Intermittent screening and treatment with artemether–lumefantrine versus intermittent preventive treatment with sulfadoxine–pyrimethamine for malaria in pregnancy: a facility-based, open-label, non-inferiority trial in Nigeria

Jul 7, 2018Malaria journal

Comparing intermittent malaria testing and treatment with artemether-lumefantrine to preventive treatment with sulfadoxine-pyrimethamine during pregnancy in Nigeria

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Abstract

The risk of third-trimester maternal parasitaemia was significantly lower by 3.96% with intermittent screening and treatment compared to the standard IPTp-SP.

  • Severe anaemia prevalence was 0.8% and moderate anaemia was 27.7% in the third trimester, with no significant difference between treatment groups.
  • The risk of third-trimester severe anaemia did not differ significantly between the two treatment arms, indicating similar anaemia outcomes.
  • ISTp-AL resulted in a significantly lower risk of low birthweight after adjusting for factors like maternal age and baseline parasitaemia.
  • Women receiving ISTp-AL reported fever more frequently compared to those receiving IPTp-SP.

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Key numbers

-1.75%
Risk Difference for Severe Anaemia
Comparison of severe anaemia prevalence between treatment groups.
-3.96%
Risk Difference for Maternal Parasitaemia
Comparison of parasitaemia risk in third trimester between treatment groups.
-1.53%
Risk Difference for Low Birth Weight
Comparison of low birth weight prevalence adjusted for maternal factors.

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What this is

  • This trial compared intermittent screening and treatment with artemether-lumefantrine (ISTp-AL) to standard intermittent preventive treatment with sulfadoxine-pyrimethamine (IPTp-SP) for malaria in pregnant women.
  • Conducted in Nigeria, it involved 459 women randomized to either treatment approach.
  • The study aimed to evaluate the effectiveness and safety of ISTp-AL in preventing maternal anaemia and low birth weight.

Essence

  • ISTp-AL was found to be non-inferior to IPTp-SP in preventing severe maternal anaemia in pregnant women. Additionally, ISTp-AL significantly reduced the risk of maternal parasitaemia and low birth weight.

Key takeaways

  • The risk of third-trimester severe anaemia (Hb < 8 g/dl) did not differ significantly between ISTp-AL and IPTp-SP, with a risk difference of -1.75%. This indicates that ISTp-AL is an effective alternative for preventing severe anaemia.
  • ISTp-AL resulted in a significantly lower risk of maternal parasitaemia compared to IPTp-SP, with a risk difference of -3.96%. This suggests that ISTp-AL may be more effective in controlling malaria infections during pregnancy.
  • The risk of low birth weight was significantly lower in the ISTp-AL group after adjusting for maternal factors, with a risk difference of -1.53%. This finding supports the potential benefits of ISTp-AL for fetal health.

Caveats

  • The analysis for third-trimester anaemia was underpowered due to a high loss to follow-up (8.5%), which may affect the reliability of the findings.
  • Potential biases may exist due to the open-label design of the trial, which could influence participant reporting of outcomes.
  • The cost of ISTp-AL may be higher than IPTp-SP, raising concerns about the feasibility of widespread implementation in resource-limited settings.

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