ChIP sequencing of cyclin D1 reveals a transcriptional role in chromosomal instability in mice
Mathew C. Casimiro, … , Andrew Arnold, Richard G. Pestell
Mathew C. Casimiro, … , Andrew Arnold, Richard G. Pestell
Published February 6, 2012
Citation Information: J Clin Invest. 2012;122(3):833-843. https://doi.org/10.1172/JCI60256.
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Research Article Oncology

ChIP sequencing of cyclin D1 reveals a transcriptional role in chromosomal instability in mice

Abstract

Chromosomal instability (CIN) in tumors is characterized by chromosomal abnormalities and an altered gene expression signature; however, the mechanism of CIN is poorly understood. CCND1 (which encodes cyclin D1) is overexpressed in human malignancies and has been shown to play a direct role in transcriptional regulation. Here, we used genome-wide ChIP sequencing and found that the DNA-bound form of cyclin D1 occupied the regulatory region of genes governing chromosomal integrity and mitochondrial biogenesis. Adding cyclin D1 back to Ccnd1–/– mouse embryonic fibroblasts resulted in CIN gene regulatory region occupancy by the DNA-bound form of cyclin D1 and induction of CIN gene expression. Furthermore, increased chromosomal aberrations, aneuploidy, and centrosome abnormalities were observed in the cyclin D1–rescued cells by spectral karyotyping and immunofluorescence. To assess cyclin D1 effects in vivo, we generated transgenic mice with acute and continuous mammary gland–targeted cyclin D1 expression. These transgenic mice presented with increased tumor prevalence and signature CIN gene profiles. Additionally, interrogation of gene expression from 2,254 human breast tumors revealed that cyclin D1 expression correlated with CIN in luminal B breast cancer. These data suggest that cyclin D1 contributes to CIN and tumorigenesis by directly regulating a transcriptional program that governs chromosomal stability.

Authors

Mathew C. Casimiro, Marco Crosariol, Emanuele Loro, Adam Ertel, Zuoren Yu, William Dampier, Elizabeth A. Saria, Alex Papanikolaou, Timothy J. Stanek, Zhiping Li, Chenguang Wang, Paolo Fortina, Sankar Addya, Aydin Tozeren, Erik S. Knudsen, Andrew Arnold, Richard G. Pestell

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Figure 6

Subtype classification of breast cancer microarray samples.

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Subtype classification of breast cancer microarray samples. (A) Heatmap ...
(A) Heatmap depicting samples from combined breast cancer microarray datasets that were assigned to the 5 breast cancer gene expression subtypes. The predicted ESR1, epidermal growth factor receptor (ERBB2), and progesterone receptor (PGR) statuses are shown together with CIN signature score and CCND1 expression level across the 5 subtypes. The luminal B subtype receptor status, CIN signature score, and cyclin D1 expression level is outlined. (B) CCND1 transcript level plotted versus average CIN signature expression level revealed that the relationship between high CIN score and high cyclin D1 expression was luminal B subtype specific (red circle). (C) Kaplan-Meier plot showing differences in metastasis-free status in this dataset (P = 6.4462 × 10–8).