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. 2000 Feb;156(2):433-7.
doi: 10.1016/S0002-9440(10)64747-5.

APC mutations in sporadic medulloblastomas

H Huang  1 B M Mahler-AraujoA SankilaL ChimelliY YonekawaP KleihuesH Ohgaki
Affiliations

APC mutations in sporadic medulloblastomas

H Huang et al. Am J Pathol. 2000 Feb.

Abstract

The cerebellar medulloblastoma (WHO Grade IV) is a highly malignant, invasive embryonal tumor with preferential manifestation in children. Several molecular alterations appear to be involved, including isochromosome 17q and the p53, PTCH, and beta-catenin gene mutations. In this study, 46 sporadic medulloblastomas were screened for the presence of mutations in genes of the Wnt signaling pathway (APC and beta-catenin). Single-strand conformational polymorphism (SSCP) analysis followed by direct DNA sequencing revealed 3 miscoding APC mutations in 2 (4.3%) medulloblastomas. One case contained a GCA-->GTA mutation at codon 1296 (Ala-->Val), and another case had double point mutations at codons 1472 (GTA-->ATA, Val-->Ile) and 1495 (AGT-->GGT, Ser-->Gly). Miscoding beta-catenin mutations were detected in 4 tumors (8.7%). Three of these were located at codon 33 (TCT -->TTT, Ser-->Phe) and another at codon 37 (TCT-->GCT, Ser-->Ala). Adenomatous polyposis coli (APC) gene and beta-catenin mutations were mutually exclusive and occurred in a total of 6 of 46 cases (13%). Although germline APC mutations are a well established cause of familial colon and brain tumors (Turcot syndrome), this study provides the first evidence that APC mutations are also operative in a subset of sporadic medulloblastomas.

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Figures

Figure 1.
Figure 1.
Representative DNA sequencing autoradiographs of β-catenin and APC mutations in sporadic medulloblastomas. Note that wild-type bases are detectable in all cases. The case numbers on the top correspond to those in Table 1 ▶ .
See this image and copyright information in PMC

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