses on the various chemical modifications and their implications in siRNA therapy.

show abstract

mentioning

confidence: 99%

Therapeutic potential of chemically modified siRNA: Recent trends

et al. 2017

View full text Add to dashboard Cite

show abstract

“…[3][4][5][6][7] The matching for "seed region" (nt 2-7 or 2-8 from 5′ end) of miRNA is pivotal for target recognition, while the perfect complementary for the left base pairs is not necessary. [8][9][10][11][12][13][14] In mammalian protein-coding genes, about 50% contain the evolutionary conserved miRNA target site and over 1,000 miRNA are encoded in human genome. [15] The first full-length structure of Argonaute protein from Pyrococcus furiosus was determined in 2004.…”

mentioning

confidence: 99%

Exploring the RNA‐bound and RNA‐free human Argonaute‐2 by molecular dynamics simulation method

Kong

Piao

et al. 2017

Chem Biol Drug Des

View full text Add to dashboard Cite

Argonaute 2 (Ago2) protein is the major vehicle of microRNAs (miRNAs)-guided gene repression and silencing processes. Although the crystal structure of human Ago2 (hAgo2) has recently been disclosed, the information of dynamically structural character of protein-RNA recognition is still lacking. Molecular dynamics simulations were used to systematically explore hAgo2 in the presence and absence of RNA duplex. Stable direct and water-mediated hydrogen bonds were observed between guide RNA backbone atoms and hAgo2, especially for nucleotides 2-7. In addition, water-mediated hydrogen bonds are indicated to be critical in the specific recognition between hAgo2 and the conserved adenine in position 1 of target RNA. The core domains (N, PAZ, MID, and PIWI) possess rigid body movements during the simulations. The motions of N-PAZ and PIWI-MID are negatively correlated with or without RNA binding and PAZ domain is identified as the most mobile domain in both systems. The reorientation of PAZ domain not only influences the binding of helix-7 and RNA duplex, the initial pairing process, but also the shape of N-PAZ cleft, where the supplemental base pairing occurs. It is speculated that PAZ domain could be a key regulator in hAgo2-mediated miRNA-induced gene regulation.

show abstract

“…Moreover, the similar feature with Si@TiO 2 @GNRs that the integral areas of CV curves enlarged along with the cycles increasing corresponds to the fact that the alloying process of Si is sluggish because of the progressive amorphization of the crystalline lattice happening in an extremely small interface, [49] and the fact that deep lithiation of silicon will be activated with the cycling. [50] To further illustrate the electrochemical performance of Si@TiO 2 @GNRs, galvanostatic charge-discharge were tested at different current densities and different cycles, as displayed in Figure 7a, b. Notably, the charge voltage plateaus of Si between 0.3 V to 0.6 V get shorter and the plateau of TiO 2 located at 2.03 V even disappears with the current densities and cycling number increasing, indicating unavoidable capacity decay.…”

Section: Resultsmentioning

confidence: 99%

Highly Porous Si Nanoframeworks Stabilized in TiO₂ Shells and Enlaced by Graphene Nanoribbons for Superior Lithium‐Ion Storage

et al. 2018

View full text Add to dashboard Cite

To enhance the rate capability and cycling stability of Si‐based materials in lithium‐ion batteries, three‐dimensional graphene nanoribbons (GNRs) enlacing Si@TiO2 nanoparticles are synthesized by magnesiothermic reduction, sol‐gel and electrostatic adsorption processes. The rigid clamping layer of TiO2 on the surface of Si prevents the whole electrode from undergoing volumetric variation. GNRs act as bridges to interconnect the adjacent Si@TiO2 nanoparticles to form a successively conductive network with decreased inner resistance. Moreover, the effect of two other kinds of carbon resources (polydopamine and resorcinol formaldehyde) on the electrochemical performance of Si@TiO2 are also discussed. The Si@TiO2@GNRs composite shows an enhanced discharge capacity of 1295 mAh g−1 at a current density of 0.5 A g−1 in the 300th cycle and achieve an outstanding rate capacity of 689.3 mAh g−1 even at 10.0 A g−1. The design of the double protecting structure provides an alternative strategy to enhance the electrochemical performance of M‐based materials (M=Si, Sn, and Ge).

show abstract

Quasi-two-body decays $$B \rightarrow D K^*(892) \rightarrow D K \pi $$ in the perturbative QCD approach

Cited by 35 publications

References 76 publications

Therapeutic potential of chemically modified siRNA: Recent trends

Therapeutic potential of chemically modified siRNA: Recent trends

Exploring the RNA‐bound and RNA‐free human Argonaute‐2 by molecular dynamics simulation method

Highly Porous Si Nanoframeworks Stabilized in TiO₂ Shells and Enlaced by Graphene Nanoribbons for Superior Lithium‐Ion Storage

Contact Info

Product

Resources

About

Quasi-two-body decays $$B \rightarrow D K^*(892) \rightarrow D K \pi $$ in the perturbative QCD approach

Cited by 35 publications

References 76 publications

Therapeutic potential of chemically modified siRNA: Recent trends

Therapeutic potential of chemically modified siRNA: Recent trends

Exploring the RNA‐bound and RNA‐free human Argonaute‐2 by molecular dynamics simulation method

Highly Porous Si Nanoframeworks Stabilized in TiO2 Shells and Enlaced by Graphene Nanoribbons for Superior Lithium‐Ion Storage

Contact Info

Product

Resources

About

Highly Porous Si Nanoframeworks Stabilized in TiO₂ Shells and Enlaced by Graphene Nanoribbons for Superior Lithium‐Ion Storage