1) Malaria remains a major global health problem, with an estimated 247 million cases and 619,000 deaths in 2021.
2) Diagnosis of malaria relies on microscopy or rapid diagnostic tests (RDTs) to confirm the presence of the parasite. Treatment of uncomplicated P. falciparum malaria involves artemisinin-based combination therapy (ACT).
3) Prevention efforts include intermittent preventive treatment for pregnant women and high-risk groups, seasonal malaria chemoprevention for children, and—for the first time—the RTS,S/AS01 malaria vaccine which has been recommended by WHO for use in children living in moderate to high transmission areas.
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Malaria.pptx
1. AN UPDATE ON MALARIA
Dr A P Naveen Kumar
DNB FICP
Chief Specialist – General
Medicine
Visakha Steel General Hospital
2. EPIDEMIOLOGY
Malaria continues to cause unacceptably high levels of disease and death
There were an estimated 247 million cases and 619 000 deaths globally in 2021
Malaria is preventable and treatable
Global priority is to reduce the burden of disease and death while retaining the long-term
vision of malaria eradication
3. World Malaria Day 2023 will be marked under the theme
“Time to deliver zero malaria
invest, innovate, implement”
Within this theme, WHO will focus on the third “i” –
implement – and notably the critical importance of reaching
marginalized populations with the tools and strategies that are
available today
5. Parasitological diagnosis
All cases of suspected malaria should have a parasitological test (microscopy or RDT) to
confirm the diagnosis
Both microscopy and RDTs should be supported by a quality assurance programme.
6. Light microscopy
Microscopy not only provides a highly sensitive, specific diagnosis of malaria when performed well
but also allows quantification of malaria parasites and identification of the infecting species
Light microscopy involves relatively high costs for training and supervision, and the accuracy of
diagnosis is strongly dependent on the competence of the microscopist
Microscopy technicians may also contribute to the diagnosis of non-malarial diseases
7. Rapid Diagnosis Tests -RDT
Current tests are based on the detection of histidine-rich protein 2 (HRP2), which is specific for P. falciparum,
pan-specific or species-specific Plasmodium lactate dehydrogenase (pLDH) or pan-specific aldolase
The tests have many potential advantages, including:
• rapid provision of results and extension of diagnostic services to the lowest-level health facilities
• fewer requirements for training and skilled personnel
• reinforcement of patient confidence in the diagnosis and in the health service in general.
8. At present, molecular diagnostic tools based on nucleic-acid amplification techniques
(e.g. loop-mediated isothermal amplification or polymerase chain reaction [PCR]) do
not have a role in the clinical management of malaria
PCR can be used to diagnose placental infection in asymptomatic women
10. RECOMMENDATIONS ,BENEFIT AND HARM
Recommendation: Treat adults and children with uncomplicated P. falciparum malaria (including
infants, pregnant women in their second and third trimesters and breastfeeding women) with an
ACT
Desirable effects
• Studies have consistently demonstrated that the six WHO-recommended ACTs result in < 5% PCR-
adjusted treatment failures in settings with no resistance to the partner drug (high- quality
evidence)
Undesirable effects
• Increased cost.
11. Artemisinin-based combination therapy -ACT
Children and adults with uncomplicated P. falciparum malaria
should be treated with one of the following ACTs*
• artemether-lumefantrine (AL)
• artesunate-amodiaquine (AS+AQ)
• artesunate-mefloquine (ASMQ)
• dihydroartemisinin-piperaquine (DHAP)
• artesunate + sulfadoxine-pyrimethamine (AS+SP)
• artesunate-pyronaridine (ASPY) (2022)
12. NEWER COMBINATIONS
Arterolane + piperaquine is a combination of a synthetic ozonide and piperaquine phosphate that is
registered in India
Artemisinin + piperaquine base combines two well-established, well-tolerated compounds. It differs
from previous treatments in that the piperaquine is in the base form, the artemisinin dose is
relatively low, and the current recommendation is for only a 2-day regimen
Artemisinin + naphthoquine is also a combination of two relatively old compounds that is currently
being promoted as a single-dose regimen
13. DURATION OF TREATMENT
A 3-day course of the artemisinin component of ACTs covers two asexual cycles, ensuring that
only a small fraction of parasites remain for clearance by the partner drug, thus reducing the
potential development of resistance to the partner drug
Shorter courses (1–2 days) are therefore not recommended, as they are less effective, have less
effect on gametocytes and provide less protection for the slowly eliminated partner drug.
14. Reducing the transmissibility of treated
infection
In low-transmission areas, a single dose of 0.25 mg/kg bw primaquine should
be given with an ACT to patients with P. falciparum malaria (except pregnant
women, infants aged < 6 months and women breastfeeding infants aged < 6
months) to reduce transmission
G6PD testing is not required
15. Recurrent falciparum malaria
Recurrence of P. falciparum malaria can result from reinfection or recrudescence
(treatment failure )
Failure within 28 days - The recommended second-line treatment is an alternative
ACT known to be effective in the region
Failure after 28 days Recurrence of fever and parasitaemia > 4 weeks after
treatment may be due to either recrudescence or a new infection
16. CO INFECTED WITH HIV
Patients co-infected with HIV and uncomplicated P. falciparum malaria,
artesunate + SP is not recommended if they are being treated with co-
trimoxazole
Artesunate + amodiaquine is not recommended if they are being treated with
efavirenz or zidovudine.
17. Seasonal malaria chemoprevention
In areas of seasonal malaria transmission, children belonging to age groups at high risk of severe malaria
should be given antimalarial medicines during peak malaria transmission seasons to reduce disease burden
The added value of a seasonally targeted intervention is likely to be greatest where transmission is intensely
seasonal
Monthly cycles of sulfadoxine-pyrimethamine plus amodiaquine (SP+AQ) have been widely used for SMC in
African children under 5 years old and have been shown to be efficacious, safe, well tolerated, available and
inexpensive
3-5 cycles
19. Malaria in pregnant women is associated with high risks of both maternal and perinatal morbidity and
mortality
reduced immune response
less effectively clear malaria infections
malaria parasites sequester and replicate in the placenta
20. Intermittent preventive treatment of malaria
in pregnancy (IPTp)
In malaria-endemic areas, pregnant women of all gravidities should be given antimalarial medicine at
predetermined intervals to reduce disease burden in pregnancy and adverse pregnancy and birth
outcomes.
Remark:
• Sulfadoxine-pyrimethamine (SP) has been widely used for malaria chemoprevention during pregnancy
and remains effective in improving key pregnancy outcomes.
• IPTp-SP should start as early as possible in the second trimester and not before week 13 of pregnancy.
• Doses should be given at least one month apart, with the objective of ensuring that at least three doses
are received.
• IPTp is generally highly cost-effective, widely accepted, feasible for delivery and justified by a large body
of evidence generated over several decades.
21. UNCOMPLICATED MALARIA TREATMENT IN
PREGNANCY
Pregnant women of all gestational ages diagnosed with uncomplicated malaria acquired in areas with
chloroquine-resistant P. falciparum can be treated
artemether-lumefantrine
mefloquine
combination of quinine sulfate and clindamycin
Quinine treatment should continue for seven days for P. falciparum infections acquired in Southeast
Asia and for three days for infections acquired elsewhere; clindamycin treatment should continue for
seven days regardless of where the infection was acquired
22.
23. RADICAL TREATMENT
For P. vivax or P. ovale infections, primaquine phosphate and tafenoquine for
radical treatment of hypnozoites should not be given during pregnancy
Pregnant patients with P. vivax or P. ovale infections should be maintained on
chloroquine chemoprophylaxis for the duration of their pregnancy. The
chemoprophylactic dose of chloroquine phosphate is 300 mg base (500 mg salt)
orally once per week.
24. After delivery, for pregnant patients with normal G6PD activity infected with P. vivax or P. ovale
subsequent treatment with primaquine phosphate or tafenoquine
Tafenoquine is not recommended during breastfeeding.
25.
26. CONTRAINDICATED
Doxycycline and tetracycline are generally not indicated for use in pregnant women
However, in rare instances, doxycycline or tetracycline can be used in combination with quinine if other
treatment options are not available
Atovaquone-proguanil is not indicated for use in pregnant women
27. Chemoprophylaxis in pregnant travellers
Avoid travel to endemic areas
Travellers to chloroquine sensitive areas –Chloroquine phosphate 500 mgs salt
once a week started 2 weeks before travel and continued for 4 weeks after the
last exposure
Travellers to chloroquine resistant areas –Mefloquine phosphate 250 mgs salt
once a week started 2 weeks before travel and continued for 4 weeks after the
last exposure
28. VACCINE IN PREGNANCY
A membrane protein, PfEMP1-P falciparum erythrocyte membrane protein also
called VAR2CSA -antigen has been identified and under evalaution
29. MALARIA VACCINE
WHO recommends the RTS,S/AS01 (RTS,S) MOSQUIRIX by GSK malaria
vaccine to prevent malaria in children at risk
The recommendation for the first malaria vaccine was informed by results
from the ongoing pilot programme in Ghana, Kenya and Malawi
Four years on for the pilots, nearly 1.5 million children have been
reached with their first dose of malaria vaccine since 2019.
30. Strong recommendation for , High certainty evidence
The RTS,S/AS01 malaria vaccine should be used for the prevention of P. falciparum malaria in children living in
regions with moderate to high transmission as defined by WHO
• The RTS,S/AS01 malaria vaccine should be provided in a 4-dose schedule in children from 5 months age
• Countries may consider providing the RTS,S/AS01 vaccine seasonally, with a five-dose strategy, in areas with highly
seasonal malaria or with perennial malaria transmission with seasonal peaks
• Countries that choose to introduce the vaccine in a five-dose seasonal strategy are encouraged to document their
experiences, including adverse events following immunization
• RTS,S/AS01 malaria vaccine should be provided as part of a comprehensive malaria control strategy.
31. Vaccine characteristics, content, dosage, administration and
storage
RTS,S/AS01 is a pre-erythrocytic recombinant protein vaccine, based on the RTS,S recombinant antigen. It comprises
the hybrid polypeptide RTS, in which regions of the P. falciparum circumsporozoite protein known to induce humoral
(R region) and cellular (T region) immune responses are covalently bound to the hepatitis B virus surface antigen (S)
After reconstitution, the total volume is 1ml (two doses of 0.5 ml)
Vial should be discarded within six hours after reconstitution
The reconstituted 0.5ml vaccine should be administered by injection into the deltoid muscle in children aged 5 months
or older
The shelf life of the RTS,S/AS01 vaccine is three years
32. SCHEDULE
WHO recommends that the first dose of vaccine be administered from 5 months of age
There should be a minimum interval of four weeks between doses
The vaccine should be administered in a three-dose primary schedule, with a fourth dose provided
12–18 months after the third dose to prolong the duration of protection
However, there can be flexibility in the schedule to optimize delivery, for example, to align the
fourth dose with other vaccines given in the second year of life
33. CO ADMINISTRATION
RTS,S/AS01 given in conjunction with routine childhood vaccines has been evaluated in several trials
RTS,S/AS01 can be given concomitantly with any of the following monovalent or combination
vaccines: diphtheria, tetanus, whole cell pertussis, acellular pertussis, hepatitis B, Haemophilus
influenzae type b, oral poliovirus, measles, rubella, yellow fever, rotavirus and pneumococcal
conjugate vaccines
No co-administration studies have been conducted with RTS,S/AS01 and meningococcus A, typhoid
conjugate, cholera, Japanese encephalitis, Tick-borne encephalitis, rabies, mumps, influenza or
varicella vaccines
34. Benefits and harms
There were significant reductions in clinical malaria (51%); and severe malaria (45%), demonstrated
after 12 months' follow-up of the first three doses in the Phase 3 trial
There were 1774 clinical malaria cases averted per 1000 children vaccinated with four RTS,S/AS01
doses over 46 months' follow-up in the Phase 3 trial
There were significant reductions in clinical malaria (24%) demonstrated after 7 years’ follow-up
after vaccination among a subset of children in the Phase 3 trial living in areas of moderate to high
transmission; they did not have an excess risk of clinical or severe malaria
35. The RTS,S/AS01 vaccine is safe and well tolerated
There is a small risk of febrile seizures within seven days (mainly within 2–3 days) of vaccination
As with any vaccine introduction, proper planning and training of staff to conduct appropriate
pharmacovigilance should take place beforehand
36. NEWER VACCINES
Two vaccine candidates are approaching late-stage clinical evaluation: the R21/MatrixM vaccine candidate
targeting PfCSP protein and the attenuated whole sporozoite vaccine PfSPZ
Additional candidates targeting other malaria lifecycle stages include the Rh5 blood-stage vaccine candidate
[148] and Pfs25 and Pfs230 vaccine candidates targeting sexual-stage antigens to prevent human-to-mosquito
transmission (NCT02942277)
New technologies, such as DNAand mRNA-based vaccines , the ongoing development of adjuvants [150], and
delivery platforms such as virus-like particles (VLPs; the delivery platform used for RTS,S/AS01) and vesicle-
based technologies are being explored for use in malaria vaccines