Human Mesenchymal Stem Cell Homing to Glioma Stem Cell Xenografts

Wildburger, Norelle Christine

Human Mesenchymal Stem Cell Homing to Glioma Stem Cell Xenografts

dc.contributor.advisor	Nilsson, Carol L
dc.contributor.committeeMember	Emmett, Mark R
dc.contributor.committeeMember	Taglialatela, Giulio
dc.contributor.committeeMember	Hamill, Owen
dc.contributor.committeeMember	Kroes, Roger A
dc.contributor.committeeMember	Conrad, Charles A
dc.contributor.committeeMember	Lang , Frederick F
dc.contributor.committeeMember	Ullrich, Robert L
dc.creator	Wildburger, Norelle Christine
dc.date.accessioned	2016-05-05T21:22:02Z
dc.date.available	2016-05-05T21:22:02Z
dc.date.created	2015-08
dc.date.submitted	August 2015
dc.date.updated	2016-05-05T21:22:02Z
dc.description.abstract	Glioblastoma (GBM) is the most common adult primary brain tumor with a median survival of approximately one year. The current standard of care for GBM includes the maximal surgical resection, followed by concurrent chemotherapy, radiotherapy, and in some cases and adjuvant chemotherapy. Yet, despite this aggressive multimodal approach, GBM is a nearly universally fatal disease. The poor outcome is in large part due to the lack of effective therapeutic agents that can penetrate the blood-brain and blood-tumor barriers to deliver anti-glioma therapeutics to the whole tumor and the microsatellite populations of tumor cells scattered throughout the brain parenchyma. However, bone marrow-derived human mesenchymal stem cells (hMSCs) offer a viable alternative to enhance therapeutic delivery – one that overcomes current limitations. hMSCs are a population of cells with the capability of self-renewal and multilineage differentiation that can be safely isolated in routine clinical procedures and pose no ethical quandaries. hMSCs demonstrate an intrinsic tropism towards gliomas and are capable of migrating across the blood-brain and blood-tumor barriers. These cells have been used as delivery vehicles to convey immunotherapy, enzymes for chemotherapeutic pro-drugs, and oncolytic viruses with some success in pre-clinical models. Despite the promise of hMSCs, previous studies have relied for the most part on xenografts derived from commercially available immortalized GBM cell lines. These cell lines poorly mimic patient tumors in vivo and thus do not adequately translate into the clinical setting. Glioma stem cells (GSCs) rectify this shortcoming by faithfully recapitulating the genotype and phenotype of the human tumor from which they were isolated. However, studies from our collaborators at MD Anderson Cancer Center show that hMSCs demonstrate variable tropism towards GSC-derived tumors (GSC xenografts; GSCXs). Those GSC xenografts that attract hMSCs are referred to as ‘attractors’, whereas those that fail to evoke hMSC homing are designated ‘non-attractors’. The underlying biological mechanism of hMSCs differential homing capacity towards GSCXs is virtually unknown. Given the clinical potential of hMSCs as therapeutic delivery vehicles of anti-glioma agents, the rationale behind this project was to elucidate the molecular mechanisms that underlie the variable localization of hMSCs to gliomas by use of GSCXs as a clinically relevant brain tumor model. The long-term goal is to understand the essential factors in hMSC homing to gliomas, in order to successfully harness hMSCs for clinical use or to identify patients most appropriate for hMSC-mediated therapeutic delivery. This work is significant because the outcomes will identify differences between attractor and non-attractor GSCXs, which will be critical in advancing our knowledge for continued development of hMSCs as a viable therapeutic strategy.
dc.format.mimetype	application/pdf
dc.identifier.uri	http://hdl.handle.net/2152.3/643
dc.subject	Glioblastoma, Glioma stem cells, xenografts, bone marrow-derived mesenchymal stem cells, homing, lipidomics, proteomics, transcriptomics
dc.title	Human Mesenchymal Stem Cell Homing to Glioma Stem Cell Xenografts
dc.type	Thesis
dc.type.material	text
thesis.degree.department	Neuroscience
thesis.degree.discipline	Neuroscience
thesis.degree.grantor	The University of Texas Medical Branch at Galveston
thesis.degree.level	Doctoral
thesis.degree.name	Neuroscience (Doctoral)