The affinity of RSK for cylitol analogues of SL0101 is critically dependent on the B-ring C-4'-hydroxy.

Yu Li,George A O'Doherty,Sharia Yasmin,Deborah A Lannigan,Pedro Seber,Eric B Wright

doi:10.1039/d0cc00128g

The affinity of RSK for cylitol analogues of SL0101 is critically dependent on the B-ring C-4'-hydroxy.

Yu Li, George A O'Doherty + Show 4 more

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https://doi.org/10.1039/d0cc00128g

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Journal: Chemical Communications	Publication Date: Jan 1, 2020
Citations: 8

Affiliation: St Vincent Hospital, Biologie du Développement et Cellules Souches, Vanderbilt University

#Anticancer Natural Product #Synthesis Of Carbohydrates #Asymmetric Synthesis #Natural Product

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Five cyclitol analogues of SL0101 with variable substitution at the C-4' position (i.e., OH, Cl, F, H, OMe) were synthesized. The series of analogues were evaluated for their ability to inhibit p90 ribosomal S6 kinase (RSK) activity. The study demonstrated the importance of the B-ring C-4' hydroxy group for RSK1/2 inhibition.

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The affinity of RSK for cylitol analogues of SL0101 is critically dependent on the B-ring C-4'-hydroxy.