Data are from IPTi trials conducted in Manhiça (Mozambique), Lambarene (Gabon), Ifakara (Tanzania) and Navrongo, Kumasi and Tamale (Ghana). Detailed descriptions of the study population, methodology and outcome in each study included in this analysis have been published elsewhere 2345678. A summary of the study designs and their epidemiological background is shown in Table 1. The model output was compared to data derived from the IPTi Consortium's Statistical Working Group (SWG) Report of September 2007. The SWG used common definitions for time at risk and for an episode of clinical malaria across all six studies. For time at risk a child treated for clinical malaria was censured for 21 days in order to prevent double counting of cases and to allow for any prophylactic effect of the antimalarial. A case of clinical malaria was defined as measured fever or history of fever with any parasitaemia of P. falciparum (definition of duration of history of fever differed between studies: for Ifakara and Manhica studies it was 24 hours and for remaining studies it was 48 hours). In this paper, all references to the PE of IPTi refers to the PE against episodes of clinical malaria up to 12 months of age based on incidence rates of multiple episodes of clinical malaria, not time to first or only episodes.

The relationship between the observed PE of IPTi and the following potential determinants of PE were explored: resistance to SP; estimated ITN coverage (% of the study population reporting use of ITN); and malaria transmission intensity (mean incidence of malaria per child per year in the placebo group). Day-14 parasitological and clinical failure rates were used to define resistance because five out of the six IPTi trials had published this information within two years of conducting the IPTi trial 1011121314. One site in Ghana, Kumasi, did not have data on day 14 parasitological and clinical failure of SP and therefore the estimate from Tamale, relatively close geographically, was used.

An age-structured model (Figure 1) was developed to represent the acquisition of malaria infection and clinical disease and the development of immunity in the study cohort of infants between the ages of two and 24 months. The modelling exercise only examines the specific cohort as studied in the trials, thus age and calendar times are equivalent and the model output is expressed in terms of the age of the children. At any point in time children can be in one of two states – uninfected and susceptible to new infection S(a) or infected with parasites which can remain asymptomatic or can become symptomatic, A(a). It is assumed that the rate of acquisition of new infections is determined by the force of infection in the study area, λ(a), which may vary through time (and hence by age). Once infected and in the asymptomatic state, children return to the susceptible state through one of three routes. First, they may become a clinical case and receive an effective treatment. It is assumed that in clinical trial settings, every case of malaria detected was adequately treated and parasites cleared. Secondly, they may receive antimalarial treatment for asymptomatic parasitaemia eg IPTi. Finally, they may remain asymptomatic and recover naturally. Symptomatic cases of malaria that are not detected by surveillance systems will remain in the asymptomatic state in the model until they die of severe disease or their immune response clears parasites. The model does not incorporate children leaving the asymptomatic pool by death, assuming this will be a very small number because most of the cases would be detected in time to receive effective treatment in a trial setting.

Ignoring mortality from other causes and migration, the model without interventions can be expressed by the following equation:

d A ( a ) d a = λ ( a ) ( N − A ( a ) ) − ( c ( a ) + r ( a ) ) A ( a ) MathType@MTEF@5@5@+=feaafiart1ev1aaatCvAUfKttLearuWrP9MDH5MBPbIqV92AaeXatLxBI9gBaebbnrfifHhDYfgasaacPC6xNi=xI8qiVKYPFjYdHaVhbbf9v8qqaqFr0xc9vqFj0dXdbba91qpepeI8k8fiI+fsY=rqGqVepae9pg0db9vqaiVgFr0xfr=xfr=xc9adbaqaaeGaciGaaiaabeqaaeqabiWaaaGcbaqcfa4aaSaaaeaacqWGKbazcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkaeaacqWGKbazcqWGHbqyaaGccqGH9aqpcqaH7oaBcqGGOaakcqWGHbqycqGGPaqkcqGGOaakcqWGobGtcqGHsislcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkcqGGPaqkcqGHsislcqGGOaakcqWGJbWycqGGOaakcqWGHbqycqGGPaqkcqGHRaWkcqWGYbGCcqGGOaakcqWGHbqycqGGPaqkcqGGPaqkcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkaaa@5282@

where N is the fixed population size, r(a) is the age-dependent rate of natural clearance of parasitaemia and c(a) is the age-dependent rate of development of clinical disease which is then treated.

In endemic areas the risk of developing clinical disease decreases with exposure to infection but rates of parasitaemia remain almost constant in early childhood. The model incorporates functions that mimic the development of immunity so that as children age the rate at which they develop clinical disease decreases and the rate at which they clear parasites increases. For simplicity, the model assumes that both immunity functions are linearly dependent on the expected number of malaria infections at age a:

E [ I ( a ) ] = 1 N ∫ 0 a λ ( a ' ) S ( a ' ) d a ' MathType@MTEF@5@5@+=feaafiart1ev1aaatCvAUfKttLearuWrP9MDH5MBPbIqV92AaeXatLxBI9gBaebbnrfifHhDYfgasaacPC6xNi=xI8qiVKYPFjYdHaVhbbf9v8qqaqFr0xc9vqFj0dXdbba91qpepeI8k8fiI+fsY=rqGqVepae9pg0db9vqaiVgFr0xfr=xfr=xc9adbaqaaeGaciGaaiaabeqaaeqabiWaaaGcbaGaemyrauKaei4waSLaemysaKKaeiikaGIaemyyaeMaeiykaKIaeiyxa0Laeyypa0tcfa4aaSaaaeaacqaIXaqmaeaacqWGobGtaaGcdaWdXbqaaiabeU7aSjabcIcaOiabdggaHjabcEcaNiabcMcaPiabdofatjabcIcaOiabdggaHjabcEcaNiabcMcaPiabdsgaKjabdggaHjabcEcaNaWcbaGaeGimaadabaGaemyyaeganiabgUIiYdaaaa@4A2E@

The rate of development of clinical disease is given by the logistic function

c ( a ) = ϕ α 1 + 1 α 1 + e α 2 E [ I ( a ) ] MathType@MTEF@5@5@+=feaafiart1ev1aaatCvAUfKttLearuWrP9MDH5MBPbIqV92AaeXatLxBI9gBaebbnrfifHhDYfgasaacPC6xNi=xI8qiVKYPFjYdHaVhbbf9v8qqaqFr0xc9vqFj0dXdbba91qpepeI8k8fiI+fsY=rqGqVepae9pg0db9vqaiVgFr0xfr=xfr=xc9adbaqaaeGaciGaaiaabeqaaeqabiWaaaGcbaGaem4yamMaeiikaGIaemyyaeMaeiykaKIaeyypa0Jaeqy1dOwcfa4aaSaaaeaacqaHXoqydaWgaaqaaiabigdaXaqabaGaey4kaSIaeGymaedabaGaeqySde2aaSbaaeaacqaIXaqmaeqaaiabgUcaRiabdwgaLnaaCaaabeqaaiabeg7aHnaaBaaabaGaeGOmaidabeaacqWGfbqrcqGGBbWwcqWGjbqscqGGOaakcqWGHbqycqGGPaqkcqGGDbqxaaaaaaaa@47C5@

where ϕ is the rate of development of clinical disease in the absence of immunity and α₁ and α₂ are parameters which determine the number of infections after which full immunity to clinical disease occurs. The rate of natural clearance of parasites is assumed to be linear within the range of interest and hence is given by

r(a) = min(ωE [I(a)], 1))

where 1/ω is the mean number of infections after which full parasite immunity is obtained and it was assumed that at full immunity parasites are cleared after a mean of one day.

A generic maternal protective function which acts to reduce the force of infection following birth was incorporated. Maternal protection is complicated and multifaceted 15, incorporating both biological immunity as well as behavioural factors that limit exposure. Given the paucity of data with which to determine an appropriate function, the following factors were used, which act on the force of infection up to six months of age: 0.05, 0.15, 0.4 and 0.8 at age 2, 3, 4 and 5 months of age respectively, which represent a gradual loss of immunity.

The model was numerically evaluated as difference equations in 1-month time-steps using Excel.

To compare the model results to the trial data the two interventions were incorporated. Firstly, use of ITNs is included by reducing the force of infection in the group assigned to ITNs by a factor θ:

d A ( a ) d a = ( 1 − θ ) λ ( a ) ( N − A ( a ) ) − ( c ( a ) + r ( a ) ) A ( a ) MathType@MTEF@5@5@+=feaafiart1ev1aaatCvAUfKttLearuWrP9MDH5MBPbIqV92AaeXatLxBI9gBaebbnrfifHhDYfgasaacPC6xNi=xI8qiVKYPFjYdHaVhbbf9v8qqaqFr0xc9vqFj0dXdbba91qpepeI8k8fiI+fsY=rqGqVepae9pg0db9vqaiVgFr0xfr=xfr=xc9adbaqaaeGaciGaaiaabeqaaeqabiWaaaGcbaqcfa4aaSaaaeaacqWGKbazcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkaeaacqWGKbazcqWGHbqyaaGccqGH9aqpcqGGOaakcqaIXaqmcqGHsislcqaH4oqCcqGGPaqkcqaH7oaBcqGGOaakcqWGHbqycqGGPaqkcqGGOaakcqWGobGtcqGHsislcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkcqGGPaqkcqGHsislcqGGOaakcqWGJbWycqGGOaakcqWGHbqycqGGPaqkcqGHRaWkcqWGYbGCcqGGOaakcqWGHbqycqGGPaqkcqGGPaqkcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkaaa@57C7@

The model only examines the personal protection gained from an ITN and does not examine any other effects, such as effects on transmission.

IPT use across all age-groups modelled (two to 24 months) is assumed to act in three ways, clearing parasites in a proportion (1-σ) of the population, ie the treatment effect, prophylaxes against new infection (factor σ reducing the force of infection) and reducing the rate of development of clinical disease by the same factor. As the model is defined in monthly time-steps, the parameter σ can be interpreted as the PCR uncorrected day 28 Adequate Clinical and Parasitological Response (ACPR) which measures the proportion that will clear parasitaemia and be protected against new infection 28 days post treatment. For simplicity, it was assumed that the ACPR acts with equal efficacy to clear parasites, to protect against new infection and prevent development of disease.

d A ( a ) d a = ( 1 − σ ) λ ( a ) ( N − A ( a ) ) − ( ( 1 − σ ) c ( a ) + r ( a ) ) A ( a ) − σ A ( a ) MathType@MTEF@5@5@+=feaafiart1ev1aaatCvAUfKttLearuWrP9MDH5MBPbIqV92AaeXatLxBI9gBaebbnrfifHhDYfgasaacPC6xNi=xI8qiVKYPFjYdHaVhbbf9v8qqaqFr0xc9vqFj0dXdbba91qpepeI8k8fiI+fsY=rqGqVepae9pg0db9vqaiVgFr0xfr=xfr=xc9adbaqaaeGaciGaaiaabeqaaeqabiWaaaGcbaqcfa4aaSaaaeaacqWGKbazcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkaeaacqWGKbazcqWGHbqyaaGccqGH9aqpcqGGOaakcqaIXaqmcqGHsislcqaHdpWCcqGGPaqkcqaH7oaBcqGGOaakcqWGHbqycqGGPaqkcqGGOaakcqWGobGtcqGHsislcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkcqGGPaqkcqGHsislcqGGOaakcqGGOaakcqaIXaqmcqGHsislcqaHdpWCcqGGPaqkcqWGJbWycqGGOaakcqWGHbqycqGGPaqkcqGHRaWkcqWGYbGCcqGGOaakcqWGHbqycqGGPaqkcqGGPaqkcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkcqGHsislcqaHdpWCcqWGbbqqcqGGOaakcqWGHbqycqGGPaqkaaa@63DE@

Equation (6) is applied to the model only for months when IPTi doses are given. For months in those children who used ITNs and receive IPT equations (5) and (6) are combined.

For the modelling exercise, the coverage of ITNs (reported ownership) in each trial site was used because the use of ITN at the individual level was not available for all trials. The expected incidence of clinical disease in each trial arm (placebo and IPT) is therefore calculated as a weighted combination of the model predictions with and without ITNs. The protective efficacy of IPT predicted by the model is calculated as 1-relative risk = 1-clinical incidence in IPTi group/clinical incidence in placebo group.

It is assumed that that on average after 5 infections of malaria an individual is totally protected against clinical disease and that after 50 infections an individual can clear parasites rapidly. A sensitivity analysis for these parameters can be found later in this paper. Parameters that reproduce these patterns are given in Table 2. The force of infection, λ(a) was assumed to be constant for the baseline scenarios. At a later stage the modelling exercise used scenarios in which the force of infection was decreased in early childhood due to maternal protective factors and separately allowed to increase or decrease linearly as the children aged reflecting changes in transmission over time. The force of infection was initially estimated directly as the mean incidence of clinical malaria in the placebo group. This approximation was based on the observation that the age-specific incidence of clinical malaria is highest in infants, the IPTi target age group and that the age group with the highest incidence should have the lowest immunity. The observed data from the Navrongo study (the only full dataset available to the study team) was compared with the model estimates of clinical disease, which were found to be half of that observed in the study. Thus, the mean incidence of clinical malaria in the placebo group was multiplied by a factor of two to estimate the force of infection. Entomological Inoculation Rates (EIR) were not used as a measure of transmission in the model for two reasons: EIRs measured concurrently with the IPTi trials were not available for most sites and in the studies with EIRs there was no common methodology. Secondly, these large cohort studies had enrolled children from a large geographical area over several years (two to four years). Thus a single measure of EIR would not suffice to represent the whole study area or the whole study period.

The proportion of infected children becoming symptomatic and treated in the absence of immunity was assumed to be 90% in one month. This was derived from a study of asymptomatic parasitaemia in 6–59 month old children in a moderate malaria setting in Kampala, Uganda 16; in this population 50% of children with asymptomatic parasitaemia developed clinical malaria after 30 days. As the Ugandan study was undertaken in partially immune children we assumed a higher rate of development of disease. Clinical malaria cases are assumed to recover within a month post treatment, twice the average terminal half-life of the antimalarials used for treatment and rejoin the susceptible population. Deaths and migrations were not included in the model.

For those children receiving IPT, it is assumed that treatment, prophylaxis, and prevention of developing clinical disease effects of SP will be equally affected by the PCR uncorrected day 28 ACPR of SP. Day 28 PCR uncorrected ACPR is a measure of both the treatment and prophylactic effect combined (it includes both recrudescence's and re-infections) and is more likely to represent the effects of the drugs when used for prevention as opposed to treatment. The sensitivity analysis for how changes in ACPR affect PE is shown in the in the results section. Briefly, as drug resistance increases PE declines. The day 28 ACPR was only available for 2 sites, the sites with the highest and lowest resistances at day 14, namely Ifakara 10 and Tamale 14 respectively. The extrapolation from day 14 to 28 efficacy for the 3 studies 111213 without day 28 ACPR is the mid point between these two studies.

For those children using ITNs, we assume that the protective efficacy of an ITN is 0.5 17. The model parameters are summarised in Table 2.

A sensitivity analysis of how ACPR, ITN coverage and immunity functions affects predicted PE was carried out.

Figure 2 shows the relationship between PE of IPTi and resistance to SP, estimated ITN coverage, and malaria transmission intensity in each study site. The Ifakara study site had the highest IPTi PE (59%) despite having the highest resistance to SP (31% day-14 parasitological and clinical failure rate). This site also had the highest ITN coverage (67%). Resistance to SP was 14 – 22% and ITN coverage was 0 – 20% in the other five sites.

The model predicted a similar pattern across the six trials, with a transient decline in incidence among the groups receiving IPTi (with and without ITN coverage) as well as a generally lower incidence among groups with ITNs (with and without IPTi). Using the Navrongo study as an example (IPTi doses given at 3, 4, 9 and 12 months of age), Figure 3 shows the models prediction of monthly incidence of clinical disease cases in groups with and without ITNs (Figure 3A), the combined model weighted by ITN coverage (Figure 3B) and observed data from the Navrongo 18 study for comparison (Figure 3C). In those trial settings with higher incidence the model generates a small increase in the numbers of cases shortly after each IPTi dose due to delayed acquisition of immunity which continues into the second year of life (the rebound effect).

The predicted PE of IPTi in the six sites with the observed data are shown in Table 3. The mean ratio between model to actual PE was 1.02 (range 0.39 – 1.59) with the predicted PE lying within the 95% confidence interval from the trial data in all but the Ifakara study. The main differences between the Ifakara and the other studies were the high ITN coverage and the higher resistance to SP. There seems no obvious explanation to why IPTi should be more effective with higher drug resistance. However, high ITN coverage may have an effect on transmission. Thus the effect of changing transmission on the PE predicted by the model is further explored.

Table 4 shows the change in both PE and the effect of delayed immunity (rebound effect) predicted by the model for Ifakara under four scenarios with changing transmission during the study period with both maternal immunity function removed and included – (a) increasing at a rate of 25% per month, (b) increasing at a rate of 5% per month, (c) stable, (d) a decline of 5% per month and (e) a decline of 25% per month. In the scenarios of changing transmission, PE is dominated when the effect of IPTi is most efficacious, ie when transmission is highest. In the output of the model without the maternal immunity function (Figure 4A) the overall PE measured by the trial is dominated by its early efficacy with the first two doses of IPTi. Thus, because most of the efficacy is predicted to occur during the months in which doses are given (at 2, 3 and 9 months of age in this trial), the measured overall PE is high. Conversely, if transmission is increasing then the overall measure of PE will be dominated by what is happening during the later months when doses are no longer being given and hence a lower overall protective efficacy will be estimated. When including the maternal immunity function (Figure 4B) the 3^rd dose of IPTi given at nine months of age has the dominant effect on the PE. Changes in transmission affect the extent to which rebound or prolonged protection are observed in the months following the IPTi doses independently of maternal immunity. If overall transmission is being reduced, this in turn reduces the probability of infection once the direct protection afforded by IPTi is removed and hence reduces the potential for the rebound effect to be observed and increases the probability of observing prolonged protection.

The results of the sensitivity analysis of ACPR are shown in Table 5. PE increases when the ACPR is high (i.e. there is little resistance) as the IPT effect is greatest under this scenario and visa versa. Varying ITN coverage from 0–100% had little effect on predicted PEs of the trials (range of variation of PE from baseline (results shown in Table 3): 0–0.6%). Increasing the mean number of infections to become immune against clinical disease from 5 to 10 reduced predicted PE but the magnitude was small (range of variation of PE from baseline: 0.3–0.8%). Varying the effect of number of infections to get anti-parasite immunity also had little effect on predicted PE (range of number attacks required to get anti-parasite immunity: 20–100, range of variation of PE from baseline: 0–0.3%). The maternal immunity function greatly affected predicted PE. Table 6 shows the effect on PE when (a) no immunity is predicted, (b) the models fixed non-parametric form is used (baseline) and (c) a function of maternal immunity against severe disease published elsewhere 19. Without maternal immunity PE is enhanced.