In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.

C5-substituted 2,4-diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS (DAQ-DcpSi) have been developed for the treatment of spinal muscular atrophy (SMA), which is caused by genetic deficiency in the Survival Motor Neuron (SMN) protein. These compounds are claimed to act as SMN2 tra...

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Main Authors: Jonathan J Cherry, Christine J DiDonato, Elliot J Androphy, Alessandro Calo, Kyle Potter, Sara K Custer, Sarah Du, Timothy L Foley, Ariamala Gopalsamy, Emily J Reedich, Susana M Gordo, William Gordon, Natalie Hosea, Lyn H Jones, Daniel K Krizay, Gregory LaRosa, Hongxia Li, Sachin Mathur, Carol A Menard, Paraj Patel, Rebeca Ramos-Zayas, Anne Rietz, Haojing Rong, Baohong Zhang, Michael A Tones
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5612656?pdf=render
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spelling doaj-d509895517b840fca86c06c702f957d62020-11-25T01:46:00ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01129e018507910.1371/journal.pone.0185079In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.Jonathan J CherryChristine J DiDonatoElliot J AndrophyAlessandro CaloKyle PotterSara K CusterSarah DuTimothy L FoleyAriamala GopalsamyEmily J ReedichSusana M GordoWilliam GordonNatalie HoseaLyn H JonesDaniel K KrizayGregory LaRosaHongxia LiSachin MathurCarol A MenardParaj PatelRebeca Ramos-ZayasAnne RietzHaojing RongBaohong ZhangMichael A TonesC5-substituted 2,4-diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS (DAQ-DcpSi) have been developed for the treatment of spinal muscular atrophy (SMA), which is caused by genetic deficiency in the Survival Motor Neuron (SMN) protein. These compounds are claimed to act as SMN2 transcriptional activators but data underlying that claim are equivocal. In addition it is unclear whether the claimed effects on SMN2 are a direct consequence of DcpS inhibitor or might be a consequence of lysosomotropism, which is known to be neuroprotective. DAQ-DcpSi effects were characterized in cells in vitro utilizing DcpS knockdown and 7-methyl analogues as probes for DcpS vs non-DcpS-mediated effects. We also performed analysis of Smn transcript levels, RNA-Seq analysis of the transcriptome and SMN protein in order to identify affected pathways underlying the therapeutic effect, and studied lysosomotropic and non-lysosomotropic DAQ-DCpSi effects in 2B/- SMA mice. Treatment of cells caused modest and transient SMN2 mRNA increases with either no change or a decrease in SMNΔ7 and no change in SMN1 transcripts or SMN protein. RNA-Seq analysis of DAQ-DcpSi-treated N2a cells revealed significant changes in expression (both up and down) of approximately 2,000 genes across a broad range of pathways. Treatment of 2B/- SMA mice with both lysomotropic and non-lysosomotropic DAQ-DcpSi compounds had similar effects on disease phenotype indicating that the therapeutic mechanism of action is not a consequence of lysosomotropism. In striking contrast to the findings in vitro, Smn transcripts were robustly changed in tissues but there was no increase in SMN protein levels in spinal cord. We conclude that DAQ-DcpSi have reproducible benefit in SMA mice and a broad spectrum of biological effects in vitro and in vivo, but these are complex, context specific, and not the result of simple SMN2 transcriptional activation.http://europepmc.org/articles/PMC5612656?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jonathan J Cherry
Christine J DiDonato
Elliot J Androphy
Alessandro Calo
Kyle Potter
Sara K Custer
Sarah Du
Timothy L Foley
Ariamala Gopalsamy
Emily J Reedich
Susana M Gordo
William Gordon
Natalie Hosea
Lyn H Jones
Daniel K Krizay
Gregory LaRosa
Hongxia Li
Sachin Mathur
Carol A Menard
Paraj Patel
Rebeca Ramos-Zayas
Anne Rietz
Haojing Rong
Baohong Zhang
Michael A Tones
spellingShingle Jonathan J Cherry
Christine J DiDonato
Elliot J Androphy
Alessandro Calo
Kyle Potter
Sara K Custer
Sarah Du
Timothy L Foley
Ariamala Gopalsamy
Emily J Reedich
Susana M Gordo
William Gordon
Natalie Hosea
Lyn H Jones
Daniel K Krizay
Gregory LaRosa
Hongxia Li
Sachin Mathur
Carol A Menard
Paraj Patel
Rebeca Ramos-Zayas
Anne Rietz
Haojing Rong
Baohong Zhang
Michael A Tones
In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.
PLoS ONE
author_facet Jonathan J Cherry
Christine J DiDonato
Elliot J Androphy
Alessandro Calo
Kyle Potter
Sara K Custer
Sarah Du
Timothy L Foley
Ariamala Gopalsamy
Emily J Reedich
Susana M Gordo
William Gordon
Natalie Hosea
Lyn H Jones
Daniel K Krizay
Gregory LaRosa
Hongxia Li
Sachin Mathur
Carol A Menard
Paraj Patel
Rebeca Ramos-Zayas
Anne Rietz
Haojing Rong
Baohong Zhang
Michael A Tones
author_sort Jonathan J Cherry
title In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.
title_short In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.
title_full In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.
title_fullStr In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.
title_full_unstemmed In vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS: Context-specific modulation of SMN transcript levels.
title_sort in vitro and in vivo effects of 2,4 diaminoquinazoline inhibitors of the decapping scavenger enzyme dcps: context-specific modulation of smn transcript levels.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description C5-substituted 2,4-diaminoquinazoline inhibitors of the decapping scavenger enzyme DcpS (DAQ-DcpSi) have been developed for the treatment of spinal muscular atrophy (SMA), which is caused by genetic deficiency in the Survival Motor Neuron (SMN) protein. These compounds are claimed to act as SMN2 transcriptional activators but data underlying that claim are equivocal. In addition it is unclear whether the claimed effects on SMN2 are a direct consequence of DcpS inhibitor or might be a consequence of lysosomotropism, which is known to be neuroprotective. DAQ-DcpSi effects were characterized in cells in vitro utilizing DcpS knockdown and 7-methyl analogues as probes for DcpS vs non-DcpS-mediated effects. We also performed analysis of Smn transcript levels, RNA-Seq analysis of the transcriptome and SMN protein in order to identify affected pathways underlying the therapeutic effect, and studied lysosomotropic and non-lysosomotropic DAQ-DCpSi effects in 2B/- SMA mice. Treatment of cells caused modest and transient SMN2 mRNA increases with either no change or a decrease in SMNΔ7 and no change in SMN1 transcripts or SMN protein. RNA-Seq analysis of DAQ-DcpSi-treated N2a cells revealed significant changes in expression (both up and down) of approximately 2,000 genes across a broad range of pathways. Treatment of 2B/- SMA mice with both lysomotropic and non-lysosomotropic DAQ-DcpSi compounds had similar effects on disease phenotype indicating that the therapeutic mechanism of action is not a consequence of lysosomotropism. In striking contrast to the findings in vitro, Smn transcripts were robustly changed in tissues but there was no increase in SMN protein levels in spinal cord. We conclude that DAQ-DcpSi have reproducible benefit in SMA mice and a broad spectrum of biological effects in vitro and in vivo, but these are complex, context specific, and not the result of simple SMN2 transcriptional activation.
url http://europepmc.org/articles/PMC5612656?pdf=render
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