HOME HELP FEEDBACK SUBSCRIPTIONS ARCHIVE SEARCH TABLE OF CONTENTS		QUICK SEARCH:   [advanced] Author: Keyword(s): Year:  Vol:  Page:

This Article Abstract Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Citation Map Services Similar articles in this journal Similar articles in Web of Science Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Web of Science (42) Citing Articles via Google Scholar Google Scholar Articles by TER KUILE, F. O. Articles by NAHLEN, B. L. Search for Related Content PubMed PubMed Citation Articles by TER KUILE, F. O. Articles by NAHLEN, B. L. Related Collections Health Outcomes Malaria Medical Entomology

IMPACT OF PERMETHRIN-TREATED BED NETS ON MALARIA, ANEMIA, AND GROWTH IN INFANTS IN AN AREA OF INTENSE PERENNIAL MALARIA TRANSMISSION IN WESTERN KENYA

ABSTRACT

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

 
As part of a community-based, group-randomized, controlled trial of insecticide-treated bed nets (ITNs) in an area with intense malaria transmission in western Kenya, a birth cohort (n = 833) was followed monthly until the age of 24 months to determine the potential beneficial and adverse effects of reduced malaria exposure during pregnancy and infancy. Malaria transmission and morbidity were comparable pre-intervention. The ITNs reduced malaria attack rates (force of infection) in infancy by 74%, and delayed the median time-to-first parasitemia (4.5 to 10.7 months; P < 0.0001). The incidence of both clinical malaria and moderate-severe anemia (hemoglobin level <7 g/dL) were reduced by 60% (P < 0.001 for both). Protective efficacy was greatest in infants less than three months old and similar in older infants and one-year-old children. Efficacy was lowest in the dry season. Infants from ITN villages experienced better height and weight gain. In areas of intense perennial malaria transmission, ITNs substantially reduce exposure to malaria and subsequent malaria-associated morbidity in children less than 24 months old. Reduced malaria exposure during infancy did not result, with continued ITN use, in increased malaria morbidity in one-year-old children.

INTRODUCTION

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

 
Insecticide-treated bed nets (ITNs) have been demonstrated to markedly reduce malaria morbidity and mortality over a wide range of malaria-endemic settings.¹ Little information is available from randomized controlled trials on the effects of ITNs in settings with intense and perennial malaria transmission,¹ such as in our study site in western Kenya, where the burden of malaria is predominantly in pregnancy and in very young children 2–16 months old.²

We show elsewhere in this supplement that ITNs reduce both the number of malaria transmitting mosquitoes by as much as 90%,³ and adverse effects of malaria in pregnancy, resulting in improved birth weights.⁴ Previous reports by others^5,6 have indicated a further beneficial impact on weight gain with continued ITN use during infancy, likely reflecting improved overall health from reduced episodes of clinical malaria.⁷ One of the previous studies, conducted in an area with low-to-moderate and seasonal malaria transmission in The Gambia, also assessed the impact on linear growth in children, but found none. Infants were not included in this study.⁸ In areas of intense malaria transmission, the periods of maximum vulnerability to malaria and maximum annual growth velocity coincide. It is thus possible, but remains to be determined, that protection from malaria morbidity by ITNs in the first year of life could potentially result in improved linear growth, a benefit that may be sustained beyond the period of highest malaria susceptibility.

Although ITNs have the potential to impart considerable infant health benefit, any intervention that substantially reduces exposure to malaria may also have undesirable consequences. During the first few months of life infants are partially protected from symptomatic malaria through a combination of reduced exposure to mosquito biting, physiologic (e.g., fetal hemoglobin) and immunologic factors, including the transfer of maternal IgG antibodies and possibly sensitization of the fetus in utero.^9,10 Although the mechanisms of these immunologic factors are incompletely understood,⁹ they do suggest that maternal or fetal exposure to malaria during pregnancy may contribute to immune protection in early infancy. While ITNs reduced malaria-associated morbidity in pregnancy,⁴ they also reduced maternal antibody responses to liver and blood stage antigens and the transfer of these antibodies to the newborn, potentially affecting passive immune protection in young infants.¹¹

Similarly, a marked decrease in exposure to malaria early in life may result in a delay in the acquisition of clinical immunity against malaria, which in the long term could result in increased clinical disease and possibly malaria-associated deaths in these children at older ages.^12,13 This is a particular concern in areas of intense malaria transmission, where children experience approximately 10–11 blood-stage infections before the age of one year.¹⁴ It is unclear whether a reduction in this high attack rate will prolong the period of vulnerability beyond 16 months, or may actually result in better antibody responses to malaria blood-stage antigens, possibly resulting from less, but more efficient, immune stimulation, as is suggested by our previous immuno-epidemiologic cohort studies and from our bed net cross-sectional surveys.^15,16

To address the risks and benefits of bed net use before birth and during infancy, we have followed a cohort of pregnant women and their infants as part of the Asembo Bay Cohort Project; a study of the epidemiology of malaria in pregnancy and the acquisition of natural immunity to malaria in children less than five years of age.¹⁷ We report here the impact of bed nets on the dynamics of malaria parasitemia and subsequent malaria morbidity, severe anemia, and growth in the first two years of life. This study also provided the opportunity to evaluate several determinants of ITN efficacy in this young age group.

MATERIALS AND METHODS

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

 
Study site and population. This study was conducted within the context of a large community-based, group-randomized, controlled trial designed to assess the impact of bed nets on mortality in children less than five years of age.¹⁸ The mortality surveillance of the bed net trial was conducted in both Asembo and Gem in an area of 500 km² in Bondo and Siaya districts of western Kenya.¹⁹ The Asembo Bay Cohort Project was conducted in an area of 70 km² (18,000 people) in the southernmost part of Asembo on the shores of Lake Victoria. Full details of the study site have been described elsewhere.^20,21 Briefly, the area has intense perennial malaria transmission (60–300 infective bites per person annually), with Anopheles gambiae as the predominant malaria vector.²² Malaria transmission occurs throughout the year, with peaks during May through July, and October through November. The point prevalence of Plasmodium falciparum parasitemia in children less than five years old ranges between 60% and 80%, depending on the season.¹⁷ More than 95% of these infections are due to P. falciparum, and almost all of the remainder is due to P. malariae. Infections with P. ovale are rare.¹⁷ High-grade chloroquinine resistance is widespread,²³ and parasitologic treatment failure by day 7 with sulfadoxine-pyrimethamine was approximately 20% by the start of the ITN study (ter Kuile FO, unpublished data). Malnutrition is common; 30% of children less than five years old are stunted and 20% are underweight.²⁴ Infant and under-five mortality are very high: 176 and 257 per 1,000 live births, respectively.²⁵

Study design and randomization. Half of the villages in Asembo were randomly assigned to the intervention group and each household in these villages received ITNs, covering all bed spaces, during the fourth quarter of 1996, providing a coverage ratio of 1.5 persons per ITN.²⁶ Households in control villages received ITNs in April 1999 after the mortality trial was completed. Four of the 15 original villages in the Asembo Bay Cohort Project²⁰ were much larger than the remaining 11 and were split into two at the beginning of the ITN project, giving a total of 19 village clusters, henceforth referred to as villages. At distribution, bed nets were pre-treated with permethrin (Siamdutch Mosquito Netting Co., Bangkok, Thailand), and re-treated twice a year by the study team to maintain a target dose of 500 mg of permethrin/m².¹⁹

Asembo Bay Cohort Project. The infants in this cohort were born to women of all parities identified through monthly census by trained village monitors and/or trained traditional birth attendants residing in the same village. All resident pregnant women and their newborns were eligible for enrollment. Full details of recruitment procedures and follow-up of pregnant women and their newborns have been described elsewhere.⁴ Briefly, between June 1992 and April 1999, pregnant women were enrolled and followed at monthly intervals, until the final month of gestation, when weekly visits were conducted. A traditional birth attendant monitored the deliveries and completed a data form that described details of each birth event. At the time of delivery, birth weight and gestational age²⁷ were determined and blood samples obtained from the mother, placenta and cord for determination of malaria parasitemia, hemoglobin concentrations, and malaria serology. Seven and 14 days after birth, and every two weeks thereafter, each newborn child was visited by a village monitor until the end of the study, the child’s second birthday, or until the child’s death, whichever came first. If children moved out of the cohort study area for six or more months, they were dropped from the study (from 1997 onwards). Children born in 1992–1996 were followed until their fifth birthday, but only observations in the first two years of life have been included in this analysis. At each visit, a standard morbidity questionnaire was administered and the axillary temperature was recorded. At every other visit (i.e., every four weeks), a finger or heel prick blood sample (250–500 µL) was taken for determination of hemoglobin (Hb) concentrations or packed cell volume (hematocrit) and the presence of malaria parasites. Anthropometric measurements were also performed at this time. Children with non-severe symptomatic malaria (axillary temperature 37.5°C with any malaria parasitemia) or high density infections (5,000/mm³ [1997 onwards]) detected at follow-up visits, or when the child was ill in between routine visits, received a supervised dose of sulfadoxine-pyrimethamine. All children with severe malaria, with hemoglobin concentrations less than 5 g/dL (hematocrit <15%) or with any other severe disease requiring hospitalization were referred immediately to the local mission hospital for further management free of charge.

The sample size was based on the number of deliveries required to detect a 25% reduction in the prevalence of adverse birth outcome defined as described elsewhere.⁴

Laboratory analysis. All laboratory assays were processed at the Kenya Medical Research Institute/Centers for Disease Control and Prevention laboratories in Kisian, 40 km from the field site. Thick and thin blood smears were stained with Giemsa and examined for parasites. Parasite densities were counted against 300 leukocytes and expressed per mm³ of blood using an estimated leukocyte count of 8,000/mm³. Slides were considered negative if no asexual parasites were found in 200 high-power ocular fields of the thick smear. Between 1992 and 1996, hemoglobin concentrations were measured using the HemoCue system (HemoCue, Angelholm, Sweden). From 1997 onwards, heparinized capillary tubes containing whole blood obtained by finger prick were centrifuged at 10,000 cycles/second for three minutes to determine the hematocrit. All hematocrit values have been divided by a factor of three and are presented as hemoglobin values for consistency with the 1992–1996 data. Hemoglobin electrophoresis was conducted prospectively for all enrolled children born during the intervention phase to determine hemoglobin phenotype. The hemoglobin A and S genes for children born between 1992 and 1996 were typed retrospectively using a polymerase chain reaction method as described by Wu and others.²⁸

Definitions. Malaria parasitemia was defined as asexual blood stage malaria parasites of any Plasmodium species and density detected on a thick blood smear. High-density parasitemia was defined as malaria parasitemia (any species) above an age-dependent threshold parasite density (0–5 months = 1,500/mm³; 6–11 months = 6,000/mm³; and 12–35 months = 7,000/mm³).¹⁷ Symptomatic malaria was defined as a documented axillary temperature 37.5°C in the presence of any malaria parasitemia. Symptomatic high-density malaria was defined as a documented axillary temperature 37.5°C in the presence of high-density parasitemia.¹⁷ Moderately severe and severe anemia were defined as hemoglobin concentrations <7 g/dL and 5 g/dL, respectively, and moderately severe and severe malarial anemia were defined as hemoglobin concentrations <7 g/dL and 5 g/dL, respectively, in the presence of any malaria parasitemia. Force of infection was defined as the attack rate of malaria parasitemia per day per child obtained from a reversible catalytic model (see also Data analysis). The educational status of the caretaker was ranked and grouped in terciles based on the total years of education and categorized as low, medium, high, or missing. Socioeconomic status was divided into percentiles for bivariate analysis and in modeling as a categorical variable as low, medium, high (terciles), or missing, according to the rank position of the computed wealth index based on type of house and ownership of livestock, radios, bicycles, and sofas.²⁹ Each observation was defined to have occurred in the rainy, post-rainy, or dry season using equal rank groups based on rainfall data collected in the study area in the period 30–90 days before the observation. Wasted, underweight, and stunted were defined as having at least two consecutive Z-score values <-2 below the reference median Z-scores for weight-for-length, weight-for-age, and length-for-age, respectively. Nutritional Z-scores were calculated using Epi-Info, version 2000 (Centers for Disease Control and Prevention, Atlanta, GA).

Data analysis. Incidence of morbidity. The age-specific incidence of several morbidity parameters, identified at either the two weekly (clinical assessment) or four weekly (malaria smear and anemia) routine follow-up visits, or in-between scheduled visits, were obtained by dividing the number of episodes fulfilling the case definition by the total number of days at risk for the appropriate age group. The days at risk were obtained by dividing the observation period into time intervals of approximately two weeks (clinical assessment) or four weeks (malaria smears and anemia) corresponding to either the number of days in-between routine home visits, or until an extra visit was made because of an episode fulfilling the case definition, whichever came first. Only intervals of less than 21 days (fever assessment) or 35 days (malaria smears and anemia) were included (i.e., a two or four weekly routine visit could be no more than six days late).¹⁴ Each time interval was assigned to the appropriate age group based on the age of the child at the midpoint of each interval. Observations were included in the time at risk analysis from birth until the child had reached the age of 24 months, was lost to follow-up, or until the date of death, or the end of the study period (December 31, 1996 for the pre-intervention cohort and March 31, 1999 for intervention cohort), whichever came first. All episodes and time at risk, occurring within 28 days (malaria and all cause morbidity) or 84 days (i.e., 3 x 4 weeks) (anemia) after each episode, were excluded from the analysis.³⁰

Force of infection (instantaneous attack rates). Because the standard estimates of infection rates underestimate the true acquisition of malaria infection, the force of infection was also approximated for each intervention group as the acquisition rate (h) per child per day using a reversible catalytic model, which allows for the possibility that a child both gained and cleared (in the absence of treatment) an infection in a given time interval, as described in detail by others.³¹ All episodes and time at risk after each treated episode (sulfadoxine-pyrimethamine) were excluded for a 28-day period from the analysis.

Time to first event. An analysis of determinants of the time and risk of first infection was modeled using Cox-proportional hazards regression models with age independent co-variables (maternal, household, and birth characteristics, including season of birth). Median time to first infection was obtained from Kaplan-Meier survival analysis. Children who missed more than one follow-up visit (interval of 35 days or greater) were considered censored at the age of the last visit (status unknown after that age).

Statistical analysis. All analyses were based on intention-to-treat, and took the cluster design at the village level into account. SUDAAN release 8 (Research Triangle Institute, Research Triangle Park, NC), Statistical Analysis System (SAS 8.2; SAS Institute, Cary, NC), and STATA (Intercooled version 7; Stata Corp., College Station, TX) software packages were used.

Data collected before the start of the ITN study, i.e., between June 1992 and December 31, 1996, were used to compare the distribution of the endpoints and characteristics prior to the introduction of ITNs. Data collected between January 1, 1997 and April 1, 1999 were used to assess the impact of ITNs. The statistical significance of the differences in the incidence of morbidity measures between (subsequent) ITN and control villages was tested using Poisson regression with the number of days at risk as the offset. The magnitude of the effect of ITNs was expressed as the protective efficacy and estimated as 100 x (1 – adjusted rate ratio)% or 100 x (1 – adjusted hazard ratio). All Poisson or Cox-proportional hazard regression models allowed for the effect of age by including age as categorical variables (as 0–2, 3–5, 6–8, 9–11, 12–15, and 16–23 months unless indicated otherwise), and also included sickle hemoglobin phenotype (HbAS, HbAA, HbSS, or missing) rainfall and gravidity. Years of education of the caretakers were unequally divided between ITN and control villages and associated with some of the morbidity endpoints independent of maternal age. Educational status, ranked in three categories based on reported years of schooling was, therefore, included as covariate in all subsequent models to adjust for any potential confounding.

To compare the differences between the mean nutritional score in the ITN and control groups, a repeated measure analysis in SAS proc mixed, using maximum likelihood estimation and a compound symmetry covariance structure to account for the within village clustering, was implemented. To account for any misspecification in the covariance structure a robust (empirical) variance estimator was used. Because of a difference in mean length-for-age Z-scores by randomization status before the introduction of ITNs, we also assessed the impact of ITNs using a historical comparison by adding an interaction term for the time-effect and randomization-group to the models. The time-effect indicated whether the observation was before or after January 1, 1997 (the start of the ITN study). Two sided P values <0.05 were considered statistically significant.

Ethical clearance. The ITN study and the Asembo Bay Cohort Project were approved by the institutional review boards of the Kenya Medical Research Institute (Nairobi, Kenya) and the Centers for Disease Control and Prevention (Atlanta, GA). Informed consent was obtained from all caretakers after explanation of the study procedures in the local language.

RESULTS

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

 
In the pre-intervention period, 1,501 single live births were enrolled at birth or within 14 days thereafter, and a further 860 during the intervention period (Figure 1). Of these, 1,451 (96.7%) pre-intervention and 831 (96.6%) during intervention contributed at least 28 days follow-up time and were included in the analysis (Table 1).

View larger version (58K): [in this window] [in a new window]   FIGURE 1. Trial profile. LTFU = lost to follow-up, ITN = insecticide-treated bed net.

Characteristics of the study sample. During the intervention period, children from ITN and control villages were born to households with equal socioeconomical status, but the caretakers from ITN villages had more years of education (P = 0.01) (Table 1). Prompted questioning showed that 94.7% of the infants from households in the ITN villages (1997 onwards) were reported to sleep under an ITN on a regular basis, of whom 99.7% (i.e., 94.4% of the intervention group) reportedly used the study net. Only 8.4% of the households in the control villages reported using an ITN (1997 onwards), of whom 26.5% reported using the treated study ITN (i.e. 2.2% of the control group).

Malaria parasitology. The overall crude median time to first infection was 3.1 months in the pre-intervention period (pre-ITN = 3.3, pre-control = 3.0), and 10.7 (ITN) versus 4.5 (control) months during the intervention period (Figure 2). In the pre-intervention period, the estimates of the daily attack (h) rate, obtained from the catalytic conversion model (force of infection) was 0.0233 (95% confidence interval [CI] = 0.0221–0.0245). Results were similar in pre-ITN and pre-control villages: (0.0218 [95% CI = 0.0200–0.0233] and 0.0249 [95% CI = 0.0231–0.0267], respectively). During the intervention period, h was 69% lower in ITN than control villages (0.0041 [95% CI = 0.0033–0.0048]) versus 0.0133 [95% CI = 0.0116–0.0151], respectively). The reduction in h from the force of infection model containing only infants was 74%.

View larger version (24K): [in this window] [in a new window]   FIGURE 2. Time to first parasitemia. ITN = insecticide-treated bed net; PE = protective efficacy. Value in parenthesis is the 95% confidence interval.

View larger version (24K): [in this window] [in a new window]   FIGURE 3. Incidence of high-density symptomatic malaria (top graph) and moderate-severe anemia (hemoglobin level < 7 g/dL) (bottom graph) by age and randomization status. PE = protective efficacy: 100 x (1 – hazard ratio ITN/control); ITN = insecticide-treated bed net; CI = confidence interval.

View larger version (17K): [in this window] [in a new window]   FIGURE 4. Mean nutritional Z-scores, by age and randomization status during the intervention phase. The x-axis values represent the mean age for each age category for each point estimate. ITN = insecticide-treated bed net; WHZ = weight-for-length Z-score; WAZ = weight-for-age Z-score; HAZ = length-for-age Z-score.

DISCUSSION

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

The ITNs were found to reduce the force of infection in infancy by 74%, resulting in a delay in time to first infection from 4.5 to 10.7 months. The clinical benefits of this reduced exposure were found to be substantial; the incidence of symptomatic high-density malaria, as well as moderately severe anemia, was reduced by 60%. These efficacy estimates on malaria morbidity are higher than those found in our separate cross-sectional surveys conducted simultaneously in 60 adjacent study villages (44% and 39%, respectively),³² reflecting the younger age group in this birth cohort and the assessment of incidence instead of prevalence. Our estimate of protective efficacy for all cause severe anemia is remarkably similar to that obtained from the social-marketing program of ITN in Ifakara Tanzania (63%), which also included children less than two years old.³³ Spatial analyses presented in a companion report in this supplement suggest that the true efficacy of ITNs may be even higher because the high ITN coverage resulted in an area wide reduction in malaria transmission, which in turn reduced malaria-associated morbidity in young children from control households located within 300 meters of an ITN village (community or mass effect).³⁴ In addition to reduced rainfall in 1998 compared with 1992–1996,²¹ the community effect also partly explains the lower morbidity and longer time to first infection in the control villages during the intervention period compared with pre-intervention (4.5 versus 3.0 months).

The efficacy of ITNs was greatest in the rainy season and the months following the rains, when malaria transmission is highest, and lowest in the dry season, consistent with our passive surveillance studies.³⁵ There was no indication that the efficacy was lower in the second study year, consistent with our mortality analysis,¹⁸ but different from the results of our passive surveillance monitoring³⁵ and some of the previous mortality trials.³⁶

Similar to reports by others,^5,6,8 mid-upper-arm circumference and weight-for-age Z-scores were better in children from intervention villages. The weight gain benefit was only apparent in infancy. In addition, a significant difference in length-for-age Z-scores was apparent (mean difference in Z-score = 0.36). Although this difference was statistically significant (P = 0.01), it could not be concluded with certainty that this was associated with the introduction of ITNs because of an existing difference, albeit smaller and not statistically significant, in length-for-age Z-scores pre-intervention (mean difference in Z-score = 0.17; P = 0.08). Of interest is that unlike weight gain, the beneficial effect on linear growth was maintained in the second year of life. Thus, ITN use in infancy, the period of maximum annual growth velocity in life, could potentially result in sustained benefits, since the opportunity for catch-up growth later in life is limited for children who remain in the same unfavorable environment, as is the case in most parts of the developing world.^37,38

The frequency of non-malaria-related illnesses, including the incidence of mild upper respiratory symptoms and ear and eye infections, remained unaffected by ITNs. A higher incidence of non-malaria fevers was observed in ITN villages (P = 0.06) during the intervention period. This is unlikely to reflect replacement morbidity by other diseases following the reduction in malaria, but more likely reflects the unexplained 50% decrease in the incidence of non-malaria fevers in the control villages from pre to post-intervention, whereas in ITN villages it remained the same.

We reported elsewhere that ITN use in pregnancy reduced maternal IgG antibody concentrations in the cord blood of newborns against blood-stage antigens (merozoite surface protein-1).¹¹ These maternal antibodies may provide important passive immune protection against malaria in the first few months of life.⁹ Our current epidemiologic observations suggest that, with continued ITN use by the newborn, this does not result in increased risks of blood stage infection or clinical malaria in the first few months of life. Indeed, the efficacy of ITNs appeared greatest in the infants less than three months old. The protective efficacy estimates were greater than 70% for all malaria morbidity parameters in this age group.

Although ITNs had the greatest impact in the youngest infants, they were also found to be protective in children between 16 and 24 months of age. The efficacy in this older age group was the same as in children 3–11 or 12–15 months of age. Although these findings do not exclude the possibility that decreased exposure to malaria early in life may result in delayed acquisition of immunity against malaria,^12,13,39 they do suggest that, with continued ITN use, this does not result in increased clinical disease in one-year-old children. This is consistent with the finding from our cross-sectional surveys that reduced exposure to malaria does not compromise, but may improve humoral immune responses in young children to well-characterized pre-erythrocytic and erythrocytic malaria vaccine candidate antigens.¹⁶

It is important to note the limitations of these findings. They only apply to children who continue using properly retreated ITNs after infancy, but tell us little what will happen if children stop using ITNs on a regular basis post-infancy. Furthermore, the observation time contributed by children in the 16–24-months-old age group was limited, as well as the precision of the corresponding efficacy estimates (Figure 3). This was because only 30% of the cohort was born in time to reach the age of 16 months before the end of the study, and 25% of them had died (12%) or defaulted (13%) by 12 months. Furthermore, our observation time was restricted to 24 months and a shift in morbidity to older children can thus not be excluded. Further investigations with larger numbers and longer bed net use and follow-up (four years) are under way to validate and extend these findings.

The sample included in this cohort represented approximately 84% of all births that occurred during the intervention period in these 19 villages. Approximately 3.6% of the approached households with pregnant women refused to participate, but no information was available from the remaining non-participants. They likely include recent arrivals and also young unmarried teenage primigravidae, who are more mobile than multigravidae in this rural community, and often move temporarily to other family households for the perinatal period (Alaii JA, unpublished data). For the same reasons, enrolled infants of young mothers were the most likely to be lost-to-follow-up, but the default rate was equally divided between ITN and control villages. Mothers of newborns from intervention villages had more years of education (P = 0.01), but this potential source of bias was adjusted for in multivariate analysis. Furthermore, malaria transmission and malaria morbidity in the four years prior to the start of the ITN study were comparable in the ITN and control villages, and the observed benefit was greatest for the malaria-specific parameters and absent for non-malaria illness. We believe therefore that these results are valid and representative for areas with intense perennial malaria transmission and high coverage of continued bed net use.

We conclude that in this area of intense perennial malaria transmission, ITNs not only reduce malaria and its adverse effects in gravidae 1–4,⁴ but also reduce malaria-associated morbidity in their newborns by 60% and improve growth, regardless of birth order. The ITNs were equally as effective in the second year of life as in infancy. Thus, although follow-up was limited to 24 months, there was no evidence that, with continued use of properly re-treated bed nets, a 74% reduction in the force of infection in infancy was associated with an increased risk of malaria morbidity in one-year old children. These results suggest that the use of ITNs by pregnant women and their newborns can result in substantial health benefits which outweigh any potential adverse effects in areas of intense malaria transmission.

Acknowledgments: We express our gratitude to the children and caretakers who participated in the study and the many people that assisted with this project. We thank Pauline Abdullah, Benta Kamire, Lucy Atieno, Christi Murray, Erik Schoute, Sue Binder, and Dan Colley for their continued support. We are grateful to Drs. Laurence Slutsker and Richard Steketee (Centers for Disease Control and Prevention) for reviewing this manuscript. We also thank the Director of the Kenya Medical Research Institute for his permission to publish this work.

Financial support: The ITN project was funded by the United States Agency for International Development. Feiko O. ter Kuile and Dianne J. Terlouw were partly supported by a grant from the Nether-lands Foundation for the Advancement of Tropical Research (WOTRO) (The Hague, The Netherlands). Lisa B. Mirel acknowledges administrative support from the Oak Ridge Institute for Science and Education. Jennifer F. Friedman was supported by a United States Fulbright Award.

Disclaimer: The opinions or assertions contained in this manuscript are the private ones of the authors and are not to be construed as official or reflecting the views of the U.S. Public Health Service or Department of Health and Human Services. Use of trade names is for identification only and does not imply endorsement by the U.S. Public Health Service or Department of Health and Human Services.

Authors’ addresses: Feiko O. ter Kuile, Dianne J. Terlouw, Penelope A. Phillips-Howard, Lisa B. Mirel, William A. Hawley, Margarette S. Kolczak, and Altaf A. Lal, Division of Parasitic Diseases, National Center for Infectious Diseases, Centers for Disease Control and Prevention, Mailstop F-22, 4770 Buford Highway, Atlanta, GA 30341. Simon K. Kariuki, Ya Ping Shi, and John M. Vulule, Centre for Vector Biology and Control Research, Kenya Medical Research Institute, PO Box 1578, Kisumu, Kenya. Jennifer F. Friedman, International Health Institute, Brown University, Box G-B 495, Providence, RI 02912. Bernard L. Nahlen, Roll Back Malaria, World Health Organization, Avenue Appia 20, 1211 Geneva 27, Switzerland.

REFERENCES

TOP ABSTRACT INTRODUCTION MATERIALS AND METHODS RESULTS DISCUSSION REFERENCES

 

1. Lengeler C, 2000. Insecticide-treated bednets and curtains for preventing malaria. Cochrane Database Syst Rev 320: CD000363.
2. Aidoo M, Terlouw DJ, Kolczak MS, McElroy PD, ter Kuile FO, Kariuki S, Nahlen BL, Lal AA, Udhayakumar V, 2002. Protective effects of the sickle cell gene against malaria morbidity and mortality. Lancet 359: 1311–1312.[Web of Science][Medline]
3. Gimnig JE, Vulule JM, Lo TQ, Kamau L, Kolczak MS, Phillips-Howard PA, Mathenge EM, ter Kuile FO, Nahlen BL, High-tower AW, Hawley WA, 2003. Impact of permethrin-treated bed nets on entomologic indices in an area of intense year round malaria transmission. Am J Trop Med Hyg 68(Suppl 4): 16–22.[Abstract/Free Full Text]
4. ter Kuile FO, Terlouw DJ, Phillips-Howard PA, Hawley WA, Friedman JF, Kariuki SK, Shi YP, Kolczak MS, Lal AA, Vulule JM, Nahlen BL, 2003. Reduction of malaria during pregnancy by permethrin-treated bed nets in an area of intense perennial malaria transmission in western Kenya. Am J Trop Med Hyg 68(Suppl 4): 50–60.[Abstract/Free Full Text]
5. Shiff C, Checkley W, Winch P, Premji Z, Minjas J, Lubega P, 1996. Changes in weight gain and anaemia attributable to malaria in Tanzanian children living under holoendemic conditions. Trans R Soc Trop Med Hyg 90: 262–265.[Web of Science][Medline]
6. Snow RW, Molyneux CS, Njeru EK, Omumbo J, Nevill CG, Muniu E, Marsh K, 1997. The effects of malaria control on nutritional status in infancy. Acta Trop 65: 1–10.[Web of Science][Medline]
7. Rowland MG, Cole TJ, Whitehead RG, 1977. A quantitative study into the role of infection in determining nutritional status in Gambian village children. Br J Nutr 37: 441–450.[Web of Science][Medline]
8. D’Alessandro U, Olaleye BO, McGuire W, Langerock P, Bennett S, Aikins MK, Thomson MC, Cham MK, Cham BA, Greenwood BM, 1995. Mortality and morbidity from malaria in Gambian children after introduction of an impregnated bed-net programme. Lancet 345: 479–483.[Web of Science][Medline]
9. Riley EM, Wagner GE, Akanmori BD, Koram KA, 2001. Do maternally acquired antibodies protect infants from malaria infection? Parasite Immunol 23: 51–59.[Web of Science][Medline]
10. King CL, Malhotra I, Wamachi A, Kioko J, Mungai P, Wahab SA, Koech D, Zimmerman P, Ouma J, Kazura JW, 2002. Acquired immune responses to Plasmodium falciparum merozoite surface protein-1 in the human fetus. J Immunol 168: 356–364.[Abstract/Free Full Text]
11. Kariuki SK, ter Kuile FO, Wannemuehler KA, Terlouw DJ, Kolczak MS, Hawley WA, Phillips-Howard PA, Orago ASS, Nahlen BL, Lal AA, Shi YP, 2003. Effects of permethrin-treated bed nets on immunity to malaria in western Kenya. I: Antibody responses in pregnant women and cord blood in an area of intense malaria transmission. Am J Trop Med Hyg 68(Suppl 4): 61–67.[Abstract/Free Full Text]
12. Snow RW, Marsh K, 1995. Will reducing Plasmodium falciparum transmission alter malaria mortality among African children? Parasitol Today 11: 188–190.[Web of Science]
13. Snow RW, Omumbo JA, Lowe B, Molyneux CS, Obiero JO, Palmer A, Weber MW, Pinder M, Nahlen B, Obonyo C, New-bold C, Gupta S, Marsh K, 1997. Relation between severe malaria morbidity in children and level of Plasmodium falciparum transmission in Africa. Lancet 349: 1650–1654.[Web of Science][Medline]
14. Kitua AY, Smith T, Alonso PL, Masanja H, Urassa H, Menendez C, Kimario J, Tanner M, 1996. Plasmodium falciparum malaria in the first year of life in an area of intense and perennial transmission. Trop Med Int Health 1: 475–484.[Web of Science][Medline]
15. Branch OH, Oloo AJ, Nahlen BL, Kaslow D, Lal AA, 2000. Anti-merozoite surface protein-1 19-kDa IgG in mother-infant pairs naturally exposed to Plasmodium falciparum: subclass analysis with age, exposure to asexual parasitemia, and protection against malaria. V. The Asembo Bay Cohort Project. J Infect Dis 181: 1746–1752.[Web of Science][Medline]
16. Kariuki SK, Lal AA, Terlouw DJ, ter Kuile FO, Ong’echa JMO, Phillips-Howard PA, Orago ASS, Kolczak MS, Hawley WA, Nahlen BL, Shi YP, 2003. Effects of permethrin-treated bed nets on immunity to malaria in western Kenya. II: Antibody responses in young children in an area of intense malaria transmission. Am J Trop Med Hyg 68(Suppl 4): 108–114.[Abstract/Free Full Text]
17. Bloland PB, Boriga DA, Ruebush TK, McCormick JB, Roberts JM, Oloo AJ, Hawley W, Lal A, Nahlen B, Campbell CC, 1999. Longitudinal cohort study of the epidemiology of malaria infections in an area of intense malaria transmission II. Descriptive epidemiology of malaria infection and disease among children. Am J Trop Med Hyg 60: 641–648.[Abstract]
18. Phillips-Howard PA, Nahlen BL, Kolczak MS, Hightower AW, ter Kuile FO, Alaii JA, Gimnig JE, Arudo J, Vulule JM, Odacha A, Kachur SP, Schoute E, Rosen DH, Sexton JD, Oloo AJ, Hawley WA, 2003. Efficacy of permethrin-treated bed nets in the prevention of mortality in young children in an area of high perennial malaria transmission in western Kenya. Am J Trop Med Hyg 68(Suppl 4): 23–29.[Abstract/Free Full Text]
19. Phillips-Howard PA, ter Kuile FO, Nahlen BL, Alaii JA, Gimnig JE, Kolczak MS, Terlouw DJ, Kariuki SK, Shi YP, Kachur SP, Hightower AW, Vulule JM, Hawley WA, 2003. The efficacy of permethrin-treated bed nets on child mortality and morbidity in western Kenya. II: Study design and methods. Am J Trop Med Hyg 68(Suppl 4): 10–15.[Abstract/Free Full Text]
20. Bloland PB, Ruebush TK, McCormick JB, Ayisi J, Boriga DA, Oloo AJ, Beach R, Hawley W, Lal A, Nahlen B, Udhayakumar V, Campbell CC, 1999. Longitudinal cohort study of the epidemiology of malaria infections in an area of intense malaria transmission I. Description of study site, general methodology, and study population. Am J Trop Med Hyg 60: 635–640.[Abstract]
21. Phillips-Howard PA, Nahlen BL, Alaii JA, ter Kuile FO, Gimnig JE, Terlouw DJ, Kachur SP, Hightower AW, Lal AA, Schoute E, Oloo AJ, Hawley WA, 2003. The efficacy of permethrin-treated bed nets on child mortality and morbidity in western Kenya. I: Development of infrastructure and description of study site. Am J Trop Med Hyg 68(Suppl 4): 3–9.[Abstract/Free Full Text]
22. Beier JC, Oster CN, Onyango FK, Bales JD, Sherwood JA, Perkins PV, Chumo DK, Koech DV, Whitmire RE, Roberts CR, 1994. Plasmodium falciparum incidence relative to entomologic inoculation rates at a site proposed for testing malaria vaccines in western Kenya. Am J Trop Med Hyg 50: 529–536.
23. Bloland PB, Lackritz EM, Kazembe PN, Were JB, Steketee R, Campbell CC, 1993. Beyond chloroquine: implications of drug resistance for evaluating malaria therapy efficacy and treatment policy in Africa. J Infect Dis 167: 932–937.[Web of Science][Medline]
24. Kwena AM, Terlouw DJ, de Vlas SJ, Phillips-Howard PA, Hawley WA, Friedman JF, Vulule JM, Nahlen BL, Sauerwein RW, ter Kuile FO, 2003. Prevalence and severity of malnutrition in pre-school children in a rural area in western Kenya. Am J Trop Med Hyg 68(Suppl 4): 94–99.[Abstract/Free Full Text]
25. McElroy PD, ter Kuile FO, Hightower AW, Hawley WA, Phillips-Howard PA, Oloo AJ, Lal AA, Nahlen BL, 2001. All-cause mortality among young children in western Kenya. VI: the Asembo Bay Cohort Project. Am J Trop Med Hyg 64: 18–27.[Abstract/Free Full Text]
26. Alaii JA, Hawley WA, Kolczak MS, ter Kuile FO, Gimnig JE, Vulule JM, Odhacha A, Oloo AJ, Nahlen BL, Phillips-Howard PA, 2003. Factors affecting use of permethrin-treated bed nets during a randomized-controlled trial in western Kenya. Am J Trop Med Hyg 68(Suppl 4): 137–141.[Abstract/Free Full Text]
27. Ballard JL, Novak KK, Driver M, 1979. A simplified score for assessment of fetal maturation of newly born infants. J Pediatr 95: 769–774.[Web of Science][Medline]
28. Wu DY, Ugozzoli L, Pal BK, Wallace RB, 1989. Allele-specific enzymatic amplification of beta-globin genomic DNA for diagnosis of sickle cell anemia. Proc Natl Acad Sci USA 86: 2757–2760.[Abstract/Free Full Text]
29. Meltzer MI, Terlouw DJ, Kolczak MS, Odhacha A, ter Kuile FO, Vulule JM, Alaii JA, Nahlen BL, Hawley WA, Phillips-Howard PA, 2003. The household-level economics of using permethrin-treated bed nets to prevent malaria in children less than five years of age. Am J Trop Med Hyg 68(Suppl 4): 149–160.[Abstract/Free Full Text]
30. Smith T, Charlwood JD, Kitua AY, Masanja H, Mwankusye S, Alonso PL, Tanner M, 1998. Relationships of malaria morbidity with exposure to Plasmodium falciparum in young children in a highly endemic area. Am J Trop Med Hyg 59: 252–257.[Abstract]
31. Charlwood JD, Smith T, Lyimo E, Kitua AY, Masanja H, Booth M, Alonso PL, Tanner M, 1998. Incidence of Plasmodium falciparum infection in infants in relation to exposure to sporozoite-infected anophelines. Am J Trop Med Hyg 59: 243–251.[Abstract]
32. ter Kuile FO, Terlouw DJ, Phillips-Howard PA, Hawley WA, Friedman JF, Kolczak MS, Kariuki SK, Shi YP, Kwena AM, Vulule JM, Nahlen BL, 2003. Impact of permethrin-treated bed nets on malaria and all-cause morbidity in young children in an area of intense perennial malaria transmission in western Kenya: Cross-sectional survey. Am J Trop Med Hyg 68(Suppl 4): 100–107.[Abstract/Free Full Text]
33. Abdulla S, Schellenberg JA, Nathan R, Mukasa O, Marchant T, Smith T, Tanner M, Lengeler C, 2001. Impact on malaria morbidity of a programme supplying insecticide treated nets in children aged under 2 years in Tanzania: community cross sectional study. BMJ 322: 270–273.[Abstract/Free Full Text]
34. Hawley WA, Phillips-Howard PA, ter Kuile FO, Terlouw DJ, Vulule JM, Ombok M, Nahlen BL, Gimnig JE, Kariuki SK, Kolczak MS, Hightower AW, 2003. Community-wide effects of permethrin-treated bed nets on child mortality and malaria morbidity in western Kenya. Am J Trop Med Hyg 68(Suppl 4): 121–127.[Abstract/Free Full Text]
35. Phillips-Howard PA, Nahlen BL, Wannemuehler KA, Kolczak MS, ter Kuile FO, Gimnig JE, Alaii JA, Odacha A, Vulule JM, Hawley WA, 2003. Impact of permethrin-treated bed nets on the incidence of sick child visits to peripheral health facilities. Am J Trop Med Hyg 68(Suppl 4): 38–43.[Abstract/Free Full Text]
36. Habluetzel A, Diallo DA, Esposito F, Lamizana L, Pagnoni F, Lengeler C, Traore C, Cousens SN, 1997. Do insecticide-treated curtains reduce all-cause child mortality in Burkina Faso? Trop Med Int Health 2: 855–862.[Web of Science][Medline]
37. Martorell R, Kettel Khan L, Schroeder DG, 1994. Reversability of stunting: epidemiological findings in children from developing countries. Eur J Clin Nutr 48(Suppl 1): S45–S57.
38. Golden MH, 1994. Is complete catch-up possible for stunted malnourished children? Eur J Clin Nutr 48(Suppl 1): S58–S70 and discussion S71.
39. Askjaer N, Maxwell C, Chambo W, Staalsoe T, Nielsen M, Hviid L, Curtis C, Theander TG, 2001. Insecticide-treated bed nets reduce plasma antibody levels and limit the repertoire of antibodies to Plasmodium falciparum variant surface antigens. Clin Diagn Lab Immunol 8: 1289–1291.[Abstract/Free Full Text]

This article has been cited by other articles:

				J. G. Siri, M. L. Wilson, S. Murray, D. H. Rosen, J. M. Vulule, L. Slutsker, and K. A. Lindblade Significance of Travel to Rural Areas as a Risk Factor for Malarial Anemia in an Urban Setting Am J Trop Med Hyg, March 1, 2010; 82(3): 391 - 397. [Abstract] [Full Text] [PDF]

				F. Fillol, A. Cournil, C. Cames, C. Sokhna, and K. B. Simondon Active Malaria Morbidity Management Has Limited Impact on Height Status of Preschool Senegalese Children J. Nutr., March 1, 2010; 140(3): 625 - 629. [Abstract] [Full Text] [PDF]

				H. Z. Ouedraogo, A. Zeba, M. Dramaix-Wilmet, and P. Donnen Moderate-to-Severe Anaemia due to Afebrile Plasmodium falciparum Infection in Children aged 6-23 Months from the Rural District of Kongoussi, Burkina Faso J Trop Pediatr, December 1, 2008; 54(6): 395 - 400. [Abstract] [Full Text] [PDF]

				R. W. Steketee, N. Sipilanyambe, J. Chimumbwa, J. J. Banda, A. Mohamed, J. Miller, S. Basu, S. K. Miti, and C. C. Campbell National Malaria Control and Scaling Up for Impact: The Zambia Experience through 2006 Am J Trop Med Hyg, July 1, 2008; 79(1): 45 - 52. [Abstract] [Full Text] [PDF]

				B. Ntab, B. Cisse, D. Boulanger, C. Sokhna, G. Targett, J. Lines, N. Alexander, J.-F. Trape, F. Simondon, B. M. Greenwood, et al. Impact of Intermittent Preventive Anti-Malarial Treatment on the Growth and Nutritional Status of Preschool Children in Rural Senegal (West Africa) Am J Trop Med Hyg, September 1, 2007; 77(3): 411 - 417. [Abstract] [Full Text] [PDF]

				J. F. FRIEDMAN, A. M. KWENA, L. B. MIREL, S. K. KARIUKI, D. J. TERLOUW, P. A. PHILLIPS-HOWARD, W. A. HAWLEY, B. L. NAHLEN, Y. P. SHI, and F. O. T. KUILE MALARIA AND NUTRITIONAL STATUS AMONG PRE-SCHOOL CHILDREN: RESULTS FROM CROSS-SECTIONAL SURVEYS IN WESTERN KENYA Am J Trop Med Hyg, October 1, 2005; 73(4): 698 - 704. [Abstract] [Full Text] [PDF]

				T. P. EISELE, K. A. LINDBLADE, K. A. WANNEMUEHLER, J. E. GIMNIG, F. ODHIAMBO, W. A. HAWLEY, F. O. TER KUILE, P. PHILLIPS-HOWARD, D. H. ROSEN, B. L. NAHLEN, et al. EFFECT OF SUSTAINED INSECTICIDE-TREATED BED NET USE ON ALL-CAUSE CHILD MORTALITY IN AN AREA OF INTENSE PERENNIAL MALARIA TRANSMISSION IN WESTERN KENYA Am J Trop Med Hyg, July 1, 2005; 73(1): 149 - 156. [Abstract] [Full Text] [PDF]

				M. R. DESAI, D. J. TERLOUW, A. M. KWENA, P. A. PHILLIPS-HOWARD, S. K. KARIUKI, K. A. WANNEMUEHLER, A. ODHACHA, W. A. HAWLEY, Y. P. SHI, B. L. NAHLEN, et al. FACTORS ASSOCIATED WITH HEMOGLOBIN CONCENTRATIONS IN PRE-SCHOOL CHILDREN IN WESTERN KENYA: CROSS-SECTIONAL STUDIES Am J Trop Med Hyg, January 1, 2005; 72(1): 47 - 59. [Abstract] [Full Text] [PDF]

				A. M Nyakeriga, M. Troye-Blomberg, A. K Chemtai, K. Marsh, and T. N Williams Malaria and nutritional status in children living on the coast of Kenya Am. J. Clinical Nutrition, December 1, 2004; 80(6): 1604 - 1610. [Abstract] [Full Text] [PDF]

				S. Pinchinat, C. Enel, G. Pison, G. Duthe, E. Lagarde, F. Simondon, and K. B Simondon No improvement in weight-for-age of young children in southern Senegal, 1969-1992, despite a drastic reduction in mortality. Evidence from a growth monitoring programme Int. J. Epidemiol., December 1, 2004; 33(6): 1202 - 1208. [Abstract] [Full Text] [PDF]

				J. CRAWLEY REDUCING THE BURDEN OF ANEMIA IN INFANTS AND YOUNG CHILDREN IN MALARIA-ENDEMIC COUNTRIES OF AFRICA: FROM EVIDENCE TO ACTION Am J Trop Med Hyg, August 1, 2004; 71(2_suppl): 25 - 34. [Abstract] [Full Text] [PDF]

				K. A. Lindblade, T. P. Eisele, J. E. Gimnig, J. A. Alaii, F. Odhiambo, F. O. ter Kuile, W. A. Hawley, K. A. Wannemuehler, P. A. Phillips-Howard, D. H. Rosen, et al. Sustainability of Reductions in Malaria Transmission and Infant Mortality in Western Kenya With Use of Insecticide-Treated Bednets: 4 to 6 Years of Follow-up JAMA, June 2, 2004; 291(21): 2571 - 2580. [Abstract] [Full Text] [PDF]

				P. B. Soeters, M. C. G. van de Poll, W. G. van Gemert, and C. H. C. Dejong Amino Acid Adequacy in Pathophysiological States J. Nutr., June 1, 2004; 134(6): 1575S - 1582S. [Abstract] [Full Text] [PDF]

				D. J Terlouw, M. R Desai, K. A Wannemuehler, S. K Kariuki, C. M Pfeiffer, P. A Kager, Y. P. Shi, and F. O ter Kuile Relation between the response to iron supplementation and sickle cell hemoglobin phenotype in preschool children in western Kenya Am. J. Clinical Nutrition, March 1, 2004; 79(3): 466 - 472. [Abstract] [Full Text] [PDF]

				D. J. Terlouw, B. L. Nahlen, J. M. Courval, S. K. Kariuki, O. S. Rosenberg, A. J. Oloo, M. S. Kolczak, W. A. Hawley, A. A. Lal, and F. O. t. Kuile Sulfadoxine-Pyrimethamine in Treatment of Malaria in Western Kenya: Increasing Resistance and Underdosing Antimicrob. Agents Chemother., September 1, 2003; 47(9): 2929 - 2932. [Abstract] [Full Text] [PDF]

				P. A. PHILLIPS-HOWARD, F. O. TER KUILE, B. L. NAHLEN, J. A. ALAII, J. E. GIMNIG, M. S. KOLCZAK, D. J. TERLOUW, S. K. KARIUKI, Y. P. SHI, S. P. KACHUR, et al. THE EFFICACY OF PERMETHRIN-TREATED BED NETS ON CHILD MORTALITY AND MORBIDITY IN WESTERN KENYA II. STUDY DESIGN AND METHODS Am J Trop Med Hyg, April 1, 2003; 68(90040): 10 - 15. [Abstract] [Full Text] [PDF]

				P. A. PHILLIPS-HOWARD, B. L. NAHLEN, M. S. KOLCZAK, A. W. HIGHTOWER, F. O. TER KUILE, J. A. ALAII, J. E. GIMNIG, J. ARUDO, J. M. VULULE, A. ODHACHA, et al. EFFICACY OF PERMETHRIN-TREATED BED NETS IN THE PREVENTION OF MORTALITY IN YOUNG CHILDREN IN AN AREA OF HIGH PERENNIAL MALARIA TRANSMISSION IN WESTERN KENYA Am J Trop Med Hyg, April 1, 2003; 68(90040): 23 - 29. [Abstract] [Full Text] [PDF]

				P. A. PHILLIPS-HOWARD, B. L. NAHLEN, K. A. WANNEMUEHLER, M. S. KOLCZAK, F. O. TER KUILE, J. E. GIMNIG, K. OLSON, J. A. ALAII, A. ODHACHA, J. M. VULULE, et al. IMPACT OF PERMETHRIN-TREATED BED NETS ON THE INCIDENCE OF SICK CHILD VISITS TO PERIPHERAL HEALTH FACILITIES Am J Trop Med Hyg, April 1, 2003; 68(90040): 38 - 43. [Abstract] [Full Text] [PDF]

				F. O. TER KUILE, D. J. TERLOUW, P. A. PHILLIPS-HOWARD, W. A. HAWLEY, J. F. FRIEDMAN, S. K. KARIUKI, Y. P. SHI, M. S. KOLCZAK, A. A. LAL, J. M. VULULE, et al. REDUCTION OF MALARIA DURING PREGNANCY BY PERMETHRIN-TREATED BED NETS IN AN AREA OF INTENSE PERENNIAL MALARIA TRANSMISSION IN WESTERN KENYA Am J Trop Med Hyg, April 1, 2003; 68(90040): 50 - 60. [Abstract] [Full Text] [PDF]

				S. K. KARIUKI, F. O. TER KUILE, K. WANNEMUEHLER, D. J. TERLOUW, M. S. KOLCZAK, W. A. HAWLEY, P. A. PHILLIPS-HOWARD, A. S. S. ORAGO, B. L. NAHLEN, A. A. LAL, et al. EFFECTS OF PERMETHRIN-TREATED BED NETS ON IMMUNITY TO MALARIA IN WESTERN KENYA I. ANTIBODY RESPONSES IN PREGNANT WOMEN AND CORD BLOOD IN AN AREA OF INTENSE MALARIA TRANSMISSION Am J Trop Med Hyg, April 1, 2003; 68(90040): 61 - 67. [Abstract] [Full Text] [PDF]

				T. LEENSTRA, P. A. PHILLIPS-HOWARD, S. K. KARIUKI, W. A. HAWLEY, J. A. ALAII, D. H. ROSEN, A. J. OLOO, B. L. NAHLEN, P. A. KAGER, and F. O. TER KUILE PERMETHRIN-TREATED BED NETS IN THE PREVENTION OF MALARIA AND ANEMIA IN ADOLESCENT SCHOOLGIRLS IN WESTERN KENYA Am J Trop Med Hyg, April 1, 2003; 68(90040): 86 - 93. [Abstract] [Full Text] [PDF]

				A. M. KWENA, D. J. TERLOUW, S. J. DE VLAS, P. A. PHILLIPS-HOWARD, W. A. HAWLEY, J. F. FRIEDMAN, J. M. VULULE, B. L. NAHLEN, R. W. SAUERWEIN, and F. O. TER KUILE PREVALENCE AND SEVERITY OF MALNUTRITION IN PRE-SCHOOL CHILDREN IN A RURAL AREA OF WESTERN KENYA Am J Trop Med Hyg, April 1, 2003; 68(90040): 94 - 99. [Abstract] [Full Text] [PDF]

				F. O. TER KUILE, D. J. TERLOUW, P. A. PHILLIPS-HOWARD, W. A. HAWLEY, J. F. FRIEDMAN, M. S. KOLCZAK, S. K. KARIUKI, Y. P. SHI, A. M. KWENA, J. M. VULULE, et al. IMPACT OF PERMETHRIN-TREATED BED NETS ON MALARIA AND ALL-CAUSE MORBIDITY IN YOUNG CHILDREN IN AN AREA OF INTENSE PERENNIAL MALARIA TRANSMISSION IN WESTERN KENYA: CROSS-SECTIONAL SURVEY Am J Trop Med Hyg, April 1, 2003; 68(90040): 100 - 107. [Abstract] [Full Text] [PDF]

				S. K. KARIUKI, A. A. LAL, D. J. TERLOUW, F. O. TER KUILE, J. M. O. ONG'ECHA, P. A. PHILLIPS-HOWARD, A. S. S. ORAGO, M. S. KOLCZAK, W. A. HAWLEY, B. L. NAHLEN, et al. EFFECTS OF PERMETHRIN-TREATED BED NETS ON IMMUNITY TO MALARIA IN WESTERN KENYA II. ANTIBODY RESPONSES IN YOUNG CHILDREN IN AN AREA OF INTENSE MALARIA TRANSMISSION Am J Trop Med Hyg, April 1, 2003; 68(90040): 108 - 114. [Abstract] [Full Text] [PDF]

				W. A. HAWLEY, F. O. TER KUILE, R. S. STEKETEE, B. L. NAHLEN, D. J. TERLOUW, J. E. GIMNIG, Y. P. SHI, J. M. VULULE, J. A. ALAII, A. W. HIGHTOWER, et al. IMPLICATIONS OF THE WESTERN KENYA PERMETHRIN-TREATED BED NET STUDY FOR POLICY, PROGRAM IMPLEMENTATION, AND FUTURE RESEARCH Am J Trop Med Hyg, April 1, 2003; 68(90040): 168 - 173. [Abstract] [Full Text] [PDF]

This Article Abstract Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Citation Map Services Similar articles in this journal Similar articles in Web of Science Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Web of Science (42) Citing Articles via Google Scholar Google Scholar Articles by TER KUILE, F. O. Articles by NAHLEN, B. L. Search for Related Content PubMed PubMed Citation Articles by TER KUILE, F. O. Articles by NAHLEN, B. L. Related Collections Health Outcomes Malaria Medical Entomology