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Merck

Long-term hepatitis B virus infection of rhesus macaques requires suppression of host immunity.

Nature communications (2022-06-01)
Sreya Biswas, Lauren N Rust, Jochen M Wettengel, Sofiya Yusova, Miranda Fischer, Julien N Carson, Josie Johnson, Lei Wei, Trason Thode, Mohan R Kaadige, Sunil Sharma, Majd Agbaria, Benjamin N Bimber, Thomas Tu, Ulrike Protzer, Alexander Ploss, Jeremy V Smedley, Gershon Golomb, Jonah B Sacha, Benjamin J Burwitz
RESUMEN

Hepatitis B virus has infected a third of the world's population, and 296 million people are living with chronic infection. Chronic infection leads to progressive liver disease, including hepatocellular carcinoma and liver failure, and there remains no reliable curative therapy. These gaps in our understanding are due, in large part, to a paucity of animal models of HBV infection. Here, we show that rhesus macaques regularly clear acute HBV infection, similar to adult humans, but can develop long-term infection if immunosuppressed. Similar to patients, we longitudinally detected HBV DNA, HBV surface antigen, and HBV e antigen in the serum of experimentally infected animals. In addition, we discovered hallmarks of HBV infection in the liver, including RNA transcription, HBV core and HBV surface antigen translation, and covalently closed circular DNA biogenesis. This pre-clinical animal model will serve to accelerate emerging HBV curative therapies into the clinic.

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Casein from bovine milk, technical grade
Roche
Kit iniciador de detección y marcaje de ADN DIG-High Prime, sufficient for 12 labeling reactions (10 ng to 3 μg per assay), sufficient for 24 blots (blots of 100 cm2)