An Ex Vivo Human Tumor Assay Shows Distinct Patterns of EGFR Trafficking in Squamous Cell Carcinoma Correlating to Therapeutic Outcomes

Joseph, Shannon R.; Gaffney, Daniel C; Barry, Rachael; Hu, Lingbo; Banushi, Blerida; Wells, James W.; Lambie, Duncan; Strutton, Geoffrey; Porceddu, Sandro; Burmeister, Bryan; Leggatt, Graham R.; Schaider, Helmut; Dolcetti, Riccardo; Frazer, Ian H.; Saunders, Nicholas A.; Foote, Matthew; Soyer, H. Peter; Simpson, Fiona

doi:10.1016/j.jid.2018.06.190

Cited by 21 publications

(22 citation statements)

References 38 publications

(50 reference statements)

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“…This also eliminates the need for early animal sacrifice to assess outcomes, although the advantage of histopathological analysis remains accessible at the end of the experiment. although recent data has illustrated that receptor trafficking and polarisation can influence the metastatic potential (189,224). In combination with previous findings from our laboratory, our data supports EGFR as a driver of PNS in cSCCHN rather than the process of perineural invasion and spread engendering EGFR overexpression (66).…”

Section: Optimisation Of An In Vivo Model To Study Pnssupporting

confidence: 89%

“…Currently, EGFR is not regarded as a prognostic indicator or biomarker in cSCC, and cSCCHN with or without PNI. Whilst associated with metastatic disease, in fully formed tumours there is no clinical correlation of EGFR with tumour growth or patient outcome, although recent data has illustrated that receptor trafficking and polarisation can influence the metastatic potential (189,224). However, in combination with previous findings from our laboratory, our data supports EGFR as a driver of PNS in cSCCHN rather than the process of perineural invasion and spread engendering EGFR overexpression (66).…”

Section: Cscchn Overexpress Egfr Highlighting Its Potential Role In Psupporting

confidence: 46%

“…The EGFR expression in the metastases were diffusely and strongly positive compared to weakly positive in the primary tumours with genomic hybridization leading to the hypothesis that EGFR is required to confer metastatic potential (204). Our own observations in actinic keratoses, Bowen's disease and cSCC highlight that EGFR can become polarised to the leading edge of the basal layer of tumours (189). Given that cellular cytokinetic response to EGFR signalling can lead to migration and metastasis, the potential for invasion in polarised cells is high and it will be of interest analysing the potential of an actinic keratosis with high polarisation to develop into an SCC.…”

Section: Cscchn Overexpress Egfr Highlighting Its Potential Role In Pmentioning

confidence: 71%

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Investigating therapeutic possibilities for treatment of perineural invasion

Huang¹

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Perineural invasion (PNI) is a pathological diagnosis whereby tumour cells infiltrate the perineural space of a peripheral nerve. This can lead to perineural spread (PNS) with dissemination of tumour cells away from the original tumour mass eventuating in a sensory or motor deficit. PNI is an accepted risk factor for poorer prognosis in cutaneous squamous cell carcinoma of the head and neck (cSCCHN) with increased locoregional recurrence, more aggressive disease and metastasis. Not exclusive to cutaneous malignancies, it also portends poorer prognosis in colorectal, cervical, gastric and prostate cancers. Despite its prognostic ramifications, PNI and PNS are poorly understood forms of I acknowledge that an electronic copy of my thesis must be lodged with the University Library and, subject to the policy and procedures of The University of Queensland, the thesis be made available for research and study in accordance with the Copyright Act 1968 unless a period of embargo has been approved by the Dean of the Graduate School.

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Section: Optimisation Of An In Vivo Model To Study Pnssupporting

confidence: 89%

Section: Cscchn Overexpress Egfr Highlighting Its Potential Role In Psupporting

confidence: 46%

Section: Cscchn Overexpress Egfr Highlighting Its Potential Role In Pmentioning

confidence: 71%

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Investigating therapeutic possibilities for treatment of perineural invasion

Huang¹

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“…EGFR is a member of the ErbB receptor family. Studies have shown that EGFR overexpression may be associated with tumor cell proliferation, invasion, metastasis, apoptosis, and angiogenesis in a variety of solid tumors and that EGFR mutations contribute to the malignant transformation of epithelial cells [30]. In this study, EGFR protein expression was significantly inhibited as Bim protein expression increased, which may be the mechanism by which MT1JP inhibits the invasion and migration of A549 cells.…”

Section: Discussionmentioning

confidence: 53%

Long-Chain Non-Coding RNA (lncRNA) MT1JP Suppresses Biological Activities of Lung Cancer by Regulating miRNA-423-3p/Bim Axis

Yan

Zhang

et al. 2019

Med Sci Monit

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Background This study aimed to explain the effects and mechanism of MT1JP in lung cancer development and treatment. Material/Methods Thirty non-small cell lung cancer (NSCLC) (stages I–II, 17 cases; stages III–IV, 13 cases) and adjacent normal tissues were obtained. MT1JP and miRNA-423-3p levels were assessed by in situ hybridization and Bim protein expression by immunohistochemistry, and the correlations determined were analyzed. Cell proliferation was determined using MTT and colony formation assay, and cell apoptosis was measured using flow cytometry. A549 cell invasion and migration were assessed by Transwell migration and scratch wound healing assays. Relative mRNA and protein expressions were assessed using real-time polymerase chain reaction and western blotting. Correlations between miRNA-423-3p and Bim protein were investigated using luciferase activity assay, and Bim protein expression was evaluated using western blotting. Results MT1JP, miRNA-423-3p, and Bim expressions in NSCLC cancer tissues and those in adjacent cancer tissues were significantly different ( P <0.01 or P <0.001) with increasing stage. Compared with those in the normal control (NC) group, cell proliferation rates were significantly suppressed ( P <0.01 or P <0.001) and cell apoptosis rates significantly increased ( P <0.01 or P <0.001) in the miRNA inhibitor and lncRNA+miRNA inhibitor groups. Invasion cell numbers and wound healing rates were also significantly inhibited in the miRNA inhibitor and lncRNA+miRNA inhibitor groups ( P <0.01 or P <0.001) compared with those in the NC group. Conclusions The lncRNA MT1JP suppresses NSCLC biological activities by regulating the miRNA-423-3p/Bim axis.

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“…Based on these assumptions, endocytosis inhibitors can be used to move tumor cell antigens targeted by therapeutic monoclonal antibodies to the cell surface, in order to improve the ADCC and clinical responses to these agents. An ex vivo human tumor assay has shown distinct patterns of EGFR trafficking in SCC, correlating with therapeutic outcomes [ 21 ]. The study shows that tumors can be classified into those where EGF was, or was not, able to be endocytosed.…”

Section: Anti-pd-1 and Anti-pd-l1 Antibodies And Endocytosismentioning

confidence: 99%

Non-Small-Cell Lung Cancer Signaling Pathways, Metabolism, and PD-1/PD-L1 Antibodies

Santarpía

Aguilar

Chaib

et al. 2020

Cancers

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Treatment of advanced (metastatic) non-small-cell lung cancer (NSCLC) is currently mainly based on immunotherapy with antibodies against PD-1 or PD-L1, alone, or in combination with chemotherapy. In locally advanced NSCLC and in early resected stages, immunotherapy is also employed. Tumor PD-L1 expression by immunohistochemistry is considered the standard practice. Response rate is low, with median progression free survival very short in the vast majority of studies reported. Herein, numerous biological facets of NSCLC are described involving driver genetic lesions, mutations ad fusions, PD-L1 glycosylation, ferroptosis and metabolic rewiring in NSCLC and lung adenocarcinoma (LUAD). Novel concepts, such as immune-transmitters and the effect of neurotransmitters in immune evasion and tumor growth, the nascent relevance of necroptosis and pyroptosis, possible new biomarkers, such as gasdermin D and gasdermin E, the conundrum of K-Ras mutations in LUADs, with the growing recognition of liver kinase B1 (LKB1) and metabolic pathways, including others, are also commented. The review serves to charter diverse treatment solutions, depending on the main altered signaling pathways, in order to have effectual immunotherapy. Tumor PDCD1 gene (encoding PD-1) has been recently described, in equilibrium with tumor PD-L1 (encoded by PDCD1LG1). Such description explains tumor hyper-progression, which has been reported in several studies, and poises the fundamental criterion that IHC PD-L1 expression as a biomarker should be revisited.

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An Ex Vivo Human Tumor Assay Shows Distinct Patterns of EGFR Trafficking in Squamous Cell Carcinoma Correlating to Therapeutic Outcomes

Cited by 21 publications

References 38 publications

Investigating therapeutic possibilities for treatment of perineural invasion

Investigating therapeutic possibilities for treatment of perineural invasion

Long-Chain Non-Coding RNA (lncRNA) MT1JP Suppresses Biological Activities of Lung Cancer by Regulating miRNA-423-3p/Bim Axis

Non-Small-Cell Lung Cancer Signaling Pathways, Metabolism, and PD-1/PD-L1 Antibodies

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