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Polymerase-mediated ultramutagenesis in mice produces diverse cancers with high mutational load
Hao-Dong Li, … , He Zhang, Diego H. Castrillon
Hao-Dong Li, … , He Zhang, Diego H. Castrillon
Published August 20, 2018
Citation Information: J Clin Invest. 2018;128(9):4179-4191. https://doi.org/10.1172/JCI122095.
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Research Article Genetics Oncology

Polymerase-mediated ultramutagenesis in mice produces diverse cancers with high mutational load

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Abstract

Mutations underlie all cancers, and their identification and study are the foundation of cancer biology. We describe what we believe to be a novel approach to mutagenesis and cancer studies based on the DNA polymerase ε (POLE) ultramutator phenotype recently described in human cancers, in which a single amino acid substitution (most commonly P286R) in the proofreading domain results in error-prone DNA replication. We engineered a conditional PoleP286R allele in mice. PoleP286R/+ embryonic fibroblasts exhibited a striking mutator phenotype and immortalized more efficiently. PoleP286R/+ mice were born at Mendelian ratios but rapidly developed lethal cancers of diverse lineages, yielding the most cancer-prone monoallelic model described to date, to our knowledge. Comprehensive whole-genome sequencing analyses showed that the cancers were driven by high base substitution rates in the range of human cancers, overcoming a major limitation of previous murine cancer models. These data establish polymerase-mediated ultramutagenesis as an efficient in vivo approach for the generation of diverse animal cancer models that recapitulate the high mutational loads inherent to human cancers.

Authors

Hao-Dong Li, Ileana Cuevas, Musi Zhang, Changzheng Lu, Md Maksudul Alam, Yang-Xin Fu, M. James You, Esra A. Akbay, He Zhang, Diego H. Castrillon

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Figure 3

PoleP286R/+ mice rapidly succumb to diverse cancers.

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PoleP286R/+ mice rapidly succumb to diverse cancers.
(A) Survival analy...
(A) Survival analysis of 50 PoleP286R/+, 22 sibling control (+/+) mice, and 2 PoleP286R LSL-PoleP286R mice. P values were determined by log-rank test. (B–G) Examples of malignant neoplasms. (B) Large thymic T cell lymphoma expanding the chest cavity, with infiltration into the lungs (lg) and below the heart (h). (C) Angiosarcoma of the hind leg, with hemorrhage. (D) Angiosarcoma of the shoulder (different mouse from that shown in C). (E) Histiocytic “sarcoma” involving 1 ovary. These tumors are not true sarcomas, but rather malignant hematopoietic neoplasms with histiocytic differentiation. The tumor was disseminated and present in other tissues. (F) Aggressive SCC of the snout. (G) Adenocarcinoma of the lung. Scale bars: 1 cm.

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