A subtractive thyroid cDNA library was constructed from two human thyroid carcinoma cell lines originating from an anaplastic carcinoma and a papillary thyroid carcinoma. The library was used to identify genes correlated with the progression to a highly malignant phenotype. The thymosin β-10 gene was isolated and found to be expressed at much higher levels in the anaplastic cell line than in the papillary cells. The thymosin β-10 gene was overexpressed in five carcinoma cell lines compared with normal thyroid tissue and normal thyroid primary culture cells. The highest expression occurred in the most malignant cell lines. Thymosin β-10 gene expression was also increased in surgically removed human thyroid carcinomas and was highest in the anaplastic carcinomas.

Thymosin β-10 gene expression was correlated with the degree of the malignant phenotype also in rat thyroid cells transfected with cellular and viral oncogenes of different tumorigenicity. These results show that thymosin β-10 overexpression is a general event of thyroid cell neoplastic transformation and suggest that the gene is involved in the progression of thyroid carcinogenesis. Finally, the thymosin β-10 gene was located on chromosome 2q37 by fluorescence in situ hybridization analysis.

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This work was supported by the Associazione Italiana per la Ricerca sul Cancro, the Consiglio Nazionale delle Ricerche Progetto Finalizzato “Applicazioni Cliniche della Ricerca Oncologica,” and the Ministero della Sanità Fondo Sanitario Nazionale 1994. C. M. and F. T. are recipients of a fellowship from the Associazione Italiana per la Ricerca sul Cancro. A. F. was the recipient of a fellowship from the American-Italian Cancer Foundation.

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©1998 American Association for Cancer Research.
1998
American Association for Cancer Research, Inc.