Modelling the Impact of Cell-To-Cell Transmission in Hepatitis B Virus
Authored by Ashish Goyal, John M Murray
Date Published: 2016
DOI: 10.1371/journal.pone.0161978
Sponsors:
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Platforms:
MATLAB
Model Documentation:
Other Narrative
Mathematical description
Model Code URLs:
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Abstract
Cell-free virus is a well-recognized and efficient mechanism for the
spread of hepatitis B virus (HBV) infection in the liver. Cell-to-cell
transmission (CCT) can be a more efficient means of virus propagation.
Despite experimental evidence implying CCT occurs in HBV, its relative
impact is uncertain. We develop a 3-D agent-based model where each
hepatocyte changes its viral state according to a dynamical process
driven by cell-free virus infection, CCT and intracellular replication.
We determine the relative importance of CCT in the development and
resolution of acute HBV infection in the presence of cytolytic (CTL) and
non-CTL mechanisms. T cell clearance number is defined as the minimum
number of infected cells needed to be killed by each T cell at peak
infection that results in infection clearance within 12 weeks with
hepatocyte turnover (HT, number of equivalent livers) <= 3. We find that
CCT has very little impact on the establishment of infection as the mean
cccDNA copies/cell remains between 15 to 20 at the peak of the infection
regardless of CCT strength. In contrast, CCT inhibit immune-mediated
clearance of acute HBV infection as higher CCT strength requires higher
T cell clearance number and increases the probability of T cell
exhaustion. An effective non-CTL inhibition can counter these negative
effects of higher strengths of CCT by supporting rapid, efficient viral
clearance and with little liver destruction. This is evident as the T
cell clearance number drops by approximately 50\% when non-CTL
inhibition is increased from 10\% to 80\%. Higher CCT strength also
increases the probability of the incidence of fulminant hepatitis with
this phenomenon being unlikely to arise for no CCT. In conclusion, we
report the possibility of CCT impacting HBV clearance and its
contribution to fulminant hepatitis.
Tags
Dynamics
Spread
Clearance
Hepatocyte turnover
Hepadnavirus infections
Viral-infection
Half-life
Liver
Transient
Dna