Abstract
BACKGROUND
Medulloblastoma is a malignant, invasive embryonic tumor of the cerebellum. Sonic hedgehog (SHH) is a secreted glycoprotein that has a major role in the developing cerebellum. Activation of the SHH pathway resulting from mutations in the PATCH gene, which is an inhibitor of the pathway, are associated with hereditary and sporadic medulloblastomas. The GLI3 protein is another negative regulator of SHH signaling. The authors hypothesized that mutations in GLI3 may be associated with meduloblastomas.
METHODS
The authors describe a patient with hereditary Greig syndrome, which was caused by mutations in GLI3, and medulloblastoma. Another such patient was described in the literature. They also sequenced the GLI3 gene, including all exonβintron boundaries, in an additional 12 sporadic medulloblastomas.
RESULTS
The authors detected a new nonsense germline mutation in a child with Greig syndrome and medulloblastoma. This mutation generates a stop codon in position 809 of GLI3 that has been predicted to result in massive truncation of the protein. Several new polymorphisms, but no tumorβassociated mutations, were found in sporadic tumors.
CONCLUSIONS
Gli3 is mutated rarely in medulloblastoma. Cancer 2002;95:28β31. Β© 2002 American Cancer Society.
DOI 10.1002/cncr.10642