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by
Jane Heffernan
Centre for Disease Modelling, York University
Coauthors: Seyed Moghadas, Centre for Disease Modelling, York University
Minisymposium
Abstract:
Multidisciplinary has become the watchword of modern biology. The
integration of several disciplines has created a rapidly growing
multidisciplinary field of research, the so-called “Mathematical
Immunology”. In simple terms, mathematical immunology attempts
to uncover the biological mechanisms underlying the dynamics of
pathogen-host interactions by employing mathematical, statistical,
and computational models. In recent years, the field of mathematical
immunology has blossomed with the availability of large and rich
datasets due to the genomics revolution and increased sensitivity
of laboratory and clinical tools; the development of mathematical
tools capable of encapsulating complex nonlinear systems; and the
advancement in computing power for large-scale calculations, simulation,
and visualization. Interest in the computer simulation of biological
processes to reduce complications incurred in human and animal research
(such as ethical and practical considerations, costs, and risks)
has also increased attention to this field. Although not old, mathematical
immunology has contributed greatly to the understanding of within-host
dynamics of many diseases that have been the bane of humanity for
many centuries, such as Tuberculosis (TB), Influenza, Measles and
Malaria, and infections that have been discovered in the past few
decades including the Human Immunodeficiency Virus (HIV), and Hepatits
B and C viruses (HBV and HCV).
This symposium provides an opportunity to present important contributions
to the field of mathematical immunology that have been made by several
members and collaborators of the York University Centre for Disease
Modelling. We hope that the presentations and interactions during
this symposium will lead to further collaborations in
the subject area.
Jane Heffernan, York University
A two compartment model for HBV/HCV
HBV
and HCV can cause chronic infections of the liver. Liver transplantation
was originally thought to be a cure of chronic HBV or HCV, however,
reinfection of the new liver graft would occur. This points to
a second compartment of infection. We have developed a mathematical
model of HBV or HCV in-host including a second compartment of
infection. A backward bifurcation is found relating to production
rates of the virus and the death rates of infected cells in both
compartments of infection.
Robert Smith?, University of Ottawa
Modelling Mutation to a Cytotoxic T-lymphocyte HIV Vaccine
Abstract:
Resistance to a postinfection HIV vaccine that stimulates cytotoxic
T-lymphocytes (CTLs) depends on the relationship between the vaccine
strength, the fitness cost of the mutant strain, and the rate
of mutant escape. If the vaccine is strong enough, both strains
of the virus should be controlled by administering the vaccine
sufficiently often. However, if escape mutation to the vaccine
occurs, then either the wild type or the mutant can outcompete
the other strain. Imperfect adherence may result in the persistence
of the mutant, while fluctuations in the vaccination time - even
if no vaccines are missed - may result in the mutant outcompeting
the wild type.
Glenn
Webb, Vanderbilt University
Mathematical
Models of Antibiotic Resistant Bacterial Infections in Hospitals
The
development of drug-resistant strains of bacteria is an increasing
threat to society, especially in hospital settings. Many antibiotics
that were formerly effective in combating bacterial infections
in hospital patients are no longer effective due to the evolution
of resistant strains. The evolution of these resistant strains
compromises medical care worldwide. Recent examples are vancomycin-resistant
enterococci epidemics and methicillin-resistant staphylococci
epidemics in US and Canadian hospitals. The objectives of this
work are to investigate mathematical models to analyze the dynamic
elements of patient in-host acquisition and transmission of non-resistant
and resistant bacteria strains in hospital settings, and to provide
understanding of measures to mitigate these epidemics.
Amy
Hurford (York University)
Does the risk of inducing autoimmunity select against molecular
mimicry in parasites?
Parasites
that are molecular mimics capitalize on a host’s natural
aversion to inflict self-harm and are more likely to evade the
immune system and be transmitted. However, in the case of infection-induced
autoimmunity, the immune response is to both normal host cells
and to the parasite, and so parasite strains that are molecular
mimics no longer have a selective advantage. In this talk, I will
show that the evolution of molecular mimicry in parasites is selected
against when there is a substantial risk and cost of inducing
autoimmunity. I will describe characteristics of the parasite
that could be identified to confirm that autoimmunity affects
parasite evolution, and I will show that medical interventions
intended to reduce the risk of autoimmunity may select for molecular
mimicry in parasites and, paradoxically, increase the risk of
infection-induced autoimmunity. This is joint work with Troy Day
(Queen's).
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(withdrawn)Troy
Day (Queen's University)
Theoretical Insights into the Evolution of Drug Resistance
The
evolution of resistance to drugs used for combating infectious
diseases has become one of the most seriouspublic health problems
in modern medicine. In this talk I will present some theoretical
results that explore this problem from several different perspectives,
with the goal of better mitigating the emergence and spread of
resistance. I will show how simple mathematical models of the
within-host dynamics of pathogen replication, can contribute to
this goal. I will conclude by illustrating how these theoretical
results suggest a new approach for preventing the evolution of
resistance.
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