Background
In sub-Saharan Africa,
Plasmodium falciparum infection increases the risk of maternal anaemia and low birthweight, and prematurity in women and their neonates, respectively [
1,
2]. It was estimated that without pregnancy-specific interventions, 9·5 million pregnant women were exposed to infection in 2010, leading to 750,000 low birthweight deliveries. Recommended malaria prophylactic treatment was estimated to prevent 128,000 low birthweight deliveries by 2015 [
3]. Despite recent decline in malaria transmission in Africa, the burden of malaria in pregnancy (MiP) in the absence of adequate prevention remains substantial [
3]. In geographical areas with high transmission, the impact of malaria on maternal health depends on age, gravidity, trimester of pregnancy, coinfection [
1,
4] nutritional status [
5] the intensity of malaria transmission (increased in rural populations), season, and use of malaria prevention [
6].
In most African countries, SP remains the recommended drug for IPTp. SP provides intermittent clearance or suppression of existing asymptomatic infections from the placenta (the treatment effect) and may prevent new infections from occurring for several weeks by maintenance of suppressive drug levels (the post-treatment prophylactic effect) [
7]. Based on the findings of multi-centre trials on the evaluation of IPTp-SP, three or more doses of IPTp-SP were associated with less placental malaria, higher mean birth weight and fewer LBW births compared with two doses [
8]. Thus, the WHO policy on IPTp-SP was revised and recommends uptake of at least three SP doses with each dose administered at each scheduled antenatal care visit, at least 1 month apart up to the time of delivery and ideally by direct observed therapy [
9]. Although there has been a fivefold increase in the percentage of women receiving the recommended three or more doses of IPTp in 20 African countries, coverage in Cameroon remains low (29%) [
10].
The effectiveness of IPTp-SP is threatened by rising levels of parasite resistance to SP in several countries across Africa [
11]. Emergence and successive acquisition of polymorphisms in both the
P. falciparum dihydrofolate reductase/dihydropteroate synthetase (
pfdhfr/pfdhps) genes are associated with a high-level of SP resistance and clinical treatment failure in several epidemiological settings. Parasites harbouring the K540E mutation, which is a proxy for the
pfdhfr‐
pfdhps quintuple mutant is strongly linked with resistance rendering SP ineffective to clear
P. falciparum infections [
12]. Sextuple mutant parasites (quintuple mutant plus the additional
pfdhps A581G mutation) defined as super-resistant parasites [
13] have been associated with a loss of IPTp-SP efficacy [
14‐
18]. Although resistance to SP reduces the parasitological efficacy of IPTp, beneficial associations between the use of IPTp-SP and low birthweight are still seen in areas where prevalence of parasites with quintuple mutations is > 90% [
11,
12,
17]. IPTp-SP appears to protect against malaria as well as other non-malarial causes of LBW such as sexually transmitted and reproductive tract infections (STIs/RTIs). SP may exert its protection through antibacterial or anti-inflammatory actions [
19,
20].
The wide spread of SP super-resistance in Africa is expected with continued SP use and may undermined anti-malarial policies [
17]. In Yaoundé, Cameroon, highly resistant parasites (octuple mutation genes) to SP have been isolated from pregnant women with symptomatic
P. falciparum infection [
21]. Also, a high prevalence of
P. falciparum SP resistant parasites among pregnant [
22] and non-pregnant [
23,
24] populations has been reported along the slope of Mount Cameroon. On this basis, continuous monitoring and evaluation of SP efficacy in Cameroon is crucial. Thus, this study determined the coverage of IPTp-SP since the transition from a 2-dose to 3-dose IPTp-SP policy in Cameroon in 2012. Secondly, the study ascertained whether 3 or more doses of SP to the 2-dose regimen for intermittent preventive therapy during pregnancy provide any additional benefits in reducing the risk of PM infection and LBW in some selected semi-rural and semi-urban settings in Mount Cameroon area, South West Region, Cameroon.
Methods
Ethics statement
The study was approved by the Institutional Review Board of the University of Buea (Ref No: 2016/0351/UB/FHS/IRB), whereas administrative authorization was obtained from the South West Regional Delegation of Public Health. Written informed consent was obtained from all the study participants.
Study area
The study was conducted at the maternity units in four selected medical facilities (Mutengene Medical Centre (MMC), Bolifamba Health Centre (BHC), Buea, Government integrated health centre Munyenge (MIHC), and Muyuka District hospital (MDH) located on the eastern slope of Mount Cameroon from November 2016 to December 2017. The localities of these antenatal clinics were selected based on the level of malaria transmission intensity; semi-rural (Munyenge and Bolifamba and semi-urban (Muyuka and Mutengene) settings. Munyenge is a semi-rural setting, endemic for urogenital schistosomiasis and located about 27 km from Muyuka, a semi-urban town in the Mount Cameroon area. Muyuka is found at a lower altitude of 87 m above sea level (asl), while that of Munyenge ranges from 87 to 168 m (asl). Both areas have a temperature and average annual rainfall of 24–27 °C and 3126 mm, respectively. These localities are both characterized by a heterogenous population and intensive farming [
25]. Mutengene is a semi-urban road-junction town with a highly heterogenous population located at 197 m (asl). Mutengene is characterized by mean temperature of 25 °C, mean relative humidity of 83% (Cameroon Development Corporation (CDC) weather record). Bolifamba is semi-rural community in Buea located at 530 m asl. Buea has a mean relative humidity of 80%, average rainfall of 4000 mm and a temperature range of 18–27 °C [
26]. All medical facilities selected for the study are government-owned institutions that offer antenatal care, preventive, curative and delivery services at affordable costs and are highly accessible facilitating utilization of ANC services [
27].
In the Mount Cameroon area, malaria parasite transmission is perennial [
28]. Pregnant women living in rural areas are highly exposed to malaria parasitaemia (39.2%) [
29] than those from semi-urban/urban communities (13.4–22.4%) [
30,
31]. Placental malaria in pregnancy in the Mount Cameroon area is most sensitively diagnosed by placental histology compared with placental blood smear microscopy. But placental microscopic infection has epidemiological and clinical significance than low submicroscopic parasitaemia diagnosed by placenta histology only [
32]. Cameroon transitioned from a 2-dose to a 3-dose recommendation for IPTp-SP in 2012 [
33]. Monitoring studies on the coverage and usage of lPTp-SP and ITN (insecticide-treated nets) in pregnancy in the study area showed that the proportion of women who receive at least two or more doses of IPTp- SP (64%) has increased over the years [
30,
34] but levels remain below recommended target (80–100%). Also, recent findings confirm the additional benefits of repeated doses of SP in combination with ITN use in reducing peripheral malaria parasitaemia and maternal anaemia [
30].
Study design and population
Consenting pregnant women were enrolled consecutively through a cross-sectional survey at delivery in health facilities. Enrolment by the time of delivery ensured uptake of adequate doses of IPTp-SP (at least three doses of SP) as stipulated by the World Health Organization (WHO) [
35]. Mothers with evidence of complicated pregnancy (including hypertension, preeclampsia, diabetes and twin births) were not eligible for the study. An interview-guided administered questionnaire was used to obtain information relating to demographic data (age, residence) antenatal clinic data (gestational age, parity and number of antenatal care visits), fever history and ITN usage the night prior to the survey. The use of IPTp-SP and number of doses as well as new-born birth weights were documented and verified by checking ANC cards, patient’s medical record book and health centre maternal care register. Axial body temperature was measured using a digital thermometer to determine fever. Evidence of any chronic illness such as HIV/AIDS was noted.
Sample collection
A maternal finger-prick blood sample was collected before delivery for haemoglobin (Hb) measurement. After the delivery of the placenta, a small piece of tissue (0.5 cm
2) from a healthy paracentric area (approximately a quarter of the distance from the centre of the placenta) was excised to prepare impression smears for detection of PM infection [
32]. All samples were transported on ice bath to the Malaria Research Laboratory, University of Buea for analysis.
Sample processing and analysis
Haematological analysis
Haemoglobin concentration was determined using a haemoglobinometer (HemoCue, Angelholm, Sweden). Maternal anaemia was defined as a haemoglobin level of < 11 g/dL [
36]. Anaemia severity was defined as follows: mild anaemia (Hb: 10–10.9 g/dL), moderate anaemia (Hb: 7–9.9 g/dL), and severe anaemia (Hb < 7.0 g/dL) [
36].
Placental malaria parasitaemia determination
Thin impression smears of placental blood were prepared and stained with 10% Giemsa (Sigma-Aldrich, St. Louis, MO), as described previously [
32]. The malaria parasitaemia status (the presence of any malaria parasite stages; trophozoites, schizonts) and density were determined under oil immersion with the 100× objective of a binocular Olympus microscope. Blood smears were considered negative if no parasites and/or pigment in macrophages were found after counting 100 high-power fields. To determine the percentage of malaria parasitization in the placenta, malaria parasite-infected red cells were counted against 1000 erythrocytes. All slides were read by 2 independent microscopists blinded to each other’s results. In case of discordant findings, a third reader was used.
Outcome variables
The primary study outcomes were placental malaria infection and birth weight. Secondary outcomes included maternal haemoglobin levels and anaemia.
Definitions
1.
Placental malaria infection was defined as detection by microscopy of P. falciparum asexual stages, any density and/or haemozoin in macrophages.
2.
Low birth weight was defined as a birth weight < 2500 g.
3.
Anaemia was defined as haemoglobin concentration < 11 g/dL.
4.
Coverage of IPTp-SP was defined as uptake of SP (doses) by the time of delivery.
5.
Febrile status was defined as body temperature greater than 37.5 °C.
6.
Placental malaria parasite density was expressed as percentage of parasitization.
Independent variables
Demographics included setting (semi-rural and semi-urban), maternal age (< 21, 21–25, > 25 years), parity status (primiparae, secundiparae, multiparae) and ITN usage. Semi -rural areas (Munyenge and Bolifamba) are geographic areas located outside semi-urban towns of Muyuka and Buea, respectively.
Data analysis
All data were entered, validated and analysed using SPSS Statistics 20 (SPSS Inc., Chicago, IL). The significance of differences in proportions were explored using the Pearson’s Chi square test, whereas the differences in group means were assessed using Student t test, analysis of variance (ANOVA). Association analysis of number of SP doses, PM infection and LBW was undertaken by multinominal logistic regression. Maternal age, parity, setting, ANC attendance, ITN usage were included in the model as possible confounders. For multivariate models, the variables were selected based on statistical significance in the univariate models (p < 0.2), explanatory plausibility and collinearity considerations. Percentage change in crude odd ratios of confounders associated with risk of PM and LBW were calculated. Missing data are presented in the tables, but data points were generally complete. A p value < 0.05 was considered statistically significant.
Sample size determination
The sample size was calculated using the formula n = Z
2pq/d
2 [
35] where n = the sample size required, z = 1.96: confidence level test statistic at the desired level of significance, p = 15%: proportion of placental blood malaria parasitaemia at delivery [
37], q = 1 − p: proportion of malaria parasite negative and d = acceptable error willing to be committed. N = (1.96)
2 × 0.15 (1 − 0.15)/(0.05)
2 = 195.9. The minimum estimated sample size calculated per setting was 196. For statistical power, 238 and 227 consented participants from semi-rural and semi-urban areas were enrolled into the study.
Discussion
This study reports on the coverage of SP (doses) in the Mount Cameroon area since the transition from a 2-dose to 3-dose IPTp-SP policy in Cameroon in 2012. Given that the effectiveness of this strategy is being challenged by rising levels of parasite resistance, this study provide evidence on the extent at which ≥ 3 doses of SP compared with the 2-dose IPTp-SP regimen is effective against PM infection and LBW in the study area.
This study revealed an increased in the percentage of women receiving the recommended three or more doses of IPTp in the area consistent with World Malaria Report 2016 [
38]. About two (47.0%) out of five women received the full WHO-recommended schedule which is higher than 29.3% from the National Demographic Health Survey (DHS) data collected in 2011 in Cameroon [
10]. An overall prevalence of 29.5% for three doses of IPTp-SP was obtained from Malaria Indicator Surveys (MIS) conducted in Burkina Faso, Ghana, Mali, Malawi, Kenya, Nigeria, Sierra Leone, and Uganda with considerable inter- and intra-country variations in the adequate uptake of IPTp [
39].
Comparatively, the coverage of IPTp (≥ 3) in the Mount Cameroon area appears to be better than in many other countries in sub-Saharan Africa, except for Ghana where a higher coverage of 60% has been reported [
40]. Ten years after implementation of IPTp- SP in Cameroon, coverage with at least two doses in this part of the country has increased from 64.7% in 2009 [
34] to 81.7% in 2017 as stipulated by the WHO previous policy on IPTp-SP [
41]. Most women who did not take chemoprophylaxis during their pregnancy were from semi-rural setting, however the coverage of the IPTp-SP doses and ITN usage were similar in both semi-rural and urban areas. This observation highlights the positive contribution of malaria control programmes towards bridging disparities and inequities in accessing malaria health services between rural and urban women [
10,
42]. Access to chemoprophylaxis and ITNs among pregnant women have become more equitable in Cameroon due to provision of IPTp-SP free of charge and affordable essential drug schemes which lower costs [
10].
In conformity with reports of several studies, ANC initiation in the first trimester or earlier in the second trimester as well as frequent ANC visits made before delivery allowed for more SP doses to be taken [
34,
43,
44]. Uptake of ≥ 3 doses was also associated with type of health care facility where MDH had the highest coverage (72%). In Cameroon, the health district is the implementer unit of the health system and thus it not uncommon for the availability of SP at MDH to form the basis for high IPTp-SP coverage among pregnant women attending ANC in this facility. The relatively low uptake of SP at the level of the health centres may be due to unavailability of SP as a result of stock outs. During stock outs, IPTp is suspended until stocks are replenished or women are asked to buy SP from local drug vendors. Stock outs may be related to drug shortage at the central unit or challenges in supply chain management programs [
45]. Periodic shortage of SP in rural health facilities has been reported as a major barrier to the implementation of IPTp-SP programme in some malaria endemic countries [
46,
47].
Earlier studies of IPTp in Cameroon demonstrated a clear reduction in placental parasitaemia following receipt of SP [
32,
48]. Also, data from a meta-analysis showed that ≥ 3 doses was associated with less placental malaria [
8]. Contrarily, our study did not show prophylactic effectiveness of IPTp-SP in reducing PM infection. The risk of placental parasitaemia increased by 42% among delivery women having taken ≥ 3 doses. Although, PM parasitaemia was generally scarce as reported in previous studies [
32], increase parasite load was noted mainly among women from urban areas who had adequate SP doses. The ineffectiveness of IPTp-SP on PM infection was noteworthy among primiparae. It is well known that in areas of intense transmission, primigravidae have higher vulnerability to malaria infection and its adverse consequences [
1]. Thus, the effect of IPTp-SP against malaria should be more profound in these individuals than in secundi- and multigravidae as suggested by Valea et al. [
49]. The lack of prophylactic effect of IPTp-SP in the prevention of malaria parasitaemia observed may be due to the presence of highly drug resistant
P. falciparum parasites among infected pregnant women in south-western Cameroon. Agbor and Apinjoh [
22] provide evidence of a high prevalence (51.1%) of
pfdhps A581G mutation among pregnant women along the slope of mount Cameroon. Also, Chauvin et al. [
21] reported
pfdhfr/pfdhps octuple mutant alleles with A581G and A613S mutations among parasites isolated from pregnant women with symptomatic
P. falciparum infection in Yaoundé, Cameroon. Although
pfdhps K540E mutation was not observed in the study area [
22], its presence, though rare, was confirmed in studies in Yaoundé [
21]. In several countries in East Africa, SP resistance linked to vast predominance of highly resistant strains of
pfdhps 540E and
pfdhps 581G mutations in these populations has been associated with in vivo therapeutic failure to SP [
11,
14‐
18,
50,
51]. IPTp use in areas with 581G mutation facilitate increase in parasite density whereby these highly resistant parasites out-compete the wild type populations and overgrow under drug pressure [
14]. This may partly explain the increase placenta parasite load seen among women especially those from high IPTp-SP coverage areas, such as Muyuka. In line with reports from Benin by Moussiliou et al. [
52], which highlight the inability of SP to ensure optimal antiplasmodial protection in late pregnancy, these present findings further suggest that SP is potentially failing in Central-West Africa. Future studies in the mount Cameroon area to link SP drug resistance molecular markers and efficacy of IPTp-SP are crucial taking into consideration the WHO recommendation to discontinue IPTp-SP in areas with A581G mutation > 10% [
53].
Although ineffective in reducing PM infection, IPTp-SP showed improvement of infant outcomes in the area. Chemoprophylaxis with IPTp –SP (≥ 3 doses) was associated with reduced odds of LBW by 22%. From this study, the association between timing of ANC initiation and dosage frequency suggests that earlier dosing reduces odds of PM infection and thus improves birth weight outcome than late dosing which is linked to late antenatal enrolment. Comparable with reports from Burkina Faso [
49], increased number of doses from 2 to ≥ 3 doses did not confer additional protection from LBW nor significantly increase birth weight. Gutman et al. [
50] suggested that under conditions of resistance, more doses would be required to achieve the same benefit seen with only 2 doses in areas without resistance. SP resistance increases the minimum inhibitory concentration, leading to a shorter duration of prophylaxis. Interestingly, particularly among primiparae, adequate doses of SP was seen associated with improved birth weight outcome despite evidence of no parasitological response in clearance of placental infection. This is consistent with extensive reports on beneficial associations between the use of IPTp-SP and low birthweight still seen in areas where the efficacy of SP to clear parasitaemia has clearly decreased [
11,
12]. Besides its anti-malarial activity, IPTp-SP appears to confer benefit through yet undefined pathways [
19,
20,
54]. Sulfadoxine is a broad-spectrum antibiotic that possibly exerts an inhibitory effect against non-malaria causes of LBW and preterm birth [
55]. Its antibacterial activity can lead to maternal and infant weight gain through changes in gut and vagina bacteria flora associated with indirect metabolic benefits and reduction in the impact of urogenital tract infections [
56,
57], respectively. SP exposure inhibits (immunomodulatory role) maternal inflammatory responses to infections that are known to trigger preterm delivery [
58].
Limitations
This study has some limitations. These data were collected from a cross-sectional delivery survey. Although the effects of potential confounders have been corrected by using appropriate statistical methods, as in any observational study, unmeasured confounders, such as socioeconomic data may have had reasonable influence on the observations reported. Although SP was given as directly observed treatment (DOT) to ensure that pregnant women take the full dose, assessment of the reliability of IPTp-SP uptake is by evaluating the presence of measurable sulfa in maternal plasma during pregnancy. HIV screening is routinely undertaken during antenatal clinic visit, but the HIV status was not available for all study participants enrolled. However, the overall prevalence of HIV infection in the present study area was 4.6%. Despite these limitations, the data presented provide useful information on the coverage and effectiveness of IPTp-SP in the context increasing SP resistance parasite strains in the Mount Cameroon area.
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