Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies

Zacary P. Germon; Jonathan R. Sillar; Abdul Mannan; Ryan J. Duchatel; Dilana Staudt; Heather C. Murray; Izac J. Findlay; Evangeline R. Jackson; Holly P. McEwen; Alicia M. Douglas; Tabitha McLachlan; John E. Schjenken; David A. Skerrett-Byrne; Honggang Huang; Marcella N. Melo-Braga; Maximilian W. Plank; Frank Alvaro; Janis Chamberlain; Geoff De Iuliis; R. John Aitken; Brett Nixon; Andrew H. Wei; Anoop K. Enjeti; Yizhou Huang; Richard B. Lock; Martin R. Larsen; Heather Lee; Vijesh Vaghjiani; Jason E. Cain; Charles E. de Bock; Nicole M. Verrills; Matthew D. Dun

doi:10.1126/scisignal.abp9586

Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies

Zacary P. Germon, Jonathan R. Sillar, Abdul Mannan, Ryan J. Duchatel, Dilana Staudt, Heather C. Murray, Izac J. Findlay, Evangeline R. Jackson, Holly P. McEwen, Alicia M. Douglas, Tabitha McLachlan, John E. Schjenken, David A. Skerrett-Byrne, Honggang Huang, Marcella N. Melo-Braga, Maximilian W. Plank, Frank Alvaro, Janis Chamberlain, Geoff De Iuliis, R. John AitkenBrett Nixon, Andrew H. Wei, Anoop K. Enjeti, Yizhou Huang, Richard B. Lock, Martin R. Larsen, Heather Lee, Vijesh Vaghjiani, Jason E. Cain, Charles E. de Bock, Nicole M. Verrills, Matthew D. Dun

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Abstract

Mutations in the type III receptor tyrosine kinase FLT3 are frequent in patients with acute myeloid leukemia (AML) and are associated with a poor prognosis. AML is characterized by the overproduction of reactive oxygen species (ROS), which can induce cysteine oxidation in redox-sensitive signaling proteins. Here, we sought to characterize the specific pathways affected by ROS in AML by assessing oncogenic signaling in primary AML samples. The oxidation or phosphorylation of signaling proteins that mediate growth and proliferation was increased in samples from patient subtypes with FLT3 mutations. These samples also showed increases in the oxidation of proteins in the ROS-producing Rac/NADPH oxidase-2 (NOX2) complex. Inhibition of NOX2 increased the apoptosis of FLT3-mutant AML cells in response to FLT3 inhibitors. NOX2 inhibition also reduced the phosphorylation and cysteine oxidation of FLT3 in patient-derived xenograft mouse models, suggesting that decreased oxidative stress reduces the oncogenic signaling of FLT3. In mice grafted with FLT3 mutant AML cells, treatment with a NOX2 inhibitor reduced the number of circulating cancer cells, and combining FLT3 and NOX2 inhibitors increased survival to a greater extent than either treatment alone. Together, these data raise the possibility that combining NOX2 and FLT3 inhibitors could improve the treatment of FLT3 mutant AML.

Original language	English
Article number	eabp9586
Number of pages	18
Journal	Science Signaling
Volume	16
Issue number	778
DOIs	https://doi.org/10.1126/scisignal.abp9586
Publication status	Published - 28 Mar 2023

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Germon, Z. P., Sillar, J. R., Mannan, A., Duchatel, R. J., Staudt, D., Murray, H. C., Findlay, I. J., Jackson, E. R., McEwen, H. P., Douglas, A. M., McLachlan, T., Schjenken, J. E., Skerrett-Byrne, D. A., Huang, H., Melo-Braga, M. N., Plank, M. W., Alvaro, F., Chamberlain, J., Iuliis, G. D., ... Dun, M. D. (2023). Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies. Science Signaling, 16(778), Article eabp9586. https://doi.org/10.1126/scisignal.abp9586

@article{a55f3ec22bc04611a07172452d5378b2,

title = "Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies",

abstract = "Mutations in the type III receptor tyrosine kinase FLT3 are frequent in patients with acute myeloid leukemia (AML) and are associated with a poor prognosis. AML is characterized by the overproduction of reactive oxygen species (ROS), which can induce cysteine oxidation in redox-sensitive signaling proteins. Here, we sought to characterize the specific pathways affected by ROS in AML by assessing oncogenic signaling in primary AML samples. The oxidation or phosphorylation of signaling proteins that mediate growth and proliferation was increased in samples from patient subtypes with FLT3 mutations. These samples also showed increases in the oxidation of proteins in the ROS-producing Rac/NADPH oxidase-2 (NOX2) complex. Inhibition of NOX2 increased the apoptosis of FLT3-mutant AML cells in response to FLT3 inhibitors. NOX2 inhibition also reduced the phosphorylation and cysteine oxidation of FLT3 in patient-derived xenograft mouse models, suggesting that decreased oxidative stress reduces the oncogenic signaling of FLT3. In mice grafted with FLT3 mutant AML cells, treatment with a NOX2 inhibitor reduced the number of circulating cancer cells, and combining FLT3 and NOX2 inhibitors increased survival to a greater extent than either treatment alone. Together, these data raise the possibility that combining NOX2 and FLT3 inhibitors could improve the treatment of FLT3 mutant AML.",

author = "Germon, \{Zacary P.\} and Sillar, \{Jonathan R.\} and Abdul Mannan and Duchatel, \{Ryan J.\} and Dilana Staudt and Murray, \{Heather C.\} and Findlay, \{Izac J.\} and Jackson, \{Evangeline R.\} and McEwen, \{Holly P.\} and Douglas, \{Alicia M.\} and Tabitha McLachlan and Schjenken, \{John E.\} and Skerrett-Byrne, \{David A.\} and Honggang Huang and Melo-Braga, \{Marcella N.\} and Plank, \{Maximilian W.\} and Frank Alvaro and Janis Chamberlain and Iuliis, \{Geoff De\} and \{John Aitken\}, R. and Brett Nixon and Wei, \{Andrew H.\} and Enjeti, \{Anoop K.\} and Yizhou Huang and Lock, \{Richard B.\} and Larsen, \{Martin R.\} and Heather Lee and Vijesh Vaghjiani and Cain, \{Jason E.\} and \{de Bock\}, \{Charles E.\} and Verrills, \{Nicole M.\} and Dun, \{Matthew D.\}",

note = "Funding Information: Acknowledgments:N.SmithfromtheUniversityofNewcastleAnalyticalandBiomolecular ResearchFacility(ABRF)providedMSsupport.TheAcademicandResearchComputingSupport (ARCS)team,withinITServicesattheUniversityofNewcastle,providedhigh-performance computing(HPC)infrastructureforsupportingthebioinformatics.Figure1wascreatedusing www.biorender.com.SummarycartooninFig.7wascreatedwiththankstowww. somersault1824.com.GlaxoSmithKlineprovidedtheNOX2inhibitorGSK2795039andAptaBio providedpan-NOXinhibitorAPX115.Funding:ThisstudywassupportedbyCancerInstitute NSWFellowships(M.D.D.,N.MV ., andH.L.).M.D.D.issupportedbyanNHMRCInvestigatorgrant, GNT1173892.ThisprojectissupportedbyanNHMRCIdeaGrantAPP1188400.R.B.L.is supportedbyanNHMRCFellowship(APP1157871).Thecontentsofthepublishedmaterialare solely the responsibility of the research institutions involved or individual authors and do not reflect the views of NHMRC. Grants from the Hunter Medical Research Institute, Hunter Children{\textquoteright}s Research Foundation, Jurox Animal Health, Zebra Equities, Hunter District Hunting ClubandSkiforKids,andtheEstateofJamesScottLawriegrants.TheARCprovidedaFuture Fellowship(N.M.V .), HNE/NSWHealthPathology/CMNaClinicalTr ansla tionalResearch Fellowship(A.K.E.)andtheCancerInstituteNSWinpartnershipwiththeFa culty ofHealthand MedicinefromtheUniversityofNewcastlefundedtheMSplatform.AuthorContributions: J.R.S.,Z.P .G., M.R.L.,N.M.V ., andM.D.D.conceivedanddesignedthestudyandinterpretedthe results;Z.P .G., J.R.S.,A.M.,R.J.D.,H.C.M.,I.J.F ., M.R.L.,andM.D.D.conductedtheexperimentsand performeddataanalysis;D.S.,I.J.F ., H.C.M.,J.E.S.,D.A.S.-B.,M.N.M.-B.,H.H.,V .V ., Y .H., andC.E.d.B. helped with experimental work and/or interpretation of results; D.A.S.-B. assisted with bioinformaticanalyses;M.W .P ., G.D.I,B.N.,R.J.A.,F .A., J.E.C.,andR.B.L.provideddiscipline-specificexpertise;A.K.E.andA.H.W .assistedwithobtainingandprocessingofpatientsamples; J.R.S.,Z.P .G., A.M.D.,andM.D.D.wroteandeditedthemanuscript;andallauthorsdiscussedthe results and commented on the manuscript. Competing Interests: M.W .P . is a full-time employeeofGlaxoSmithKline.Theotherauthorsdeclarethattheyhav enocompetinginterests. Dataandmaterialsavailability:MT Aagreementsandpublicallyaccessibledataasdescribed inMaterialsandMethods. Publisher Copyright: {\textcopyright} 2023 The Authors.",

year = "2023",

month = mar,

day = "28",

doi = "10.1126/scisignal.abp9586",

language = "English",

volume = "16",

journal = "Science Signaling",

issn = "1945-0877",

publisher = "American Association for the Advancement of Science (AAAS)",

number = "778",

}

Germon, ZP, Sillar, JR, Mannan, A, Duchatel, RJ, Staudt, D, Murray, HC, Findlay, IJ, Jackson, ER, McEwen, HP, Douglas, AM, McLachlan, T, Schjenken, JE, Skerrett-Byrne, DA, Huang, H, Melo-Braga, MN, Plank, MW, Alvaro, F, Chamberlain, J, Iuliis, GD, John Aitken, R, Nixon, B, Wei, AH, Enjeti, AK, Huang, Y, Lock, RB, Larsen, MR, Lee, H, Vaghjiani, V, Cain, JE, de Bock, CE, Verrills, NM & Dun, MD 2023, 'Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies', Science Signaling, vol. 16, no. 778, eabp9586. https://doi.org/10.1126/scisignal.abp9586

TY - JOUR

T1 - Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies

AU - Germon, Zacary P.

AU - Sillar, Jonathan R.

AU - Mannan, Abdul

AU - Duchatel, Ryan J.

AU - Staudt, Dilana

AU - Murray, Heather C.

AU - Findlay, Izac J.

AU - Jackson, Evangeline R.

AU - McEwen, Holly P.

AU - Douglas, Alicia M.

AU - McLachlan, Tabitha

AU - Schjenken, John E.

AU - Skerrett-Byrne, David A.

AU - Huang, Honggang

AU - Melo-Braga, Marcella N.

AU - Plank, Maximilian W.

AU - Alvaro, Frank

AU - Chamberlain, Janis

AU - Iuliis, Geoff De

AU - John Aitken, R.

AU - Nixon, Brett

AU - Wei, Andrew H.

AU - Enjeti, Anoop K.

AU - Huang, Yizhou

AU - Lock, Richard B.

AU - Larsen, Martin R.

AU - Lee, Heather

AU - Vaghjiani, Vijesh

AU - Cain, Jason E.

AU - de Bock, Charles E.

AU - Verrills, Nicole M.

AU - Dun, Matthew D.

N1 - Funding Information: Acknowledgments:N.SmithfromtheUniversityofNewcastleAnalyticalandBiomolecular ResearchFacility(ABRF)providedMSsupport.TheAcademicandResearchComputingSupport (ARCS)team,withinITServicesattheUniversityofNewcastle,providedhigh-performance computing(HPC)infrastructureforsupportingthebioinformatics.Figure1wascreatedusing www.biorender.com.SummarycartooninFig.7wascreatedwiththankstowww. somersault1824.com.GlaxoSmithKlineprovidedtheNOX2inhibitorGSK2795039andAptaBio providedpan-NOXinhibitorAPX115.Funding:ThisstudywassupportedbyCancerInstitute NSWFellowships(M.D.D.,N.MV ., andH.L.).M.D.D.issupportedbyanNHMRCInvestigatorgrant, GNT1173892.ThisprojectissupportedbyanNHMRCIdeaGrantAPP1188400.R.B.L.is supportedbyanNHMRCFellowship(APP1157871).Thecontentsofthepublishedmaterialare solely the responsibility of the research institutions involved or individual authors and do not reflect the views of NHMRC. Grants from the Hunter Medical Research Institute, Hunter Children’s Research Foundation, Jurox Animal Health, Zebra Equities, Hunter District Hunting ClubandSkiforKids,andtheEstateofJamesScottLawriegrants.TheARCprovidedaFuture Fellowship(N.M.V .), HNE/NSWHealthPathology/CMNaClinicalTr ansla tionalResearch Fellowship(A.K.E.)andtheCancerInstituteNSWinpartnershipwiththeFa culty ofHealthand MedicinefromtheUniversityofNewcastlefundedtheMSplatform.AuthorContributions: J.R.S.,Z.P .G., M.R.L.,N.M.V ., andM.D.D.conceivedanddesignedthestudyandinterpretedthe results;Z.P .G., J.R.S.,A.M.,R.J.D.,H.C.M.,I.J.F ., M.R.L.,andM.D.D.conductedtheexperimentsand performeddataanalysis;D.S.,I.J.F ., H.C.M.,J.E.S.,D.A.S.-B.,M.N.M.-B.,H.H.,V .V ., Y .H., andC.E.d.B. helped with experimental work and/or interpretation of results; D.A.S.-B. assisted with bioinformaticanalyses;M.W .P ., G.D.I,B.N.,R.J.A.,F .A., J.E.C.,andR.B.L.provideddiscipline-specificexpertise;A.K.E.andA.H.W .assistedwithobtainingandprocessingofpatientsamples; J.R.S.,Z.P .G., A.M.D.,andM.D.D.wroteandeditedthemanuscript;andallauthorsdiscussedthe results and commented on the manuscript. Competing Interests: M.W .P . is a full-time employeeofGlaxoSmithKline.Theotherauthorsdeclarethattheyhav enocompetinginterests. Dataandmaterialsavailability:MT Aagreementsandpublicallyaccessibledataasdescribed inMaterialsandMethods. Publisher Copyright: © 2023 The Authors.

PY - 2023/3/28

Y1 - 2023/3/28

N2 - Mutations in the type III receptor tyrosine kinase FLT3 are frequent in patients with acute myeloid leukemia (AML) and are associated with a poor prognosis. AML is characterized by the overproduction of reactive oxygen species (ROS), which can induce cysteine oxidation in redox-sensitive signaling proteins. Here, we sought to characterize the specific pathways affected by ROS in AML by assessing oncogenic signaling in primary AML samples. The oxidation or phosphorylation of signaling proteins that mediate growth and proliferation was increased in samples from patient subtypes with FLT3 mutations. These samples also showed increases in the oxidation of proteins in the ROS-producing Rac/NADPH oxidase-2 (NOX2) complex. Inhibition of NOX2 increased the apoptosis of FLT3-mutant AML cells in response to FLT3 inhibitors. NOX2 inhibition also reduced the phosphorylation and cysteine oxidation of FLT3 in patient-derived xenograft mouse models, suggesting that decreased oxidative stress reduces the oncogenic signaling of FLT3. In mice grafted with FLT3 mutant AML cells, treatment with a NOX2 inhibitor reduced the number of circulating cancer cells, and combining FLT3 and NOX2 inhibitors increased survival to a greater extent than either treatment alone. Together, these data raise the possibility that combining NOX2 and FLT3 inhibitors could improve the treatment of FLT3 mutant AML.

AB - Mutations in the type III receptor tyrosine kinase FLT3 are frequent in patients with acute myeloid leukemia (AML) and are associated with a poor prognosis. AML is characterized by the overproduction of reactive oxygen species (ROS), which can induce cysteine oxidation in redox-sensitive signaling proteins. Here, we sought to characterize the specific pathways affected by ROS in AML by assessing oncogenic signaling in primary AML samples. The oxidation or phosphorylation of signaling proteins that mediate growth and proliferation was increased in samples from patient subtypes with FLT3 mutations. These samples also showed increases in the oxidation of proteins in the ROS-producing Rac/NADPH oxidase-2 (NOX2) complex. Inhibition of NOX2 increased the apoptosis of FLT3-mutant AML cells in response to FLT3 inhibitors. NOX2 inhibition also reduced the phosphorylation and cysteine oxidation of FLT3 in patient-derived xenograft mouse models, suggesting that decreased oxidative stress reduces the oncogenic signaling of FLT3. In mice grafted with FLT3 mutant AML cells, treatment with a NOX2 inhibitor reduced the number of circulating cancer cells, and combining FLT3 and NOX2 inhibitors increased survival to a greater extent than either treatment alone. Together, these data raise the possibility that combining NOX2 and FLT3 inhibitors could improve the treatment of FLT3 mutant AML.

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U2 - 10.1126/scisignal.abp9586

DO - 10.1126/scisignal.abp9586

M3 - Article

C2 - 36976863

AN - SCOPUS:85151114308

SN - 1945-0877

VL - 16

JO - Science Signaling

JF - Science Signaling

IS - 778

M1 - eabp9586

ER -

Blockade of ROS production inhibits oncogenic signaling in acute myeloid leukemia and amplifies response to recision therapies

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