A Comparative Quantitative LC-MS/MS Profiling Analysis of Human Pancreatic Adenocarcinoma, Adjacent-Normal Tissue, and Patient-Derived Tumour Xenografts

Coleman, Orla; Henry, Michael; O’Neill, Fiona; Roche, Sandra; Swan, Niall; Boyle, Lorraine; Murphy, J. J.; Meiller, Justine; Conlon, Neil T.; Geoghegan, Justin; Conlon, Kevin C.; Lynch, Vincent J.; Straubinger, Ninfa L.; Straubinger, Robert M.; McVey, G.; Moriarty, M.; Clynes, Martin

doi:10.3390/proteomes6040045

Cited by 22 publications

(23 citation statements)

References 38 publications

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“…In comparison, between F1 and F2 generation of PDX tumour, only eight human-specific proteins were differentially expressed when analysed by quantitative label-free differential analysis. This demonstrates the fidelity of tumour phenotype once engrafted [30]. This is in line with previously published data the shows, once established, xenografts tend to be robust with stable gene expression profile between early and late passage PDX tumours [31].…”

Section: Discussionsupporting

confidence: 89%

Establishment and Characterisation by Expression Microarray of Patient-Derived Xenograft Panel of Human Pancreatic Adenocarcinoma Patients

Roche

O’Neill

Murphy

et al. 2020

IJMS

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Pancreatic cancer remains among the most lethal cancers worldwide, with poor early detection rates and poor survival rates. Patient-derived xenograft (PDX) models have increasingly been used in preclinical and clinical research of solid cancers to fulfil unmet need. Fresh tumour samples from human pancreatic adenocarcinoma patients were implanted in severe combined immunodeficiency (SCID) mice. Samples from 78% of treatment-naïve pancreatic ductal adenocarcinoma patients grew as PDX tumours and were confirmed by histopathology. Frozen samples from F1 PDX tumours could be later successfully passaged in SCID mice to F2 PDX tumours. The human origin of the PDX was confirmed using human-specific antibodies; however, the stromal component was replaced by murine cells. Cell lines were successfully developed from three PDX tumours. RNA was extracted from eight PDX tumours and where possible, corresponding primary tumour (T) and adjacent normal tissues (N). mRNA profiles of tumour vs. F1 PDX and normal vs. tumour were compared by Affymetrix microarray analysis. Differential gene expression showed over 5000 genes changed across the N vs. T and T vs. PDX samples. Gene ontology analysis of a subset of genes demonstrated genes upregulated in normal vs. tumour vs. PDX were linked with cell cycle, cycles cell process and mitotic cell cycle. Amongst the mRNA candidates elevated in the PDX and tumour vs. normal were SERPINB5, FERMT1, AGR2, SLC6A14 and TOP2A. These genes have been associated with growth, proliferation, invasion and metastasis in pancreatic cancer previously. Cumulatively, this demonstrates the applicability of PDX models and transcriptomic array to identify genes associated with growth and proliferation of pancreatic cancer.

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Section: Discussionsupporting

confidence: 89%

Establishment and Characterisation by Expression Microarray of Patient-Derived Xenograft Panel of Human Pancreatic Adenocarcinoma Patients

Roche

O’Neill

Murphy

et al. 2020

IJMS

Self Cite

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“…provides a comprehensive view of the proteomic inconsistency between PDX models and parental tumors. In our study, the researchers used liquid chromatography–tandem mass spectrometry (LC–MS/MS) technology to profile the proteome and identified human‐specific and species‐indistinguishable proteins . In contrast to matched PDAC parental tumors, a total of 143 (32 upregulated and 111 downregulated) human‐specific proteins were differentially expressed in Passage 1 xenograft tumors.…”

Section: Differences In Molecular Characteristics Among Pdx Modelsmentioning

confidence: 99%

“…Particular proteins and pathways in PDX models show a poor correlation with the corresponding tumors (Table ), such as erb‐b2 receptor tyrosine kinase 2 (HER2), EGFR and P53 in two pancreatic carcinoma PDX models and mechanistic target of rapamycin kinase (mTOR) pathway activation and elevated ribosomal protein S6 (pS235 or pS240) levels in estrogen receptor‐positive breast cancer PDX models. In addition, the subcellular localization of various proteins is markedly different in xenograft tumors than in parental tumors.…”

Section: Differences In Molecular Characteristics Among Pdx Modelsmentioning

confidence: 99%

“…profiled the proteomes of xenograft tumors over two passages by using an LC–MS/MS approach. A subsequent comparison of 10 Passage 2 xenograft tumors with their corresponding Passage 1 tumors yielded a list of differentially expressed proteins, including 8 human‐specific and 41 species‐indistinguishable proteins …”

Section: Differences In Molecular Characteristics Among Pdx Modelsmentioning

confidence: 99%

“…Serially transplanted PDX tumors are more aggressive than parental tumors at the molecular level and are more similar to metastatic or recurrent tumors. In a proteomics study, the lower average coefficient of variance for differentially expressed proteins suggested the orthogenesis of xenograft tumors . Gene ontology (GO) analysis revealed that cell division and catabolic process gene sets are upregulated in PDX tumors; conversely, ECM organization, immune response and angiogenesis gene sets are downregulated .…”

Section: Intratumoral Heterogeneity (Ith)‐derived Mechanismmentioning

confidence: 99%

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The fidelity of cancer cells in PDX models: Characteristics, mechanism and clinical significance

Shi

Jia

et al. 2019

Intl Journal of Cancer

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Patient‐derived xenograft (PDX) models are widely used as preclinical cancer models and are considered better than cell culture models in recapitulating the histological features, molecular characteristics and intratumoral heterogeneity (ITH) of human tumors. While the PDX model is commonly accepted for use in drug discovery and other translational studies, a growing body of evidence has suggested its limitations. Recently, the fidelity of cancer cells within a PDX has been questioned, which may impede the future application of these models. In this review, we will focus the variable phenotypes of xenograft tumors and the genomic instability and molecular inconsistency of PDX tumors after serial transplantation. Next, we will discuss the underlying mechanism of ITH and its clinical relevance. Stochastic selection bias in the sampling process and/or deterministic clonal dynamics due to murine selective pressure may have detrimental effects on the results of personalized medicine and drug screening studies. In addition, we aim to identify a possible solution for the issue of fidelity in current PDX models and to discuss emerging next‐generation preclinical models.

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Neoadjuvant chemotherapy is associated with an altered metabolic profile and increased cancer stemness in patients with pancreatic ductal adenocarcinoma

et al. 2022

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The modest clinical benefits of neoadjuvant chemotherapy (NAT) in pancreatic ductal adenocarcinoma (PDAC) are associated with a lack of robust data on treatment‐induced changes in the tumor. To this end, comparative proteomic profiling of tumor tissue samples from treatment‐naïve (TN, n = 20) and NAT‐treated (n = 22) PDACs was performed. Differentially expressed proteins were identified and correlation with overall survival (OS) was performed. Tumors were also examined for histopathological changes and expression of cancer stem cell (CSC) markers. Serum from 33 matched patients was analyzed for metabolic markers. Cytotoxicity, proliferation, and expression of CSC markers were assessed in chemoresistant Panc‐1 and Mia PaCa‐2 cells. Of the 2265 proteins identified, 227 and 144 proteins showed significantly altered expression and differential phosphorylation, respectively, in NAT compared with TN samples. The majority of these were metabolism‐related proteins, and 14 of these correlated moderately with OS. NAT‐treated tumors and chemoresistant cancer cells showed increased expression of CSC markers. Serum ALDH1A1 was higher in NAT compared with TN. Differentially phosphorylated proteins were mainly involved in cytoskeleton organization, cell locomotion, motility, and migration, and 17 of these showed a strong positive correlation with OS. This study provides evidence of the effects of NAT on PDAC metabolism at both the tumor and the systemic levels. NAT‐treated tumors showed significantly lower expression of metabolic proteins, and patients who underwent NAT showed reduced serum lactate and high‐density lipoprotein‐cholesterol. Lastly, cancer cells that survived cytotoxic treatment expressed higher CSC markers, both in vivo and in vitro.

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A Comparative Quantitative LC-MS/MS Profiling Analysis of Human Pancreatic Adenocarcinoma, Adjacent-Normal Tissue, and Patient-Derived Tumour Xenografts

Cited by 22 publications

References 38 publications

Establishment and Characterisation by Expression Microarray of Patient-Derived Xenograft Panel of Human Pancreatic Adenocarcinoma Patients

Establishment and Characterisation by Expression Microarray of Patient-Derived Xenograft Panel of Human Pancreatic Adenocarcinoma Patients

The fidelity of cancer cells in PDX models: Characteristics, mechanism and clinical significance

Neoadjuvant chemotherapy is associated with an altered metabolic profile and increased cancer stemness in patients with pancreatic ductal adenocarcinoma

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