Medicine (RMH) - Research Publications

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Author: Boussioutas, Alex × Author: Giles, Graham × Author: Hopper, John × Author: Winship, Ingrid × Start date: 2013 × Type: Journal Article ×

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    Family history-based colorectal cancer screening in Australia: A modelling study of the costs, benefits, and harms of different participation scenarios
    Dillon, M ; Flander, L ; Buchanan, DD ; Macrae, FA ; Emery, JD ; Winship, IM ; Boussioutas, A ; Giles, GG ; Hopper, JL ; Jenkins, MA ; Ouakrim, DA ; Shapiro, SD (PUBLIC LIBRARY SCIENCE, 2018-08)
    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.
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    Are the common genetic variants associated with colorectal cancer risk for DNA mismatch repair gene mutation carriers?
    Win, AK ; Hopper, JL ; Buchanan, DD ; Young, JP ; Tenesa, A ; Dowty, JG ; Giles, GG ; Goldblatt, J ; Winship, I ; Boussioutas, A ; Young, GP ; Parry, S ; Baron, JA ; Duggan, D ; Gallinger, S ; Newcomb, PA ; Haile, RW ; Le Marchand, L ; Lindor, NM ; Jenkins, MA (ELSEVIER SCI LTD, 2013-05)
    BACKGROUND: Genome-wide association studies have identified at least 15 independent common genetic variants associated with colorectal cancer (CRC) risk. The aim of this study was to investigate whether 11 of these variants are associated with CRC risk for carriers of germline mutations in DNA mismatch repair (MMR) genes. METHODS: A total of 927 MMR gene mutation carriers (360 MLH1, 442 MSH2, 85 MSH6 and 40 PMS2) from 315 families enrolled in the Colon Cancer Family Registry, were genotyped for the single nucleotide polymorphisms (SNPs): rs16892766 (8q23.3), rs6983267 (8q24.21), rs719725 (9p24), rs10795668 (10p14), rs3802842 (11q23.1), rs4444235 (14q22.2), rs4779584 (15q13.3), rs9929218 (16q22.1), rs4939827 (18q21.1), rs10411210 (19q13.1) and rs961253 (20p12.3). We used a weighted Cox regression to estimate CRC risk for homozygous and heterozygous carriers of the risk allele compared with homozygous non-carriers as well as for an additive per allele model (on the log scale). RESULTS: Over a total of 40,978 person-years observation, 426 (46%) carriers were diagnosed with CRC at a mean age of 44.3 years. For all carriers combined, we found no evidence of an association between CRC risk and the total number of risk alleles (hazard ratio [HR] per risk allele=0.97, 95% confidence interval [CI]=0.88-1.07, p=0.52). CONCLUSIONS: We found no evidence that the SNPs associated with CRC in the general population are modifiers of the risk for MMR gene mutation carriers overall, and therefore any evidence of proven clinical utility in Lynch syndrome.
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    Tumor testing to identify lynch syndrome in two Australian colorectal cancer cohorts
    Buchanan, DD ; Clendenning, M ; Rosty, C ; Eriksen, SV ; Walsh, MD ; Walters, RJ ; Thibodeau, SN ; Stewart, J ; Preston, S ; Win, AK ; Flander, L ; Ouakrim, DA ; Macrae, FA ; Boussioutas, A ; Winship, IM ; Giles, GG ; Hopper, JL ; Southey, MC ; English, D ; Jenkins, MA (WILEY, 2017-02)
    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.
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    Risk factors for metachronous colorectal cancer following a primary colorectal cancer: A prospective cohort study
    Jayasekara, H ; Reece, JC ; Buchanan, DD ; Rosty, C ; Dashti, SG ; Ouakrim, DA ; Winship, IM ; Macrae, FA ; Boussioutas, A ; Giles, GG ; Ahnen, DJ ; Lowery, J ; Casey, G ; Haile, RW ; Gallinger, S ; Le Marchand, L ; Newcomb, PA ; Lindor, NM ; Hopper, JL ; Parry, S ; Jenkins, MA ; Win, AK (WILEY-BLACKWELL, 2016-09-01)
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    Risk of Colorectal Cancer for Carriers of Mutations in MUTYH, With and Without a Family History of Cancer
    Win, AK ; Dowty, JG ; Cleary, SP ; Kim, H ; Buchanan, DD ; Young, JP ; Clendenning, M ; Rosty, C ; MacInnis, RJ ; Giles, GG ; Boussioutas, A ; Macrae, FA ; Parry, S ; Goldblatt, J ; Baron, JA ; Burnett, T ; Le Marchand, L ; Newcomb, PA ; Haile, RW ; Hopper, JL ; Cotterchio, M ; Gallinger, S ; Lindor, NM ; Tucker, KM ; Winship, IM ; Jenkins, MA (W B SAUNDERS CO-ELSEVIER INC, 2014-05)
    We studied 2332 individuals with monoallelic mutations in MUTYH among 9504 relatives of 264 colorectal cancer (CRC) cases with a MUTYH mutation. We estimated CRC risks through 70 years of age of 7.2% for male carriers of monoallelic mutations (95% confidence interval [CI], 4.6%-11.3%) and 5.6% for female carriers of monoallelic mutations (95% CI, 3.6%-8.8%), irrespective of family history. For monoallelic MUTYH mutation carriers with a first-degree relative with CRC diagnosed by 50 years of age who does not have the MUTYH mutation, risks of CRC were 12.5% for men (95% CI, 8.6%-17.7%) and 10% for women (95% CI, 6.7%-14.4%). Risks of CRC for carriers of monoallelic mutations in MUTYH with a first-degree relative with CRC are sufficiently high to warrant more intensive screening than for the general population.