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Event Date Event Title Event Description: http://www.timetoast.com/timelines/ malaria-timeline 23rd Jun, 0323 Death of Alexander the Great On the route to India beyond Mesopotamia, it was believed Alexander died of Malaria. 23rd Jun, 0400 First Malariolo gist 400 BCE Hippocrates was the first malariologist, who described various malaria and described the difference between continuous fever and the intermittent malarial fever. 23rd Jun, 1227 Death of Genghis Khan The Mongol warlord, who had set up one of the largest land empire ever known have suffered from malaria in the spring of 1227. On the banks of the Nile River residents recorded observations

Event DateEvent Title Event Description: 23rd Jun, 0323 Death of Alexander the Great On the route to

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Page 1: Event DateEvent Title Event Description:  23rd Jun, 0323 Death of Alexander the Great On the route to

Event Date Event Title Event Description:http://www.timetoast.com/timelines/malaria-timeline

23rd Jun, 0323

Death of Alexander the Great

On the route to India beyond Mesopotamia, it was believed Alexander died of Malaria.

23rd Jun, 0400

First Malariologist

400 BCE

Hippocrates was the first malariologist, who described various malaria and described the difference between continuous fever and the intermittent malarial fever.

23rd Jun, 1227

Death of Genghis Khan

The Mongol warlord, who had set up one of the largest land empire ever known have suffered from malaria in the spring of 1227.

1st Jan, 1570 1570 BCE

On the banks of the Nile River residents recorded observations of diseases into the oldest surviving medical document from Ancient Egypt, the Ebers Papyrus. Ebers Papyrus consisted of 700 drugs and 800 creations

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This day relenting GodHath placed within my handA wondrous thing; and GodBe praised. At his command,

Seeking his secret deedsWith tears and toiling breath,I find thy cunning seeds,O million-murdering Death.

I know this little thing A myriad men will save,O Death, where is thy sting?Thy victory, O Grave?

- Ronald Ross 20 August 1897http://www.malariasite.com/malaria/ross.htm

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February 10 -19, 2014Lipa City, Philippines

UNIT 4: APPROACHES ANDTOOLS SPECIFIC TO

ELIMINATION PROGRAMMES

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Review the interventions, which can be applied from the pre-elimination to the prevention of reintroduction stage, and decide which are most appropriate under specific conditions in each stage

List the four approaches (strategic elements) that define a malaria elimination programme, giving examples of relevant tools for each and explain why these approaches are critical to achieving malaria elimination

List the objectives of malaria treatment in elimination programmes

Learning objectives

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Describe and justify antimalarial treatment policies for P. falciparum and P. vivax in malaria elimination programmes

Describe the indications and objectives of mass drug administration

List the different vector control methods and their value and limitations in the different stages of malaria elimination

Describe the technical and operational issues related to vector control measures

Learning objectives

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Control StrategyApplication of menu interventions to gradually reduce the burden of the disease in a population

Elimination StrategyApplication of targeted and locally adapted measures to track down the last foci and cases of malaria – making sure parasites are killed

Control strategy

vs. Elimination

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4 Approaches/Strategic Elements

2. TREAT

1. DETECT

3. Manage FOCI

4. Prevent IMPORTATION

Take other measures to prevent infection of anophelines/

infection of other

persons by anophelines already infected

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Treat all infections in a community, symptomatic or asymptomatic,

to interrupt transmission

Malaria Case Management

Rapidly Reducing the Parasite Reservoir Prevent Transmission

as well as Cure Disease

Avert Complications & Death

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In an elimination setting all malaria cases should be detected and confirmed by parasitological tests that

identify species, stage and load of infection.

Microscopy - highly sensitive and specific in identifying parasite species, stages and quantification of malaria parasites.

A system for quality assurance is essential.

Rapid diagnostic tests (RDTs) may be useful for (i) the screening of travellers (ii) wherever there is lack skilled microscopy Polymerase chain reaction (PCR) may be used for population screening and for identifying morphologically similar species e.g.. P. malariae and P. knowlesi). It is presently not indicated for the case management of fever.Serologic methods detect antibodies that may be due to current or past infection. They may

be useful in epidemiological studies to get an idea about the load of malaria in the community.

Diagnosis in a Malaria Elimination programme

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Treatment of Malaria casesIn the context of elimination aim is at complete parasitological cure (radical cure), including killing of the parasites in their sexual stages

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Radical treatment of Pf Radical treatment of Pv Treatment of Severe Malaria

(addition of single dose primaquine once patient can take oral meds)

Use of antimalarials for reducing parasite reservoir

Chemoprophylaxis

Use of Antimalarial

Medicines

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Artemisinins (ACTs) destroy immature, developing gametocytes , less effective on mature gametocytes

Primaquine selectively kills gametocytes. A single oral dose of 0.75 mg base/kg body weight primaquine

(45 mg base for adults) is recommended to reduce falciparum transmission provided risk of G6PD deficient patients are considered (given on the first day of ACT treatment, NOT in pregnancy and in young children),

Gametocytocidal Treatment(Radical treatment of PF)

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Updated WHO Policy Recommendation (October 2012 )

A single 0.25 mg base/kg primaquine dose be given to all patients with parasitologically-confirmed P. falciparum malaria in:

(1) areas threatened by artemisinin resistance where single dose primaquine as a gametocytocide for P. falciparum malaria is not being implemented, and

(2) elimination areas which have not yet adopted primaquine

http://www.who.int/malaria/pq_updated_policy_ recommendation_en_102012.pdf

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P. vivax for chloroquine-sensitive, oral chloroquine 25 mg/kg, given at

an initial dose of 10 mg/kg followed by 10 mg/kg on the 2nd day and 5 mg/kg on the third day

W/o G6PD - To be given with primaquine, anti-relapse medicine at a dose of 0.25 mg base/kg bw, once a day for 14 days

For Southeast Asia and Oceania – dose is 0.5 mg/kg bwAlternatively 0.75 mg base/kg bw given once a week for 8

weeks

P. ovale – same as P. vivax

P. malariae - Chloroquine

Uncomplicated Non-falciparum malaria

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Maintain Small Stocks of- Quality Assured

Anti-malarial Medicines

- Effective for rapid treatment

-Within expiry date

Quality Assurance and logistics of

Anti-malarial Medicines for Case

Management

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Full cooperation of the private health sector. All patients, whether nationals, temporary or permanent

immigrants, people in transit, or residents of neighbouring countries who live in border areas can easily access services --- FOC diagnosis & treatment including consultation fees.

Monitoring of the national supply of antimalarial medicines; STOP over-the-counter sale of antimalarial medicines; maintenance of skills of health personnel and updating of

their knowledge.

Role of Private health care sector and other sectors providing services

Elimination programmes aim – 100% detection and notification of malaria cases

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Mass Screening and Treatment (MSAT)

Mass Drug Administration(MDA)

Seasonal Treatment to reduce P. vivax hypnozoite carriers

Use of antimalarial

medicinesfor reducing

parasite reservoir

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Mass screening for parasitaemia and treating all infected persons in a targeted area or population, regardless whether they are symptomatic or not = aim is to rapidly reduce the size of infectious reservoir in targeted area screening tools : RDT vs. Microscopy vs. PCR repeated at intervals once or twice time-consuming and may miss low-density parasitaemia.Exclusions: contraindications to the medicines used, pregnant women, young infants and other population groupsNot for relapsing malarias (no test for detecting hypnozoites)

MSAT or FSAT

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Campaign for treating every individual in a defined population or geographical area with antimalarial treatment on a given day, in a coordinated manner.A well conducted MDA can result in a major reduction in the parasite mass The treatment is usually the same as is used in case management for

the species, which is targeted. usually considered in the end-stage, for management of last

remaining small foci, with accessible population and very low risk of importation

Full cooperation of the community is essential to reach 100% coverage

MDA

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Rebound The area can return to its original prevalence levels, if vectorial

capacity is not reduced and maintained at below the critical level. time to return to the original levels of transmission depends on

the prevailing vectorial capacity. The rebound may be associated with higher morbidity and

mortality if people lost herd-immunity against malaria. A coordinated attack of vector control and use of drugs to reduce

the parasite reservoir may solve the problem of rebound . Enhance resistance against the medicines if larger population of

parasites targeted with MDA Mass drug administration difficult to explain to the population Side effects, especially of primaquine

MDA - concerns

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Used to interrupt transmission in areas with seasonal transmission of P. vivax (about 3-5 months) , where foci are small and high coverage can be achieved,

All individuals to be treated with primaquine for 14 days (Except pregnant women and children under one year)

Usually conducted in spring, about two months before the onset of transmission.

The pre-condition: primaquine is not associated with any significant risk of toxicity in the target population, population is fully informed of signs of primaquine toxicity, fully cooperative.

Seasonal Treatment of P. vivax Hypnozoite Carriers

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Which is the FOCUS? Surveillance, malaria surveys,

GR vector control and

entomological investigations; involvement of local

authorities, local communities and inter-sectoral action.

Management of malaria

foci

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inter-country coordination and collaboration; prevention of malaria in residents who travel to

endemic countries, including chemoprophylaxis, prevention of mosquito bites, standby treatment and case management;

screening, health education, easy access to free-of-charge diagnosis and treatment and other measures to cope with the importation of parasites by international travellers and migrants;

Management of importation of malaria parasites

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Chemoprophylaxis for travellers (source: http://www.who.int/ith/chapters/ith2012en_countrylist.pdf).

Risk type Malaria risk Type of prevention

Type I Very limited risk of malaria transmission Mosquito bite prevention only

Type II Risk of P. vivax malaria only; or fully chloroquine-sensitive P. falciparum

Mosquito bite prevention plus chloroquine chemoprophylaxis

Type IIIaRisk of P. vivax and P. falciparum malaria transmission, combined with emerging chloroquine resistant

Mosquito bite prevention plus chloroquine+proguanil chemoprophylaxis

Type IV (1) High risk of P. falciparum malaria, in combination with reported antimalarial drug resistance; or (2) Moderate/low risk of P. falciparum malaria, in combination with reported high level of drug resistance

Mosquito bite prevention plus atovaquone-proguanil, doxycycline or mefloquine chemoprophylaxis (selected according to reported resistance pattern)

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Be Aware of the risk, the incubation period, the possibility of delayed onset, and the main symptoms.

Avoid being Bitten by mosquitoes, especially between dusk and dawn.

Take Chemoprophylaxis when appropriate, to prevent infection from developing into clinical disease.

Immediately seek Diagnosis and treatment if a fever develops 1 week or more after entering an area where there is a malaria risk and up to 3 months (or, rarely, later) after departure from a risk area.

ABCD 4 Principles of Malaria Protection

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Vector Control

Know your

enemy

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Operational Issues

Combining IRS and LLIN Space spraying LSM and other larval

control measures Withdrawal of prevention

measures with NO or LOW transmission

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Parameters min max Baseline m value a value p value Duration combi combi

m = mosquito densities per person 0 500 78.5 40 78.5 78.5 78.5 78.5 15

a = antropophilic index 0 1 0.7 0.7 0.35 0.7 0.7 0.7 0.7p = daily survival rate

of the vector 0.05 0.95 0.71 0.71 0.71 0.35 0.71 0.61 0.71n =number of days for

full maturation of sporozoites 12 30 15 15 15 15 15 15 15

b =effectiveness of a vector 0 1 0.01 0.01 0.01 0.01 0.01 0.01 0.01

duration of infection 1 400 15 15 15 15 7.5 7.5 7.5

r =recovery rate 1 0.0025 0.0667 0.0667 0.0667 0.06667 0.1333 0.1333 0.1333Results

ma^2 38.465 19.6 9.6162 38.465 38.465 38.465 7.35p^n 0.00587 0.00587 0.00587 1.4488E-07 0.00587 0.00060 0.00587

-LN(p) 0.3425 0.3425 0.3425 1.049822 0.3425 0.4943 0.3425

C =vectorial capacity 0.65962 0.33611 0.16491 5.3085E-060.659620.0469 0.1260R(0) =basic

reproduction rate 9.89427 5.04167 2.47357 7.963E-05 4.947140.3516 0.9453 LSM, Repel Zoophro Adult VC EDPT EDPT + EDPT +

LLIN, IRS Non-irritant Adult VCLSM, Repel

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In all these approaches, malaria surveillance is a common

denominator.

It is the backbone of any elimination programme.

Indicators of Effective Surveillance

Continuing detection of imported malaria casesAbsence of gametocyte

positive P. falciparum case

Surveillance: key intervention for elimination

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Case-based SS – each case can be easily classified by its probable geographic origin

Incidence of malaria is analyzed village-wise

Surveillance is complete: Nearly all fever cases are observed by the health services in accordance with the 3T principle (tested, treated and tracked) and all results of malaria testing reported. Whether or not this is the case can be assessed by population surveys for treatment seeking behaviour and health facility surveys for completeness of reporting.

Need for Strong Surveillance

System

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4 Approaches/Strategic ElementsElimination Phase

2. TREAT

1. DETECT

3. Manage FOCI

4. Prevent IMPORTATION

Take other measures to prevent infection of anophelines/

infection of other persons by anophelines already infected

1. EARLY DETECTION OF ALL CASES

2. PREVENTION OF ONWARD TRANSMISSION FROM CASES

3. MANAGEMENT OF FOCI

4. MANAGEMENT OF IMPORTATION OF MALARIA PARASITES

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legislation making malaria a notifiable disease.

quality assured microscopy as the standard routine method;

epidemiological investigation of every confirmed case;

national malaria case register; radical treatment; active case detection as routine

or reactively, as needed; vector control as necessary; if possible, parasite genotyping

and parasite isolate banks.

Early detection of cases and

prevention of transmission

from them

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VigilanceFull integration to GHS ?ACD in high risk area?MSAT ?IEC ? – travellers,

prescribersMedicine Stock

Chemoprophylaxis Vector Control Pro-active Reactive

Approachesin the Prevention

of Re-introduction of Malaria

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Discuss the technical and operational conditions for optimal implementation of IRS and LLINs interventions, respectively.

Exercise 4.1- Group 3

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What factors determine whether and how quickly malaria returns if vector control is stopped?

Exercise 4.2- Group 4

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In what ways can operational research guide and promote case management in malaria elimination, including diagnosis and the use of antimalarial drugs?

Exercise 4.3Group 3 & 4

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After two years with zero reported locally transmitted falciparum malaria cases in a country in the Arabian peninsula, three cases are detected in an oasis, where there are 3000 inhabitants. The oasis frequently hosts overland travellers, some of whom might come from areas where malaria is endemic. The spray-team has started a total coverage operation. The Minister of Health wants you to do mass drug administration (MDA), unless you have convincing arguments for a better strategy. The Minister has also told you that any severe side effects of MDA must be avoided. What are your options? Discuss pros and cons for each.

Exercise 4.4.Group 1

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Prepare a matrix of rows representing all the interventions discussed here and 4 columns representing the 4 phases from control to prevention of reintroduction. Fill in the cells for a selected country or area contemplating elimination to identify the role of each intervention in each phase.

Exercise 4.5Group 2

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Discuss pros and cons of combining IRS and LLINs in the elimination phase.

Exercise 4.6Group 1 & 2