The c-Myc/TBX3 axis promotes cellular transformation of sarcoma-initiating cells

Damerell, Victoria; Ambele, Melvin Anyasi; Salisbury, Shanel; Neumann-Mufweba, Alexis; Durandt, Chrisna; Pepper, Michael Sean; Prince, Sharon

dc.contributor.author	Damerell, Victoria
dc.contributor.author	Ambele, Melvin Anyasi
dc.contributor.author	Salisbury, Shanel
dc.contributor.author	Neumann-Mufweba, Alexis
dc.contributor.author	Durandt, Chrisna
dc.contributor.author	Pepper, Michael Sean
dc.contributor.author	Prince, Sharon
dc.date.accessioned	2022-07-29T05:28:39Z
dc.date.available	2022-07-29T05:28:39Z
dc.date.issued	2022-01-25
dc.description.abstract	Sarcomas are highly aggressive cancers of mesenchymal origin whose clinical management is highly complex. This is partly due to a lack of understanding of the molecular mechanisms underpinning the transformation of mesenchymal stromal/stem cells (MSCs) which are presumed to be the sarcoma-initiating cells. c-Myc is amplified/ overexpressed in a range of sarcomas where it has an established oncogenic role and there is evidence that it contributes to the malignant transformation of MSCs. T-box transcription factor 3 (TBX3) is upregulated by c-Myc in a host of sarcoma subtypes where it promotes proliferation, tumor formation, migration, and invasion. This study investigated whether TBX3 is a c-Myc target in human MSCs (hMSCs) and whether overexpressing TBX3 in hMSCs can phenocopy c-Myc overexpression to promote malignant transformation. Using siRNA, qRT-PCR, luciferase reporter and chromatinimmunoprecipitation assays, we show that c-Myc binds and directly activates TBX3 transcription in hMSCs at a conserved E-box motif. When hMSCs were engineered to stably overexpress TBX3 using lentiviral gene transfer and the resulting cells characterised in 2D and 3D, the overexpression of TBX3 was shown to promote self-renewal, bypass senescence, and enhance proliferation which corresponded with increased levels of cell cycle progression markers (cyclin A, cyclin B1, CDK2) and downregulation of the p14ARF/ MDM2/p53 tumor suppressor pathway. Furthermore, TBX3 promoted the migratory and invasive ability of hMSCs which associated with increased levels of markers of migration (Vimentin, SLUG, SNAIL, TWIST1) and invasion (MMP2, MMP9). Transcriptomic analysis revealed that genes upregulated upon TBX3 overexpression overlapped with c-myc targets, were involved in cell cycle progression, and were associated with sarcomagenesis. Together, the data described indicate that the c-Myc/TBX3 oncogenic molecular pathway may be a key mechanism that transforms hMSCs into sarcomas.	en_US
dc.description.department	Immunology	en_US
dc.description.department	Oral Pathology and Oral Biology	en_US
dc.description.librarian	dm2022	en_US
dc.description.sponsorship	South Africa Medical Research Council (SAMRC); National Research Foundation (NRF); Cancer Association of South Africa (CANSA); Universities of Cape Town and Pretoria.	en_US
dc.description.uri	https://www.frontiersin.org/journals/oncology	en_US
dc.identifier.citation	Damerell, V., Ambele, M.A., Salisbury, S., Neumann-Mufweba, A., Durandt, C., Pepper, M.S. & Prince, S. (2022) The c-Myc/TBX3 Axis Promotes Cellular Transformation of Sarcoma-Initiating Cells. Frontiers in Oncology 11:801691, doi: 10.3389/fonc.2021.801691.	en_US
dc.identifier.issn	2234-943X (online)
dc.identifier.issn	10.3389/fonc.2021.801691
dc.identifier.uri	https://repository.up.ac.za/handle/2263/86574
dc.language.iso	en	en_US
dc.publisher	Frontiers Media S.A.	en_US
dc.rights	© 2022 Damerell, Ambele, Salisbury, Neumann-Mufweba, Durandt, Pepper and Prince. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY).	en_US
dc.subject	Mesenchymal stromal/stem cells (MSCs)	en_US
dc.subject	Sarcoma	en_US
dc.subject	c-Myc	en_US
dc.subject	Oncogene	en_US
dc.subject	Tumorigenesis	en_US
dc.subject	T-box transcription factor 3 (TBX3)	en_US
dc.title	The c-Myc/TBX3 axis promotes cellular transformation of sarcoma-initiating cells	en_US
dc.type	Article	en_US