Your search keyword '"Macrae, Finlay A."' showing total 36 results

1. Survival by colon cancer stage and screening interval in Lynch syndrome: a prospective Lynch syndrome database report

Author

Dominguez-Valentin, Mev, Seppälä, Toni T., Sampson, Julian R., Macrae, Finlay, Winship, Ingrid, Evans, D. Gareth, Scott, Rodney J., Burn, John, Möslein, Gabriela, Bernstein, Inge, Pylvänäinen, Kirsi, Renkonen-Sinisalo, Laura, Lepistö, Anna, Lindblom, Annika, Plazzer, John-Paul, Tjandra, Douglas, Thomas, Huw, Green, Kate, Lalloo, Fiona, Crosbie, Emma J., Hill, James, Capella, Gabriel, Pineda, Marta, Navarro, Matilde, Vidal, Joan Brunet, Rønlund, Karina, Nielsen, Randi Thyregaard, Yilmaz, Mette, Elvang, Louise Laurberg, Katz, Lior, Nielsen, Maartje, ten Broeke, Sanne W., Nakken, Sigve, Hovig, Eivind, Sunde, Lone, Kloor, Matthias, Knebel Doeberitz, Magnus v, Ahadova, Aysel, Lindor, Noralane, Steinke-Lange, Verena, Holinski-Feder, Elke, Mecklin, Jukka-Pekka, and Møller, Pål

Published

2019

2. Outcomes of screening and surveillance in people with two parents affected by colorectal cancers: experiences from the Familial Bowel Cancer Service

Author

Pan, Jennifer, Slattery, Masha, Shea, Natalie, and Macrae, Finlay

Published

2019

3. Phenotypic confirmation of oligodontia, colorectal polyposis and cancer in a family carrying an exon 7 nonsense variant in the AXIN2 gene.

Author

Beard, Catherine, Purvis, Rebecca, Winship, Ingrid M., Macrae, Finlay A., and Buchanan, Daniel D.

Subjects

COLON cancer, HYPODONTIA, ECTODERMAL dysplasia, ADENOMATOUS polyps, WNT signal transduction, GENES, FAMILIES

Abstract

The AXIN2 gene, like APC, plays a role in the Wnt signalling pathway involved in colorectal tumour formation. Heterozygous mutations in AXIN2 have been shown to cause ectodermal dysplasia (including tooth agenesis, or more specifically, oligodontia), and, in some carriers, colorectal cancer and/or adenomatous polyposis develops. There is a paucity of published AXIN2 families making genotype-phenotype (polyposis, colorectal cancer and oligodontia) correlations challenging. In this case report we describe a family with c.1972delA, p.Ser658Alafs*31 nonsense variant in AXIN2 where the three confirmed carriers presented with both oligodontia and colorectal adenomatous polyposis; mean number of teeth missing in carriers was 16.5 (range 11–22) and mean number of polyps in carriers was 49 (range 5->100, polyps were predominantly adenomatous). This highlights the importance of confirming phenotypic information in familial polyposis, to guide appropriate genetic investigations, as well as providing additional phenotypic and penetrance data to aid in clinical risk management recommendations. Our experience supports the inclusion of AXIN2 on panels for testing of patients with polyposis. [ABSTRACT FROM AUTHOR]

Published

2019

4. 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

5. 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

6. 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

7. ' 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

8. Improving adherence to colorectal cancer surveillance guidelines: results of a randomised controlled trial.

Author

Carey, Mariko, Sanson-Fisher, Robert, Macrae, Finlay, Cameron, Emilie, Hill, David, D'Este, Catherine, and Doran, Christopher

Subjects

COLON cancer, RANDOMIZED controlled trials, COLONOSCOPY, CANCER relapse

Abstract

Background: Colorectal cancer (CRC) survivors are at increased risk of developing the disease again. Surveillance guidelines are aimed at maximising the early detection of recurring or new cancers and pre-cancerous polyps. The frequency and type of surveillance recommended depends on the type of treatment for the initial CRC, the extent of colonoscopic investigation prior to treatment and the results of previous surveillance tests. This paper aimed to test the effect of a paper-based educational intervention to improve adherence to colonoscopy following treatment for colorectal cancer.Methods: People with a diagnosis of colorectal cancer within the last 10 months, aged ≥18 and English speaking were recruited through a population-based cancer registry in Australia. Participants were randomly allocated to either the intervention or control. Participants completed an interview at baseline. Self-reported participation in colonoscopy was obtained at 12 month followup by survey. Those allocated to the control received a generic pamphlet on colorectal cancer treatment; while intervention participants received a letter which provided specific information about guideline recommendations for surveillance colonoscopy. Rates of guideline adherence were compared between groups. The guideline recommendations for the timing of surveillance colonoscopy changed part way through the study. This change occurred after all intervention materials had been sent, but prior to all participants completing the 12 month follow up. Post hoc analyses were conducted to assess adherence to the new guidelines.Results: Of the 767 participants, 604 (79%) had had surgery, had stage I - III disease and completed the baseline interview within 12 months of diagnosis (intervention = 305; control = 299). There was no significant difference between those adherent to surveillance colonoscopy guidelines, in the control (67, 27%) and intervention groups (80, 31%) at followup (difference = 4.3% (95%CI:-3.7%, 12%), χ 2(1df) = 1.09, P = 0.296). Overall, 246 (49%) participants were adherent to the new guidelines, compared to 147 (29%) adherent to the old guidelines.Conclusions: Results indicate the paper-based educational intervention is not effective in improving adherence to colorectal cancer surveillance guidelines for colonoscopy.Trial Registration Number: ACTRN12609000628246 Registration date: 28/07/2009. [ABSTRACT FROM AUTHOR]

Published

2017

9. 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

10. Ideal colonoscopic surveillance intervals to reduce incidence of advanced adenoma and colorectal cancer.

Author

Good, Norm M, Macrae, Finlay A, Young, Graeme P, O'Dywer, John, Slattery, Masha, Venables, William, Lockett, Trevor J, and O'Dwyer, Marilla

Subjects

*COLONOSCOPY, *CERVICAL intraepithelial neoplasia, *COLON cancer, *ADENOMA, *ADENOMATOUS polyposis coli

Abstract

Background and Aims There is limited information about the interplay between multiple risk factors contributing to the risk of advanced neoplasia. We determined the actual risk for advanced neoplasia in relation to lapsed time between colonoscopies in people enrolled in a structured surveillance program. This risk information can be used to guide the selection of optimal surveillance intervals. Methods Patients were recruited into programs at two major tertiary hospitals, with a personal or family history of advanced neoplasia. Five thousand one hundred forty-one patients had an index and one or more surveillance colonoscopies. Fifty-one percent had a family history of colorectal neoplasia while the remainder had a personal history. Results Patients with an immediately prior colonoscopy result (prior result) of advanced adenoma had a risk for advanced neoplasia 7.1 times greater than those with a normal prior result. Cancer as a prior result did not confer a greater risk than either a hyperplastic polyp or a nonadvanced adenoma. Being female reduced risk, age increased risk. Only a family history of a first-degree relative diagnosed under 55, or definite or suspected hereditary nonpolyposis colorectal cancer ( HNPCC) conferred an increased risk over a personal history of advanced neoplasia. Conclusions Most family history categories did not confer excess risk above personal history of advanced neoplasia. A prior cancer poses less of a risk than a prior advanced adenoma. Based on our models, a person with an advanced adenoma should be scheduled for colonoscopy at 3 years, corresponding to a 15% risk of advanced neoplasia for a male aged under 56. Guidelines should be updated that uses a 15% risk as a benchmark for calculating surveillance intervals. [ABSTRACT FROM AUTHOR]

Published

2015

11. Familial colorectal cancer syndromes: an overview of clinical management.

Author

Sammour, Tarik, Hayes, Ian P, Hill, Andrew G, Macrae, Finlay A, and Winter, Des C

Subjects

INTESTINAL disease treatment, COLON cancer, CROHN'S disease, SKIN cancer, COLITIS treatment, ULCERATIVE colitis

Abstract

Familial colorectal cancer syndromes pose a complex challenge to the treating clinician. Once a syndrome is recognized, genetic testing is often required to confirm the clinical suspicion. Management from that point is usually based on disease-specific guideline recommendations targeting risk reduction for the patient and their relatives through surgery, surveillance and chemoprophylaxis. The aim of this paper is to provide an up-to-date summary of the most common familial syndromes and their medical and surgical management, with specific emphasis on evidence-based interventions that improve patient outcome, and to present the information in a manner that is easily readable and clinically relevant to the treating clinician. [ABSTRACT FROM AUTHOR]

Published

2015

12. Applicability of Next Generation Sequencing Technology in Microsatellite Instability Testing.

Author

Gan, Chun, Love, Clare, Beshay, Victoria, Macrae, Finlay, Fox, Stephen, Waring, Paul, and Taylor, Graham

Subjects

MICROSATELLITE repeats, RISK assessment, CANCER chemotherapy, NUCLEOTIDE sequence, COLON cancer

Abstract

Microsatellite instability (MSI) is a useful marker for risk assessment, prediction of chemotherapy responsiveness and prognosis in patients with colorectal cancer. Here, we describe a next generation sequencing approach for MSI testing using the MiSeq platform. Different from other MSI capturing strategies that are based on targeted gene capture, we utilize "deep resequencing", where we focus the sequencing on only the microsatellite regions of interest. We sequenced a series of 44 colorectal tumours with normal controls for five MSI loci (BAT25, BAT26, BAT34c4, D18S55, D5S346) and a second series of six colorectal tumours (no control) with two mononucleotide loci (BAT25, BAT26). In the first series, we were able to determine 17 MSI-High, 1 MSI-Low and 26 microsatellite stable (MSS) tumours. In the second series, there were three MSI-High and three MSS tumours. Although there was some variation within individual markers, this NGS method produced the same overall MSI status for each tumour, as obtained with the traditional multiplex PCR-based method. [ABSTRACT FROM AUTHOR]

Published

2015

13. Lack of evidence for germline RNF43 mutations in patients with serrated polyposis syndrome from a large multinational study.

Author

Buchanan, Daniel D., Clendenning, Mark, Li Zhuoer, Stewart, Jenna R., Joseland, Sharelle, Woodall, Sonja, Arnold, Julie, Semotiuk, Kara, Aronson, Melyssa, Holter, Spring, Gallinger, Steven, Jenkins, Mark A., Sweet, Kevin, Macrae, Finlay A., Winship, Ingrid M., Parry, Susan, and Rosty, Christophe

Subjects

GERM cells, POLYPS, COLON cancer, EXOMES, NUCLEOTIDE sequencing

Published

2017

14. Little evidence for association between the TGFBR1*6A variant and colorectal cancer: a family-based association study on non-syndromic family members from Australia and Spain.

Author

Ross, Jason P., Lockett, Linda J., Tabor, Bruce, Saunders, Ian W., Young, Graeme P., Macrae, Finlay, Blanco, Ignacio, Capella, Gabriel, Brown, Glenn S., Lockett, Trevor J., and Hannan, Garry N.

Subjects

COLON cancer, DISEASE susceptibility, TRANSFORMING growth factors-beta, DELETION mutation

Abstract

Background Genome-wide linkage studies have identified the 9q22 chromosomal region as linked with colorectal cancer (CRC) predisposition. A candidate gene in this region is transforming growth factor β receptor 1 (TGFBR1). Investigation of TGFBR1 has focused on the common genetic variant rs11466445, a short exonic deletion of nine base pairs which results in truncation of a stretch of nine alanine residues to six alanine residues in the gene product. While the six alanine (*6A) allele has been reported to be associated with increased risk of CRC in some population based study groups this association remains the subject of robust debate. To date, reports have been limited to population-based case--control association studies, or case--control studies of CRC families selecting one affected individual per family. No study has yet taken advantage of all the genetic information provided by multiplex CRC families. Methods We have tested for an association between rs11466445 and risk of CRC using several family- based statistical tests in a new study group comprising members of non-syndromic high risk CRC families sourced from three familial cancer centres, two in Australia and one in Spain. Results We report a finding of a nominally significant result using the pedigree-based association test approach (PBAT; p = 0.028), while other family-based tests were non-significant, but with a p-value < 0.10 in each instance. These other tests included the Generalised Disequilibrium Test (GDT; p = 0.085), parent of origin GDT Generalised Disequilibrium Test (GDT-PO; p = 0.081) and empirical Family-Based Association Test (FBAT; p = 0.096, additive model). Related-person case--control testing using the "More Powerful" Quasi-Likelihood Score Test did not provide any evidence for association (MQLS ; p = 0.41). Conclusions After conservatively taking into account considerations for multiple hypothesis testing, we find little evidence for an association between the TGFBR1*6A allele and CRC risk in these families. The weak support for an increase in risk in CRC predisposed families is in agreement with recent meta-analyses of case--control studies, which estimate only a modest increase in sporadic CRC risk among 6*A allele carriers. [ABSTRACT FROM AUTHOR]

Published

2014

15. An association between the PTGS2 rs5275 polymorphism and colorectal cancer risk in families with inherited non-syndromic predisposition.

Author

Ross, Jason, Lockett, Linda, Brookes, Diana, Tabor, Bruce, Duesing, Konsta, Buckley, Michael, Lockett, Trevor, Molloy, Peter, Macrae, Finlay, Young, Graeme, Blanco, Ignacio, Capella, Gabriel, and Hannan, Garry N

Subjects

COLON cancer, GENETIC disorders, GENETIC polymorphisms, DISEASE susceptibility, HEREDITY

Abstract

Recently our group completed a genome-wide linkage study investigating Australian and Spanish families with inherited risk of colorectal cancer (CRC). A minor linkage peak from that study located on chromosome 1 correlates with the location of a known CRC risk-modifying gene, prostaglandin synthase (PTGS2). PTGS2 encodes the inducible prostaglandin synthase enzyme cyclooxygenase-2 (COX-2). Prostaglandins are implicated in the initiation of carcinogenesis and progression of tumours. Sequencing of PTGS2 in a small subset of affected individuals identified a high frequency of the minor C allele of single nucleotide polymorphism rs5275. We then genotyped the rs5275 polymorphism in 183 affected and 223 unaffected individuals from our CRC predisposed families. Tests for association in the presence of linkage were made using family-based association tests. The C allele was found to be significantly associated (P<0.01) with diagnosis of hereditary non-syndromic CRC (P=0.0094, dominant model) and an earlier age of diagnosis (P=0.0089, heterozygous-advantage model). Interestingly, by stratifying the age of diagnosis data, we observed a speculative gender-discordant effect. Relative to other groups, female CC carriers were diagnosed less when young, but by 60 years of age were the most at risk group. Conversely, CT carriers of both genders showed a consistently earlier diagnosis relative to TT carriers. Our results suggest potential differential age-and gender-dependent efficacies of chemopreventative COX-2 inhibitors in the context of non-syndromic colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2013

16. Risks of Primary Extracolonic Cancers Following Colorectal Cancer in Lynch Syndrome.

Author

Win, Aung Ko, Lindor, Noralane M., Young, Joanne P., Macrae, Finlay A., Young, Graeme P., Williamson, Elizabeth, Parry, Susan, Goldblatt, Jack, Lipton, Lara, Winship, Ingrid, Leggett, Barbara, Tucker, Katherine M., Giles, Graham G., Buchanan, Daniel D., Clendenning, Mark, Rosty, Christophe, Arnold, Julie, Levine, A. Joan, Haile, Robert W., and Gallinger, Steven

Subjects

COLON cancer, LYNCH syndrome II, CANCER prognosis, CANCER risk factors, GERM cells

Abstract

Background Lynch syndrome is a highly penetrant cancer predisposition syndrome caused by germline mutations in DNA mismatch repair (MMR) genes. We estimated the risks of primary cancers other than colorectal cancer following a diagnosis of colorectal cancer in mutation carriers. Methods We obtained data from the Colon Cancer Family Registry for 764 carriers of an MMR gene mutation (316 MLH1, 357 MSH2, 49 MSH6, and 42 PMS2), who had a previous diagnosis of colorectal cancer. The Kaplan–Meier method was used to estimate their cumulative risk of cancers 10 and 20 years after colorectal cancer. We estimated the age-, sex-, country- and calendar period–specific standardized incidence ratios (SIRs) of cancers following colorectal cancer, compared with the general population. Results Following colorectal cancer, carriers of MMR gene mutations had the following 10-year risk of cancers in other organs: kidney, renal pelvis, ureter, and bladder (2%, 95% confidence interval [CI] = 1% to 3%); small intestine, stomach, and hepatobiliary tract (1%, 95% CI = 0.2% to 2%); prostate (3%, 95% CI = 1% to 5%); endometrium (12%, 95% CI = 8% to 17%); breast (2%, 95% CI = 1% to 4%); and ovary (1%, 95% CI = 0% to 2%). They were at elevated risk compared with the general population: cancers of the kidney, renal pelvis, and ureter (SIR = 12.54, 95% CI = 7.97 to 17.94), urinary bladder (SIR = 7.22, 95% CI = 4.08 to 10.99), small intestine (SIR = 72.68, 95% CI = 39.95 to 111.29), stomach (SIR = 5.65, 95% CI = 2.32 to 9.69), and hepatobiliary tract (SIR = 5.94, 95% CI = 1.81 to 10.94) for both sexes; cancer of the prostate (SIR = 2.05, 95% CI = 1.23 to 3.01), endometrium (SIR = 40.23, 95% CI = 27.91 to 56.06), breast (SIR = 1.76, 95% CI = 1.07 to 2.59), and ovary (SIR = 4.19, 95% CI = 1.28 to 7.97). Conclusion Carriers of MMR gene mutations who have already had a colorectal cancer are at increased risk of a greater range of cancers than the recognized spectrum of Lynch syndrome cancers, including breast and prostate cancers. [ABSTRACT FROM PUBLISHER]

Published

2012

17. Colorectal cancer screening in Australia: a community-level perspective.

Author

Courtney, Ryan J., Paul, Christine L., Sanson-Fisher, Robert W., Macrae, Finlay A., Carey, Mariko L., Attia, John R., and McEvoy, Mark A.

Subjects

AT-risk people, COLON cancer, VOTING registers, FECAL occult blood tests

Abstract

The article discusses a community-based study of at-risk people for colorectal cancer (CRC) in order to assess for respondents at each level of risk. Participants were randomly chosen from the New South Wales electoral roll and were asked whether they had faecal occult blood testing (FOBT), colonoscopy or sigmoidoscopy. The study found that 16% of asymptomatic people had a colonoscopy in the past 5 years although colonoscopy screening is not endorsed for people at a certain level or risk.

Published

2012

18. Evidence of linkage to chromosomes 10p15.3-p15.1, 14q24.3-q31.1 and 9q33.3-q34.3 in non-syndromic colorectal cancer families.

Author

Saunders, Ian W, Ross, Jason, Macrae, Finlay, Young, Graeme P, Blanco, Ignacio, Brohede, Jesper, Brown, Glenn, Brookes, Diana, Lockett, Trevor, Molloy, Peter L, Moreno, Victor, Capella, Gabriel, and Hannan, Garry N

Subjects

COLON cancer, HEREDITY, CELL nuclei, GENOMES, GENETIC polymorphisms

Abstract

Up to 25% of colorectal cancer (CRC) may be caused by inherited genetic variants that have yet to be identified. Previous genome-wide linkage studies (GWLSs) have identified a new loci postulated to contain novel CRC risk genes amongst affected families carrying no identifiable mutations in any of the known susceptibility genes for familial CRC syndromes. To undertake a new GWLS, we recruited members from 54 non-syndromic families from Australia and Spain where at least two first-degree relatives were affected by CRC. We used single-nucleotide polymorphism arrays to genotype 98 concordant affected relative pairs that were informative for linkage analyses. We tested for genome-wide significance (GWS) for linkage to CRC using a quantile statistic method, and we found that GWS was achieved at the 5% level. Independently, using the PSEUDO gene-dropping algorithm, we also found that GWS for linkage to CRC was achieved (P=0.02). Merlin non-parametric linkage analysis revealed significant linkage to CRC for chromosomal region 10p15.3-p15.1 and suggestive linkage to CRC for regions on 14q and 9q. The 10p15.3-p15.1 has not been reported to be linked to hereditary CRC in previous linkage studies, but this region does harbour the Kruppel-like factor 6 (KLF6) gene that is known to be altered in common CRC. Further studies aimed at localising the responsible genes, and characterising their function will give insight into the factors responsible for susceptibility in such families, and perhaps shed further light on the mechanisms of CRC development. [ABSTRACT FROM AUTHOR]

Published

2012

19. Factors associated with consultation behaviour for primary symptoms potentially indicating colorectal cancer: A cross-sectional study on response to symptoms.

Author

Courtney, Ryan J., Paul, Christine L., Sanson-Fisher, Robert W., Macrae, Finlay A., Attia, John, and McEvoy, Mark

Subjects

COLON cancer, MEDICAL care, QUESTIONNAIRES, PHYSICIANS, BEHAVIOR

Abstract

Background: Little data exists on the factors associated with health care seeking behaviour for primary symptoms of colorectal cancer (CRC). This study aimed to identify individual, provider and psychosocial factors associated with (i) ever seeking medical advice and (ii) seeking early medical advice for primary symptoms of colorectal cancer (CRC). Methods: 1592 persons aged 56–88 years randomly selected from the Hunter Community Study (HCS) were sent a questionnaire. Results: Males and those who had received screening advice from a doctor were at significantly higher odds of ever seeking medical advice for rectal bleeding. Persons who had private health coverage, consulted a doctor because the ‘symptom was serious’, or who did not wait to consult a doctor for another reason were at significantly higher odds of seeking early medical advice (< 2 weeks). For change in bowel habit, persons with lower income, within the healthy weight range, or who had discussed their family history of CRC irrespective of whether informed of ‘increased risk’ were at significantly higher odds of ever seeking medical advice. Persons frequenting their GP less often and seeing their doctor because the symptom persisted were at significantly higher odds of seeking early medical advice (< 2 weeks). Conclusions: The seriousness of symptoms, importance of early detection, and prompt consultation must be articulated in health messages to at-risk persons. This study identified modifiable factors, both individual and provider-related to consultation behaviour. Effective health promotion efforts must heed these factors and target sub-groups less likely to seek early medical advice. [ABSTRACT FROM AUTHOR]

Published

2012

20. Metachronous colorectal cancer risk for mismatch repair gene mutation carriers: the advantage of more extensive colon surgery.

Author

Parry, Susan, Aung Ko Win, Parry, Bryan, Macrae, Finlay A., Gurrin, Lyle C., Church, James M., Baron, John A., Giles, Graham G., Leggett, Barbara A., Winship, Ingrid, Lipton, Lara, Young, Graeme P., Young, Joanne P., Lodge, Caroline J., Southey, Melissa C., Newcomb, Polly A., Le Marchand, Loïc, Haile, Robert W., Lindor, Noralane M., and Gallinger, Steven

Subjects

COLON cancer, COLON surgery, HEREDITARY nonpolyposis colorectal cancer, COLONOSCOPY, DECISION making

Abstract

Background Surgical management of colon cancer for patients with Lynch syndrome who carry a mismatch repair (MMR) gene mutation is controversial. The decision to remove more or less of the colon involves the consideration of a relatively high risk of metachronous colorectal cancer (CRC) with the impact of more extensive surgery. Objective To estimate and compare the risks of metachronous CRC for patients with Lynch syndrome undergoing either segmental or extensive (subtotal or total) resection for first colon cancer. Design Risk of metachronous CRC was estimated for 382 MMR gene mutation carriers (172 MLH1, 167 MSH2, 23 MSH6 and 20 PMS2) from the Colon Cancer Family Registry, who had surgery for their first colon cancer, using retrospective cohort analysis. Agedependent cumulative risks of metachronous CRC were calculated using the KaplaneMeier method. Risk factors for metachronous CRC were assessed by a Cox proportional hazards regression. Results None of 50 subjects who had extensive colectomy was diagnosed with metachronous CRC (incidence rate 0.0; 95% CI 0.0 to 7.2 per 1000 personyears). Of 332 subjects who had segmental resections, 74 (22%) were diagnosed with metachronous CRC (incidence rate 23.6; 95% CI 18.8 to 29.7 per 1000 person-years). For those who had segmental resections, incidence was statistically higher than for those who had extensive surgery (P<0.001). Cumulative risk of metachronous CRC was 16% (95% CI 10% to 25%) at 10 years, 41% (95% CI 30% to 52%) at 20 years and 62% (95% CI 50% to 77%) at 30 years after segmental colectomy. Risk of metachronous CRC reduced by 31% (95% CI 12% to 46%; p=0.002) for every 10 cm of bowel removed. Conclusions Patients with Lynch syndrome with first colon cancer treated with more extensive colonic resection have a lower risk of metachronous CRC than those receiving less extensive surgery. This finding will better inform decision-making about the extent of primary surgical resection. [ABSTRACT FROM AUTHOR]

Published

2011

21. Risks of Lynch Syndrome Cancers for MSH6 Mutation Carriers.

Author

Baglietto, Laura, Lindor, Noralane M., Dowty, James G., White, Darren M., Wagner, Anja, Garcia, Encarna B. Gomez, Vriends, Annette H. J. T., Cartwright, Nicola R., Barnetson, Rebecca A., Farrington, Susan M., Tenesa, Albert, Hampel, Heather, Buchanan, Daniel, Arnold, Sven, Young, Joanne, Walsh, Michael D., Jass, Jeremy, Macrae, Finlay, Antill, Yoland, and Winship, Ingrid M.

Subjects

CANCER risk factors, COLON cancer, GENETIC mutation, GENETIC disorders, DNA repair, GENES

Abstract

Background: Germline mutations in MSH6 account for 10%–20% of Lynch syndrome colorectal cancers caused by hereditary DNA mismatch repair gene mutations. Because there have been only a few studies of mutation carriers, their cancer risks are uncertain. [ABSTRACT FROM PUBLISHER]

Published

2010

22. Is uptake of genetic testing for colorectal cancer influenced by knowledge of insurance implications?

Author

Keogh, Louise A., Van Vliet, Christine M., Studdert, David M., Maskiell, Judith A., Macrae, Finlay A., St John, D. James, Gaff, Clara L., Young, Mary Anne, Southey, Melissa C., Giles, Graham G., Rosenthal, Doreen A., Hopper, John L., and Jenkins, Mark A.

Subjects

HUMAN chromosome abnormality diagnosis, COLON cancer, DNA repair, COST effectiveness, GENETIC mutation

Abstract

The article presents information on a study which investigated whether knowledge of insurance implications influenced uptake of genetic testing for colorectal cancer. The study was conducted from 1999 to 2003 and from 2003 to 2006. Participants were from population-based Victorian Colorectal Cancer Family Study. The researchers conclude that identification of patients with a mutation in DNA mismatch repair (MMR) genes has clinical significance and is cost-effective in reducing the problem of colorectal cancer in the community.

Published

2009

23. Hyperplastic Polyposis Syndrome: Phenotypic Presentations and the Role of MBD4 and MYH.

Author

Chow, Elizabeth, Lipton, Lara, Lynch, Elly, D’Souza, Rebecca, Aragona, Clelia, Hodgkin, Lindy, Brown, Gregor, Winship, Ingrid, Barker, Melissa, Buchanan, Daniel, Cowie, Shannon, Nasioulas, Steve, du Sart, Desiree, Young, Joanne, Leggett, Barbara, Jass, Jeremy, and Macrae, Finlay

Subjects

HYPERPLASIA, POLYPS, CANCER patients, COLON cancer, GENES, MEDICAL research

Abstract

Background & Aims: Hyperplastic polyposis syndrome (HPS) is defined phenotypically with multiple, large and/or proximal hyperplastic polyps. There is no known germ-line predisposition. We aimed to characterize the clinicopathologic features of 38 patients with HPS and explore the role of germ-line mutations in the base excision repair genes MBD4 and MYH. Methods: Utilizing clinical databases of The Royal Melbourne Hospital Bowel Cancer Surveillance Service and the Familial Cancer Clinic, 38 patients with HPS were recruited. The patients were analyzed for age at first diagnosis, features of hyperplastic polyposis, family histories of polyposis and colorectal cancer (CRC), coexisting adenomas, serrated adenomas, incidence of CRC, and microsatellite instability in the tumours. Mutation analysis of MBD4 and MYH were performed. Results: Serrated adenomas were common (26%), and 19 (50%) of the 38 patients had a first-degree relative with CRC. Family history of HPS was uncommon, with only 2 cases found. Ten patients developed CRC, and 3 required surgery for polyposis. No pathogenic mutations in MBD4 were detected in the 27 patients tested, but 6 single nucleotide polymorphisms of uncertain functional significance were identified. Pathogenic biallelic MYH mutations were detected in 1 patient. Conclusions: Mutations in MBD4 are unlikely to be implicated in HPS; MYH mutations should be studied, especially when adenomas occur in the same patient. The clinical, histopathologic, and molecular findings of this study should contribute to our understanding of HPS and its relationship to the serrated neoplasia pathway. [Copyright &y& Elsevier]

Published

2006

24. Cancer Risks For Mismatch Repair Gene Mutation Carriers: A Population-Based Early Onset Case-Family Study.

Author

Jenkins, Mark A., Baglietto, Laura, Dowty, James G., Van Vliet, Christine M., Smith, Letitia, Mead, Leeanne J., Macrae, Finlay A., St. John, D. James B., Jass, Jeremy R., Giles, Graham G., Hopper, John L., and Southey, Melissa C.

Subjects

CANCER patients, COLON cancer, GENEALOGY, GENETIC mutation

Abstract

Background & Aims: Cancer risks for mismatch repair gene mutation carriers have been derived almost exclusively using families ascertained owing to their strong cancer family history. These may be overestimates, due to analytic problems, and not generalizable. We estimated average cancer risks for mutations identified in population-based early onset colorectal cancer cases (probands) unselected for family history. Methods: Data were cancer histories and mutation status (carrier, non-carrier, or unknown) of 17 mismatch repair gene mutation carrier probands with colorectal cancer diagnosed before age 45 (8 hMLH1, 4 hMSH2, 4 hMSH6, 1 hPMS2) and their first- and second-degree relatives. We used modified segregation analysis theory, adjusting for the family being ascertained through the proband being an early onset mutation carrier. Results: Eleven carrier probands (64%) were from families meeting the Amsterdam II criteria for hereditary nonpolyposis colorectal cancer. The cumulative risk for colorectal cancer (95% confidence interval) to age 70 was 45% (29%–62%) for men and 38% (19%–51%) for women. Corresponding risks were 67% (47%–84%) and 72% (48%–85%) for any hereditary nonpolyposis colorectal cancer–related cancer. Compared with the general population, colorectal cancer incidence for men was approximately 180-fold higher before age 50, but about the same after age 50. For women, incidence was approximately 100-fold higher before age 50 and 7-fold higher thereafter. Conclusions: For carriers of the mutations in the mismatch repair genes that cause early onset colorectal cancer, colorectal cancer increases rapidly until age 50, and the incidence decreases to general population levels at older ages. [Copyright &y& Elsevier]

Published

2006

25. A review of Juvenile Polyposis Syndrome.

Author

Chow, Elizabeth and MacRae, Finlay

Subjects

*COLON cancer, *COLON diseases, *GENETICS, *TRANSFORMING growth factors-beta, *HUMAN chromosome abnormality diagnosis, *DISEASE management

Abstract

Juvenile Polyposis Syndrome is an uncommon hamartomatous disorder with significant gastrointestinal malignant potential. Mutations in SMAD4 and BMPR1A, implicated in the Transforming Growth Factor β pathway, have recently been characterized, and hold significance in the management of patients and at risk family members. This article reviews our knowledge to date of the genetics and clinicopathological features of the Juvenile Polyposis Syndrome, and discusses the current expert recommendations for genetic testing, disease screening and management. [ABSTRACT FROM AUTHOR]

Published

2005

26. Two mismatch repair gene mutations found in a colon cancer patient – which one is pathogenic?

Author

Kariola, Reetta, Otway, Robyn, Lönnqvist, Karin E., Raevaara, Tiina E., Macrae, Finlay, Vos, Yvonne J., Kohonen-Corish, Maija, Hofstra, Robert M., and Nyström-Lahti, Minna

Subjects

COLON cancer, GENETIC mutation, GENES, GENE expression, GENETIC regulation, GENETICS

Abstract

Hereditary nonpolyposis colorectal cancer (HNPCC) is a dominantly inherited cancer syndrome. Germline mutations in five different mismatch repair (MMR) genes, MSH2, MSH6, MLH1, MLH3, and PMS2 are linked to HNPCC. Here, we describe two colon cancer families in which the index patients carry missense mutations in both MSH2 and MSH6. The MSH2 mutation, I145M, is the same in both families, whereas the MSH6 mutations are different (R1095H and L1354Q). The families do not fulfil the international criteria for HNPCC, one family comprising two and the other family four colon cancer patients, all in one generation, resembling a recessive rather than dominant inheritance characteristic of HNPCC. The tumors of the index patients showed microsatellite instability. Functional analysis was performed to determine which one of the mutations could primarily underlie the cancer susceptibility in the families. MSH2 and MSH6 are known to form a heterodimeric complex (MutSα) responsible for mismatch recognition. The interaction of each mutated protein with its wild-type partner and with its mutated partner present in the colon cancer patient, and the MMR function of the mutated MutSα complexes were determined. Since none of the three mutations affected the MSH2–MSH6 interaction or the function of MutSα in an in-vitro MMR assay, our results suggest that alone the mutations do not cause MMR deficiency typical of HNPCC. However, our results do not exclude the possible compound pathogenicity of the two mutations. [ABSTRACT FROM AUTHOR]

Published

2003

27. CORRESPONDENCE.

Author

Ameyaw, Margaret-Mary, Thornton, Nadia, McLeod, Howard L., Paterson, Adrienne C., Leeding, Kerri S., Bach, Leon A., Baldwin, Graham S., Macrae, Finlay A., Shulkes, Arthur, Jing Ma, Stampfer, Meir, Pollak, Michael, Renehan, Andrew G., O'Dwyer, Sarah T., Shalet, Stephen M., Archer, David F., Bush, Trudy, Nachtigall, Lila E., and Pike, Malcolm C.

Subjects

CANCER, HER2 gene, GENETIC polymorphisms, BREAST cancer, COLON cancer

Abstract

Presents comments on various articles published in the 'Journal of the National Cancer Institute' as of December 6, 2000. Case-control study of Her-2 genetic polymorphism and breast cancer risk; Colorectal cancer risk in men and plasma levels of insulin-like growth factors; Effect of replacement therapy on breast cancer risk.

Published

2000

28. Changes in serum carotenoids in subjects with colorectal adenomas after 24 mo of β-carotene supplementation.

Author

Wahlqvist, Mark L., Wattanapenpaiboon, Naiyana, Macrae, Finlay A., Lambert, John R., MacLennan, Robert, and Hsu-Hage, Bridget H-H.

Subjects

BETA carotene, CAROTENOIDS, COLON cancer, ADENOMA, LUTEIN, ZEAXANTHIN, LYCOPENE, PATIENTS, THERAPEUTICS

Abstract

The effect of β-carotene supplementation on major serum carotenoid fractions (lutein/zeaxanthin, β-cryptoxanthin, lycopene, a-carotene, and β-carotene) was investigated in 224 people with colorectal adenomas (139 men, 85 women) recruited for the Australian Polyp Prevention Project (APPP). Each subject was randomly assigned to take either 20 mg β-carotene/d or placebo over 24 mo. Besides the expected increase in serum concentration of β-carotene (1073% in men, 839% in women), lycopene (176% in men) and a-carotene (211% in men and 166% in women) concentrations were also increased after body mass index, baseline concentration, change in respective carotenoid intake, and other confounding factors were adjusted for. The increase in serum concentrations of these carotenoids after β-carotene supplementation suggests that fl-carotene may interact biologically with other carotenoids and such interaction would need to be taken into consideration when the protective effect of β-carotene supplementation for cancer or other diseases is examined. [ABSTRACT FROM AUTHOR]

Published

1994

29. Comparing theory and non-theory based implementation approaches to improving referral practices in cancer genetics: a cluster randomised trial protocol.

Author

Morrow, April, Hogden, Emily, Kang, Yoon-Jung, Steinberg, Julia, Canfell, Karen, Solomon, Michael J., Kench, James G., Gill, Anthony J., Shaw, Tim, Pachter, Nicholas, Parkinson, Bonny, Wolfenden, Luke, Mitchell, Gillian, Macrae, Finlay, Tucker, Kathy, and Taylor, Natalie

Subjects

CANCER genetics, HEREDITARY nonpolyposis colorectal cancer, GENE clusters, MEDICAL personnel, COLON cancer, ENDOMETRIAL cancer, 22Q11 deletion syndrome

Abstract

Background: Lynch syndrome (LS) is an inherited, cancer predisposition syndrome associated with an increased risk of colorectal, endometrial and other cancer types. Identifying individuals with LS allows access to cancer risk management strategies proven to reduce cancer incidence and improve survival. However, LS is underdiagnosed and genetic referral rates are poor. Improving LS referral is complex, and requires multisystem behaviour change. Although barriers have been identified, evidence-based strategies to facilitate behaviour change are lacking. The aim of this study is to compare the effectiveness of a theory-based implementation approach against a non-theory based approach for improving detection of LS amongst Australian patients with colorectal cancer (CRC).Methods: A two-arm parallel cluster randomised trial design will be used to compare two identical, structured implementation approaches, distinguished only by the use of theory to identify barriers and design targeted intervention strategies, to improve LS referral practices in eight large Australian hospital networks. Each hospital network will be randomly allocated to a trial arm, with stratification by state. A trained healthcare professional will lead the following phases at each site: (1) undertake baseline clinical practice audits, (2) form multidisciplinary Implementation Teams, (3) identify target behaviours for practice change, (4) identify barriers to change, (5) generate intervention strategies, (6) support staff to implement interventions and (7) evaluate the effectiveness of the intervention using post-implementation clinical data. The theoretical and non-theoretical components of each trial arm will be distinguished in phases 4-5. Study outcomes include a LS referral process map for each hospital network, with evaluation of the proportion of patients with risk-appropriate completion of the LS referral pathway within 2 months of CRC resection pre and post implementation.Discussion: This trial will determine the more effective approach for improving the detection of LS amongst patients with CRC, whilst also advancing understanding of the impact of theory-based implementation approaches in complex health systems and the feasibility of training healthcare professionals to use them. Insights gained will guide the development of future interventions to improve LS identification on a larger scale and across different contexts, as well as efforts to address the gap between evidence and practice in the rapidly evolving field of genomic research.Trial Registration: ANZCTR, ACTRN12618001072202 . Registered on 27 June 2018. [ABSTRACT FROM AUTHOR]

Published

2019

30. Lack of association between screening interval and cancer stage in Lynch syndrome may be accounted for by over-diagnosis; a prospective Lynch syndrome database report.

Author

Seppälä, Toni T., Ahadova, Aysel, Dominguez-Valentin, Mev, Macrae, Finlay, Evans, D. Gareth, Therkildsen, Christina, Sampson, Julian, Scott, Rodney, Burn, John, Möslein, Gabriela, Bernstein, Inge, Holinski-Feder, Elke, Pylvänäinen, Kirsi, Renkonen-Sinisalo, Laura, Lepistö, Anna, Lautrup, Charlotte Kvist, Lindblom, Annika, Plazzer, John-Paul, Winship, Ingrid, and Tjandra, Douglas

Subjects

HEREDITARY nonpolyposis colorectal cancer, COLON cancer, EARLY detection of cancer, COLONOSCOPY

Abstract

Background: Recent epidemiological evidence shows that colorectal cancer (CRC) continues to occur in carriers of pathogenic mismatch repair (path_MMR) variants despite frequent colonoscopy surveillance in expert centres. This observation conflicts with the paradigm that removal of all visible polyps should prevent the vast majority of CRC in path_MMR carriers, provided the screening interval is sufficiently short and colonoscopic practice is optimal. Methods: To inform the debate, we examined, in the Prospective Lynch Syndrome Database (PLSD), whether the time since last colonoscopy was associated with the pathological stage at which CRC was diagnosed during prospective surveillance. Path_MMR carriers were recruited for prospective surveillance by colonoscopy. Only variants scored by the InSiGHT Variant Interpretation Committee as class 4 and 5 (clinically actionable) were included. CRCs detected at the first planned colonoscopy, or within one year of this, were excluded as prevalent cancers. Results: Stage at diagnosis and interval between last prospective surveillance colonoscopy and diagnosis were available for 209 patients with 218 CRCs, including 162 path_MLH1, 45 path_MSH2, 10 path_MSH6 and 1 path_PMS2 carriers. The numbers of cancers detected within < 1.5, 1.5–2.5, 2.5–3.5 and at > 3.5 years since last colonoscopy were 36, 93, 56 and 33, respectively. Among these, 16.7, 19.4, 9.9 and 15.1% were stage III–IV, respectively (p = 0.34). The cancers detected more than 2.5 years after the last colonoscopy were not more advanced than those diagnosed earlier (p = 0.14). Conclusions: The CRC stage and interval since last colonoscopy were not correlated, which is in conflict with the accelerated adenoma-carcinoma paradigm. We have previously reported that more frequent colonoscopy is not associated with lower incidence of CRC in path_MMR carriers as was expected. In contrast, point estimates showed a higher incidence with shorter intervals between examinations, a situation that may parallel to over-diagnosis in breast cancer screening. Our findings raise the possibility that some CRCs in path_MMR carriers may spontaneously disappear: the host immune response may not only remove CRC precursor lesions in path_MMR carriers, but may remove infiltrating cancers as well. If confirmed, our suggested interpretation will have a bearing on surveillance policy for path_MMR carriers. [ABSTRACT FROM AUTHOR]

Published

2019

31. Worldwide Practice Patterns in Lynch Syndrome Diagnosis and Management, Based on Data From the International Mismatch Repair Consortium.

Author

Pan, Jennifer Y., Haile, Robert W., Templeton, Allyson, Macrae, Finlay, Qin, FeiFei, Sundaram, Vandana, and Ladabaum, Uri

Abstract

Background & Aims Families with a history of Lynch syndrome often do not adhere to guidelines for genetic testing and screening. We investigated practice patterns related to Lynch syndrome worldwide, to ascertain potential targets for research and public policy efforts. Methods We collected data from the International Mismatch Repair Consortium (IMRC), which comprises major research and clinical groups engaged in the care of families with Lynch syndrome worldwide. IMRC institutions were invited to complete a questionnaire to characterize diagnoses of Lynch syndrome and management practice patterns. Results Fifty-five providers, representing 63 of 128 member institutions (49%) in 21 countries, completed the questionnaire. For case finding, 55% of respondents reported participating in routine widespread population tumor testing among persons with newly diagnosed Lynch syndrome–associated cancers, whereas 27% reported relying on clinical criteria with selective tumor and/or germline analyses. Most respondents (64%) reported using multigene panels for germline analysis, and only 28% reported testing tumors for biallelic mutations for cases in which suspected pathogenic mutations were not confirmed by germline analysis. Respondents reported relying on passive dissemination of information to at-risk family members, and there was variation in follow through of genetic testing recommendations. Reported risk management practices varied—nearly all programs (98%) recommended colonoscopy every 1 to 2 years, but only 35% recommended chemoprevention with aspirin. Conclusions There is widespread heterogeneity in management practices for Lynch syndrome worldwide among IMRC member institutions. This may reflect the rapid pace of emerging technology, regional differences in resources, and the lack of definitive data for many clinical questions. Future efforts should focus on the large numbers of high-risk patients without access to state-of-the-art Lynch syndrome management. [ABSTRACT FROM AUTHOR]

Published

2018

32. The use of a risk assessment and decision support tool (CRISP) compared with usual care in general practice to increase risk-stratified colorectal cancer screening: study protocol for a randomised controlled trial.

Author

Walker, Jennifer G., Macrae, Finlay, Winship, Ingrid, Oberoi, Jasmeen, Saya, Sibel, Milton, Shakira, Bickerstaffe, Adrian, Dowty, James G., De Abreu Lourenço, Richard, Clark, Malcolm, Galloway, Louise, Fishman, George, Walter, Fiona M., Flander, Louisa, Chondros, Patty, Ait Ouakrim, Driss, Pirotta, Marie, Trevena, Lyndal, Jenkins, Mark A., and Emery, Jon D.

Subjects

*COLON cancer diagnosis, *RANDOMIZED controlled trials, *COLON cancer, *COLONOSCOPY, *CANCER prevention, *PRIMARY care

Abstract

Background: Australia and New Zealand have the highest incidence rates of colorectal cancer worldwide. In Australia there is significant unwarranted variation in colorectal cancer screening due to low uptake of the immunochemical faecal occult blood test, poor identification of individuals at increased risk of colorectal cancer, and over-referral of individuals at average risk for colonoscopy. Our pre-trial research has developed a novel Colorectal cancer RISk Prediction (CRISP) tool, which could be used to implement precision screening in primary care. This paper describes the protocol for a phase II multi-site individually randomised controlled trial of the CRISP tool in primary care.Methods: This trial aims to test whether a standardised consultation using the CRISP tool in general practice (the CRISP intervention) increases risk-appropriate colorectal cancer screening compared to control participants who receive standardised information on cancer prevention. Patients between 50 and 74 years old, attending an appointment with their general practitioner for any reason, will be invited into the trial. A total of 732 participants will be randomised to intervention or control arms using a computer-generated allocation sequence stratified by general practice. The primary outcome (risk-appropriate screening at 12 months) will be measured using baseline data for colorectal cancer risk and objective health service data to measure screening behaviour. Secondary outcomes will include participant cancer risk perception, anxiety, cancer worry, screening intentions and health service utilisation measured at 1, 6 and 12 months post randomisation.Discussion: This trial tests a systematic approach to implementing risk-stratified colorectal cancer screening in primary care, based on an individual's absolute risk, using a state-of-the-art risk assessment tool. Trial results will be reported in 2020.Trial Registration: Australian and New Zealand Clinical Trial Registry, ACTRN12616001573448p . Registered on 14 November 2016. [ABSTRACT FROM AUTHOR]

Published

2018

33. Re: Revised Bethesda Guidelines for Hereditary Nonpolyposis Colorectal Cancer (Lynch Syndrome) and Microsatellite Instability.

Author

Macrae, Finlay and Harris, Marion

Subjects

*LETTERS to the editor, *COLON cancer, *MICROSATELLITE repeats

Abstract

Presents a letter to the editor about the revised Bethesda Guidelines for hereditary nonpolyposis colorectal cancer and microsatellite instability.

Published

2005

34. Risk of Colorectal Cancer for Carriers of Mutations in MUTYH, With and Without a Family History of Cancer.

Author

Win, Aung Ko, Dowty, James G., Cleary, Sean P., Kim, Hyeja, Buchanan, Daniel D., Young, Joanne P., Clendenning, Mark, Rosty, Christophe, MacInnis, Robert J., Giles, Graham G., Boussioutas, Alex, Macrae, Finlay A., Parry, Susan, Goldblatt, Jack, Baron, John A., Burnett, Terrilea, Le Marchand, Loïc, Newcomb, Polly A., Haile, Robert W., and Hopper, John L.

Abstract

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. [Copyright &y& Elsevier]

Published

2014

35. Investigating rectal bleeding: red faced or reliable?

Author

Macrae, Finlay

Subjects

*RECTUM, *COLON cancer, *HEMORRHAGE

Abstract

Editorial. Comments on an article about rectal bleeding. Relationship between rectal bleeding and colorectal cancer; Incidence of colorectal cancer; Investigation of rectal bleeding.

Published

2001

36. Effect of Aspirin or Resistant Starch on Colorectal Neoplasia in the Lynch Syndrome.

Author

Burn, John, Bishop, D. Timothy, Mecklin, Jukka-Pekka, Macrae, Finlay, Möslein, Gabriela, Olschwang, Sylviane, Bisgaard, Marie-Luise, Ramesar, Raj, Eccles, Diana, Maher, Eamonn R., Bertario, Lucio, Jarvinen, Heikki J., Lindblom, Annika, Evans, D. Gareth, Lubinski, Jan, Morrison, Patrick J., Ho, Judy W.C., Vasen, Hans F.A., Side, Lucy, and Thomas, Huw J.W.

Subjects

*RANDOMIZED controlled trials, *COLON cancer, *ASPIRIN, *ADENOMA, *CANCER prevention, *GENETIC disorders

Abstract

Background: Observational and epidemiologic data indicate that the use of aspirin reduces the risk of colorectal neoplasia; however, the effects of aspirin in the Lynch syndrome (hereditary nonpolyposis colon cancer) are not known. Resistant starch has been associated with an antineoplastic effect on the colon. Methods: In a randomized, placebo-controlled trial, we used a two-by-two design to investigate the effects of aspirin, at a dose of 600 mg per day, and resistant starch (Novelose), at a dose of 30 g per day, in reducing the risk of adenoma and carcinoma among persons with the Lynch syndrome. Results: Among 1071 persons in 43 centers, 62 were ineligible to participate in the study, 72 did not enter the study, and 191 withdrew from the study. These three categories were equally distributed across the study groups. Over a mean period of 29 months (range, 7 to 74), colonic adenoma or carcinoma developed in 141 participants. Of 693 participants randomly assigned to receive aspirin or placebo, neoplasia developed in 66 participants receiving aspirin (18.9%), as compared with 65 receiving placebo (19.0%) (relative risk, 1.0; 95% confidence interval [CI], 0.7 to 1.4). There were no significant differences between the two groups with respect to the development of advanced neoplasia (7.4% and 9.9%, respectively; P=0.33). Among the 727 participants receiving resistant starch or placebo, neoplasia developed in 67 participants receiving starch (18.7%), as compared with 68 receiving placebo (18.4%) (relative risk, 1.0; 95% CI, 0.7 to 1.4). Advanced adenomas and colorectal cancers were evenly distributed in the two groups. The prevalence of serious adverse events was low, and the events were evenly distributed. Conclusions: The use of aspirin, resistant starch, or both for up to 4 years has no effect on the incidence of colorectal adenoma or carcinoma among carriers of the Lynch syndrome. (Current Controlled Trials number, ISRCTN59521990.) N Engl J Med 2008;359:2567-78. [ABSTRACT FROM AUTHOR]

Published

2008