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Does immunodominance maintain the diversity of the common cold?

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This corresponds to an area around a particular strain in the genetic domain ... Continuous time, single strain, SIR model with births/deaths (constant pop. ... – PowerPoint PPT presentation

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Title: Does immunodominance maintain the diversity of the common cold?


1
Does immunodominance maintain the diversity of
the common cold?
  • William Koppelman
  • University of Utah
  • Masters Oral Examination

2
Outline
  • Biological background
  • Mathematical model
  • Analysis/Simulations
  • Results
  • Conclusions

3
Biological Background
  • Rhinovirus characteristics
  • Mutation
  • Cross-reactivity
  • Immunodominance

4
Human Rhinovirus (HRV)
  • Co-circulation of over 100 strains
  • Cause 50 of common colds
  • Limited to high level primates
  • Adults average 2-3 colds per year
  • Able to survive outside host for up to 3 days

5
HRV cont.
  • Sufficient dose is 1-30 particles of the virus
  • Attaches to ICAM-1 receptor of nasal cells
  • Replication of the virus and rupture of the host
    cell leads to infection of other nasal cells
  • Incubation period of 8-12 hours

6
HRV Mutation
  • RNA virus (typically have high mutation rates
  • Predicted to have 0.67 mutations per genome per
    replication
  • 21 replications/infection 14 mutations per
    infection
  • Suggested that new serotype created in 2 to 4
    years from mutation (Stott Walker, 1969)

7
HRV Cross-Reactivity
  • Cross-reactivity is the ability of B and T cells
    to react with an epitope on the antigen that they
    are not designated for.
  • A single HRV serotype is, on average, related to
    3.75 other serotypes (Cooney et al., 1975).
  • Therefore, related serotypes may elicit similar
    immune responses.

8
HRV Immunodominance
  • A process in which the immune response focuses on
    only a few of the many potential epitopes.
  • Original antigenic sin is a process in which the
    sequence a host encounters antigenic variants
    influences the specificity of the immune response.

Antigens Immune Response
Primary Exposure A a
Secondary Exposure A a
9
Mathematical Model
  • Discrete
  • Stochastic
  • Multiple Strain
  • SIRS dynamics

10
Model Components
  • HRV strains exist in a 2-D genetic space.
  • Domain is a 10 x 10 grid with periodic boundaries
  • Each 1 x 1 square represents a strain (i.e. 100
    strains)

11
Model Components cont.
  • Mutation is a distance in the genetic domain.
  • Strains differ by 10 or 800 sites
  • From derived mutation rate gt 50 infections to
    produce new serotype
  • Therefore, a mutation distance of 1/50 per
    infection is reasonable for the domain.

12
Model Components cont.
  • Serotypes will cross-react with related serotypes
  • This corresponds to an area around a particular
    strain in the genetic domain
  • Equivalent to a circle (radius Xim) not including
    the original serotype

13
Model Components cont.
  • Immunodominance will affect the transmission of
    HRV
  • The function of transmission will be related to
    the amount of variance from strains previously
    seen by the immune system
  • Step function is simplest, realistic form

14
Model components cont.
  • Sub-population of environmental surfaces obey SIS
    dynamics
  • Stochastic elements
  • Random contact (uniform)
  • Random mutation (normal)
  • Random recovery time (log-normal)
  • Random birth death (uniform)
  • Transmitting antigen compared against hosts
    immunity history

15
Analysis of continuous equivalent
  • Continuous time, single strain, SIR model with
    births/deaths (constant pop.)
  • Assuming the birth rate is much smaller than the
    recovery rate then i is the equilibrium
    prevalence

16
Endemic analysis
  • Strain remains endemic if R0gt1
  • Using estimated parameters from discrete model
  • Human birth rate is O(10-4)

17
Sub-population analysis
  • Model with hosts following SIR dynamics and
    surfaces following SIS dynamics
  • System has two equilibria with the trivial
    solution never being unstable

18
Simulations (Infection)
19
Simulations (Immunity)
20
Simulations (Prev. Div.)
21
Results
  • In order to consider mechanisms influencing
    serotype diversity, the virus must be endemic in
    hosts
  • Different functions of transmission should lead
    to endemic by increasing virus dynamics within
    cross-reactivity distance.

22
Conclusions
  • Virus must be endemic to analyze diversity
  • Serotype interactions are crucial to virus
    remaining endemic
  • Once endemic, the diversity of serotypes will
    evolve through serotype interactions
  • Serotype interactions are governed by
    immunodominance

23
Thanks
  • Dr. Adler
  • Drs. Keener Coley
  • Dr. Guy
  • Brynja Kohler
  • John Zobitz
  • Dr. Sherry
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