Your search keyword '"Winship, Ingrid M."' showing total 9 results

1. Assessment of a Polygenic Risk Score for Colorectal Cancer to Predict Risk of Lynch Syndrome Colorectal Cancer.

Author

Jenkins, Mark A, Buchanan, Daniel D, Lai, John, Makalic, Enes, Dite, Gillian S, Win, Aung K, Clendenning, Mark, Winship, Ingrid M, Hayes, Richard B, Huyghe, Jeroen R, Peters, Ulrike, Gallinger, Steven, Marchand, Loïc Le, Figueiredo, Jane C, Pai, Rish K, Newcomb, Polly A, Church, James M, Casey, Graham, and Hopper, John L

Subjects

COLORECTAL cancer, DNA mismatch repair

Abstract

It was not known whether the polygenic risk scores (PRSs) that predict colorectal cancer could predict colorectal cancer for people with inherited pathogenic variants in DNA mismatch repair genes—people with Lynch syndrome. We tested a PRS comprising 107 established single-nucleotide polymorphisms associated with colorectal cancer in European populations for 826 European-descent carriers of pathogenic variants in DNA mismatch repair genes (293 MLH1 , 314 MSH2 , 126 MSH6 , 71 PMS2 , and 22 EPCAM) from the Colon Cancer Family Registry, of whom 504 had colorectal cancer. There was no evidence of an association between the PRS and colorectal cancer risk, irrespective of which DNA mismatch repair gene was mutated, or sex (all 2-sided P  >  .05). The hazard ratio per standard deviation of the PRS for colorectal cancer was 0.97 (95% confidence interval = 0.88 to 1.06; 2-sided P  =  .51). Whereas PRSs are predictive of colorectal cancer in the general population, they do not predict Lynch syndrome colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2021

2. The Impact of a Comprehensive Risk Prediction Model for Colorectal Cancer on a Population Screening Program.

Author

Saya, Sibel, Emery, Jon D, Dowty, James G, McIntosh, Jennifer G, Winship, Ingrid M, and Jenkins, Mark A

Subjects

COLON cancer, FECAL occult blood tests, COLONOSCOPY, CANCER, CANCER risk factors

Abstract

Background In many countries, population colorectal cancer (CRC) screening is based on age and family history, though more precise risk prediction could better target screening. We examined the impact of a CRC risk prediction model (incorporating age, sex, lifestyle, genomic, and family history factors) to target screening under several feasible screening scenarios. Methods We estimated the model's predicted CRC risk distribution in the Australian population. Predicted CRC risks were categorized into screening recommendations under 3 proposed scenarios to compare with current recommendations: 1) highly tailored, 2) 3 risk categories, and 3) 4 sex-specific risk categories. Under each scenario, for 35- to 74-year-olds, we calculated the number of CRC screens by immunochemical fecal occult blood testing (iFOBT) and colonoscopy and the proportion of predicted CRCs over 10 years in each screening group. Results Currently, 1.1% of 35- to 74-year-olds are recommended screening colonoscopy and 56.2% iFOBT, and 5.7% and 83.2% of CRCs over 10 years were predicted to occur in these groups, respectively. For the scenarios, 1) colonoscopy was recommended to 8.1% and iFOBT to 37.5%, with 36.1% and 50.1% of CRCs in each group; 2) colonoscopy was recommended to 2.4% and iFOBT to 56.0%, with 13.2% and 76.9% of cancers in each group; and 3) colonoscopy was recommended to 5.0% and iFOBT to 54.2%, with 24.5% and 66.5% of cancers in each group. Conclusions A highly tailored CRC screening scenario results in many fewer screens but more cancers in those unscreened. Category-based scenarios may provide a good balance between number of screens and cancers detected and are simpler to implement. [ABSTRACT FROM AUTHOR]

Published

2020

3. Insights into sudden cardiac death: exploring the potential relevance of non-diagnostic autopsy findings.

Author

Raju, Hariharan, Parsons, Sarah, Thompson, Tina N, Morgan, Natalie, Zentner, Dominica, Trainer, Alison H, James, Paul A, Winship, Ingrid M, Kalman, Jonathan M, and Vohra, Jitendra

Abstract

View large Download slide View large Download slide Aims Unexplained sudden cardiac death (SCD) may be attributable to cardiogenetic disease. Presence or absence of autopsy anomalies detected following premature sudden death direct appropriate clinical evaluation of at-risk relatives towards inherited cardiomyopathies or primary arrhythmia syndromes, respectively. We investigated the relevance of non-diagnostic pathological abnormalities of indeterminate causality (uncertain) such as myocardial hypertrophy, fibrosis, or inflammatory infiltrates to SCD. Methods and results At-risk relatives of unexplained SCD cases aged 1–64 years without prior cardiac disease (n  = 98) with either normal and negative (40%, true sudden arrhythmic death syndrome; SADS) or isolated non-diagnostic (60%, uncertain sudden unexplained death; SUD) cardiac histological autopsy findings at a central forensic pathology unit were referred to the regional unexplained SCD clinic for clinical cardiac phenotyping. Uncertain SUD were older than true SADS cases (31.8 years vs. 21.1 years, P  < 0.001). A cardiogenetic diagnosis was established in 24 families (24.5%) following investigation of 346 referred relatives. The proportions of uncertain SUD and true SADS explained by familial cardiogenetic diagnoses were similar (20% vs. 31%, P  = 0.34, respectively), with primary arrhythmia syndromes predominating. Unexplained SCD cases were more likely than matched non-cardiac premature death controls to demonstrate at least one uncertain autopsy finding (P  < 0.001). Conclusion Primary arrhythmia syndromes predominate as familial cardiogenetic diagnoses amongst both uncertain SUD and true SADS cases. Non-diagnostic or uncertain histological findings associate with SUD, though cannot be attributed a causative status. At-risk relatives of uncertain SUD cases should be evaluated for phenotypic evidence of both ion channel disorders and cardiomyopathies. [ABSTRACT FROM AUTHOR]

Published

2019

4. 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

5. Aspirin, Ibuprofen, and the Risk of Colorectal Cancer in Lynch Syndrome.

Author

Ouakrim, Driss Ait, Dashti, Seyedeh Ghazaleh, Chau, Rowena, Buchanan, Daniel D., Clendenning, Mark, Rosty, Christophe, Winship, Ingrid M., Young, Joanne P., Giles, Graham G., Leggett, Barbara, Macrae, Finlay A., Ahnen, Dennis J., Casey, Graham, Gallinger, Steven, Haile, Robert W., Le Marchand, Loïc, Thibodeau, Stephen N., Lindor, Noralane M., Newcomb, Polly A., and Potter, John D.

Subjects

TUMOR prevention, COLON tumor prevention, ADENOSINE triphosphatase, ANTINEOPLASTIC agents, ASPIRIN, CARRIER proteins, COLON tumors, DNA, ENZYMES, GENETIC mutation, NONSTEROIDAL anti-inflammatory agents, PROTEINS, QUESTIONNAIRES, RECTUM tumors, RESEARCH funding, IBUPROFEN, DNA-binding proteins, RESEARCH bias, ACQUISITION of data, DISEASE prevalence, PROPORTIONAL hazards models, NUCLEAR proteins, GENETIC carriers, HEREDITARY nonpolyposis colorectal cancer, CONFOUNDING variables

Abstract

Background: Inheritance of a germline mutation in one of the DNA mismatch repair (MMR) genes MLH1, MSH2, MSH6, and PMS2 causes a high risk of colorectal and other cancers (Lynch Syndrome). Use of aspirin has been shown to be associated with a reduced risk of colorectal cancer for the general population as well as for MMR gene mutation carriers. The aim of this study was to determine whether use of aspirin and ibuprofen in a nontrial setting is associated with the risk of colorectal cancer risk for MMR gene mutation carriers. Methods: We included 1858 participants in the Colon Cancer Family Registry who had been found to have a pathogenic germline mutation in a MMR gene (carriers). We used weighted Cox proportional hazards regression to estimate hazard ratios (HRs) and 95% confidence intervals (CIs). All statistical tests were two-sided. Results: A total of 714 carriers (38%) were diagnosed with colorectal cancer at a mean age of 42.4 (standard deviation 10.6) years. A reduced risk of colorectal cancer was associated with aspirin use (for 1 month to 4.9 years: HR = 0.49, 95% CI = 0.27 to 0.90, P = .02; for ≥5 years: HR = 0.25, 95% CI = 0.10 to 0.62, P = .003) and ibuprofen use (for 1 month to 4.9 years: HR = 0.38, 95% CI = 0.18 to 0.79, P = .009; for ≥5 years: HR = 0.26, 95% CI = 0.10 to 0.69, P = .007), compared with less than one month of use. Conclusion: Our results provide additional evidence that, for MMR gene mutation carriers, use of aspirin and ibuprofen might be effective in reducing their high risk of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2015

6. 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

7. An investigation into FOXE1 polyalanine tract length in premature ovarian failure.

Author

Watkins, Wendy J., Harris, Sarah E., Craven, Megan J., Vincent, Andrea L., Winship, Ingrid M., Gersak, Ksenija, and Shelling, Andrew N.

Published

2006

8. INHA promoter polymorphisms are associated with premature ovarian failure.

Author

Harris, Sarah E., Chand, Ashwini L., Winship, Ingrid M., Gersak, Ksenija, Nishi, Yoshihiro, Yanase, Toshihiko, Nawata, Hajime, and Shelling, Andrew N.

Published

2005

9. Inhibin: a candidate gene for premature ovarian failure.

Author

Shelling, Andrew N., Burton, Karen A., Chand, Ashwini L., van Ee, Cynthia C., France, John T., Farquhar, Cynthia M., Milsom, Stella R., Love, Donald R., Gersak, Ksenija, Aittomaki, Kristiina, Winship, Ingrid M., Shelling, A N, Burton, K A, Chand, A L, van Ee, C C, France, J T, Farquhar, C M, Milsom, S R, Love, D R, and Gersak, K

Abstract

Premature ovarian failure (POF) occurs in 1% of all women, and in 0.1% of women under the age of 30 years. The mechanisms that give rise to POF are largely unknown. Inhibin has a role in regulating the pituitary secretion of FSH, and is therefore a potential candidate gene for ovarian failure. Using single-stranded conformation polymorphism (SSCP) and DNA sequencing, DNA samples were screened from 43 women with POF for mutations in the three inhibin genes. Two variants were found: a 1032C-->T transition in the INHssA gene in one patient, and a 769G-->A transition in the INHalpha gene in three patients. The INHssA variant appears to be a polymorphism, as there was no change in the amino acid sequence of the gene product. The INHalpha variant resulted in a non-conservative amino acid change, with a substitution from alanine to threonine. This alanine is highly conserved across species, and has the potential to affect receptor binding. The INHalpha variant is significantly associated with POF (3/43 patients; 7%) compared with control samples (1/150 normal controls; 0.7%) (Fisher's exact test, P < 0.035). Further analysis of the inhibin gene in POF patients and matched controls will determine its role in the aetiology of POF. [ABSTRACT FROM AUTHOR]

Published

2000