Details

Autor(en) / Beteiligte

• Kim, Dong-Wook
• Wu, Nan
• Kim, Young-Chul
• Cheng, Pei Feng
• Basom, Ryan
• Kim, Dongkyoon
• Dunn, Colin T
• Lee, Anastasia Y
• Kim, Keebeom
• Lee, Chang Sup
• Singh, Andrew
• Gazdar, Adi F
• Harris, Chris R
• Eisenman, Robert N
• Park, Kwon-Sik
• MacPherson, David

Titel

Genetic requirement for Mycl and efficacy of RNA Pol I inhibition in mouse models of small cell lung cancer

Ist Teil von

• Genes & development, 2016-06, Vol.30 (11), p.1289-1299

Ort / Verlag

United States: Cold Spring Harbor Laboratory Press

Erscheinungsjahr

2016

Quelle

MEDLINE

Beschreibungen/Notizen

• Small cell lung cancer (SCLC) is a devastating neuroendocrine carcinoma. MYCL (L-Myc) is frequently amplified in human SCLC, but its roles in SCLC progression are poorly understood. We isolated preneoplastic neuroendocrine cells from a mouse model of SCLC and found that ectopic expression of L-Myc, c-Myc, or N-Myc conferred tumor-forming capacity. We focused on L-Myc, which promoted pre-rRNA synthesis and transcriptional programs associated with ribosomal biogenesis. Deletion of Mycl in two genetically engineered models of SCLC resulted in strong suppression of SCLC. The high degree of suppression suggested that L-Myc may constitute a therapeutic target for a broad subset of SCLC. We then used an RNA polymerase I inhibitor to target rRNA synthesis in an autochthonous Rb/p53-deleted mouse SCLC model and found significant tumor inhibition. These data reveal that activation of RNA polymerase I by L-Myc and other MYC family proteins provides an axis of vulnerability for this recalcitrant cancer.