Expansion, in vivo–ex vivo cycling, and genetic manipulation of primary human hepatocytes

et al. 2020

Cell Host & Microbe

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Section: Author Contributionsmentioning

confidence: 99%

A Combination of Human Broadly Neutralizing Antibodies against Hepatitis B Virus HBsAg with Distinct Epitopes Suppresses Escape Mutations

Wang

et al. 2020

Cell Host & Microbe

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“…To investigate how the human graft in liver chimeric mouse models responds to a hypercaloric diet, we first created humanized mice by transplanting primary human hepatocytes (PHH) into preconditioned immunocompromised Fah -/-NOD Rag1 -/-Il2rg null (FNRG) mice as described previously. 24,25 Cycling the protective drug nitisinone 26 resulted in at least 50% humanization after which mice were subjected to an ad libitum Western-style diet (WD), which consists of 60% fat in diet and 10% sucrose in drinking water (Fig 1a). WD feeding did not result in graft loss as determined by persistently high [27][28][29] human serum albumin (hAlb) levels (Suppl Fig S1a).…”

Section: Human Hepatocytes In Chimeric Mice On Western Diet Rapidly Dmentioning

confidence: 99%

Human hepatocyte PNPLA3 148M exacerbates rapid non-alcoholic steatohepatitis development in chimeric mice

Kabbani

Steensels

et al. 2020

Preprint

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Advanced non-alcoholic fatty liver disease (NAFLD) is a rapidly emerging global health problem associated with pre-disposing genetic polymorphisms, most strikingly an isoleucine to methionine substitution in patatin-like phospholipase domain-containing protein 3 (PNPLA3-I148M). Here, we study how human hepatocytes with PNPLA3 148I and 148M variants engrafted in the livers of chimeric mice respond to a hypercaloric Western-style diet. As early as 4 weeks, mice developed dyslipidemia, impaired glucose tolerance, and steatohepatitis selectively in the human graft, followed by pericellular fibrosis after 8 weeks of hypercaloric feeding. The PNPLA3 148M variant, either from a homozygous 148M human donor or overexpressed in a homozygous 148I donor background, caused widespread microvesicular steatosis and even more severe steatohepatitis. We conclude that PNPLA3 148M in human hepatocytes exacerbates NAFLD. These models will facilitate mechanistic studies into human genetic variants associated with advanced fatty liver diseases.

“…The 50% inhibitory concentration (IC 50 ) values were calculated based on HBsAg/HBeAg ELISA or immunofluorescence staining for HBcAg expression (Michailidis et al, 2017) (Figure 5C). Neutralizing activity was further verified by in vitro neutralization assays using primary human hepatocytes (Michailidis et al, 2020) (Figure 5C and 5D). Fourteen of the 20 antibodies tested showed neutralizing activity with IC 50 values as low as 5 ng/ml (Figure 5C).…”

Section: Resultsmentioning

confidence: 82%

Public broadly neutralizing antibodies against hepatitis B virus in individuals with elite serologic activity

Wang

et al. 2020

Preprint

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SUMMARYAlthough there is no effective cure for chronic hepatitis B virus (HBV) infection, antibodies are protective and constitute clinical correlates of recovery from infection. To examine the human neutralizing antibody response to HBV in elite neutralizers we screened 144 individuals. The top individuals produced shared clones of broadly neutralizing antibodies (bNAbs) that targeted 3 non-overlapping epitopes on the HBV S antigen (HBsAg). Single bNAbs protected humanized mice against infection, but selected for resistance mutations in mice with established infection. In contrast, infection was controlled by a combination of bNAbs targeting non-overlapping epitopes with complementary sensitivity to mutations that commonly emerge during human infection. The co-crystal structure of one of the bNAbs with a peptide epitope containing residues frequently mutated in human immune escape variants revealed a loop anchored by oppositely charged residues. The structure provides a molecular explanation for why immunotherapy for HBV infection may require combinations of complementary bNAbs.