A four-drug combination chemotherapy (bleomycin-methotrexate-vinblastine-CCNU) had been used in 38 evaluable patients with recurrent squamous cell carcinoma of the head and neck region on an outpatient basis. A large number of these patients had carcinoma of the oral cavity (45% of total). Nineteen
Evidence for a clonal origin of head and neck tumors
โ Scribed by Philip J. Fialkow; George M. Martin; George Klein; Peter Clifford; Surjit Singh
- Publisher
- John Wiley and Sons
- Year
- 1972
- Tongue
- French
- Weight
- 671 KB
- Volume
- 9
- Category
- Article
- ISSN
- 0020-7136
No coin nor oath required. For personal study only.
โฆ Synopsis
Abstract
According to the inactiveโX hypothesis only one of the two genes at Xโlinked loci is active in somatic cells of females. Thus, in women heterozygous for the A and B genes at the Xโlinked glucoseโ6โphosphate dehydrogenase (Gโ6โPD) locus, single cells or clones of cells show either type A or type B enzyme. Similarly, pure tumors with a clonal origin arising in Gโ6โPD heterozygotes exhibit only type A or B enzyme, while those with multiple cell origin may show both A and B enzymes. The Gโ6โPD types of normal and neoplastic tissue were determined in 28 patients with tumors of the head and neck who were heterozygous at the Gโ6โPD locus. Normal tissues contained two enzyme types. Only one tumor from the 11 patients with anaplastic carcinoma of the nasopharynx was pure enough (i. e., with a relatively small number of nonโtumor cells) to allow firm conclusions. This tumor had a single enzyme phenotype and this is compatible with a clonal origin. Single enzyme phenotypes were also found in the two benign tumors and in single cases of plasmacytoma, melanoma, neuroblastoma and reticulumโcell sarcoma. The data from three cases of carcinoma of the palate and from single cases of carcinoma of an ectopic salivary gland and the thyroid gland respectively are also compatible with a clonal origin. Only one relatively pure tumor had a double enzyme phenotype, but even in this case, the evidence for a multiple cell origin is not convincing. Thus, the data in this and other studies suggest that at least one step in the development of most human neoplasms occurs in a single cell, i. e., the mature tumors have a clonal origin.
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