Microwave‐Assisted Synthesis of C‐4′‐(1,5‐disubstituted)‐triazole‐spiro‐α‐L‐arabinofuranosyl Nucleosides

Rungta, Pallavi; Mangla, Priyanka; Maikhuri, Vipin K.; Singh, Sunil Kumar; Prasad, Ashok K.

doi:10.1002/slct.201701111

Cited by 8 publications

(8 citation statements)

References 34 publications

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“…Puckering amplitude (ν max =59.24), backbone angle (γ=32.88) as well as the torsion describing the anomeric bond (χ=‐171.54) support the inference. The conformational parameters of nucleoside 13 d was found to be comparable with the parent 2′‐ O ,4′‐ C ‐methylene‐α‐L‐ribofuranosyl‐uracil nucleoside monomer ( P =199.67) …”

Section: Resultsmentioning

confidence: 82%

“…Although, ASOs involving 2′‐ O ,4′‐ C ‐methyleneribofuranosyl‐nucleosides are known for high affinity recognition, their use is also accompanied with the risk of hepatotoxicity . This has persuaded researchers to explore modifications in their scaffold in pursuit of mitigation of the toxic effect while maintaining the antisense activity ,. Among other modifications, methyl substitution at their methylene bridge, i. e .…”

Section: Introductionmentioning

confidence: 99%

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Synthesis of 6′‐Methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ ribofuranosyl‐pyrimidine Nucleosides

et al. 2019

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Herein, we report the efficient synthesis of (6′R)‐ and (6′S)‐6′‐methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ribofuranosyl‐thymine, and (6′R)‐ and (6′S)‐6′‐methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ribofuranosyl‐uracil starting from diacetone glucofuranose in overall yields of 6.3, 4.7, 5.4 and 4.0%, respectively. The key step in the synthesis of stereochemically defined 6′‐Me‐bicyclic‐nucleosides is the nucleophilic addition of methyl group at methylene carbon of 4‐C–CH2OH moiety of the 4‐C‐tert‐butyldiphenylsilyloxymethylated sugar precursor. Thus, the methyl group was added on the aldehyde obtained from Dess‐Martin periodinane oxidation of the precursor alcohol employing AlMe3 in hexane. Both (6′R)‐ and (6′S)‐stereoisomers of bicyclic nucleosides T and U were successfully synthesized following Vorbrüggen nucleobase coupling of T and U with triacetylated glycosyl donor obtained from acetolysis of (5R)‐ and (5 S)‐4‐C‐(tert‐butyldiphenylsilyloxymethyl)‐5‐C‐methyl‐1,2‐O‐isopropylidene‐3‐O‐(2‐naphthylmethyl)‐α‐D‐xylofuranoses and further cyclization and deprotection of the resulted nucleoside. One of the nucleosides, (6′R)‐6′‐methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ribofuranosyl‐uracil has been reported earlier in 1.8% yield, while the present methodology yielded the nucleoside in 5.4% yield. All the synthesized 6′‐Me‐bicyclic‐nucleosides showed no significant anti‐viral activity against H1 N1 strain of influenza A virus (A/Puerto Rico/8/1934).

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Section: Resultsmentioning

confidence: 82%

Section: Introductionmentioning

confidence: 99%

Synthesis of 6′‐Methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ ribofuranosyl‐pyrimidine Nucleosides

et al. 2019

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“…In order to intramolecular 1,3-dipolar cycloaddition, Prasad and co-workers demonstrated the microwave assisted cyclization of sugar derived azido-alkyne functionality in order to produce triazole appended spiro nucleosides. [181] Intra- Basavaiah et al reported a metal-free high-yielding and convenient synthesis of triazole-fused benzoxazonines 242 starting from Baylis-Hillman-Basavaiah adduct 240 (Scheme 56). [182] Thus, Baylis-Hillman alcohol obtained Scheme 52.…”

Section: Intramolecular Cycloaddition Of Azido-alkyne Precursors Unde...mentioning

confidence: 99%

“…Synthesis of spiro-nucleoside 237 via intramolecular click chemistry from azido-alkyne sugar 233. [181] azides 247 produces the respective triazolo-benzoxazepine scaffolds 248 in moderate yields. The in vitro anticancer activity of novel triazolo-benzoxazepine scaffolds 248 were evaluated against three cancer cells such as Neura 2a (a neuroblastoma cell line), Hep G2 (a liver cancer cell line), and Hek 293 (a kidney cancer cell line) using MTT assay.…”

Section: Intramolecular Cycloaddition Of Azido-alkyne Precursors Unde...mentioning

confidence: 99%

Growing Impact of Intramolecular Click Chemistry in Organic Synthesis

Jaiswal

Tiwari

2023

The Chemical Record

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Click Chemistry, a modular, rapid, and one of the most reliable tool for the regioselective 1,2,3‐triazole forming [3+2] reaction of organic azide and terimal alkyne is widely explored in various emerging domains of research ranging from chemical biology to catalysis and medicinal chemistry to material science. This regioselective reaction from a diverse range of azido‐alkyne scaffolds has been well performed in both intermolecular as well as intramolecular fashions. In comparison to the intermolecular metal (Cu/Ru/Ni) variant of ‘Click Chemistry’, the intramolecular click tool is little addressed. The intramolecular click chemistry is exemplified as a mordern tool of cyclization which involves metal‐catalyzed (CuAAC/RuAAC) cyclization, organo‐catalyzed cyclization, and thermal‐induced topochemical reaction. Thus, we report herein the recent approaches on intramolecular azide‐alkyne cycloaddition ‘Click Chemistry‘ with their wide‐spread emerging applications in the developement of a diverse range of molecules including fused‐heterocycles, well‐defined peptidomemics, and macrocyclic architectures of various notable features.

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“…In the past few years, our research group has aimed and successfully executed the synthesis of various sugar modified nucleosides following chemical and biochemical pathways. 6′-Methyl-2′-O,4′-C-methylene--L-ribofuranosylpyrimidines, 36 -L-ribofuranosylnucleosides, 37 C-4′spiro-oxetano--L-ribonucleosides 38 were synthesized following chemical pathway, whereas 2′-O,4′-C-methyleneribonucleosides C, 39 C-4′-spiro-oxetanoribonucleosides, 40 homolyxofuranosylpyrimidines D 41 were synthesized following chemoenzymatic pathway. Herein, a facile and efficient methodology has been described for the synthesis of LNA nucleosides 8a,b following a chemoenzymatic pathway (Figure 1).…”

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confidence: 99%

Chemoenzymatic Synthesis of arabino-Configured Bicyclic Nucleosides

et al. 2023

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A convergent route for the synthesis of a new class of bicyclic nucleosides has been developed. The synthetic route to the corresponding arabino-configured uracil and thymine bicyclic nucleosides proceeds in 24 and 27% overall yields, respectively, starting from 1,2,5,6-di-O-isopropylidene-α-d-glucofuranose. This synthetic protocol includes some crucial steps such as Vorbrüggen base coupling and chemo-enzymatic regioselective acetylation of the primary hydroxyl group by using Lipozyme® TL IM where it was found that Lipozyme® TL IM could be recovered and reused for selective acetylation without losing its selectivity.

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Microwave‐Assisted Synthesis of C‐4′‐(1,5‐disubstituted)‐triazole‐spiro‐α‐L‐arabinofuranosyl Nucleosides

Cited by 8 publications

References 34 publications

Synthesis of 6′‐Methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ ribofuranosyl‐pyrimidine Nucleosides

Synthesis of 6′‐Methyl‐2′‐O,4′‐C‐methylene‐α‐L‐ ribofuranosyl‐pyrimidine Nucleosides

Growing Impact of Intramolecular Click Chemistry in Organic Synthesis

Chemoenzymatic Synthesis of arabino-Configured Bicyclic Nucleosides

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