Structure–Activity Relationship of Flavin Analogues That Target the Flavin Mononucleotide Riboswitch

Vicens, Quentin; Mondragón, Estefanía; Reyes, F.E.; Coish, Philip; Aristoff, Paul A.; Berman, Judd; Kaur, Harpreet; Kells, Kevin W.; Wickens, P.; Wilson, Jeffery; Gadwood, Robert C.; Schostarez, Heinrich J.; Suto, R.K.; Blount, Ken; Batey, Robert T.

doi:10.1021/acschembio.8b00533

Cited by 51 publications

(68 citation statements)

References 65 publications

(165 reference statements)

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“…The flavin mononucleotide (FMN) riboswitch is notable because it senses the cofactor FMN as well as the natural product roseoflavin, which acts as an antibacterial (23,127). This vulnerability has fostered efforts to target the JBC REVIEWS: Molecular recognition of HIV TAR RNA FMN riboswitch with novel antibiotics (19,21,22,25,26). Recent structure-guided design led to the discovery of compound BRX1555-an FMN analogue that binds with a K D of 39.0 Ϯ 0.7 nM based on in-line probing (Fig.…”

Section: Model Ncrna-inhibitor Interactions: Base Pairing and Shape Cmentioning

confidence: 99%

“…Recent structure-guided design led to the discovery of compound BRX1555-an FMN analogue that binds with a K D of 39.0 Ϯ 0.7 nM based on in-line probing (Fig. 4C) (25). The ligand has an in vitro EC 50 of 1.70 Ϯ 0.18 M in single-turnover transcription termination assays and an IC 50 of 0.49 Ϯ 0.09 M in bacterial growth inhibition assays (25).…”

Section: Model Ncrna-inhibitor Interactions: Base Pairing and Shape Cmentioning

confidence: 99%

“…4C) (25). The ligand has an in vitro EC 50 of 1.70 Ϯ 0.18 M in single-turnover transcription termination assays and an IC 50 of 0.49 Ϯ 0.09 M in bacterial growth inhibition assays (25).…”

Section: Model Ncrna-inhibitor Interactions: Base Pairing and Shape Cmentioning

confidence: 99%

“…These properties are suited for shape-specific recognition of small molecules or peptides and provide a basis to manipulate conformation or dynamics to alter downstream function. Several notable achievements accentuate such efforts, including the identification of inhibitors that target the following: cancerassociated miR-21; CUG repeats of myotonic dystrophy; riboswitches in pathogenic bacteria; and exon splicing in spinal muscular atrophy (17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27)(28). These successes underscore the feasibility of sequence-specific targeting of RNAs to create research tools or as a means to treat human disease.…”

mentioning

confidence: 99%

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Face-time with TAR: Portraits of an HIV-1 RNA with diverse modes of effector recognition relevant for drug discovery

Chavali

Bonn-Breach

Wedekind

2019

Journal of Biological Chemistry

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Section: Model Ncrna-inhibitor Interactions: Base Pairing and Shape Cmentioning

confidence: 99%

Section: Model Ncrna-inhibitor Interactions: Base Pairing and Shape Cmentioning

confidence: 99%

“…4C) (25). The ligand has an in vitro EC 50 of 1.70 Ϯ 0.18 M in single-turnover transcription termination assays and an IC 50 of 0.49 Ϯ 0.09 M in bacterial growth inhibition assays (25).…”

Section: Model Ncrna-inhibitor Interactions: Base Pairing and Shape Cmentioning

confidence: 99%

mentioning

confidence: 99%

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Face-time with TAR: Portraits of an HIV-1 RNA with diverse modes of effector recognition relevant for drug discovery

Chavali

Bonn-Breach

Wedekind

2019

Journal of Biological Chemistry

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“…Numerous studies have highlighted how complex structural folds in RNA molecules confer specific functions including riboswitches (Knappenberger, Reiss, & Strobel, ; Liberman et al, ; Peselis & Serganov, ; Vicens et al, ; B. Zhao, Guffy, Williams, & Zhang, ; also reviewed by Jones & Ferre‐D'Amare, ; Roth & Breaker, ), ribozymes (Chan et al, ; Costa, Walbott, Monachello, Westhof, & Michel, ; Meyer et al, ; L. A. Nguyen, Wang, & Steitz, ; Qu et al, ; Suslov et al, ; C. Zhao, Rajashankar, Marcia, & Pyle, ; also reviewed by Pyle, ; Ren, Micura, & Patel, ), and viral elements (Akiyama et al, ; Au et al, ; Imai, Kumar, Hellen, D'Souza, & Wagner, ; Keane et al, ). Additionally, recent studies have identified highly structured ncRNAs as important regulators in various cellular processes and linked misregulation of ncRNAs to important human diseases (Esteller, ).…”

Section: Introductionmentioning

confidence: 99%

Advances that facilitate the study of large RNA structure and dynamics by nuclear magnetic resonance spectroscopy

Zhang

Keane

2019

WIREs RNA

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The characterization of functional yet nonprotein coding (nc) RNAs has expanded the role of RNA in the cell from a passive player in the central dogma of molecular biology to an active regulator of gene expression. The misregulation of ncRNA function has been linked with a variety of diseases and disorders ranging from cancers to neurodegeneration. However, a detailed molecular understanding of how ncRNAs function has been limited; due, in part, to the difficulties associated with obtaining high-resolution structures of large RNAs. Tertiary structure determination of RNA as a whole is hampered by various technical challenges, all of which are exacerbated as the size of the RNA increases. Namely, RNAs tend to be highly flexible and dynamic molecules, which are difficult to crystallize. Biomolecular nuclear magnetic resonance (NMR) spectroscopy offers a viable alternative to determining the structure of large RNA molecules that do not readily crystallize, but is itself hindered by some technical limitations. Recently, a series of advancements have allowed the biomolecular NMR field to overcome, at least in part, some of these limitations. These advances include improvements in sample preparation strategies as well as methodological improvements. Together, these innovations pave the way for the study of ever larger RNA molecules that have important biological function.

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Medicinal Chemical Biology

Jones

2021

Burger's Medicinal Chemistry and Drug Discovery

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Arguably, the two most important decisions facing drug discovery teams are selecting the target and the therapeutic modality as the focus of their research efforts. This article highlights the recent technical advances in medicinal chemical biology that strongly influence these early, yet centrally important, choices. The article is not meant to be a comprehensive review of all innovations in the area. Examples are chosen that illustrate the impact chemical biology has had recently on drug discovery research. Medicinal chemical biology is ideally suited to expand druggable space through the development of target identification and validation technologies. Equally, innovative therapeutic modalities are required to enhance the medicinal toolkit to ensure that high‐quality clinical candidates are delivered that effectively target pathogenesis. Opportunities and challenges are described that serve to inspire further therapeutic research at the chemistry–biology interface.

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Structure–Activity Relationship of Flavin Analogues That Target the Flavin Mononucleotide Riboswitch

Cited by 51 publications

References 65 publications

Face-time with TAR: Portraits of an HIV-1 RNA with diverse modes of effector recognition relevant for drug discovery

Face-time with TAR: Portraits of an HIV-1 RNA with diverse modes of effector recognition relevant for drug discovery

Advances that facilitate the study of large RNA structure and dynamics by nuclear magnetic resonance spectroscopy

Medicinal Chemical Biology

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