280 research outputs found
A resampling-based test to detect person-to-person transmission of infectious disease
Early detection of person-to-person transmission of emerging infectious
diseases such as avian influenza is crucial for containing pandemics. We
developed a simple permutation test and its refined version for this purpose. A
simulation study shows that the refined permutation test is as powerful as or
outcompetes the conventional test built on asymptotic theory, especially when
the sample size is small. In addition, our resampling methods can be applied to
a broad range of problems where an asymptotic test is not available or fails.
We also found that decent statistical power could be attained with just a small
number of cases, if the disease is moderately transmissible between humans.Comment: Published at http://dx.doi.org/10.1214/07-AOAS105 in the Annals of
Applied Statistics (http://www.imstat.org/aoas/) by the Institute of
Mathematical Statistics (http://www.imstat.org
Optimizing Vaccine Allocation at Different Points in Time during an Epidemic
For current pandemic influenza H1N1, vaccine production started in the early summer, and vaccination started in the fall. In most countries, by the time vaccination started, the second wave of H1N1 was already under way. With limited supplies of vaccine, it might be a good strategy to vaccinate the high-transmission groups earlier in the epidemic, but it might be a better use of resources to protect instead the high-risk groups later on. We develop a deterministic epidemic model with two age-groups (children and adults) and further subdivide each age group in low and high risk. We compare optimal vaccination strategies started at various points in time in two different settings: a population in the United States (US) where children account for 24% of the population, and a population in Senegal, where children make up for the majority of the population, 55%. For each of these populations, we minimize mortality and we find an optimal vaccination vector that gives us the best vaccine allocation given a starting vaccination date and vaccine coverage level. We find that there is a switch in the optimal vaccination strategy at some time point just before the peak of the epidemic. For instance, with 25% vaccine coverage, it is better to protect the high-transmission groups before this point, but it is optimal to protect the most vulnerable groups afterward
Molecular Infectious Disease Epidemiology: Survival Analysis and Algorithms Linking Phylogenies to Transmission Trees
Recent work has attempted to use whole-genome sequence data from pathogens to
reconstruct the transmission trees linking infectors and infectees in
outbreaks. However, transmission trees from one outbreak do not generalize to
future outbreaks. Reconstruction of transmission trees is most useful to public
health if it leads to generalizable scientific insights about disease
transmission. In a survival analysis framework, estimation of transmission
parameters is based on sums or averages over the possible transmission trees. A
phylogeny can increase the precision of these estimates by providing partial
information about who infected whom. The leaves of the phylogeny represent
sampled pathogens, which have known hosts. The interior nodes represent common
ancestors of sampled pathogens, which have unknown hosts. Starting from
assumptions about disease biology and epidemiologic study design, we prove that
there is a one-to-one correspondence between the possible assignments of
interior node hosts and the transmission trees simultaneously consistent with
the phylogeny and the epidemiologic data on person, place, and time. We develop
algorithms to enumerate these transmission trees and show these can be used to
calculate likelihoods that incorporate both epidemiologic data and a phylogeny.
A simulation study confirms that this leads to more efficient estimates of
hazard ratios for infectiousness and baseline hazards of infectious contact,
and we use these methods to analyze data from a foot-and-mouth disease virus
outbreak in the United Kingdom in 2001. These results demonstrate the
importance of data on individuals who escape infection, which is often
overlooked. The combination of survival analysis and algorithms linking
phylogenies to transmission trees is a rigorous but flexible statistical
foundation for molecular infectious disease epidemiology.Comment: 28 pages, 11 figures, 3 table
Models of epidemics and endemicity in genetically variable host populations
A discrete time genetics model is developed for populations that are undergoing selection due to infectious disease. It is assumed that the generation time of the host and infectious agent are non-synchronous and that only the host population is evolving. Two classes of epidemic processes are considered. The first class is for infectious agents that confer immunity following infection, while the second class is for those that do not confer immunity. The necessary and sufficient conditions are found in order for the disease to persist in a stable polymorphic host population. These conditions are shown to depend on the density of susceptibles, the selection coefficients, and the severity and class of the disease process.Peer Reviewedhttp://deepblue.lib.umich.edu/bitstream/2027.42/46943/1/285_2004_Article_BF00276518.pd
Preclinical Assessment of HIV Vaccines and Microbicides by Repeated Low-Dose Virus Challenges
BACKGROUND: Trials in macaque models play an essential role in the evaluation of biomedical interventions that aim to prevent HIV infection, such as vaccines, microbicides, and systemic chemoprophylaxis. These trials are usually conducted with very high virus challenge doses that result in infection with certainty. However, these high challenge doses do not realistically reflect the low probability of HIV transmission in humans, and thus may rule out preventive interventions that could protect against “real life” exposures. The belief that experiments involving realistically low challenge doses require large numbers of animals has so far prevented the development of alternatives to using high challenge doses. METHODS AND FINDINGS: Using statistical power analysis, we investigate how many animals would be needed to conduct preclinical trials using low virus challenge doses. We show that experimental designs in which animals are repeatedly challenged with low doses do not require unfeasibly large numbers of animals to assess vaccine or microbicide success. CONCLUSION: Preclinical trials using repeated low-dose challenges represent a promising alternative approach to identify potential preventive interventions
Estimating within-household contact networks from egocentric data
Acute respiratory diseases are transmitted over networks of social contacts.
Large-scale simulation models are used to predict epidemic dynamics and
evaluate the impact of various interventions, but the contact behavior in these
models is based on simplistic and strong assumptions which are not informed by
survey data. These assumptions are also used for estimating transmission
measures such as the basic reproductive number and secondary attack rates.
Development of methodology to infer contact networks from survey data could
improve these models and estimation methods. We contribute to this area by
developing a model of within-household social contacts and using it to analyze
the Belgian POLYMOD data set, which contains detailed diaries of social
contacts in a 24-hour period. We model dependency in contact behavior through a
latent variable indicating which household members are at home. We estimate
age-specific probabilities of being at home and age-specific probabilities of
contact conditional on two members being at home. Our results differ from the
standard random mixing assumption. In addition, we find that the probability
that all members contact each other on a given day is fairly low: 0.49 for
households with two 0--5 year olds and two 19--35 year olds, and 0.36 for
households with two 12--18 year olds and two 36+ year olds. We find higher
contact rates in households with 2--3 members, helping explain the higher
influenza secondary attack rates found in households of this size.Comment: Published in at http://dx.doi.org/10.1214/11-AOAS474 the Annals of
Applied Statistics (http://www.imstat.org/aoas/) by the Institute of
Mathematical Statistics (http://www.imstat.org
Estimating within-school contact networks to understand influenza transmission
Many epidemic models approximate social contact behavior by assuming random
mixing within mixing groups (e.g., homes, schools and workplaces). The effect
of more realistic social network structure on estimates of epidemic parameters
is an open area of exploration. We develop a detailed statistical model to
estimate the social contact network within a high school using friendship
network data and a survey of contact behavior. Our contact network model
includes classroom structure, longer durations of contacts to friends than
nonfriends and more frequent contacts with friends, based on reports in the
contact survey. We performed simulation studies to explore which network
structures are relevant to influenza transmission. These studies yield two key
findings. First, we found that the friendship network structure important to
the transmission process can be adequately represented by a dyad-independent
exponential random graph model (ERGM). This means that individual-level sampled
data is sufficient to characterize the entire friendship network. Second, we
found that contact behavior was adequately represented by a static rather than
dynamic contact network.Comment: Published in at http://dx.doi.org/10.1214/11-AOAS505 the Annals of
Applied Statistics (http://www.imstat.org/aoas/) by the Institute of
Mathematical Statistics (http://www.imstat.org
Predictive Modeling of Cholera Outbreaks in Bangladesh
Despite seasonal cholera outbreaks in Bangladesh, little is known about the
relationship between environmental conditions and cholera cases. We seek to
develop a predictive model for cholera outbreaks in Bangladesh based on
environmental predictors. To do this, we estimate the contribution of
environmental variables, such as water depth and water temperature, to cholera
outbreaks in the context of a disease transmission model. We implement a method
which simultaneously accounts for disease dynamics and environmental variables
in a Susceptible-Infected-Recovered-Susceptible (SIRS) model. The entire system
is treated as a continuous-time hidden Markov model, where the hidden Markov
states are the numbers of people who are susceptible, infected, or recovered at
each time point, and the observed states are the numbers of cholera cases
reported. We use a Bayesian framework to fit this hidden SIRS model,
implementing particle Markov chain Monte Carlo methods to sample from the
posterior distribution of the environmental and transmission parameters given
the observed data. We test this method using both simulation and data from
Mathbaria, Bangladesh. Parameter estimates are used to make short-term
predictions that capture the formation and decline of epidemic peaks. We
demonstrate that our model can successfully predict an increase in the number
of infected individuals in the population weeks before the observed number of
cholera cases increases, which could allow for early notification of an
epidemic and timely allocation of resources.Comment: 43 pages, including appendices, 5 figures, 1 table in the main tex
Neuraminidase Inhibitor Resistance in Influenza: Assessing the Danger of Its Generation and Spread
Neuraminidase Inhibitors (NI) are currently the most effective drugs against influenza. Recent cases of NI resistance are a cause for concern. To assess the danger of NI resistance, a number of studies have reported the fraction of treated patients from which resistant strains could be isolated. Unfortunately, those results strongly depend on the details of the experimental protocol. Additionally, knowing the fraction of patients harboring resistance is not too useful by itself. Instead, we want to know how likely it is that an infected patient can generate a resistant infection in a secondary host, and how likely it is that the resistant strain subsequently spreads. While estimates for these parameters can often be obtained from epidemiological data, such data is lacking for NI resistance in influenza. Here, we use an approach that does not rely on epidemiological data. Instead, we combine data from influenza infections of human volunteers with a mathematical framework that allows estimation of the parameters that govern the initial generation and subsequent spread of resistance. We show how these parameters are influenced by changes in drug efficacy, timing of treatment, fitness of the resistant strain, and details of virus and immune system dynamics. Our study provides estimates for parameters that can be directly used in mathematical and computational models to study how NI usage might lead to the emergence and spread of resistance in the population. We find that the initial generation of resistant cases is most likely lower than the fraction of resistant cases reported. However, we also show that the results depend strongly on the details of the within-host dynamics of influenza infections, and most importantly, the role the immune system plays. Better knowledge of the quantitative dynamics of the immune response during influenza infections will be crucial to further improve the results
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