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Synthesis and Structure-Activity Relationship Study of 5a-Carbasugar Analogues of SL0101.


ABSTRACT: The Ser/Thr protein kinase, RSK, is associated with oncogenesis, and therefore, there are ongoing efforts to develop RSK inhibitors that are suitable for use in vivo. SL0101 is a natural product that demonstrates selectivity for RSK inhibition. However, SL0101 has a short biological half-life in vivo. To address this issue we designed a set of eight cyclitol analogues, which should be resistant to acid catalyzed anomeric bond hydrolysis. The analogues were synthesized and evaluated for their ability to selectively inhibit RSK in vitro and in cell-based assays. All the analogues were prepared using a stereodivergent palladium-catalyzed glycosylation/cyclitolization for installing the aglycon. The l-cyclitol analogues were found to inhibit RSK2 in in vitro kinase activity with a similar efficacy to that of SL0101, however, the analogues were not specific for RSK in cell-based assays. In contrast, the d-isomers showed no RSK inhibitory activity in in vitro kinase assay.

SUBMITTER: Li M 

PROVIDER: S-EPMC4291707 | biostudies-literature | 2015 Jan

REPOSITORIES: biostudies-literature

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Synthesis and Structure-Activity Relationship Study of 5a-Carbasugar Analogues of SL0101.

Li Mingzong M   Li Yu Y   Mrozowski Roman M RM   Sandusky Zachary M ZM   Shan Mingde M   Song Xiwen X   Wu Bulan B   Zhang Qi Q   Lannigan Deborah A DA   O'Doherty George A GA  

ACS medicinal chemistry letters 20141126 1


The Ser/Thr protein kinase, RSK, is associated with oncogenesis, and therefore, there are ongoing efforts to develop RSK inhibitors that are suitable for use in vivo. SL0101 is a natural product that demonstrates selectivity for RSK inhibition. However, SL0101 has a short biological half-life in vivo. To address this issue we designed a set of eight cyclitol analogues, which should be resistant to acid catalyzed anomeric bond hydrolysis. The analogues were synthesized and evaluated for their abi  ...[more]

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