Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.

Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.

Sphingosine kinases (SKs) are promising new therapeutic targets for cancer because they regulate the balance between pro-apoptotic ceramides and mitogenic sphingosine-1-phosphate. The functions of the two SK isoenzymes, SK1 and SK2, are not redundant, with genetic ablation of SK2 having more pronoun...

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Main Authors: Peng Gao, Yuri K Peterson, Ryan A Smith, Charles D Smith
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3438171?pdf=render
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spelling doaj-da1f15be80654752b6f6d8879757d9e22020-11-25T02:32:13ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0179e4454310.1371/journal.pone.0044543Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.Peng GaoYuri K PetersonRyan A SmithCharles D SmithSphingosine kinases (SKs) are promising new therapeutic targets for cancer because they regulate the balance between pro-apoptotic ceramides and mitogenic sphingosine-1-phosphate. The functions of the two SK isoenzymes, SK1 and SK2, are not redundant, with genetic ablation of SK2 having more pronounced anticancer effects than removal of SK1. Although several small molecule inhibitors of SKs have been described in the literature, detailed characterization of their molecular and cellular pharmacology, particularly their activities against human SK1 and SK2, have not been completed. Computational modeling of the putative active sites of SK1 and SK2 suggests structural differences that might allow isozyme-selective inhibitors. Therefore, we characterized several SK-inhibitory compounds which revealed differential inhibitory effects on SK1 and SK2 as follows: SKI-II and ABC294735 are SK1/2-dual inhibitors; CB5468139 is a SK1-selective inhibitor; and ABC294640 is a SK2-selective inhibitor. We examined the effects of the SK inhibitors on several biochemical and phenotypic processes in A498 kidney adenocarcinoma cells. The SK2-selective inhibitor ABC294640 demonstrated the most pronounced effects on SK1 and SK2 mRNA expression, decrease of S1P levels, elevation of ceramide levels, cell cycle arrest, and inhibition of proliferation, migration and invasion. ABC294640 also down-regulated the expression or activation of several signaling proteins, including STAT3, AKT, ERK, p21, p53 and FAK. These effects were equivalent or superior to responses to the SK1/2-dual inhibitors. Overall, these results suggest that inhibition of SK2 results in stronger anticancer effects than does inhibition of SK1 or both SK1 and SK2.http://europepmc.org/articles/PMC3438171?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Peng Gao
Yuri K Peterson
Ryan A Smith
Charles D Smith
spellingShingle Peng Gao
Yuri K Peterson
Ryan A Smith
Charles D Smith
Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
PLoS ONE
author_facet Peng Gao
Yuri K Peterson
Ryan A Smith
Charles D Smith
author_sort Peng Gao
title Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
title_short Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
title_full Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
title_fullStr Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
title_full_unstemmed Characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
title_sort characterization of isoenzyme-selective inhibitors of human sphingosine kinases.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Sphingosine kinases (SKs) are promising new therapeutic targets for cancer because they regulate the balance between pro-apoptotic ceramides and mitogenic sphingosine-1-phosphate. The functions of the two SK isoenzymes, SK1 and SK2, are not redundant, with genetic ablation of SK2 having more pronounced anticancer effects than removal of SK1. Although several small molecule inhibitors of SKs have been described in the literature, detailed characterization of their molecular and cellular pharmacology, particularly their activities against human SK1 and SK2, have not been completed. Computational modeling of the putative active sites of SK1 and SK2 suggests structural differences that might allow isozyme-selective inhibitors. Therefore, we characterized several SK-inhibitory compounds which revealed differential inhibitory effects on SK1 and SK2 as follows: SKI-II and ABC294735 are SK1/2-dual inhibitors; CB5468139 is a SK1-selective inhibitor; and ABC294640 is a SK2-selective inhibitor. We examined the effects of the SK inhibitors on several biochemical and phenotypic processes in A498 kidney adenocarcinoma cells. The SK2-selective inhibitor ABC294640 demonstrated the most pronounced effects on SK1 and SK2 mRNA expression, decrease of S1P levels, elevation of ceramide levels, cell cycle arrest, and inhibition of proliferation, migration and invasion. ABC294640 also down-regulated the expression or activation of several signaling proteins, including STAT3, AKT, ERK, p21, p53 and FAK. These effects were equivalent or superior to responses to the SK1/2-dual inhibitors. Overall, these results suggest that inhibition of SK2 results in stronger anticancer effects than does inhibition of SK1 or both SK1 and SK2.
url http://europepmc.org/articles/PMC3438171?pdf=render
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AT ryanasmith characterizationofisoenzymeselectiveinhibitorsofhumansphingosinekinases
AT charlesdsmith characterizationofisoenzymeselectiveinhibitorsofhumansphingosinekinases
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