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Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation

The frequency of poor outcomes in relapsed leukemia patients underscores the need for novel therapeutic approaches. The FDA-approved immunosuppressant FTY720 limits leukemia progression by activating protein phosphatase 2A and restricting nutrient access. Unfortunately, FTY720 cannot be re-purposed...

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Autores principales: McCracken, Alison N., McMonigle, Ryan J., Tessier, Jérémie, Fransson, Rebecca, Perryman, Michael S., Chen, Bin, Keebaugh, Andrew, Selwan, Elizabeth, Barr, Sarah A., Kim, Seong M., Roy, Saurabh G., Liu, Gang, Fallegger, Daniel, Sernissi, Lorenzo, Brandt, Cordelia, Moitessier, Nicolas, Snider, Ashley J., Clare, Simon, Müschen, Markus, Huwiler, Andrea, Kleinman, Michael T., Hanessian, Stephen, Edinger, Aimee L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5332311/
https://www.ncbi.nlm.nih.gov/pubmed/27573555
http://dx.doi.org/10.1038/leu.2016.244
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author McCracken, Alison N.
McMonigle, Ryan J.
Tessier, Jérémie
Fransson, Rebecca
Perryman, Michael S.
Chen, Bin
Keebaugh, Andrew
Selwan, Elizabeth
Barr, Sarah A.
Kim, Seong M.
Roy, Saurabh G.
Liu, Gang
Fallegger, Daniel
Sernissi, Lorenzo
Brandt, Cordelia
Moitessier, Nicolas
Snider, Ashley J.
Clare, Simon
Müschen, Markus
Huwiler, Andrea
Kleinman, Michael T.
Hanessian, Stephen
Edinger, Aimee L.
author_facet McCracken, Alison N.
McMonigle, Ryan J.
Tessier, Jérémie
Fransson, Rebecca
Perryman, Michael S.
Chen, Bin
Keebaugh, Andrew
Selwan, Elizabeth
Barr, Sarah A.
Kim, Seong M.
Roy, Saurabh G.
Liu, Gang
Fallegger, Daniel
Sernissi, Lorenzo
Brandt, Cordelia
Moitessier, Nicolas
Snider, Ashley J.
Clare, Simon
Müschen, Markus
Huwiler, Andrea
Kleinman, Michael T.
Hanessian, Stephen
Edinger, Aimee L.
author_sort McCracken, Alison N.
collection PubMed
description The frequency of poor outcomes in relapsed leukemia patients underscores the need for novel therapeutic approaches. The FDA-approved immunosuppressant FTY720 limits leukemia progression by activating protein phosphatase 2A and restricting nutrient access. Unfortunately, FTY720 cannot be re-purposed for use in cancer patients due to on-target toxicity associated with S1P receptor activation at the elevated, anti-neoplastic dose. Here we show that the constrained azacyclic FTY720 analog SH-RF-177 lacks S1P receptor activity but maintains anti-leukemic activity in vitro and in vivo. SH-RF-177 was not only more potent than FTY720, but killed via a distinct mechanism. Phosphorylation is dispensable for FTY720’s anti-leukemic actions. However, chemical biology and genetic approaches demonstrated that the sphingosine kinase 2- (SPHK2) mediated phosphorylation of SH-RF-177 led to engagement of a pro-apoptotic target and increased potency. The cytotoxicity of membrane-permeant FTY720 phosphonate esters suggests that the enhanced potency of SH-RF-177 stems from its more efficient phosphorylation. The tight inverse correlation between SH-RF-177 IC(50) and SPHK2 mRNA expression suggests a useful biomarker for SH-RF-177 sensitivity. In summary, these studies indicate that FTY720 analogs that are efficiently phosphorylated but fail to activate S1P receptors may be superior anti-leukemic agents compared to compounds that avoid cardiotoxicity by eliminating phosphorylation.
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spelling pubmed-53323112017-03-02 Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation McCracken, Alison N. McMonigle, Ryan J. Tessier, Jérémie Fransson, Rebecca Perryman, Michael S. Chen, Bin Keebaugh, Andrew Selwan, Elizabeth Barr, Sarah A. Kim, Seong M. Roy, Saurabh G. Liu, Gang Fallegger, Daniel Sernissi, Lorenzo Brandt, Cordelia Moitessier, Nicolas Snider, Ashley J. Clare, Simon Müschen, Markus Huwiler, Andrea Kleinman, Michael T. Hanessian, Stephen Edinger, Aimee L. Leukemia Article The frequency of poor outcomes in relapsed leukemia patients underscores the need for novel therapeutic approaches. The FDA-approved immunosuppressant FTY720 limits leukemia progression by activating protein phosphatase 2A and restricting nutrient access. Unfortunately, FTY720 cannot be re-purposed for use in cancer patients due to on-target toxicity associated with S1P receptor activation at the elevated, anti-neoplastic dose. Here we show that the constrained azacyclic FTY720 analog SH-RF-177 lacks S1P receptor activity but maintains anti-leukemic activity in vitro and in vivo. SH-RF-177 was not only more potent than FTY720, but killed via a distinct mechanism. Phosphorylation is dispensable for FTY720’s anti-leukemic actions. However, chemical biology and genetic approaches demonstrated that the sphingosine kinase 2- (SPHK2) mediated phosphorylation of SH-RF-177 led to engagement of a pro-apoptotic target and increased potency. The cytotoxicity of membrane-permeant FTY720 phosphonate esters suggests that the enhanced potency of SH-RF-177 stems from its more efficient phosphorylation. The tight inverse correlation between SH-RF-177 IC(50) and SPHK2 mRNA expression suggests a useful biomarker for SH-RF-177 sensitivity. In summary, these studies indicate that FTY720 analogs that are efficiently phosphorylated but fail to activate S1P receptors may be superior anti-leukemic agents compared to compounds that avoid cardiotoxicity by eliminating phosphorylation. 2016-08-30 2017-03 /pmc/articles/PMC5332311/ /pubmed/27573555 http://dx.doi.org/10.1038/leu.2016.244 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
McCracken, Alison N.
McMonigle, Ryan J.
Tessier, Jérémie
Fransson, Rebecca
Perryman, Michael S.
Chen, Bin
Keebaugh, Andrew
Selwan, Elizabeth
Barr, Sarah A.
Kim, Seong M.
Roy, Saurabh G.
Liu, Gang
Fallegger, Daniel
Sernissi, Lorenzo
Brandt, Cordelia
Moitessier, Nicolas
Snider, Ashley J.
Clare, Simon
Müschen, Markus
Huwiler, Andrea
Kleinman, Michael T.
Hanessian, Stephen
Edinger, Aimee L.
Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation
title Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation
title_full Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation
title_fullStr Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation
title_full_unstemmed Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation
title_short Phosphorylation of a constrained azacyclic FTY720 analog enhances anti-leukemic activity without inducing S1P receptor activation
title_sort phosphorylation of a constrained azacyclic fty720 analog enhances anti-leukemic activity without inducing s1p receptor activation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5332311/
https://www.ncbi.nlm.nih.gov/pubmed/27573555
http://dx.doi.org/10.1038/leu.2016.244
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