Wt1 ablation and Igf2 upregulation in mice result in Wilms tumors with elevated ERK1/2 phosphorylation
Qianghua Hu, … , Richard R. Behringer, Vicki Huff
Qianghua Hu, … , Richard R. Behringer, Vicki Huff
Published December 1, 2010
Citation Information: J Clin Invest. 2011;121(1):174-183. https://doi.org/10.1172/JCI43772.
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Wt1 ablation and Igf2 upregulation in mice result in Wilms tumors with elevated ERK1/2 phosphorylation

Abstract

Wilms tumor (WT) is a genetically heterogeneous childhood kidney tumor. Several genetic alterations have been identified in WT patients, including inactivating mutations in WT1 and loss of heterozygosity or loss of imprinting at 11p15, which results in biallelic expression of IGF2. However, the mechanisms by which one or a combination of genetic alterations results in tumorigenesis has remained challenging to determine, given the lack of a mouse model of WT. Here, we engineered mice to sustain mosaic, somatic ablation of Wt1 and constitutional Igf2 upregulation, mimicking a subset of human tumors. Mice with this combination of genetic alterations developed tumors at an early age. Mechanistically, Wt1 ablation blocked mesenchyme differentiation, and increased Igf2 expression upregulated ERK1/2 phosphorylation. Importantly, a subset of human tumors similarly displayed upregulation of ERK1/2 phosphorylation, which suggests ERK signaling might contribute to WT development. Thus, we have generated a biologically relevant mouse model of WT and defined one combination of driver alterations for WT. This mouse model will provide a powerful tool to study the biology of WT initiation and progression and to investigate therapeutic strategies for cancers with IGF pathway dysregulation.

Authors

Qianghua Hu, Fei Gao, Weihua Tian, E. Cristy Ruteshouser, Yaqing Wang, Alexander Lazar, John Stewart, Louise C. Strong, Richard R. Behringer, Vicki Huff

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Figure 5

Increased pERK1/2 and pIRS1 expression in Wt1-Igf2 tumors and human tumors.

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Increased pERK1/2 and pIRS1 expression in Wt1-Igf2 tumors and human tumo...
(A) Heatmap of RPPA protein expression data in Wt1-Igf2 tumors and newborn Wt1–/flH19+/–m kidneys. Expression differences between tumors and controls were significant (P < 0.05) for pIRS1 and pERK1/2, but not for pPDK1 or pAKT. (B) Western blot analysis of Wt1–/flH19+/–m kidneys and tumors. (C and D) pERK1/2 IHC of newborn and E14.5 kidneys (Wt1+/flH19+/–m) and tumors. Scale bar: 200 μm (C and D). (E) RPPA protein expression of IGF-IR pathway components in human WTs (T). Expression level in fetal kidney (FK) was designated as 1.