Your search keyword '"Rita Barfoot"' showing total 23 results

1. A multicenter study of cancer incidence in CHEK2 1100delC mutation carriers

Author

Sheila Seal, Barbara L. Weber, Jenny Chang-Claude, Lesley McGuffog, Jan Klijn, Rosalind A. Eeles, P. Andrew Futreal, Katherine L. Nathanson, Nazneen Rahman, Rita Barfoot, Mieke Schutte, Richard S. Houlston, Michael R. Stratton, Deborah J. Thompson, Anthony Renwick, Hanne Meijers-Heijboer, Marijke Wasielewski, Douglas F. Easton, Nayanta Sodha, Susan Shanley, Human Genetics, Medical Oncology, and Clinical Genetics

Subjects

Male, Risk, Oncology, medicine.medical_specialty, Pathology, Epidemiology, Colorectal cancer, Population, Breast Neoplasms, Protein Serine-Threonine Kinases, Article, Prostate cancer, Sex Factors, Breast cancer, SDG 3 - Good Health and Well-being, Germany, Neoplasms, Internal medicine, Genotype, Humans, Medicine, Lung cancer, education, Netherlands, education.field_of_study, business.industry, Genetic Carrier Screening, Incidence, Cancer, medicine.disease, United Kingdom, United States, Checkpoint Kinase 2, Relative risk, Mutation, Female, business

Abstract

The CHEK2 1100delC protein-truncating mutation has a carrier frequency of ∼0.7% in Northern and Western European populations and confers an ∼2-fold increased risk of breast cancer. It has also been suggested to increase risks of colorectal and prostate cancer, but its involvement with these or other types of cancer has not been confirmed. The incidence of cancer other than breast cancer in 11,116 individuals from 734 non-BRCA1/2 breast cancer families from the United Kingdom, Germany, Netherlands, and the United States was compared with that predicted by population rates. Relative risks (RR) to carriers and noncarriers were estimated by maximum likelihood, via the expectation-maximization algorithm to allow for unknown genotypes. Sixty-seven families contained at least one tested CHEK2 1100delC mutation carrier. There was evidence of underreporting of cancers in male relatives (422 cancers observed, 860 expected) but not in females (322 observed, 335 expected); hence, we focused on cancer risks in female carriers. The risk of cancers other than breast cancer in female carriers was not significantly elevated, although a modest increase in risk could not be excluded (RR, 1.18; 95% confidence interval, 0.64-2.17). The carrier risk was not significantly raised for any individual cancer site, including colorectal cancer (RR, 1.60; 95% confidence interval, 0.54-4.71). However, between ages 20 to 50 years, the risks of colorectal and lung cancer were both higher in female carriers than noncarriers (P = 0.041 and 0.0001, respectively). There was no evidence of a higher prostate cancer risk in carriers than noncarriers (P = 0.26), although underreporting of male cancers limited our power to detect such a difference. Our results suggest that the risk of cancer associated with CHEK2 1100delC mutations is restricted to breast cancer, although we cannot rule out a small increase in overall cancer risk. (Cancer Epidemiol Biomarkers Prev 2006;15(12):2542–5)

Published

2006

2. Case of interstitial 12q deletion in association with Wilms tumor

Author

Elizabeth A. Rapley, Kathy Pritchard-Jones, Isobel Moore, Darren Hargrave, Martin Radford, Michael R. Stratton, Nazneen Rahman, Nina Persinguhe, and Rita Barfoot

Subjects

Family Health, Male, Genetics, Chromosomes, Human, Pair 12, Genotype, Infant, Chromosome, Locus (genetics), Wilms' tumor, DNA, Biology, medicine.disease, Wilms Tumor, Genetic predisposition, medicine, Humans, Female, Chromosome Deletion, Lod Score, Allele, Gene, Genetics (clinical), Chromosome 12, Microsatellite Repeats

Abstract

A 14-month-old boy presenting with Wilms tumor (WT) was found to have a small de novo deletion of the long arm of chromosome 12 (12q11-12q13.11). Microsatellite analysis of this region from constitutional DNA showed that the paternal allele was absent between the markers D12S331 and D12S1713 (inclusive). In the WT there was no evidence of loss of the maternal chromosome. Constitutional chromosome abnormalities can often point to the presence of genes that are important in disease, and the deletion of chromosome 12 in this patient may indicate a gene involved in WT. To determine whether a WT predisposition locus exists at 12q we examined the region in two familial Wilms tumor (FWT) pedigrees unlinked to the known FWT genes on chromosomes 17q (FWT1), 19q (FWT2), and 11p (WT1). In both families WT did not segregate with chromosome 12q markers located within the deletion boundaries.

Published

2001

3. Allelotype of Uterine Leiomyomas

Author

Rita Barfoot, Michael R. Stratton, Douglas F. Easton, Adrienne M. Flanagan, Rifat Hamoudi, and Xin Mao

Subjects

Cancer Research, Loss of Heterozygosity, Biology, Benign tumor, Loss of heterozygosity, Genetics, Genetic predisposition, medicine, Humans, Genetic Predisposition to Disease, Allele, Allelotype, neoplasms, Molecular Biology, Alleles, Uterine leiomyoma, Leiomyoma, Myometrium, medicine.disease, Haplotypes, Uterine Neoplasms, Cancer research, Female, Chromosomes, Human, Pair 7, Microsatellite Repeats

Abstract

Uterine leiomyomas are the most common benign tumor that arise from smooth muscle cells of the myometrium. Little is known about the etiology and pathogenesis of this tumor. To investigate the molecular pathogenesis of these tumors, we have conducted an allelotype of 102 leiomyomas from 12 patients, using 67 fluorescently-tagged oligonucleotide primers amplifying microsatellite loci covering all autosomes. No areas of the genome showed frequent loss of heterozygosity (LOH); however, the highest rate of LOH (9%) was observed on 7q, consistent with previous cytogenetic observations. Uterine leiomyomas are sometimes multiple. In general, multiplicity of other types of neoplasm is associated with genetic predisposition to the disease. Because multiple tumors were available from each of the 12 patients studied, we looked for evidence of allele-specific LOH, which might indicate the presence of an underlying predisposition gene. However, no evidence for allele-specific LOH was detected, indicating that if cases of multiple uterine leiomyoma are due to an underlying predisposition gene, it is unlikely to be a recessive oncogene.

Published

1999

4. The Gene for Cherubism Maps to Chromosome 4p16.3

Author

John V. Townend, Adrienne M. Flanagan, Sarah Edkins, Jonathan Mangion, Michael R. Stratton, Rita Barfoot, David R. FitzPatrick, Asgeir Sigurdsson, Trang Nguyen, and Nazneen Rahman

Subjects

Adult, Genetic Markers, Male, Genetic-linkage analysis, Locus (genetics), Biology, Gene mapping, SH3BP2, Genetics, medicine, Humans, Genetics(clinical), Genetics (clinical), Chromosome Mapping, Cherubism, Chromosome, Fibroblast growth factor receptor 3, medicine.disease, Osteochondrodysplasia, Pedigree, Genetic marker, Chromosome 4p, Female, Chromosomes, Human, Pair 4, Lod Score, Research Article

Abstract

Summary Cherubism is a rare familial disease of childhood characterized by proliferative lesions within the mandible and maxilla that lead to prominence of the lower face and an appearance reminiscent of the cherubs portrayed in Renaissance art. Resolution of these bony abnormalities is often observed after puberty. Many cases are inherited in an autosomal dominant fashion, although several cases without a family history have been reported. Using two families with clinically, radiologically, and/or histologically proved cherubism, we have performed a genomewide linkage search and have localized the gene to chromosome 4p16.3, with a maximum multipoint LOD score of 5.64. Both families showed evidence of linkage to this locus. Critical meiotic recombinants place the gene in a 3-cM interval between D4S127 and 4p-telomere. Within this region a strong candidate is the gene for fibroblast growth factor receptor 3 (FGFR3); mutations in this gene have been implicated in a diverse set of disorders of bone development.

Published

1999

5. Prevalence of BRCA1 and BRCA2 Gene Mutations in Patients With Early-Onset Breast Cancer

Author

Judith Deacon, Sheila Seal, Julian Peto, Christopher H. Evans, Rita Barfoot, N. Collins, Michael R. Stratton, Douglas F. Easton, William H. Warren, and Nazneen Rahman

Subjects

Adult, Risk, Cancer Research, medicine.medical_specialty, Pathology, endocrine system diseases, Population, Genes, BRCA1, Breast Neoplasms, Gene mutation, Breast cancer, Internal medicine, Prevalence, Humans, Medicine, Genes, Tumor Suppressor, Genetic Predisposition to Disease, Risk factor, skin and connective tissue diseases, education, education.field_of_study, business.industry, Incidence, Incidence (epidemiology), Middle Aged, medicine.disease, Penetrance, United Kingdom, Standardized mortality ratio, Oncology, Case-Control Studies, Population Surveillance, Mutation, Female, business, Ovarian cancer

Abstract

Background Mutations in the BRCA1 and BRCA2 genes are found in most families with cases of both breast and ovarian cancer or with many cases of early-onset breast cancer. However, in an outbred population, the prevalence of BRCA1 and BRCA2 mutations in patients with breast cancer who were unselected for a family history of this disease has not been determined. Methods Mutations in the BRCA1 and BRCA2 genes were detected in blood samples from two population-based series of young patients with breast cancer from Britain. Results Mutations were detected in 15 (5.9%) of 254 women diagnosed with breast cancer before age 36 years (nine [3.5%] in BRCA1 and six [2.4%] in BRCA2) and in 15 (4.1%) of 363 women diagnosed from ages 36 through 45 years (seven [1.9%] in BRCA1 and eight [2.2%] in BRCA2). Eleven percent (six of 55) of patients with a first-degree relative who developed ovarian cancer or breast cancer by age 60 years were mutation carriers, compared with 45% (five of 11) of patients with two or more affected first- or second-degree relatives. The standardized incidence ratio for breast cancer in mothers and sisters was 365 (five observed and 1.37 expected) for 30 mutation carriers and 199 (64 observed and 32.13 expected) for 587 noncarriers. If we assume recent penetrance estimates, the respective proportions of BRCA1 and BRCA2 mutation carriers are 3.1% and 3.0%, respectively, of patients with breast cancer who are younger than age 50 years, 0.49% and 0.84% of patients with breast cancer who are age 50 years or older, and 0.11% and 0.12% of women in the general population. Conclusions Mutations in the BRCA1 and BRCA2 genes make approximately equal contributions to early-onset breast cancer in Britain and account for a small proportion of the familial risk of breast cancer.

Published

1999

6. Heterozygosity for mutations in the ataxia telangiectasia gene is not a major cause of radiotherapy complications in breast cancer patients

Author

Richard Wooster, Judith M Bliss, M Moohan, Rita Barfoot, Nazneen Rahman, Michael R. Stratton, A. Ashton, Sheila Seal, Roger G. Owen, N. Collins, J. Regan, M Shayeghi, and John Yarnold

Subjects

Oncology, Heterozygote, Cancer Research, medicine.medical_specialty, Pathology, medicine.medical_treatment, Molecular Sequence Data, Breast Neoplasms, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, Protein Serine-Threonine Kinases, Biology, Radiation Tolerance, Loss of heterozygosity, Ataxia Telangiectasia, Breast cancer, Internal medicine, medicine, Humans, Radiosensitivity, Base Sequence, Tumor Suppressor Proteins, Dose fractionation, Proteins, Cancer, medicine.disease, DNA-Binding Proteins, Radiation therapy, Ataxia-telangiectasia, Female, Dose Fractionation, Radiation, Oligonucleotide Probes, Research Article

Abstract

Of patients being treated by radiotherapy for cancer, a small proportion develop marked long-term radiation damage. It is believed that this is due, at least in part, to intrinsic individual differences in radiosensitivity, but the underlying mechanism is unknown. Individuals affected by the recessive disease ataxia telangiectasia (AT) exhibit extreme sensitivity to ionizing radiation. Cells from such individuals are also radiosensitive in in vitro assays, and cells from AT heterozygotes are reported to show in vitro radiosensitivity at an intermediate level between homozygotes and control subjects. In order to examine the possibility that a defect in the ATM gene may account for a proportion of radiotherapy complications, 41 breast cancer patients developing marked changes in breast appearance after radiotherapy and 39 control subjects who showed no clinically detectable reaction after radiotherapy were screened for mutations in the ATM gene. One out of 41 cases showing adverse reactions was heterozygous for a mutation (insertion A at NT 898) that is predicted to generate a truncated protein of 251 amino acids. No truncating mutations were detected in the control subjects. On the basis of this result, the estimated percentage (95% confidence interval) of AT heterozygous patients in radiosensitive cases was 2.4% (0.1-12.9%) and in control subjects (0-9.0%). We conclude that ATM gene defects are not the major cause of radiotherapy complications in women with breast cancer.

Published

1998

7. A missense mutation in the BRCA2 gene in three siblings with ovarian cancer

Author

Lauri A. Aaltonen, Shayehgi M, Annika Auranen, Michael R. Stratton, Ralf Bützow, N. Collins, Sheila Seal, Rita Barfoot, Laura Sarantaus, Seija Grénman, Nazneen Rahman, Alan Ashworth, Stina Roth, Klemi Pj, P. Kristo, and Heli Nevanlinna

Subjects

Male, Cancer Research, endocrine system diseases, Genetic Linkage, medicine.disease_cause, Polymerase Chain Reaction, Mice, 0302 clinical medicine, Missense mutation, skin and connective tissue diseases, Ovarian Neoplasms, Genetics, 0303 health sciences, Mutation, Middle Aged, BRCA2 Protein, female genital diseases and pregnancy complications, Neoplasm Proteins, Pedigree, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Cystadenocarcinoma, Papillary, Female, Research Article, Adult, Genetic Markers, Molecular Sequence Data, Biology, Nuclear Family, 03 medical and health sciences, medicine, Animals, Humans, Point Mutation, Neoplastic transformation, Amino Acid Sequence, Aged, DNA Primers, Neoplasm Staging, 030304 developmental biology, Sequence Homology, Amino Acid, Point mutation, Cancer, medicine.disease, Cancer research, Ovarian cancer, Carcinogenesis, Chickens, Transcription Factors

Abstract

Inherited susceptibility to ovarian cancer has been associated with germline defects at several loci. The major known ovarian cancer susceptibility gene is BRCA1 on chromosome 17q, which confers a risk of approximately 60% by the age of 70 years. Truncating mutations in BRCA2 on chromosome 13q also predispose to ovarian cancer, although they confer a lower risk than mutations in BRCA1. We have studied the molecular basis of ovarian cancer predisposition in a Finnish family with three affected sisters. Analysis of polymorphic markers provided evidence against linkage to BRCA1, but the sibship was consistent with linkage to BRCA2. Conformation-sensitive gel electrophoresis was used to screen the entire coding sequence of BRCA2. A G to A transition at nucleotide 8702 was observed, which is predicted to convert glycine 2901 to aspartate in the encoded protein. This sequence variant was not detected in 220 cancer-free Finnish control individuals, or in several hundred cancer families of many nationalities previously screened for BRCA2 mutations. Taken together with the fact that this amino acid residue and the surrounding region of BRCA2 is identical in mouse and chicken, the data suggest that this alteration is a disease-causing BRCA2 missense mutation. Previously published data indicate that the risks of breast and ovarian cancer conferred by BRCA2-truncating mutations varies with the position of the mutation in the gene. The missense mutation reported here suggests that the BRCA2 domain including and surrounding glycine 2901 may be more important in preventing neoplastic transformation in ovarian epithelium than in breast epithelium. Images Figure 1

Published

1998

8. Candidate regions for testicular cancer susceptibility genes

Author

Douglas F. Easton, Gillian P. Crockford, Michael R. Stratton, Elizabeth A. Rapley, Robert Huddart, J. G. Bodmer, Michael Leahy, Colin Cooper, Michael Friedlander, Paul Goss, Jenny Donald, D. Timothy Bishop, Ian Thomlinson, David Hogg, Sandeep Patel, R. Timothy D. Oliver, Sophie D. Fosså, Dawn Teare, Jonathon Moses, Fellicity Collins, Rita Barfoot, Susan Tonks, Rachael Hunter, Ketil Heimdal, Rifat Hamoudi, Hong Qi Peng, Katherine M. Tucker, Sandra Gill, Sheila Seal, Patrick J. Biggs, and David Forman

Subjects

Microbiology (medical), Genetics, Susceptibility gene, General Medicine, Biology, medicine.disease, Genome, Pathology and Forensic Medicine, Family studies, Etiology, medicine, Immunology and Allergy, Testis cancer, Gene, Testicular cancer

Abstract

Although the aetiology of testicular cancer is unknown, a clear familial component has been identified in a number of studies. In an effort to identify susceptibility genes for testicular cancer, the International Testis Cancer Linkage Consortium has been collecting families with multiple cases of testicular cancer. These families have been genotyped for a set of markers across the genome in two separate studies. The family information has also been pooled across the two studies so that the combined evidence can be assessed. While no genomic region gives overwhelming support for a testicular cancer predisposition gene, several regions, notably on chromosomes 3, 5, 12 and 18 show suggestive evidence worthy of further examination. The Consortium is now attempting to identify further families in an attempt to confirm or deny these leads.

Published

1998

9. [Untitled]

Author

Rifat Hamoudi, Rita Barfoot, Mark Noble, and Xin Mao

Subjects

Genetics, Cancer Research, Lineage (genetic), Biology, medicine.disease_cause, Oligodendrocyte, Cell biology, medicine.anatomical_structure, Neurology, Oncology, Cell culture, Precursor cell, medicine, Human genome, Neurology (clinical), Progenitor cell, Carcinogenesis, Astrocyte

Abstract

We have conducted alleletyping of two novel cell lines derived from glioblastoma multiforme, which appear to have arisen from different glial lineages, by using 76 fluorescently labeled oligonucleotide primers amplifying microsatellite loci covering the entire human genome. One cell line, Hu-O-2A/Gb1, expresses antigens and metabolic profiles characteristic of the oligodendrocyte-type-2 astrocyte (0-2A) lineage of the rat central nervous system. This cell line generated, in vitro, cells with characteristics of 0-2A progenitor cells, oligodendrocytes and astrocytes. The second cell line, IN1434, is derived from an astrocyte or a precursor cell restricted to astrocytic differentiation. Hu-O-2A/Gb1 cells show allelic losses of loci on chromosomes 2, 5, 6, 7, 8, 9, 10, 11, 13, 15, 16, 17, 20 and 21. IN1434 cells are likely to have allelic losses of loci on chromosomes 1, 3, 8 and 10, although no control DNA is available for this cell line. These results, for the first time, provide a detailed information of the molecular genetic defects occurring in Hu-O-2A/Gb1 and IN1434.

Published

1998

10. Truncating mutations in the Fanconi anemia J gene BRIP1 are low-penetrance breast cancer susceptibility alleles

Author

Douglas F. Easton, Bernard North, D. Gareth Evans, Anna Elliott, Katarina Spanova, Diana Eccles, Tasnim Chagtai, Anthony Renwick, Hiran Jayatilake, Nazneen Rahman, Munaza Ahmed, Rita Barfoot, Michael R. Stratton, Deborah J. Thompson, Sheila Seal, Lesley McGuffog, and Patrick Kelly

Subjects

Adult, PALB2, Breast Neoplasms, Penetrance, Biology, medicine.disease_cause, Breast cancer, Gene Frequency, Fanconi anemia, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, skin and connective tissue diseases, Mutation, Genetic Carrier Screening, BRIP1, Middle Aged, medicine.disease, Fanconi Anemia Complementation Group Proteins, Pedigree, DNA-Binding Proteins, Codon, Nonsense, Cancer research, RAD51C, RNA Helicases

Abstract

We identified constitutional truncating mutations of the BRCA1-interacting helicase BRIP1 in 9/1,212 individuals with breast cancer from BRCA1/BRCA2 mutation-negative families but in only 2/2,081 controls (P = 0.0030), and we estimate that BRIP1 mutations confer a relative risk of breast cancer of 2.0 (95% confidence interval = 1.2-3.2, P = 0.012). Biallelic BRIP1 mutations were recently shown to cause Fanconi anemia complementation group J. Thus, inactivating truncating mutations of BRIP1, similar to those in BRCA2, cause Fanconi anemia in biallelic carriers and confer susceptibility to breast cancer in monoallelic carriers.

Published

2006

11. ATM mutations that cause ataxia-telangiectasia are breast cancer susceptibility alleles

Author

Nazneen Rahman, Douglas F. Easton, D. Gareth Evans, Tasnim Chagtai, Patrick Kelly, Bernard North, Katarina Spanova, Sheila Seal, Hiran Jayatilake, Lesley McGuffog, Diana Eccles, Deborah J. Thompson, Munaza Ahmed, Rita Barfoot, Michael R. Stratton, and Anthony Renwick

Subjects

Male, PALB2, Breast Neoplasms, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, Protein Serine-Threonine Kinases, Biology, medicine.disease_cause, Ataxia Telangiectasia, Breast cancer, Genetics, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Allele, Alleles, Mutation, Tumor Suppressor Proteins, BRIP1, Case-control study, medicine.disease, Pedigree, DNA-Binding Proteins, Case-Control Studies, Immunology, Ataxia-telangiectasia, Cancer research, Female

Abstract

We screened individuals from 443 familial breast cancer pedigrees and 521 controls for ATM sequence variants and identified 12 mutations in affected individuals and two in controls (P = 0.0047). The results demonstrate that ATM mutations that cause ataxia-telangiectasia in biallelic carriers are breast cancer susceptibility alleles in monoallelic carriers, with an estimated relative risk of 2.37 (95% confidence interval (c.i.) = 1.51-3.78, P = 0.0003). There was no evidence that other classes of ATM variant confer a risk of breast cancer.

Published

2006

12. DICER1 syndrome: clarifying the diagnosis, clinical features and management implications of a pleiotropic tumour predisposition syndrome

Author

Ingrid Slade, Bruce Morland, Derek J. King, Charles A. Stiller, Kathryn Pritchard-Jones, Clare Turnbull, Lucy Side, Sucheta Vaidya, Anne Murray, Helen Davies, Katrina Prescott, Barry Pizer, Paul Ward, Heidi Traunecker, Rita Barfoot, Anand Saggar, Richard S. Houlston, Helen Jenkinson, Sandra Hanks, Michael R. Stratton, Gordan M. Vujanic, Andrew G. Nicholson, Julia C. Chisholm, Nazneen Rahman, P. Andrew Futreal, Martin Hewitt, Amos Burke, Fatemeh Abbaszadeh, Jenny Douglas, John R. Priest, Neil J. Sebire, and Chiara Bacchelli

Subjects

Ribonuclease III, endocrine system, Molecular Sequence Data, Pleuropulmonary blastoma, Haploinsufficiency, Biology, medicine.disease_cause, DEAD-box RNA Helicases, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Neoplasms, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, Genetics (clinical), Germ-Line Mutation, 030304 developmental biology, DICER1 Syndrome, Medulloblastoma, 0303 health sciences, Mutation, Cystic nephroma, Cancer, Sequence Analysis, DNA, Syndrome, medicine.disease, 3. Good health, 030220 oncology & carcinogenesis, Cancer research

Abstract

BACKGROUND: Constitutional DICER1 mutations were recently reported to cause familial pleuropulmonary blastoma (PPB). AIM: To investigate the contribution and phenotypic spectrum of constitutional and somatic DICER1 mutations to cancer. METHODS AND RESULTS: The authors sequenced DICER1 in constitutional DNA from 823 unrelated patients with a variety of tumours and in 781 cancer cell lines. Constitutional DICER1 mutations were identified in 19 families including 11/14 with PPB, 2/3 with cystic nephroma, 4/7 with ovarian Sertoli-Leydig-type tumours, 1/243 with Wilms tumour (this patient also had a Sertoli-Leydig tumour), 1/1 with intraocular medulloepithelioma (this patient also had PPB), 1/86 with medulloblastoma/infratentorial primitive neuroectodermal tumour, and 1/172 with germ cell tumour. The inheritance was investigated in 17 families. DICER1 mutations were identified in 25 relatives: 17 were unaffected, one mother had ovarian Sertoli-Leydig tumour, one half-sibling had cystic nephroma, and six relatives had non-toxic thyroid cysts/goitre. Analysis of eight tumours from DICER1 mutation-positive patients showed universal retention of the wild-type allele. DICER1 truncating mutations were identified in 4/781 cancer cell lines; all were in microsatellite unstable lines and therefore unlikely to be driver mutations. CONCLUSION: Constitutional DICER1 haploinsufficiency predisposes to a broad range of tumours, making a substantial contribution to PPB, cystic nephroma and ovarian Sertoli-Leydig tumours, but a smaller contribution to other tumours. Most mutation carriers are unaffected, indicating that tumour risk is modest. The authors define the clinical contexts in which DICER1 mutation testing should be considered, the associated tumour risks, and the implications for at-risk individuals. They have termed this condition 'DICER1 syndrome'. ACCESSION NUMBERS: The cDNA Genbank accession number for the DICER1 sequence reported in this paper is NM_030621.2.

Published

2011

13. PALB2, which encodes a BRCA2-interacting protein, is a breast cancer susceptibility gene

Author

D. Gareth Evans, Michael R. Stratton, Diana Eccles, Anna Elliott, Sandra Hanks, Douglas F. Easton, Rita Barfoot, Katarina Spanova, Deborah J. Thompson, Nazneen Rahman, Hiran Jayatilake, Sarah Reid, Sheila Seal, Lesley McGuffog, Patrick Kelly, Anthony Renwick, and Tasnim Chagtai

Subjects

Adult, Male, Tumor suppressor gene, PALB2, Breast Neoplasms, Biology, medicine.disease_cause, Article, Breast cancer, Fanconi anemia, Genetics, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, skin and connective tissue diseases, BRCA2 Protein, Mutation, Tumor Suppressor Proteins, BRIP1, Nuclear Proteins, Middle Aged, medicine.disease, Pedigree, Cancer research, RAD51C, Female, Fanconi Anemia Complementation Group N Protein

Abstract

PALB2 interacts with BRCA2, and biallelic mutations in PALB2 (also known as FANCN), similar to biallelic BRCA2 mutations, cause Fanconi anemia. We identified monoallelic truncating PALB2 mutations in 10/923 individuals with familial breast cancer compared with 0/1,084 controls (P = 0.0004) and show that such mutations confer a 2.3-fold higher risk of breast cancer (95% confidence interval (c.i.) = 1.4–3.9, P = 0.0025). The results show that PALB2 is a breast cancer susceptibility gene and further demonstrate the close relationship of the Fanconi anemia–DNA repair pathway and breast cancer predisposition.

Published

2006

14. A genome wide linkage search for breast cancer susceptibility genes

Author

Ruby T. Senie, Melissa C. Southey, Fabrice Odefrey, Barbara L. Weber, Inge van Leeuwen, David E. Goldgar, Hanne Meijers-Heijboer, P. Andrew Futreal, Douglas F. Easton, Fergus J. Couch, D. Gareth Evans, Henry T. Lynch, Christi J. van Asperen, Georgia Chenevix-Trench, Nazneen Rahman, Linda Baskcomb, Paula L. Smith, Lesley McGuffog, Sheila Seal, Margaret R. E. McCredie, Jon Mangion, Irene L. Andrulis, Graham J. Mann, Helene Renard, Diana Eccles, Graham G. Giles, John L. Hopper, Jaennelle Kraan, Beth Newman, Elizabeth A. Rapley, Gulietta M. Pupo, Karin Kroeze-Jansema, Cees J. Cornelisse, Rita Barfoot, Jenny Chang-Claude, Saundra S. Buys, Peter Devilee, Csilla Szabo, Jan Klijn, Sarah Edkins, Rogier A. Oldenburg, Richard Wooster, Dominique Stoppa-Lyonnet, Katherine L. Nathanson, Michael R. Stratton, A Hall, Hans F. A. Vasen, Human Genetics, Clinical Genetics, and Medical Oncology

Subjects

Male, Cancer Research, Genetic Linkage, Genes, BRCA2, Genes, BRCA1, Breast Neoplasms, Biology, Article, Breast cancer, SDG 3 - Good Health and Well-being, Genetic linkage, Genetics, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Genetic Testing, skin and connective tissue diseases, Genetic testing, Linkage (software), Models, Statistical, medicine.diagnostic_test, Genome, Human, Family aggregation, medicine.disease, Chromosome 4, Human genome, Female, Lod Score

Abstract

Mutations in known breast cancer susceptibility genes account for a minority of the familial aggregation of the disease. To search for further breast cancer susceptibility genes, we performed a combined analysis of four genome-wide linkage screens, which included a total of 149 multiple case breast cancer families. All families included at least three cases of breast cancer diagnosed below age 60 years, at least one of whom had been tested and found not to carry a BRCA1 or BRCA2 mutation. Evidence for linkage was assessed using parametric linkage analysis, assuming both a dominant and a recessive mode of inheritance, and using nonparametric methods. The highest LOD score obtained in any analysis of the combined data was 1.80 under the dominant model, in a region on chromosome 4 close to marker D4S392. Three further LOD scores over 1 were identified in the parametric analyses and two in the nonparametric analyses. A maximum LOD score of 2.40 was found on chromosome arm 2p in families with four or more cases of breast cancer diagnosed below age 50 years. The number of linkage peaks did not differ from the number expected by chance. These results suggest regions that may harbor novel breast cancer susceptibility genes. They also indicate that no single gene is likely to account for a large fraction of the familial aggregation of breast cancer that is not due to mutations in BRCA1 or BRCA2.

Published

2006

15. Variation of risks of breast and ovarian cancer associated with different germline mutations of the BRCA2 gene

Author

Michael R. Stratton, Sheila Seal, Douglas F. Easton, Bruce A.J. Ponder, Paul Russell, Simon A. Gayther, Jonathon Mangion, and Rita Barfoot

Subjects

Male, endocrine system diseases, DNA Mutational Analysis, Breast Neoplasms, Biology, medicine.disease_cause, Prostate cancer, Germline mutation, Breast cancer, Risk Factors, Pancreatic cancer, Genetics, medicine, Humans, Genetic Predisposition to Disease, Frameshift Mutation, skin and connective tissue diseases, Germ-Line Mutation, BRCA2 Protein, Ovarian Neoplasms, Mutation, medicine.disease, Neoplasm Proteins, Male breast cancer, Cancer research, Female, Ovarian cancer, Transcription Factors

Abstract

The breast cancer susceptibility gene BRCA2 on chromosome 13q12-13 has recently been identified. Germline mutations of BRCA2 are predicted to account for approximately 35% of families with multiple case, early onset female breast cancer, and they are also associated with an increased risk of male breast cancer, ovarian cancer, prostate cancer and pancreatic cancer. Germline mutations of a second cancer susceptibility gene BRCA1 (ref. 5), are associated with a strong predisposition to ovarian cancer as well as female breast cancer. Recent studies have suggested that the phenotype in BRCA1 families with respect to the ratio of breast to ovarian cancer varies with the location of the BRCA1 mutation. To determine whether germline mutations in BRCA2 are associated with a similar variation in phenotypic risk, we have analysed the distribution of mutations in 25 families with multiple cases of breast and/or ovarian cancer ascertained in the United Kingdom and Eire. These mutations all lead to premature truncation of BRCA2 as a result of frameshift deletions/insertions or nonsense mutations. Analysis of the mutation distribution along the length of the gene indicates a significant genotype-phenotype correlation. Truncating mutations in families with the highest risk of ovarian cancer relative to breast cancer are clustered in a region of approximately 3.3 kb in exon 11 (P = 0.0004). Published data on mutations in 45 other BRCA2-linked families provide support for this correlation.

Published

1997

16. Evaluation of RAD50 in familial breast cancer predisposition

Author

Carl Blomqvist, Sheila Seal, Jiri Bartek, Michael R. Stratton, Jirina Bartkova, Milja Kaare, Rita Barfoot, D. Gareth Evans, Päivi Heikkilä, Johanna Tommiska, Heli Nevanlinna, Anitta Tamminen, Nazneen Rahman, Linda Baskcomb, Diana Eccles, Jonna Tallila, Hiran Jayatilake, Kristiina Aittomäki, and Anthony Renwick

Subjects

Cancer Research, DNA Repair, DNA repair, DNA Mutational Analysis, Breast Neoplasms, Biology, medicine.disease_cause, Breast cancer, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Allele, Finland, Aged, Genetics, Mutation, Cancer, Middle Aged, medicine.disease, Null allele, United Kingdom, Acid Anhydride Hydrolases, DNA-Binding Proteins, DNA Repair Enzymes, Oncology, Case-Control Studies, Female, Haploinsufficiency, DNA Damage

Abstract

The genes predisposing to familial breast cancer are largely unknown, but 5 of the 6 known genes are involved in DNA damage repair. RAD50 is part of a highly conserved complex important in recognising, signalling and repairing DNA double-strand breaks. Recently, a truncating mutation in the RAD50 gene, 687delT, was identified in 2 Finnish breast cancer families. To evaluate the contribution of RAD50 to familial breast cancer, we screened the whole coding region for mutations in 435 UK and 46 Finnish familial breast cancer cases. We identified one truncating mutation, Q350X, in one UK family. We screened a further 544 Finnish familial breast cancer cases and 560 controls for the 687delT mutation, which was present in 3 cases (0.5%) and 1 control (0.2%). Neither Q350X nor 687delT segregated with cancer in the families in which they were identified. Functional analyses suggested that RAD50 687delT is a null allele as there was no detectable expression of the mutant protein. However, the wild-type allele was retained and expressed in breast tumors from mutation carriers. The abundance of the full-length RAD50 protein was reduced in carrier lymphoblastoid cells, suggesting a possible haploinsufficiency mechanism. These data indicate that RAD50 mutations are rare in familial breast cancer and either carry no, or a very small, increased risk of cancer. Altogether, these results suggest RAD50 can only be making a very minor contribution to familial breast cancer predisposition in UK and Finland.

Published

2005

17. Evaluation of Fanconi Anemia genes in familial breast cancer predisposition

Author

Sheila, Seal, Rita, Barfoot, Hiran, Jayatilake, Paula, Smith, Anthony, Renwick, Linda, Bascombe, Lesley, McGuffog, D Gareth, Evans, Diana, Eccles, Douglas F, Easton, Michael R, Stratton, and Nazneen, Rahman

Subjects

Fanconi Anemia Complementation Group D2 Protein, Fanconi Anemia Complementation Group C Protein, Genetic Variation, Nuclear Proteins, Proteins, RNA-Binding Proteins, Breast Neoplasms, Cell Cycle Proteins, DNA, Neoplasm, Exons, Middle Aged, Fanconi Anemia Complementation Group E Protein, Fanconi Anemia Complementation Group Proteins, Introns, DNA-Binding Proteins, Fanconi Anemia Complementation Group F Protein, Fanconi Anemia, Case-Control Studies, Humans, Genetic Predisposition to Disease, Fanconi Anemia Complementation Group G Protein

Abstract

Fanconi Anemia (FA) is an autosomal recessive syndrome characterized by congenital abnormalities, progressive bone marrow failure, and susceptibility to cancer. FA has eight known complementation groups and is caused by mutations in at least seven genes. Biallelic BRCA2 mutations were shown recently to cause FA-D1. Monoallelic (heterozygous) BRCA2 mutations confer a high risk of breast cancer and are a major cause of familial breast cancer. To investigate whether heterozygous variants in other FA genes are high penetrance breast cancer susceptibility alleles, we screened germ-line DNA from 88 BRCA1/2-negative families, each with at least three cases of breast cancer, for mutations in FANCA, FANCC, FANCD2, FANCE, FANCF, and FANCG. Sixty-nine sequence variants were identified of which 25 were exonic. None of the exonic variants resulted in translational frameshifts or nonsense codons and 14 were polymorphisms documented previously. Of the remaining 11 exonic variants, 2 resulted in synonymous changes, and 7 were present in controls. Only 2 conservative missense variants, 1 in FANCA and 1 in FANCE, were each found in a single family and were not present in 300 controls. The results indicate that FA gene mutations, other than in BRCA2, are unlikely to be a frequent cause of highly penetrant breast cancer predisposition.

Published

2003

18. Localization to Xq27 of a susceptibility gene for testicular germ-cell tumours

Author

Paul E. Goss, S. Edwards, R. Timothy D. Oliver, Robert Huddart, Sophie D. Fosså, Peter A. Daly, Michael R. Stratton, Michael Friedlander, Julia G. Bodmer, Douglas F. Easton, Patrick J. Biggs, Sheila Seal, Michael Leahy, D. Timothy Bishop, Ketil Heimdal, Gillian P. Crockford, Wilma Ormiston, Rifat Hamoudi, David Hogg, Dawn Teare, Elizabeth A. Rapley, Axel Heidenreich, David Forman, Felicity Collins, Katherine L. Tucker, Colin Cooper, Jenny Donald, and Rita Barfoot

Subjects

Infertility, Oncology, Adult, Genetic Markers, Male, medicine.medical_specialty, X Chromosome, Adolescent, Locus (genetics), Biology, Gene mapping, Testicular Neoplasms, Risk Factors, Internal medicine, Genetics, medicine, Humans, Family, Genetic Predisposition to Disease, Family history, X chromosome, Germinoma, Incidence, Chromosome Mapping, medicine.disease, Genetic marker, Relative risk, Female, Lod Score

Abstract

Testicular germ-cell tumours (TGCT) affect 1 in 500 men and are the most common cancer in males aged 15-40 in Western European populations. The incidence of TGCT has risen dramatically over the last century. Known risk factors for TGCT include a history of undescended testis (UDT), testicular dysgenesis, infertility, previously diagnosed TGCT (ref. 7) and a family history of the disease. Brothers of men with TGCT have an 8-10-fold risk of developing TGCT (refs 8,9), whereas the relative risk to fathers and sons is fourfold (ref. 9). This familial relative risk is much higher than that for most other types of cancer. We have collected samples from 134 families with two or more cases of TGCT, 87 of which are affected sibpairs. A genome-wide linkage search yielded a heterogeneity lod (hlod) score of 2.01 on chromosome Xq27 using all families compatible with X inheritance. We obtained a hlod score of 4.7 from families with at least one bilateral case, corresponding to a genome-wide significance level of P=0.034. The proportion of families with UDT linked to this locus was 73% compared with 26% of families without UDT (P=0.03). Our results provide evidence for a TGCT susceptibility gene on chromosome Xq27 that may also predispose to UDT.

Published

2000

19. Inherited susceptibility to colorectal adenomas and carcinomas: evidence for a new predisposition gene on 15q14-q22

Author

Nazneen Rahman, K Neale, Rita Barfoot, Ian C. Talbot, Michael R. Stratton, Richard S. Houlston, Shirley Hodgson, Rifat Hamoudi, Huw Thomas, J. M. A. Northover, Jon Mangion, Sheila Seal, Ian Tomlinson, and Ian M. Frayling

Subjects

Adenoma, Adult, Male, Colorectal cancer, Genetic Linkage, Loss of Heterozygosity, Colorectal adenoma, Biology, Familial adenomatous polyposis, Loss of heterozygosity, Genetic linkage, medicine, Carcinoma, Humans, Genetic Predisposition to Disease, Family history, Aged, Genetics, Chromosomes, Human, Pair 15, Hepatology, Gastroenterology, Middle Aged, medicine.disease, Haplotypes, Mutation, Cancer research, Female, Colorectal Neoplasms

Abstract

BACKGROUND and AIMS: The aim of this study was to evaluate the role of known colorectal adenoma and carcinoma susceptibility genes and to locate a novel susceptibility gene in an Ashkenazi family (SM1311) with dominantly inherited predisposition to colorectal adenomas and carcinomas. METHODS: Clinicopathologic and family history data were collected. Genetic linkage and mutational analyses were used to investigate the genetic basis of the family's disease. RESULTS: Affected members of SM1311 develop multiple tubular, villous, tubulovillous, and/or serrated colorectal adenomas throughout the large bowel, and some develop colon carcinoma. There are no extracolonic features clearly associated with disease in SM1311. We have shown that the family's phenotype does not result from APC mutations (including the I1307K variant) or from genetic changes in the other known genes that predispose to colon cancer. Using genetic linkage analysis, supplemented by allele loss in tumors, we have provided evidence for a new colorectal cancer susceptibility gene, CRAC1 (colorectal adenoma and carcinoma), mapping to chromosome 15q14-q22. CONCLUSIONS: We provide evidence for a novel colorectal adenoma and carcinoma susceptibility gene on chromosome 15q14-q22. Further studies are needed to confirm this localization and to evaluate the contribution of CRAC1 to this disease.

Published

1999

20. BRCA2 mutations in primary breast and ovarian cancers

Author

N. Collins, Andrew Berchuck, Charles Cochran, Sheila Seal, Rifat Hamoudi, Curtis Gumbs, P. Andrew Futreal, Catharina Larsson, Michael R. Stratton, Johnathan M. Lancaster, Jonathon Mangion, Roger W. Wiseman, Sandeep Patel, Catherine M. Phelan, Jeffrey R. Marks, J. Dirk Iglehart, Graham R. Bignell, Richard Wooster, Rita Barfoot, and Alan Ashworth

Subjects

Genetic Markers, medicine.medical_specialty, Heterozygote, endocrine system diseases, Tumor suppressor gene, Mammary gland, Molecular Sequence Data, Breast Neoplasms, Biology, Retinoblastoma Protein, Loss of heterozygosity, Breast cancer, Germline mutation, Internal medicine, Genetics, medicine, Missense mutation, Humans, Lymphocytes, skin and connective tissue diseases, Aged, DNA Primers, Sequence Deletion, BRCA2 Protein, Ovarian Neoplasms, Base Sequence, Middle Aged, medicine.disease, female genital diseases and pregnancy complications, Neoplasm Proteins, medicine.anatomical_structure, Endocrinology, Mutation, Cancer research, Female, Ovarian cancer, Transcription Factors

Abstract

The second hereditary breast cancer gene, BRCA2, was recently isolated. Germline mutations of this gene predispose carriers to breast cancer, and, to a lesser extent, ovarian cancer. Loss of heterozygosity (LOH) at the BRCA2 locus has been observed in 30-40% of sporadic breast and ovarian tumours, implying that BRCA2 may act as a tumour suppressor gene in a proportion of sporadic cases. To define the role of BRCA2 in sporadic breast and ovarian cancer, we screened the entire gene for mutations using a combination of techniques in 70 primary breast carcinomas and in 55 primary epithelial ovarian carcinomas. Our analysis revealed alterations in 2/70 breast tumours and none of the ovarian carcinomas. One alteration found in the breast cancers was a 2-basepair (bp) deletion (4710delAG) which was subsequently shown to be a germline mutation, the other was a somatic missense mutation (Asp3095Glu) of unknown significance. Our results suggest that BRCA2 is a very infrequent target for somatic inactivation in breast and ovarian carcinomas, similar to the results obtained for BRCA1.

Published

1996

21. Identification of the breast cancer susceptibility gene BRCA2

Author

Frances Connor, Rifat Hamoudi, Jonathan Mangion, Sheila Seal, Rosa Bjork Barkadottir, Steven A. Narod, David P. Kelsell, Curtis Gumbs, Henry T. Lynch, Michael R. Stratton, Amanda Smith, Yasmin Hashim, Richard Wooster, Simon G. Gregory, Nigel K. Spurr, Julian Peto, Peter Devilee, Bruce A.J. Ponder, Sandeep Patel, D. Timothy Bishop, P. Andrew Futreal, Sally Swift, Graham R. Bignell, Julius Gudmundsson, Rosalind A. Eeles, Patrick J. Biggs, N. Collins, Adelgeir Arason, Catherine M. Rice, Patricia N. Tonin, Douglas F. Easton, David R. Bentley, Cees J. Cornelisse, Rita Barfoot, Gos Michlem, David Ficenec, Valdgardur Egilsson, Gilbert M. Lenoir, D Ford, Alan Ashworth, and Jonathan Lancaster

Subjects

Male, Tumor suppressor gene, Molecular Sequence Data, Susceptibility gene, Breast Neoplasms, Biology, Frameshift mutation, Breast Neoplasms, Male, Open Reading Frames, Germline mutation, Breast cancer, Gene mapping, Medicine, Humans, Genetic Predisposition to Disease, Amino Acid Sequence, skin and connective tissue diseases, Frameshift Mutation, Chromosomes, Artificial, Yeast, Germ-Line Mutation, Sequence Deletion, BRCA2 Protein, Multidisciplinary, Hereditary breast–ovarian cancer syndrome, Base Sequence, Chromosomes, Human, Pair 13, business.industry, Chromosome Mapping, DNA, Neoplasm, medicine.disease, Neoplasm Proteins, Cancer research, Identification (biology), Female, Breast Cancer Genetics, business, Transcription Factors

Abstract

IN Western Europe and the United States approximately 1 in 12 women develop breast cancer. A small proportion of breast cancer cases, in particular those arising at a young age, are attributable to a highly penetrant, autosomal dominant predisposition to the disease. The breast cancer susceptibility gene, BRCA2, was recently localized to chromosome 13q12-q13. Here we report the identification of a gene in which we have detected six different germline mutations in breast cancer families that are likely to be due to BRCA2. Each mutation causes serious disruption to the open reading frame of the transcriptional unit. The results indicate that this is the BRCA2 gene.

Published

1995

22. Evidence for susceptibility genes to familial Wilms tumour in addition to WT1, FWT1 and FWT2

Author

Nazneen Rahman, A. Weirich, N Perusinghe, Jane Skeen, Anthony E. Reeve, E. A. Rapley, William D. Foulkes, Michael R. Stratton, Agnès Chompret, S de Tourreil, Catherine Bonaïti-Pellié, Valérie Schumacher, Rita Barfoot, Brigitte Royer-Pokora, Kathy Pritchard-Jones, and Andrew N. Shelling

Subjects

Genetic Markers, Male, Cancer Research, Tumor suppressor gene, FWT1, Genetic Linkage, Wilms tumour, Biology, FWT2, Wilms Tumor, familial predisposition, Genetic linkage, Genetic predisposition, Familial predisposition, medicine, Humans, Genetic Predisposition to Disease, WT1 Proteins, Genetics, Chromosomes, Human, Pair 11, Chromosome, Wilms' tumor, Regular Article, medicine.disease, Pedigree, DNA-Binding Proteins, Oncology, Genetic marker, Female, Chromosomes, Human, Pair 17, Transcription Factors

Abstract

Three loci have been implicated in familial Wilms tumour: WT1 located on chromosome 11p13, FWT1 on 17q12-q21, and FWT2 on 19q13. Two out of 19 Wilms tumour families evaluated showed strong evidence against linkage at all three loci. Both of these families contained at least three cases of Wilms tumour indicating that they were highly likely to be due to genetic susceptibility and therefore that one or more additional familial Wilms tumour susceptibility genes remain to be found. © 2000 Cancer Research Campaign

23. Identification of the familial cylindromatosis tumour-suppressor gene

Author

Patrick J. Biggs, Jaakko Leisti, Frits A. Beemer, Bertrand Delpech, P Chapman, Rita Barfoot, Christiane Fenske, Ranbir Chaggar, Piu Banerjee, Sally Swift, D. Gareth Evans, Sunil R. Lakhani, Elizabeth A. Rapley, Daniel Hohl, William Warren, Sheila Seal, Michael R. Stratton, Juliana E. Hansen, Reiner Siebert, John Burn, Dicky J. J. Halley, Irene M. Leigh, Sonja A. Rasmussen, N Leonard, Alan Ashworth, Naoki Oiso, Margaret R. Wallace, Samantha Merrett, Marcel Huber, Connie Schrander-Stumpel, B. Hofmann, Meiko Takahashi, Chris Jones, Carolanne Brown, Edward Blair, Helen Green, Gwen Turner, Mark G. Cleveland, Graham R. Bignell, Ans M.W. van den Ouweland, Anna Smith, and Clinical Genetics

Subjects

Male, Skin Neoplasms, Somatic cell, Molecular Sequence Data, Loss of Heterozygosity, Biology, Deubiquitinating Enzyme CYLD, Neoplasms, Multiple Primary, Contig Mapping, Germline mutation, Catalytic Domain, Genetics, medicine, Genetic predisposition, Humans, Genes, Tumor Suppressor, Genetic Predisposition to Disease, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Gene, Peptide sequence, Germ-Line Mutation, Genes, Dominant, Sequence Tagged Sites, Polymorphism, Genetic, Multiple familial trichoepithelioma, Sequence Homology, Amino Acid, Tumor Suppressor Proteins, Proteins, Chromosome, Exons, medicine.disease, Mutation, Female, Thiolester Hydrolases, Ubiquitin Thiolesterase, Chromosomes, Human, Pair 16

Abstract

Familial cylindromatosis is an autosomal dominant genetic predisposition to multiple tumours of the skin appendages. The susceptibility gene (CYLD) has previously been localized to chromosome 16q and has the genetic attributes of a tumour-suppressor gene (recessive oncogene). Here we have identified CYLD by detecting germline mutations in 21 cylindromatosis families and somatic mutations in 1 sporadic and 5 familial cylindromas. All mutations predict truncation or absence of the encoded protein. CYLD encodes three cytoskeletal-associated-protein-glycine-conserved (CAP-GLY) domains, which are found in proteins that coordinate the attachment of organelles to microtubules. CYLD also has sequence homology to the catalytic domain of ubiquitin carboxy-terminal hydrolases (UCH).