Xinhe Wang scite author profile

The prion hypothesis posits that a misfolded form of prion protein (PrP) is responsible for the infectivity of prion disease. Using recombinant murine PrP purified from Escherichia coli, we created a recombinant prion with the hallmarks of the pathogenic PrP isoform: aggregated, protease-resistant, and self-perpetuating. After intracerebral injection of the recombinant prion, wild-type mice developed neurological signs in ~130 days and reached the terminal stage of disease in ~150 days. Characterization of diseased mice revealed classic neuropathology of prion disease, the presence of protease-resistant PrP, and the capability of serially transmitting the disease, confirming that these mice succumbed to prion disease. Thus, as postulated by the prion hypothesis, the infectivity in mammalian prion disease results from an altered conformation of PrP.

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Foxm1b transcription factor is essential for development of hepatocellular carcinomas and is negatively regulated by the p19^ARF tumor suppressor

Kalinichenko¹,

Major²,

Wang³

et al. 2004

Genes Dev.

351

410

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The Forkhead Box m1b transcription factor is essential for hepatocyte DNA replication and mitosis during mouse liver regeneration

Wang

Kiyokawa

Dennewitz

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

306

354

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The Forkhead Box (Fox) proteins are an extensive family of transcription factors that shares homology in the winged helix DNAbinding domain and whose members play essential roles in cellular proliferation, differentiation, transformation, longevity, and metabolic homeostasis. Liver regeneration studies with transgenic mice demonstrated that FoxM1B regulates the onset of hepatocyte DNA replication and mitosis by stimulating expression of cell cycle genes. Here, we demonstrate that albumin-promoter-driven Cre recombinase-mediated hepatocyte-specific deletion of the Foxm1b Floxed (fl) targeted allele resulted in significant reduction in hepatocyte DNA replication and inhibition of mitosis after partial hepatectomy. Reduced DNA replication in regenerating Foxm1b ؊/؊ hepatocytes was associated with sustained increase in nuclear staining of the cyclin-dependent kinase (Cdk) inhibitor p21 Cip1 (p21) protein between 24 and 40 h after partial hepatectomy. Furthermore, increased nuclear p21 levels and reduced expression of Cdc25A phosphatase coincided with decreases in Cdk2 activation and hepatocyte progression into S-phase. Moreover, the significant reduction in hepatocyte mitosis was associated with diminished mRNA levels and nuclear expression of Cdc25B phosphatase and delayed accumulation of cyclin B1 protein, which is required for Cdk1 activation and entry into mitosis. Cotransfection studies demonstrate that FoxM1B protein directly activated transcription of the Cdc25B promoter region. Our present study shows that the mammalian Foxm1b transcription factor regulates expression of cell cycle proteins essential for hepatocyte entry into DNA replication and mitosis.knock-out mouse ͉ Cdc25A ͉ Cdc25B ͉ cyclin-dependent kinase inhibitor p21 Cip1

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Xinhe Wang

Generating a Prion with Bacterially Expressed Recombinant Prion Protein

Foxm1b transcription factor is essential for development of hepatocellular carcinomas and is negatively regulated by the p19^ARF tumor suppressor

The Forkhead Box m1b transcription factor is essential for hepatocyte DNA replication and mitosis during mouse liver regeneration

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About

Xinhe Wang

Generating a Prion with Bacterially Expressed Recombinant Prion Protein

Foxm1b transcription factor is essential for development of hepatocellular carcinomas and is negatively regulated by the p19ARF tumor suppressor

The Forkhead Box m1b transcription factor is essential for hepatocyte DNA replication and mitosis during mouse liver regeneration

Contact Info

Product

Resources

About

Foxm1b transcription factor is essential for development of hepatocellular carcinomas and is negatively regulated by the p19^ARF tumor suppressor