Germline APC variants in patients with multiple colorectal adenomas, with evidence for the particular importance of E1317Q

Mendelian tumour syndromes are caused by rare mutations, which usually lead to protein inactivation. Few studies have determined whether or not the same genes harbour other, more common variants, which might have a lower penetrance and/or cause mild disease, perhaps indistinguishable from sporadic d...

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Veröffentlicht in:	Human molecular genetics 2000-09, Vol.9 (15), p.2215-2221
Hauptverfasser:	LAMLUM, Hanan, AL TASSAN, Nada, WILLIAMS, Christopher, GILBERT, John, CHEADLE, Jeremy, BELL, Jennie, HOULSTON, Richard, BODMER, Walter, SAMPSON, Julian, TOMLINSON, Ian, JAEGER, Emma, FRAYLING, Ian, SIEBER, Oliver, FAISAL BIN REZA, ECKERT, Maria, ROWAN, Andrew, BARCLAY, Ella, ATKIN, Wendy
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Sprache:	eng
Schlagworte:	Adenoma - genetics Adenomatous Polyposis Coli - genetics Adolescent Adult APC gene Biological and medical sciences Colorectal Neoplasms - genetics DNA Mutational Analysis Frameshift Mutation Gastroenterology. Liver. Pancreas. Abdomen Genes, APC Genes, Tumor Suppressor Germ-Line Mutation Humans Medical sciences Middle Aged Mutation, Missense Polymerase Chain Reaction Polymorphism, Single-Stranded Conformational Sequence Deletion Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Tumors
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creator	LAMLUM, Hanan AL TASSAN, Nada WILLIAMS, Christopher GILBERT, John CHEADLE, Jeremy BELL, Jennie HOULSTON, Richard BODMER, Walter SAMPSON, Julian TOMLINSON, Ian JAEGER, Emma FRAYLING, Ian SIEBER, Oliver FAISAL BIN REZA ECKERT, Maria ROWAN, Andrew BARCLAY, Ella ATKIN, Wendy
description	Mendelian tumour syndromes are caused by rare mutations, which usually lead to protein inactivation. Few studies have determined whether or not the same genes harbour other, more common variants, which might have a lower penetrance and/or cause mild disease, perhaps indistinguishable from sporadic disease and accounting for a considerable proportion of the unexplained inherited risk of tumours in the general population. Germline variants at the APC locus are excellent candidates for explaining why some individuals are predisposed to colorectal adenomas, but do not have the florid phenotype of familial adenomatous polyposis. We have screened 164 unrelated patients with 'multiple' (3-100) colorectal adenomas for germline variants throughout the APC gene, including promoter mutations. In addition to three Ashkenazi patients with I1307K, we found seven patients with the E1317Q variant. E1317Q is significantly associated with multiple colorectal adenomas (OR = 11. 17, 95% CI = 2.30-54.3, p < 0.001), accounting for approximately 4% of all patients with multiple colorectal adenomas. In addition, four patients with truncating APC variants in exon 9 or in the 3' part of the gene were identified. Germline APC variants account for approximately 10% of patients with multiple adenomas. Unidentified predisposition genes almost certainly exist. We argue that it is worthwhile to screen multiple adenoma patients for a restricted number of germline APC variants, namely the missense changes E1317Q and I1307K (if of Ashkenazi descent), and, if there is a family history of colorectal tumours, for truncating mutations 5' to exon 5, in exon 9 and 3' to codon 1580.
doi_str_mv	10.1093/oxfordjournals.hmg.a018912
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Few studies have determined whether or not the same genes harbour other, more common variants, which might have a lower penetrance and/or cause mild disease, perhaps indistinguishable from sporadic disease and accounting for a considerable proportion of the unexplained inherited risk of tumours in the general population. Germline variants at the APC locus are excellent candidates for explaining why some individuals are predisposed to colorectal adenomas, but do not have the florid phenotype of familial adenomatous polyposis. We have screened 164 unrelated patients with 'multiple' (3-100) colorectal adenomas for germline variants throughout the APC gene, including promoter mutations. In addition to three Ashkenazi patients with I1307K, we found seven patients with the E1317Q variant. E1317Q is significantly associated with multiple colorectal adenomas (OR = 11. 17, 95% CI = 2.30-54.3, p < 0.001), accounting for approximately 4% of all patients with multiple colorectal adenomas. In addition, four patients with truncating APC variants in exon 9 or in the 3' part of the gene were identified. Germline APC variants account for approximately 10% of patients with multiple adenomas. Unidentified predisposition genes almost certainly exist. 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Abdomen ; Genes, APC ; Genes, Tumor Suppressor ; Germ-Line Mutation ; Humans ; Medical sciences ; Middle Aged ; Mutation, Missense ; Polymerase Chain Reaction ; Polymorphism, Single-Stranded Conformational ; Sequence Deletion ; Stomach. Duodenum. Small intestine. Colon. Rectum. 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Few studies have determined whether or not the same genes harbour other, more common variants, which might have a lower penetrance and/or cause mild disease, perhaps indistinguishable from sporadic disease and accounting for a considerable proportion of the unexplained inherited risk of tumours in the general population. Germline variants at the APC locus are excellent candidates for explaining why some individuals are predisposed to colorectal adenomas, but do not have the florid phenotype of familial adenomatous polyposis. We have screened 164 unrelated patients with 'multiple' (3-100) colorectal adenomas for germline variants throughout the APC gene, including promoter mutations. In addition to three Ashkenazi patients with I1307K, we found seven patients with the E1317Q variant. E1317Q is significantly associated with multiple colorectal adenomas (OR = 11. 17, 95% CI = 2.30-54.3, p < 0.001), accounting for approximately 4% of all patients with multiple colorectal adenomas. In addition, four patients with truncating APC variants in exon 9 or in the 3' part of the gene were identified. Germline APC variants account for approximately 10% of patients with multiple adenomas. Unidentified predisposition genes almost certainly exist. We argue that it is worthwhile to screen multiple adenoma patients for a restricted number of germline APC variants, namely the missense changes E1317Q and I1307K (if of Ashkenazi descent), and, if there is a family history of colorectal tumours, for truncating mutations 5' to exon 5, in exon 9 and 3' to codon 1580.</description><subject>Adenoma - genetics</subject><subject>Adenomatous Polyposis Coli - genetics</subject><subject>Adolescent</subject><subject>Adult</subject><subject>APC gene</subject><subject>Biological and medical sciences</subject><subject>Colorectal Neoplasms - genetics</subject><subject>DNA Mutational Analysis</subject><subject>Frameshift Mutation</subject><subject>Gastroenterology. Liver. Pancreas. Abdomen</subject><subject>Genes, APC</subject><subject>Genes, Tumor Suppressor</subject><subject>Germ-Line Mutation</subject><subject>Humans</subject><subject>Medical sciences</subject><subject>Middle Aged</subject><subject>Mutation, Missense</subject><subject>Polymerase Chain Reaction</subject><subject>Polymorphism, Single-Stranded Conformational</subject><subject>Sequence Deletion</subject><subject>Stomach. Duodenum. Small intestine. Colon. Rectum. 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Few studies have determined whether or not the same genes harbour other, more common variants, which might have a lower penetrance and/or cause mild disease, perhaps indistinguishable from sporadic disease and accounting for a considerable proportion of the unexplained inherited risk of tumours in the general population. Germline variants at the APC locus are excellent candidates for explaining why some individuals are predisposed to colorectal adenomas, but do not have the florid phenotype of familial adenomatous polyposis. We have screened 164 unrelated patients with 'multiple' (3-100) colorectal adenomas for germline variants throughout the APC gene, including promoter mutations. In addition to three Ashkenazi patients with I1307K, we found seven patients with the E1317Q variant. E1317Q is significantly associated with multiple colorectal adenomas (OR = 11. 17, 95% CI = 2.30-54.3, p < 0.001), accounting for approximately 4% of all patients with multiple colorectal adenomas. In addition, four patients with truncating APC variants in exon 9 or in the 3' part of the gene were identified. Germline APC variants account for approximately 10% of patients with multiple adenomas. Unidentified predisposition genes almost certainly exist. We argue that it is worthwhile to screen multiple adenoma patients for a restricted number of germline APC variants, namely the missense changes E1317Q and I1307K (if of Ashkenazi descent), and, if there is a family history of colorectal tumours, for truncating mutations 5' to exon 5, in exon 9 and 3' to codon 1580.</abstract><cop>Oxford</cop><pub>Oxford University Press</pub><pmid>11001924</pmid><doi>10.1093/oxfordjournals.hmg.a018912</doi><tpages>7</tpages><oa>free_for_read</oa></addata></record>
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subjects	Adenoma - genetics Adenomatous Polyposis Coli - genetics Adolescent Adult APC gene Biological and medical sciences Colorectal Neoplasms - genetics DNA Mutational Analysis Frameshift Mutation Gastroenterology. Liver. Pancreas. Abdomen Genes, APC Genes, Tumor Suppressor Germ-Line Mutation Humans Medical sciences Middle Aged Mutation, Missense Polymerase Chain Reaction Polymorphism, Single-Stranded Conformational Sequence Deletion Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Tumors
title	Germline APC variants in patients with multiple colorectal adenomas, with evidence for the particular importance of E1317Q
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