Nucleobase modified neamines with a lysine as a linker, their inhibition specificity for TAR-Tat derived from HIV-1

Nucleobase modified neamines with a lysine as a linker, their inhibition specificity for TAR-Tat derived from HIV-1

[Display omitted] Nucleobase modified neamines with a lysine as the linker (NbK-neamines) were synthesized and their binding toward hairpin RNAs derived from HIV-1 activator region were studied. NbK-neamines were bind those RNAs with micro molar level of binding affinities and compete with correspon...

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Veröffentlicht in:Bioorganic & medicinal chemistry 2015-05, Vol.23 (9), p.2139-2147
Hauptverfasser: Inoue, Ryo, Watanabe, Kentarou, Katou, Toyofusa, Ikezawa, Yasunori, Hamasaki, Keita
Format: Artikel
Sprache:eng
Schlagworte:
Adenine - chemistry
Aminoglycoside
Cytosine - chemistry
Framycetin - chemical synthesis
Framycetin - chemistry
Framycetin - pharmacology
Guanine - chemistry
HIV Long Terminal Repeat - drug effects
HIV-1 - chemistry
HIV-1 - genetics
Lysine - chemistry
Molecular Structure
Neamine
Nucleobase
Potential inhibitor
RRE RNA
Structure-Activity Relationship
TAR RNA
tat Gene Products, Human Immunodeficiency Virus - antagonists & inhibitors
Thymine - chemistry
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Zusammenfassung:[Display omitted] Nucleobase modified neamines with a lysine as the linker (NbK-neamines) were synthesized and their binding toward hairpin RNAs derived from HIV-1 activator region were studied. NbK-neamines were bind those RNAs with micro molar level of binding affinities and compete with corresponding activator peptide for TAR RNA, but not for RRE RNA. GbK-neamine denotes the highest binding affinity with TAR RNA, three to five times higher than other three NbK-neamines. GbK-neamine could be a candidate of potential inhibitor for TAR-Tat.
ISSN:0968-0896
1464-3391
DOI:10.1016/j.bmc.2015.03.001