Estimated risk of placental infection and low birthweight attributable to Plasmodium falciparum malaria in Africa in 2010: a modelling study

Patrick G.T. Walker; Feiko Ter Kuile; Tini Garske; Clara Menendez; Azra C. Ghani

doi:10.1016/s2214-109x(14)70256-6

Estimated risk of placental infection and low birthweight attributable to Plasmodium falciparum malaria in Africa in 2010: a modelling study

Patrick G.T. Walker
, Feiko Ter Kuile
, Tini Garske
, Clara Menendez
, Azra C. Ghani

Clinical Sciences

Imperial College London
Wellcome Trust Research Laboratories Nairobi
University of Barcelona
Centro de investigação de Saúde de Manhiça

Research output: Contribution to journal › Article › peer-review

117 Citations (Scopus)

Abstract

Background

Plasmodium falciparum infection during pregnancy leads to adverse outcomes including low birthweight; however, contemporary estimates of the potential burden of malaria in pregnancy in Africa (in the absence of interventions) are poor. We aimed to estimate the need to protect pregnant women from malaria across Africa.

Methods

Using a mathematical model applied to estimates of the geographical distribution of P falciparum across Africa in 2010, we estimated the number of pregnant women who would have been exposed to infection that year in the absence of pregnancy-specific intervention. We then used estimates of the parity-dependent acquisition of immunity to placental infection and associated risk of low birthweight to estimate the number of women who would have been affected.

Findings

We estimate that, without pregnancy-specific protection, 12·4 million pregnant women (44·9% of all 27·6 million livebirths in malaria endemic areas in Africa in 2010) would have been exposed to infection, with 11·4 million having placental infection (41·2% of all livebirths). This infection leads to an estimated 900 000 (95% credible interval [CrI] 530 000—1 240 000) low birthweight deliveries per year. Around the end of the first trimester, when the placenta becomes susceptible to infection, is a key period during which we estimate that 65·2% (95% CrI 60·9—70·0) of placental infections first occur.

Interpretation

Our calculations are the only contemporary estimates of the geographical distribution of placental infection and associated low birthweight. The risk of placental infection across Africa in unprotected women is high. Prevention of malaria before conception or very early in pregnancy is predicted to greatly reduce incidence of low birthweight, especially in primigravidae. The underlying lifetime risk of low birthweight changes slowly with decreasing transmission, drawing attention to the need to maintain protection as transmission falls.

Original language	English
Pages (from-to)	e460-e467
Journal	The Lancet Global Health
Volume	2
Issue number	8
DOIs	https://doi.org/10.1016/s2214-109x(14)70256-6
Publication status	Published - 1 Aug 2014

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Access to Document

10.1016/s2214-109x(14)70256-6Licence: CC BY

Lancet Glob Heal 2 8 e460-e467Final published version, 3.02 MBLicence: CC BY

Cite this

@article{70d68527a8574582848d4844468ab104,

title = "Estimated risk of placental infection and low birthweight attributable to Plasmodium falciparum malaria in Africa in 2010: a modelling study",

abstract = "BackgroundPlasmodium falciparum infection during pregnancy leads to adverse outcomes including low birthweight; however, contemporary estimates of the potential burden of malaria in pregnancy in Africa (in the absence of interventions) are poor. We aimed to estimate the need to protect pregnant women from malaria across Africa.MethodsUsing a mathematical model applied to estimates of the geographical distribution of P falciparum across Africa in 2010, we estimated the number of pregnant women who would have been exposed to infection that year in the absence of pregnancy-specific intervention. We then used estimates of the parity-dependent acquisition of immunity to placental infection and associated risk of low birthweight to estimate the number of women who would have been affected.FindingsWe estimate that, without pregnancy-specific protection, 12·4 million pregnant women (44·9\% of all 27·6 million livebirths in malaria endemic areas in Africa in 2010) would have been exposed to infection, with 11·4 million having placental infection (41·2\% of all livebirths). This infection leads to an estimated 900 000 (95\% credible interval [CrI] 530 000—1 240 000) low birthweight deliveries per year. Around the end of the first trimester, when the placenta becomes susceptible to infection, is a key period during which we estimate that 65·2\% (95\% CrI 60·9—70·0) of placental infections first occur.InterpretationOur calculations are the only contemporary estimates of the geographical distribution of placental infection and associated low birthweight. The risk of placental infection across Africa in unprotected women is high. Prevention of malaria before conception or very early in pregnancy is predicted to greatly reduce incidence of low birthweight, especially in primigravidae. The underlying lifetime risk of low birthweight changes slowly with decreasing transmission, drawing attention to the need to maintain protection as transmission falls.",

author = "Walker, \{Patrick G.T.\} and \{Ter Kuile\}, Feiko and Tini Garske and Clara Menendez and Ghani, \{Azra C.\}",

year = "2014",

month = aug,

day = "1",

doi = "10.1016/s2214-109x(14)70256-6",

language = "English",

volume = "2",

pages = "e460--e467",

journal = "The Lancet Global Health",

issn = "2572-116X",

publisher = "Elsevier Ltd",

number = "8",

}

TY - JOUR

T1 - Estimated risk of placental infection and low birthweight attributable to Plasmodium falciparum malaria in Africa in 2010: a modelling study

AU - Walker, Patrick G.T.

AU - Ter Kuile, Feiko

AU - Garske, Tini

AU - Menendez, Clara

AU - Ghani, Azra C.

PY - 2014/8/1

Y1 - 2014/8/1

N2 - BackgroundPlasmodium falciparum infection during pregnancy leads to adverse outcomes including low birthweight; however, contemporary estimates of the potential burden of malaria in pregnancy in Africa (in the absence of interventions) are poor. We aimed to estimate the need to protect pregnant women from malaria across Africa.MethodsUsing a mathematical model applied to estimates of the geographical distribution of P falciparum across Africa in 2010, we estimated the number of pregnant women who would have been exposed to infection that year in the absence of pregnancy-specific intervention. We then used estimates of the parity-dependent acquisition of immunity to placental infection and associated risk of low birthweight to estimate the number of women who would have been affected.FindingsWe estimate that, without pregnancy-specific protection, 12·4 million pregnant women (44·9% of all 27·6 million livebirths in malaria endemic areas in Africa in 2010) would have been exposed to infection, with 11·4 million having placental infection (41·2% of all livebirths). This infection leads to an estimated 900 000 (95% credible interval [CrI] 530 000—1 240 000) low birthweight deliveries per year. Around the end of the first trimester, when the placenta becomes susceptible to infection, is a key period during which we estimate that 65·2% (95% CrI 60·9—70·0) of placental infections first occur.InterpretationOur calculations are the only contemporary estimates of the geographical distribution of placental infection and associated low birthweight. The risk of placental infection across Africa in unprotected women is high. Prevention of malaria before conception or very early in pregnancy is predicted to greatly reduce incidence of low birthweight, especially in primigravidae. The underlying lifetime risk of low birthweight changes slowly with decreasing transmission, drawing attention to the need to maintain protection as transmission falls.

AB - BackgroundPlasmodium falciparum infection during pregnancy leads to adverse outcomes including low birthweight; however, contemporary estimates of the potential burden of malaria in pregnancy in Africa (in the absence of interventions) are poor. We aimed to estimate the need to protect pregnant women from malaria across Africa.MethodsUsing a mathematical model applied to estimates of the geographical distribution of P falciparum across Africa in 2010, we estimated the number of pregnant women who would have been exposed to infection that year in the absence of pregnancy-specific intervention. We then used estimates of the parity-dependent acquisition of immunity to placental infection and associated risk of low birthweight to estimate the number of women who would have been affected.FindingsWe estimate that, without pregnancy-specific protection, 12·4 million pregnant women (44·9% of all 27·6 million livebirths in malaria endemic areas in Africa in 2010) would have been exposed to infection, with 11·4 million having placental infection (41·2% of all livebirths). This infection leads to an estimated 900 000 (95% credible interval [CrI] 530 000—1 240 000) low birthweight deliveries per year. Around the end of the first trimester, when the placenta becomes susceptible to infection, is a key period during which we estimate that 65·2% (95% CrI 60·9—70·0) of placental infections first occur.InterpretationOur calculations are the only contemporary estimates of the geographical distribution of placental infection and associated low birthweight. The risk of placental infection across Africa in unprotected women is high. Prevention of malaria before conception or very early in pregnancy is predicted to greatly reduce incidence of low birthweight, especially in primigravidae. The underlying lifetime risk of low birthweight changes slowly with decreasing transmission, drawing attention to the need to maintain protection as transmission falls.

U2 - 10.1016/s2214-109x(14)70256-6

DO - 10.1016/s2214-109x(14)70256-6

M3 - Article

SN - 2572-116X

VL - 2

SP - e460-e467

JO - The Lancet Global Health

JF - The Lancet Global Health

IS - 8

ER -

Estimated risk of placental infection and low birthweight attributable to Plasmodium falciparum malaria in Africa in 2010: a modelling study

Abstract

UN SDGs

Access to Document

Fingerprint

Cite this