β-Catenin Activation in a Novel Liver Progenitor Cell Type Is Sufficient to Cause Hepatocellular Carcinoma and Hepatoblastoma

Mokkapati, Sharada; Niopek, Katharina; Huang, Le; Cunniff, Kegan J.; Ruteshouser, E. Cristy; deCaestecker, Mark; Finegold, Milton J.; Huff, Vicki

doi:10.1158/0008-5472.can-13-3275

Cited by 93 publications

(74 citation statements)

References 45 publications

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“…␤-catenin as the key effector of the Wnt-pathway has been shown to modulate numerous processes including gene expression, cell proliferation, epithelial-mesenchymal transition, and tumor progression (15,27,64,65). Although the role of ␤-catenin in many cellular processes has been known for many years, we are still at the beginning of understanding how its multiple dynamic and interdependent functions are orchestrated in a spatial and temporal manner.…”

Section: Discussionmentioning

confidence: 99%

Monitoring Interactions and Dynamics of Endogenous Beta-catenin With Intracellular Nanobodies in Living Cells*

Traenkle

Emele

Anton

et al. 2015

Molecular & Cellular Proteomics

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Section: Discussionmentioning

confidence: 99%

Monitoring Interactions and Dynamics of Endogenous Beta-catenin With Intracellular Nanobodies in Living Cells*

Traenkle

Emele

Anton

et al. 2015

Molecular & Cellular Proteomics

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“…Moreover, as tumors frequently show hyperstabilization of Myc, mRNA profiling of HBs in the absence of follow up analysis of Myc at the protein level runs the risk of underestimating and diminishing the significance of this oncogenic transcription factor in HB (63,64). However, in light of the fact that Myc emerged as the dominant driver of HBs in this study and that Myc is overexpressed in chemically induced mouse HBs (65) as well as in HBs and HCCs that develop in mouse models following expression of oncogenes other than Myc (33,36), we propose that Myc serves as a central signaling hub for an array of other oncogenic HB drivers, making it a potentially important therapeutic target in HB that could benefit from the array of promising new drugs that target Myc and its network (66,67). Therefore, the feasibility of adopting Myc inhibitory strategies for the treatment of pediatric liver cancers and other embryonal tumors with evidence of Myc amplification/ overexpression should be explored.…”

Section: Mycmentioning

confidence: 81%

“…However, this is unlikely to be the case in Tet-O-Myc mice or other mouse models that develop HBs following oncogene activation in mature hepatocytes (32,33), raising the question of whether HB transcriptomes and immunoprofiles reflect a hepatoblast cell of origin or the end result of dedifferentiation or reprogramming of mature hepatocytes (34). While an abundance of experimental evidence indicates that aberrant activation of Wnt/β-catenin alone is not sufficient for HB development, this has recently been challenged by the creation of a genetically engineered mouse strain that develops HBs and HCCs when mutant β-catenin is targeted to rare hepatic progenitor cells that express the CBP/p300 transcriptional coactivator protein and Myc target, Cited1 (35,36). Although the experimental strategy used to target β-catenin to the liver in this strain differs from ours, in both instances, the timing of β-catenin activation overlaps with a period of high fetal liver expression of Myc (37).…”

Section: Discussionmentioning

confidence: 99%

Hepatoblastoma modeling in mice places Nrf2 within a cancer field established by mutant β-catenin

Comerford¹,

Hinnant²,

Chen³

et al. 2016

JCI Insight

Self Cite

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“…The company filed a first patent in 2011 on PI3K/mTOR inhibitors,334 of which one, SPR965, has reached the preclinical evaluation stage 335, 336. The compound is likely to be structurally related, if not identical to a compound recently described in a publication 337.…”

Section: Drug Discovery In Indiamentioning

confidence: 99%

The Drug Discovery and Development Industry in India—Two Decades of Proprietary Small‐Molecule R&D

Differding¹

2017

ChemMedChem

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This review provides a comprehensive survey of proprietary drug discovery and development efforts performed by Indian companies between 1994 and mid‐2016. It is based on the identification and detailed analysis of pharmaceutical, biotechnology, and contract research companies active in proprietary new chemical entity (NCE) research and development (R&D) in India. Information on preclinical and clinical development compounds was collected by company, therapeutic indication, mode of action, target class, and development status. The analysis focuses on the overall pipeline and its evolution over two decades, contributions by type of company, therapeutic focus, attrition rates, and contribution to Western pharmaceutical pipelines through licensing agreements. This comprehensive analysis is the first of its kind, and, in our view, represents a significant contribution to the understanding of the current state of the drug discovery and development industry in India.

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β-Catenin Activation in a Novel Liver Progenitor Cell Type Is Sufficient to Cause Hepatocellular Carcinoma and Hepatoblastoma

Cited by 93 publications

References 45 publications

Monitoring Interactions and Dynamics of Endogenous Beta-catenin With Intracellular Nanobodies in Living Cells*

Monitoring Interactions and Dynamics of Endogenous Beta-catenin With Intracellular Nanobodies in Living Cells*

Hepatoblastoma modeling in mice places Nrf2 within a cancer field established by mutant β-catenin

The Drug Discovery and Development Industry in India—Two Decades of Proprietary Small‐Molecule R&D

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