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EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
by Hoffer Konstantin , Brend Tim , Struve, Nina , Bagley, Stephen J , Kurian, Kathreena M , Faulkner, Claire , Anna-Sophie, Weik , Müller-Goebel Justus , Henze, Marvin , Stead, Lucy F , Bußmann Lara , Short, Susan C , Petersen, Cordula , Krug Leonie , Rothkamm Kai , O´ Rourke Donald M , Kriegs Malte , Rieckmann Thorsten , Ott, Leonie , Binder, Zev A , Morrissette Jennifer J D , Schüller, Ulrich
in Brain cancer / Deoxyribonucleic acid / DNA / DNA damage / DNA methyltransferase / DNA repair / Epidermal growth factor / Glioblastoma / Methylguanine / Mismatch repair / MMR protein / MSH2 protein / MSH6 protein / O6-methylguanine-DNA methyltransferase / Protein expression / Temozolomide / Tumors
2020
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EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
by Hoffer Konstantin , Brend Tim , Struve, Nina , Bagley, Stephen J , Kurian, Kathreena M , Faulkner, Claire , Anna-Sophie, Weik , Müller-Goebel Justus , Henze, Marvin , Stead, Lucy F , Bußmann Lara , Short, Susan C , Petersen, Cordula , Krug Leonie , Rothkamm Kai , O´ Rourke Donald M , Kriegs Malte , Rieckmann Thorsten , Ott, Leonie , Binder, Zev A , Morrissette Jennifer J D , Schüller, Ulrich
in Brain cancer / Deoxyribonucleic acid / DNA / DNA damage / DNA methyltransferase / DNA repair / Epidermal growth factor / Glioblastoma / Methylguanine / Mismatch repair / MMR protein / MSH2 protein / MSH6 protein / O6-methylguanine-DNA methyltransferase / Protein expression / Temozolomide / Tumors
2020
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EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
by Hoffer Konstantin , Brend Tim , Struve, Nina , Bagley, Stephen J , Kurian, Kathreena M , Faulkner, Claire , Anna-Sophie, Weik , Müller-Goebel Justus , Henze, Marvin , Stead, Lucy F , Bußmann Lara , Short, Susan C , Petersen, Cordula , Krug Leonie , Rothkamm Kai , O´ Rourke Donald M , Kriegs Malte , Rieckmann Thorsten , Ott, Leonie , Binder, Zev A , Morrissette Jennifer J D , Schüller, Ulrich
in Brain cancer / Deoxyribonucleic acid / DNA / DNA damage / DNA methyltransferase / DNA repair / Epidermal growth factor / Glioblastoma / Methylguanine / Mismatch repair / MMR protein / MSH2 protein / MSH6 protein / O6-methylguanine-DNA methyltransferase / Protein expression / Temozolomide / Tumors
2020

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EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma
Journal Article

EGFRvIII upregulates DNA mismatch repair resulting in increased temozolomide sensitivity of MGMT promoter methylated glioblastoma

Hoffer Konstantin,
Brend Tim,
Struve, Nina,
Bagley, Stephen J,
Kurian, Kathreena M,
Faulkner, Claire,
Anna-Sophie, Weik,
Müller-Goebel Justus,
Henze, Marvin,
Stead, Lucy F,
Bußmann Lara,
Short, Susan C,
Petersen, Cordula,
Krug Leonie,
Rothkamm Kai,
O´ Rourke Donald M,
Kriegs Malte,
Rieckmann Thorsten,
Ott, Leonie,
Binder, Zev A,
Morrissette Jennifer J D,
Schüller, Ulrich
2020
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Overview
The oncogene epidermal growth factor receptor variant III (EGFRvIII) is frequently expressed in glioblastomas (GBM) but its impact on therapy response is still under controversial debate. Here we wanted to test if EGFRvIII influences the sensitivity towards the alkylating agent temozolomide (TMZ). Therefore, we retrospectively analyzed the survival of 336 GBM patients, demonstrating that under standard treatment, which includes TMZ, EGFRvIII expression is associated with prolonged survival, but only in patients with O6-methylguanine-DNA methyltransferase (MGMT) promoter methylated tumors. Using isogenic GBM cell lines with endogenous EGFRvIII expression we could demonstrate that EGFRvIII increases TMZ sensitivity and results in enhanced numbers of DNA double-strand breaks and a pronounced S/G2-phase arrest after TMZ treatment. We observed a higher expression of DNA mismatch repair (MMR) proteins in EGFRvIII+ cells and patient tumor samples, which was most pronounced for MSH2 and MSH6. EGFRvIII-specific knockdown reduced MMR protein expression thereby increasing TMZ resistance. Subsequent functional kinome profiling revealed an increased activation of p38- and ERK1/2-dependent signaling in EGFRvIII expressing cells, which regulates MMR protein expression downstream of EGFRvIII. In summary, our results demonstrate that the oncoprotein EGFRvIII sensitizes a fraction of GBM to current standard of care treatment through the upregulation of DNA MMR.
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Publisher
Nature Publishing Group
Subject

Brain cancer

/ Deoxyribonucleic acid

/ DNA

/ DNA damage

/ DNA methyltransferase

/ DNA repair

/ Epidermal growth factor

/ Glioblastoma

/ Methylguanine

/ Mismatch repair

/ MMR protein

/ MSH2 protein

/ MSH6 protein

/ O6-methylguanine-DNA methyltransferase

/ Protein expression

/ Temozolomide

/ Tumors

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