c-Src and EGFR Inhibition in Molecular Cancer Therapy: What Else Can We Improve?

Belli, Stefania; Esposito, Daniela; Servetto, Alberto; Pesapane, Ada; Formisano, Luigi; Bianco, Roberto

doi:10.3390/cancers12061489

Cited by 50 publications

(34 citation statements)

References 106 publications

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“…In line with the findings, PC9/ER cells showed resistance to the corresponding EGFR TKI after a prolonged culture in the absence of drug for more than a month ( Figure S5 ). PC9/ER and PC9 cells were further analyzed for activation status of several RTKs [MET, IGF-1R, and AXL], a nonreceptor tyrosine kinase Src, and IGFBP-3, all of which have been implicated in resistance to EGFR TKIs 49 , 50 . We observed greater activation of IGF-1R, Src, and AXL and weaker expression of IGFBP-3 in PC9/ER than in PC9 cells ( Figure 2 C ).…”

Section: Resultsmentioning

confidence: 99%

Development of the phenylpyrazolo[3,4-d]pyrimidine-based, insulin-like growth factor receptor/Src/AXL-targeting small molecule kinase inhibitor

et al. 2021

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Section: Resultsmentioning

confidence: 99%

Development of the phenylpyrazolo[3,4-d]pyrimidine-based, insulin-like growth factor receptor/Src/AXL-targeting small molecule kinase inhibitor

et al. 2021

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“…There are currently 11 family members discovered, and Src is currently one of the most studied members [23]. Src consists of SH4 domain, speci c fragments, SH3 domain, SH2 domain, linker, SH1 domain (protein tyrosine kinase domain) and carboxy-terminal regulatory tail [24].…”

Section: Discussionmentioning

confidence: 99%

Study on the effects of Polyphyllin I and Curcumin on liver cancer based on the cross-action of ferroptosis and energy metabolism

Gao

Zeng

et al. 2021

Preprint

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Background: To investigate the effect and mechanism of Polyphyllin I(PPI) and Curcumin(Cur) on human liver cancer HepG2 and HepG2.2.15 cells. Methods: Download the hepatocellular carcinoma specimens and normal control specimens from the TCGA database, take the intersection with ferroptosis-related genes, and screen the differentially expressed ferroptosis genes; again, make the intersection with the selected differential genes related to energy metabolism; conduct survival analysis; construct prognosis Risk scoring model and evaluation of model performance; through molecular docking to verify the binding effect of PPI, Cur and Ribonucleoside-diphosphate reductase subunit M2(RRM2), SRC(SRC), Acetyl-CoA carboxylase alpha(ACACA) and other genes. Human hepatocellular carcinoma cells were cultured in vitro, PPI and Cur intervened, and Cell Counting Kit-8(CCK-8) was used to detect cell inhibition rate; FeRhoNox-1 fluorescent probe staining to observe the intracellular Fe 2+ status; lactate dehydrogenase (LDH) release Experiment to detect cell LDH release rate; JC-1 staining to detect mitochondrial membrane potential; reactive oxygen species(ROS) kit to detect ROS level;Western blotting (WB) to detect RRM2 and SRC , ACACA and other genes protein expression levels. Results: Through screening, 25 differential genes related to ferroptosis and energy metabolism in liver cancer were obtained;; through survival analysis, three ferroptosis-related genes, such as RRM2, SRC, and ACACA, were obtained，the results showed that these three genes showed high expression and predicted poor overall survival(OS) and disease-free survival(DFS); molecular docking results showed that PPI, Cur It has good affinity with RRM2, SRC and ACACA. The results of in vitro experiments show that PPI and Cur inhibit cell proliferation in a concentration-dependent manner ( P <0.01). PPI and Cur can significantly increase the intracellular Fe2+ concentration, LDH release rate and intracellular ROS levels of HepG2, HepG2.2.15 ( P <0.01), and the effect on mitochondrial membrane potential was significantly lower than that of the blank group ( P <0.01), and significantly down-regulated the protein expression levels of RRM2, SRC, and ACACA ( P <0.01). Conclusion: The high expression of RRM2, SRC, ACACA and other three genes related to ferroptosis and energy metabolism in liver cancer indicate poor OS and DFS; PPI and Cur can up-regulate the LDH release rate, ROS and Fe 2+ levels of liver cancer cells, and down-regulate the cell mitochondrial membrane potential and other methods to inhibit the proliferation of liver cancer cells; and down-regulate the expression of RRM2, SRC, ACACA and other proteins to affect the prognosis of liver cancer.

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“…While SRC is rarely mutated in cancer, it often functions downstream of oncogenic drivers in signalling cascades including those initiated by receptor tyrosine kinases (RTKs) and at integrin-linked focal adhesions (4). SRC has been a target for drug discovery projects for decades with multiple small molecule ATP-competitive inhibitors being tested in clinical trials (2, 5-11). Dasatinib, a multi-kinase SRC inhibitor, is currently approved for the treatment of chronic myeloid and acute lymphoblastic leukaemias (12).…”

Section: Introductionmentioning

confidence: 99%

Pathway profiling of a novel SRC inhibitor, AZD0424, in combination with MEK inhibitors

Dawson

Munro

Macleod

et al. 2021

Preprint

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A more comprehensive understanding of how cells respond to drug intervention, the likely immediate signalling responses and how resistance may develop within different microenvironments allows us anticipate how cells adapt to targeted therapy enabling more informed prediction of rational drug combinations. The non-receptor tyrosine kinase SRC regulates many cellular signalling processes and pharmacological inhibition has long been a target of drug discovery projects for the treatment of cancer. Here we describe the in vitro and in vivo characterisation of the small molecule SRC inhibitor, AZD0424. We show that AZD0424 potently inhibits the phosphorylation of tyrosine-416 of SRC (IC50 ~ 100 nM) in many cancer cell lines; however inhibition of cell viability, via a G1 cell cycle arrest, was observed only in a sub-set of cancer cell lines in the low (on target) micromolar range. We profiled the changes in intracellular pathway signalling in cancer cells following exposure to AZD0424 and other targeted therapies using Reverse Phase Protein Array analysis. We demonstrate that SRC is activated in response to MEK inhibitor (trametinib or AZD6244)-treatment of KRAS mutant colorectal cell lines (HCT116 and DLD1) and that AZD0424 abrogates this. Cell lines treated with trametinib or AZD6244 in combination with AZD0424 revealed reduction of EGFR, FAK and SRC compensatory activation, and, synergistically inhibits cell viability in vitro. In vivo, trametinib-treatment of mice bearing HCT116 tumours increased phosphorylation of SRC on Tyr416, and when combined with AZD0424, inhibition of tumour growth is greater than trametinib alone. We also demonstrate that drug-induced resistance to trametinib is not re-sensitised by AZD0424 treatment in vitro, likely as a result of multiple compensatory signalling mechanisms; however inhibition of SRC remains an effective way to block invasion of trametinib resistant tumour cells. These data imply that inhibiting SRC may offer a useful addition to MEK inhibitor combination strategies.

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c-Src and EGFR Inhibition in Molecular Cancer Therapy: What Else Can We Improve?

Cited by 50 publications

References 106 publications

Development of the phenylpyrazolo[3,4-d]pyrimidine-based, insulin-like growth factor receptor/Src/AXL-targeting small molecule kinase inhibitor

Development of the phenylpyrazolo[3,4-d]pyrimidine-based, insulin-like growth factor receptor/Src/AXL-targeting small molecule kinase inhibitor

Study on the effects of Polyphyllin I and Curcumin on liver cancer based on the cross-action of ferroptosis and energy metabolism

Pathway profiling of a novel SRC inhibitor, AZD0424, in combination with MEK inhibitors

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