Everolimus improves the efficacy of dasatinib in PDGFRα-driven glioma

Miklja, Zachary; Vn, Yadav; Cartaxo, Rodrigo; Siada, Ruby; Mullan, Brendan; Stallard, Stefanie; Paul, Alyssa; Ak, Bruzek; Wierzbicki, Kyle; Yang, Tao; García, Teresa; Wolfe, Ian; Parmar, Hemant; Leonard, Marcia; Pl, Robertson; Garton, Hugh; Venneti, Sriram; Kumar‐Sinha, Chandan; Chinnaiyan, Arul M.; Mody, Rajen; Pp, Manjunath; Tn, Phoenix; Bl, Marini; Koschmann, Carl

doi:10.1101/2019.12.28.19015974

Cited by 8 publications

(10 citation statements)

References 38 publications

(83 reference statements)

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“…In contrast, their differential response to statins ranged from modest (DIPG-XIII) to substantial (DIPG-XIII-P*) ( Supplementary Figures 6E-H ). Notably, the murine cell line of P 53 P DGFRA H3 K 27M DIPG (PPK cells), which has been demonstrated to replicate the H3K27M DIPG biology 38 and was similarly established in culture as either GS or DGC, also displayed differential sensitivity to Phenformin and Pitavastatin ( Supplementary Figures 6J-K ).…”

Section: Resultsmentioning

confidence: 99%

“…IUE was performed using sterile technique on isoflurane/oxygen-anesthetized pregnant C57BL/6 or CD1 females at E13.5. Tumors were generated with lateral ventricle (forebrain) introduction of plasmids: (1) PB-CAG-DNp53-Ires-Luciferase (dominant negative T P 53), (2) PB-CAG-PdgfraD824V-Ires-eGFP ( P DGFRA D842V), and (3) PB-CAG-H3.3 K 27M-Ires-eGFP (H3K27M), and therefore referred to as “PPK” model 38 . PPK gliomaspheres were cultured in base media containing Neurobasal-A medium (1X), MEM sodium pyruvate solution (1mM), MEM Non-Essential Amino Acids (1X), L-glutamine (2 mM), Antibiotic-Antimycotic (1X), and supplemented with fresh B27, N2, heparin (2 μg/mL), EGF (20 ng/mL), FGF (20 ng/mL).…”

Section: Methodsmentioning

confidence: 99%

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Therapeutic targeting of differentiation state-dependent metabolic vulnerabilities in DIPG

Mbah

Myers

Chung

et al. 2022

Preprint

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H3K27M diffuse intrinsic pontine gliomas (DIPG) exhibit cellular heterogeneity comprising less-differentiated, stem-like glioma cells that resemble oligodendrocyte precursors (OPC) and more differentiated astrocyte (AC)-like cells. H3K27M DIPG stem-like cells exhibit tumor-seeding capabilities in vivo, a feature lost or greatly diminished in the more differentiated AC-like cells. In this study, we established isogenic in vitro models of DIPG that closely recapitulated the OPC-like and AC-like phenotypes of DIPG cells. Using these tools, we performed transcriptomics, metabolomics, and bioenergetic profiling to identify metabolic programs operative in the different cellular states. From this, we defined new strategies to selectively target metabolic vulnerabilities within the specific tumor populations. Namely, we showed that the AC-like cells exhibited a more mesenchymal phenotype and were thus sensitized to ferroptotic cell death. In contrast, OPC-like cells upregulated cholesterol metabolism and mitochondrial oxidative phosphorylation (OXPHOS) and were accordingly more sensitive to statins and OXPHOS inhibitors. Additionally, statins and OXPHOS inhibitors showed efficacy and extended survival in preclinical orthotopic models established with stem-like H3K27M DIPG cells. Together, this study demonstrates that cellular subtypes within DIPGs harbor distinct metabolic vulnerabilities that can be uniquely and selectively targeted for therapeutic gain.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Therapeutic targeting of differentiation state-dependent metabolic vulnerabilities in DIPG

Mbah

Myers

Chung

et al. 2022

Preprint

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“…The experience of everolimus in this age group may be of particular importance given the reservations expressed about the ability to provide clinical doses of the drug at sufficient concentrations to elicit significant inhibition of Pg-P (52). Notably, another recent study reported the use of everolimus to improve the CNS penetration of dasatinib in PDGFRA-driven high grade gliomas in children (53). Here, the authors found an increase in both plasma (11.2 ng/mL to 31.5 ng/mL) and CSF (0.44 ng/mL to 0.91 mg/mL) dasatinib levels in two patients after one week of dasatinib monotherapy and then after two cycles of dual therapy with dasatinib and everolimus (53), and pointed to adult phase I studies of higher doses of everolimus (up to 70 mg weekly) that were well-tolerated and resulted in mean peak levels of everolimus 10-fold higher than standard regimens (54).…”

Section: Discussionmentioning

confidence: 99%

Repurposing Vandetanib plus Everolimus for the Treatment ofACVR1-Mutant Diffuse Intrinsic Pontine Glioma

Carvalho

Richardson²,

Olaciregui

et al. 2021

Cancer Discovery

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Somatic mutations in ACVR1 are found in a quarter of children with diffuse intrinsic pontine glioma (DIPG), however there are no ACVR1 inhibitors licensed for the disease. Using an Artificial Intelligence-based platform to search for approved compounds for ACVR1-mutant DIPG, the combination of vandetanib and everolimus was identified as a possible therapeutic approach. Vandetanib, an inhibitor of VEGFR/RET/EGFR, was found to target ACVR1 (Kd=150nM) and reduce DIPG cell viability in vitro, but has limited ability to cross the bloodbrain-barrier. In addition to mTOR, everolimus inhibits ABCG2 (BCRP) and ABCB1 (P-gp) transporters, and was synergistic in DIPG cells when combined with vandetanib in vitro. This combination is well-tolerated in vivo, and significantly extended survival and reduced tumor burden in an orthotopic ACVR1-mutant patient-derived DIPG xenograft model. Four patients with ACVR1-mutant DIPG were treated with vandetanib plus mTOR inhibitor, informing the dosing and toxicity profile of this combination for future clinical studies. STATEMENT OF SIGNIFICANCE25% patients with the incurable brainstem tumour DIPG harbour somatic activating mutations in ACVR1, however there are no approved drugs targeting the receptor. Using Artificial Intelligence, we identify and validate the novel combination of vandetanib and everolimus in these children based upon both signalling and pharmacokinetic synergies, experimentally and clinically.Research.

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“…Growth factor signaling inhibitors: Growth factor signaling inhibitors have typically been explored in combination with additional treatments given concerns regarding the subclonal nature of relevant mutations as well as redundancy in the downstream signaling networks. PDGFRA signaling inhibition with dasatinib prolonged survival in an IUE-based H3.3K27M pHGG model, and combination with the mTOR inhibitor everolimus demonstrated synergy [ 33 ].…”

Section: Development Of Novel Therapiesmentioning

confidence: 99%

Histone-Mutant Glioma: Molecular Mechanisms, Preclinical Models, and Implications for Therapy

Graham

Mellinghoff

2020

IJMS

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Pediatric high-grade glioma (pHGG) is the leading cause of cancer death in children. Despite histologic similarities, it has recently become apparent that this disease is molecularly distinct from its adult counterpart. Specific hallmark oncogenic histone mutations within pediatric malignant gliomas divide these tumors into subgroups with different neuroanatomic and chronologic predilections. In this review, we will summarize the characteristic molecular alterations of pediatric high-grade gliomas, with a focus on how preclinical models of these alterations have furthered our understanding of their oncogenicity as well as their potential impact on developing targeted therapies for this devastating disease.

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Everolimus improves the efficacy of dasatinib in PDGFRα-driven glioma

Cited by 8 publications

References 38 publications

Therapeutic targeting of differentiation state-dependent metabolic vulnerabilities in DIPG

Therapeutic targeting of differentiation state-dependent metabolic vulnerabilities in DIPG

Repurposing Vandetanib plus Everolimus for the Treatment ofACVR1-Mutant Diffuse Intrinsic Pontine Glioma

Histone-Mutant Glioma: Molecular Mechanisms, Preclinical Models, and Implications for Therapy

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