Your search keyword '"Hammet F"' showing total 6 results

1. Population-based estimates of the age-specific cumulative risk of breast cancer for pathogenic variants in CHEK2: Findings from the australian breast cancer family registry.

Author

Southey M.C., Tsimiklis H., Winship I.M., Giles G.G., Milne R.L., Hopper J.L., Nguyen-dumont T.U., Dowty J.G., Steen J.A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., Rewse A., Southey M.C., Tsimiklis H., Winship I.M., Giles G.G., Milne R.L., Hopper J.L., Nguyen-dumont T.U., Dowty J.G., Steen J.A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., and Rewse A.

Abstract

Case-control studies of breast cancer have consistently shown that pathogenic variants in CHEK2 are associated with about a 3-fold increased risk of breast cancer. Information about the recurrent protein-truncating variant CHEK2 c.1100delC dominates this estimate. There have been no formal estimates of age-specific cumulative risk of breast cancer for all CHEK2 pathogenic (in-cluding likely pathogenic) variants combined. We conducted a population-based case-control-fam-ily study of pathogenic CHEK2 variants (26 families, 1071 relatives) and estimated the age-specific cumulative risk of breast cancer using segregation analysis. The estimated hazard ratio for carriers of pathogenic CHEK2 variants (combined) was 4.9 (95% CI 2.5-9.5) relative to non-carriers. The HR for carriers of the CHEK2 c.1100delC variant was estimated to be 3.5 (95% CI 1.02-11.6) and the HR for carriers of all other CHEK2 variants combined was estimated to be 5.7 (95% CI 2.5-12.9). The age-specific cumulative risk of breast cancer was estimated to be 18% (95% CI 11-30%) and 33% (95% CI 21-48%) to age 60 and 80 years, respectively. These findings provide important information for the clinical management of breast cancer risk for women carrying pathogenic variants in CHEK2.Copyright © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Published

2021

2. Rare germline pathogenic variants identified by multigene panel testing and the risk of aggressive prostate cancer.

Author

Milne R.L., Giles G.G., Nguyen-Dumont T., Dowty J.G., Macinnis R.J., Steen J.A., Riaz M., Dugue P.-A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., Tsimiklis H., Severi G., Bolton D., Lacaze P., Sebra R., Schadt E., McNeil J., Southey M.C., Milne R.L., Giles G.G., Nguyen-Dumont T., Dowty J.G., Macinnis R.J., Steen J.A., Riaz M., Dugue P.-A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., Tsimiklis H., Severi G., Bolton D., Lacaze P., Sebra R., Schadt E., McNeil J., and Southey M.C.

Abstract

While gene panel sequencing is becoming widely used for cancer risk prediction, its clinical utility with respect to predicting aggressive prostate cancer (PrCa) is limited by our current understanding of the genetic risk factors associated with predisposition to this potentially lethal disease phenotype. This study included 837 men diagnosed with aggressive PrCa and 7261 controls (unaffected men and men who did not meet criteria for aggressive PrCa). Rare germline pathogenic variants (including likely pathogenic variants) were identified by targeted sequencing of 26 known or putative cancer predisposition genes. We found that 85 (10%) men with aggressive PrCa and 265 (4%) controls carried a pathogenic variant (p < 0.0001). Aggressive PrCa odds ratios (ORs) were estimated using unconditional logistic regression. Increased risk of aggressive PrCa (OR (95% confidence interval)) was identified for pathogenic variants in BRCA2 (5.8 (2.7-12.4)), BRCA1 (5.5 (1.8-16.6)), and ATM (3.8 (1.6-9.1)). Our study provides further evidence that rare germline pathogenic variants in these genes are associated with increased risk of this aggressive, clinically relevant subset of PrCa. These rare genetic variants could be incorporated into risk prediction models to improve their precision to identify men at highest risk of aggressive prostate cancer and be used to identify men with newly diagnosed prostate cancer who require urgent treatment.Copyright © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Published

2021

3. Vtrna2-1: Genetic variation, heritable methylation and disease association.

Author

Dugue P.-A., Yu C., McKay T., Wong E.M., Joo J.E., Tsimiklis H., Hammet F., Mahmoodi M., Theys D., Kconfab, Hopper J.L., Giles G.G., Milne R.L., Steen J.A., Dowty J.G., Nguyen-dumont T., Southey M.C., Dugue P.-A., Yu C., McKay T., Wong E.M., Joo J.E., Tsimiklis H., Hammet F., Mahmoodi M., Theys D., Kconfab, Hopper J.L., Giles G.G., Milne R.L., Steen J.A., Dowty J.G., Nguyen-dumont T., and Southey M.C.

Abstract

VTRNA2-1 is a metastable epiallele with accumulating evidence that methylation at this region is heritable, modifiable and associated with disease including risk and progression of cancer. This study investigated the influence of genetic variation and other factors such as age and adult lifestyle on blood DNA methylation in this region. We first sequenced the VTRNA2-1 gene region in multiple-case breast cancer families in which VTRNA2-1 methylation was identified as heritable and associated with breast cancer risk. Methylation quantitative trait loci (mQTL) were investigated using a prospective cohort study (4500 participants with genotyping and methylation data). The cis-mQTL analysis (334 variants +/- 50 kb of the most heritable CpG site) identified 43 variants associated with VTRNA2-1 methylation (p < 1.5 x 10-4 ); however, these explained little of the methylation variation (R2 < 0.5% for each of these variants). No genetic variants elsewhere in the genome were found to strongly influence VTRNA2-1 methylation. SNP-based heritability estimates were consistent with the mQTL findings (h2 = 0, 95%CI: -0.14 to 0.14). We found no evidence that age, sex, country of birth, smoking, body mass index, alcohol consumption or diet influenced blood DNA methylation at VTRNA2-1. Genetic factors and adult lifestyle play a minimal role in explaining methylation var-iability at the heritable VTRNA2-1 cluster.Copyright © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Published

2021

4. Population-based estimates of the age-specific cumulative risk of breast cancer for pathogenic variants in CHEK2: Findings from the australian breast cancer family registry.

Author

Southey M.C., Tsimiklis H., Winship I.M., Giles G.G., Milne R.L., Hopper J.L., Nguyen-dumont T.U., Dowty J.G., Steen J.A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., Rewse A., Southey M.C., Tsimiklis H., Winship I.M., Giles G.G., Milne R.L., Hopper J.L., Nguyen-dumont T.U., Dowty J.G., Steen J.A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., and Rewse A.

Abstract

Case-control studies of breast cancer have consistently shown that pathogenic variants in CHEK2 are associated with about a 3-fold increased risk of breast cancer. Information about the recurrent protein-truncating variant CHEK2 c.1100delC dominates this estimate. There have been no formal estimates of age-specific cumulative risk of breast cancer for all CHEK2 pathogenic (in-cluding likely pathogenic) variants combined. We conducted a population-based case-control-fam-ily study of pathogenic CHEK2 variants (26 families, 1071 relatives) and estimated the age-specific cumulative risk of breast cancer using segregation analysis. The estimated hazard ratio for carriers of pathogenic CHEK2 variants (combined) was 4.9 (95% CI 2.5-9.5) relative to non-carriers. The HR for carriers of the CHEK2 c.1100delC variant was estimated to be 3.5 (95% CI 1.02-11.6) and the HR for carriers of all other CHEK2 variants combined was estimated to be 5.7 (95% CI 2.5-12.9). The age-specific cumulative risk of breast cancer was estimated to be 18% (95% CI 11-30%) and 33% (95% CI 21-48%) to age 60 and 80 years, respectively. These findings provide important information for the clinical management of breast cancer risk for women carrying pathogenic variants in CHEK2.Copyright © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Published

2021

5. Rare germline pathogenic variants identified by multigene panel testing and the risk of aggressive prostate cancer.

Author

Milne R.L., Giles G.G., Nguyen-Dumont T., Dowty J.G., Macinnis R.J., Steen J.A., Riaz M., Dugue P.-A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., Tsimiklis H., Severi G., Bolton D., Lacaze P., Sebra R., Schadt E., McNeil J., Southey M.C., Milne R.L., Giles G.G., Nguyen-Dumont T., Dowty J.G., Macinnis R.J., Steen J.A., Riaz M., Dugue P.-A., Renault A.-L., Hammet F., Mahmoodi M., Theys D., Tsimiklis H., Severi G., Bolton D., Lacaze P., Sebra R., Schadt E., McNeil J., and Southey M.C.

Abstract

While gene panel sequencing is becoming widely used for cancer risk prediction, its clinical utility with respect to predicting aggressive prostate cancer (PrCa) is limited by our current understanding of the genetic risk factors associated with predisposition to this potentially lethal disease phenotype. This study included 837 men diagnosed with aggressive PrCa and 7261 controls (unaffected men and men who did not meet criteria for aggressive PrCa). Rare germline pathogenic variants (including likely pathogenic variants) were identified by targeted sequencing of 26 known or putative cancer predisposition genes. We found that 85 (10%) men with aggressive PrCa and 265 (4%) controls carried a pathogenic variant (p < 0.0001). Aggressive PrCa odds ratios (ORs) were estimated using unconditional logistic regression. Increased risk of aggressive PrCa (OR (95% confidence interval)) was identified for pathogenic variants in BRCA2 (5.8 (2.7-12.4)), BRCA1 (5.5 (1.8-16.6)), and ATM (3.8 (1.6-9.1)). Our study provides further evidence that rare germline pathogenic variants in these genes are associated with increased risk of this aggressive, clinically relevant subset of PrCa. These rare genetic variants could be incorporated into risk prediction models to improve their precision to identify men at highest risk of aggressive prostate cancer and be used to identify men with newly diagnosed prostate cancer who require urgent treatment.Copyright © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Published

2021

6. Vtrna2-1: Genetic variation, heritable methylation and disease association.

Author

Dugue P.-A., Yu C., McKay T., Wong E.M., Joo J.E., Tsimiklis H., Hammet F., Mahmoodi M., Theys D., Kconfab, Hopper J.L., Giles G.G., Milne R.L., Steen J.A., Dowty J.G., Nguyen-dumont T., Southey M.C., Dugue P.-A., Yu C., McKay T., Wong E.M., Joo J.E., Tsimiklis H., Hammet F., Mahmoodi M., Theys D., Kconfab, Hopper J.L., Giles G.G., Milne R.L., Steen J.A., Dowty J.G., Nguyen-dumont T., and Southey M.C.

Abstract

VTRNA2-1 is a metastable epiallele with accumulating evidence that methylation at this region is heritable, modifiable and associated with disease including risk and progression of cancer. This study investigated the influence of genetic variation and other factors such as age and adult lifestyle on blood DNA methylation in this region. We first sequenced the VTRNA2-1 gene region in multiple-case breast cancer families in which VTRNA2-1 methylation was identified as heritable and associated with breast cancer risk. Methylation quantitative trait loci (mQTL) were investigated using a prospective cohort study (4500 participants with genotyping and methylation data). The cis-mQTL analysis (334 variants +/- 50 kb of the most heritable CpG site) identified 43 variants associated with VTRNA2-1 methylation (p < 1.5 x 10-4 ); however, these explained little of the methylation variation (R2 < 0.5% for each of these variants). No genetic variants elsewhere in the genome were found to strongly influence VTRNA2-1 methylation. SNP-based heritability estimates were consistent with the mQTL findings (h2 = 0, 95%CI: -0.14 to 0.14). We found no evidence that age, sex, country of birth, smoking, body mass index, alcohol consumption or diet influenced blood DNA methylation at VTRNA2-1. Genetic factors and adult lifestyle play a minimal role in explaining methylation var-iability at the heritable VTRNA2-1 cluster.Copyright © 2021 by the authors. Licensee MDPI, Basel, Switzerland.

Published

2021