Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways

[Image: see text] The natural product neocarzilin A (NCA) was discovered decades ago, and despite its potent cytotoxic effects no mode of action studies have been performed up to date. Synthesis of neocarzilins A, B, and C and a stereoisomer of NCA provided insights into structural preferences as we...

Descripción completa

Detalles Bibliográficos
Autores principales: Gleissner, Carolin M.-L., Pyka, Carolin L., Heydenreuter, Wolfgang, Gronauer, Thomas F., Atzberger, Carina, Korotkov, Vadim S., Cheng, Weiting, Hacker, Stephan M., Vollmar, Angelika M., Braig, Simone, Sieber, Stephan A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2019
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6661975/
https://www.ncbi.nlm.nih.gov/pubmed/31403069
http://dx.doi.org/10.1021/acscentsci.9b00266
_version_ 1783439562368876544
author Gleissner, Carolin M.-L.
Pyka, Carolin L.
Heydenreuter, Wolfgang
Gronauer, Thomas F.
Atzberger, Carina
Korotkov, Vadim S.
Cheng, Weiting
Hacker, Stephan M.
Vollmar, Angelika M.
Braig, Simone
Sieber, Stephan A.
author_facet Gleissner, Carolin M.-L.
Pyka, Carolin L.
Heydenreuter, Wolfgang
Gronauer, Thomas F.
Atzberger, Carina
Korotkov, Vadim S.
Cheng, Weiting
Hacker, Stephan M.
Vollmar, Angelika M.
Braig, Simone
Sieber, Stephan A.
author_sort Gleissner, Carolin M.-L.
collection PubMed
description [Image: see text] The natural product neocarzilin A (NCA) was discovered decades ago, and despite its potent cytotoxic effects no mode of action studies have been performed up to date. Synthesis of neocarzilins A, B, and C and a stereoisomer of NCA provided insights into structural preferences as well as access to probes for functional studies. NCA turned out to be the most active member and was not only effective against cell proliferation but also migration, a novel and so far overlooked activity. To decipher the molecular mode of action, we applied chemical proteomics for target discovery and revealed that NCA targets cancer cell migration via irreversible binding to the largely uncharacterized synaptic vesicle membrane protein VAT-1. A corresponding knockout of the protein confirmed the phenotype, and pull-down studies showed the interaction with an intricate network of key migration mediators such as Talin-1. Overall, we introduce VAT-1 as a promising novel target for the development of selective migration inhibitors with the perspective to limit toxicity in the absence of antiproliferative effects.
format Online
Article
Text
id pubmed-6661975
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher American Chemical Society
record_format MEDLINE/PubMed
spelling pubmed-66619752019-08-09 Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways Gleissner, Carolin M.-L. Pyka, Carolin L. Heydenreuter, Wolfgang Gronauer, Thomas F. Atzberger, Carina Korotkov, Vadim S. Cheng, Weiting Hacker, Stephan M. Vollmar, Angelika M. Braig, Simone Sieber, Stephan A. ACS Cent Sci [Image: see text] The natural product neocarzilin A (NCA) was discovered decades ago, and despite its potent cytotoxic effects no mode of action studies have been performed up to date. Synthesis of neocarzilins A, B, and C and a stereoisomer of NCA provided insights into structural preferences as well as access to probes for functional studies. NCA turned out to be the most active member and was not only effective against cell proliferation but also migration, a novel and so far overlooked activity. To decipher the molecular mode of action, we applied chemical proteomics for target discovery and revealed that NCA targets cancer cell migration via irreversible binding to the largely uncharacterized synaptic vesicle membrane protein VAT-1. A corresponding knockout of the protein confirmed the phenotype, and pull-down studies showed the interaction with an intricate network of key migration mediators such as Talin-1. Overall, we introduce VAT-1 as a promising novel target for the development of selective migration inhibitors with the perspective to limit toxicity in the absence of antiproliferative effects. American Chemical Society 2019-06-18 2019-07-24 /pmc/articles/PMC6661975/ /pubmed/31403069 http://dx.doi.org/10.1021/acscentsci.9b00266 Text en Copyright © 2019 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Gleissner, Carolin M.-L.
Pyka, Carolin L.
Heydenreuter, Wolfgang
Gronauer, Thomas F.
Atzberger, Carina
Korotkov, Vadim S.
Cheng, Weiting
Hacker, Stephan M.
Vollmar, Angelika M.
Braig, Simone
Sieber, Stephan A.
Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways
title Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways
title_full Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways
title_fullStr Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways
title_full_unstemmed Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways
title_short Neocarzilin A Is a Potent Inhibitor of Cancer Cell Motility Targeting VAT-1 Controlled Pathways
title_sort neocarzilin a is a potent inhibitor of cancer cell motility targeting vat-1 controlled pathways
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6661975/
https://www.ncbi.nlm.nih.gov/pubmed/31403069
http://dx.doi.org/10.1021/acscentsci.9b00266
work_keys_str_mv AT gleissnercarolinml neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT pykacarolinl neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT heydenreuterwolfgang neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT gronauerthomasf neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT atzbergercarina neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT korotkovvadims neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT chengweiting neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT hackerstephanm neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT vollmarangelikam neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT braigsimone neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways
AT sieberstephana neocarzilinaisapotentinhibitorofcancercellmotilitytargetingvat1controlledpathways

Ejemplares similares