Your search keyword '"Anaka, M"' showing total 42 results

1. Managing 5FU Cardiotoxicity in Colorectal Cancer Treatment

Author

Anaka M and Abdel-Rahman O

Subjects

fluoropyrimidine, chemotherapy, adverse events, capecitabine, fluorouracil., Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Matthew Anaka, Omar Abdel-Rahman Department of Oncology, Cross Cancer Institute, University of Alberta, Edmonton, AB, CanadaCorrespondence: Omar Abdel-RahmanDepartment of Oncology, Cross Cancer Institute, University of Alberta, 11560 University Avenue, Edmonton, AB, T6G 1Z2, Canada, Tel +1 780-432-8290, Fax +1 780-432-8888, Email Omar.abdelsalam@ahs.caAbstract: Fluorouracil (5FU) is the backbone chemotherapy agent in the treatment of colorectal cancer (CRC). Cardiotoxicity represents an uncommon but serious side effect of treatment with 5FU. Here, we review the current literature on 5FU-cardiotoxicity in the setting of CRC specifically, with a focus on data from the modern era of combination chemotherapy. Despite decades of study, there is little consensus on risk factors and biomarkers for 5FU-cardiotoxicity, nor how patients with CRC should be managed following a cardiotoxicity event. Given the elevated risk of recurrent cardiotoxicity on rechallenge, the use of alternative regimens that do not contain 5FU is a critical aspect of management. Data on the cardiotoxicity risk and efficacy of non-5FU regimens in CRC are therefore reviewed in detail.Keywords: fluoropyrimidine, chemotherapy, adverse events, capecitabine, fluorouracil

Published

2022

2. Canonical WNT signalling determines lineage specificity in Wilms tumour

Author

Fukuzawa, R, Anaka, M R, Weeks, R J, Morison, I M, and Reeve, A E

Published

2009

3. Aberrant pregnancy-associated plasma protein-A expression in breast cancers prognosticates clinical outcomes

Author

Prithviraj, P, Anaka, M, Thompson, EW, Sharma, R, Walkiewicz, M, Tutuka, CSA, Behren, A, Kannourakis, G, Jayachandran, A, Prithviraj, P, Anaka, M, Thompson, EW, Sharma, R, Walkiewicz, M, Tutuka, CSA, Behren, A, Kannourakis, G, and Jayachandran, A

Abstract

Elevated levels of pregnancy-associated plasma protein-A (PAPP-A) have been implicated in the pathogenesis of various malignancies, including breast cancers. Breast cancer is one of the most frequent carcinomas and is the second most common cancer type detected in women of child-bearing age. Throughout pregnancy PAPP-A is produced and secreted by the placental syncytiotrophoblast cells; co-incidentally pregnancy-associated breast cancers often have an aggressive clinical course. The components of the PAPP-A/IGF axis was assessed in a panel of breast cancer cell lines. Using neutralising antibodies the impact of PAPP-A/IGF axis on cell motility was evaluated. PAPP-A was expressed in four of the twelve breast cancer cell lines tested. Blocking PAPP-A and IGFBP4 with neutralising antibodies significantly decreased motiliy of MDA-MB-231 cells. Upregulation of PAPP-A expression in breast tumours resulted in a trend towards worse overall survival. Notably, PAPP-A expression also positively correlated with epithelial-to-mesenchymal transition markers. In conclusion, these results indicate that PAPP-A plays an important role in breast cancer progression and it may be a promising therapeutic target in breast cancer.

Published

2020

4. P09.04 Changing Survival and Treatment Patterns in Patients with Stage IV Non-Small Cell Lung Cancer (NSCLC) in Alberta, Canada

Author

Anaka, M., primary, Gibson, A., additional, Dean, M., additional, Elegbede, A., additional, Petersen, L., additional, Tudor, R., additional, Sangha, R., additional, and Bebb, D.G., additional

Published

2021

5. FP02.03 Changing Survival and Treatment Patterns in Patients Aged 80 or Older with Stage IV Non-Small Cell Lung Cancer (NSCLC)

Author

Anaka, M., primary, Gibson, A., additional, Dean, M., additional, Elegbede, A., additional, Petersen, L., additional, Tudor, R., additional, Sangha, R., additional, and Bebb, D.G., additional

Published

2021

6. Slow-Cycling Melanoma Cells are Resistant to Therapy and Exhibit a Targetable EMT-Related Expression Profile: FC-039

Author

Behren, A., Anaka, M., Hudson, C., McKeown, S., Jayachandran, A., and Cebon, J.

Published

2013

7. Characterizing the effects of FOXP3 on melanoma cell function

Author

Tan, B. S., Anaka, M., Deb, S., Behren, A., Cebon, J., Mariadason, J., and Chen, W.

Published

2012

8. Heterogeneity and plasticity in melanoma leads to treatment failure and increased invasiveness that can be blocked by targeting TSP-1 and/or SNAIL

Author

Behren, A., Jayachandran, A., Anaka, M., Hudson, C., McKeown, S., and Cebon, J.

Published

2012

9. Wilms tumour histology is determined by distinct types of precursor lesions and not epigenetic changes#π

Author

Fukuzawa, R, Anaka, M R, Heathcott, R W, McNoe, L A, Morison, I M, Perlman, E J, and Reeve, A E

Published

2008

10. Consensus-Derived Quality Performance Indicators for Neuroendocrine Tumour Care

Author

Woodhouse, B, Pattison, S, Segelov, E, Singh, S, Parker, K, Kong, G, Macdonald, W, Wyld, D, Meyer-Rochow, G, Pavlakis, N, Conroy, S, Gordon, V, Koea, J, Kramer, N, Michael, M, Wakelin, K, Asif, T, Lo, D, Price, T, Lawrence, B, Anaka, M, Asmis, T, Asselah, J, Boekhoud, J, Card, C, Carroll, R, Cehic, G, Chaudhury, P, Corsini, N, Elston, M, Goodwin, R, Gould, A, Gray, D, Hayes, A, Kevat, D, Laidley, D, Law, C, Leyden, S, Love, A, Mandarino, E, Marginean, C, Modahl, L, Mumford, J, Myrehaug, S, O'Callaghan, C, Patel, D, Ransom, D, Roach, P, Strickland, A, Thawer, A, Vickers, M, Wieler, M, Xu, B, Yelamanchili, R, Woodhouse, B, Pattison, S, Segelov, E, Singh, S, Parker, K, Kong, G, Macdonald, W, Wyld, D, Meyer-Rochow, G, Pavlakis, N, Conroy, S, Gordon, V, Koea, J, Kramer, N, Michael, M, Wakelin, K, Asif, T, Lo, D, Price, T, Lawrence, B, Anaka, M, Asmis, T, Asselah, J, Boekhoud, J, Card, C, Carroll, R, Cehic, G, Chaudhury, P, Corsini, N, Elston, M, Goodwin, R, Gould, A, Gray, D, Hayes, A, Kevat, D, Laidley, D, Law, C, Leyden, S, Love, A, Mandarino, E, Marginean, C, Modahl, L, Mumford, J, Myrehaug, S, O'Callaghan, C, Patel, D, Ransom, D, Roach, P, Strickland, A, Thawer, A, Vickers, M, Wieler, M, Xu, B, and Yelamanchili, R

Abstract

Quality performance indicators (QPIs) are used to monitor the delivery of cancer care. Neuroendocrine tumours (NETs) are a family of individually uncommon cancers that derive from neuroendocrine cells or their precursors, and can occur in most organs. There are currently no QPIs available for NETs and their heterogeneity makes QPI development difficult. CommNETs is a collaboration between NET clinicians, researchers and advocates in Canada, Australia and New Zealand. We created QPIs for NETs using a three-step consensus process. First, a multidisciplinary team used the nominal group technique to create candidates (n = 133) which were then curated into appropriateness statements (62 statements, 44 sub-statements). A two-stage modified RAND/UCLA Delphi consensus process was conducted: an online survey rated the statement appropriateness then the top-ranked statements (n = 20) were assessed in a face-to-face meeting. Finally, 10 QPIs met consensus criteria; documentation of primary site, proliferative index, differentiation, tumour board review, use of a structured pathology report, presence of distant metastasis, 5- and 10-year disease-free and overall survival. These NET QPIs will be trialed as a method to monitor and improve care for people with NETs and to facilitate international comparison.

Published

2019

11. Identifying and targeting determinants of melanoma cellular invasion

Author

Jayachandran, A, Prithviraj, P, Lo, P-H, Walkiewicz, M, Anaka, M, Woods, BL, Tan, B, Behren, A, Cebon, J, McKeown, SJ, Jayachandran, A, Prithviraj, P, Lo, P-H, Walkiewicz, M, Anaka, M, Woods, BL, Tan, B, Behren, A, Cebon, J, and McKeown, SJ

Abstract

Epithelial-to-mesenchymal transition is a critical process that increases the malignant potential of melanoma by facilitating invasion and dissemination of tumor cells. This study identified genes involved in the regulation of cellular invasion and evaluated whether they can be targeted to inhibit melanoma invasion. We identified Peroxidasin (PXDN), Netrin 4 (NTN4) and GLIS Family Zinc Finger 3 (GLIS3) genes consistently elevated in invasive mesenchymal-like melanoma cells. These genes and proteins were highly expressed in metastatic melanoma tumors, and gene silencing led to reduced melanoma invasion in vitro. Furthermore, migration of PXDN, NTN4 or GLIS3 siRNA transfected melanoma cells was inhibited following transplantation into the embryonic chicken neural tube compared to control siRNA transfected melanoma cells. Our study suggests that PXDN, NTN4 and GLIS3 play a functional role in promoting melanoma cellular invasion, and therapeutic approaches directed toward inhibiting the action of these proteins may reduce the incidence or progression of metastasis in melanoma patients.

Published

2016

12. Iterative sorting reveals CD133+and CD133-melanoma cells as phenotypically distinct populations

Author

Grasso, C, Anaka, M, Hofmann, O, Sompallae, R, Broadley, K, Hide, W, Berridge, MV, Cebon, J, Behren, A, McConnell, MJ, Grasso, C, Anaka, M, Hofmann, O, Sompallae, R, Broadley, K, Hide, W, Berridge, MV, Cebon, J, Behren, A, and McConnell, MJ

Abstract

BACKGROUND: The heterogeneity and tumourigenicity of metastatic melanoma is attributed to a cancer stem cell model, with CD133 considered to be a cancer stem cell marker in melanoma as well as other tumours, but its role has remained controversial. METHODS: We iteratively sorted CD133+ and CD133- cells from 3 metastatic melanoma cell lines, and observed tumourigenicity and phenotypic characteristics over 7 generations of serial xeno-transplantation in NOD/SCID mice. RESULTS: We demonstrate that iterative sorting is required to make highly pure populations of CD133+ and CD133- cells from metastatic melanoma, and that these two populations have distinct characteristics not related to the cancer stem cell phenotype. In vitro, gene set enrichment analysis indicated CD133+ cells were related to a proliferative phenotype, whereas CD133- cells were of an invasive phenotype. However, in vivo, serial transplantation of CD133+ and CD133- tumours over 7 generations showed that both populations were equally able to initiate and propagate tumours. Despite this, both populations remained phenotypically distinct, with CD133- cells only able to express CD133 in vivo and not in vitro. Loss of CD133 from the surface of a CD133+ cell was observed in vitro and in vivo, however CD133- cells derived from CD133+ retained the CD133+ phenotype, even in the presence of signals from the tumour microenvironment. CONCLUSION: We show for the first time the necessity of iterative sorting to isolate pure marker-positive and marker-negative populations for comparative studies, and present evidence that despite CD133+ and CD133- cells being equally tumourigenic, they display distinct phenotypic differences, suggesting CD133 may define a distinct lineage in melanoma.

Published

2016

13. Transketolase-like 1 ectopic expression is associated with DNA hypomethylation and induces the Warburg effect in melanoma cells

Author

Jayachandran, A, Lo, P-H, Chueh, AC, Prithviraj, P, Molania, R, Davalos-Salas, M, Anaka, M, Walkiewicz, M, Cebon, J, Behren, A, Jayachandran, A, Lo, P-H, Chueh, AC, Prithviraj, P, Molania, R, Davalos-Salas, M, Anaka, M, Walkiewicz, M, Cebon, J, and Behren, A

Abstract

BACKGROUND: The metabolism of cancer cells is often reprogrammed by dysregulation of metabolic enzymes. Transketolase-like 1 (TKTL1) is a homodimeric transketolase linking the pentose-phosphate pathway with the glycolytic pathway. It is generally silenced at a transcriptional level in somatic tissues. However, in human cancers its expression is associated with the acquisition of a glycolytic phenotype (the Warburg effect) by cancer cells that contributes to the progression of malignant tumors. In melanoma, defective promoter methylation results in the expression of genes and their products that can affect the tumor cell's phenotype including the modification of immune and functional characteristics. The present study evaluates the role of TKTL1 as a mediator of disease progression in melanoma associated with a defective methylation phenotype. METHODS: The expression of TKTL1 in metastatic melanoma tumors and cell lines was analysed by qRT-PCR and immunohistochemistry. The promoter methylation status of TKTL1 in melanoma cells was evaluated by quantitative methylation specific PCR. Using qRT-PCR, the effect of a DNA demethylating agent 5-aza-2'-deoxycytidine (5aza) on the expression of TKTL1 was examined. Biochemical and molecular analyses such as glucose consumption, lactate production, invasion, proliferation and cell cycle progression together with ectopic expression and siRNA mediated knockdown were used to investigate the role of TKTL1 in melanoma cells. RESULTS: Expression of TKTL1 was highly restricted in normal adult tissues and was overexpressed in a subset of metastatic melanoma tumors and derived cell lines. The TKTL1 promoter was activated by hypomethylation and treatment with 5aza induced TKTL1 expression in melanoma cells. Augmented expression of TKTL1 in melanoma cells was associated with a glycolytic phenotype. Loss and gain of function studies revealed that TKTL1 contributed to enhanced invasion of melanoma cells. CONCLUSIONS: Our data provide eviden

Published

2016

14. Systems analysis identifies miR-29b regulation of invasiveness in melanoma

Author

Andrews, MC, Cursons, J, Hurley, DG, Anaka, M, Cebon, JS, Behren, A, Crampin, EJ, Andrews, MC, Cursons, J, Hurley, DG, Anaka, M, Cebon, JS, Behren, A, and Crampin, EJ

Abstract

BACKGROUND: In many cancers, microRNAs (miRs) contribute to metastatic progression by modulating phenotypic reprogramming processes such as epithelial-mesenchymal plasticity. This can be driven by miRs targeting multiple mRNA transcripts, inducing regulated changes across large sets of genes. The miR-target databases TargetScan and DIANA-microT predict putative relationships by examining sequence complementarity between miRs and mRNAs. However, it remains a challenge to identify which miR-mRNA interactions are active at endogenous expression levels, and of biological consequence. METHODS: We developed a workflow to integrate TargetScan and DIANA-microT predictions into the analysis of data-driven associations calculated from transcript abundance (RNASeq) data, specifically the mutual information and Pearson's correlation metrics. We use this workflow to identify putative relationships of miR-mediated mRNA repression with strong support from both lines of evidence. Applying this approach systematically to a large, published collection of unique melanoma cell lines - the Ludwig Melbourne melanoma (LM-MEL) cell line panel - we identified putative miR-mRNA interactions that may contribute to invasiveness. This guided the selection of interactions of interest for further in vitro validation studies. RESULTS: Several miR-mRNA regulatory relationships supported by TargetScan and DIANA-microT demonstrated differential activity across cell lines of varying matrigel invasiveness. Strong negative statistical associations for these putative regulatory relationships were consistent with target mRNA inhibition by the miR, and suggest that differential activity of such miR-mRNA relationships contribute to differences in melanoma invasiveness. Many of these relationships were reflected across the skin cutaneous melanoma TCGA dataset, indicating that these observations also show graded activity across clinical samples. Several of these miRs are implicated in cancer progression (miR

Published

2016

15. Pregnancy associated plasma protein-A links pregnancy and melanoma progression by promoting cellular migration and invasion

Author

Prithviraj, P, Anaka, M, McKeown, SJ, Permezel, M, Walkiewicz, M, Cebon, J, Behren, A, Jayachandran, A, Prithviraj, P, Anaka, M, McKeown, SJ, Permezel, M, Walkiewicz, M, Cebon, J, Behren, A, and Jayachandran, A

Abstract

Melanoma is the most common cancer diagnosed in pregnant women and an aggressive course with poorer outcomes is commonly described during pregnancy or shortly after childbirth. The underlying mechanisms for this are not understood. Here, we report that melanoma migration, invasiveness and progression are promoted by Pregnancy-Associated Plasma Protein-A (PAPPA), a pregnancy-associated metalloproteinase produced by the placenta that increases the bioavailability of IGF1 by cleaving it from a circulating complex formed with IGFBP4. We show that PAPPA is widely expressed by metastatic melanoma tumors and is elevated in melanoma cells exhibiting mesenchymal, invasive and label-retaining phenotypes. Notably, inhibition of PAPPA significantly reduced invasion and migration of melanoma cells in vitro and in vivo within the embryonic chicken neural tube. PAPPA-enriched pregnancy serum treatment enhanced melanoma motility in vitro. Furthermore, we report that IGF1 can induce the phenotypic and functional effects of epithelial-to-mesenchymal transition (EMT) in melanoma cells. In this study, we establish a clear relationship between a pregnancy-associated protein PAPPA, melanoma and functional effects mediated through IGF1 that provides a plausible mechanism for accelerated melanoma progression during pregnancy. This opens the possibility of targeting the PAPPA/IGF1 axis therapeutically.

Published

2015

16. FOXP3 over-expression inhibits melanoma tumorigenesis via effects on proliferation and apoptosis

Author

Tan, B, Anaka, M, Deb, S, Freyer, C, Ebert, LM, Chueh, AC, Al-Obaidi, S, Behren, A, Jayachandran, A, Cebon, J, Chen, W, Mariadason, JM, Tan, B, Anaka, M, Deb, S, Freyer, C, Ebert, LM, Chueh, AC, Al-Obaidi, S, Behren, A, Jayachandran, A, Cebon, J, Chen, W, and Mariadason, JM

Abstract

The Forkhead box P3 (FOXP3) transcription factor is the key driver of regulatory T cell (Treg cells) differentiation and immunosuppressive function. In addition, FOXP3 has been reported to be expressed in many tumors, including melanoma. However, its role in tumorigenesis is conflicting, with both tumor suppressive and tumor promoting functions described. The aim of the current study was to characterize the expression and function of FOXP3 in melanoma. FOXP3 expression was detected by immunohistochemistry (IHC) in 12% (18/146) of stage III and IV melanomas. However expression was confined to fewer than 1% of cells in these tumors. Stable over-expression of FOXP3 in the SK-MEL-28 melanoma cell line reduced cell proliferation and clonogenicity in vitro, and reduced xenograft growth in vivo. FOXP3 over-expression also increased pigmentation and the rate of apoptosis of SK-MEL-28 cells. Based on its infrequent expression in human melanoma, and its growth inhibitory and pro-apoptotic effect in over-expressing melanoma cells, we conclude that FOXP3 is not likely to be a key tumor suppressor or promoter in melanoma.

Published

2014

17. Thrombospondin 1 promotes an aggressive phenotype through epithelial-to-mesenchymal transition in human melanoma

Author

Jayachandran, A, Anaka, M, Prithviraj, P, Hudson, C, McKeown, SJ, Lo, P-H, Vella, LJ, Goding, CR, Cebon, J, Behren, A, Jayachandran, A, Anaka, M, Prithviraj, P, Hudson, C, McKeown, SJ, Lo, P-H, Vella, LJ, Goding, CR, Cebon, J, and Behren, A

Abstract

Epithelial-to-mesenchymal transition (EMT), in which epithelial cells loose their polarity and become motile mesenchymal cells, is a determinant of melanoma metastasis. We compared gene expression signatures of mesenchymal-like melanoma cells with those of epithelial-like melanoma cells, and identified Thrombospondin 1 (THBS1) as highly up-regulated in the mesenchymal phenotype. This study investigated whether THBS1, a major physiological activator of transforming growth factor (TGF)-beta, is involved in melanoma EMT-like process. We sought to examine expression patterns in distinct melanoma phenotypes including invasive, de-differentiated, label-retaining and drug resistant populations that are putatively associated with an EMT-like process. Here we show that THBS1 expression and secretion was elevated in melanoma cells exhibiting invasive, drug resistant, label retaining and mesenchymal phenotypes and correlated with reduced expression of genes involved in pigmentation. Elevated THBS1 levels were detected in Vemurafenib resistant melanoma cells and inhibition of THBS1 led to significantly reduced chemoresistance in melanoma cells. Notably, siRNA-mediated silencing of THBS1 and neutralizing antibody to THBS1 reduced invasion in mesenchymal-like melanoma cells, while ectopic THBS1 expression in epithelial-like melanoma cells enhanced invasion. Furthermore, the loss of THBS1 inhibited in vivo motility of melanoma cells within the embryonic chicken neural tube. In addition, we found aberrant THBS1 protein expression in metastatic melanoma tumor biopsies. These results implicate a role for THBS1 in EMT, and hence THBS1 may serve as a novel target for strategies aimed at the treatment of melanoma invasion and drug resistance.

Published

2014

18. Intratumoral genetic heterogeneity in metastatic melanoma is accompanied by variation in malignant behaviors

Author

Anaka, M, Hudson, C, Lo, P-H, Do, H, Caballero, OL, Davis, ID, Dobrovic, A, Cebon, J, Behren, A, Anaka, M, Hudson, C, Lo, P-H, Do, H, Caballero, OL, Davis, ID, Dobrovic, A, Cebon, J, and Behren, A

Abstract

BACKGROUND: Intratumoral heterogeneity is a major obstacle for the treatment of cancer, as the presence of even minor populations that are insensitive to therapy can lead to disease relapse. Increased clonal diversity has been correlated with a poor prognosis for cancer patients, and we therefore examined genetic, transcriptional, and functional diversity in metastatic melanoma. METHODS: Amplicon sequencing and SNP microarrays were used to profile somatic mutations and DNA copy number changes in multiple regions from metastatic lesions. Clonal genetic and transcriptional heterogeneity was also assessed in single cell clones from early passage cell lines, which were then subjected to clonogenicity and drug sensitivity assays. RESULTS: MAPK pathway and tumor suppressor mutations were identified in all regions of the melanoma metastases analyzed. In contrast, we identified copy number abnormalities present in only some regions in addition to homogeneously present changes, suggesting ongoing genetic evolution following metastatic spread. Copy number heterogeneity from a tumor was represented in matched cell line clones, which also varied in their clonogenicity and drug sensitivity. Minor clones were identified based on dissimilarity to the parental cell line, and these clones were the most clonogenic and least sensitive to drugs. Finally, treatment of a polyclonal cell line with paclitaxel to enrich for drug-resistant cells resulted in the adoption of a gene expression profile with features of one of the minor clones, supporting the idea that these populations can mediate disease relapse. CONCLUSION: Our results support the hypothesis that minor clones might have major consequences for patient outcomes in melanoma.

Published

2013

19. Systems analysis identifies miR-29b regulation of invasiveness in melanoma

Author

Miles Andrews, Cursons J, Dg, Hurley, Anaka M, Js, Cebon, Behren A, and Ej, Crampin

20. Patient Priorities Concerning Treatment Decisions for Advanced Neuroendocrine Tumors Identified by Discrete Choice Experiments.

Author

Anaka M, Chan D, Pattison S, Thawer A, Franco B, Moody L, Jackson C, Segelov E, and Singh S

Subjects

Humans, Patient Preference, Somatostatin therapeutic use, Randomized Controlled Trials as Topic, Neuroectodermal Tumors, Primitive, Neuroendocrine Tumors pathology

Abstract

Background: Patients with advanced neuroendocrine tumors (NETs) have multiple treatment options. Ideally, treatment decisions are shared between physician and patient; however, previous studies suggest that oncologists and patients place different value on treatment attributes such as adverse event (AE) rates. High-quality information on NET patient treatment preferences may facilitate patient-centered decision making by helping clinicians understand patient priorities., Methods: This study used 2 discrete choice experiments (DCE) to elicit preferences of NET patients regarding advanced midgut and pancreatic NET (pNET) treatments. The DCEs used the "potentially all pairwise rankings of all possible alternatives" (PAPRIKA) method. The primary objective was to determine relative utility rankings for treatment attributes, including progression-free survival (PFS), treatment modality, and AE rates. Ranking of attribute profiles matching specific treatments was also determined. Levels for treatment attributes were obtained from randomized clinical trial data of NET treatments., Results: One hundred and 10 participants completed the midgut NET DCE, and 132 completed the pNET DCE. Longer PFS was the highest ranked treatment attribute in 64.5% of participants in the midgut NET DCE, and in 59% in the pNET DCE. Approximately, 40% of participants in both scenarios prioritized lower AE rates or less invasive treatment modalities over PFS. Ranking of treatment profiles in the midgut NET scenario identified 60.9% of participants favoring peptide receptor radionuclide therapy (PRRT), and 30.0% somatostatin analogue dose escalation., Conclusion: NET patients have heterogeneous priorities when choosing between treatment options based on the results of 2 independent DCEs. These results highlight the importance of shared decision making for NET patients., (© The Author(s) 2023. Published by Oxford University Press.)

Published

2024

21. Changing Rates of Goals of Care Designations in Patients With Advanced Pancreatic Cancer During a Multifactorial Advanced Care Planning Initiative: A Real-World Evidence Study.

Author

Anaka M, Lee M, Lim E, Ghosh S, Cheung WY, and Spratlin J

Subjects

Humans, Patient Care Planning, Retrospective Studies, Pancreatic Neoplasms, Advance Care Planning, Oncologists, Pancreatic Neoplasms epidemiology, Pancreatic Neoplasms therapy

Abstract

Purpose: Goals of care (GoC) designations are an important part of advanced care planning (ACP) for patients with incurable cancers. Studies of outpatient oncology records show that most patients do not have GoC documented. We performed a retrospective analysis of changes in GoC designations in patients with advanced pancreatic cancer in Northern Alberta, Canada, during a system-wide ACP quality improvement initiative., Methods: Four hundred seventy-one patients with newly diagnosis of advanced, non-neuroendocrine pancreatic cancer between 2010 and 2015 in Northern Alberta, Canada, were included. The ACP initiation launched April 2014, and included educational materials for patients and families, and a coded system of GoC designations describing care philosophies and preferences for resuscitation and medical interventions. Data sources included the Alberta Cancer Registry and oncology-specific electronic medical records., Results: 25.5% of patients had a documented GoC, which increased over the study period (Mantel-Haenszel test-of-trend P < .001; increased from 7.8% in 2010 to 50.0% in 2015). GoC designations occurred later in patients who received palliative chemotherapy versus those who did not (median 130 days from diagnosis [95% CI, 76.019 to 183.981] v 36 days [95% CI, 28.107 to 43.893]; P < .001), and coincided with the end of treatment (median 4.5 days from last treatment). 64.8% of GoC designations were documented by palliative care physicians, but the proportion documented by medical oncologists increased with time (Mantel-Haenszel test-of-trend P = .020; increased from 0% in 2010 to 52.1% in 2015)., Conclusion: GoC documentation increased in the outpatient records of patients with advanced pancreatic cancer during the system-wide, multifactorial ACP initiative. GoC documentation by medical oncologists also increased. These data provide real-world evidence supporting the impact of a specific ACP initiative to improve rates of GoC designation in patients with advanced cancer., Competing Interests: Matthew AnakaStock and Other Ownership Interests: Gilead Sciences, Madrigal Pharmaceuticals, Xenon Pharma, Viking Therapeutics, Sangamo Therapeutics, Regenxbio Jennifer SpratlinHonoraria: Celgene, Sanofi, Lilly/ImClone, Eisai, Taiho PharmaceuticalConsulting or Advisory Role: Celgene, Sanofi, Lilly/ImClone, Taiho Pharmaceutical, Astellas Pharma, EisaiResearch Funding: Sanofi, Celgene (Inst)Travel, Accommodations, Expenses: Astellas PharmaNo other potential conflicts of interest were reported.

Published

2022

22. Prognostic Role of Immune Checkpoint Regulators in Cholangiocarcinoma: A Pilot Study.

Author

Cao L, Prithviraj P, Shrestha R, Sharma R, Anaka M, Bridle KR, Kannourakis G, Crawford DHG, and Jayachandran A

Abstract

Cholangiocarcinoma (CCA) is a hepatobiliary malignancy associated with steadily increasing incidence and poor prognosis. Ongoing clinical trials are assessing the effectiveness and safety of a few immune checkpoint inhibitors (ICIs) in CCA patients. However, these ICI treatments as monotherapies may be effective for a proportion of patients with CCA. The prevalence and distribution of other immune checkpoints (ICs) in CCA remain unclear. In this pilot study, we screened databases of CCA patients for the expression of 19 ICs and assessed the prognostic significance of these ICs in CCA patients. Notably, expression of immune modulator IDO1 and PD-L1 were linked with poor overall survival, while FASLG and NT5E were related to both worse overall survival and progression-free survival. We also identified immune modulators IDO1, FASLG, CD80, HAVCR2, NT5E, CTLA-4, LGALS9, VTCN1 and TNFRSF14 that synergized with PD-L1 and correlated with worse patient outcomes. In vitro studies revealed that the expression of ICs was closely linked with aggressive CCA subpopulations, such as cancer stem cells and cells undergoing TGF-β and TNF-α-mediated epithelial-to-mesenchymal transition. These findings suggest that the aforementioned IC molecules may serve as potential prognostic biomarkers and drug targets in CCA patients, leading to lasting and durable treatment outcomes.

Published

2021

23. Proposal for 'segmented peer review' of multidisciplinary papers.

Author

Dinakaran D, Anaka M, and Mackey JR

Abstract

We propose a new process for peer review of multidisciplinary journal submissions called 'segmented peer review'. The current translational research environment increasingly requires complex and multidisciplinary studies that span multiple distinct specialties within a single paper. Such papers present logistic and practical barriers to effective peer review. To address these barriers, papers undergoing segmented peer review require authors to explicitly i) identify each of the areas of expertise required to review the paper, ii) direct each reviewer to the relevant portions of the manuscript, and iii) suggest in-field reviewers. This segmentation of the paper is then followed by a 'segmented peer review request' tailored to the expertise of each potential reviewer, with a request to confine his / her review to those 'in-scope' aspects of the paper, while de-emphasizing any optional 'out-of-scope' comments. Each reviewer indicates the fitness for publication, or suitability for revision, of their particular segment of the manuscript. The segmented peer review process is completed when the editors integrate the segmented peer reviews. We propose segmented peer review as a fit-for-purpose process with tangible advantages for authors, reviewers, and journal editors. It should reduce the specific barriers to publication inherent in the evaluation of multidisciplinary research efforts., Competing Interests: Declaration of Competing Interest None, (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

24. Aberrant pregnancy-associated plasma protein-A expression in breast cancers prognosticates clinical outcomes.

Author

Prithviraj P, Anaka M, Thompson EW, Sharma R, Walkiewicz M, Tutuka CSA, Behren A, Kannourakis G, and Jayachandran A

Subjects

Antibodies, Neutralizing immunology, Antibodies, Neutralizing pharmacology, Cell Line, Tumor, Cell Movement, Cell Proliferation, Epithelial-Mesenchymal Transition physiology, Female, Humans, Insulin-Like Growth Factor Binding Protein 4 antagonists & inhibitors, Insulin-Like Growth Factor I metabolism, Neoplasm Invasiveness, Pregnancy, Pregnancy-Associated Plasma Protein-A antagonists & inhibitors, Prognosis, Trophoblasts metabolism, Breast Neoplasms pathology, Disease Progression, Insulin-Like Growth Factor Binding Protein 4 metabolism, Pregnancy-Associated Plasma Protein-A metabolism

Abstract

Elevated levels of pregnancy-associated plasma protein-A (PAPP-A) have been implicated in the pathogenesis of various malignancies, including breast cancers. Breast cancer is one of the most frequent carcinomas and is the second most common cancer type detected in women of child-bearing age. Throughout pregnancy PAPP-A is produced and secreted by the placental syncytiotrophoblast cells; co-incidentally pregnancy-associated breast cancers often have an aggressive clinical course. The components of the PAPP-A/IGF axis was assessed in a panel of breast cancer cell lines. Using neutralising antibodies the impact of PAPP-A/IGF axis on cell motility was evaluated. PAPP-A was expressed in four of the twelve breast cancer cell lines tested. Blocking PAPP-A and IGFBP4 with neutralising antibodies significantly decreased motiliy of MDA-MB-231 cells. Upregulation of PAPP-A expression in breast tumours resulted in a trend towards worse overall survival. Notably, PAPP-A expression also positively correlated with epithelial-to-mesenchymal transition markers. In conclusion, these results indicate that PAPP-A plays an important role in breast cancer progression and it may be a promising therapeutic target in breast cancer.

Published

2020

25. Rearrangement bursts generate canonical gene fusions in bone and soft tissue tumors.

Author

Anderson ND, de Borja R, Young MD, Fuligni F, Rosic A, Roberts ND, Hajjar S, Layeghifard M, Novokmet A, Kowalski PE, Anaka M, Davidson S, Zarrei M, Id Said B, Schreiner LC, Marchand R, Sitter J, Gokgoz N, Brunga L, Graham GT, Fullam A, Pillay N, Toretsky JA, Yoshida A, Shibata T, Metzler M, Somers GR, Scherer SW, Flanagan AM, Campbell PJ, Schiffman JD, Shago M, Alexandrov LB, Wunder JS, Andrulis IL, Malkin D, Behjati S, and Shlien A

Subjects

Adolescent, Bone Neoplasms pathology, Child, DNA Replication, Evolution, Molecular, Female, Genome, Human, Humans, Male, Mutation, Neoplasm Metastasis, Neoplasm Recurrence, Local genetics, Neoplasm Recurrence, Local pathology, Soft Tissue Neoplasms pathology, Bone Neoplasms genetics, Gene Rearrangement, Oncogene Proteins, Fusion genetics, Sarcoma, Ewing genetics, Soft Tissue Neoplasms genetics

Abstract

Sarcomas are cancers of the bone and soft tissue often defined by gene fusions. Ewing sarcoma involves fusions between EWSR1 , a gene encoding an RNA binding protein, and E26 transformation-specific (ETS) transcription factors. We explored how and when EWSR1-ETS fusions arise by studying the whole genomes of Ewing sarcomas. In 52 of 124 (42%) of tumors, the fusion gene arises by a sudden burst of complex, loop-like rearrangements, a process called chromoplexy, rather than by simple reciprocal translocations. These loops always contained the disease-defining fusion at the center, but they disrupted multiple additional genes. The loops occurred preferentially in early replicating and transcriptionally active genomic regions. Similar loops forming canonical fusions were found in three other sarcoma types. Chromoplexy-generated fusions appear to be associated with an aggressive form of Ewing sarcoma. These loops arise early, giving rise to both primary and relapse Ewing sarcoma tumors, which can continue to evolve in parallel., (Copyright © 2018 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2018

26. Monitoring Immune Checkpoint Regulators as Predictive Biomarkers in Hepatocellular Carcinoma.

Author

Shrestha R, Prithviraj P, Anaka M, Bridle KR, Crawford DHG, Dhungel B, Steel JC, and Jayachandran A

Abstract

The global burden of hepatocellular carcinoma (HCC), one of the frequent causes of cancer-related deaths worldwide, is rapidly increasing partly due to the limited treatment options available for this disease and recurrence due to therapy resistance. Immune checkpoint inhibitors that are proved to be beneficial in the treatment of advanced melanoma and other cancer types are currently in clinical trials in HCC. These ongoing trials are testing the efficacy and safety of a few select checkpoints in HCC. Similar to observations in other cancers, these immune checkpoint blockade treatments as monotherapy may benefit only a fraction of HCC patients. Studies that assess the prevalence and distribution of other immune checkpoints/modulatory molecules in HCC have been limited. Moreover, robust predictors to identify which HCC patients will respond to immunotherapy are currently lacking. The objective of this study is to perform a comprehensive evaluation on different immune modulators as predictive biomarkers to monitor HCC patients at high risk for poor prognosis. We screened publically available HCC patient databases for the expression of previously well described immune checkpoint regulators and evaluated the usefulness of these immune modulators to predict high risk, patient overall survival and recurrence. We also identified the immune modulators that synergized with known immune evasion molecules programmed death receptor ligand-1 (PD-L1), programmed cell death protein-1 (PD-1), and cytotoxic T lymphocyte-associated antigen-4 (CTLA-4) and correlated with worse patient outcomes. We evaluated the association between the expression of epithelial-to-mesenchymal transition (EMT) markers and PD-L1 in HCC patient tumors. We also examined the relationship of tumor mutational burden with HCC patient survival. Notably, expression of immune modulators B7-H4, PD-L2, TIM-3 , and VISTA were independently associated with worse prognosis, while B7-H4, CD73 , and VISTA predicted low recurrence-free survival. Moreover, the prognosis of patients expressing high PD-L1 with high B7-H4, TIM-3, VISTA, CD73 , and PD-L2 expression was significantly worse. Interestingly, PD-L1 expression in HCC patients in the high-risk group was closely associated with EMT marker expression and prognosticates poor survival. In HCC patients, high tumor mutational burden (TMB) predicted worse patient outcomes than those with low TMB.

Published

2018

27. Impact of Reflex EGFR/ ALK Testing on Time to Treatment of Patients With Advanced Nonsquamous Non-Small-Cell Lung Cancer.

Author

Cheema PK, Menjak IB, Winterton-Perks Z, Raphael S, Cheng SY, Verma S, Muinuddin A, Freedman R, Toor N, Perera J, Anaka M, and Victor JC

Subjects

Aged, Anaplastic Lymphoma Kinase, Biomarkers, Tumor genetics, Carcinoma, Non-Small-Cell Lung therapy, Female, Humans, Lung Neoplasms therapy, Male, Middle Aged, Molecular Diagnostic Techniques, Precision Medicine methods, Retrospective Studies, Carcinoma, Non-Small-Cell Lung genetics, ErbB Receptors genetics, Lung Neoplasms genetics, Receptor Protein-Tyrosine Kinases genetics, Time-to-Treatment

Abstract

Purpose: Optimal first-line systemic therapy for patients with advanced nonsquamous (nonsq) non-small-cell lung cancer (NSCLC) requires confirmation of EGFR/ ALK status, which can delay treatment. We evaluated the impact of reflex testing, defined as pathologists initiating EGFR/ ALK testing at the time of diagnosis of nonsq NSCLC, on time to treatment (TTT)., Methods: We conducted a retrospective review of patients with nonsq NSCLC with medical oncology consultation at Sunnybrook Odette Cancer Centre between March 18, 2010 and April 30, 2014. Data were compared during routine and reflex testing. TTT was defined as the interval between the first medical oncology visit with advanced NSCLC and the initiation of systemic therapy., Results: A total of 306 patients were included (n = 232 for routine testing, n = 74 for reflex testing). There was a trend to improvement in median TTT with reflex testing (36 days [interquartile range {IQR}, 16 to 71 days v 26 days [IQR, 8 to 41 days], P = .071). Omitting patients with intentional delays in systemic therapy for low-volume disease, poor performance status, comorbidity management, and/or radiation therapy, median TTT improved (34 days [IQR, 15 to 67 days] v 22 days [IQR, 8 to 42 days], P = .049). Time to optimal first-line systemic therapy according to published guidelines improved (median, 36 days [IQR, 16 to 91 days] v 24 days [IQR, 8 to 43 days], P = .036). There was no impact on receipt of any first-line systemic therapy (55% v 59%, P = .66). The quality of biomarker testing improved, with fewer unsuccessful tests ( EGFR, 14% v 4%, P = .039; and ALK, 17% v 3%, P = .037)., Conclusion: Reflex testing of EGFR/ ALK improved the time to optimal systemic therapy and the quality of biomarker testing for patients with advanced nonsq NSCLC.

Published

2017

28. Systems analysis identifies miR-29b regulation of invasiveness in melanoma.

Author

Andrews MC, Cursons J, Hurley DG, Anaka M, Cebon JS, Behren A, and Crampin EJ

Subjects

Algorithms, Cell Line, Tumor, Cell Movement genetics, Computational Biology methods, Disease Progression, Gene Expression Profiling, Humans, Neoplasm Invasiveness, Phenotype, RNA Interference, RNA Processing, Post-Transcriptional, RNA Stability, RNA, Messenger genetics, Transcriptome, Workflow, Gene Expression Regulation, Neoplastic, Melanoma genetics, Melanoma pathology, MicroRNAs genetics

Abstract

Background: In many cancers, microRNAs (miRs) contribute to metastatic progression by modulating phenotypic reprogramming processes such as epithelial-mesenchymal plasticity. This can be driven by miRs targeting multiple mRNA transcripts, inducing regulated changes across large sets of genes. The miR-target databases TargetScan and DIANA-microT predict putative relationships by examining sequence complementarity between miRs and mRNAs. However, it remains a challenge to identify which miR-mRNA interactions are active at endogenous expression levels, and of biological consequence., Methods: We developed a workflow to integrate TargetScan and DIANA-microT predictions into the analysis of data-driven associations calculated from transcript abundance (RNASeq) data, specifically the mutual information and Pearson's correlation metrics. We use this workflow to identify putative relationships of miR-mediated mRNA repression with strong support from both lines of evidence. Applying this approach systematically to a large, published collection of unique melanoma cell lines - the Ludwig Melbourne melanoma (LM-MEL) cell line panel - we identified putative miR-mRNA interactions that may contribute to invasiveness. This guided the selection of interactions of interest for further in vitro validation studies., Results: Several miR-mRNA regulatory relationships supported by TargetScan and DIANA-microT demonstrated differential activity across cell lines of varying matrigel invasiveness. Strong negative statistical associations for these putative regulatory relationships were consistent with target mRNA inhibition by the miR, and suggest that differential activity of such miR-mRNA relationships contribute to differences in melanoma invasiveness. Many of these relationships were reflected across the skin cutaneous melanoma TCGA dataset, indicating that these observations also show graded activity across clinical samples. Several of these miRs are implicated in cancer progression (miR-211, -340, -125b, -221, and -29b). The specific role for miR-29b-3p in melanoma has not been well studied. We experimentally validated the predicted miR-29b-3p regulation of LAMC1 and PPIC and LASP1, and show that dysregulation of miR-29b-3p or these mRNA targets can influence cellular invasiveness in vitro., Conclusions: This analytic strategy provides a comprehensive, systems-level approach to identify miR-mRNA regulation in high-throughput cancer data, identifies novel putative interactions with functional phenotypic relevance, and can be used to direct experimental resources for subsequent experimental validation. Computational scripts are available: http://github.com/uomsystemsbiology/LMMEL-miR-miner.

Published

2016

29. Iterative sorting reveals CD133+ and CD133- melanoma cells as phenotypically distinct populations.

Author

Grasso C, Anaka M, Hofmann O, Sompallae R, Broadley K, Hide W, Berridge MV, Cebon J, Behren A, and McConnell MJ

Subjects

AC133 Antigen metabolism, Animals, Cell Line, Tumor, Cell Lineage, Cell Proliferation, Humans, Melanoma immunology, Mice, Mice, Inbred NOD, Mice, SCID, Neoplasm Metastasis, Neoplasm Transplantation, Neoplastic Stem Cells pathology, Phenotype, Tumor Microenvironment, AC133 Antigen genetics, Cell Separation methods, Melanoma pathology, Neoplastic Stem Cells immunology

Abstract

Background: The heterogeneity and tumourigenicity of metastatic melanoma is attributed to a cancer stem cell model, with CD133 considered to be a cancer stem cell marker in melanoma as well as other tumours, but its role has remained controversial., Methods: We iteratively sorted CD133+ and CD133- cells from 3 metastatic melanoma cell lines, and observed tumourigenicity and phenotypic characteristics over 7 generations of serial xeno-transplantation in NOD/SCID mice., Results: We demonstrate that iterative sorting is required to make highly pure populations of CD133+ and CD133- cells from metastatic melanoma, and that these two populations have distinct characteristics not related to the cancer stem cell phenotype. In vitro, gene set enrichment analysis indicated CD133+ cells were related to a proliferative phenotype, whereas CD133- cells were of an invasive phenotype. However, in vivo, serial transplantation of CD133+ and CD133- tumours over 7 generations showed that both populations were equally able to initiate and propagate tumours. Despite this, both populations remained phenotypically distinct, with CD133- cells only able to express CD133 in vivo and not in vitro. Loss of CD133 from the surface of a CD133+ cell was observed in vitro and in vivo, however CD133- cells derived from CD133+ retained the CD133+ phenotype, even in the presence of signals from the tumour microenvironment., Conclusion: We show for the first time the necessity of iterative sorting to isolate pure marker-positive and marker-negative populations for comparative studies, and present evidence that despite CD133+ and CD133- cells being equally tumourigenic, they display distinct phenotypic differences, suggesting CD133 may define a distinct lineage in melanoma.

Published

2016

30. Identifying and targeting determinants of melanoma cellular invasion.

Author

Jayachandran A, Prithviraj P, Lo PH, Walkiewicz M, Anaka M, Woods BL, Tan B, Behren A, Cebon J, and McKeown SJ

Subjects

Animals, Cell Line, Tumor, Chick Embryo, Gene Expression Regulation, Neoplastic drug effects, Genetic Association Studies, Humans, Molecular Targeted Therapy, Neoplasm Invasiveness, Neoplasm Metastasis, RNA, Small Interfering pharmacology, Transcriptome drug effects, Biomarkers, Tumor genetics, Cell Movement genetics, Epithelial-Mesenchymal Transition genetics, Melanoma genetics, Melanoma pathology, Skin Neoplasms genetics, Skin Neoplasms pathology

Abstract

Epithelial-to-mesenchymal transition is a critical process that increases the malignant potential of melanoma by facilitating invasion and dissemination of tumor cells. This study identified genes involved in the regulation of cellular invasion and evaluated whether they can be targeted to inhibit melanoma invasion. We identified Peroxidasin (PXDN), Netrin 4 (NTN4) and GLIS Family Zinc Finger 3 (GLIS3) genes consistently elevated in invasive mesenchymal-like melanoma cells. These genes and proteins were highly expressed in metastatic melanoma tumors, and gene silencing led to reduced melanoma invasion in vitro. Furthermore, migration of PXDN, NTN4 or GLIS3 siRNA transfected melanoma cells was inhibited following transplantation into the embryonic chicken neural tube compared to control siRNA transfected melanoma cells. Our study suggests that PXDN, NTN4 and GLIS3 play a functional role in promoting melanoma cellular invasion, and therapeutic approaches directed toward inhibiting the action of these proteins may reduce the incidence or progression of metastasis in melanoma patients., Competing Interests: None to declare.

Published

2016

31. Transketolase-like 1 ectopic expression is associated with DNA hypomethylation and induces the Warburg effect in melanoma cells.

Author

Jayachandran A, Lo PH, Chueh AC, Prithviraj P, Molania R, Davalos-Salas M, Anaka M, Walkiewicz M, Cebon J, and Behren A

Subjects

Azacitidine analogs & derivatives, Azacitidine pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Decitabine, Epigenesis, Genetic, Gene Expression Regulation, Neoplastic drug effects, Humans, Melanoma metabolism, Neoplasm Invasiveness, Neoplasm Metastasis, Promoter Regions, Genetic drug effects, Transketolase metabolism, DNA Methylation drug effects, Glycolysis, Melanoma genetics, Transketolase genetics, Up-Regulation

Abstract

Background: The metabolism of cancer cells is often reprogrammed by dysregulation of metabolic enzymes. Transketolase-like 1 (TKTL1) is a homodimeric transketolase linking the pentose-phosphate pathway with the glycolytic pathway. It is generally silenced at a transcriptional level in somatic tissues. However, in human cancers its expression is associated with the acquisition of a glycolytic phenotype (the Warburg effect) by cancer cells that contributes to the progression of malignant tumors. In melanoma, defective promoter methylation results in the expression of genes and their products that can affect the tumor cell's phenotype including the modification of immune and functional characteristics. The present study evaluates the role of TKTL1 as a mediator of disease progression in melanoma associated with a defective methylation phenotype., Methods: The expression of TKTL1 in metastatic melanoma tumors and cell lines was analysed by qRT-PCR and immunohistochemistry. The promoter methylation status of TKTL1 in melanoma cells was evaluated by quantitative methylation specific PCR. Using qRT-PCR, the effect of a DNA demethylating agent 5-aza-2'-deoxycytidine (5aza) on the expression of TKTL1 was examined. Biochemical and molecular analyses such as glucose consumption, lactate production, invasion, proliferation and cell cycle progression together with ectopic expression and siRNA mediated knockdown were used to investigate the role of TKTL1 in melanoma cells., Results: Expression of TKTL1 was highly restricted in normal adult tissues and was overexpressed in a subset of metastatic melanoma tumors and derived cell lines. The TKTL1 promoter was activated by hypomethylation and treatment with 5aza induced TKTL1 expression in melanoma cells. Augmented expression of TKTL1 in melanoma cells was associated with a glycolytic phenotype. Loss and gain of function studies revealed that TKTL1 contributed to enhanced invasion of melanoma cells., Conclusions: Our data provide evidence for an important role of TKTL1 in aerobic glycolysis and tumor promotion in melanoma that may result from defective promoter methylation. This epigenetic change may enable the natural selection of tumor cells with a metabolic phenotype and thereby provide a potential therapeutic target for a subset of melanoma tumors with elevated TKTL1 expression.

Published

2016

32. Mismatch in epitope specificities between IFNγ inflamed and uninflamed conditions leads to escape from T lymphocyte killing in melanoma.

Author

Woods K, Knights AJ, Anaka M, Schittenhelm RB, Purcell AW, Behren A, and Cebon J

Abstract

Background: A current focus in cancer treatment is to broaden responses to immunotherapy. One reason these therapies may prove inadequate is that T lymphocytes fail to recognize the tumor due to differences in immunogenic epitopes presented by the cancer cells under inflammatory or non-inflammatory conditions. The antigen processing machinery of the cell, the proteasome, cleaves proteins into peptide epitopes for presentation on MHC complexes. Immunoproteasomes in inflammatory melanomas, and in antigen presenting cells of the immune system, are enzymatically different to standard proteasomes expressed by tumors with no inflammation. This corresponds to alterations in protein cleavage between proteasome subtypes, and a disparate repertoire of MHC-presented epitopes., Methods: We assessed steady state and IFNγ-induced immunoproteasome expression in melanoma cells. Using epitope specific T-lymphocyte clones, we studied processing and presentation of three NY-ESO-1 HLA-Cw3 restricted epitopes by melanoma cell lines. Our experimental model allowed comparison of the processing of three distinct epitopes from a single antigen presented on the same HLA complex. We further investigated processing of these epitopes by direct inhibition, or siRNA mediated knockdown, of the immunoproteasome catalytic subunit LMP7., Results: Our data demonstrated a profound difference in the way in which immunogenic T-lymphocyte epitopes are presented by melanoma cells under IFNγ inflammatory versus non-inflammatory conditions. These alterations led to significant changes in the ability of T-lymphocytes to recognize and target melanoma cells., Conclusions: Our results illustrate a little-studied mechanism of immune escape by tumor cells which, with appropriate understanding and treatment, may be reversible. These data have implications for the design of cancer vaccines and adoptive T cell therapies.

Published

2016

33. Mycoplasma Infection Alters Cancer Stem Cell Properties in Vitro.

Author

Gedye C, Cardwell T, Dimopoulos N, Tan BS, Jackson H, Svobodová S, Anaka M, Behren A, Maher C, Hofmann O, Hide W, Caballero O, Davis ID, and Cebon J

Subjects

Bacterial Typing Techniques, Cell Culture Techniques standards, Cell Line, Tumor, Host-Pathogen Interactions, Humans, Melanoma genetics, Melanoma metabolism, Melanoma microbiology, Melanoma pathology, Mycoplasma hyorhinis genetics, Neoplasm Proteins metabolism, Neoplastic Stem Cells metabolism, Polymerase Chain Reaction, Primary Cell Culture, Quality Control, RNA, Ribosomal, 16S genetics, Reproducibility of Results, Skin Neoplasms genetics, Skin Neoplasms metabolism, Skin Neoplasms microbiology, Skin Neoplasms pathology, Gene Expression Regulation, Neoplastic, Mycoplasma hyorhinis isolation & purification, Neoplasm Proteins genetics, Neoplastic Stem Cells microbiology, RNA, Ribosomal, 16S isolation & purification

Abstract

Cancer cell lines can be useful to model cancer stem cells. Infection with Mycoplasma species is an insidious problem in mammalian cell culture. While investigating stem-like properties in early passage melanoma cell lines, we noted poorly reproducible results from an aliquot of a cell line that was later found to be infected with Mycoplasma hyorhinis. Deliberate infection of other early passage melanoma cell lines aliquots induced variable and unpredictable effects on expression of putative cancer stem cell markers, clonogenicity, proliferation and global gene expression. Cell lines established in stem cell media (SCM) were equally susceptible. Mycoplasma status is rarely reported in publications using cultured cells to study the cancer stem cell hypothesis. Our work highlights the importance of surveillance for Mycoplasma infection while using any cultured cells to interrogate tumor heterogeneity.

Published

2016

34. Pregnancy associated plasma protein-A links pregnancy and melanoma progression by promoting cellular migration and invasion.

Author

Prithviraj P, Anaka M, McKeown SJ, Permezel M, Walkiewicz M, Cebon J, Behren A, and Jayachandran A

Subjects

Animals, Cell Line, Tumor, Cell Movement genetics, Chick Embryo, Coculture Techniques, Disease Progression, Epithelial-Mesenchymal Transition physiology, Female, Gene Knockdown Techniques, Gene Silencing, Humans, Insulin-Like Growth Factor I biosynthesis, Insulin-Like Growth Factor I genetics, Insulin-Like Growth Factor I metabolism, Insulin-Like Growth Factor I pharmacology, Melanoma genetics, Melanoma pathology, Pregnancy, Pregnancy-Associated Plasma Protein-A genetics, Pregnancy-Associated Plasma Protein-A metabolism, RNA, Messenger biosynthesis, RNA, Messenger genetics, RNA, Small Interfering administration & dosage, RNA, Small Interfering genetics, Transfection, Transforming Growth Factor beta1 pharmacology, Melanoma metabolism, Pregnancy-Associated Plasma Protein-A biosynthesis

Abstract

Melanoma is the most common cancer diagnosed in pregnant women and an aggressive course with poorer outcomes is commonly described during pregnancy or shortly after childbirth. The underlying mechanisms for this are not understood. Here, we report that melanoma migration, invasiveness and progression are promoted by Pregnancy-Associated Plasma Protein-A (PAPPA), a pregnancy-associated metalloproteinase produced by the placenta that increases the bioavailability of IGF1 by cleaving it from a circulating complex formed with IGFBP4. We show that PAPPA is widely expressed by metastatic melanoma tumors and is elevated in melanoma cells exhibiting mesenchymal, invasive and label-retaining phenotypes. Notably, inhibition of PAPPA significantly reduced invasion and migration of melanoma cells in vitro and in vivo within the embryonic chicken neural tube. PAPPA-enriched pregnancy serum treatment enhanced melanoma motility in vitro. Furthermore, we report that IGF1 can induce the phenotypic and functional effects of epithelial-to-mesenchymal transition (EMT) in melanoma cells. In this study, we establish a clear relationship between a pregnancy-associated protein PAPPA, melanoma and functional effects mediated through IGF1 that provides a plausible mechanism for accelerated melanoma progression during pregnancy. This opens the possibility of targeting the PAPPA/IGF1 axis therapeutically.

Published

2015

35. Thrombospondin 1 promotes an aggressive phenotype through epithelial-to-mesenchymal transition in human melanoma.

Author

Jayachandran A, Anaka M, Prithviraj P, Hudson C, McKeown SJ, Lo PH, Vella LJ, Goding CR, Cebon J, and Behren A

Subjects

Animals, Cell Differentiation, Cell Line, Tumor, Epithelial-Mesenchymal Transition, Gene Expression, Heterografts, Humans, Melanoma genetics, Melanoma pathology, Mice, Phenotype, Thrombospondin 1 genetics, Thrombospondin 1 metabolism, Melanoma metabolism, Thrombospondin 1 biosynthesis

Abstract

Epithelial-to-mesenchymal transition (EMT), in which epithelial cells loose their polarity and become motile mesenchymal cells, is a determinant of melanoma metastasis. We compared gene expression signatures of mesenchymal-like melanoma cells with those of epithelial-like melanoma cells, and identified Thrombospondin 1 (THBS1) as highly up-regulated in the mesenchymal phenotype. This study investigated whether THBS1, a major physiological activator of transforming growth factor (TGF)-beta, is involved in melanoma EMT-like process. We sought to examine expression patterns in distinct melanoma phenotypes including invasive, de-differentiated, label-retaining and drug resistant populations that are putatively associated with an EMT-like process. Here we show that THBS1 expression and secretion was elevated in melanoma cells exhibiting invasive, drug resistant, label retaining and mesenchymal phenotypes and correlated with reduced expression of genes involved in pigmentation. Elevated THBS1 levels were detected in Vemurafenib resistant melanoma cells and inhibition of THBS1 led to significantly reduced chemoresistance in melanoma cells. Notably, siRNA-mediated silencing of THBS1 and neutralizing antibody to THBS1 reduced invasion in mesenchymal-like melanoma cells, while ectopic THBS1 expression in epithelial-like melanoma cells enhanced invasion. Furthermore, the loss of THBS1 inhibited in vivo motility of melanoma cells within the embryonic chicken neural tube. In addition, we found aberrant THBS1 protein expression in metastatic melanoma tumor biopsies. These results implicate a role for THBS1 in EMT, and hence THBS1 may serve as a novel target for strategies aimed at the treatment of melanoma invasion and drug resistance.

Published

2014

36. FOXP3 over-expression inhibits melanoma tumorigenesis via effects on proliferation and apoptosis.

Author

Tan B, Anaka M, Deb S, Freyer C, Ebert LM, Chueh AC, Al-Obaidi S, Behren A, Jayachandran A, Cebon J, Chen W, and Mariadason JM

Subjects

Animals, Apoptosis physiology, Carcinogenesis, Cell Growth Processes physiology, Cell Line, Tumor, Forkhead Transcription Factors genetics, Humans, Melanoma genetics, Mice, Mice, Inbred BALB C, Mice, Nude, Neoplasm Metastasis, Transfection, Forkhead Transcription Factors biosynthesis, Melanoma metabolism, Melanoma pathology

Abstract

The Forkhead box P3 (FOXP3) transcription factor is the key driver of regulatory T cell (Treg cells) differentiation and immunosuppressive function. In addition, FOXP3 has been reported to be expressed in many tumors, including melanoma. However, its role in tumorigenesis is conflicting, with both tumor suppressive and tumor promoting functions described. The aim of the current study was to characterize the expression and function of FOXP3 in melanoma. FOXP3 expression was detected by immunohistochemistry (IHC) in 12% (18/146) of stage III and IV melanomas. However expression was confined to fewer than 1% of cells in these tumors. Stable over-expression of FOXP3 in the SK-MEL-28 melanoma cell line reduced cell proliferation and clonogenicity in vitro, and reduced xenograft growth in vivo. FOXP3 over-expression also increased pigmentation and the rate of apoptosis of SK-MEL-28 cells. Based on its infrequent expression in human melanoma, and its growth inhibitory and pro-apoptotic effect in over-expressing melanoma cells, we conclude that FOXP3 is not likely to be a key tumor suppressor or promoter in melanoma.

Published

2014

37. Intratumoral genetic heterogeneity in metastatic melanoma is accompanied by variation in malignant behaviors.

Author

Anaka M, Hudson C, Lo PH, Do H, Caballero OL, Davis ID, Dobrovic A, Cebon J, and Behren A

Subjects

Cell Line, Tumor, Clone Cells pathology, DNA Copy Number Variations, Female, Humans, Male, Neoplasm Metastasis, Oligonucleotide Array Sequence Analysis, Polymorphism, Single Nucleotide, Transcriptome, Genetic Variation, Melanoma genetics, Melanoma pathology

Abstract

Background: Intratumoral heterogeneity is a major obstacle for the treatment of cancer, as the presence of even minor populations that are insensitive to therapy can lead to disease relapse. Increased clonal diversity has been correlated with a poor prognosis for cancer patients, and we therefore examined genetic, transcriptional, and functional diversity in metastatic melanoma., Methods: Amplicon sequencing and SNP microarrays were used to profile somatic mutations and DNA copy number changes in multiple regions from metastatic lesions. Clonal genetic and transcriptional heterogeneity was also assessed in single cell clones from early passage cell lines, which were then subjected to clonogenicity and drug sensitivity assays., Results: MAPK pathway and tumor suppressor mutations were identified in all regions of the melanoma metastases analyzed. In contrast, we identified copy number abnormalities present in only some regions in addition to homogeneously present changes, suggesting ongoing genetic evolution following metastatic spread. Copy number heterogeneity from a tumor was represented in matched cell line clones, which also varied in their clonogenicity and drug sensitivity. Minor clones were identified based on dissimilarity to the parental cell line, and these clones were the most clonogenic and least sensitive to drugs. Finally, treatment of a polyclonal cell line with paclitaxel to enrich for drug-resistant cells resulted in the adoption of a gene expression profile with features of one of the minor clones, supporting the idea that these populations can mediate disease relapse., Conclusion: Our results support the hypothesis that minor clones might have major consequences for patient outcomes in melanoma.

Published

2013

38. The Ludwig institute for cancer research Melbourne melanoma cell line panel.

Author

Behren A, Anaka M, Lo PH, Vella LJ, Davis ID, Catimel J, Cardwell T, Gedye C, Hudson C, Stan R, and Cebon J

Subjects

Antigens, Neoplasm metabolism, Cell Differentiation, Cluster Analysis, Female, Gene Expression Regulation, Neoplastic, HLA Antigens metabolism, Humans, Male, Mutation, Oligonucleotide Array Sequence Analysis, Proto-Oncogene Proteins B-raf metabolism, ras Proteins metabolism, Cell Line, Tumor, Drug Screening Assays, Antitumor, Melanoma metabolism

Published

2013

39. FOXP3 is not mutated in human melanoma.

Author

Tan B, Behren A, Anaka M, Vella L, Cebon J, Mariadason JM, and Chen W

Subjects

Base Sequence, Cell Line, Tumor, Chromosomes, Human, X genetics, DNA Mutational Analysis, Female, Humans, Male, Molecular Sequence Data, Mutation physiology, Forkhead Transcription Factors genetics, Melanoma genetics, Skin Neoplasms genetics

Published

2012

40. Stem cell media culture of melanoma results in the induction of a nonrepresentative neural expression profile.

Author

Anaka M, Freyer C, Gedye C, Caballero O, Davis ID, Behren A, and Cebon J

Subjects

Animals, Antigens, Differentiation genetics, Antigens, Differentiation metabolism, Cell Culture Techniques, Cell Proliferation, Cluster Analysis, DNA Copy Number Variations, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Humans, Male, Mice, Mice, Inbred NOD, Mice, SCID, Neoplasm Transplantation, Cell Line, Tumor metabolism, Culture Media, Melanoma pathology, Stem Cells metabolism

Abstract

The ability of cell lines to accurately represent cancer is a major concern in preclinical research. Culture of glioma cells as neurospheres in stem cell media (SCM) has been shown to better represent the genotype and phenotype of primary glioblastoma in comparison to serum cell lines. Despite the use of neurosphere-like models of many malignancies, there has been no robust analysis of whether other cancers benefit from a more representative phenotype and genotype when cultured in SCM. We analyzed the growth properties, transcriptional profile, and genotype of melanoma cells grown de novo in SCM, as while melanocytes share a common precursor with neural cells, melanoma frequently demonstrates divergent behavior in cancer stem cell assays. SCM culture of melanoma cells induced a neural lineage gene expression profile that was not representative of matched patient tissue samples and which could be induced in serum cell lines by switching them into SCM. There was no enrichment for expression of putative melanoma stem cell markers, but the SCM expression profile did overlap significantly with that of SCM cultures of glioma, suggesting that the observed phenotype is media-specific rather than melanoma-specific. Xenografts derived from either culture condition provided the best representation of melanoma in situ. Finally, SCM culture of melanoma did not prevent ongoing acquisition of DNA copy number abnormalities. In conclusion, SCM culture of melanoma does not provide a better representation of the phenotype or genotype of metastatic melanoma, and the resulting neural bias could potentially confound therapeutic target identification., (Copyright © 2011 AlphaMed Press.)

Published

2012

41. Genomic imprinting in Drosophila has properties of both mammalian and insect imprinting.

Author

Anaka M, Lynn A, McGinn P, and Lloyd VK

Subjects

Animals, Female, Gene Silencing, Male, X Chromosome, Drosophila melanogaster genetics, Genomic Imprinting, Mammals genetics

Abstract

Genomic imprinting is a process that marks DNA, causing a change in gene or chromosome behavior, depending on the sex of the transmitting parent. In mammals, most examples of genomic imprinting affect the transcription of individual or small clusters of genes whereas in insects, genomic imprinting tends to silence entire chromosomes. This has been interpreted as evidence of independent evolutionary origins for imprinting. To investigate how these types of imprinting are related, we performed a phenotypic, molecular, and cytological analysis of an imprinted chromosome in Drosophila melanogaster. Analysis of this chromosome reveals that the imprint results in transcriptional silencing. Yet, the domain of transcriptional silencing is very large, extending at least 1.2 Mb and encompassing over 100 genes, and is associated with decreased somatic polytenization of the entire chromosome. We propose that repression of somatic replication in polytenized cells, as a secondary response to the imprint, acts to extend the size of the imprinted domain to an entire chromosome. Thus, imprinting in Drosophila has properties of both typical mammalian and insect imprinting which suggests that genomic imprinting in Drosophila and mammals is not fundamentally different; imprinting is manifest as transcriptional silencing of a few genes or silencing of an entire chromosome depending on secondary processes such as differences in gene density and polytenization.

Published

2009

42. The white gene of Drosophila melanogaster encodes a protein with a role in courtship behavior.

Author

Anaka M, MacDonald CD, Barkova E, Simon K, Rostom R, Godoy RA, Haigh AJ, Meinertzhagen IA, and Lloyd V

Subjects

Animals, COS Cells, Cell Line, Chlorocebus aethiops, Drosophila melanogaster physiology, Endosomes metabolism, Gene Expression, Genotype, Homosexuality, Male genetics, Humans, Learning physiology, Male, Movement physiology, Mutation, Smell genetics, Transformation, Genetic, ATP-Binding Cassette Transporters genetics, Drosophila Proteins genetics, Drosophila melanogaster genetics, Eye Proteins genetics, Genes, Insect, Sexual Behavior, Animal physiology

Abstract

The white gene of Drosophila melanogaster has been extensively studied, yet it is still not understood how its ectopic overexpression induces male-male courtship. To investigate the cellular basis of this behavior, we examined the sexual behavior of several classes of mutants. We find that male-male courtship is seen not only in flies overexpressing the white gene, but also in mutants expected to have mislocalized White protein. This finding confirms that mislocalizing White transporter in the cells in which it is normally expressed will produce male-male courtship behaviors; the courtship behavior is not an indirect consequence of aberrant physiological changes elsewhere in the body. Male-male courtship is also seen in some mutants with altered monoamine metabolism and deficits in learning and memory, but can be distinguished from that produced by White mislocalization by its reduced intensity and locomotor activity. Double mutants overexpressing white and with mutations in genes for serotonergic neurons suggest that male-male courtship produced by mislocalizing White may not be mediated exclusively by serotonergic neurons. We also find decreased olfactory learning in white mutants and in individuals with mutations in the genes for White's binding partners, brown and scarlet. Finally, in cultured Drosophila and mammalian cells, the White transporter is found in the endosomal compartment. The additional genes identified here as being involved in male-male courtship increase the repertoire of mutations available to study sexual behavior in Drosophila.

Published

2008