Your search keyword '"Boussioutas, Alex"' showing total 66 results

1. DCLK1 induces a pro-tumorigenic phenotype to drive gastric cancer progression.

Author

Afshar-Sterle, Shoukat, Carli, Annalisa L.E., O'Keefe, Ryan, Tse, Janson, Fischer, Stefanie, Azimpour, Alexander I., Baloyan, David, Elias, Lena, Thilakasiri, Pathum, Patel, Onisha, Ferguson, Fleur M., Eissmann, Moritz F., Chand, Ashwini L., Gray, Nathanael S., Busuttil, Rita, Boussioutas, Alex, Lucet, Isabelle S., Ernst, Matthias, and Buchert, Michael

Subjects

STROMAL cell-derived factor 1, CANCER stem cells, STOMACH cancer, EPITHELIAL-mesenchymal transition, TUMOR growth

Abstract

Doublecortin-like kinase 1 (DCLK1) is a proposed driver of gastric cancer (GC) that phosphorylates serine and threonine residues. Here, we showed that the kinase activity of DCLK1 orchestrated cancer cell–intrinsic and–extrinsic processes that led to pro-invasive and pro-metastatic reprogramming of GC cells. Inhibition of the kinase activity of DCLK1 reduced the growth of subcutaneous xenograft tumors formed from MKN1 human gastric carcinoma cells in mice and decreased the abundance of the stromal markers α-Sma, vimentin, and collagen. Similar effects were seen in mice with xenograft tumors formed from MKN1 cells expressing a kinase-inactive DCLK1 mutant (MKN1D511N). MKN1D511N cells also had reduced in vitro migratory potential and stemness compared with control cells. Mice orthotopically grafted with MKN1 cells overexpressing DCLK1 (MKN1DCLK1) showed increased invasiveness and had a greater incidence of lung metastases compared with those grafted with control MKN1 cells. Mechanistically, we showed that the chemokine CXCL12 acted downstream of DCLK1 in cultured MKN1 cells and in mice subcutaneously implanted with gastric tumors formed by MKN1DCLK1 cells. Moreover, inhibition of the kinase activity of DCLK1 or the expression of DCLK1D511N reversed the pro-tumorigenic and pro-metastatic phenotype. Together, this study establishes DCLK1 as a broadly acting and potentially targetable promoter of GC. Editor's summary: The serine/threonine kinase DCLK1 is a putative cancer stem cell marker that is associated with the progression of gastric cancers. Afshar-Sterle et al. found that mutating the kinase domain of DCLK1 or inhibiting its kinase activity reduced tumor growth, abundance of markers of stromal remodeling, and induction of epithelial-to-mesenchymal transition (EMT). The tumor-intrinsic and -extrinsic effects of DCLK1 at least partially depended on increased amounts of CXCL12, which correlated with DCLK1 abundance and acted downstream of DCLK1. These results shed light on the mechanistic contribution of DCLK1 in shaping gastric cancer progression. —Amy E. Baek [ABSTRACT FROM AUTHOR]

Published

2024

2. Associations between pathological features and risk of metachronous colorectal cancer.

Author

Zhang, Ye, Win, Aung Ko, Makalic, Enes, Buchanan, Daniel D., Pai, Rish K., Phipps, Amanda I., Rosty, Christophe, Boussioutas, Alex, Karahalios, Amalia, and Jenkins, Mark A.

Subjects

COLORECTAL cancer, HEREDITARY nonpolyposis colorectal cancer, COLON cancer, CONFIDENCE intervals, REGRESSION analysis, TUMORS

Abstract

Survivors of colorectal cancer (CRC) are at risk of developing another primary colorectal cancer ‐ metachronous CRC. Understanding which pathological features of the first tumour are associated with risk of metachronous CRC might help tailor existing surveillance guidelines. Population‐based CRC cases were recruited from the United States, Canada and Australia between 1997 and 2012 and followed prospectively until 2022 by the Colon Cancer Family Registry. Metachronous CRC was defined as a new primary CRC diagnosed at least 1 year after the initial CRC. Those with the genetic cancer predisposition Lynch syndrome or MUTYH mutation carriers were excluded. Cox regression models were fitted to estimate hazard ratios (HRs) and corresponding 95% confidence intervals (CIs) for the associations. Of 6085 CRC cases, 138 (2.3%) were diagnosed with a metachronous CRC over a median follow‐up time of 12 years (incidence: 2.0 per 1000 person‐years). CRC cases with a synchronous CRC were 3.4‐fold more likely to develop a metachronous CRC (adjusted HR: 3.36, 95% CI: 1.89–5.98) than those without a synchronous tumour. CRC cases with MMR‐deficient tumours had a 72% increased risk of metachronous CRC (adjusted HR: 1.72, 95% CI: 1.11–2.64) compared to those with MMR‐proficient tumours. Compared to cases who had an adenocarcinoma histologic type, those with an undifferentiated histologic type were 77% less likely to develop a metachronous CRC (adjusted HR: 0.23, 95% CI: 0.06–0.94). Existing surveillance guidelines for CRC survivors could be updated to include increased surveillance for those whose first CRC was diagnosed with a synchronous CRC or was MMR‐deficient. [ABSTRACT FROM AUTHOR]

Published

2024

3. Marginal zone lymphomas: a consensus practice statement from the Australasian Lymphoma Alliance.

Author

Lasica, Masa, Anderson, Mary A., Boussioutas, Alex, Gregory, Gareth P., Hamad, Nada, Manos, Kate, McKelvie, Penny, Ng, Michael, Campbell, Belinda, Palfreyman, Emma, Salvaris, Ross, Weinkove, Robert, Wight, Joel, Opat, Stephen, and Tam, Constantine

Subjects

CONSENSUS (Social sciences), MEDICAL protocols, NON-Hodgkin's lymphoma, CANCER relapse, TREATMENT effectiveness, SYMPTOMS

Abstract

Marginal zone lymphomas (MZLs) are a rare, indolent group of non‐Hodgkin lymphomas with different diagnostic, genetic and clinical features and therapeutic implications. The most common is extranodal MZL of mucosa‐associated lymphoid tissue, followed by splenic MZL and nodal MZL. Patients with MZL generally have good outcomes with long survival rates but frequently have a relapsing/remitting course requiring several lines of therapy. The heterogeneous presentation and relapsing course present the clinician with several diagnostic and therapeutic challenges. This position statement presents evidence‐based recommendations in the setting of Australia and New Zealand. [ABSTRACT FROM AUTHOR]

Published

2024

4. Searching for low phospholipid associated cholelithiasis among patients with post‐cholecystectomy biliary pain.

Author

Trinh, Andrew, Tjandra, Doug, Park, Yeung‐Ae, Sood, Siddharth, Thomson, Benjamin, Speer, Tony, Buchanan, Daniel, Boussioutas, Alex, and Metz, Andrew J.

Subjects

CHOLANGIOGRAPHY, GALLSTONES, BILE ducts, BILE acids, CHOLECYSTITIS, WOMEN patients, ABDOMINAL pain

Abstract

Introduction: Low phospholipid associated cholelithiasis (LPAC) is associated with variants of the adenosine triphosphate‐binding cassette subfamily B, member 4 (ABCB4) gene and is characterized by reduced phosphatidylcholine secretion into bile, impairing the formation of micelles and thus exposing bile ducts to toxic bile acids and increasing cholesterol saturation. LPAC is present in 1% of patients with gallstones and post‐cholecystectomy pain is common in this group. LPAC is an under‐appreciated cause of post‐cholecystectomy pain. The aim of this study is to assess a cohort of patients with post‐cholecystectomy pain to identify those with clinical features suggesting that further investigations for LPAC would be beneficial. Methods: A retrospective chart review was performed of the first 2 years of post‐operative follow‐up for all patients under 40 years of age undergoing cholecystectomy for symptomatic gallstones at a tertiary centre between January 2016 and December 2017. Results: 258 patients under the age of 40 underwent a cholecystectomy. 50 patients (19.4%) reported abdominal pain post‐cholecystectomy. Five patients (1.9%) fulfilled the criteria for suspected LPAC. Family history of gallstones was documented in 33 of 258 (12.8%) of cases. Obstetric history was obtained in 69 of 197 (35%) female patients. None of the five patients identified above who satisfied the criteria of LPAC had the diagnosis of LPAC considered by their treating clinicians. Conclusion: LPAC is an under‐recognized cause of post‐cholecystectomy pain. Treatment can avoid long‐term symptoms and complications. Clinicians should take a family history and obstetric history to alert them to the diagnosis of LPAC. [ABSTRACT FROM AUTHOR]

Published

2024

5. Li Fraumeni Syndrome predisposes to gastro-esophageal junction tumours.

Author

Tjandra, Douglas and Boussioutas, Alex

Subjects

LI-Fraumeni syndrome, GASTROINTESTINAL cancer, TUMORS, ESOPHAGEAL cancer, BRAIN cancer, STOMACH cancer

Abstract

Li-Fraumeni Syndrome (LFS), caused by germline pathogenic variants in TP53, predisposes to a wide range of young-onset malignancies, particularly sarcoma, breast and brain cancer. More recently, an increased risk of gastric adenocarcinoma has been recognised, although uptake of surveillance upper endoscopy is unclear. Our retrospective review of 65 patients with LFS, of whom 53.8% had undergone endoscopy, identified four patients (6.2%) with gastro-esophageal junction (GEJ) adenocarcinomas. Two cases were found on asymptomatic screening and were early stage. No cases had family history of gastrointestinal malignancy. Reviewing genomic data from The Cancer Genome Atlas Program, 76.4% of sporadic esophageal adenocarcinomas harboured somatic TP53 pathogenic variants, compared with 39.9% of non-cardia gastric cancers. This similar pattern observed in germline and sporadic cases warrants further investigation. We propose that upper endoscopy be recommended to all patients with LFS, with a focus on appropriate surveillance of the GEJ. [ABSTRACT FROM AUTHOR]

Published

2024

6. Gastric Intestinal Metaplasia: Challenges and the Opportunity for Precision Prevention.

Author

Tjandra, Douglas, Busuttil, Rita A., and Boussioutas, Alex

Subjects

GASTROINTESTINAL disease diagnosis, STOMACH tumors, PUBLIC health surveillance, HEALTH services accessibility, HELICOBACTER pylori, ACCURACY, ARTIFICIAL intelligence, METAPLASIA, PREVENTIVE health services, CANCER patients, RISK assessment, SURVIVAL rate, PRECANCEROUS conditions, HEALTH promotion

Abstract

Simple Summary: Gastric adenocarcinoma is the fifth most common cancer worldwide and the fourth most lethal. It is often asymptomatic at an early stage, when survival rates are highest (>90%) with minimally invasive endoscopic intervention or surgery. Gastric intestinal metaplasia (GIM) is a persistent, premalignant lesion in the stomach, arising in the context of chronic inflammation, which predisposes one to gastric cancer. It is considered a pivotal stage along a continuum to gastric cancer and has a median latency period of ~6 years before progression to cancer typically occurs, offering a window of opportunity for intervention. However, only a small proportion (0.25–2.5%) with GIM ultimately progress to cancer; therefore, approaches to surveillance vary widely around the world. We summarise the current evidence supporting best clinical practice in the diagnosis, assessment and management of GIM, and the opportunities to achieve precision in predictions in the coming decades. GIM is a persistent, premalignant lesion whereby gastric mucosa is replaced by metaplastic mucosa resembling intestinal tissue, arising in the setting of chronic inflammation, particularly in the context of Helicobacter pylori. While the overall rates of progression to gastric adenocarcinoma are low, estimated at from 0.25 to 2.5%, there are features that confer a much higher risk and warrant follow-up. In this review, we collate and summarise the current knowledge regarding the pathogenesis of GIM, and the clinical, endoscopic and histologic risk factors for cancer. We examine the current state-of-practice with regard to the diagnosis and management of GIM, which varies widely in the published guidelines and in practice. We consider the emerging evidence in population studies, artificial intelligence and molecular markers, which will guide future models of care. The ultimate goal is to increase the detection of early gastric dysplasia/neoplasia that can be cured while avoiding unnecessary surveillance in very low-risk individuals. [ABSTRACT FROM AUTHOR]

Published

2023

7. Infliximab Trough Levels Are Associated With Transmural Sonographic Healing in Inflammatory Bowel Disease.

Author

Vaughan, Rose, Murphy, Elise, Nalder, Michelle, Gibson, Robert N, Ardalan, Zaid, Boussioutas, Alex, and Christensen, Britt

Published

2023

8. Becoming and being a parent with an inherited predisposition to diffuse gastric cancer: A qualitative study of young adults with a CDH1 pathogenic variant.

Author

Tutty, Erin, Forbes Shepherd, Rowan, Hoskins, Cass, Purvis, Rebecca, Shanahan, Mary, Boussioutas, Alex, and Forrest, Laura E.

Subjects

STOMACH tumors, PARENT attitudes, HUMAN reproduction, GENETIC mutation, COUNSELING, ONCOGENES, RESEARCH methodology, CELL cycle proteins, INTERVIEWING, PARENTHOOD, QUALITATIVE research, RISK assessment, EXPERIENCE, GASTRECTOMY, PARENTING, DISEASE susceptibility, AUSTRALIANS, DECISION making, HUMAN reproductive technology, RESEARCH funding, THEMATIC analysis, ADULTS, DISEASE risk factors

Abstract

This study explored the experiences of young people with hereditary diffuse gastric cancer (HDGC), an inherited cancer predisposition syndrome, as they navigate becoming and being a parent. We used interpretive description and conducted semi-structured interviews with 13 young Australians (18–39 years) with a CDH1 pathogenic variant (PV). Data were analyzed using team-based, reflexive thematic analysis. Participants' reproductive decisions centered on the perceived manageability of HDGC, namely via gastrectomy, and timing of their genetic testing. Participants yet to have children and those with challenging gastrectomy experiences favored using reproductive technologies to prevent passing on their PV. Parents who had children before genetic testing described complicated decisions about having more children. Gastrectomy was considered a parental responsibility but recovery diminished parenting abilities. Young people with HDGC face unique challenges navigating reproductive decision-making and parenting with gastrectomy. Findings lend credence to calls for longitudinal, developmentally sensitive genetic counseling services. [ABSTRACT FROM AUTHOR]

Published

2023

9. A tumor focused approach to resolving the etiology of DNA mismatch repair deficient tumors classified as suspected Lynch syndrome.

Author

Walker, Romy, Mahmood, Khalid, Joo, Jihoon E., Clendenning, Mark, Georgeson, Peter, Como, Julia, Joseland, Sharelle, Preston, Susan G., Antill, Yoland, Austin, Rachel, Boussioutas, Alex, Bowman, Michelle, Burke, Jo, Campbell, Ainsley, Daneshvar, Simin, Edwards, Emma, Gleeson, Margaret, Goodwin, Annabel, Harris, Marion T., and Henderson, Alex

Subjects

DNA mismatch repair, HEREDITARY nonpolyposis colorectal cancer, ETHYLCELLULOSE, ETIOLOGY of diseases, TUMORS, GENETIC variation

Abstract

Routine screening of tumors for DNA mismatch repair (MMR) deficiency (dMMR) in colorectal (CRC), endometrial (EC) and sebaceous skin (SST) tumors leads to a significant proportion of unresolved cases classified as suspected Lynch syndrome (SLS). SLS cases (n = 135) were recruited from Family Cancer Clinics across Australia and New Zealand. Targeted panel sequencing was performed on tumor (n = 137; 80×CRCs, 33×ECs and 24xSSTs) and matched blood-derived DNA to assess for microsatellite instability status, tumor mutation burden, COSMIC tumor mutational signatures and to identify germline and somatic MMR gene variants. MMR immunohistochemistry (IHC) and MLH1 promoter methylation were repeated. In total, 86.9% of the 137 SLS tumors could be resolved into established subtypes. For 22.6% of these resolved SLS cases, primary MLH1 epimutations (2.2%) as well as previously undetected germline MMR pathogenic variants (1.5%), tumor MLH1 methylation (13.1%) or false positive dMMR IHC (5.8%) results were identified. Double somatic MMR gene mutations were the major cause of dMMR identified across each tumor type (73.9% of resolved cases, 64.2% overall, 70% of CRC, 45.5% of ECs and 70.8% of SSTs). The unresolved SLS tumors (13.1%) comprised tumors with only a single somatic (7.3%) or no somatic (5.8%) MMR gene mutations. A tumor-focused testing approach reclassified 86.9% of SLS into Lynch syndrome, sporadic dMMR or MMR-proficient cases. These findings support the incorporation of tumor sequencing and alternate MLH1 methylation assays into clinical diagnostics to reduce the number of SLS patients and provide more appropriate surveillance and screening recommendations. [ABSTRACT FROM AUTHOR]

Published

2023

10. Diet and risk of Barrett's oesophagus: Melbourne collaborative cohort study.

Author

Wang, Sabrina E., Hodge, Allison, Dashti, S Ghazaleh, Dixon-Suen, Suzanne C., Castaño-Rodríguez, Natalia, Thomas, Robert, Giles, Graham, Boussioutas, Alex, Kendall, Bradley, and English, Dallas R.

Subjects

FOOD habits, CONFIDENCE intervals, FOOD consumption, NUTRITIONAL requirements, CASE-control method, BARRETT'S esophagus, CAROTENOIDS, RISK assessment, QUESTIONNAIRES, RESEARCH funding, LOGISTIC regression analysis, ODDS ratio, SENSITIVITY & specificity (Statistics), ESOPHAGEAL tumors, LONGITUDINAL method, DISEASE risk factors, DISEASE complications

Abstract

Barrett's oesophagus (BE) is the precursor of oesophageal adenocarcinoma, which has become the most common type of oesophageal cancer in many Western populations. Existing evidence on diet and risk of BE predominantly comes from case–control studies, which are subject to recall bias in measurement of diet. We aimed to investigate the potential effect of diet, including macronutrients, carotenoids, food groups, specific food items, beverages and dietary scores, on risk of BE in over 20 000 participants of the Melbourne Collaborative Cohort Study. Diet at baseline (1990–1994) was measured using a food frequency questionnaire. The outcome was BE diagnosed between baseline and follow-up (2007–2010). Logistic regression models were used to estimate OR and 95 % CI for diet in relation to risk of BE. Intakes of leafy vegetables and fruit were inversely associated with risk of BE (highest v. lowest quartile: OR = 0·59; CI: 0·38, 0·94; P -trend = 0·02 and OR = 0·58; CI: 0·37, 0·93; P -trend = 0·02 respectively), as were dietary fibre and carotenoids. Stronger associations were observed for food than the nutrients found in them. Positive associations were observed for discretionary food (OR = 1·54; CI: 0·97, 2·44; P -trend = 0·04) and total fat intake (OR per 10 g/d = 1·11; CI: 1·00, 1·23), the association for fat was less robust in sensitivity analyses. No association was observed for meat, protein, dairy products or diet scores. Diet is a potential modifiable risk factor for BE. Public health and clinical guidelines that incorporate dietary recommendations could contribute to reduction in risk of BE and, thereby, oesophageal adenocarcinoma. [ABSTRACT FROM AUTHOR]

Published

2023

11. Targeted liver ultrasound performed by an expert is the pivotal imaging examination for low phospholipid-associated cholelithiasis.

Author

Su, Shu, Trinh, Andrew, Metz, Andrew J., Speer, Tony, Simkin, Paul, Buchanan, Daniel, Boussioutas, Alex, and Gibson, Robert

Published

2023

12. Immune-Related Adverse Events of the Gastrointestinal System.

Author

Nicolaides, Steven and Boussioutas, Alex

Subjects

GASTROINTESTINAL system, IMMUNE checkpoint inhibitors, GUT microbiome, TUMORS, DRUG side effects, COLITIS

Abstract

Simple Summary: Immunotherapy is an effective cancer treatment that activates the immune system to target and destroy cancer cells. The emerging use of a form of immunotherapy referred to as immune checkpoint inhibitors is often limited by the development of immune-related adverse events. This often leads to the discontinuation of treatment and limits good outcomes. In this review, we summarize the spectrum of immune-related adverse events of the gastrointestinal system with a focus on their management and emerging therapies. Immune checkpoint inhibitors (ICI) are a form of immunotherapy that have revolutionized the treatment of a number of cancers. Specifically, they are antibodies targeted against established and emerging immune checkpoints, such as cytotoxic T-cell antigen 4 (CTLA4), programmed cell death ligand 1 (PD-L1) and programmed cell death 1 protein (PD-1) on CD8-positive T cells, which promote the destruction of tumor cells. While the immune checkpoint inhibitors are very effective in the treatment of a number of cancers, their use is limited by serious and in some cases life-threatening immune-related adverse events. While these involve many organs, one of the most prevalent serious adverse events is immune checkpoint inhibitor colitis, occurring in a significant proportion of patients treated with this therapy. In this review, we aim to broadly describe the immune-related adverse events known to occur within the gastrointestinal system and the potential role played by the intestinal microbiome. [ABSTRACT FROM AUTHOR]

Published

2023

13. Therapeutic Drug Monitoring of Subcutaneous Infliximab in Inflammatory Bowel Disease—Understanding Pharmacokinetics and Exposure Response Relationships in a New Era of Subcutaneous Biologics.

Author

Little, Robert D., Ward, Mark G., Wright, Emily, Jois, Asha J., Boussioutas, Alex, Hold, Georgina L., Gibson, Peter R., and Sparrow, Miles P.

Subjects

DRUG monitoring, INFLAMMATORY bowel diseases, CROHN'S disease, PHARMACOKINETICS, INFLIXIMAB

Abstract

CT-P13 is the first subcutaneous infliximab molecule approved for the management of inflammatory bowel disease (IBD). Compared to intravenous therapy, SC infliximab offers a range of practical, micro- and macroeconomic advantages. Data from the rheumatological literature suggest that subcutaneous CT-P13 may lead to superior disease outcomes in comparison to intravenous infliximab. Existing studies in IBD have focussed on pharmacokinetic comparisons and are inadequately powered to evaluate efficacy and safety differences between the two modes of administration. However, emerging clinical trial and real-world data support comparable clinical, biochemical, endoscopic and safety outcomes between subcutaneous and intravenous infliximab in both luminal Crohn's disease and ulcerative colitis. Across the available data, subcutaneous CT-P13 provides relative pharmacokinetic stability and higher trough drug levels when compared to intravenous administration. The clinical impact of this observation on immunogenicity and treatment persistence is yet to be determined. Trough levels between the two methods of administration should not be compared in isolation as any subcutaneous advantage must be considered in the context of comparable total drug exposure and the theoretical disadvantage of lower peak concentrations compared to intravenous therapy. Furthermore, target drug levels for subcutaneous CT-P13 associated with remission are not known. In this review, we present the available literature surrounding the pharmacokinetics of subcutaneous CT-P13 in the context of therapeutic drug monitoring and highlight the potential significance of these observations on the clinical management of patients with IBD. [ABSTRACT FROM AUTHOR]

Published

2022

14. DEMoS: a deep learning-based ensemble approach for predicting the molecular subtypes of gastric adenocarcinomas from histopathological images.

Author

Wang, Yanan, Hu, Changyuan, Kwok, Terry, Bain, Christopher A, Xue, Xiangyang, Gasser, Robin B, Webb, Geoffrey I, Boussioutas, Alex, Shen, Xian, Daly, Roger J, and Song, Jiangning

Subjects

DEEP learning, HISTOPATHOLOGY, STOMACH cancer, ADENOCARCINOMA, SOURCE code, PROGNOSTIC tests

Abstract

Motivation The molecular subtyping of gastric cancer (adenocarcinoma) into four main subtypes based on integrated multiomics profiles, as proposed by The Cancer Genome Atlas (TCGA) initiative, represents an effective strategy for patient stratification. However, this approach requires the use of multiple technological platforms, and is quite expensive and time-consuming to perform. A computational approach that uses histopathological image data to infer molecular subtypes could be a practical, cost- and time-efficient complementary tool for prognostic and clinical management purposes. Results Here, we propose a deep learning ensemble approach (called DEMoS) capable of predicting the four recognized molecular subtypes of gastric cancer directly from histopathological images. DEMoS achieved tile-level area under the receiver-operating characteristic curve (AUROC) values of 0.785, 0.668, 0.762 and 0.811 for the prediction of these four subtypes of gastric cancer [i.e. (i) Epstein–Barr (EBV)-infected, (ii) microsatellite instability (MSI), (iii) genomically stable (GS) and (iv) chromosomally unstable tumors (CIN)] using an independent test dataset, respectively. At the patient-level, it achieved AUROC values of 0.897, 0.764, 0.890 and 0.898, respectively. Thus, these four subtypes are well-predicted by DEMoS. Benchmarking experiments further suggest that DEMoS is able to achieve an improved classification performance for image-based subtyping and prevent model overfitting. This study highlights the feasibility of using a deep learning ensemble-based method to rapidly and reliably subtype gastric cancer (adenocarcinoma) solely using features from histopathological images. Availability and implementation All whole slide images used in this study was collected from the TCGA database. This study builds upon our previously published HEAL framework, with related documentation and tutorials available at http://heal.erc.monash.edu.au. The source code and related models are freely accessible at https://github.com/Docurdt/DEMoS.git. Supplementary information Supplementary data are available at Bioinformatics online. [ABSTRACT FROM AUTHOR]

Published

2022

15. Toward transmural healing: Sonographic healing is associated with improved long‐term outcomes in patients with Crohn's disease.

Author

Vaughan, Rose, Tjandra, Douglas, Patwardhan, Ashwin, Mingos, Nicholas, Gibson, Robert, Boussioutas, Alex, Ardalan, Zaid, Al‐Ani, Aysha, Gibson, Peter R., and Christensen, Britt

Subjects

CROHN'S disease, HEALING, TREATMENT effectiveness, DISEASE remission

Abstract

Background and Aims: Transmural healing has emerged as a treatment target in Crohn's disease (CD). We investigated whether transmural healing assessed with intestinal ultrasound (IUS) is associated with improved clinical outcomes in patients with CD in clinical remission. Methods: Patients with CD in clinical remission at baseline (HBI <4) having IUS between August 2017 and June 2020 with at least 6‐months' follow‐up were retrospectively studied. Time to medication escalation, corticosteroid use and CD‐related hospitalisation or surgery were compared by the presence or absence of sonographic healing, defined as bowel wall thickness ≤3 mm without hyperemia on color Doppler, inflammatory fat, or disrupted bowel wall stratification. Factors associated with survival were analyzed by Kaplan–Meier analysis using Cox proportional‐hazard model. Results: Of 202 consecutive patients (50% male), sonographic inflammation was present in 61%. During median follow‐up of 19 (IQR 13–27) months, medication escalation occurred in 52%, corticosteroid use in 23%, hospitalisation in 21%, and CD‐related surgery in 13%. Sonographic healing was significantly associated with a reduced risk of medication escalation (p = 0.0018), corticosteroid use (p = 0.0247), hospitalisation (p = 0.0102), and surgery (p = 0.083). On multivariable analysis, sonographic healing was significantly associated with an increased odds of medication escalation‐free survival (hazard ratio [HR]:1.94; 95% CI 1.23–3.06; p = 0.004) and corticosteroid‐free survival (HR:2.41; 95% CI 1.24–4.67; p = 0.009), but not with hospitalisation or surgery. Conclusion: In patients with CD in clinical remission, sonographic healing is associated with improved clinical outcomes. Further studies are needed to determine whether sonographic healing should be a treatment target. [ABSTRACT FROM AUTHOR]

Published

2022

16. Cell graph neural networks enable the precise prediction of patient survival in gastric cancer.

Author

Wang, Yanan, Wang, Yu Guang, Hu, Changyuan, Li, Ming, Fan, Yanan, Otter, Nina, Sam, Ikuan, Gou, Hongquan, Hu, Yiqun, Kwok, Terry, Zalcberg, John, Boussioutas, Alex, Daly, Roger J., Montúfar, Guido, Liò, Pietro, Xu, Dakang, Webb, Geoffrey I., and Song, Jiangning

Subjects

OVERALL survival, STOMACH cancer, RECEIVER operating characteristic curves, TUMOR microenvironment, STATISTICAL significance

Abstract

Gastric cancer is one of the deadliest cancers worldwide. An accurate prognosis is essential for effective clinical assessment and treatment. Spatial patterns in the tumor microenvironment (TME) are conceptually indicative of the staging and progression of gastric cancer patients. Using spatial patterns of the TME by integrating and transforming the multiplexed immunohistochemistry (mIHC) images as Cell-Graphs, we propose a graph neural network-based approach, termed Cell−GraphSignatureorCGSignature, powered by artificial intelligence, for the digital staging of TME and precise prediction of patient survival in gastric cancer. In this study, patient survival prediction is formulated as either a binary (short-term and long-term) or ternary (short-term, medium-term, and long-term) classification task. Extensive benchmarking experiments demonstrate that the CGSignature achieves outstanding model performance, with Area Under the Receiver Operating Characteristic curve of 0.960 ± 0.01, and 0.771 ± 0.024 to 0.904 ± 0.012 for the binary- and ternary-classification, respectively. Moreover, Kaplan–Meier survival analysis indicates that the "digital grade" cancer staging produced by CGSignature provides a remarkable capability in discriminating both binary and ternary classes with statistical significance (P value < 0.0001), significantly outperforming the AJCC 8th edition Tumor Node Metastasis staging system. Using Cell-Graphs extracted from mIHC images, CGSignature improves the assessment of the link between the TME spatial patterns and patient prognosis. Our study suggests the feasibility and benefits of such an artificial intelligence-powered digital staging system in diagnostic pathology and precision oncology. [ABSTRACT FROM AUTHOR]

Published

2022

17. Mutant TP53 switches therapeutic vulnerability during gastric cancer progression within interleukin-6 family cytokines.

Author

Huber, Anne, Allam, Amr H., Dijkstra, Christine, Thiem, Stefan, Huynh, Jennifer, Poh, Ashleigh R., Konecnik, Joshua, Jacob, Saumya P., Busuttil, Rita, Liao, Yang, Chisanga, David, Shi, Wei, Alorro, Mariah G., Forrow, Stephen, Tauriello, Daniele V.F., Batlle, Eduard, Boussioutas, Alex, Williams, David S., Buchert, Michael, and Ernst, Matthias

Abstract

Although aberrant activation of the KRAS and PI3K pathway alongside TP53 mutations account for frequent aberrations in human gastric cancers, neither the sequence nor the individual contributions of these mutations have been clarified. Here, we establish an allelic series of mice to afford conditional expression in the glandular epithelium of Kras G12D ; Pik3ca H1047R or Trp53 R172H and/or ablation of Pten or Trp53. We find that Kras G12D ; Pik3ca H1047R is sufficient to induce adenomas and that lesions progress to carcinoma when also harboring Pten deletions. An additional challenge with either Trp53 loss- or gain-of-function alleles further accelerated tumor progression and triggered metastatic disease. While tumor-intrinsic STAT3 signaling in response to gp130 family cytokines remained as a gatekeeper for all stages of tumor development, metastatic progression required a mutant Trp53 -induced interleukin (IL)-11 to IL-6 dependency switch. Consistent with the poorer survival of patients with high IL-6 expression, we identify IL-6/STAT3 signaling as a therapeutic vulnerability for TP53-mutant gastric cancer. [Display omitted] • Mutant TP53 licenses progression to invasive stomach carcinoma with synchronous metastasis • Gain- and loss-of-function TP53 mutants advance gastric cancer upon loss of heterozygosity • Gastric cancer's STAT3 addiction switches from IL-11 to IL-6 dependency when being TP53 mutant Huber et al. demonstrate that gain-of-function and loss-of-expression TP53 mutations drive gastric disease progression to aggressive carcinomas with synchronous metastasis. While STAT3 signaling remains rate limiting throughout gastric cancer progression, its cytokine dependency switches from IL-11 to IL-6 in response to the TP53 mutations observed during the transition to carcinomas. [ABSTRACT FROM AUTHOR]

Published

2024

18. CD10 and Das1: a biomarker study using immunohistochemistry to subtype gastric intestinal metaplasia.

Author

Koulis, Athanasios, Di Costanzo, Natasha, Mitchell, Catherine, Lade, Stephen, Goode, David, Busuttil, Rita A., and Boussioutas, Alex

Abstract

Background: Intestinal metaplasia (IM) is considered a key pivot point in the Correa model of gastric cancer (GC). It is histologically subtyped into the complete and incomplete subtypes, the latter being associated with a greater risk of progression. However, the clinical utility of IM subtyping remains unclear, partially due to the absence of reliable defining biomarkers.Methods: Based on gene expression data and existing literature, we selected CD10 and Das1 as candidate biomarkers to distinguish complete and incomplete IM glands in tissues from patients without GC (IM-GC) and patients with GC (IM + GC). Immunohistochemical staining of individually subtyped IM glands was scored after blinding by two researchers using tissue belonging to both IM-GC and IM + GC patients. Whole tissue Das1 staining was further assessed using digital image quantification (cellSens Dimension, Olympus).Results: Across both cohorts CD10 stained the IM brush border and was shown to have a high sensitivity (87.5% and 94.9% in IM-GC and IM + GC patients respectively) and specificity (100.0% and 96.7% respectively) with an overall AUROC of 0.944 for complete IM glands. By contrast Das1 stained mainly goblet cells and the apical membrane of epithelial cells, mostly of incomplete IM glands with a low sensitivity (28.6% and 29.3% in IM-GC and IM + GC patients respectively) but high specificity (98.3% and 85.1% respectively) and an overall AUROC of 0.603 for incomplete IM glands. A combined logistic regression model showed a significant increase in AUROC for detecting complete IM glands (0.955 vs 0.970). Whole tissue digital quantification of Das1 staining showed a significant association with incomplete IM compared to complete IM, both in IM-GC and in IM + GC patients (p = 0.016 and p = 0.009 respectively, Mann-Whitney test and unpaired t test used). Additionally, complete IM in IM + GC patients exhibited significantly more Das1 staining than in IM-GC patients (p = 0.019, Mann-Whitney test).Conclusions: These findings suggest that CD10 is an outstanding biomarker for complete IM and Das1 may be useful as a secondary biomarker for IM glands at greater risk of progression irrespective of IM subtype. Overall, the clinical use of these biomarkers could lead to improved patient stratification and targeted surveillance. [ABSTRACT FROM AUTHOR]

Published

2022

19. Young people's experiences of a CDH1 pathogenic variant: Decision‐making about gastric cancer risk management.

Author

Hoskins, Cass, Tutty, Erin, Purvis, Rebecca, Shanahan, Mary, Boussioutas, Alex, and Forrest, Laura

Abstract

The most effective option for gastric cancer risk management in individuals with a CDH1 germline pathogenic or likely pathogenic variant (PV) in Australia is prophylactic total gastrectomy (PTG). There is, however, increasing confidence in endoscopic surveillance as a risk management strategy thus affording individuals with a CDH1 PV with challenging decisions regarding their gastric cancer risk management. For young people, this decision‐making comes at a complex development stage of emerging and young adulthood. This study aims to explore the factors that influence young people's decision‐making about their gastric cancer risk management due to a CDH1 PV. Potential participants were identified and approached through the Parkville Familial Cancer Centre in Melbourne, Australia. Thematic analysis was used to interpret and analyze the data. Qualitative interviews were conducted with 13 people with a CDH1 PV aged 18 to 39 years, inclusive. The interviews found that participants' familial and shared experiences of cancer and risk management, perceived tolerance of uncertainty, and desire for control over their cancer risk were fundamental in their decision‐making about their gastric cancer risk management. The participants' young adult life stage was also deemed particularly important in decisions about the timing of PTG. The findings of this study are vital to inform decisional counseling discussions with this unique population. [ABSTRACT FROM AUTHOR]

Published

2022

20. Diet and risk of gastro-oesophageal reflux disease in the Melbourne Collaborative Cohort Study.

Author

Wang, Sabrina E, Hodge, Allison M, Dashti, S Ghazaleh, Dixon-Suen, Suzanne C, Mitchell, Hazel, Thomas, Robert JS, Williamson, Elizabeth M, Makalic, Enes, Boussioutas, Alex, Haydon, Andrew M, Giles, Graham G, Milne, Roger L, Kendall, Bradley J, and English, Dallas R

Subjects

RESEARCH, ANIMAL experimentation, RESEARCH methodology, DIET, MEDICAL cooperation, EVALUATION research, GASTROESOPHAGEAL reflux, COMPARATIVE studies, FRUIT, QUESTIONNAIRES, LONGITUDINAL method

Abstract

Objective: To examine associations between diet and risk of developing gastro-oesophageal reflux disease (GERD).Design: Prospective cohort with a median follow-up of 15·8 years. Baseline diet was measured using a FFQ. GERD was defined as self-reported current or history of daily heartburn or acid regurgitation beginning at least 2 years after baseline. Sex-specific logistic regressions were performed to estimate OR for GERD associated with diet quality scores and intakes of nutrients, food groups and individual foods and beverages. The effect of substituting saturated fat for monounsaturated or polyunsaturated fat on GERD risk was examined.Setting: Melbourne, Australia.Participants: A cohort of 20 926 participants (62 % women) aged 40-59 years at recruitment between 1990 and 1994.Results: For men, total fat intake was associated with increased risk of GERD (OR 1·05 per 5 g/d; 95 % CI 1·01, 1·09; P = 0·016), whereas total carbohydrate (OR 0·89 per 30 g/d; 95 % CI 0·82, 0·98; P = 0·010) and starch intakes (OR 0·84 per 30 g/d; 95 % CI 0·75, 0·94; P = 0·005) were associated with reduced risk. Nutrients were not associated with risk for women. For both sexes, substituting saturated fat for polyunsaturated or monounsaturated fat did not change risk. For both sexes, fish, chicken, cruciferous vegetables and carbonated beverages were associated with increased risk, whereas total fruit and citrus were associated with reduced risk. No association was observed with diet quality scores.Conclusions: Diet is a possible risk factor for GERD, but food considered as triggers of GERD symptoms might not necessarily contribute to disease development. Potential differential associations for men and women warrant further investigation. [ABSTRACT FROM AUTHOR]

Published

2021

21. SFRP4 drives invasion in gastric cancer and is an early predictor of recurrence.

Author

Busuttil, Rita A., George, Joshy, House, Colin M., Lade, Stephen, Mitchell, Catherine, Di Costanzo, Natasha S., Pattison, Sharon, Huang, Yu-Kuan, Tan, Patrick, Cheong, Jae-Ho, Rha, Sun Young, and Boussioutas, Alex

Subjects

STOMACH cancer, CANCER relapse, DISEASE relapse, PROTEIN analysis, ONCOLOGIC surgery, REVERSE genetics

Abstract

Objective: Gastric cancer patients generally have a poor outcome, particularly those with advanced-stage disease which is defined by the increased invasion of cancer locally and is associated with higher metastatic potential. This study aimed to identify genes that were functional in the most fundamental hallmark of cancer, namely invasion. We then wanted to assess their value as biomarkers of gastric cancer progression and recurrence. Design: Data from a cohort of patients profiled on cDNA expression arrays was interrogated using K-means analysis. This genomic approach classified the data based on patterns of gene expression allowing the identification of the genes most correlated with the invasion of GC. We evaluated the functional role of a key protein from this analysis in invasion and as a biomarker of recurrence after curative resection. Results: Expression of secreted frizzled-related protein 4 (SFRP4) was identified as directly proportional to gastric cancer invasion. This finding was validated in multiple, independent datasets and its functional role in invasion was also confirmed using invasion assays. A change in serum levels of SFRP4 after curative resection, when coupled with AJCC stage, can accurately predict the risk of disease recurrence after curative therapy in an assay we termed PredictR. Conclusions: This simple ELISA-based assay can help predict recurrence of disease after curative gastric cancer surgery irrespective of adjuvant therapy. The results require further evaluation in a prospective trial but would help in the rational prescription of cancer therapies and surveillance to prevent under or over treatment of patients after curative resection. [ABSTRACT FROM AUTHOR]

Published

2021

22. A cohort study and meta-analysis of the evidence for consideration of Lauren subtype when prescribing adjuvant or palliative chemotherapy for gastric cancer.

Author

Wang, Kunning, Li, Enxiao, Busuttil, Rita A., Kong, Joseph C., Pattison, Sharon, Sung, Joseph J. Y., Yu, Jun, El-Omar, Emad M., Simpson, Julie A., and Boussioutas, Alex

Abstract

Background: The association between the survival or efficacy of chemotherapy and the Lauren subtype of gastric cancer (GC) remains unclear. We aimed to clarify whether patients with different Lauren subtypes have different survival after treatment with systemic chemotherapy: intestinal gastric cancer (IGC) patients survived better than patients with mixed type gastric cancer (MGC) or diffuse gastric cancer (DGC) after treatment with systemic chemotherapy. Patients & methods: Relevant studies for the meta-analysis were identified through searching Pubmed, Embase, Cochrane and Ovid up to March 2020. We also included our own prospectively collected cohort of patients that were followed over a 10-year period. Sub-group and sensitivity analyses were also performed. Results: In our prospective cohort, the overall survival (OS) of IGC patients receiving systemic chemotherapy (chemoIGC) [median OS 5.01 years, interquartile range (IQR) 2.63–6.71] was significantly higher than that of DGC patients receiving the same chemotherapy (chemoDGC) (median OS 1.33 years, IQR 0.78–3.33, p = 0.0001). After adjusting for age, gender and cancer stage, there was a significant difference in OS in patients treated with chemotherapy based on the Lauren classification of GC {hazard ratio (HR) for OS of the IGC versus DGC 0.33, [95% confidence interval (CI), 0.17–0.65; p < 0.001]}. In the IGC patients, the adjusted HR associated with chemotherapy was 0.26 (95% CI, 0.12–0.56; p = 0.001), whereas the association was 0.64 (95% CI, 0.30–1.33; p = 0.23) in the DGC patient group. In our meta-analysis, 33 studies comprising 10,246 patients treated with systemic chemotherapy (chemoIGC n = 4888, chemoDGC n = 5358) met all the selection criteria. While we accounted for much of the heterogeneity in these studies, we found that chemoIGC patients showed significantly improved OS [HR, 0.76 (95% CI, 0.71–0.82); p < 0.00001] when compared with similarly treated chemoDGC patients. Conclusion: Our results support the consideration of Lauren subtype when prescribing systemic chemotherapy for GC, particularly for MGC or DGC, which may not benefit from chemotherapy. Lauren classification should be considered to stratify chemotherapy regimens to GC patients in future clinical trials, with particular relevance to MGC or DGC, which is more difficult to treat with current regimens. [ABSTRACT FROM AUTHOR]

Published

2020

23. High‐dimensional analyses reveal a distinct role of T‐cell subsets in the immune microenvironment of gastric cancer.

Author

Wang, Minyu, Huang, Yu‐Kuan, Kong, Joseph CH, Sun, Yu, Tantalo, Daniela G, Yeang, Han Xian Aw, Ying, Le, Yan, Feng, Xu, Dakang, Halse, Heloise, Di Costanzo, Natasha, Gordon, Ian R, Mitchell, Catherine, Mackay, Laura K, Busuttil, Rita A, Neeson, Paul J, and Boussioutas, Alex

Subjects

STOMACH cancer, PROGRAMMED cell death 1 receptors, GENE expression profiling, T cells, CELL analysis, BLOOD cells

Abstract

Objectives: To facilitate disease prognosis and improve precise immunotherapy of gastric cancer (GC) patients, a comprehensive study integrating immune cellular and molecular analyses on tumor tissues and peripheral blood was performed. Methods: The association of GC patients' outcomes and the immune context of their tumors was explored using multiplex immunohistochemistry (mIHC) and transcriptome profiling. Potential immune dysfunction mechanism/s in the tumors on the systemic level was further examined using mass cytometry (CyTOF) in complementary peripheral blood from selected patients. GC cohorts with mIHC and gene expression profiling data were also used as validation cohorts. Results: Increased CD4+FOXP3+ T‐cell density in the GC tumor correlated with prolonged survival. Interestingly, CD4+FOXP3+ T cells had a close interaction with CD8+ T cells rather than tumor cells. High densities of CD4+FOXP3+ T cells and CD8+ T cells (High‐High) independently predicted prolonged patient survival. Furthermore, the interferon‐gamma (IFN‐γ) gene signature and PDL1 expression were up‐regulated in this group. Importantly, a subgroup of genomically stable (GS) tumors and tumors with chromosomal instability (CIN) within this High‐High group also had excellent survival. The High‐High GS/CIN tumors were coupled with increased frequencies of Tbet+CD4+ T cells and central memory CD4+ T cells in the peripheral blood. Conclusion: These novel findings identify the combination of CD8+ T cells and FOXP3+CD4+ T cells as a significant prognostic marker for GC patients, which also could potentially be targeted and applied in the combination therapy with immune checkpoint blockades in precision medicine. [ABSTRACT FROM AUTHOR]

Published

2020

24. The predicted impact and cost-effectiveness of systematic testing of people with incident colorectal cancer for Lynch syndrome.

Author

Kang, Yoon‐Jung, Killen, James, Caruana, Michael, Simms, Kate, Taylor, Natalie, Frayling, Ian M, Snowsill, Tristan, Huxley, Nicola, Coupe, Veerle MH, Hughes, Suzanne, Freeman, Victoria, Boussioutas, Alex, Trainer, Alison H, Ward, Robyn L, Mitchell, Gillian, Macrae, Finlay A, Canfell, Karen, and Kang, Yoon-Jung

Subjects

HEREDITARY nonpolyposis colorectal cancer, DNA mismatch repair, COLORECTAL cancer, COST effectiveness, GENETIC testing, DIAGNOSIS of hereditary nonpolyposis colorectal cancer, RESEARCH, COLONOSCOPY, IMMUNOHISTOCHEMISTRY, RESEARCH methodology, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, RESEARCH funding

Abstract

Objectives: To evaluate the health impact and cost-effectiveness of systematic testing for Lynch syndrome (LS) in people with incident colorectal cancer (CRC) in Australia.Design, Setting, Participants: We investigated the impact of LS testing strategies in a micro-simulation model (Policy1-Lynch), explicitly modelling the cost of testing all patients diagnosed with incident CRC during 2017, with detailed modelling of outcomes for patients identified as LS carriers (probands) and their at-risk relatives throughout their lifetimes. For people with confirmed LS, we modelled ongoing colonoscopic surveillance.Main Outcome Measures: Cost-effectiveness of six universal tumour testing strategies (testing for DNA mismatch repair deficiencies) and of universal germline gene panel testing of patients with incident CRC; impact on cost-effectiveness of restricting testing by age at CRC diagnosis (all ages, under 50/60/70 years) and of colonoscopic surveillance interval (one, two years).Results: The cost-effectiveness ratio of universal tumour testing strategies (annual colonoscopic surveillance, no testing age limit) compared with no testing ranged from $28 915 to $31 904/life-year saved (LYS) (indicative willingness-to-pay threshold: $30 000-$50 000/LYS). These strategies could avert 184-189 CRC deaths with an additional 30 597-31 084 colonoscopies over the lifetimes of 1000 patients with incident CRC with LS and 1420 confirmed LS carrier relatives (164-166 additional colonoscopies/death averted). The most cost-effective strategy was immunohistochemistry and BRAF V600E testing (incremental cost-effectiveness ratio [ICER], $28 915/LYS). Universal germline gene panel testing was not cost-effective compared with universal tumour testing strategies (ICER, $2.4 million/LYS). Immunohistochemistry and BRAF V600E testing was cost-effective at all age limits when paired with 2-yearly colonoscopic surveillance (ICER, $11 525-$32 153/LYS), and required 4778-15 860 additional colonoscopies to avert 46-181 CRC deaths (88-103 additional colonoscopies/death averted).Conclusions: Universal tumour testing strategies for guiding germline genetic testing of people with incident CRC for LS in Australia are likely to be cost-effective compared with no testing. Universal germline gene panel testing would not currently be cost-effective. [ABSTRACT FROM AUTHOR]

Published

2020

25. Dietary Intake of Nutrients Involved in One-Carbon Metabolism and Risk of Gastric Cancer: A Prospective Study.

Author

Dugué, Pierre-Antoine, Bassett, Julie K., Brinkman, Maree T., Southey, Melissa C., Joo, Jihoon E., Wong, Ee Ming, Milne, Roger L., English, Dallas R., Giles, Graham G., Boussioutas, Alex, Mitchell, Hazel, and Hodge, Allison M.

Subjects

STOMACH tumors, CARBON metabolism, AMINES, AMINO acids, CONFIDENCE intervals, DNA, GENE expression, HELICOBACTER diseases, INGESTION, LONGITUDINAL method, NUTRITIONAL requirements, QUESTIONNAIRES, VITAMIN B complex, LOGISTIC regression analysis, ODDS ratio, TUMOR risk factors

Abstract

Dietary intakes of B vitamins and other components involved in one-carbon metabolism, which is necessary for DNA replication, DNA repair, and regulation of gene expression, may be associated with carcinogenesis. We investigated associations between intakes of 11 nutrients (thiamine, riboflavin, niacin, pantothenic acid, vitamin B6, biotin, folate, vitamin B12, methionine, choline, and betaine) and gastric cancer risk. A total of 159 incident gastric cancer cases were identified from the Melbourne Collaborative Cohort Study (N = 41,513) and matched with 159 controls on year of birth, sex, and country of birth using incidence density sampling. Dietary intakes of nutrients were estimated at baseline (1990–1994) using a 121-item food frequency questionnaire. Odds ratios (ORs) and 95% confidence intervals were estimated using conditional logistic regression models adjusting for Helicobacter pylori infection, and other potential confounders. We observed a positive association between intake of niacin and overall gastric cancer risk (OR = 1.33, 95%CI: 1.01–1.75 per SD increment). For thiamine, heterogeneity by subtype (cardia and non-cardia) was found (Phet = 0.05), with weak evidence of an inverse association with cardia cancer risk. Our results do not support increasing intakes of B vitamins or other nutrients involved in one-carbon metabolism to reduce gastric cancer risk in a well-nourished population. [ABSTRACT FROM AUTHOR]

Published

2019

26. Current mismatch repair deficiency tumor testing practices and capabilities: A survey of Australian pathology providers.

Author

Mascarenhas, Lyon, Shanley, Susan, Mitchell, Gillian, Spurdle, Amanda B., Macrae, Finlay, Pachter, Nicholas, Buchanan, Daniel D., Ward, Robyn L., Fox, Stephen, Duxbury, Elaine, Driessen, Rebecca, and Boussioutas, Alex

Subjects

HEREDITARY nonpolyposis colorectal cancer, COLON cancer, CANCER cells, CANCER chemotherapy, BRAF genes

Abstract

Aim & Methods: An electronic survey of the Royal College of Pathologists of Australasia accredited pathology services was conducted to assess Lynch syndrome tumor screening practices and to identify barriers and capabilities to screen newly diagnosed colorectal and endometrial tumors in Australia. Results: Australia lacks a national policy for universal mismatch repair‐deficient (dMMR) testing of incident colorectal and endometrial tumors cases. Routine Lynch syndrome tumor screening program for colorectal and/or endometrial tumors was applied by 95% (37/39) of laboratories. Tumor dMMR screening methods varied; MMR protein immunohistochemistry (IHC) alone was undertaken by 77% of 39 laboratories, 18% performed both IHC and microsatellite instability testing, 5% did not have the capacity to perform in‐house testing. For colorectal tumors, 47% (17/36) reported following a universal approach without age limit, 30% (11/36) tested only "red flag" cases; 6% (3/36) on clinician request only. For endometrial tumors, 37% (12/33) reported clinician request generated testing, 27% (9/33) were screening only "red flag" cases, and 12% (4/33) carried out universal screening without an age criteria. BRAF V600E mutation testing of colorectal tumors demonstrating aberrant MLH1 protein expression by IHC was the most common secondary tumor test, with 53% of laboratories performing the test; 15% of laboratories also applied the BRAF V600E test to endometrial tumors with aberrant MLH1 expression despite no evidence for its utility. Tumor testing for MLH1 promoter methylation was performed by less than 15% laboratories. Conclusion: Although use of tumor screening for evidence of dMMR is widely available, protocols for its use in Australia vary widely. This national survey provides a snapshot of the current availability and practice of tumor dMMR screening and identifies the need for a uniform national testing policy. [ABSTRACT FROM AUTHOR]

Published

2018

27. Revised Australian national guidelines for colorectal cancer screening: family history.

Author

Jenkins, Mark A., Ouakrim, Driss Ait, Boussioutas, Alex, Hopper, John L., Ee, Hooi C., Emery, Jon D., Macrae, Finlay A., Chetcuti, Albert, Wuellner, Laura, John, D. James B. St., Ait Ouakrim, Driss, and St John, D James B

Subjects

COLON cancer, EARLY detection of cancer, FECAL occult blood tests

Abstract

Introduction: Screening is an effective means for colorectal cancer prevention and early detection. Family history is strongly associated with colorectal cancer risk. We describe the rationale, evidence and recommendations for colorectal cancer screening by family history for people without a genetic syndrome, as reported in the 2017 revised Australian guidelines. Main recommendations: Based on 10-year risks of colorectal cancer, people at near average risk due to no or weak family history (category 1) are recommended screening by immunochemical faecal occult blood test (iFOBT) every 2 years from age 50 to 74 years. Individuals with moderate risk due to their family history (category 2) are recommended biennial iFOBT from age 40 to 49 years, then colonoscopy every 5 years from age 50 to 74 years. People with a high risk due to their family history (category 3) are recommended biennial iFOBT from age 35 to 44 years, then colonoscopy every 5 years from age 45 to 74 years. Changes in management as a result of the guidelines: By 2019, the National Bowel Cancer Screening Program will offer all Australians free biennial iFOBT screening from age 50 to 74 years, consistent with the recommendations in these guidelines for category 1. Compared with the 2005 guidelines, there are some minor changes in the family history inclusion criteria for categories 1 and 2; the genetic syndromes have been removed from category 3 and, as a consequence, colonoscopy screening is now every 5 years; and for categories 2 and 3, screening begins with iFOBT for people aged 40 and 35 years, respectively, before transitioning to colonoscopy after 10 years. [ABSTRACT FROM AUTHOR]

Published

2018

28. Family history-based colorectal cancer screening in Australia: A modelling study of the costs, benefits, and harms of different participation scenarios.

Author

Dillon, Mary, Flander, Louisa, Buchanan, Daniel D., Macrae, Finlay A., Emery, Jon D., Winship, Ingrid M., Boussioutas, Alex, Giles, Graham G., Hopper, John L., Jenkins, Mark A., and Ait Ouakrim, Driss

Subjects

COLON cancer, EARLY detection of cancer, FAMILY history (Medicine), FECAL occult blood tests, PATIENT compliance, QUALITY of life, COST effectiveness, MICROSIMULATION modeling (Statistics)

Abstract

Background: The Australian National Bowel Cancer Screening Programme (NBCSP) was introduced in 2006. When fully implemented, the programme will invite people aged 50 to 74 to complete an immunochemical faecal occult blood test (iFOBT) every 2 years.Methods and Findings: To investigate colorectal cancer (CRC) screening occurring outside of the NBCSP, we classified participants (n = 2,480) in the Australasian Colorectal Cancer Family Registry (ACCFR) into 3 risk categories (average, moderately increased, and potentially high) based on CRC family history and assessed their screening practices according to national guidelines. We developed a microsimulation to compare hypothetical screening scenarios (70% and 100% uptake) to current participation levels (baseline) and evaluated clinical outcomes and cost for each risk category. The 2 main limitations of this study are as follows: first, the fact that our cost-effectiveness analysis was performed from a third-party payer perspective, which does not include indirect costs and results in overestimated cost-effectiveness ratios, and second, that our natural history model of CRC does not include polyp sojourn time, which determines the rate of cancerous transformation. Screening uptake was low across all family history risk categories (64%-56% reported no screening). For participants at average risk, 18% reported overscreening, while 37% of those in the highest risk categories screened according to guidelines. Higher screening levels would substantially reduce CRC mortality across all risk categories (95 to 305 fewer deaths per 100,000 persons in the 70% scenario versus baseline). For those at average risk, a fully implemented NBCSP represented the most cost-effective approach to prevent CRC deaths (AUS$13,000-16,000 per quality-adjusted life year [QALY]). For those at moderately increased risk, higher adherence to recommended screening was also highly cost-effective (AUS$19,000-24,000 per QALY).Conclusion: Investing in public health strategies to increase adherence to appropriate CRC screening will save lives and deliver high value for money. [ABSTRACT FROM AUTHOR]

Published

2018

29. ' Why don't I need a colonoscopy?': A novel approach to communicating risks and benefits of colorectal cancer screening.

Author

Emery, Jon D., Pirotta, Marie, Macrae, Finlay, Walker, Jennifer G., Qama, Ashleigh, Boussioutas, Alex, and Jenkins, Mark

Subjects

COLONOSCOPY, COLON cancer, EARLY detection of cancer, RISK communication, FECAL occult blood tests

Abstract

Background and objectives There is significant growth in demand for colonoscopies, with over 700,000 performed in Australia in 2012-13. For every one million Australians aged 50 years and older, 80,000 people at average risk of colorectal cancer are being over-screened with colonoscopy, and 29,000 people at increased risk are not having the colonoscopy they need. Methods Using monitoring data from the Australian National Bowel Cancer Screening Program and published data on colonoscopic screening, we have developed expected frequency trees (EFTs) to demonstrate projected outcomes of different colorectal cancer screening options for participants at different levels of colorectal cancer risk in Australia. Results The EFTs highlight the overall balance in favour of faecal occult blood screening for those at average risk in terms of fewer deaths and complications. Discussion This novel method of risk communication can be used to promote appropriate patient choice of colorectal cancer screening modality and potentially reduce the number of referrals for colonoscopy in patients who are not at increased risk of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2018

30. Down-regulation of a pro-apoptotic pathway regulated by PCAF/ADA3 in early stage gastric cancer.

Author

Brasacchio, Daniella, Busuttil, Rita A., Noori, Tahereh, Johnstone, Ricky W., Boussioutas, Alex, and Trapani, Joseph A.

Published

2018

31. The conundrum of quality in colonoscopy.

Author

Chittleborough, Timothy J., Luck, Andrew, Boussioutas, Alex, Warrier, Satish, and Heriot, Alexander G.

Subjects

COLONOSCOPY, HEALTH outcome assessment, COLON examination, COLON cancer, MEDICAL practice

Abstract

The article presents author's views on improvement in standard surgical practice and quality of care for improved in patient outcomes. Topics discussed include adenoma detection rate (ADR) and caecal intubation rate; bowel cancer screening programme in Great Britain and quality of colonoscopy; and Cancer Council Australia (CCA).

Published

2018

32. Early relapses after adjuvant chemotherapy suggests primary chemoresistance in diffuse gastric cancer.

Author

Pattison, Sharon, Mitchell, Catherine, Lade, Stephen, Leong, Trevor, Busuttil, Rita A., and Boussioutas, Alex

Subjects

PHYSIOLOGICAL effects of chemotherapy, CHEMICAL resistance, GASTROINTESTINAL cancer treatment, FLUOROPYRIMIDINES, ADJUVANT treatment of cancer, THERAPEUTICS

Abstract

Background: Survival from gastric cancer remains poor, particularly in Western populations. Previous pre-clinical and subgroup analyses of clinical trials have suggested differing benefits from fluoropyrimidine-based chemotherapeutics for diffuse and intestinal gastric cancer. This analysis examines patterns of relapse with and without adjuvant chemotherapy after curative resection for gastric cancer in these subtypes to explore the Lauren classification as a predictive marker of benefit for fluoropyrimidine-based adjuvant chemotherapy. Patients and methods: Gastric cancer patients enrolled in an ongoing tissue banking study were analysed, 164 patients who would currently be considered for adjuvant therapy after curative resection were included in the analysis. Patients who did and did not receive adjuvant chemotherapy were compared. The primary end point was relapse free survival. Results: Approximately 50% of patients received adjuvant chemotherapy, the majority receiving a fluoropyrimidine-based regimen. The comparison of Kaplan-Meier curves for patients who did and did not receive adjuvant chemotherapy are different between patients with intestinal and diffuse gastric cancer, and suggest that there may be a benefit in intestinal gastric cancer. The hazard ratio for adjuvant chemotherapy for intestinal gastric cancer was 0.56, (95% CI 0.27–1.17), suggesting a trend towards benefit that was lacking in diffuse gastric cancer patients (1.26, 95% CI 0.70–2.38). The patterns of relapse after adjuvant chemotherapy also differed between diffuse and intestinal gastric cancer. More than 50% of diffuse gastric cancer patients who received adjuvant chemotherapy relapsed within 12 months of surgery despite similar surgical parameters. Conclusions: Lauren classification is prognostic in gastric cancer. This analysis adds further evidence that it may also be predictive of benefit for fluoropyrimidine-based chemotherapeutics, with lower chemosensitivity seen in diffuse gastric cancer. Treating diffuse and intestinal gastric cancer as separate entities, with identification of efficacious treatments for diffuse gastric cancer will help in improving outcomes from gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2017

33. TOPGEAR: A Randomized, Phase III Trial of Perioperative ECF Chemotherapy with or Without Preoperative Chemoradiation for Resectable Gastric Cancer: Interim Results from an International, Intergroup Trial of the AGITG, TROG, EORTC and CCTG.

Author

Leong, Trevor, Smithers, B., Haustermans, Karin, Michael, Michael, Gebski, Val, Miller, Danielle, Zalcberg, John, Boussioutas, Alex, Findlay, Michael, O'Connell, Rachel, Verghis, Jaclyn, Willis, David, Kron, Tomas, Crain, Melissa, Murray, William, Lordick, Florian, Swallow, Carol, Darling, Gail, Simes, John, and Wong, Rebecca

Abstract

Background: Postoperative chemoradiation and perioperative chemotherapy using epirubicin/cisplatin/5-fluorouracil (ECF) represent two standards of care for resectable gastric cancer. In the TOPGEAR (Trial Of Preoperative therapy for Gastric and Esophagogastric junction AdenocaRcinoma) trial, we hypothesized that adding preoperative chemoradiation to perioperative ECF will improve survival; however, the safety and feasibility of preoperative chemoradiation have yet to be determined. Methods: TOPGEAR is an international phase III trial in which patients with adenocarcinoma of the stomach were randomized to perioperative ECF alone or with preoperative chemoradiation. The ECF-alone group received three preoperative cycles of ECF, while the chemoradiation group received two cycles of preoperative ECF followed by chemoradiation. Both groups received three postoperative cycles of ECF. A planned interim analysis of the first 120 patients was conducted, and was reviewed by the Independent Data Safety Monitoring Committee to assess treatment compliance, toxicity/safety, and response rates. Results: The proportion of patients who received all cycles of preoperative chemotherapy was 93% (ECF group) and 98% (chemoradiation group), while 65 and 53%, respectively, received all cycles of postoperative chemotherapy. Overall, 92% of patients allocated to preoperative chemoradiation received this treatment. The proportion of patients proceeding to surgery was 90% (ECF group) and 85% (chemoradiation group). Grade 3 or higher surgical complications occurred in 22% of patients in both groups. Furthermore, grade 3 or higher gastrointestinal toxicity occurred in 32% (ECF group) and 30% (chemoradiation group) of patients, while hematologic toxicity occurred in 50 and 52% of patients. Conclusions: These results demonstrate that preoperative chemoradiation can be safely delivered to the vast majority of patients without a significant increase in treatment toxicity or surgical morbidity. [ABSTRACT FROM AUTHOR]

Published

2017

34. Tumor testing to identify lynch syndrome in two Australian colorectal cancer cohorts.

Author

Buchanan, Daniel D, Clendenning, Mark, Rosty, Christophe, Eriksen, Stine V, Walsh, Michael D, Walters, Rhiannon J, Thibodeau, Stephen N, Stewart, Jenna, Preston, Susan, Win, Aung Ko, Flander, Louisa, Ait Ouakrim, Driss, Macrae, Finlay A, Boussioutas, Alex, Winship, Ingrid M, Giles, Graham G, Hopper, John L, Southey, Melissa C, English, Dallas, and Jenkins, Mark A

Subjects

HEREDITARY nonpolyposis colorectal cancer, COLON cancer, GENETIC disorders, LYNCH syndrome II, IMMUNOHISTOCHEMISTRY, MICROSATELLITE repeats

Abstract

Background and Aim Tumor testing of colorectal cancers (CRC) for mismatch repair (MMR) deficiency is an effective approach to identify carriers of germline MMR gene mutation (Lynch syndrome). The aim of this study was to identify MMR gene mutation carriers in two cohorts of population-based CRC utilizing a combination of tumor and germline testing approaches. Methods Colorectal cancers from 813 patients diagnosed with CRC < 60 years of age from the Australasian Colorectal Cancer Family Registry (ACCFR) and from 826 patients from the Melbourne Collaborative Cohort Study (MCCS) were tested for MMR protein expression using immunohistochemistry, microsatellite instability (MSI), BRAFV600E somatic mutation, and for MLH1 methylation. MMR gene mutation testing (Sanger sequencing and Multiplex Ligation Dependent Probe Amplification) was performed on germline DNA of patients with MMR-deficient tumors and a subset of MMR-proficient CRCs. Results Of the 813 ACCFR probands, 90 probands demonstrated tumor MMR deficiency (11.1%), and 42 had a MMR gene germline mutation (5.2%). For the MCCS, MMR deficiency was identified in the tumors of 103 probands (12.5%) and seven had a germline mutation (0.8%). All the mutation carriers were diagnosed prior to 70 years of age. Probands with a MMR-deficient CRC without MLH1 methylation and a gene mutation were considered Lynch-like and comprised 41.1% and 25.2% of the MMR-deficient CRCs for the ACCFR and MCCS, respectively. Conclusions Identification of MMR gene mutation carriers in Australian CRC-affected patients is optimized by immunohistochemistry screening of CRC diagnosed before 70 years of age. A significant proportion of MMR-deficient CRCs will have unknown etiology (Lynch-like) proving problematic for clinical management. [ABSTRACT FROM AUTHOR]

Published

2017

35. Pathophysiology of Hereditary Diffuse Gastric Cancer.

Author

Pattison, Sharon and Boussioutas, Alex

Published

2015

36. Risk factors for metachronous colorectal cancer following a primary colorectal cancer: A prospective cohort study.

Author

Jayasekara, Harindra, Reece, Jeanette C., Buchanan, Daniel D., Rosty, Christophe, Dashti, S. Ghazaleh, Ait Ouakrim, Driss, Winship, Ingrid M., Macrae, Finlay A., Boussioutas, Alex, Giles, Graham G., Ahnen, Dennis J., Lowery, Jan, Casey, Graham, Haile, Robert W., Gallinger, Steven, Le Marchand, Loic, Newcomb, Polly A., Lindor, Noralane M., Hopper, John L., and Parry, Susan

Abstract

Individuals diagnosed with colorectal cancer (CRC) are at risk of developing a metachronous CRC. We examined the associations between personal, tumour-related and lifestyle risk factors, and risk of metachronous CRC. A total of 7,863 participants with incident colon or rectal cancer who were recruited in the USA, Canada and Australia to the Colon Cancer Family Registry during 1997-2012, except those identified as high-risk, for example, Lynch syndrome, were followed up approximately every 5 years. We estimated the risk of metachronous CRC, defined as the first new primary CRC following an interval of at least one year after the initial CRC diagnosis. Observation time started at the age at diagnosis of the initial CRC and ended at the age at diagnosis of the metachronous CRC, last contact or death whichever occurred earliest, or were censored at the age at diagnosis of any metachronous colorectal adenoma. Cox regression was used to derive hazard ratios (HRs) and 95% confidence intervals (CIs). During a mean follow-up of 6.6 years, 142 (1.81%) metachronous CRCs were diagnosed (mean age at diagnosis 59.8; incidence 2.7/1,000 person-years). An increased risk of metachronous CRC was associated with the presence of a synchronous CRC (HR = 2.73; 95% CI: 1.30-5.72) and the location of cancer in the proximal colon at initial diagnosis (compared with distal colon or rectum, HR = 4.16; 95% CI: 2.80-6.18). The presence of a synchronous CRC and the location of the initial CRC might be useful for deciding the intensity of surveillance colonoscopy for individuals diagnosed with CRC. [ABSTRACT FROM AUTHOR]

Published

2016

37. Predictors of outcome after surgery for gastric cancer in a Western cohort.

Author

Pattison, Sharon, Mann, G. Bruce, Crosthwaite, Gary, Lade, Stephen, Mitchell, Catherine, Leong, Trevor, Busuttil, Rita A., and Boussioutas, Alex

Subjects

SURGERY, CANCER, MEDICINE, DISEASES, HEALTH facilities

Abstract

Background Gastric cancer ( GC) is a common cause of cancer mortality. There are well-documented prognostic factors for GC but these have not been rigorously examined in an Australian context. This study examines the clinical, surgical and histopathological variables associated with survival in a GC cohort from a predominantly Caucasian-based population. Methods A multi-centre cohort of patients undergoing curative resection for GC enrolled in an ongoing tissue bank study from 1999 to 2009 was retrospectively analysed. Prospectively collected demographic, surgical and pathological variables were available for this cohort. The primary endpoints investigated were cancer-specific survival and recurrence-free survival using multivariate Cox proportional hazard modelling. Results Five-year cancer-specific survival was 45.9%, 5-year relapse-free survival was 44.7% and 30-day mortality was 2.2%. Variables showing significance on multivariate analysis for cancer-specific and relapse-free survival were AJCC stage, Lauren classification and age at surgery. Conclusion This study demonstrates that the prognostic variables for a predominantly Caucasian GC population are congruent with published prognostic features. These findings emphasize the importance of the pathological review in allocating prognosis in GC. [ABSTRACT FROM AUTHOR]

Published

2016

38. Multivitamin, calcium and folic acid supplements and the risk of colorectal cancer in Lynch syndrome.

Author

Chau, Rowena, Ghazaleh, Seyedeh, Dashti, Ouakrim, Driss Ait, Buchanan, Daniel D., Clendenning, Mark, Rosty, Christophe, Winship, Ingrid M., Young, Joanne P., Giles, Graham G., Macrae, Finlay A., Boussioutas, Alex, Parry, Susan, Figueiredo, Jane C., Levine, A. Joan, Ahnen, Dennis J., Casey, Graham, Haile, Robert W., Gallinger, Steven, and Marchand, Loïc Le

Subjects

CANCER risk factors, HEREDITARY nonpolyposis colorectal cancer, FOLIC acid in human nutrition, CALCIUM supplements, DNA repair, GENETIC mutation, CALCIUM, DIETARY supplements, DNA, FOLIC acid, RESEARCH funding, VITAMINS, ACQUISITION of data, PROPORTIONAL hazards models, GENETIC carriers

Abstract

Background: People with a DNA mismatch repair (MMR) gene mutation have a substantially elevated risk of colorectal cancer (CRC) but the modifiers of this risk are not well established. We investigated the association between dietary supplement intake and CRC risk for carriers.Methods: This study included 1966 (56% female) carriers of an MMR gene mutation (719 MLH1, 931 MSH2, 211 MSH6 and 105 PMS2) who were recruited from the USA, Canada, Australia and New Zealand into the Colon Cancer Family Registry between 1997 and 2012. Information on lifestyle factors including supplement intake was collected at the time of recruitment. Using Cox proportional hazards regression weighted to correct for ascertainment bias, we estimated hazard ratios (HRs) and 95% confidence intervals (CIs) for associations between self-reported multivitamin, calcium and folic acid supplement intake and CRC risk.Results: Of 744 carriers with CRC, 18%, 6% and 5% reported intake of multivitamin, calcium and folic acid supplements for at least 1 month, respectively, compared with 27%, 11% and 10% of 1222 carriers without CRC. After adjusting for identified confounding variables, a decreased CRC risk was associated with multivitam inintake for at least 3 years (HR 0.47, 95% CI 0.32-0.69) and calcium intake for at least 3 years(HR 0.42, 95% CI 0.23-0.74), compared with never users. There was no evidence of an association between folic acid supplement intake and CRC risk (P = 0.82).Conclusion: Intake of multivitamin and calcium supplements might be associated with a decreased risk of CRC for MMR gene mutation carriers. [ABSTRACT FROM AUTHOR]

Published

2016

39. Germline mutations in PMS2 and MLH1 in individuals with solitary loss of PMS2 expression in colorectal carcinomas from the Colon Cancer Family Registry Cohort.

Author

Rosty, Christophe, Clendenning, Mark, Walsh, Michael D., Eriksen, Stine V., Southey, Melissa C., Winship, Ingrid M., Macrae, Finlay A., Boussioutas, Alex, Poplawski, Nicola K., Parry, Susan, Arnold, Julie, Young, Joanne P., Casey, Graham, Haile, Robert W., Gallinger, Steven, Le Marchand, Loïc, Newcomb, Polly A., Potter, John D., DeRycke, Melissa, and Lindor, Noralane M.

Abstract

Objectives: Immunohistochemistry for DNA mismatch repair proteins is used to screen for Lynch syndrome in individuals with colorectal carcinoma (CRC). Although solitary loss of PMS2 expression is indicative of carrying a germline mutation in PMS2, previous studies reported MLH1 mutation in some cases. We determined the prevalence of MLH1 germline mutations in a large cohort of individuals with a CRC demonstrating solitary loss of PMS2 expression. Design: This cohort study included 88 individuals affected with a PMS2-deficient CRC from the Colon Cancer Family Registry Cohort. Germline PMS2 mutation analysis (long-range PCR and multiplex ligation-dependent probe amplification) was followed by MLH1 mutation testing (Sanger sequencing and multiplex ligation-dependent probe amplification). Results: Of the 66 individuals with complete mutation screening, we identified a pathogenic PMS2 mutation in 49 (74%), a pathogenic MLH1 mutation in 8 (12%) and a MLH1 variant of uncertain clinical significance predicted to be damaging by in silico analysis in 3 (4%); 6 (9%) carried variants likely to have no clinical significance. Missense point mutations accounted for most alterations (83%; 9/11) in MLH1. The MLH1 c.113A> G p.Asn38Ser mutation was found in 2 related individuals. One individual who carried the MLH1 intronic mutation c.677+3A>G p.Gln197Argfs*8 leading to the skipping of exon 8, developed 2 tumours, both of which retained MLH1 expression. Conclusions: A substantial proportion of CRCs with solitary loss of PMS2 expression are associated with a deleterious MLH1 germline mutation supporting the screening for MLH1 in individuals with tumours of this immunophenotype, when no PMS2 mutation has been identified. [ABSTRACT FROM AUTHOR]

Published

2016

40. Signatures of tumour immunity distinguish Asian and non-Asian gastric adenocarcinomas.

Author

Lin, Suling J., Gagnon-Bartsch, Johann A., Tan, Iain Beehuat, Earle, Sophie, Ruff, Louise, Pettinger, Katherine, Ylstra, Bauke, van Grieken, Nicole, Sun Young Rha, Hyun Cheol Chung, Ju-Seog Lee, Jae Ho Cheong, Sung Hoon Noh, Toru Aoyama, Yohei Miyagi, Akira Tsuburaya, Takaki Yoshikawa, Ajani, Jaffer A., Boussioutas, Alex, and Khay Guan Yeoh

Subjects

TUMOR immunology, GENE expression, HEALTH outcome assessment, CLINICAL trials, IMMUNOHISTOCHEMISTRY

Abstract

Objective: Differences in gastric cancer (GC) clinical outcomes between patients in Asian and non-Asian countries has been historically attributed to variability in clinical management. However, recent international Phase III trials suggest that even with standardised treatments, GC outcomes differ by geography. Here, we investigated gene expression differences between Asian and non-Asian GCs, and if these molecular differences might influence clinical outcome. Design: We compared gene expression profiles of 1016 GCs from six Asian and three non-Asian GC cohorts, using a two-stage meta-analysis design and a novel biostatistical method (RUV-4) to adjust for technical variation between cohorts. We further validated our findings by computerised immunohistochemical analysis on two independent tissue microarray (TMA) cohorts from Asian and non-Asian localities (n=665). Results: Gene signatures differentially expressed between Asians and non-Asian GCs were related to immune function and inflammation. Non-Asian GCs were significantly enriched in signatures related to T-cell biology, including CTLA-4 signalling. Similarly, in the TMA cohorts, non-Asian GCs showed significantly higher expression of T-cell markers (CD3, CD45R0, CD8) and lower expression of the immunosuppressive T-regulatory cell marker FOXP3 compared to Asian GCs (p<0.05). Inflammatory cell markers CD66b and CD68 also exhibited significant cohort differences (p<0.05). Exploratory analyses revealed a significant relationship between tumour immunity factors, geographic localityspecific prognosis, and postchemotherapy outcomes. Conclusions: Analyses of >1600 GCs suggest that Asian and non-Asian GCs exhibit distinct tumour immunity signatures related to T-cell function. These differences may influence geographical differences in clinical outcome, and the design of future trials particularly in immuno-oncology. [ABSTRACT FROM AUTHOR]

Published

2015

41. TOPGEAR: a randomised phase III trial of perioperative ECF chemotherapy versus preoperative chemoradiation plus perioperative ECF chemotherapy for resectable gastric cancer (an international, intergroup trial of the AGITG/ TROG/EORTC/NCIC CTG).

Author

Leong, Trevor, Smithers, B. Mark, Michael, Michael, Gebski, Val, Boussioutas, Alex, Miller, Danielle, Simes, John, Zalcberg, John, Haustermans, Karin, Lordick, Florian, Schuhmacher, Christoph, Swallow, Carol, Darling, Gail, and Wong, Rebecca

Subjects

RANDOMIZED controlled trials, PERIOPERATIVE care, CANCER chemotherapy, CANCER radiotherapy, STOMACH cancer treatment, STOMACH cancer patients

Abstract

Background: The optimal management of patients with resectable gastric cancer continues to evolve in Western countries. Following publication of the US Intergroup 0116 and UK Medical Research Council MAGIC trials, there are now two standards of care for adjuvant therapy in resectable gastric cancer, at least in the Western world: postoperative chemoradiotherapy and perioperative epirubicin/cisplatin/fluorouracil (ECF) chemotherapy. We hypothesize that adding chemoradiation to standard perioperative ECF chemotherapy will achieve further survival gains. We also believe there are advantages to administering chemoradiation in the preoperative rather than postoperative setting. In this article, we describe the TOPGEAR trial, which is a randomised phase III trial comparing control arm therapy of perioperative ECF chemotherapy with experimental arm therapy of preoperative chemoradiation plus perioperative ECF chemotherapy. Methods/Design: Eligible patients with resectable adenocarcinoma of the stomach or gastroesophageal junction will be randomized to receive either perioperative chemotherapy alone (3 preoperative and 3 postoperative cycles of ECF) or perioperative chemotherapy plus preoperative chemoradiation. In the chemoradiation arm, patients receive 2 cycles of ECF plus chemoradiation prior to surgery, and then following surgery 3 further cycles of ECF are given. The trial is being conducted in two Parts; Part 1 (phase II component) has recruited 120 patients with the aim of assessing feasibility, safety and preliminary efficacy of preoperative chemoradiation. Part 2 (phase III component) will recruit a further 632 patients to provide a total sample size of 752 patients. The primary endpoint of the phase III trial is overall survival. The trial includes quality of life and biological substudies, as well as a health economic evaluation. In addition, the trial incorporates a rigorous quality assurance program that includes real time central review of radiotherapy plans and central review of surgical technique. Discussion: TOPGEAR is an international, intergroup collaboration led by the Australasian Gastro-Intestinal Trials Group (AGITG), in collaboration with the Trans-Tasman Radiation Oncology Group (TROG), European Organisation for Research and Treatment of Cancer (EORTC) and the NCIC Clinical Trials Group. It addresses a globally significant question that will help inform future international standards for clinical practice in resectable gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2015

42. Lamina propria macrophage phenotypes in relation to Escherichia coli in Crohn's disease.

Author

Elliott, Timothy R., Rayment, Neil B., Hudspith, Barry N., Hands, Rebecca E., Taylor, Kirstin, Parkes, Gareth C., Prescott, Natalie J., Petrovska, Liljana, Hermon-Taylor, John, Brostoff, Jonathan, Boussioutas, Alex, Mathew, Christopher G., Bustin, Stephen A., and Sanderson, Jeremy D.

Subjects

CROHN'S disease, MACROPHAGES, ESCHERICHIA coli, PHENOTYPES, ULCERATIVE colitis, INFLAMMATORY bowel disease treatment, PATIENTS, DISEASES

Abstract

Background: Abnormal handling of E. coli by lamina propria (LP) macrophages may contribute to Crohn's disease (CD) pathogenesis. We aimed to determine LP macrophage phenotypes in CD, ulcerative colitis (UC) and healthy controls (HC), and in CD, to compare macrophage phenotypes according to E. coli carriage. Methods: Mucosal biopsies were taken from 35 patients with CD, 9 with UC and 18 HCs. Laser capture microdissection was used to isolate E. coli-laden and unladen LP macrophages from ileal or colonic biopsies. From these macrophages, mRNA was extracted and cytokine and activation marker expression measured using RT-qPCR. Results: E. coli-laden LP macrophages were identified commonly in mucosal biopsies from CD patients (25/35, 71 %), rarely in UC (1/9, 11 %) and not at all in healthy controls (0/18). LP macrophage cytokine mRNA expression was greater in CD and UC than healthy controls. In CD, E. coli-laden macrophages expressed high IL-10 & CD163 and lower TNFα, IL-23 & iNOS irrespective of macroscopic inflammation. In inflamed tissue, E. coli-unladen macrophages expressed high TNFα, IL-23 & iNOS and lower IL-10 & CD163. In uninflamed tissue, unladen macrophages had low cytokine mRNA expression, closer to that of healthy controls. Conclusion: In CD, intra-macrophage E. coli are commonly found and LP macrophages express characteristic cytokine mRNA profiles according to E. coli carriage. Persistence of E. coli within LP macrophages may provide a stimulus for chronic inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

43. Hereditary diffuse gastric cancer: updated clinical guidelines with an emphasis on germline CDH1 mutation carriers.

Author

van der Post, Rachel S., Vogelaar, Ingrid P., Carneiro, Fátima, Guilford, Parry, Huntsman, David, Hoogerbrugge, Nicoline, Caldas, Carlos, Chelcun Schreiber, Karen E., Hardwick, Richard H., Ausems, Margreet G. E. M., Bardram, Linda, Benusiglio, Patrick R., Bisseling, Tanya M., Blair, Vanessa, Bleiker, Eveline, Boussioutas, Alex, Cats, Annemieke, Coit, Daniel, DeGregorio, Lynn, and Figueiredo, Joana

Subjects

GERM cells, GENETIC mutation, BREAST cancer, GASTRECTOMY, GENETIC testing

Abstract

Germline CDH1 mutations confer a high lifetime risk of developing diffuse gastric (DGC) and lobular breast cancer (LBC). A multidisciplinary workshop was organised to discuss genetic testing, surgery, surveillance strategies, pathology reporting and the patient's perspective on multiple aspects, including diet post gastrectomy. The updated guidelines include revised CDH1 testing criteria (taking into account first-degree and second-degree relatives): (1) families with two or more patients with gastric cancer at any age, one confirmed DGC; (2) individuals with DGC before the age of 40 and (3) families with diagnoses of both DGC and LBC (one diagnosis before the age of 50). Additionally, CDH1 testing could be considered in patients with bilateral or familial LBC before the age of 50, patients with DGC and cleft lip/palate, and those with precursor lesions for signet ring cell carcinoma. Given the high mortality associated with invasive disease, prophylactic total gastrectomy at a centre of expertise is advised for individuals with pathogenic CDH1 mutations. Breast cancer surveillance with annual breast MRI starting at age 30 for women with a CDH1 mutation is recommended. Standardised endoscopic surveillance in experienced centres is recommended for those opting not to have gastrectomy at the current time, those with CDH1 variants of uncertain significance and those that fulfil hereditary DGC criteria without germline CDH1 mutations. Expert histopathological confirmation of (early) signet ring cell carcinoma is recommended. The impact of gastrectomy and mastectomy should not be underestimated; these can have severe consequences on a psychological, physiological and metabolic level. Nutritional problems should be carefully monitored. [ABSTRACT FROM AUTHOR]

Published

2015

44. TOPGEAR: a randomised phase III trial of perioperative ECF chemotherapy versus preoperative chemoradiation plus perioperative ECF chemotherapy for resectable gastric cancer (an international, intergroup trial of the AGITG/ TROG/EORTC/NCIC CTG)

Author

Leong, Trevor, Smithers, B Mark, Michael, Michael, Gebski, Val, Boussioutas, Alex, Miller, Danielle, Simes, John, Zalcberg, John, Haustermans, Karin, Lordick, Florian, Schuhmacher, Christoph, Swallow, Carol, Darling, Gail, and Wong, Rebecca

Abstract

Background: The optimal management of patients with resectable gastric cancer continues to evolve in Western countries. Following publication of the US Intergroup 0116 and UK Medical Research Council MAGIC trials, there are now two standards of care for adjuvant therapy in resectable gastric cancer, at least in the Western world: postoperative chemoradiotherapy and perioperative epirubicin/cisplatin/fluorouracil (ECF) chemotherapy. We hypothesize that adding chemoradiation to standard perioperative ECF chemotherapy will achieve further survival gains. We also believe there are advantages to administering chemoradiation in the preoperative rather than postoperative setting. In this article, we describe the TOPGEAR trial, which is a randomised phase III trial comparing control arm therapy of perioperative ECF chemotherapy with experimental arm therapy of preoperative chemoradiation plus perioperative ECF chemotherapy. Methods/Design: Eligible patients with resectable adenocarcinoma of the stomach or gastroesophageal junction will be randomized to receive either perioperative chemotherapy alone (3 preoperative and 3 postoperative cycles of ECF) or perioperative chemotherapy plus preoperative chemoradiation. In the chemoradiation arm, patients receive 2 cycles of ECF plus chemoradiation prior to surgery, and then following surgery 3 further cycles of ECF are given. The trial is being conducted in two Parts; Part 1 (phase II component) has recruited 120 patients with the aim of assessing feasibility, safety and preliminary efficacy of preoperative chemoradiation. Part 2 (phase III component) will recruit a further 632 patients to provide a total sample size of 752 patients. The primary endpoint of the phase III trial is overall survival. The trial includes quality of life and biological substudies, as well as a health economic evaluation. In addition, the trial incorporates a rigorous quality assurance program that includes real time central review of radiotherapy plans and central review of surgical technique. Discussion: TOPGEAR is an international, intergroup collaboration led by the Australasian Gastro-Intestinal Trials Group (AGITG), in collaboration with the Trans-Tasman Radiation Oncology Group (TROG), European Organisation for Research and Treatment of Cancer (EORTC) and the NCIC Clinical Trials Group. It addresses a globally significant question that will help inform future international standards for clinical practice in resectable gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2015

45. Lamina propria macrophage phenotypes in relation to Escherichia coli in Crohn’s disease.

Author

Elliott, Timothy R., Rayment, Neil B., Hudspith, Barry N., Hands, Rebecca E., Taylor, Kirstin, Parkes, Gareth C., Prescott, Natalie J., Petrovska, Liljana, Hermon-Taylor, John, Brostoff, Jonathan, Boussioutas, Alex, Mathew, Christopher G., Bustin, Stephen A., and Sanderson, Jeremy D.

Abstract

Background: Abnormal handling of E. coli by lamina propria (LP) macrophages may contribute to Crohn’s disease (CD) pathogenesis. We aimed to determine LP macrophage phenotypes in CD, ulcerative colitis (UC) and healthy controls (HC), and in CD, to compare macrophage phenotypes according to E. coli carriage. Methods: Mucosal biopsies were taken from 35 patients with CD, 9 with UC and 18 HCs. Laser capture microdissection was used to isolate E. coli-laden and unladen LP macrophages from ileal or colonic biopsies. From these macrophages, mRNA was extracted and cytokine and activation marker expression measured using RT-qPCR. Results: E. coli-laden LP macrophages were identified commonly in mucosal biopsies from CD patients (25/35, 71 %), rarely in UC (1/9, 11 %) and not at all in healthy controls (0/18). LP macrophage cytokine mRNA expression was greater in CD and UC than healthy controls. In CD, E. coli-laden macrophages expressed high IL-10 & CD163 and lower TNFα, IL-23 & iNOS irrespective of macroscopic inflammation. In inflamed tissue, E. coli-unladen macrophages expressed high TNFα, IL-23 & iNOS and lower IL-10 & CD163. In uninflamed tissue, unladen macrophages had low cytokine mRNA expression, closer to that of healthy controls. Conclusion: In CD, intra-macrophage E. coli are commonly found and LP macrophages express characteristic cytokine mRNA profiles according to E. coli carriage. Persistence of E. coli within LP macrophages may provide a stimulus for chronic inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

46. Role of tumour molecular and pathology features to estimate colorectal cancer risk for first-degree relatives.

Author

Win, Aung Ko, Buchanan, Daniel D., Rosty, Christophe, Maclnnis, Robert J., Dowty, James G., Dite, Gillian S., Giles, Graham G., Southey, Melissa C., Young, Joanne P., Clendenning, Mark, Walsh, Michael D., Walters, Rhiannon J., Boussioutas, Alex, Smyrk, Thomas C., Thibodeau, Stephen N., Baron, John A., Potter, John D., Newcomb, Polly A., Marchand, Loïc Le, and Haile, Robert W.

Subjects

COLON cancer risk factors, CANCER invasiveness, HEREDITARY nonpolyposis colorectal cancer, MOLECULAR pathology, COLON cancer diagnosis

Abstract

Objective To estimate risk of colorectal cancer (CRC) for first-degree relatives of CRC cases based on CRC molecular subtypes and tumour pathology features. Design We studied a cohort of 33 496 first-degree relatives of 4853 incident invasive CRC cases (probands) who were recruited to the Colon Cancer Family Registry through population cancer registries in the USA, Canada and Australia. We categorised the first-degree relatives into four groups: 28 156 of 4095 mismatch repair (MMR)- proficient probands, 2302 of 301 MMR-deficient non- Lynch syndrome probands, 1799 of 271 suspected Lynch syndrome probands and 1239 of 186 Lynch syndrome probands. We compared CRC risk for first-degree relatives stratified by the absence or presence of specific tumour molecular pathology features in probands across each of these four groups and for all groups combined. Results Compared with first-degree relatives of MMRproficient CRC cases, a higher risk of CRC was estimated for first-degree relatives of CRC cases with suspected Lynch syndrome (HR 2.06, 95% CI 1.59 to 2.67) and with Lynch syndrome (HR 5.37, 95% CI 4.16 to 6.94), but not with MMR-deficient non-Lynch syndrome (HR 1.04, 95% CI 0.82 to 1.31). A greater risk of CRC was estimated for first-degree relatives if CRC cases were diagnosed before age 50 years, had proximal colon cancer or if their tumours had any of the following: expanding tumour margin, peritumoral lymphocytes, tumour-infiltrating lymphocytes or synchronous CRC. Conclusions Molecular pathology features are potentially useful to refine screening recommendations for first-degree relatives of CRC cases and to identify which cases are more likely to be caused by genetic or other familial factors. [ABSTRACT FROM AUTHOR]

Published

2015

47. Contribution of the -Omics Era to Our Understanding of Preinvasive Disease and Progression to Cancer.

Author

Busuttil, Rita A. and Boussioutas, Alex

Abstract

The term -omics refers to a biological field of study in which large scale network analysis techniques are used to interrogate various biological processes. Omics based technologies have been widely applied to studies of primary cancers. More recently, improvements in these techniques, such as increased sensitivity and decreased amounts of input sample has allowed their utilisation in the study of p-remalignant and preinvasive disease. Many premalignant lesions are known to persist for lengthy periods of time before progressing to cancer in only a small proportion of patients. Identification of the key genes and molecular mechanisms involved in progression may aid in identifying patients at high risk of progression and play a role in determining potential targets for prevention or treatment. This chapter outlines the current contribution of -omics technologies to our understanding of preinvasive and premalignant lesions of various types of adenocarcinomas. [ABSTRACT FROM AUTHOR]

Published

2011

48. Gene Ontology Assisted Exploratory Microarray Clustering and Its Application to Cancer.

Author

Macintyre, Geoff, Bailey, James, Gustafsson, Daniel, Boussioutas, Alex, Haviv, Izhak, and Kowalczyk, Adam

Abstract

Gene expression profiling provides insight into the functions of genes at a molecular level. Clustering of gene expression profiles can facilitate the identification of the underlying driving biological program causing genes΄ co-expression. Standard clustering methods, grouping genes based on similar expression values, fail to capture weak expression correlations potentially causing genes in the same biological process to be grouped separately. We have developed a novel clustering algorithm which incorporates functional gene information from the Gene Ontology into the clustering process, resulting in more biologically meaningfull clusters. We have validated our method using a multi-cancer microarray dataset. In addition, we show the potential of such methods for the exploration of cancer etiology. [ABSTRACT FROM AUTHOR]

Published

2008

49. Cost-effectiveness of family history-based colorectal cancer screening in Australia.

Author

Ouakrim, Driss A., Boussioutas, Alex, Lockett, Trevor, Hopper, John L., and Jenkins, Mark A.

Subjects

COLON cancer diagnosis, COLONOSCOPY, FAMILY history (Medicine), CANCER-related mortality, COST effectiveness

Abstract

Background: With 14.234 diagnoses and over 4047 deaths reported in 2007, colorectal cancer (CRC) is the second most common cancer and second most common cause of cancer-related mortality in Australia. The direct treatment cost has recently been estimated to be around AU$1.2 billion for the year 2011, which corresponds to a four-fold increase, compared the cost reported in 2001. Excluding CRCs due to known rare genetic disorders, 20% to 25% of all CRCs occur in a familial aggregation setting due to genetic variants or shared environmental risk factors that are yet to be characterised. A targeted screening strategy addressed to this segment of the population is a potentially valuable tool for reducing the overall burden of CRC. Methods: We developed a Markov model to assess the cost-effectiveness of three screening strategies offered to people at increased risk due to a strong family history of CRC. The model simulated the evolution of a cohort of 10,000 individuals fromage 50 to 90 years. We compared screening with biennial iFOBT, five-yearly colonoscopy and ten-yearly colonoscopy versus the current strategy of the Australian National Bowel Cancer Screening Programme (i.e. base case). Results: Under the NBCSP scenario, 6,491 persons developed CRC with an average screening lifetime cost of AU$3,441 per person. In comparison, screening with biennial iFOBT, colonoscopy every ten years, and colonoscopy every five years reduced CRC incidence by 27%, 35% and 60%, and mortality by 15%, 26% and 46% respectively. All three screening strategies had a cost under AU$50,000 per life year gained, which is regarded as the upper limit of acceptable cost-effectiveness in the Australian health system. At AU$12,405 per life year gained and an average lifetime expectancy of 16.084 years, five-yearly colonoscopy screening was the most cost-effective strategy. Conclusion: The model demonstrates that intensive CRC screening strategies targeting people at increased risk would be cost-effective in the Australian context. Our findings provide evidence that substantial health benefits can be generated from risk-based CRC screening at a relatively modest incremental cost. [ABSTRACT FROM AUTHOR]

Published

2014

50. Cost-effectiveness of family history-based colorectal cancer screening in Australia.

Author

Ouakrim, Driss A., Boussioutas, Alex, Lockett, Trevor, Hopper, John L., and Jenkins, Mark A.

Subjects

COST effectiveness, FAMILY history (Medicine), COLON cancer patients, MEDICAL screening, CANCER-related mortality, MEDICAL care costs

Abstract

Background: With 14.234 diagnoses and over 4047 deaths reported in 2007, colorectal cancer (CRC) is the second most common cancer and second most common cause of cancer-related mortality in Australia. The direct treatment cost has recently been estimated to be around AU$1.2 billion for the year 2011, which corresponds to a four-fold increase, compared the cost reported in 2001. Excluding CRCs due to known rare genetic disorders, 20% to 25% of all CRCs occur in a familial aggregation setting due to genetic variants or shared environmental risk factors that are yet to be characterised. A targeted screening strategy addressed to this segment of the population is a potentially valuable tool for reducing the overall burden of CRC. Methods: We developed a Markov model to assess the cost-effectiveness of three screening strategies offered to people at increased risk due to a strong family history of CRC. The model simulated the evolution of a cohort of 10,000 individuals from age 50 to 90 years. We compared screening with biennial iFOBT, five-yearly colonoscopy and ten-yearly colonoscopy versus the current strategy of the Australian National Bowel Cancer Screening Programme (i.e. base case). Results: Under the NBCSP scenario, 6,491 persons developed CRC with an average screening lifetime cost of AU$3,441 per person. In comparison, screening with biennial iFOBT, colonoscopy every ten years, and colonoscopy every five years reduced CRC incidence by 27%, 35% and 60%, and mortality by 15%, 26% and 46% respectively. All three screening strategies had a cost under AU$50,000 per life year gained, which is regarded as the upper limit of acceptable cost-effectiveness in the Australian health system. At AU$12,405 per life year gained and an average lifetime expectancy of 16.084 years, five-yearly colonoscopy screening was the most cost-effective strategy. Conclusion: The model demonstrates that intensive colorectal cancer screening strategies targeting people at increased risk would be cost-effective in the Australian context. Our findings provide evidence that substantial health benefits can be generated from risk-based CRC screening at a relatively modest incremental cost. [ABSTRACT FROM AUTHOR]

Published

2014