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The opportunities provided by the NCI
intramural program allowed us to carry out a long-term prospective study
that characterized the subsequent risk of cancer in 24 families that we
assembled with this dominantly inherited, devastating syndrome. It featured
sarcomas of soft tissue and bone, breast cancer, brain tumors, leukemia and
adrenocortical tumors, with several other cancers appearing to arise at
lower levels of relative risk. The family members were also prone to
multiple primary tumors, including a predisposition to sarcomas following
radiotherapy. Biospecimens were collected in a search for an underlying
mechanism that might explain this wide range of tumors. But we came up
empty-handed until 20 years after the original report when Stephen Friend at
Harvard and Esther Chang at the Uniformed Services University across the
street independently detected germline mutations of the tumor suppressor
gene, p53, in our families. The gene was a candidate for study since somatic
mutations had recently been identified in about 50% of all cancer, including
each of the tumors that we were seeing in the syndrome. |
