Your search keyword '"Bodmer, WF"' showing total 23 results

1. Role of rare variants in undetermined multiple adenomatous polyposis and early-onset colorectal cancer.

Author

Lefevre JH, Bonilla C, Colas C, Winney B, Johnstone E, Tonks S, Day T, Hutnik K, Boumertit A, Soubrier F, Midgley R, Kerr D, Parc Y, and Bodmer WF

Subjects

Adaptor Proteins, Signal Transducing genetics, Adenoma epidemiology, Adenoma genetics, Adult, Age of Onset, BRCA2 Protein genetics, Case-Control Studies, Colorectal Neoplasms epidemiology, Computer Simulation, DNA Repair Enzymes genetics, Exodeoxyribonucleases genetics, France, Gene Frequency, Humans, Middle Aged, MutL Protein Homolog 1, Nuclear Proteins genetics, Odds Ratio, United Kingdom, beta Catenin genetics, Adenomatous Polyposis Coli genetics, Colorectal Neoplasms genetics, Genetic Predisposition to Disease, Genetic Variation

Abstract

Some 15-20% of multiple adenomatous polyposis have no genetic explanation and 20-30% of colorectal cancer (CRC) cases are thought to be due to inherited multifactorial causes. Accumulation of deleterious effects of low-frequency dominant and independently acting variants may be a partial explanation for such patients. The aim of this study was to type a selection of rare and low-frequency variants (<5%) to elucidate their role in CRC susceptibility. A total of 1181 subjects were included (866 controls; 315 cases). Cases comprised UK (n=184) and French (n=131) patients with MAP (n=187) or early-onset CRC (n=128). Seventy variants in 17 genes were examined in cases and controls. The effect of the variant effect on protein function was investigated in silico. Out of the 70 variants typed, 36 (51%) were tested for association. Twenty-one variants were rare (minor allele frequency (MAF) <1%). Four rare variants were found to have a significantly higher MAF in cases (EXO1-12, MLH1-1, CTNNB1-1 and BRCA2-37, P<0.05) than in controls. Pooling all rare variants with a MAF <0.5% showed an excess risk in cases (odds ratio=3.2; 95% confidence interval=1.1-9.5; P=0.04). Rare variants are important risk factors in CRC and, as such, should be systematically assayed alongside common variation in the search for the genetic basis of complex diseases., Competing Interests: The authors declare no conflict of interest.

Published

2012

2. Bottom-up histogenesis of colorectal adenomas: origin in the monocryptal adenoma and initial expansion by crypt fission.

Author

Preston SL, Wong WM, Chan AO, Poulsom R, Jeffery R, Goodlad RA, Mandir N, Elia G, Novelli M, Bodmer WF, Tomlinson IP, and Wright NA

Subjects

Adenoma surgery, Colonoscopy, Dissection methods, Humans, Intestinal Mucosa pathology, Adenoma pathology, Adenomatous Polyposis Coli pathology, Colonic Neoplasms pathology, Intestinal Mucosa cytology

Abstract

The adenoma:carcinoma sequence is well established. Understanding the molecular pathology of the adenoma is therefore important. There is great controversy within the field. The Vogelstein group champions the "top-down" theory (colorectal adenomas arise and grow across the mucosal surface and down into the crypts), whereas other studies, including our own, propose "bottom-up" spread. Serial sections of 40 small (<3 mm) sporadic colorectal adenomas were stained with H&E, MIB-1, and for beta-catenin. 10 early adenomas were Feulgen-stained and microdissected. We also examined the flat mucosa of three patients who had undergone colectomies for familial adenomatous polyposis (FAP) and specimens from a XO/XY individual with FAP, the latter using in situ hybridization for the Y chromosome. In the earliest sporadic adenomas, there were crypts entirely filled with adenomatous epithelium, which showed proliferative activity and nuclear localization of beta-catenin. There was a sharp cutoff between crypt epithelial cells showing nuclear beta-catenin and surface cells with membrane staining. In slightly larger lesions, adenomatous spread from above was seen. Microdissected adenomas showed multiple fission events, with proliferation distributed equally throughout. In FAP tissue, numerous isolated monocryptal adenomas, which were clonal in origin, were seen. Examination of adenomas in the XO/XY individual showed no instances of XY or XO adenomatous epithelium growing down into crypts of the other genotype. Both sporadic and FAP adenomas start as a unicryptal adenomas and grow initially by crypt fission--a bottom-up pattern. Later, in sporadic adenomas, there is evidence of growth down into adjacent crypts (top-down).

Published

2003

3. An ancestral Ashkenazi haplotype at the HMPS/CRAC1 locus on 15q13-q14 is associated with hereditary mixed polyposis syndrome.

Author

Jaeger EE, Woodford-Richens KL, Lockett M, Rowan AJ, Sawyer EJ, Heinimann K, Rozen P, Murday VA, Whitelaw SC, Ginsberg A, Atkin WS, Lynch HT, Southey MC, Debinski H, Eng C, Bodmer WF, Talbot IC, Hodgson SV, Thomas HJ, and Tomlinson IP

Subjects

Chromosome Mapping, Chromosomes, Human, Pair 6 genetics, Female, Genetic Predisposition to Disease, Genetic Testing, Humans, Lod Score, Male, Pedigree, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 15 genetics, Genetic Linkage, Haplotypes genetics, Jews genetics

Abstract

The putative locus for hereditary mixed polyposis syndrome (HMPS) in a large family of Ashkenazi descent (SM96) was previously reported to map to chromosome sub-bands 6q16-q21. However, new clinical data, together with molecular data from additional family members, have shown 6q linkage to be incorrect. A high-density genomewide screen for the HMPS gene was therefore performed on SM96, using stringent criteria for assignment of affection status to minimize phenocopy rates. Significant evidence of linkage was found only on a region on chromosome 15q13-q14. Since this region encompassed CRAC1, a locus involved in inherited susceptibility to colorectal adenomas and carcinomas in another Ashkenazi family (SM1311), we determined whether HMPS and CRAC1 might be the same. We found that affected individuals from both families shared a haplotype between D15S1031 and D15S118; the haplotype was rare in the general Ashkenazi population. A third informative family, SM2952, showed linkage of disease to HMPS/CRAC1 and shared the putative ancestral haplotype, as did a further two families, SMU and RF. Although there are probably multiple causes of the multiple colorectal adenoma and cancer phenotype in Ashkenazim, an important one is the HMPS/CRAC1 locus on 15q13-q14.

Published

2003

4. CDX2 mutations do not account for juvenile polyposis or Peutz-Jeghers syndrome and occur infrequently in sporadic colorectal cancers.

Author

Woodford-Richens KL, Halford S, Rowan A, Bevan S, Aaltonen LA, Wasan H, Bicknell D, Bodmer WF, Houlston RS, and Tomlinson IP

Subjects

AMP-Activated Protein Kinase Kinases, AMP-Activated Protein Kinases, Animals, CDX2 Transcription Factor, DNA-Binding Proteins genetics, Exons, Genes, Tumor Suppressor, Genetic Carrier Screening, Homozygote, Humans, Mice, Mutation, Missense, Polymorphism, Genetic, Polymorphism, Single-Stranded Conformational, Protein Serine-Threonine Kinases genetics, Smad4 Protein, Trans-Activators genetics, Tumor Cells, Cultured, Adenomatous Polyposis Coli genetics, Colorectal Neoplasms genetics, Homeodomain Proteins genetics, Peutz-Jeghers Syndrome genetics

Abstract

Peutz-Jeghers syndrome (PJS) and juvenile polyposis (JPS) are both characterized by the presence of hamartomatous polyps and increased risk of malignancy in the gastrointestinal tract. Mutations of the LKB1 and SMAD4 genes have been shown recently to cause a number of PJS and JPS cases respectively, but there remains considerable uncharacterized genetic heterogeneity in these syndromes, particularly JPS. The mouse homologue of CDX2 has been shown to give rise to a phenotype which includes hamartomatous-like polyps in the colon and is therefore a good candidate for JPS and PJS cases which are not accounted for by the SMAD4 and LKB1 genes. By analogy with SMAD4, CDX2 is also a candidate for somatic mutation in sporadic colorectal cancer. We have screened 37 JPS families/cases without known SMAD4 mutations, 10 Peutz-Jeghers cases without known LKB1 mutations and 49 sporadic colorectal cancers for mutations in CDX2. Although polymorphic variants and rare variants of unlikely significance were detected, no pathogenic CDX2 mutations were found in any case of JPS or PJS, or in any of the sporadic cancers., (Copyright 2001 Cancer Research Campaign.)

Published

2001

5. The ABC of APC.

Author

Fearnhead NS, Britton MP, and Bodmer WF

Subjects

Adenomatous Polyposis Coli Protein, Apoptosis, Binding Sites, Colorectal Neoplasms genetics, Cytoskeletal Proteins chemistry, DNA Methylation, Genotype, Germ-Line Mutation, Humans, Models, Genetic, Mutation, Mutation, Missense, Phenotype, Promoter Regions, Genetic, Protein Structure, Tertiary, Signal Transduction, Adenomatous Polyposis Coli genetics, Cytoskeletal Proteins genetics, Cytoskeletal Proteins physiology

Abstract

Familial adenomatous polyposis (FAP) is an autosomal dominant inherited disease characterized by the presence of adenomatous polyps in the colon and rectum, with inevitable development of colorectal cancer if left untreated. FAP is caused by germline mutations in the adenomatous polyposis coli (APC) gene. Somatic mutations in the APC gene are an early event in colorectal tumorigenesis, and can be detected in the majority of colorectal tumours. The APC gene encodes a large protein with multiple cellular functions and interactions, including roles in signal transduction in the wnt-signalling pathway, mediation of intercellular adhesion, stabilization of the cytoskeleton and possibly regulation of the cell cycle and apoptosis. The fact that APC is an integral part of so many different pathways makes it an ideal target for mutation in carcinogenesis. This review deals with our understanding to date of how mutations in the APC gene translate into changes at the protein level, which in turn contribute to the role of APC in tumorigenesis.

Published

2001

6. Analysis of genetic and phenotypic heterogeneity in juvenile polyposis.

Author

Woodford-Richens K, Bevan S, Churchman M, Dowling B, Jones D, Norbury CG, Hodgson SV, Desai D, Neale K, Phillips RK, Young J, Leggett B, Dunlop M, Rozen P, Eng C, Markie D, Rodriguez-Bigas MA, Sheridan E, Iwama T, Eccles D, Smith GT, Kim JC, Kim KM, Sampson JR, Evans G, Tejpar S, Bodmer WF, Tomlinson IP, and Houlston RS

Subjects

Adenomatous Polyposis Coli diagnosis, Adolescent, Adult, Aged, Child, Child, Preschool, Codon, Terminator genetics, Diagnosis, Differential, Female, Gene Deletion, Genetic Testing, Genotype, Humans, Infant, Male, Middle Aged, Mutation, Missense genetics, PTEN Phosphohydrolase, Phenotype, Phosphoric Monoester Hydrolases genetics, Adenomatous Polyposis Coli genetics, Genetic Heterogeneity, Germ-Line Mutation genetics, Tumor Suppressor Proteins

Abstract

Background: Juvenile polyposis syndrome (JPS) is characterised by gastrointestinal (GI) hamartomatous polyposis and an increased risk of GI malignancy. Juvenile polyps also occur in the Cowden (CS), Bannayan-Ruvalcaba-Riley (BRRS) and Gorlin (GS) syndromes. Diagnosing JPS can be problematic because it relies on exclusion of CS, BRRS, and GS. Germline mutations in the PTCH, PTEN and DPC4 (SMAD4) genes can cause GS, CS/BRRS, and JPS, respectively., Aims: To examine the contribution of mutations in PTCH, PTEN, and DPC4 (SMAD4) to JPS., Methods: Forty seven individuals from 15 families and nine apparently sporadic cases with JPS were screened for germline mutations in DPC4, PTEN, and PTCH., Results: No patient had a mutation in PTEN or PTCH. Five different germline mutations were detected in DPC4; three of these were deletions, one a single base substitution creating a stop codon, and one a missense change. None of these patients had distinguishing clinical features., Conclusions: Mutations in PTEN and PTCH are unlikely to cause juvenile polyposis in the absence of clinical features indicative of CS, BRRS, or GS. A proportion of JPS patients harbour DPC4 mutations (21% in this study) but there remains uncharacterized genetic heterogeneity in JPS.

Published

2000

7. APC in the regulation of intestinal crypt fission.

Author

Wasan HS, Park HS, Liu KC, Mandir NK, Winnett A, Sasieni P, Bodmer WF, Goodlad RA, and Wright NA

Subjects

Adenoma pathology, Adenomatous Polyposis Coli pathology, Adult, Animals, Cell Division, Colon, Epithelium pathology, Humans, Male, Mice, Mice, Inbred C57BL, Mice, Mutant Strains, Models, Biological, Adenomatous Polyposis Coli genetics, Genes, APC, Germ-Line Mutation, Intestinal Mucosa pathology

Abstract

The functional effects of APC (adenomatous polyposis coli gene) germ-line mutations on crypt fission and cell proliferation were investigated in the normal intestine of human familial adenomatous polyposis (FAP) and multiple intestinal neoplasia (MIN) mice. Compared with controls, there was a 19-fold increase in the proportion of crypts in fission in FAP colon [95 per cent confidence interval (CI): 11-32, P < 0.0001], and a 75 and 61 per cent increase in MIN colon (95 per cent CI: 1.08-2.82, P < 0.02) and small bowel, respectively (95 per cent CI: 1.31-1.99, P < 0.001). In marked contrast, no significant differences in intra-cryptal epithelial cell proliferation or mitotic distribution were seen. Furthermore, 10.9 per cent of crypts in FAP were in asymmetrical fission as opposed to only 1 per cent in controls (P = 0.001). The largest relative increases in MIN crypt fission were in the colon (proximal and distal colon:190 per cent, P = 0.02 and 83 per cent, P = 0.01), suggesting that Apc mutations exert their maximal influence site-specifically. However, sites with the highest relative increases were also those with the largest eventual tumour sizes, but not the highest polyp counts. Three-dimensional serial section reconstruction analysis corroborated that FAP adenomas enlarge by crypt fission, which was frequently both asymmetrical and atypical. It is proposed that the absence of an increase in intestinal cell division infers that APC regulates intestinal crypt differentiation, specifically through the crypt cycle. This role appears analogous to the control of axis re-duplication in embryonic development, when downstream targets of APC are over-expressed. It is concluded that in vivo, the major defect in pre-neoplastic intestine harbouring APC mutations is elevated rates of crypt fission, and that this is also the mode by which micro-adenomas enlarge.

Published

1998

8. Allele loss in colorectal cancer at the Cowden disease/juvenile polyposis locus on 10q.

Author

Frayling IM, Bodmer WF, and Tomlinson IP

Subjects

Female, Humans, Male, Adenomatous Polyposis Coli genetics, Alleles, Chromosomes, Human, Pair 10 genetics, Colorectal Neoplasms genetics, Gene Deletion, Hamartoma Syndrome, Multiple genetics

Abstract

The genes that are mutated in inherited cancer syndromes are often involved in the pathogenesis of sporadic cancers of the types that characterize those syndromes. In colorectal cancer such loci include the familial adenomatous polyposis (APC) gene and the hereditary nonpolyposis colorectal cancer (DNA mismatch repair) genes. Juvenile hamartomatous polyposis syndromes, which include Juvenile Polyposis and Cowden disease, also predispose to colorectal cancer. The gene for Cowden disease has recently been localized to chromosome 10q22-q23, and a juvenile polyposis locus, JP1, has been reported as mapping to the same location. We have studied up to 70 cases of sporadic colorectal cancer for allele loss at markers predominantly on the long arm of chromosome 10, including loci flanking the putative Cowden Disease/JP1 locus. Frequencies of allele loss of about 35% were found close to this locus, whereas low frequencies of allele loss were found elsewhere on 10q. Mutations at the putative Cowden Disease/JP1 locus may therefore be important in sporadic colorectal cancer and fine mapping of allele loss on 10q in sporadic colon cancers may help to refine the position of this gene.

Published

1997

9. Clinical and molecular features of the hereditary mixed polyposis syndrome.

Author

Whitelaw SC, Murday VA, Tomlinson IP, Thomas HJ, Cottrell S, Ginsberg A, Bukofzer S, Hodgson SV, Skudowitz RB, Jass JR, Talbot IC, Northover JM, Bodmer WF, and Solomon E

Subjects

Adenomatous Polyposis Coli surgery, Adult, Aged, Chromosome Mapping, Colonic Neoplasms genetics, Female, Genetic Linkage, Humans, Male, Middle Aged, Mutation, Pedigree, Rectal Neoplasms genetics, Adenomatous Polyposis Coli genetics, Adenomatous Polyposis Coli pathology

Abstract

Background & Aims: Various inherited syndromes predispose to the development of colonic juvenile polyps and colorectal cancer, with potential importance for sporadic tumorigenesis. This study describes features of a possibly new syndrome of atypical juvenile polyps and other colonic tumors and compares these features with those of known gastrointestinal tumor syndromes., Methods: A large family, St. Mark's family 96, with a tendency to develop colonic polyps of mixed histological types is described. Genetic linkage to known polyposis syndromes has been tested., Results: Adenomatous and hyperplastic polyps occur in affected members of the family, although the characteristic lesion is an atypical juvenile polyp. Some affected individuals have developed polyps of more than one type, and individual polyps may contain features of more than one histological type. Polyps can undergo malignant change. Typically, fewer than 15 polyps are found at colonoscopy and there is no extracolonic disease associated with the development of polyps. The family's polyps seem to be inherited in an autosomal-dominant fashion, but the disease is probably unlinked to candidate loci with importance in colorectal tumorigenesis, such as APC, hMSH2, and hMLH1., Conclusions: We term this family's disease hereditary mixed polyposis syndrome (HMPS). Although mutations in the putative HMPS gene may be responsible for syndromes such as juvenile and Peutz-Jeghers polyposes, HMPS may also be a distinct disease.

Published

1997

10. Variants at the secretory phospholipase A2 (PLA2G2A) locus: analysis of associations with familial adenomatous polyposis and sporadic colorectal tumours.

Author

Tomlinson IP, Beck NE, Neale K, and Bodmer WF

Subjects

Adenomatous Polyposis Coli enzymology, Adenomatous Polyposis Coli etiology, Chi-Square Distribution, Chromosomes, Human, Pair 1, Colorectal Neoplasms enzymology, Colorectal Neoplasms etiology, Duodenum pathology, Genotype, Humans, Mutation, Phospholipases A metabolism, Phospholipases A2, Polymorphism, Genetic, Polymorphism, Single-Stranded Conformational, Sequence Analysis, DNA, Statistics, Nonparametric, Synovial Membrane enzymology, Adenomatous Polyposis Coli genetics, Colorectal Neoplasms genetics, Genetic Variation, Phospholipases A genetics

Abstract

The Min mouse is a model for human familial adenomatous polyposis (FAP), an autosomal dominant disease characterised by multiple adenomatous gastrointestinal polyps. The severity of the Min phenotype is modified by a locus (Mom1) on mouse chromosome 4, at a position syntenic with human chromosome 1p35-p36. The secretory phospholipase A2 (Pla2s) gene is a candidate for this modifier locus and there is evidence that a locus on human chromosome 1p35-p36 acts to modify the severity of human duodenal FAP. We have analysed the human secretory phospholipase A2 locus (PLA2G2A) for variants that could directly influence the FAP phenotype. We found no PLA2G2A variants predicted to result in functional variation in the phospholipase A2 protein. Two PLA2G2A polymorphisms were, however, discovered, one a 'silent' base change in exon 3 and another in a noncoding region. Three other variants (possible mutations) were found in non-coding regions. In 70 FAP patients from 20 families, no associations were found between the severity of duodenal polyposis and any PLA2G2A variant. One allele at the exon 3 polymorphic site did, however, occur more often then expected in patients with relatively severe colonic FAP. Although of borderline statistical significance, this association, if genuine, is likely to result from linkage disequilibrium between the PLA2G2A alleles studied and undetected genetic variation at a closely linked locus. The frequency of the alleles at both polymorphic sites has also been determined in the germ line of patients with sporadic colorectal adenomas and carcinomas and in random controls, but no differences were found among these groups. Our results suggest that PLA2G2A variants do not influence inherited or sporadic colonic tumours. A linked locus may be a modifier of human FAP, but does not influence the risk of colorectal tumours in the general population.

Published

1996

11. Polyclonal origin of colonic adenomas in an XO/XY patient with FAP.

Author

Novelli MR, Williamson JA, Tomlinson IP, Elia G, Hodgson SV, Talbot IC, Bodmer WF, and Wright NA

Subjects

Adenomatous Polyposis Coli pathology, Adult, Clone Cells, DNA Probes, Genotype, Humans, Ileum pathology, In Situ Hybridization, In Situ Hybridization, Fluorescence, Karyotyping, Male, Phenotype, Y Chromosome, Adenomatous Polyposis Coli genetics, Colon pathology, Intestinal Mucosa pathology, Mosaicism

Abstract

It is widely accepted that tumors are monoclonal in origin, arising from a mutation or series of mutations in a single cell and its descendants. The clonal origin of colonic adenomas and uninvolved intestinal mucosa from an XO/XY mosaic individual with familial adenomatous polyposis (FAP) was examined directly by in situ hybridization with Y chromosome probes. In this patient, the crypts of the small and large intestine were clonal, but at least 76 percent of the microadenomas were polyclonal in origin.

Published

1996

12. Genetic mapping of hereditary mixed polyposis syndrome to chromosome 6q.

Author

Thomas HJ, Whitelaw SC, Cottrell SE, Murday VA, Tomlinson IP, Markie D, Jones T, Bishop DT, Hodgson SV, Sheer D, Northover JM, Talbot IC, Solomon E, and Bodmer WF

Subjects

Adenoma genetics, Adult, Aged, Colorectal Neoplasms genetics, Female, Genetic Linkage, Heterozygote, Humans, Male, Middle Aged, Adenomatous Polyposis Coli genetics, Chromosome Mapping, Chromosomes, Human, Pair 6, Colonic Neoplasms genetics

Abstract

Hereditary mixed polyposis syndrome (HMPS) is characterized by atypical juvenile polyps, colonic adenomas, and colorectal carcinomas. HMPS appears to be inherited in an autosomal dominant manner. Genetic linkage analysis has been performed on a large family with HMPS. Data did not support linkage to the APC locus or to any of the loci for hereditary nonpolyposis colorectal cancer. Evidence that the HMPS locus lies on chromosome 6q was, however, provided by significant two-point LOD scores for linkage between HMPS and the D6S283 locus. Analysis of recombinants and multipoint linkage analysis suggested that the HMPS locus lies in a 4-cM interval containing the D6S283 locus and flanked by markers D6S468 and D6S301.

Published

1996

13. A modifying locus for familial adenomatous polyposis may be present on chromosome 1p35-p36.

Author

Tomlinson IP, Neale K, Talbot IC, Spigelman AD, Williams CB, Phillips RK, and Bodmer WF

Subjects

Adolescent, Adult, Alleles, Child, Chromosome Mapping, Duodenum pathology, Female, Genes, Dominant genetics, Genes, Suppressor genetics, Genetic Linkage genetics, Genetic Markers, Genotype, Humans, Male, Pedigree, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 1

Abstract

Mutations of the APC gene cause familial adenomatous polyposis (FAP) in humans and multiple intestinal neoplasia (Min) in laboratory mouse strains. A dominant modifying gene (Mom1), which partially suppresses the min phenotype, has been mapped to mouse chromosome 4. This region is syntenic with human chromosome 1p35-p36. The phospholipase A2 (Pla2s) locus is an excellent candidate for Mom1 and the equivalent human locus PLA2G2A is found on chromosome 1p35. It does not necessarily follow, however, than any modifier of mouse polyposis also influences human disease. In order to test whether a locus on 1p modifies FAP, subjects from 28 FAP families have been typed at microsatellite loci on this chromosome arm. The severity of their duodenal polyposis has also been assessed by endoscopy. Pedigree (lod score) linkage analysis found no evidence of a simple, dominant modifying gene, comparable with the action of Mom1 in inbred mouse strains. Given the more complex genetic and environmental interactions likely to exist in outbred human populations, it is probably more appropriate to use tests which do not specify a mode of inheritance. Using these methods of analysis, the data suggest that a locus on chromosome 1p35-p36 may influence the severity of duodenal FAP.

Published

1996

14. Phenotypic expression in familial adenomatous polyposis: partial prediction by mutation analysis.

Author

Nugent KP, Phillips RK, Hodgson SV, Cottrell S, Smith-Ravin J, Pack K, and Bodmer WF

Subjects

Adenomatous Polyposis Coli pathology, Colon pathology, DNA Mutational Analysis, Fibromatosis, Aggressive genetics, Gene Deletion, Humans, Phenotype, Adenomatous Polyposis Coli genetics, Genes, APC genetics, Mutation

Abstract

The phenotypic expression in familial adenomatous polyposis (FAP) is variable. This study compares the phenotype of 27 patients with an identical 5 base pair (bp) deletion at codon 1309 with a group of 61 matched patients with FAP where knowledge of specific mutations is not available and with seven other different mutations in 24 subjects. Patients with the codon 1309 deletion have significantly more colorectal polyps at the time of colectomy than age and sex matched FAP controls (p = 0.0001). The median number of polyps in colectomy specimens of patients with the deletion at codon 1309 was 4000 (interquartile (IQ) range 3000-4875), compared with 600 (IQ range 488-1400) in the matched controls. Mutations at codon 1323, 1407, and 233 were also associated with large numbers of polyps. Desmoid disease and extracolonic cancers were more common with the mutation at codon 1309 (p = 0.003). In conclusion, there may be a correlation between a specific germline mutation and the number of large bowel polyps. There is residual heterogeneity in phenotypic expression, however, and this may result from the influence of other genes, specific environmental factors or chance.

Published

1994

15. A long-range restriction map of human chromosome 5q21-q23.

Author

Ward JR, Cottrell S, Thomas HJ, Jones TA, Howe CM, Hampton GM, Deaven L, Sheer D, Bodmer WF, and Solomon E

Subjects

Chromosomes, Fungal, Cosmids, DNA Probes, Gene Library, Genetic Markers, Genome, Human, Humans, In Situ Hybridization, Fluorescence, Polymorphism, Restriction Fragment Length, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 5, Restriction Mapping

Abstract

A long-range restriction map encompassing the APC (adenomatous polyposis coli) gene has been constructed. The map includes 35 DNA markers and consists of two segments of 10 and 2.5 Mb. Published genetic markers have been connected using additional, nonpolymorphic DNA probes. The map clarifies marker order and allows comparison of physical and genetic data.

Published

1993

16. Molecular analysis of APC mutations in familial adenomatous polyposis and sporadic colon carcinomas.

Author

Cottrell S, Bicknell D, Kaklamanis L, and Bodmer WF

Subjects

Adenomatous Polyposis Coli blood, Base Sequence, Blotting, Southern, Chromosome Deletion, Colorectal Neoplasms blood, DNA Mutational Analysis, DNA Transposable Elements, Gene Frequency, Genetic Counseling, Genetic Testing, Humans, Molecular Sequence Data, Pedigree, Restriction Mapping, Adenomatous Polyposis Coli genetics, Colorectal Neoplasms genetics, DNA, Mutation genetics

Abstract

Mutations in the APC gene give rise to familial adenomatous polyposis (FAP) and also occur in many, perhaps most, sporadic colon cancers. By screening with single-strand conformation polymorphism analysis we identified several mutations in a small region of the APC gene in both FAP and sporadic cancers. These mutations were either point mutations or small deletions or insertions causing frameshifts, and all generated stop codons. One 5 base-pair deletion was found in a sporadic colon tumour, a colorectal cancer cell line derived from a sporadic colon tumour, and in four unrelated FAP patients. This mutation produces distinctive heteroduplex bands, which can be detected with a simple non-radioactive assay. Our findings suggest that highly localised short sequences, essentially runs that code for adenine and thymine, may account for up to 20% of all observed APC mutations.

Published

1992

17. Regional mapping of 22 microclones around the adenomatous polyposis coli (APC) locus on chromosome 5q.

Author

Hampton GM, Howe C, Leuteritz G, Thomas H, Bodmer WF, Solomon E, and Ballhausen WG

Subjects

Cells, Cultured, Chromosome Mapping, Cloning, Molecular, Genomic Library, Humans, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 5

Abstract

A previously described genomic library constructed from microdissected DNA has been used to generate a large number of probes around the adenomatous polyposis coli (APC) gene at 5q22. A total of 202 clones were hybridised directly onto a somatic cell hybrid panel containing two APC-related interstitial deletions. Of 75 microclones that gave clear hybridisation signals, 22 independent clones mapped into the region common to both deletions. In addition, 4/22 of the markers are conserved in rodent DNA. These clones should provide a valuable resource for screening cDNA libraries and cloning the DNA around the APC gene in yeast artificial chromosomes.

Published

1991

18. Characterization and mapping of microdissected genomic clones from the adenomatous polyposis coli (APC) region.

Author

Hampton G, Leuteritz G, Lüdecke HJ, Senger G, Trautmann U, Thomas H, Solomon E, Bodmer WF, Horsthemke B, and Claussen U

Subjects

Chromosome Mapping, Cloning, Molecular methods, DNA Mutational Analysis, DNA Probes, Genomic Library, Histocytochemistry, Humans, Karyotyping, Nucleic Acid Hybridization, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 5 ultrastructure

Abstract

The gene associated with adenomatous polyposis coli (APC) has been mapped to the long arm of chromosome 5. To saturate the APC region with DNA markers, two independent microdissection libraries with an emphasis on 5q21.2-21.3 and 5q22 have been constructed from GTG-banded human metaphase chromosomes. PCR-amplified insert DNA of the primary amplificate used as a probe in chromosomal in situ suppression (CISS) hybridization of human metaphase spreads revealed region-specific signals at the chromosomal site that was excised for cloning. One hundred forty-two inserts, derived from both libraries, have been characterized in more detail. Deletion mapping analysis was performed with 17 single-copy clones on a hamster-human hybrid cell panel. Seven of these clones were located within two interstitial deletions of 6-8 Mb from APC-affected individuals around chromosome bands 5q21-22. The identification of new microclones mapping into these deletions and their use in isolating YAC clones should contribute to the construction of a contiguous physical map of the APC region.

Published

1991

19. Fine mapping of probes in the adenomatous polyposis coli region of chromosome 5 by in situ hybridization.

Author

Williams SV, Jones TA, Cottrell S, Zehetner G, Varesco L, Ward T, Thomas H, Lawson PA, Solomon E, and Bodmer WF

Subjects

Cells, Cultured, Chromosome Banding, Chromosome Mapping, DNA Probes, Female, Humans, Lod Score, Lymphocytes cytology, Male, Nucleic Acid Hybridization, Pedigree, Recombination, Genetic, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 5

Abstract

The gene for adenomatous polyposis coli has been localized to 5q21-22. We have mapped six probes from this region using isotopic or nonisotopic in situ hybridization. Using tritium-labeled probes we localized II227 (D5S37) to 5q14-15 and ECB27 (D5S98) to 5q21. Following hybridization with biotin-labeled probes, the positions of signals along the chromosomes were measured as fractional length relative to the length of the chromosome arm from centromere to qter (FLcen-qter). Ninety-five percent confidence limits, compared with standard karyotypes, provided the corresponding band localization. By this method we localized Cllpll (D5S71) to FLcen-qter 0.407-0.452 (5q21.1-21.3), ECB27 to FLcen-qter 0.426-0.473 (5q21.3), YN5.48 (D5S81) to FLcen-qter 0.459-0.496 (5q21.3-22.2), and ECB134 (D5S97) to FLcen-qter 0.509-0.533 (5q22.3-23.1). ECB220 had three sites of hybridization, a major site at FLcen-qter 0.460-0.492 (5q21.3-22.1) and minor sites at FLcen-qter 0.299-0.339 (5q14.3-15) and FLcen-qter 0.629-0.691 (5q23.3-31.2). We have shown that the chromosome 5 breakpoint in a t(5;15) translocation from a patient with Gardner's syndrome (GM03314) is between Cllpll and ECB27. Linkage data are presented suggesting that ECB27 is located on the same side of the APC locus as II227. These and published results including data on several constitutional deletions (M, SD, and brothers PW and ND) give a probable order of [cen] - [II227, proximal SD breakpoint] - [Cllpll] - [proximal PW/ND, M breakpoint(s), GM03314 breakpoint] - [ECB27] - [APC] - [YN5.48] - [distal PW/ND breakpoint] - [ECB134] - [distal M breakpoint] - [qter]. The major site of ECB220 appears to be between ECB27 and the distal PW/ND breakpoint; the distal SD breakpoint is distal to YN5.48.

Published

1991

20. Genetic analysis of colorectal cancer.

Author

Bodmer WF, Cottrell S, Frischauf AM, Kerr IB, Murday VA, Rowan AJ, Smith MF, Solomon E, Thomas H, and Varesco L

Subjects

Antigens, Neoplasm genetics, Chromosome Deletion, Chromosomes, Human, Pair 17, Chromosomes, Human, Pair 5 ultrastructure, Colorectal Neoplasms immunology, DNA Mutational Analysis, Genes, Dominant, Genes, Recessive, Genes, p53, Genetic Markers, HLA Antigens genetics, Humans, Neoplasm Proteins genetics, Adenomatous Polyposis Coli genetics, Colorectal Neoplasms genetics, Oncogenes

Abstract

Adenomatous polyposis, mainly of the colon, (APC) is a rare dominantly inherited susceptibility to colon cancer in which individuals develop hundreds of polyps mainly in their large bowel. The APC gene has been localised to chromosome 5q21 by following up a case report of an individual with an interstitial deletion on chromosome 5q who had multiple developmental abnormalities together with adenomatous polyposis. A DNA marker (D5S71) was found to be closely linked to APC in family studies and localised to 5q21 by in situ annealing. Material from further patients with deletions in this region of chromosome 5 has been used, by a combination of somatic cell hybrid and long-range DNA analysis, to identify new DNA markers close to the APC gene. These and other markers now provide the basis for genetic counselling of nearly all families with APC. These studies are being extended, together with other approaches for analysing DNA clones around the APC gene, in the search for the gene itself. Allele loss in tumour as compared to normal tissue from sporadic cases of colorectal carcinomas has clearly implicated the APC gene in at least 25 to 40% of all cases of colorectal carcinomas. Similar studies by Vogelstein and others as well as ourselves have further implicated recessive changes on chromosomes 17 and 18 in the development of colorectal carcinomas. Following the demonstration by Vogelstein of the role of p53 mutations in connection with the chromosome 17 changes, we have now shown, using monoclonal antibodies to the mutant p53 products and by other approaches, that changes in the p53 gene may occur in up to 50% or more of colorectal carcinomas. Frequent mutations of the K-ras dominant oncogene, as well as changes in the expression of human leucocyte antigen (HLA)-A, B, C determinants, are further genetic changes that appear commonly to be involved in the progression of colorectal carcinomas. The latter have important implications for T cell immune response to tumours and its manipulation for treatment and even prevention of colorectal cancer. We may soon be approaching a situation when it will become possible to identify all the genetic steps and their sequence during tumour progression, as well as their functional significance largely through the induction of inappropriate growth and the suppression of differentiation.

Published

1989

21. Chromosome 5 allele loss in human colorectal carcinomas.

Author

Solomon E, Voss R, Hall V, Bodmer WF, Jass JR, Jeffreys AJ, Lucibello FC, Patel I, and Rider SH

Subjects

Alleles, Chromosome Aberrations, DNA Restriction Enzymes, DNA, Neoplasm genetics, DNA, Recombinant, Heterozygote, Humans, Nucleic Acid Hybridization, Polymorphism, Restriction Fragment Length, Adenocarcinoma genetics, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 5, Colonic Neoplasms genetics, Rectal Neoplasms genetics

Abstract

That the sporadic and inherited forms of a particular cancer could both result from mutations in the same gene was first proposed by Knudson. He further proposed that these mutations act recessively at the cellular level, and that both copies of the gene must be lost for the cancer to develop. In sporadic cases both events occur somatically whereas in dominant familial cases susceptibility is inherited through a germline mutation and the cancer develops after a somatic change in the homologous allele. This model has since been substantiated in the case of retinoblastoma, Wilms tumour, acoustic neuroma and several other tumours, in which loss of heterozygosity was shown in tumour material compared to normal tissue from the same patient. The dominantly inherited disorder, familial adenomatous polyposis (FAP, also called familial polyposis coli), which gives rise to multiple adenomatous polyps in the colon that have a relatively high probability of progressing to a malignant adenocarcinoma, provides a basis for studying recessive genes in the far more common colorectal carcinomas using this approach. Following a clue as to the location of the FAP gene given by a case report of an individual with an interstitial deletion of chromosome 5q, who had FAP and multiple developmental abnormalities, we have examined sporadic colorectal adenocarcinomas for loss of alleles on chromosome 5. Using a highly polymorphic 'minisatellite' probe which maps to chromosome 5q we have shown that at least 20% of this highly heterogeneous set of tumours lose one of the alleles present in matched normal tissue. This parallels the assignment of the FAP gene to chromosome 5 (see accompanying paper) and suggests that becoming recessive for this gene may be a critical step in the progression of a relatively high proportion of colorectal cancers.

Published

1987

22. Localization of the gene for familial adenomatous polyposis on chromosome 5.

Author

Bodmer WF, Bailey CJ, Bodmer J, Bussey HJ, Ellis A, Gorman P, Lucibello FC, Murday VA, Rider SH, and Scambler P

Subjects

Adenocarcinoma genetics, Chromosome Mapping, Colonic Neoplasms genetics, DNA genetics, DNA, Recombinant, Gene Frequency, Humans, Mutation, Nucleic Acid Hybridization, Pedigree, Adenomatous Polyposis Coli genetics, Chromosomes, Human, Pair 5

Abstract

Colorectal cancer is the second most common cancer in the United Kingdom and other developed countries in the West. Although it is usually not familial, there is a rare dominantly inherited susceptibility to colon cancer, familial adenomatous polyposis (FAP; also often previously called familial polyposis coli). During adolescence affected individuals develop from a few hundred to over a thousand adenomatous polyps in their large bowel. These are sufficiently likely to give rise to adenocarcinomas to make prophylactic removal of the colon usual in diagnosed FAP individuals. Adenomas may occur elsewhere in the gastrointestinal tract and the condition is often associated with other extracolonic lesions, such as epidermoid cysts, jaw osteomata and fibrous desmoid tumours. Adenomata have been suggested to be precancerous states for most colorectal tumours. Knudson has suggested that the mutation for a dominantly inherited cancer susceptibility may be the first step in a recessive change in the tumour cells, and that the same gene may be involved in both familial and non-familial cases of a given tumour. Following up a case report of an interstitial deletion of chromosome 5 in a mentally retarded individual with multiple developmental abnormalities and FAP, we have now shown that the FAP gene is on chromosome 5, most probably near bands 5q21-q22.

Published

1987

23. CpG island clones from a deletion encompassing the gene for adenomatous polyposis coli.

Author

Varesco L, Thomas HJ, Cottrell S, Murday V, Fennell SJ, Williams S, Searle S, Sheer D, Bodmer WF, and Frischauf AM

Subjects

Adenoma genetics, Base Sequence, Blotting, Southern methods, Cell Line, Cell Transformation, Viral, Cloning, Molecular, Gene Library, Herpesvirus 4, Human genetics, Humans, Karyotyping, Molecular Sequence Data, Nucleic Acid Amplification Techniques, Oligonucleotide Probes, Restriction Mapping, Adenomatous Polyposis Coli genetics, Chromosome Deletion, Chromosomes, Human, Pair 5, Dinucleoside Phosphates analysis, Genes, Dominant

Abstract

Adenomatous polyposis coli (APC), a dominantly inherited disorder, has been mapped to chromosome 5q15-q21 by family linkage studies. Cells from patients with deletions in this region, in one case associated with polyposis in a family, have been used to construct human hamster hybrid cell lines that retain either the normal or deleted chromosome 5. These lines have been used to identify markers from the region of the polyposis gene obtained by cloning the ends of 0.5- to 2-megabase BssHII fragments purified by pulsed-field gel electrophoresis. Three markers are described that map within the deletions and must therefore be close to the APC gene.

Published

1989