Malaria in Pregnancy
Malaria in Pregnancy
Malaria in Pregnancy
Objectives
At the end of the session each participant should: Explain why pregnancy is a risk factor in malaria Describe presentation of malaria in pregnancy Describe the management of malaria in pregnancy Describe severe malaria in pregnancy and its management Explain what is IPT and describe the role of prophylaxis Describe the importance of malaria in neonates Describe clinical features of malaria in neonates Describe management of Neonatal Malaria Describe management of malaria in infants below 5 Kg
During pregnancy the naturally acquired partial immunity to malaria declines. The decline in immunity is most pronounced during the first and second pregnancy. The reasons for the decline in immunity is yet undetermined.
Malaria is an important cause of morbidity and mortality for the pregnant woman, the foetus and the newborn. The effects of malaria in pregnancy are related to the malaria endemicity, with abortion more common in areas of low endemicity and intrauterine growth retardation more common in areas of high endemicity.
Effects of malaria on morbidity and mortality among pregnant woman, foetus and newborn
Pregnant Woman Foetus Newborn
Anaemia
Morbidity
Premature labour Hypoglycaemia Severe malaria (*) Abortion Stillbirth Congenital malaria
Mortality
Severe anaemia
The clinical presentation of malaria during pregnancy is often hidden. Some pregnant women will present with the typical features of uncomplicated and/or severe malaria However in others, anaemia may be the only recognizable clinical feature.
During history taking and physical examination elicit signs and symptoms of severe malaria. Whenever malaria is suspected, laboratory confirmation of malaria parasites should be performed if possible. If laboratory facilities are not available, treatment should be started on the basis of clinical presentation. If a laboratory is present, a negative result does not rule out malaria. RDTs have an added value, as they can be positive even if parasites are hidden in the placenta. Oral quinine is the drug of choice for treatment of uncomplicated malaria in pregnancy. Presently, Artemisinin derivatives cannot be recommended for treatment of malaria in the first trimester of pregnancy. However, they should not be withheld if treatment is considered to be life saving for the mother and other antimalarial are considered to be unsuitable.
Pregnant women infected with malaria are more susceptible to develop severe malaria. They commonly present with the following features: high fever hyperparasitemia low blood sugar severe haemolytic anaemia cerebral malaria pulmonary oedema
The drug of choice for treatment of severe malaria is intravenous quinine. Blood smear for malaria parasites should be taken daily until negative. Review adequacy of antimalarial dosage. Consider alternative or give additional drug if parasitaemia and/or clinical signs persist The risk of quinine induced hypoglycaemia is greater in pregnant than non-pregnant women. While the patient is on IV Quinine treatment, pay particular attention to the feeding of the patient.
Perform appropriate investigations (BS, peripheral blood film, stool examination, RBC indices, urinalysis) Treat the cause of anaemia if determined Give the following drugs
Full course of oral quinine Iron: Give orally 200mg ferrous sulphate three times a day Folic Acid 5 mg daily Antihelminthics (e.g. mebendazole from second trimester) Treat schistosomiasis if the patient lives in areas with high shistosomiasis transmission (after delivery)
Clinical response Hb measurement weekly Reticulocyte count
Severe anaemia has to be aggressively treated before the woman goes into labour. Before 36 weeks of gestational age if the patient is not in cardiac failure the treatment should be as for the moderate anaemia If in failure and after 36 weeks of gestational age with or without failure: Treat the cause if determined Give blood transfusion (preferably packed cells) Continue with iron and folic acid up to 3 months after delivery Follow up the patient every 7 days until Hb is normal
Prevention of anaemia
Antenatal Clinic Combined ferrous sulphate + folic acid (FeFo) once or twice daily Intermittent Preventive Treatment in the second and third trimester Early detection of anaemia Hb screening Symptom sign surveillance De-worming as indicated in the focused antenatal care (FANC) Treat any underlying infection All women should be advised on appropriate diet during pregnancy and on personal malaria protection using insecticide treated nets (ITN).
Controlling the effects of malaria infection on the pregnant woman and the foetus requires a balanced programme of effective case management of malaria illness and prevention of the consequences of asymptomatic infection. Evidence based effective preventive interventions are required. These interventions consist of intermittent preventive treatment and use of insecticide treated nets.
The drug of choice for IPT is SP. SP remains the drug of choice for IPT even though it is no longer the first line drug for malaria treatment. This is because the aim of IPT is to prevent the worst effects of malaria infection in pregnancy rather than to cure a potentially life-threatening illness. The first IPT dose is administered between 20-24 weeks of gestational age. The second IPT dose should be administered at 28-32 weeks. IPT should be administered as direct observed treatment (DOT) during an antenatal care visit If malaria is diagnosed after administration of IPT with SP a full treatment with antimalarials should be given Pregnant women who are known to have hypersensitivity to sulfonamides should not receive SP for IPT. Neither Quinine, nor ALu should be used for IPT.
Pregnant women should be advised to sleep under Insecticide Treated Nets (ITNs) at night and to take other personal protective measures to reduce contact with mosquitoes Mothers should be encouraged to protect their newborn infants with Insecticide Treated Nets (ITNs)
IMalaria in the neonate (first four weeks of life) is very rare: in Muhimbili Neonatal Unit the incidence of congenital malaria in hospitalised newborn is 3/100,000. Congenital or acquired malaria in this age group is life threatening and requires immediate treatment.
Malaria is quite uncommon in infants below 2 months of age. Since Artemether-lumefantrine is currently not recommended for infants below 5 Kg, quinine is the drug of choice in this category.