Belinda Hsi scite author profile

Tumor necrosis factor (TNF) family ligand TNF-␣ and Fas ligand (FasL) can trigger apoptosis in solid tumors, but their clinical usage has been limited by hepatotoxicity. TNF-related apoptosis-inducing ligand (TRAIL) is a newly identified member of the TNF family, and its clinical application currently is under a similar debate. Here, we report a recombinant soluble form of human TRAIL (114 to 281 amino acids) that induces apoptosis in tumor cells but not human hepatocytes. We first isolated human hepatocytes from patients and showed that the human hepatocytes expressed Fas but no TRAIL death receptor DR4 and little DR5 on the cell surface. Antibody cross-linked FasL, but not TRAIL, triggered apoptosis of the human hepatocytes through cleavage of caspases. We then examined TRAIL hepatotoxicity in severe combined immunodeficient/Alb-uPA chimeric mice harboring human hepatocytes. Intravenous injection of FasL, but not TRAIL, caused apoptotic death of human hepatocytes within the chimeric liver, thus killing the mice. Finally, we showed that repeated intraperitoneal injections of TRAIL inhibited intraperitoneal and subcutaneous tumor growth without inducing apoptosis in human hepatocytes in these chimeric mice. The results indicate that the recombinant soluble human TRAIL has a profound apoptotic effect on tumor cells but is nontoxic to human hepatocytes in vitro and in vivo.

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Anti-HCV therapies in chimericscid-Alb/uPA mice parallel outcomes in human clinical application

Kneteman

Weiner²,

O’Connell³

et al. 2006

Hepatology

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Modified apoptotic molecule (BID) reduces hepatitis C virus infection in mice with chimeric human livers

et al. 2003

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Hepatitis C virus (HCV) encodes a polyprotein consisting of core, envelope (E1, E2, p7), and nonstructural polypeptides (NS2, NS3, NS4A, NS4B, NS5A, NS5B). The serine protease (NS3/NS4A), helicase (NS3), and polymerase (NS5B) constitute valid targets for antiviral therapy. We engineered BH3 interacting domain death agonist (BID), an apoptosis-inducing molecule, to contain a specific cleavage site recognized by the NS3/NS4A protease. Cleavage of the BID precursor molecule by the viral protease activated downstream apoptotic molecules of the mitochondrial pathway and triggered cell death. We extended this concept to cells transfected with an infectious HCV genome, hepatocytes containing HCV replicons, a Sindbis virus model for HCV, and finally HCV-infected mice with chimeric human livers. Infected mice injected with an adenovirus vector expressing modified BID exhibited HCV-dependent apoptosis in the human liver xenograft and considerable declines in serum HCV titers.

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219 FasL, but not TRAIL, induces apoptosis in human hepatocytes in chimeric mice

Hao¹,

Song²,

Hsi³

et al. 2004

European Journal of Cancer Supplements

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The expression of receptors for epidermal growth factor and transferrin on human trophoblast

Yeh¹,

Mühlhauser²,

Hsi³

et al. 1989

Placenta

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Belinda Hsi

TRAIL Inhibits Tumor Growth but Is Nontoxic to Human Hepatocytes in Chimeric Mice

Anti-HCV therapies in chimericscid-Alb/uPA mice parallel outcomes in human clinical application

Modified apoptotic molecule (BID) reduces hepatitis C virus infection in mice with chimeric human livers

219 FasL, but not TRAIL, induces apoptosis in human hepatocytes in chimeric mice

The expression of receptors for epidermal growth factor and transferrin on human trophoblast

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