TY - JOUR
T1 - Somatic mutations of the APC gene in colorectal tumors
T2 - Mutation cluster region in the APC gene
AU - Mori, Yasuo
AU - Nagse, Hiroki
AU - Ando, Hiroshi
AU - Horii, Akira
AU - Ichii, Shigetoshi
AU - Nakatsuru, Shuichi
AU - Aoki, Takahisa
AU - Miki, Yoshio
AU - Mori, Takesada
AU - Nakamura, Yusuke
N1 - Funding Information:
We acknowledge with thanks for the technical assistance from Kumiko Koyama and Kiyoshi Noguchi (Cancer Institute, Tokyo). This work was supported in part by a Grant-in-Aid from the Ministry of Education, Culture and Science, Japan, and Grants from the Vehicle Racing Commemorative Foundation.
PY - 1992/7
Y1 - 1992/7
N2 - We examined somatic mutations of the adenomatous polyposis coil (APC) gene in 63 colorectal tumors (16 adenomas and 47 carcinomas) developed in familial adenomatous polyposis (FAP) and non-FAP patients. In addition to loss of heterozygosity (LOH) at the APC locus in 30 tumors, 43 other somatic mutations were detected. Twenty-one of them were point mutations; 16 nonsense and two missense mutations, and three occurred in introns at the splicing site. Twenty-two tumors had frameshift mutations due to deletion or insertion; nineteen of them were deletions of one to 31 bp and three were a 1-bp insertion. One tumor had a 1-bp deletion in an intron near the splicing site. Hence, 41 (95%) of 43 mutations resulted in truncation of the APC protein. Over 60% of the somatic mutations in the APC gene were clustered within a small region of exon 15, designated as MCR (mutation cluster region), which accounted for less than 10% of the coding region. Combining these data and the results of LOH, more than 80% of tumors (14 adenomas and 39 carcinomas) had at least one mutation in the APC gene, of which more than 60% (9 adenomas and 23 carcinomas) had two mutations. These results strongly suggest that somatic mutations of the APC gene are associated with development of a great majority of colorectal tumors.
AB - We examined somatic mutations of the adenomatous polyposis coil (APC) gene in 63 colorectal tumors (16 adenomas and 47 carcinomas) developed in familial adenomatous polyposis (FAP) and non-FAP patients. In addition to loss of heterozygosity (LOH) at the APC locus in 30 tumors, 43 other somatic mutations were detected. Twenty-one of them were point mutations; 16 nonsense and two missense mutations, and three occurred in introns at the splicing site. Twenty-two tumors had frameshift mutations due to deletion or insertion; nineteen of them were deletions of one to 31 bp and three were a 1-bp insertion. One tumor had a 1-bp deletion in an intron near the splicing site. Hence, 41 (95%) of 43 mutations resulted in truncation of the APC protein. Over 60% of the somatic mutations in the APC gene were clustered within a small region of exon 15, designated as MCR (mutation cluster region), which accounted for less than 10% of the coding region. Combining these data and the results of LOH, more than 80% of tumors (14 adenomas and 39 carcinomas) had at least one mutation in the APC gene, of which more than 60% (9 adenomas and 23 carcinomas) had two mutations. These results strongly suggest that somatic mutations of the APC gene are associated with development of a great majority of colorectal tumors.
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U2 - 10.1093/hmg/1.4.229
DO - 10.1093/hmg/1.4.229
M3 - Article
C2 - 1338904
AN - SCOPUS:0026894053
VL - 1
SP - 229
EP - 233
JO - Human Molecular Genetics
JF - Human Molecular Genetics
SN - 0964-6906
IS - 4
ER -