<i>S</i>-Ribosylhomocysteine analogues modified at the ribosyl C-4 position

Chbib, Christiane; Sobczak, Adam; Mudgal, Mukesh; González, César; Lumpuy, Daniel A.; Nagaj, Justyna; Stokowa-Sołtys, Kamila; Wnuk, Stanislaw F.

doi:10.1080/17415993.2015.1137921

Cited by 6 publications

(5 citation statements)

References 35 publications

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“…In the inhibitor S-homoribosyl-L-cysteine, the carbon (C5)-sulfur bond was replaced by a C5-C6 carbon-carbon bond, which interferes with the cleavage of the carbon-sulfur bond (Alfaro et al, 2004; Figure 2, compound 3). Recently, Chbib et al (2016) synthesized 4-C-Alkyl/aryl-SRH analogs that potentially could inhibit LuxS at the β-elimination step. The substitution of the hydrogen atom at C4 position by alkyl/aryl groups should prevent the abstraction of the C4-proton, which is important for the β-elimination step (Chbib et al, 2016).…”

Section: S-ribosylhomocysteine Lyase Inhibitorsmentioning

confidence: 99%

“…Recently, Chbib et al (2016) synthesized 4-C-Alkyl/aryl-SRH analogs that potentially could inhibit LuxS at the β-elimination step. The substitution of the hydrogen atom at C4 position by alkyl/aryl groups should prevent the abstraction of the C4-proton, which is important for the β-elimination step (Chbib et al, 2016). Interestingly, these authors suggested that the 4-C-Alkyl/aryl-SRH analogs also could inhibit LuxS by interfering with the dimerization of the enzyme.…”

Section: S-ribosylhomocysteine Lyase Inhibitorsmentioning

confidence: 99%

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Interference With Quorum-Sensing Signal Biosynthesis as a Promising Therapeutic Strategy Against Multidrug-Resistant Pathogens

Martínez

Rigueiras

Pires

et al. 2019

Front. Cell. Infect. Microbiol.

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Faced with the global health threat of increasing resistance to antibiotics, researchers are exploring interventions that target bacterial virulence factors. Quorum sensing is a particularly attractive target because several bacterial virulence factors are controlled by this mechanism. Furthermore, attacking the quorum-sensing signaling network is less likely to select for resistant strains than using conventional antibiotics. Strategies that focus on the inhibition of quorum-sensing signal production are especially attractive because the enzymes involved are expressed in bacterial cells but are not present in their mammalian counterparts. We review here various approaches that are being taken to interfere with quorum-sensing signal production via the inhibition of autoinducer-2 synthesis, PQS synthesis, peptide autoinducer synthesis, and N-acyl-homoserine lactone synthesis. We expect these approaches will lead to the discovery of new quorum-sensing inhibitors that can help to stem the tide of antibiotic resistance.

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Section: S-ribosylhomocysteine Lyase Inhibitorsmentioning

confidence: 99%

Section: S-ribosylhomocysteine Lyase Inhibitorsmentioning

confidence: 99%

Interference With Quorum-Sensing Signal Biosynthesis as a Promising Therapeutic Strategy Against Multidrug-Resistant Pathogens

Martínez

Rigueiras

Pires

et al. 2019

Front. Cell. Infect. Microbiol.

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“…In our program on developing novel inhibitors of S -ribosylhomocysteine (SRH) hydrolase (LuxS; EC 4.4.1.21), which mediates the interspecies quorum sensing among bacteria, 17, 18 we recently applied lithium triethylborohydride (LTBH, Super-Hydride ® ) 19, 20 for the reduction of lactam and lactone analogues of SRH to the corresponding azahemiacetals ( N,O -acetals) 21 or lactols ( O,O -acetals). 22 Although application of LTBH for the reduction of lactams to cyclic hemiaminals (azahemiacetals) is documented, 23, 24 the reduction of lactones to the hemiacetals with LTBH is underdeveloped. In his landmark paper from 1980, 25 Brown reported that LTBH, when used in excess (2 equiv.…”

mentioning

confidence: 99%

Reduction of sugar lactones to hemiacetals with lithium triethylborohydride

González

Kavoosi

Sanchez

et al. 2016

Carbohydrate Research

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“…97,98 Figure 12. Silicon-fluoride acceptors in octreotate 96 32 and thymidine derivatives 99 109 has been utilized for the reduction of lactam (Scheme 10) and lactone analogues of SRH to the corresponding azahemiacetals (N,O-acetals) 110,111 or lactols (O,Oacetals) 112 , a method not extensively explored. Below, the commonly used reducing agents for this type of transformation will be reviewed.…”

Section: Scheme 5 Mechanism Of Isotopic Exchange Reaction Between F mentioning

confidence: 99%

“…121,122 Although the application of LTBH in organic synthesis is well documented, [140][141][142][143] including the reduction of lactams to cyclic hemiaminals (azahemiacetals), including in sugar lactams, 110 the reduction of lactones to the lactols with LTBH is underdeveloped. In the synthesis of 4-C-alkyl/aryl-substituted Sribosylhomocysteine (SRH) analogues, 112 which were prepared by coupling of homocysteine with 4-substituted ribonolactone derivatives, a project that I was involved in, LTBH was used to reduce a series 4-C-alkyl/aryl-modified lactones to their corresponding hemiacetals (Scheme 27). These hemiacetals were then coupled to homocysteine to yield 4C-SRH analogues.…”

Section: Reduction With Ltbh: Rationalementioning

confidence: 99%

Synthesis of Gemcitabine Analogues with Silicon-Fluoride Acceptors for 18F Labeling

Gonzalez-Espinoza¹

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I would also like to thank all my collaborators whom their great help have made this dissertation what it is. I would like to thank Dr. Cheppail Ramachandran from the Department of Pathology at Nicklaus Children's Hospital for studying the cytostatic activities of my 4-N-modified gemcitabine analogues in his L1210 cell line. Also, thank you to Dr. Alejandro Barbieri at FIU's department of Biological Sciences for providing cell and fluorescence studies with his HEK 293 cell line in order to have a better understanding of cellular uptake on my 4-N-modified gemcitabine analogues. A very special and appreciated thank you to Dr. Michael van Dam and his coworkers from the Crump Institute for Molecular Imaging in the University of California Los Angeles for their work in 18 F labeling and PET imaging of my 4-N-modified gemcitabine analogues in WT C57BL/6 mice. Finally, I would like to thank my advisor, Dr. Stanislaw F. Wnuk, for all his guidance and always keeping my in the right track. I would like to thank all of my lab mates, previous and current, for their advice and friendship. vi

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S-Ribosylhomocysteine analogues modified at the ribosyl C-4 position

Cited by 6 publications

References 35 publications

Interference With Quorum-Sensing Signal Biosynthesis as a Promising Therapeutic Strategy Against Multidrug-Resistant Pathogens

Interference With Quorum-Sensing Signal Biosynthesis as a Promising Therapeutic Strategy Against Multidrug-Resistant Pathogens

Reduction of sugar lactones to hemiacetals with lithium triethylborohydride

Synthesis of Gemcitabine Analogues with Silicon-Fluoride Acceptors for 18F Labeling

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