Abstract
Cancers that exhibit the Warburg effect may elevate expression of glyoxylase 1 (GLO1) to detoxify the toxic glycolytic byproduct methylglyoxal (MG) and inhibit the formation of pro-apoptotic advanced glycation endproducts (AGEs). Inhibition of GLO1 in cancers that up-regulate glycolysis has been proposed as a therapeutic targeting strategy, but this approach has not been evaluated for glioblastoma multiforme (GBM), the most aggressive and difficult to treat malignancy of the brain. Elevated GLO1 expression in GBM was established in patient tumors and cell lines using bioinformatics tools and biochemical approaches. GLO1 inhibition in GBM cell lines and in an orthotopic xenograft GBM mouse model was examined using both small molecule and short hairpin RNA (shRNA) approaches. Inhibition of GLO1 with S-(p-bromobenzyl) glutathione dicyclopentyl ester (p-BrBzGSH(Cp)2) increased levels of the DNA-AGE N2-1-(carboxyethyl)-2′-deoxyguanosine (CEdG), a surrogate biomarker for nuclear MG exposure; substantially elevated expression of the immunoglobulin-like receptor for AGEs (RAGE); and induced apoptosis in GBM cell lines. Targeting GLO1 with shRNA similarly increased CEdG levels and RAGE expression, and was cytotoxic to glioma cells. Mice bearing orthotopic GBM xenografts treated systemically with p-BrBzGSH(Cp)2 exhibited tumor regression without significant off-target effects suggesting that GLO1 inhibition may have value in the therapeutic management of these drug-resistant tumors.
Highlights
According to the World Health Organization (Geneva, Switzerland), Grade IV glioblastoma multiforme (GBM) is one of the most aggressive and clinically challenging cancers of the central nervous system [1]
To evaluate glyoxylase 1 (GLO1) in GBM, we examined data from The Cancer Genome Atlas (TCGA) and performed gene and protein expression analyses from surgical GBM specimens and glioma cell
These results suggest that sRAGE maturation from2t.h4.eGpLlOas1mInahimbiteiomnbInrcarneaesebsyNmuceletaarllMopGraontdeiDnNasAe-sApGaErLtieavlellys protects U87 and T98 cells against the cytotoxic effects of GLO1 inhibition
Summary
According to the World Health Organization (Geneva, Switzerland), Grade IV glioblastoma multiforme (GBM) is one of the most aggressive and clinically challenging cancers of the central nervous system [1]. Measurement of GLO1 mRNA by RT-qPCR revealed modest up-regulation in both T98 (two-fold, * p < 0.05) and U87 (1.4-fold) relative to normal glial cells (astrocytes, Figure 2E). Consistent with this expression pattern, Western blots revealed 1.9- and. ShRNA Inhibition of GLO1 in GBM Induces RAGE Expression and Increases DNA-AGEs 2.6. ShRNA Inhibition of GLO1 in GBM Induces RAGE Expression and Increases DNA-AGEs To show that gene expression and protein changes observed upon treatment with p-BrBzGSH(Cp) were thTeoressuhlotwof GthLaOt 1giennheibietxiopnreassnidonrulaenodutpsrmotaelinl mcohlaencuglees ofofb-tsaerrgveetdeffuepcotsn, twtreoaGtmLeOn1t-swpeitchific shopr-tBhrBazirGpSinHR(CNpA)2sw(sehreRNthAe -r2e8sualnt dofshGRLNOA1 -i3n1h)ibaintidona annodn-rtualregeotuint gsmshaRllNmAol(eschu-lNe To)ffw-taerrgeeitnetrfofedcutsc,ed inttowTo98GaLnOd1U-s8p7ecceiflilcs.sBheocratuhsaeiropfitnheRsNtrAonsg(sMhRGN-mAe-d28iataenddcyshtoRtNoxAic-i3t1y)oafnGdLOa 1nionnh-tibaritgieotnin, kgnsohcRkNdoAwn T98(GshLcl-OoN1nTei)nswheiebxrihetiiobinnitt,rekodndosuecckvedderoiewntgnorToTw9988thcalnordneetUasr8ed7xahctieibollinste. In T98 cells, RAGE mRNA expression increased ~2-fold as a result of GLO1 knockdown (p < 0.0I0n1T; F98igcuerlels, ARA). Inhibiting GLO1 abrogated tumor growth in vivo without any discernible off-target effects on surrounding brain cells
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