Post-translational deregulation of YAP1 is genetically controlled in rat liver cancer and determines the fate and stem-like behavior of the human disease

Simile, Maria M.; Latte, Gavinella; Demartis, Maria I.; Brozzetti, Stefania; Calvisi, Diego F.; Porcu, Alberto; Feo, Claudio F; Seddaiu, Maria A.; Daino, Lucia; Berasain, Carmen; Tomasi, Maria Lauda; Avila, Matı́as A.; Feo, Francesco; Pascale, Rosa M.

doi:10.18632/oncotarget.10246

Cited by 22 publications

(22 citation statements)

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“…As shown in Table , heterogeneity analysis of the relationship between YAP expression and AFP indicated no significant heterogeneity among the studies. YAP is involved in many signalling pathways associated with HCC, but its actual role is unclear and worthy of investigation, especially because Simile's group reported that upregulation of YAP is related to HCC prognosis.…”

Section: Discussionmentioning

confidence: 99%

Overexpression of Yes‐associated protein and its association with clinicopathological features of hepatocellular carcinoma: A meta‐analysis

Lin

Lei

et al. 2017

Liver International

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BackgroundYes‐associated protein (YAP) overexpression is reported to be associated with risk of hepatocellular carcinoma (HCC) but current studies have not explored the relationship between YAP expression with HCC clinicopathological features.MethodsTo assess these associations, a meta‐analysis was performed which included four eligible studies including 391 HCC cases and 334 controls. There were eight eligible studies to investigate the association between YAP expression in HCC and clinicopathological features of liver cancer patients. Literature was obtained from PubMed, Embase, Wangfang and China National Knowledge Infrastructure.ResultsAnalysis indicated that YAP expression in HCC was greater than in adjacent non‐tumour tissue (odds ratio [OR], 15.80, 95% confidence interval [CI], 10.53‐23.70, P<.00001; heterogeneity=.30). YAP overexpression in HCC was significantly associated with vascular invasion (OR, 2.21, 95% CI, 11.64‐2.97, P<.00001, heterogeneity=.10), less cellular differentiation (OR, 2.38, 95% CI, 1.61‐3.51, P<.00001, heterogeneity=.333), tumours larger than 5 cm (OR, 2.52, 95% CI, 1.75‐3.62, P<.00001; heterogeneity=.17) and TNM tumour stage I + II (OR, 0.44, 95% CI, 0.28‐0.75, P=.00003, heterogeneity=.12).ConclusionsOverexpression of YAP contributes to HCC formation, and its overexpression is associated with vascular invasion, low cellular differentiation tumours larger than 5 cm and TNM tumour stage III + IV.

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Section: Discussionmentioning

confidence: 99%

Overexpression of Yes‐associated protein and its association with clinicopathological features of hepatocellular carcinoma: A meta‐analysis

Lin

Lei

et al. 2017

Liver International

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“…YAP increases glycolysis [ 179 ] and supports the expression of Glut3, a known driver of a cancer stem cell phenotype, whose expression is elevated in cancer [ 18 , 182 ]. YAP/TAZ/TEAD and AP-1 form a complex that synergistically activates target genes controlling S-phase entry and mitosis [ 183 ]. In addition, in HepG2, Huh7, and Hep3B cells, forced YAP1 over-expression results in the expression of stem cell markers and increases cell viability [ 182 ].…”

Section: The Warburg Effect and Tumor Therapymentioning

confidence: 99%

The Warburg Effect 97 Years after Its Discovery

Pascale

Calvisi

Simile

et al. 2020

Cancers

Self Cite

211

128

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The deregulation of the oxidative metabolism in cancer, as shown by the increased aerobic glycolysis and impaired oxidative phosphorylation (Warburg effect), is coordinated by genetic changes leading to the activation of oncogenes and the loss of oncosuppressor genes. The understanding of the metabolic deregulation of cancer cells is necessary to prevent and cure cancer. In this review, we illustrate and comment the principal metabolic and molecular variations of cancer cells, involved in their anomalous behavior, that include modifications of oxidative metabolism, the activation of oncogenes that promote glycolysis and a decrease of oxygen consumption in cancer cells, the genetic susceptibility to cancer, the molecular correlations involved in the metabolic deregulation in cancer, the defective cancer mitochondria, the relationships between the Warburg effect and tumor therapy, and recent studies that reevaluate the Warburg effect. Taken together, these observations indicate that the Warburg effect is an epiphenomenon of the transformation process essential for the development of malignancy.

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“…Activates p53 in response to mitotic stress 53,[142][143][144]149 Activates p53 in response to oncogenic Ras 117,118 Activates p53 in response to excess cholesterol 156 Activates p53 during mESC differentiation 52 YAP Loss of YAP induces p53 145,147,148 YAP represses ΔNp63 to inhibit lung cancer squamous cells transdifferentiation. 182 YAP-p73 promotes apoptosis 106,108-110, 132-134, 136,183 Yki inactivation induces Dmp53 119 p63 inhibits p73-YAPdependent apoptosis 22,137 YAP-tyr357-p73 is a marker for well differentiated HCC 85 Yki binds Dmp53 to promote apoptosis 131 YAP positively regulates p63 in epidermal stem cells 66 Locus is amplified in p53 null tumors [75][76][77]184,185 YAP positively regulates p63 in airway epithelium 71 p53 and YAP antagonistically regulate FOXM1 [186][187][188] YAP-p63 block differentiation in HNSCC 86 p53 transactivates 14-3-3σ, which inhibits YAP/TAZ 124,125 Binds p63 and prevents its degradation 88,89 YAP and p53 cooperate in apoptosis and senescence [126][127][128] Hyperactivation of YAP/TAZ induces p53 152,154 YAP and mutp53 cooperate in transformation 33,82 Mutp53 induces miRs that tar...…”

Section: Lats2mentioning

confidence: 99%

“…83 Interestingly, different post-translational modifications, which have been shown to govern YAP stability, may dictate the differentiation status of HCC. 84,85 Although hyperactivity of the YAP-TEAD functional axis predicts poor prognosis and stemness characteristics in HCC, tumors in which YAP is modified to interact with p73 (p-Y357) display more apoptotic markers and have better prognosis. 85 Thus, YAP can promote either tumor cell death or tumor-initiating properties, depending on its regulatory interactions with different members of the p53 family.…”

Section: Cancer Stem Cellsmentioning

confidence: 99%

“…84,85 Although hyperactivity of the YAP-TEAD functional axis predicts poor prognosis and stemness characteristics in HCC, tumors in which YAP is modified to interact with p73 (p-Y357) display more apoptotic markers and have better prognosis. 85 Thus, YAP can promote either tumor cell death or tumor-initiating properties, depending on its regulatory interactions with different members of the p53 family. In the next sections, we will review in more detail the YAP-p73 pro-apoptotic module and try to delineate the mechanisms that modulate the apparently opposing cellular functions of YAP.…”

Section: Cancer Stem Cellsmentioning

confidence: 99%

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p53 shades of Hippo

2017

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The three p53 family members, p53, p63 and p73, are structurally similar and share many biochemical activities. Yet, along with their common fundamental role in protecting genomic fidelity, each has acquired distinct functions related to diverse cell autonomous and non-autonomous processes. Similar to the p53 family, the Hippo signaling pathway impacts a multitude of cellular processes, spanning from cell cycle and metabolism to development and tumor suppression. The core Hippo module consists of the tumor-suppressive MST-LATS kinases and oncogenic transcriptional co-effectors YAP and TAZ. A wealth of accumulated data suggests a complex and delicate regulatory network connecting the p53 and Hippo pathways, in a highly context-specific manner. This generates multiple layers of interaction, ranging from interdependent and collaborative signaling to apparent antagonistic activity. Furthermore, genetic and epigenetic alterations can disrupt this homeostatic network, paving the way to genomic instability and cancer. This strengthens the need to better understand the nuances that control the molecular function of each component and the cross-talk between the different components. Here, we review interactions between the p53 and Hippo pathways within a subset of physiological contexts, focusing on normal stem cells and development, as well as regulation of apoptosis, senescence and metabolism in transformed cells.

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Post-translational deregulation of YAP1 is genetically controlled in rat liver cancer and determines the fate and stem-like behavior of the human disease

Cited by 22 publications

References 61 publications

Overexpression of Yes‐associated protein and its association with clinicopathological features of hepatocellular carcinoma: A meta‐analysis

Overexpression of Yes‐associated protein and its association with clinicopathological features of hepatocellular carcinoma: A meta‐analysis

The Warburg Effect 97 Years after Its Discovery

p53 shades of Hippo

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