Abstracts
INTRODUCTION: Malaria is a serious problem in the Brazilian Amazon region, and the detection of possible risk factors could be of great interest for public health authorities. The objective of this article was to investigate the association between environmental variables and the yearly registers of malaria in the Amazon region using Bayesian spatiotemporal methods. METHODS: We used Poisson spatiotemporal regression models to analyze the Brazilian Amazon forest malaria count for the period from 1999 to 2008. In this study, we included some covariates that could be important in the yearly prediction of malaria, such as deforestation rate. We obtained the inferences using a Bayesian approach and Markov Chain Monte Carlo (MCMC) methods to simulate samples for the joint posterior distribution of interest. The discrimination of different models was also discussed. RESULTS: The model proposed here suggests that deforestation rate, the number of inhabitants per km², and the human development index (HDI) are important in the prediction of malaria cases. CONCLUSIONS: It is possible to conclude that human development, population growth, deforestation, and their associated ecological alterations are conducive to increasing malaria risk. We conclude that the use of Poisson regression models that capture the spatial and temporal effects under the Bayesian paradigm is a good strategy for modeling malaria counts.
Malaria; Statistics; Deforestation; Environment; Amazon; Bayesian methods
INTRODUÇÃO: A malaria é uma doença endêmica na região da Amazônia Brasileira, e a detecção de possíveis fatores de risco pode ser de grande interesse às autoridades em saúde pública. O objetivo deste artigo é investigar a associação entre variáveis ambientais e os registros anuais de malária na região amazônica usando métodos bayesianos espaço-temporais. MÉTODOS: Utilizaram-se modelos de regressão espaço-temporais de Poisson para analisar os dados anuais de contagem de casos de malária entre os anos de 1999 a 2008, considerando a presença de alguns fatores como a taxa de desflorestamento. Em uma abordagem bayesiana, as inferências foram obtidas por métodos Monte Carlo em cadeias de Markov (MCMC) que simularam amostras para a distribuição conjunta a posteriori de interesse. A discriminação de diferentes modelos também foi discutida. RESULTADOS: O modelo aqui proposto sugeriu que a taxa de desflorestamento, o número de habitants por km² e o índice de desenvolvimento humano (IDH) são importantes para a predição de casos de malária. CONCLUSÕES: É possível concluir que o desenvolvimento humano, o crescimento populacional, o desflorestamento e as alterações ecológicas associadas a estes fatores estão associados ao aumento do risco de malária. Pode-se ainda concluir que o uso de modelos de regressão de Poisson que capturam o efeito temporal e espacial em um enfoque bayesiano é uma boa estratégia para modelar dados de contagem de malária.
Malária; Estatísticas; Desflorestamento; Meio Ambiente; Amazônia; Métodos bayesianos
ARTICLE ARTIGO
Use of Poisson spatiotemporal regression models for the Brazilian Amazon Forest: malaria count data
Uso de modelos Poisson espaço-temporal de regressão para a Floresta Amazônica Brasileira: contagem de dados de malária
Jorge Alberto AchcarI, II; Edson Zangiacomi MartinezI; Aparecida Doniseti Pires de SouzaII; Vilma Mayumi TachibanaII; Edilson Ferreira FloresII
IDepartamento de Medicina Social, Faculdade de Medicina de Ribeirão Preto, Universidade de São Paulo, Ribeirão Preto, SP
IIDepartamento de Matemática, Estatística e Computação, Faculdade de Ciências e Tecnologia, Universidade Estadual Paulista, Presidente Prudente, SP
Address to Address to: Prof. Edson Zangiacomi Martinez Deptº de Medicina Social/FMRP/USP Av. Bandeirantes 3900 14049-900 Ribeirão Preto, SP, Brazil Phone: 55 16 3602-2569 e-mail: edson@fmrp.usp.br
ABSTRACT
INTRODUCTION: Malaria is a serious problem in the Brazilian Amazon region, and the detection of possible risk factors could be of great interest for public health authorities. The objective of this article was to investigate the association between environmental variables and the yearly registers of malaria in the Amazon region using Bayesian spatiotemporal methods.
METHODS: We used Poisson spatiotemporal regression models to analyze the Brazilian Amazon forest malaria count for the period from 1999 to 2008. In this study, we included some covariates that could be important in the yearly prediction of malaria, such as deforestation rate. We obtained the inferences using a Bayesian approach and Markov Chain Monte Carlo (MCMC) methods to simulate samples for the joint posterior distribution of interest. The discrimination of different models was also discussed.
RESULTS: The model proposed here suggests that deforestation rate, the number of inhabitants per km2, and the human development index (HDI) are important in the prediction of malaria cases.
CONCLUSIONS: It is possible to conclude that human development, population growth, deforestation, and their associated ecological alterations are conducive to increasing malaria risk. We conclude that the use of Poisson regression models that capture the spatial and temporal effects under the Bayesian paradigm is a good strategy for modeling malaria counts.
Keywords: Malaria. Statistics. Deforestation. Environment. Amazon. Bayesian methods.
RESUMO
INTRODUÇÃO: A malaria é uma doença endêmica na região da Amazônia Brasileira, e a detecção de possíveis fatores de risco pode ser de grande interesse às autoridades em saúde pública. O objetivo deste artigo é investigar a associação entre variáveis ambientais e os registros anuais de malária na região amazônica usando métodos bayesianos espaço-temporais.
MÉTODOS: Utilizaram-se modelos de regressão espaço-temporais de Poisson para analisar os dados anuais de contagem de casos de malária entre os anos de 1999 a 2008, considerando a presença de alguns fatores como a taxa de desflorestamento. Em uma abordagem bayesiana, as inferências foram obtidas por métodos Monte Carlo em cadeias de Markov (MCMC) que simularam amostras para a distribuição conjunta a posteriori de interesse. A discriminação de diferentes modelos também foi discutida.
RESULTADOS: O modelo aqui proposto sugeriu que a taxa de desflorestamento, o número de habitants por km2 e o índice de desenvolvimento humano (IDH) são importantes para a predição de casos de malária.
CONCLUSÕES: É possível concluir que o desenvolvimento humano, o crescimento populacional, o desflorestamento e as alterações ecológicas associadas a estes fatores estão associados ao aumento do risco de malária. Pode-se ainda concluir que o uso de modelos de regressão de Poisson que capturam o efeito temporal e espacial em um enfoque bayesiano é uma boa estratégia para modelar dados de contagem de malária.
Palavras-chaves: Malária. Estatísticas. Desflorestamento. Meio Ambiente. Amazônia. Métodos bayesianos.
INTRODUCTION
Malaria is an endemic disease common in tropical and subtropical regions, including parts of the Americas, Asia, and Africa, and it is one of the most common infectious diseases. Malaria causes about 400-900 million cases of fever and approximately one to three million deaths annually1-2. It is a disease commonly associated with poverty. There are over 400 species of the malarial parasite (Plasmodium spp.), many of which infect different cold- and warm-blooded animals; however, only four routinely infect humans (P. falciparum, P. vivax, P. malariae, and P. ovale)3, and the two most common are P. falciparum and P. vivax4. P. falciparum causes the most severe disease and almost all fatalities4. Each one of these four malarial parasites is transmitted from one person to another by the bite of an infected female Anopheles spp. mosquito. Ecological alterations can affect the spread of these insects and, consequently, the spread of malaria.
Many papers have been introduced in the literature on the epidemiology of malaria in different forest ecological zones around the world. Dash et al.5 introduced a paper on malaria epidemics in India, a country with high incidence of the disease. They observed that heterogeneity and variability exist in the risk of malaria transmission between and within the provinces of India because many ecotypes/paradigms of malaria are recognized, with people living in forest pockets in different provinces contributing to morbidity and mortality due to malaria. Another study6 considered the use of spatiotemporal analytical tools to determine the social and environmental drivers of malaria risk in Vietnam. The authors analysed malaria data on reported P. falciparum and P. vivax infections by month and by district. They observed a strong temporal and spatial heterogeneity in counts of malaria cases and also considered some risk factors, such as the district's population living below the poverty line, the percent of districts covered by forest, median elevation, median long-term average precipitation, and minimum temperature. Owusu-Agyei et al.7 studied the epidemiology of malaria in the forest-savanna zone of Ghana. They found that the clinical malaria attack rate and the prevalence of malaria in children were very high in spite of a decrease in several parts of Africa as a result of control interventions. In another paper8, the authors concluded that the dynamics and seasonal abundance of malaria vectors in the Kintampo area of Ghana were influenced by microecology, rainfall, and temperature patterns. Reid et al.9 considered the use of Bayesian geostatistical models in mapping the malaria risk in Bangladesh. In all these studies, it is important to point out that the presence of different socioeconomic factors could have had great impact on the spread of malaria during that time. Another important point is related to the effect of neighboring regions on epidemics of malaria, which could justify the use of a space-time framework in these studies.
In Brazil, especially in the Amazon forest region, malaria is still a great health concern for health authorities. The prediction and characterization of malaria occurrence in an important world region, such as the Amazon forest, are important in malaria surveillance and control programs, and in understanding why and where resources should be redirected to present or reduce the projected increased disease occurrence. Different socioeconomic or spatiotemporal factors could be associated with the increase in malaria cases, such as the number of inhabitants per square kilometer, the proportion of urban population, the number of doctors per 10,000 inhabitants, and the human development index (HDI). Other factors, such as spatial or temporal aspects and deforestation, might be of interest, the latter being considered a strong determinant of the increasing incidence of malaria10.
In Figure 1, panel A, we have the yearly numbers of malaria fever cases per 1,000 inhabitants from 1999 to 2008 in nine provinces that belong to the Brazilian Amazon forest region (data source: DATASUS, Ministério da Saúde, Brazil). From Figure 1, we observe that, despite the Brazilian health authorities' efforts to control malaria fever, there are increasing numbers of malaria in two provinces, Acre and Rondônia, which have been undergoing great economic development in the last years (especially in the period from 1999 to 2006), resulting in population growth and increasing deforestation to create new cattle and agriculture farms. For the other seven provinces of the Amazon region, we also observe large numbers of malaria cases.
In this paper, we investigate the association between environmental variables and the yearly registers of malaria in the Brazilian Amazon region using a Poisson11-12 spatiotemporal model under the Bayesian paradigm13-14, with a latent term that captures the spatial effects of neighboring provinces and another latent term that captures the possible temporal correlation in each province through the years.
METHODS
Study design
This was an ecological study, with the Brazilian provinces of the Amazon region as units of analysis. Data were obtained from Sistema de Informações de Malária (SISMAL), Instituto Brasileiro de Geografia e Estatística (IBGE), Departamento de Informática do Sistema Único de Saúde (DATASUS), and Programa de Cálculo do Desflorestamento da Amazônia (PRODES). The study period covered the years from 1999 to 2008. A preliminary analysis of this data set gave some information on the behavior of the malaria rate and allowed us to identify isolated associated risk factors, but the proposed statistical model provided a general relationship among the malaria incidence rate and some risk factors, the spatial dependence, and the longitudinal trend over time.
The statistical model
Let Yi,j be the yearly number of malaria cases for province i in the year j, i=1, ..., n and j=1, ..., T, with a Poisson distribution, given by
where P(µ) denotes a Poisson distribution with parameter µ. In connection with the malaria data shown in Figure 1, panel A, we consider the following covariates: X1i, denoting the number of inhabitants per km2 (in the year 2004) in province i; X2i, denoting the percentage of urban population (in the year 2004) in province i; X3i, denoting the number of doctors per 10,000 inhabitants (in the year 2005) in province i; and X4i, denoting the human development index (HDI) (in the year 2005) in province i of the Amazon forest region, i=1, ..., 9. We also consider the deforestation index for province i in the year j as another covariate, denoted by X5ij, i=1,...,9, j=1,...,10 (corresponding to the years 1999 to 2008). The covariate values are introduced in Table 1.
Considering the covariates X1, X2, X3, X4, and X5, let us assume the following regression model for the Poisson distribution (1):
for i=1, ..., 9 (provinces) and j=1, ..., 10 (years); , l=1,..., 4 denotes the sample average for the covariate Xl, that is, n = . In (2), we observe that β0j, β1j, β2j, β3j, β4j, and β5j are fixed effect regression parameters associated with the covariates X1, X2, X3, X4, and X5; i=1,..., 9 and j=1, ....,10. bi is a random effect that captures the possible correlations among the malaria counts, taking into account the region effects of neighboring provinces assumed to have a normal CAR structure15-21 model, that is,
where A*(i) denotes the set of neighbors corresponding to province i, n(i) denotes the number elements in A*(i), denotes the mean of the neighboring random effects for province i, and ζb is an unknown parameter.
In (2) we also assume a random effect Wij for the longitudinal trend specified as a Gaussian process with a multivariate normal distribution with a mean vector 10 x 1, with all components equal to zero and a 10 x 10 variance-covariance matrix Σ=[Cov (Wij, Wij*)], with elements given by:
assuming a fixed value for K. Different fixed values for K can be considered, which gives a great flexibility of fit for the data, and θk, k=1, 2, ..., K, is an unknown parameter. Observe that model (4) generalizes the longitudinal trend specification introduced by Branscum et al.22
For the first stage of the hierar-chical Bayesian analysis, let us assume normal prior distributions βlj ~ N(0, a2lj), l=0,1,2,...,5, j=1,...,10, where alj are known hyperparameters. Taking large values for alj, we have highly dispersed prior distributions for the regression parameters. For the second stage of the hierarchical Bayesian analysis, let us assume uniform prior distributions ςb ~ U(0, c) and θk ~ U(0, dk) for k=1, 2, ..., K; c and dk are known hyperparameters.
For a hierarchical Bayesian analysis of the model, we consider the use of Markov Chain Monte Carlo (MCMC) methods13-14. For the model choice, assuming different values for K in (4), we use some existing Bayesian model discrimination criteria, one of which is given by the Deviance Information Criterion (DIC)23. The smaller the DIC, the better the fit of the model for the data. We also consider some goodness-of-fit techniques in choosing the best model. In this way, we compare the observed data with the fitted or estimated posterior means for µij using the simulated Gibbs samples for each parameter of the model, given by:
where l indexes the model (l=1 for model 1 and l=2 for model 2), and µij is the MCMC estimate for E(µij | y, x), i=1, ..., 9, j=1, ..., 10.
To verify if the covariate deforestation rate and the covariate number of inhabitants per km2, percentage of urban population, number of doctors per 10,000 inhabitants, and HDI index have some significative effects in the yearly counts of malaria in the Brazilian provinces of the Amazon forest region, we assume the Poisson regression considering two special cases. First, a model defined by (1) and (2), not considering the temporal random effect Wij and assuming that the random effect bi has a normal distribution N(0, σb2), where σb2 is an unknown variance; let us denote this as model 1. Second, a model defined by (1) and (2), with a normal CAR structure (3) for the random effects bi (spatial structure) and a multivariate normal distribution with covariance structure (4) for the random effect Wij (temporal structure) with K=2 (the neighboring structure is given in Table 1); let us denote this as model 2.
For a hierarchical Bayesian analysis of model 1 and model 2, let us assume a uniform U(0,1) prior distribution for ςh, where ςh =1/ σb2, the normal prior distributions for the regression parameters, βlj ~ N(0, α2lj), l=0, 1, ..., 5; j=1, 2, ..., 10; and the uniform prior distributions for ςb2 and θk, k=1, 2 with α2lj =10; b=0, c=1, d1=3, and d2=1. Using the WinBUGS software24, we simulate the two models: 10,000 initial Gibbs samples as a burn-in sample to eliminate the effect of the initial values on the Gibbs sampling algorithm. After this burn-in sample period, we simulate another 1,600 samples, taking every 50th sample to have approximately uncorrelated samples for the joint posterior distribution of all parameters of the model. Convergence of the Gibbs sampling algorithm was observed using plots of the simulated time-series samples.
RESULTS
Considering the yearly numbers of malaria cases per 1,000 inhabitants in the Amazon forest region from 1999 to 2008, we observe (Figure 1) that for most of the provinces, there was a decrease from 1999 to approximately the year 2002, an increase starting in the year 2002 to approximately the year 2005, and a decrease after the year 2005.
We also observe that the deforestation rate in the Brazilian Amazon forest region presents a behavior similar to the yearly counts of malaria cases, that is, an increase from 1999 to 2004 and a decrease after 2004 in almost all the provinces (Figure 1, panel B).
Assuming model 1, we have in Table 2 the posterior summaries of the parameters that do not include zero in the 95% credible intervals, that is, the parameters that have significative effects. From the obtained results in Table 2, we can have the following interpretations: I) the covariate X1 (number of inhabitants per km2) presents a significative effect on the malaria count in the year 2006 (zero is not included in the 95% credible interval for β18); II) the covariate X4 (HDI index) presents a significative effect on the malaria count in the years 1999 and 2000 (zero is not included in the 95% credible intervals for β41 and β42); and III) the covariate X5 (deforestation rate) presents a significative effect on the malaria count in the years 1999, 2000, 2001, 2002, and 2003 (zero is not included in the 95% credible intervals for β51, β52, β53, β54, and β55). These regression parameters correspond to the years with larger deforestation rates (Figure 1).
Assuming model 2, we have in Table 2 the posterior summaries of the parameters that present some significative effects (zero is not included in the 95% credible intervals). From the results in Table 2 (model 2), we observe that the covariate X5 (deforestation rate) presents a significative effect on the malaria count in the years 2001 and 2002 (zero is not included in the 95% credible intervals for β53 and β54).
Assuming model 1, we obtain from the WinBUGS output a Monte Carlo estimate for DIC given by DÎC = 758.994. In this case, we found C(1)=308.105 (see equation (5)).
Considering model 2, we obtained DÎC = 554.580 and C(2)=89.125. That is, model 2 is better fitted to the malaria count in the Brazilian Amazon forest region since the estimated DIC and the sum of absolute values for the differences between yij and µij give smaller values in this model.
It is also interesting to observe that model 2 in the presence of a spatiotemporal structure gives a better fit for the data when comparing the individual Monte Carlo estimates for the means of the Poisson model with the observed malaria data.
Assuming model 2, which gives the best fit for the malaria data shown in Figure 1, we have in Figure 2 the different estimates for the malaria rates in the Brazilian Amazon forest provinces in the years from 1999 to 2008. From Figure 2, we observe that the mean rates for the provinces in the Brazilian Amazon forest region increased greatly in the years from 2004 to 2007, especially for the provinces of Amazonas, Acre, and Rondônia.
DISCUSSION
Deforestation is associated with loss of biodiversity, the alteration of many fundamental aspects of ecosystems, and an increase in the prevalence and incidence of many human vector-borne diseases25. The year-round high rainfall and temperatures in tropical forests are ecological characteristics that favor the development of many kinds of mosquitoes that transmit pathogens that cause disease in humans26. Thus, the process of clearing forests and the subsequent human activities, such as agricultural and hydropower developments, have a high influence on the prevalence and incidence of diseases such as human malaria27. In a study that examined the ecological alteration in the Peruvian Amazon28, it was shown that various landscapes and ecological features associated with deforestation were positively associated with Anopheles darlingi larval breeding sites. This is considered the major South American malaria vector. Another study29 showed that in western Kenya, deforested sites had higher temperatures and relative humidities, and the overall infection rate of Anopheles mosquitoes was increased compared with that in forested sites. In addition, the vectorial capacity was estimated to be 77.7% higher in the deforested site than in the forested site. In 1981, the construction of the Tucuruí hydroelectric dam in southeast Pará province, Brazil, caused enormous environmental changes, deforestation, and human migration to the region, and a study30 confirmed the elevation of malaria to the epidemic level since then. In a review of the literature27, sixty examples of changes in anopheline ecology throughout the tropical world were identified as a consequence of deforestation and agricultural development.
The present study also found that deforestation rate is important in the prediction of malaria cases. In addition, the Bayesian model here proposed suggests that the number of inhabitants per km2 and the HDI index have some association with the number of malaria cases. The growing population in the Brazilian Amazon region is associated with human migration motivated by new agricultural settlements and informal mines (garimpos)31 that promote environmental changes and contribute to the spread of malaria. The association of malaria with the HDI index and poverty was also discussed in a recent article32, which argued that the North and Northeast regions of Brazil have the lowest HDI indexes and the highest rates of neglected tropical diseases. In this context, it is important to point out that areas with low human development tend to have poor access to health care and malaria interventions, increasing the vulnerability of the poorest.
In view of the results of the present study and other research reported in the literature, it is possible to conclude that human development, population growth, deforestation, and their associated ecological alterations are conducive to increasing malaria risk. The possible environmental interventions to reduce malaria risk in the Brazilian Amazon forest region include policies that promote sustainable agriculture aimed at protecting the rainforest and incentives for forest regeneration.
To map the malaria count data in the Amazon region, the provinces are used as geographical limits. Thus, we can note that the areas of the provinces are too large, and this is one of the limitations of the study. However, more refined data are not available for small regions, making it too costly to develop a more detailed analysis of the data. In addition, the migration of individuals into or out of the provinces is not controlled in the data analysis, which can cause ecological bias33. Another possible source of bias is the use of data from different systems of information and its subsequent limitations. As examples of this, the official records of malaria are likely to be biased and underreported given the lack of health facilities in remote or poor areas34, and the available deforestation data are subject to a possible lack of accuracy.
Finally, it is also possible to conclude that the use of Poisson regression models in the presence of random effects that capture the spatial and temporal effects under the Bayesian paradigm is a good strategy for modeling disease counts in the presence of covariates. The use of spatiotemporal models, as introduced in this paper, to analyse the malaria data of the Brazilian Amazon forest region is becoming popular in the analysis of longitudinal disease count data under the Bayesian paradigm and using MCMC methods35-41. Alternative models specifying different forms for the matrix representing the relationship between neighboring areas or even the proportion of non-registered cases can be used, but the obtained results show that the assumed model gives us efficient answers for our goals. The use of available software, such as WinBUGS, allows great simplification in simulating samples for the joint posterior distribution of interest.
CONFLICT OF INTEREST
The authors declare that there is no conflict of interest.
Received in 11/02/2011
Accepted in 28/07/2011
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1Breeman J. The ears of the hippopotamus: manifestations, determinants and estimates of the malaria burden. Am J Trop Med Hyg 2001; 64:1-11.
-
2Greenwood BM, Bojang K, Whitty CJ, Targett GA. Malaria. Lancet 2005; 365: 1487-1498.
-
3Despommier DD, Gwadz RW, Hotez PJ, Knirsch CA. Parasitic Diseases. 5th edition. New York: Apple Trees Productions; 2005.
-
4Mayxay M, Pukrittayakamee S, Newton PN, White NJ. Mixed-species malaria infections in humans. Trends Parasitol 2004; 20:233-240.
-
5Dash AP, Valecha N, Anvikar AR, Kumar A. Malaria in India: challenges and opportunities. J Biosci 2008; 33:583-592.
-
6Bui HM, Clements AC, Nguyen QT, Nguyen MH, Le XH, Hay SI, et al. Social and environmental determinants of malaria in space and time in Viet Nam. Int J Parasitol 2011; 41:109-116.
-
7Owusu-Agyei S, Asante KP, Adjuik M, Adjei G, Awini E, Adams M, et al. Epidemiology of malaria in the forest-savanna transitional zone of Ghana. Malar J 2009; 8:220.
-
8Dery DB, Brown C, Asante KP, Adams M, Dosoo D, Amenga-Etego S, et al. Patterns and seasonality of malaria transmission in the forest-savannah transitional zones of Ghana. Malar J 2010; 9:314.
-
9Reid H, Haque U, Clements AC, Tatem AJ, Vallely A, Ahmed SM, et al. Mapping malaria risk in Bangladesh using Bayesian geostatistical models. Am J Trop Med Hyg 2010; 83:861-867.
-
10Pattanayak S, Dickinson K, Corey C, Murray B, Sills E, Kramer R. Deforestation, malaria, and poverty: a call for transdisciplinary research to support the design of cross-sectoral policies. Sustainability: Science, Practice & Policy 2006; 2:45-56.
-
11Banerjee S, Carlin BP, Gelfand AE. Hierarchical modelling and analysis for spatial data. Monographs on Statistics and Applied Probability 101. London: Chapman & Hall/CRC Press; 2004.
-
12Lawson AB, Zhou H. Spatial statistical modeling of disease outbreaks with particular reference to the UK foot-and-mouth disease epidemic of 2001. Prev Vet Med 2005; 71:141-156.
-
13Gelfand AE, Smith AFM. Sampling-based approaches to calculating marginal densities. J Am Stat Assoc 1990; 85:398-409.
-
14Chib S, Greenberg E. Understanding the Metropolis-Hastings algorithm. Am Stat 1995; 49:327-335.
-
15Besag J. Spatial interaction and the statistical analysis of lattice systems (with discussion). J R Statist Soc B 1974; 1-2 (suppl):192-236.
-
16Clayton D, Kaldor J. Empiral Bayes estimates of age-standardized relative risks for use in disease mapping. Biometrics 1987; 43:671-681.
-
17Cressie N, Chan NH. Spatial modelling of regional variables. J Am Stat Assoc 1989; 84:393-401.
-
18Marshall RJ. A review of methods for the statistical analysis of spatial patterns of disease. J R Statist Soc A 1991; 154:421-441.
-
19Bernardinelli L, Clayton D, Montomoli C. Bayesian estimates of disease maps: how important are priors? Stat Med 1995; 14:2411-2431.
-
20Waller LA, Carlin BP, Xia H, Gelfand AE. Hierachical spatio-temporal mapping of disease rates. J Am Stat Assoc 1997; 92:607-617.
-
21Kelsall J, Wakefield J. Modeling spatial variation in disease risk: a geostatistical approach. J Am Stat Assoc 2002; 97:692-701.
-
22Branscum AJ, Perez AM, Johnson WO, Thurmond MC. Bayesian spatiotemporal analysis of foot-and-mouth disease data from the Republic of Turkey. Epidemiol Infect 2008; 136:833-842.
-
23Spiegelhalter DJ, Best NG, Carlin BP, Van Der Linde A. Bayesian measures of model complexity and fit (with discussion). J R Stat Soc B 2002; 64:583-639.
-
24Lunn DJ, Thomas A, Best N, Spiegelhalter D. WinBUGS - a Bayesian modelling framework: concepts, structure, and extensibility. Stat Comput 2000; 10:325-337.
-
25Sehgal RN. Deforestation and avian infectious diseases. J Exp Biol 2010; 213:955-960.
-
26Prothero RM. Malaria, forests and people in Southeast Asia. Singapore J Trop Geogr 1999; 20:76-85.
-
27Yasuoka J, Levins R. Impact of deforestation and agricultural development on anopheline ecology and malaria epidemiology. Am J Trop Med Hyg 2007; 76:450-460.
-
28Vittor AY, Pan W, Gilman RH, Tielsch J, Glass G, Shields T, et al. Linking deforestation to malaria in the Amazon: characterization of the breeding habitat of the principal malaria vector, Anopheles darlingi Am J Trop Med Hyg 2009; 81:5-12.
-
29Afrane YA, Little TJ, Lawson BW, Githeko AK, Yan G. Deforestation and vectorial capacity of Anopheles gambiae Giles mosquitoes in malaria transmission, Kenya. Emerg Infect Dis 2008; 14:1533-1538.
-
30Vasconcelos CH, Novo EM, Donalisio MR. Use of remote sensing to study the influence of environmental changes on malaria distribution in the Brazilian Amazon. Cad Saude Publica 2006; 22:517-526.
-
31Cruz Marques A. Human migration and the spread of malaria in Brazil. Parasitol Today 1987; 3:166-170.
-
32Lindoso JA, Lindoso AA. Neglected tropical diseases in Brazil. Rev Inst Med Trop Sao Paulo 2009; 51:247-253.
-
33Morgenstern H. Ecologic studies in epidemiology: concepts, principles, and methods. Annu Rev Public Health 1995; 16:61-81.
-
34Castro MC, Sawyer DO, Singer BH. Spatial patterns of malaria in the Amazon: Implications for surveillance and targeted interventions. Health & Place 2007; 13:368-380.
-
35Ugarte MD, Goicoa T, Ibáñez B, Militino AF. Evaluating the performance of spatio-temporal Bayesian models in disease mapping. Environmetrics 2009; 20:647-665.
-
36Martínez-Beneito MA, López-Quilez A, Botella-Rocamora P. An autoregressive approach to spatio-temporal disease mapping. Stat Med 2008; 27:2874-2889.
-
37Paez MS, Gamerman D. Study of the space-time effects in the concentration of airborne pollutants in the metropolitan region of Rio de Janeiro. Environmetrics 2003; 14:387-408.
-
38Nobre AA, Schmidt AM, Lopes HF. Spatio-temporal models for mapping the incidence of malaria in Pará. Environmetrics 2005; 16:291-304.
-
39Ocana-Riola R, Mayoral-Cortes JM. Spatio-temporal trends of mortality in small-areas of southern Spain. BMC Public Health 2010; 10:26.
-
40Charland KML, Buckeridge DL, Sturtevant JL, Melton F, Reis BY, Mandl KD, et al. Effect of environmental factors on the spatio-temporal patterns of influenza spread. Epidemiol Infect 2009; 137:1377-1387.
-
41Manda SOM, Feltbower RG, Gilthorpe MS. Investigating spatio-temporal similarities in the epidemiology of childhood leukaemia and diabetes. Eur J Epidemiol 2009; 24:743-752.
Address to:
Publication Dates
-
Publication in this collection
06 Jan 2012 -
Date of issue
Dec 2011
History
-
Received
11 Feb 2011 -
Accepted
28 July 2011