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Gustavo Baldassarre, Barbara Belletti, Paola Bruni, Angelo Boccia, Francesco Trapasso, Francesca Pentimalli, Maria Vittoria Barone, Gennaro Chiappetta, Maria Teresa Vento, Stefania Spiezia, Alfredo Fusco, Giuseppe Viglietto
Published in Volume 104, Issue 7
J Clin Invest. 1999; 104(7):865–874 doi:10.1172/JCI6443
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Figure 2

Expression and localization of p27 and cyclin D3 in thyroid tumors. (a) Western blot analysis of p27 or cyclin D3 expression in thyroid tumors. Lane NT, normal thyroid; lanes 1–5, papillary carcinomas; lanes 6 and 7, follicular carcinomas; lanes 8–10, anaplastic carcinomas. α-tubulin was used to assure uniform loading (third row). Bottom, Cdk2 activity in protein extracts from the same samples. (b) p27 immunoreactivity in normal and neoplastic thyroid tissue. Top left: normal thyroid, nuclear p27. Top right: papillary carcinoma, cytoplasmic p27. Bottom left: papillary carcinoma, nuclear and cytoplasmic p27. Bottom right: same tumor with antibody preincubated with antigen. ×40. (c) Western blot analysis of p27 and cyclin D3 on differentially extracted proteins. As control, antibodies to α-tubulin or cyclin H were used. (d) Cdk2 immunoprecipitates: p27 bound to Cdk2, Cdk2 level, and Cdk2 activity in total (left column) or fractionated extracts (remaining columns). (e) Correlation between cyclin D3 expression and p27 localization. Data are from Table 1.