Frequent somatic mutations and homozygous deletions of the p16 (MTS1) gene in pancreatic adenocarcinoma

Carlos Caldas; Stephan A. Hahn; Luis T. Da-Costa; Mark S. Redston; Mieke Schutte; Albert B. Seymour; Craig L. Weinstein; Ralph H. Hruban; Charles J. Yeo; Scott E. Kern

doi:10.1038/ng0994-27

Frequent somatic mutations and homozygous deletions of the p16 (MTS1) gene in pancreatic adenocarcinoma

Carlos Caldas
, Stephan A. Hahn
, Luis T. Da-Costa
, Mark S. Redston
, Mieke Schutte
, Albert B. Seymour
, Craig L. Weinstein
, Ralph H. Hruban
, Charles J. Yeo
, Scott E. Kern^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

1175 Scopus citations

Abstract

The MTS1 gene on chromosome 9p21 encodes the p16 inhibitor of cyclinD/Cdk-4 complexes, and is deleted or mutated in a variety of tumour types. We found allelic deletions of 9p21–p22 in 85% of pancreatic adenocarcinomas. Analysis of MTS1 in pancreatic carcinomas (27 xenografts and 10 cell lines) showed homozygous deletions in 15 (41%) and sequence changes in 14 (38%). These included eight point mutations (four nonsense, two missense and two splice site mutations) and six deletions/insertions, all accompanied by loss of the wild-type allele. Sequencing of MTS1 from primary tumours confirmed the mutations. Coexistent inactivations of both MTS1 and p53 was common and suggests that abnormal regulation of cyclin-dependent kinases may play an important role in the biology of pancreatic carcinoma.

Original language	English
Pages (from-to)	27-32
Number of pages	6
Journal	Nature Genetics
Volume	8
Issue number	1
DOIs	https://doi.org/10.1038/ng0994-27
State	Published - Sep 1994
Externally published	Yes

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10.1038/ng0994-27

Cite this

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title = "Frequent somatic mutations and homozygous deletions of the p16 (MTS1) gene in pancreatic adenocarcinoma",

abstract = "The MTS1 gene on chromosome 9p21 encodes the p16 inhibitor of cyclinD/Cdk-4 complexes, and is deleted or mutated in a variety of tumour types. We found allelic deletions of 9p21–p22 in 85\% of pancreatic adenocarcinomas. Analysis of MTS1 in pancreatic carcinomas (27 xenografts and 10 cell lines) showed homozygous deletions in 15 (41\%) and sequence changes in 14 (38\%). These included eight point mutations (four nonsense, two missense and two splice site mutations) and six deletions/insertions, all accompanied by loss of the wild-type allele. Sequencing of MTS1 from primary tumours confirmed the mutations. Coexistent inactivations of both MTS1 and p53 was common and suggests that abnormal regulation of cyclin-dependent kinases may play an important role in the biology of pancreatic carcinoma.",

author = "Carlos Caldas and Hahn, \{Stephan A.\} and Da-Costa, \{Luis T.\} and Redston, \{Mark S.\} and Mieke Schutte and Seymour, \{Albert B.\} and Weinstein, \{Craig L.\} and Hruban, \{Ralph H.\} and Yeo, \{Charles J.\} and Kern, \{Scott E.\}",

year = "1994",

month = sep,

doi = "10.1038/ng0994-27",

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T1 - Frequent somatic mutations and homozygous deletions of the p16 (MTS1) gene in pancreatic adenocarcinoma

AU - Caldas, Carlos

AU - Hahn, Stephan A.

AU - Da-Costa, Luis T.

AU - Redston, Mark S.

AU - Schutte, Mieke

AU - Seymour, Albert B.

AU - Weinstein, Craig L.

AU - Hruban, Ralph H.

AU - Yeo, Charles J.

AU - Kern, Scott E.

PY - 1994/9

Y1 - 1994/9

N2 - The MTS1 gene on chromosome 9p21 encodes the p16 inhibitor of cyclinD/Cdk-4 complexes, and is deleted or mutated in a variety of tumour types. We found allelic deletions of 9p21–p22 in 85% of pancreatic adenocarcinomas. Analysis of MTS1 in pancreatic carcinomas (27 xenografts and 10 cell lines) showed homozygous deletions in 15 (41%) and sequence changes in 14 (38%). These included eight point mutations (four nonsense, two missense and two splice site mutations) and six deletions/insertions, all accompanied by loss of the wild-type allele. Sequencing of MTS1 from primary tumours confirmed the mutations. Coexistent inactivations of both MTS1 and p53 was common and suggests that abnormal regulation of cyclin-dependent kinases may play an important role in the biology of pancreatic carcinoma.

AB - The MTS1 gene on chromosome 9p21 encodes the p16 inhibitor of cyclinD/Cdk-4 complexes, and is deleted or mutated in a variety of tumour types. We found allelic deletions of 9p21–p22 in 85% of pancreatic adenocarcinomas. Analysis of MTS1 in pancreatic carcinomas (27 xenografts and 10 cell lines) showed homozygous deletions in 15 (41%) and sequence changes in 14 (38%). These included eight point mutations (four nonsense, two missense and two splice site mutations) and six deletions/insertions, all accompanied by loss of the wild-type allele. Sequencing of MTS1 from primary tumours confirmed the mutations. Coexistent inactivations of both MTS1 and p53 was common and suggests that abnormal regulation of cyclin-dependent kinases may play an important role in the biology of pancreatic carcinoma.

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Frequent somatic mutations and homozygous deletions of the p16 (MTS1) gene in pancreatic adenocarcinoma

Abstract

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