Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma

The oncogenic transcription factor STAT3 is aberrantly activated in over 70% of human tumours, including Multiple myeloma (MM). The present studies use both genetic and chemical tools to validate STAT3 as a therapeutic target, and demonstrate the anti-MM activity of a novel small molecule STAT3 inhi...

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Main Author: Croucher, Danielle
Other Authors: Trudel, Suzanne
Language:en_ca
Published: 2013
Subjects:
Online Access:http://hdl.handle.net/1807/35594
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spelling ndltd-LACETR-oai-collectionscanada.gc.ca-OTU.1807-355942013-11-02T03:43:50ZTargeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple MyelomaCroucher, DanielleSTAT3Targeted therapeuticsMultiple MyelomaSmall molecule inhibitors03070992The oncogenic transcription factor STAT3 is aberrantly activated in over 70% of human tumours, including Multiple myeloma (MM). The present studies use both genetic and chemical tools to validate STAT3 as a therapeutic target, and demonstrate the anti-MM activity of a novel small molecule STAT3 inhibitor, BP-4-018. We show that shRNA-mediated STAT3 knockdown induces apoptosis in human myeloma cell lines (HMCLs). We translate these findings to a therapeutically relevant setting by demonstrating the broad anti-MM activity of BP-4-018 against HCMLs and primary patient samples, and demonstrate that BP-4-018 remains active against HMCLs co-cultured with bone marrow stroma. Inhibiting STAT3 via shRNA knockdown and BP-4-018 suppresses STAT3 transcriptional activity and down-regulates anti-apoptotic and proliferative STAT3 target genes. Finally, we show that BP-4-018 has activity in vivo, both alone and combined with subtherapeutic doses of bortezomib, without significant toxicities. Taken together, these data support the utility of STAT3 inhibitors for MM treatment.Trudel, Suzanne2013-062013-07-11T18:05:05ZNO_RESTRICTION2013-07-11T18:05:05Z2013-07-11Thesishttp://hdl.handle.net/1807/35594en_ca
collection NDLTD
language en_ca
sources NDLTD
topic STAT3
Targeted therapeutics
Multiple Myeloma
Small molecule inhibitors
0307
0992
spellingShingle STAT3
Targeted therapeutics
Multiple Myeloma
Small molecule inhibitors
0307
0992
Croucher, Danielle
Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma
description The oncogenic transcription factor STAT3 is aberrantly activated in over 70% of human tumours, including Multiple myeloma (MM). The present studies use both genetic and chemical tools to validate STAT3 as a therapeutic target, and demonstrate the anti-MM activity of a novel small molecule STAT3 inhibitor, BP-4-018. We show that shRNA-mediated STAT3 knockdown induces apoptosis in human myeloma cell lines (HMCLs). We translate these findings to a therapeutically relevant setting by demonstrating the broad anti-MM activity of BP-4-018 against HCMLs and primary patient samples, and demonstrate that BP-4-018 remains active against HMCLs co-cultured with bone marrow stroma. Inhibiting STAT3 via shRNA knockdown and BP-4-018 suppresses STAT3 transcriptional activity and down-regulates anti-apoptotic and proliferative STAT3 target genes. Finally, we show that BP-4-018 has activity in vivo, both alone and combined with subtherapeutic doses of bortezomib, without significant toxicities. Taken together, these data support the utility of STAT3 inhibitors for MM treatment.
author2 Trudel, Suzanne
author_facet Trudel, Suzanne
Croucher, Danielle
author Croucher, Danielle
author_sort Croucher, Danielle
title Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma
title_short Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma
title_full Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma
title_fullStr Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma
title_full_unstemmed Targeting Aberrant STAT3 Signaling as a Therapeutic Strategy for Multiple Myeloma
title_sort targeting aberrant stat3 signaling as a therapeutic strategy for multiple myeloma
publishDate 2013
url http://hdl.handle.net/1807/35594
work_keys_str_mv AT croucherdanielle targetingaberrantstat3signalingasatherapeuticstrategyformultiplemyeloma
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