Synthesis and biological evaluation of carbocyclic analogues of pachastrissamine

Yongseok Kwon; Jayoung Song; Hoon Bae; Woo Jung Kim; Joo Youn Lee; Geun Hee Han; Sang Kook Lee; Sanghee Kim

doi:10.3390/md13020824

Synthesis and biological evaluation of carbocyclic analogues of pachastrissamine

Yongseok Kwon, Jayoung Song, Hoon Bae, Woo Jung Kim, Joo Youn Lee, Geun Hee Han, Sang Kook Lee, Sanghee Kim

Seoul National University

Research output: Contribution to journal › Article › peer-review

22 Scopus citations

Abstract

A series of carbocyclic analogues of naturally-occurring marine sphingolipid pachastrissamine were prepared and biologically evaluated. The analogues were efficiently synthesized via a tandem enyne/diene-ene metathesis reaction as a key step. We found that the analogue 4b exhibited comparable cytotoxicity and more potent inhibitory activity against sphingosine kinases, compared to pachastrissamine. Molecular modeling studies were conducted to provide more detailed insight into the binding mode of 4b in sphingosine kinase. In our docking model, pachastrissamine and 4b were able to effectively bind to the binding pocket of sphingosine kinase 1 as co-crystalized sphingosine. However, 4b showed a hydrophobic interaction with Phe192, which suggests that it contributes to its increased inhibitory activity against sphingosine kinase 1.

Original language	English
Pages (from-to)	824-837
Number of pages	14
Journal	Marine Drugs
Volume	13
Issue number	2
DOIs	https://doi.org/10.3390/md13020824
State	Published - 1 Feb 2015
Externally published	Yes

Keywords

Carbocyclic analogue
Cytotoxicity
Jaspine B
Molecular modeling
Pachastrissamine
Sphingosine kinase inhibitor

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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title = "Synthesis and biological evaluation of carbocyclic analogues of pachastrissamine",

abstract = "A series of carbocyclic analogues of naturally-occurring marine sphingolipid pachastrissamine were prepared and biologically evaluated. The analogues were efficiently synthesized via a tandem enyne/diene-ene metathesis reaction as a key step. We found that the analogue 4b exhibited comparable cytotoxicity and more potent inhibitory activity against sphingosine kinases, compared to pachastrissamine. Molecular modeling studies were conducted to provide more detailed insight into the binding mode of 4b in sphingosine kinase. In our docking model, pachastrissamine and 4b were able to effectively bind to the binding pocket of sphingosine kinase 1 as co-crystalized sphingosine. However, 4b showed a hydrophobic interaction with Phe192, which suggests that it contributes to its increased inhibitory activity against sphingosine kinase 1.",

keywords = "Carbocyclic analogue, Cytotoxicity, Jaspine B, Molecular modeling, Pachastrissamine, Sphingosine kinase inhibitor",

author = "Yongseok Kwon and Jayoung Song and Hoon Bae and Kim, \{Woo Jung\} and Lee, \{Joo Youn\} and Han, \{Geun Hee\} and Lee, \{Sang Kook\} and Sanghee Kim",

note = "Publisher Copyright: {\textcopyright} 2015 by the authors.",

year = "2015",

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doi = "10.3390/md13020824",

language = "English",

volume = "13",

pages = "824--837",

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TY - JOUR

T1 - Synthesis and biological evaluation of carbocyclic analogues of pachastrissamine

AU - Kwon, Yongseok

AU - Song, Jayoung

AU - Bae, Hoon

AU - Kim, Woo Jung

AU - Lee, Joo Youn

AU - Han, Geun Hee

AU - Lee, Sang Kook

AU - Kim, Sanghee

PY - 2015/2/1

Y1 - 2015/2/1

N2 - A series of carbocyclic analogues of naturally-occurring marine sphingolipid pachastrissamine were prepared and biologically evaluated. The analogues were efficiently synthesized via a tandem enyne/diene-ene metathesis reaction as a key step. We found that the analogue 4b exhibited comparable cytotoxicity and more potent inhibitory activity against sphingosine kinases, compared to pachastrissamine. Molecular modeling studies were conducted to provide more detailed insight into the binding mode of 4b in sphingosine kinase. In our docking model, pachastrissamine and 4b were able to effectively bind to the binding pocket of sphingosine kinase 1 as co-crystalized sphingosine. However, 4b showed a hydrophobic interaction with Phe192, which suggests that it contributes to its increased inhibitory activity against sphingosine kinase 1.

AB - A series of carbocyclic analogues of naturally-occurring marine sphingolipid pachastrissamine were prepared and biologically evaluated. The analogues were efficiently synthesized via a tandem enyne/diene-ene metathesis reaction as a key step. We found that the analogue 4b exhibited comparable cytotoxicity and more potent inhibitory activity against sphingosine kinases, compared to pachastrissamine. Molecular modeling studies were conducted to provide more detailed insight into the binding mode of 4b in sphingosine kinase. In our docking model, pachastrissamine and 4b were able to effectively bind to the binding pocket of sphingosine kinase 1 as co-crystalized sphingosine. However, 4b showed a hydrophobic interaction with Phe192, which suggests that it contributes to its increased inhibitory activity against sphingosine kinase 1.

KW - Carbocyclic analogue

KW - Cytotoxicity

KW - Jaspine B

KW - Molecular modeling

KW - Pachastrissamine

KW - Sphingosine kinase inhibitor

UR - https://www.scopus.com/pages/publications/84923247298

U2 - 10.3390/md13020824

DO - 10.3390/md13020824

M3 - Article

C2 - 25654428

AN - SCOPUS:84923247298

SN - 1660-3397

VL - 13

SP - 824

EP - 837

JO - Marine Drugs

JF - Marine Drugs

IS - 2

ER -

Synthesis and biological evaluation of carbocyclic analogues of pachastrissamine

Abstract

Keywords

UN SDGs

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