Loss of the wild-type KRAS allele promotes pancreatic cancer progression through functional activation of YAP1

Yan, Han; Yu, Chih-Chieh; Fine, Stuart A.; Youssof, Ayman Lee; Yang, Yuxue; Yan, Jun; Karg, Dillon C.; Cheung, Edwin; Friedman, Richard A.; Ying, Haoqiang; Chen, Emily I.; Luo, Ji; Miao, Yi; Qiu, Wanglong; Su, Gloria H.

doi:10.1038/s41388-021-02040-9

Cited by 15 publications

(16 citation statements)

References 66 publications

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“…Hippo Signaling Pathway. Oncogenes often promote tumor progression by regulating the signaling pathways [12,13]. Kyoto Encyclopedia of Genes and Genomes (KEGG) enrichment analysis showed that TOP2A was associated to cell cycle, progesterone-mediated oocyte maturation, p53 signaling pathway, and Hippo signaling pathway (Figure 5(a)).…”

Section: Top2a Affecting Hcc Tumor Progression Throughmentioning

confidence: 99%

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DNA Topoisomerase II-α Regulated by miR-22-5p Promotes Hepatocellular Carcinoma Invasion and Migration through the Hippo Pathway

Zhao

Chen

Song

et al. 2022

Oxidative Medicine and Cellular Longevity

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DNA topoisomerases (TOPs) are dysregulated in various types of cancer. However, how TOP II-alpha (TOP2A) contributes to hepatocellular carcinoma (HCC) progression remains elusive. Cohort analysis revealed that the increased expression of TOP2A was associated with poor clinical outcomes and TOP2A was significantly upregulated in HCC tissues and cell lines. In vitro, TOP2A expression level is related to cell invasion and migration, which may be due to the alteration of epithelial-mesenchymal transition by the TOP2A. Moreover, we used verteporfin (a Hippo inhibitor) to test how the Hippo pathway promotes the effect of TOP2A on the HCC phenotype and found that TOP2A induces tumor progression through the Hippo pathway. Finally, miR-22-5p inhibited tumor progression by sponging TOP2A.

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Section: Top2a Affecting Hcc Tumor Progression Throughmentioning

confidence: 99%

“…Dysregulation of the Hippo signaling pathway promotes cancer progression [ 12 , 13 ]. Moya et al [ 14 ] found that the activity of yes-associated protein (YAP) and transcriptional coactivator with PDZ-binding motif (TAZ) in tumors was linked to the progression of liver tumors.…”

Section: Introductionmentioning

confidence: 99%

DNA Topoisomerase II-α Regulated by miR-22-5p Promotes Hepatocellular Carcinoma Invasion and Migration through the Hippo Pathway

Zhao

Chen

Song

et al. 2022

Oxidative Medicine and Cellular Longevity

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“…We focused on two 14-3-3 proteins, 14-3-3 zeta and 14-3-3 gamma, and two protein phosphatases, protein phosphatase 1 catalytic subunit alpha (PPP1CA) and PP2Ac (Fig. 5E), because they have been reported to participate in the regulation of YAP in multiple tissues (Hu et al, 2017; Meng et al, 2016; Qi et al, 2015; Schlegelmilch et al, 2011; Sun et al, 2021; Yan et al, 2021). It is known that the turnover of YAP is regulated through its phosphorylation and ubiquitination in a 14-3-3 dependent manner.…”

Section: Resultsmentioning

confidence: 99%

LSR Targets YAP to Modulate Intestinal Paneth Cell Differentiation

Wang

Fan

et al. 2022

Preprint

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Lipolysis-stimulated lipoprotein receptor (LSR) is a multi‐functional protein that is best known for its roles in assembly of epithelial tricellular tight junctions and hepatic clearance of lipoproteins. Here, we investigate the function of LSR in intestine biology. By using multiple conditional deletion mouse models and ex vivo cultured organoids, we find that LSR elimination in intestinal stem cells results in disappearance of Paneth cell without affecting the differentiation of other cell lineages. Mechanistic studies reveal that LSR deficiency increase abundance and nuclear localization of YAP by modulating its phosphorylation and proteasomal degradation. Intestinal LSR-deficient mice are susceptible to development of necrotizing enterocolitis. In addition, LSR can sense and interpret fatty acid signals derived from dietary lipids and transduce into inactivation of YAP. Thus, this study identifies LSR as an upstream negative regulator of YAP activity and part of the mechanism mediating connection between fat diet and YAP signaling in intestine.

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“…The relationship between YAP and the RAF/MEK/ERK cascade was discovered by genetic screens, which showed that the inhibitory combination of RAF or MEK with YAP has increased efficacy not only in BRAF-mutant cancers but also in KRAS-mutant cancers (67). In a KRAS G12C mutant PDAC model, inhibition of YAP1 improves the efficacy of KRAS blockade (68). c-MYC is another oncogenic transcription factor being involved in crucial processes such as metabolic reprograming, extracellular matrix remodeling, inflammation, and regulation of a variety of malignant features in cancer (69).…”

Section: Non-genetic Adaptive Resistance Kras G12c Inhibition: Symbio...mentioning

confidence: 99%

Section: Non-genetic Adaptive Resistance Kras G12c ...mentioning

confidence: 99%

Non-genetic adaptive resistance to KRASG12C inhibition: EMT is not the only culprit

et al. 2022

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Adaptions to therapeutic pressures exerted on cancer cells enable malignant progression of the tumor, culminating in escape from programmed cell death and development of resistant diseases. A common form of cancer adaptation is non-genetic alterations that exploit mechanisms already present in cancer cells and do not require genetic modifications that can also lead to resistance mechanisms. Epithelial-to-mesenchymal transition (EMT) is one of the most prevalent mechanisms of adaptive drug resistance and resulting cancer treatment failure, driven by epigenetic reprogramming and EMT-specific transcription factors. A recent breakthrough in cancer treatment is the development of KRASG12C inhibitors, which herald a new era of therapy by knocking out a unique substitution of an oncogenic driver. However, these highly selective agents targeting KRASG12C, such as FDA-approved sotorasib (AMG510) and adagrasib (MRTX849), inevitably encounter multiple mechanisms of drug resistance. In addition to EMT, cancer cells can hijack or rewire the sophisticated signaling networks that physiologically control cell proliferation, growth, and differentiation to promote malignant cancer cell phenotypes, suggesting that inhibition of multiple interconnected signaling pathways may be required to block tumor progression on KRASG12C inhibitor therapy. Furthermore, the tumor microenvironment (TME) of cancer cells, such as tumor-infiltrating lymphocytes (TILs), contribute significantly to immune escape and tumor progression, suggesting a therapeutic approach that targets not only cancer cells but also the TME. Deciphering and targeting cancer adaptions promises mechanistic insights into tumor pathobiology and improved clinical management of KRASG12C-mutant cancer. This review presents recent advances in non-genetic adaptations leading to resistance to KRASG12C inhibitors, with a focus on oncogenic pathway rewiring, TME, and EMT.

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Loss of the wild-type KRAS allele promotes pancreatic cancer progression through functional activation of YAP1

Cited by 15 publications

References 66 publications

DNA Topoisomerase II-α Regulated by miR-22-5p Promotes Hepatocellular Carcinoma Invasion and Migration through the Hippo Pathway

DNA Topoisomerase II-α Regulated by miR-22-5p Promotes Hepatocellular Carcinoma Invasion and Migration through the Hippo Pathway

LSR Targets YAP to Modulate Intestinal Paneth Cell Differentiation

Non-genetic adaptive resistance to KRASG12C inhibition: EMT is not the only culprit

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