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http://documenta.ciemat.es/handle/123456789/2300
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Título : | Differential development of large-cell neuroendocrine or small-cell lung carcinoma upon inactivation of 4 tumor suppressor genes |
Autor : | Lázaro, Sara Pérez-Crespo, Miriam Lorz, Corina Bernardini, Alejandra Oteo, Marta Enguita, Ana Belén Romero, Eduardo Hernández, Pilar Tomás, Laura Morcillo, Miguel Ángel Santos, Mirentxu |
Palabras clave : | LCNEC SCLC cell of origin tumor suppressor |
Fecha de publicación : | 1-feb-2024 |
Resumen : | High-grade neuroendocrine lung malignancies (large-cell neuroendocrine cell carcinoma, LCNEC, and small-cell lung carcinoma, SCLC) are among the most deadly lung cancer conditions with no optimal clinical management. The biological relationships between SCLC and LCNEC are still largely unknown and a current matter of debate as growing molecular data reveal high heterogeneity with potential therapeutic consequences. Here we describe murine models of high-grade neuroendocrine lung carcinomas generated by the loss of 4 tumor suppressors. In an Rbl1-null background, deletion of Rb1, Pten, and Trp53 floxed alleles after Ad-CMVcre infection in a wide variety of lung epithelial cells produces LCNEC. Meanwhile, inactivation of these genes using Ad-K5cre in basal cells leads to the development of SCLC, thus differentially influencing the lung cancer type developed. So far, a defined model of LCNEC has not been reported. Molecular and transcriptomic analyses of both models revealed strong similarities to their human counterparts. In addition, a 68Ga-DOTATOC-based molecular-imaging method provides a tool for detection and monitoring the progression of the cancer. These data offer insight into the biology of SCLC and LCNEC, providing a useful framework for development of compounds and preclinical investigations in accurate immunocompetent models. |
URI : | http://documenta.ciemat.es/handle/123456789/2300 |
ISSN : | 0027-8424 |
Aparece en las colecciones: | Artículos de Tecnología
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