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Deleterious Germline BLM Mutations and the Risk for Early-onset Colorectal Cancer
by
Verwiel, Eugene T.
, Henkes, Arjen
, Hoischen, Alexander
, Schackert, Hans K.
, Mensenkamp, Arjen R.
, van Zelst-Stams, Wendy A.
, Ligtenberg, Marjolijn J.L.
, de Voer, Richarda M.
, van Kessel, Ad Geurts
, Kuiper, Roland P.
, Nagtegaal, Iris D.
, Gilissen, Christian
, Marleen Kets, C.
, Spruijt, Liesbeth
, Hoogerbrugge, Nicoline
, Hahn, Marc-Manuel
in
631/208/68
/ 631/67/1504/1885
/ Adult
/ Age of Onset
/ Bloom's syndrome
/ Case-Control Studies
/ Colorectal cancer
/ Colorectal carcinoma
/ Colorectal Neoplasms - epidemiology
/ Colorectal Neoplasms - genetics
/ Datasets as Topic
/ DNA helicase
/ Exome
/ Female
/ Gene Frequency
/ Genome-Wide Association Study
/ Genomic instability
/ Germ-Line Mutation
/ Health risks
/ Hereditary diseases
/ Heterozygote
/ High-Throughput Nucleotide Sequencing
/ Humanities and Social Sciences
/ Humans
/ Loss of Heterozygosity
/ Male
/ multidisciplinary
/ Mutation
/ Mutation Rate
/ Pedigree
/ Population Surveillance
/ Probes
/ RecQ Helicases - genetics
/ Risk
/ Science
2015
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Deleterious Germline BLM Mutations and the Risk for Early-onset Colorectal Cancer
by
Verwiel, Eugene T.
, Henkes, Arjen
, Hoischen, Alexander
, Schackert, Hans K.
, Mensenkamp, Arjen R.
, van Zelst-Stams, Wendy A.
, Ligtenberg, Marjolijn J.L.
, de Voer, Richarda M.
, van Kessel, Ad Geurts
, Kuiper, Roland P.
, Nagtegaal, Iris D.
, Gilissen, Christian
, Marleen Kets, C.
, Spruijt, Liesbeth
, Hoogerbrugge, Nicoline
, Hahn, Marc-Manuel
in
631/208/68
/ 631/67/1504/1885
/ Adult
/ Age of Onset
/ Bloom's syndrome
/ Case-Control Studies
/ Colorectal cancer
/ Colorectal carcinoma
/ Colorectal Neoplasms - epidemiology
/ Colorectal Neoplasms - genetics
/ Datasets as Topic
/ DNA helicase
/ Exome
/ Female
/ Gene Frequency
/ Genome-Wide Association Study
/ Genomic instability
/ Germ-Line Mutation
/ Health risks
/ Hereditary diseases
/ Heterozygote
/ High-Throughput Nucleotide Sequencing
/ Humanities and Social Sciences
/ Humans
/ Loss of Heterozygosity
/ Male
/ multidisciplinary
/ Mutation
/ Mutation Rate
/ Pedigree
/ Population Surveillance
/ Probes
/ RecQ Helicases - genetics
/ Risk
/ Science
2015
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Deleterious Germline BLM Mutations and the Risk for Early-onset Colorectal Cancer
by
Verwiel, Eugene T.
, Henkes, Arjen
, Hoischen, Alexander
, Schackert, Hans K.
, Mensenkamp, Arjen R.
, van Zelst-Stams, Wendy A.
, Ligtenberg, Marjolijn J.L.
, de Voer, Richarda M.
, van Kessel, Ad Geurts
, Kuiper, Roland P.
, Nagtegaal, Iris D.
, Gilissen, Christian
, Marleen Kets, C.
, Spruijt, Liesbeth
, Hoogerbrugge, Nicoline
, Hahn, Marc-Manuel
in
631/208/68
/ 631/67/1504/1885
/ Adult
/ Age of Onset
/ Bloom's syndrome
/ Case-Control Studies
/ Colorectal cancer
/ Colorectal carcinoma
/ Colorectal Neoplasms - epidemiology
/ Colorectal Neoplasms - genetics
/ Datasets as Topic
/ DNA helicase
/ Exome
/ Female
/ Gene Frequency
/ Genome-Wide Association Study
/ Genomic instability
/ Germ-Line Mutation
/ Health risks
/ Hereditary diseases
/ Heterozygote
/ High-Throughput Nucleotide Sequencing
/ Humanities and Social Sciences
/ Humans
/ Loss of Heterozygosity
/ Male
/ multidisciplinary
/ Mutation
/ Mutation Rate
/ Pedigree
/ Population Surveillance
/ Probes
/ RecQ Helicases - genetics
/ Risk
/ Science
2015
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Deleterious Germline BLM Mutations and the Risk for Early-onset Colorectal Cancer
Journal Article
Deleterious Germline BLM Mutations and the Risk for Early-onset Colorectal Cancer
2015
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Overview
Bloom syndrome is an autosomal recessive disorder characterized by chromosomal instability and increased cancer risk, caused by biallelic mutations in the
RECQL
-helicase gene
BLM
. Previous studies have led to conflicting conclusions as to whether carriers of heterozygous
BLM
mutations have an increased risk to develop colorectal cancer (CRC). We recently identified two carriers of a pathogenic
BLM
mutation in a cohort of 55 early-onset CRC patients (≤45 years of age), suggesting an overrepresentation compared to the normal population. Here, we performed targeted sequencing using molecular inversion probes to screen an additional cohort of 185 CRC patients (≤50 years of age) and 532 population-matched controls for deleterious
BLM
mutations. In total, we identified three additional CRC patients (1.6%) and one control individual (0.2%) that carried a known pathogenic
BLM
mutation, suggesting that these mutations are enriched in early-onset CRC patients (
P
= 0.05516). A comparison with local and publically available databases from individuals without suspicion for hereditary cancer confirmed this enrichment (
P
= 0.003534). Analysis of family members of the five
BLM
mutation carriers with CRC suggests an incomplete penetrance for CRC development. Therefore, these data indicate that carriers of deleterious
BLM
mutations are at increased risk to develop CRC, albeit with a moderate-to-low penetrance.
Publisher
Nature Publishing Group UK,Nature Publishing Group
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