PI3K regulates TAZ/YAP and mTORC1 axes that can be synergistically targeted
Keith C. Garcia, Ali A. Khan, Krishnendu Ghosh, Souradip Sinha, Nicholas Scalora, Gillian DeWane, Colleen Fullenkamp, Nicole Merritt, Yuliia Drebot, Samuel Y. Yu, Mariah Leidinger, Michael D. Henry, Patrick J. Breheny, Michael S. Chimenti, Munir R. Tanas
Keith C. Garcia, Ali A. Khan, Krishnendu Ghosh, Souradip Sinha, Nicholas Scalora, Gillian DeWane, Colleen Fullenkamp, Nicole Merritt, Yuliia Drebot, Samuel Y. Yu, Mariah Leidinger, Michael D. Henry, Patrick J. Breheny, Michael S. Chimenti, Munir R. Tanas
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Research Article Cell biology Oncology

PI3K regulates TAZ/YAP and mTORC1 axes that can be synergistically targeted

Abstract

Sarcomas are a heterogeneous group of cancers with few shared therapeutic targets. We show that PI3K signaling is frequently activated in sarcomas due to PTEN loss (in 30%–60%), representing a common therapeutic target. The PI3K pathway has lacked a downstream oncogenic transcription factor. We show TAZ and YAP are transcriptional coactivators regulated by PI3K and drive a transcriptome necessary for tumor growth in a PI3K-driven sarcoma mouse model. This PI3K/TAZ/YAP axis exists in parallel to the known PI3K/AKT/mTORC1 axis, providing a rationale for combination therapy targeting the TAZ/YAP-TEAD interaction and mTORC1. Combination therapy using IK-930 (TEAD inhibitor) and everolimus (mTORC1 inhibitor) synergistically diminished proliferation and anchorage-independent growth of PI3K-activated sarcoma cell lines at low, physiologically achievable doses. Furthermore, this combination therapy showed a synergistic effect in vivo, suggesting that an integrated view of PI3K and Hippo signaling can be leveraged therapeutically in PI3K-activated sarcomas.

Authors

Keith C. Garcia, Ali A. Khan, Krishnendu Ghosh, Souradip Sinha, Nicholas Scalora, Gillian DeWane, Colleen Fullenkamp, Nicole Merritt, Yuliia Drebot, Samuel Y. Yu, Mariah Leidinger, Michael D. Henry, Patrick J. Breheny, Michael S. Chimenti, Munir R. Tanas

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Figure 8

Combination therapy targeting YAP/TAZ and mTORC1 inhibits tumor growth in vivo.

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Combination therapy targeting YAP/TAZ and mTORC1 inhibits tumor growth i...
(A) Tumor growth curve for SJCRH30 xenograft in NSG mice receiving IK-930, everolimus (Evo), combination IK-930 and everolimus (Combo), and DMSO (Vehicle). Arrows denote weekly administration of everolimus. (B) Tumor volumes at the end of study in A. (C) Tumor growth curve for A204 xenograft in NSG mice receiving IK-930 (75 mg/kg daily), everolimus (Evo) (5 mg/kg weekly), combination IK-930 and everolimus (Combo), and DMSO (Vehicle). Arrows denote weekly administration of everolimus. (D) Tumor volumes at the end of study in C. (E) IHC for Ki-67 on SJCRH30 tumors. (F) IHC for Ki-67 on A204 tumors. (G) Simplified working model. For photomicrographs, scale bar: 50 μm (200×). For tumor volume and histological analysis, statistical significance was evaluated using an unpaired 2-tailed t test. **P < 0.01, ***P < 0.001, ****P < 0.0001.