Src family kinases differentially influence glioma growth and motility

Lewis‐Tuffin, Laura J.; Feathers, Ryan W.; Hari, Priya; Durand, Nisha; Li, Zhimin; Rodríguez, Fausto J.; Bakken, Katie; Carlson, Brett L.; Schroeder, Mark A.; Sarkaria, Jann N.; Anastasiadis, Panos Z.

doi:10.1016/j.molonc.2015.06.001

Cited by 51 publications

(53 citation statements)

References 49 publications

(71 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…36 The lack of a clinical benefit was considered to be a potential result of the different molecular profiles of dasatinib targets between archival tumor resected at the time of the diagnosis of GBM and the profile at disease recurrence; it also was noted that response to dasatinib in patients with GBM may require driver mutations in dasatinib targets. 37 Consistent with this, higher levels of LYN expression were correlated with both a PFS6 and OS advantage in the current study, regardless of treatment. The results indicate that individual SFKs (Src, Fyn, YES, and LYN) differ significantly with regard to their importance for glioma growth and motility, and the efficacy of dasatinib therapy may depend on the relative expression of particular SFKs.…”

Section: Discussionsupporting

confidence: 88%

“…35 Recent clinical research investigating dasatinib monotherapy in patients with recurrent GBM reported a PFS6 of only 6%, despite efforts to enrich the patient population and to increase the dose of dasatinib, however. 37 It is interesting to note that depletion of LYN resulted in increased tumor growth and reduced OS in these orthotopic, patientderived GBM xenografts, suggesting a tumor suppressor function for LYN in GBM. The strategy of targeting SFK signaling has been studied recently in culture and orthotopic xenograft models.…”

Section: Discussionmentioning

confidence: 91%

“…The results indicate that individual SFKs (Src, Fyn, YES, and LYN) differ significantly with regard to their importance for glioma growth and motility, and the efficacy of dasatinib therapy may depend on the relative expression of particular SFKs. 37 It is interesting to note that depletion of LYN resulted in increased tumor growth and reduced OS in these orthotopic, patientderived GBM xenografts, suggesting a tumor suppressor function for LYN in GBM. 37 Consistent with this, higher levels of LYN expression were correlated with both a PFS6 and OS advantage in the current study, regardless of treatment.…”

Section: Discussionmentioning

confidence: 91%

“…37 It is interesting to note that depletion of LYN resulted in increased tumor growth and reduced OS in these orthotopic, patientderived GBM xenografts, suggesting a tumor suppressor function for LYN in GBM. 37 Consistent with this, higher levels of LYN expression were correlated with both a PFS6 and OS advantage in the current study, regardless of treatment. Conversely, a high level of pSRC correlated with a PFS6 disadvantage, regardless of treatment, suggesting that the increased activation of SFKs contributes to the aggressive nature of GBM.…”

Section: Discussionmentioning

confidence: 91%

See 3 more Smart Citations

A phase 1 and randomized, placebo‐controlled phase 2 trial of bevacizumab plus dasatinib in patients with recurrent glioblastoma: Alliance/North Central Cancer Treatment Group N0872

Galanis

Anderson

Twohy

et al. 2019

Cancer

Self Cite

View full text Add to dashboard Cite

BACKGROUND: Src signaling is markedly upregulated in patients with invasive glioblastoma (GBM) after the administration of bevacizumab. The Src family kinase inhibitor dasatinib has been found to effectively block bevacizumab-induced glioma invasion in preclinical models, which led to the hypothesis that combining bevacizumab with dasatinib could increase bevacizumab efficacy in patients with recurrent GBM. METHODS: After the completion of the phase 1 component, the phase 2 trial (ClinicalTrials.gov identifier NCT00892177) randomized patients with recurrent GBM 2:1 to receive 100 mg of oral dasatinib twice daily (arm A) or placebo (arm B) on days 1 to 14 of each 14-day cycle combined with 10 mg/kg of intravenous bevacizumab on day 1 of each 14-day cycle. The primary endpoint was 6-month progression-free survival (PFS6). RESULTS: In the 121 evaluable patients, the PFS6 rate was numerically, but not statistically, higher in arm A versus arm B (28.9% [95% CI, 19.5%-40.0%] vs 18.4% [95% CI, 7.7%-34.4%]; P = .22). Similarly, there was no significant difference in the median overall survival noted between the treatment arms (7.3 months and 7.7 months, respectively; P = .93). The objective response rate was 15.7% in arm A and 26.3% in arm B (P = .52), but with a significantly longer duration in patients treated on arm A (16.3 months vs 2 months). The incidence of grade ≥3 toxicity was comparable between treatment arms, with hematologic toxicities occurring more frequently in arm A versus arm B (15.7% vs 7.9%) (adverse events were assessed as per the National Cancer Institute Common Terminology Criteria for Adverse Events [version 4.0]). Correlative tissue analysis demonstrated an association between pSRC/LYN signaling in patient tumors and outcome. CONCLUSIONS: Despite upregulation of Src signaling in patients with GBM, the combination of bevacizumab with dasatinib did not appear to significantly improve the outcomes of patients with recurrent GBM compared with bevacizumab alone. Cancer 2019;125:3790-3800.We thank the patients who participated in this clinical trial and their families. We also thank the study investigators for their contributions.

show abstract

Section: Discussionsupporting

confidence: 88%

Section: Discussionmentioning

confidence: 91%

Section: Discussionmentioning

confidence: 91%

Section: Discussionmentioning

confidence: 91%

See 2 more Smart Citations

A phase 1 and randomized, placebo‐controlled phase 2 trial of bevacizumab plus dasatinib in patients with recurrent glioblastoma: Alliance/North Central Cancer Treatment Group N0872

Galanis

Anderson

Twohy

et al. 2019

Cancer

Self Cite

View full text Add to dashboard Cite

show abstract

“…Several in-vitro studies showed that FYN knockdown is associated with decreased cell migration and proliferation of glioma cells 3,8,9 . Nevertheless, in vivo human glioma xenograft models of FYN Knockdown in immune-suppressed animals failed to show any difference in survival 8 . Therefore, an immune-competent mouse model that enables the generation of FYN knockdown gliomas amenable for understanding the mechanism of anti-glioma immune response is essential.…”

Section: Introductionmentioning

confidence: 99%

FYN tyrosine kinase, a downstream target of receptor tyrosine kinases, modulates anti-glioma immune responses

Comba

Dunn

Argento

et al. 2019

Preprint

View full text Add to dashboard Cite

BackgroundHigh grade gliomas are aggressive and immunosuppressive brain tumors. Molecular mechanisms that regulate the inhibitory immune tumor microenvironment (TME) and glioma progression remain poorly understood. FYN tyrosine kinase is a downstream target of the oncogenic receptor tyrosine kinases pathway and is overexpressed in human gliomas. FYN’s role in vivo in glioma growth remains unknown. We investigated whether FYN regulates glioma initiation, growth and invasion.MethodsWe evaluated the role of FYN using genetically engineered mouse glioma models (GEMM). We also generated FYN knockdown stem cells to induce gliomas in immune-competent and immune-deficient mice (NSG, CD8−/−, CD4−/−). We analyzed molecular mechanism by RNA-Seq and bioinformatics analysis. Flow cytometry was used to characterize immune cellular infiltrates in the FYN knockdown glioma TME.ResultsWe demonstrate that FYN knockdown in diverse immune-competent GEMMs of glioma reduced tumor progression and significantly increased survival. Gene ontologies (GOs) analysis of differentially expressed genes in wild type vs. FYN knockdown gliomas showed enrichment of GOs related to immune reactivity. However, in NSG, CD8−/− and CD4−/− immune-deficient mice, FYN knockdown gliomas failed to show differences in survival. These data suggest that the expression of FYN in glioma cells reduces anti-glioma immune activation. Examination of glioma immune infiltrates by flow-cytometry displayed reduction in the amount and activity of immune suppressive myeloid derived cells (MDSCs) in the FYN glioma TME.ConclusionsGliomas employ FYN mediated mechanisms to enhance immune-suppression and promote tumor progression. We propose that FYN inhibition within glioma cells could improve the efficacy of anti-glioma immunotherapies.Key pointsInhibition of FYN tyrosine kinase in genetically engineered mouse glioma models delays tumor initiation and progression. The oncogenic effects of FYN in vivo are mediated by downregulation of anti-glioma immunity.Importance of the StudyFYN is an effector of receptor tyrosine kinases (RTK) signaling in glioma. However, its role in vivo remains unknown. Our study demonstrates that FYN tyrosine kinase is a novel regulator of the anti-glioma immune response. We show that FYN inactivation suppresses glioma growth, increases survival, and enhances anti-tumor immune reactivity. Our findings suggest that suppressing the expression of FYN in glioma cells could provide a novel therapeutic target.

show abstract

KX2-361: a novel orally bioavailable small molecule dual Src/tubulin inhibitor that provides long term survival in a murine model of glioblastoma

Ciesielski

Munich

et al. 2018

J Neurooncol

View full text Add to dashboard Cite

Src family kinases differentially influence glioma growth and motility

Cited by 51 publications

References 49 publications

A phase 1 and randomized, placebo‐controlled phase 2 trial of bevacizumab plus dasatinib in patients with recurrent glioblastoma: Alliance/North Central Cancer Treatment Group N0872

A phase 1 and randomized, placebo‐controlled phase 2 trial of bevacizumab plus dasatinib in patients with recurrent glioblastoma: Alliance/North Central Cancer Treatment Group N0872

FYN tyrosine kinase, a downstream target of receptor tyrosine kinases, modulates anti-glioma immune responses

KX2-361: a novel orally bioavailable small molecule dual Src/tubulin inhibitor that provides long term survival in a murine model of glioblastoma

Contact Info

Product

Resources

About