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MALARIA DIAGNOSIS AND
TREATMENT IN BORDER AREAS:
  WHAT SHOULD WE PAY ATTENTION TO?




              Asep Purnama
    TC Hillers Hospital, Maumere, NTT
STRATEGIES
   Prevention
    Vector control, Long Lasting Insecticide Net, Repellent etc
   Accurate diagnosis
   Prompt treatment with ACT
   Partnership
   Increase Coverage of Service



Erna Tresnaningsih, Direktur Pemberantasan Penyakit Bersumber Binatang, Depkes RI
Seminar Nasional Manajemen Malaria Terkini, Manhattan Hotel-Jakarta, 14 Juni 2008
MALARIA DIAGNOSIS
    PROBLEMS
Clinical responses to malaria infection vary widely
CLINICAL MALARIA, BLOOD SAMPLE TAKEN
     & POSITIVE DIAGNOSIS IN INDONESIA
    3,500,000

    3,000,000

    2,500,000

    2,000,000

    1,500,000

    1,000,000

     500,000

           0




                                                                       8
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                      01


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            20


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                                                                    ar
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   Not all Malaria cases are diagnosed by microscopist or RDT
   Slide positive malaria cases don’t decrease significantly
M ALARIA KLINIS DAN PE E
                                M RIKSAAN SE DIAAN DARAH
               M ALARIA DI JAWA BALI TAHUN 2000-2004
1600000                                                          Klinis     Pem SD
          1475704
1400000

1200000
                     1210530
1000000
                                   998791
800000                                            756833
600000
                                                                 480048
400000

200000

     0

            2000          2001      2002               2003          2004


                   MALARIA KLINIS DAN
          PEMERIKSAAN SEDIAAN DARAH MALARIA DI
             LUAR JAWA BALI TAHUN 2000-2004

                                     1974882
   2000000   1702508           1732557
                         1686176           Kl i ni s    Pem SD

   1800000         1522831
   1600000
   1400000
   1200000
   1000000

                   404714 389477 337583 348366 479441
    800000
    600000
    400000
    200000
         0

                   2000     2001      2002             2003        2004
S ED I A A N D A R A H M A L A R I A P OS I T I F
                      D A N M A L A R I A P f D A N M I X D I J A WA B A L I
                                     TA H U N 2 0 0 0 - 2 0 0 4

  120000
                                                                   SD Positif           Pf + mix
  100000

   80000

   60000

   40000

   20000

         0
               2000             2001             2002              2003           2004


   SED I A A N D A R A H M A LA R I A PO SI T I F D A N M A LA R I A Pf D A N
                              M I X D I LU A R JA W A B A LI
                                   T A HU N 2 0 0 0 - 2 0 0 4

                                                                          SD Posit if      Pf + mix
200000                     181315
             155796                                               148478
150000                                       140769                             132095
100000


50000


    0
              2000             2001             2002               2003            2004
MALARIA DIAGNOSIS
    What should we pay attention to?
   Prompt and accurate diagnosis is critical to the
    effective management of malaria
   Based on microscopic diagnosis/RDT
   Capacity building
   Equipment (microscope, RDT)
   Cost
   Quality Control
Survey of General Practitioner’s
Knowledge, Attitude and Practice on Malaria
in Sikka District, East Nusa Tenggara 2008


           Jane Hidayat, Asep Purnama
MALARIA TREATMENT
    PROBLEMS
P. falsiparum : chloroquine resistance




           Countries with at least one study indicating chloroquine total failure rate > 20%
           Countries with at least one study indicating chloroquine total failure rate > 10%
           No recent data available
P. falsiparum:
Sulfadoxin-pyrimethamine resistance




          Countries with at least one study indicating sulfadoxine-pyrimethamine total failure rate > 20%
          Countries with at least one study indicating sulfadoxine-pyrimethamine total failure rate > 10%
          Sulfadoxine-pyrimethamine total failure rate < 10%
          No failure reported
          No recent data available
P. vivax
prophylactic or treatment failure




          P. vivax prophylactic or treatment failure
Anti Malaria Drug Resistance In Indonesia,
RESISTANCE OF PLASMODIUM TO
 MALARIA DRUGS IN INDONESIA
                 1978 - 2003
SAFE & EFFECTIVE DRUGS
COMPLIANCE
COST
MALARIA TREATMENT
    What should we pay attention to?
 Artemisinin based Combination Treatment
 Radical treatment is essential
 Outcome focus on clinical cure, parasitological
  clearance, and blocking transmission
 Monitoring therapeutic efficacy of antimalarial drugs
  based on clinical and parasitological responses (in-
  vivo 28 days)
74 countries have adopted ACTs                                                    Updated
                                                                                              1 Oct 2007

Continent                                 Countries                                         Drug Line
            Burundi, Cameroon, Congo, Côte d'Ivoire, Democratic Republic of Congo, Eq.      AS + AQ        1st
            Guinea, Gabon, Ghana, Guinea, Liberia, Madagascar, Eritrea, Mali, Mauritania,
             Senegal,          Sao Tomé & Principe (ST&P), Sierra Leone, Sudan (S),
 AFRICA                                 Tchad, Zanzibar
              Angola, Benin, Botswana, Burkina Faso, Central African Republic, Comoros,       AL           1st
            Ethiopia, Gambia, Guinea Bissau, Kenya, Malawi, Mozambique, Namibia, Niger,
                Nigeria, Rwanda, Uganda, S. Africa, Tanzania, Togo, Zambia, Zimbabwe
                      Côte d'Ivoire, Djibouti, Gabon, Sudan (N), ST&P, Zanzibar               AL       2nd
                                    Djibouti, Somalia, Sudan (N)                            AS + SP        1st
                              Cambodia, Malaysia, Myanmar, Thailand                          AS +          1st
                                                                                             MQ
             Bangladesh, Bhutan, Laos, Philippines, Solomon Islands, Sri Lanka, Vanuatu       AL           1st
  ASIA                                        Indonesia                                     AS + AQ        1st
                  Afghanistan, India, Iran, Pakistan, Saudi Arabia, Tajikistan, Yemen       AS + SP        1st
                                          Viet Nam, China                                     DP           1st
                                         Papua New Guinea                                   AS + SP    2nd
                                         Iran, Saudi Arabia,                                  AL       2nd
  SOUTH                                    Ecuador, Peru                                    AS + SP        1st
 AMERICA                         Bolivia, Colombia, Peru, Venezuela                          AS +          1st
                                                                                             MQ
                                Brazil, Colombia, Guyana, Suriname                            AL           1st
INDONESIA’S TREATMENT POLICY

Uncomplicated Pf       Complicated Pf
   ATS3+AQ3+PQ           QN parenteral-oral7+Dx7/Clin7
   DHP3+PQ               Artemether im-AQ3+ATS3
   QN7+DX7/Clin7+PQ      Artesunate iv-AQ3+ATS3


Uncomplicated Pv       Prophylaxis
   ATS3+AQ3+PQ14         Doxycycline
   DHP3+PQ14
                       Outbreak containment (MFS)
   QN7+PQ14
                          AQ3+ATS3+PQ1
   Since 2004 Artesunate-amodiaquine as the first line
    ACT for P.falciparum malaria (based on the African
    study Adjuik M et al, Lancet 2002).

   Efficacy of Artesunate-amodiaquine varied between
    study sites 78-96% (Gasem H et al, 2004 ; Tjitra E et al, 2004; and
    Sutanto I et al, 2004; Setyoningrum E et al, 2005; Hasugian et al, CID 2006 ).


   Utility of Artesunate-amodiaquine reported low (<50%)
    due to poor compliance and adherent events because
    of need to take large number of pills (personal
    communication)
ASSESMENT OF CHLOROQUINE AND ARTESUNATE-
   AMODIAQUINE COMBINATION EFFICACY FOR THE
TREATMENT OF UNCOMPLICATED FALCIPARUM MALARIA
     IN BELU DISTRICT, EAST NUSA TENGGARA




      Asep Purnama et al, IJIM 2006:38;327-31
RESULTS
   Due to an increase in the chloroquine treatment failure rate
    to 47,62%, recruitment was terminated prematurely

   A total of 95 of the originally recruited 203 patients were
    enrolled in the study
   Artesunate-amodiaquine showed superior 28-day cure rate
   Chloroquine versus artesunate-amodiaquine was 22/42
    [52,38%] versus 49/53 [92,45%]; p<0,01
   However , efficacy of As+Aq was <95%, below than WHO
    standard
ARTESUNATE - AMODIAQUINE VERSUS CHLOROQUINE
     FOR THE TREATMENT OF VIVAX MALARIA
       IN MAUMERE, EAST NUSA TENGGARA




      National Institute of Health Research and
            Development, MOH, Jakarta
RESULTS
   A prospective comparative clinical trial of efficacy, safety
    and tolerability of As+Aq versus chloroquine for treatment
    of uncomplicated vivax malaria with a 28-day follow up

   Of a total 105 enrolled patients there were 100 patients
    could be analysed
   The efficacies of As+Aq and Chloroquine were 88% and
    40,8% on day 28 by ITT and 93,2% and 47,2% by
    PP, respectively
   However , efficacy of As+Aq was <95%, below than WHO
    standard
NEED ALTERNATIVE ACTs

ATS3+AQ3                           QN7+Dx7/Clind
   Efficacy <95% (Papua 70-87%)      Efficacy ?
   AR: nausea and vomiting           AR: dizziness, tinnitus
   Compliance? (no of pills)         Poor compliance
   Cost and accessibility?
IMPROVING ACT

COMPLIANCE                    CURE RATE
                               Effective: rapid
 Tolerate: tasteless

 Safe: risk groups (infancy
                                           broad spectrum
                               Practice : all species
        and pregnancy)
        adverse events                     single dose only
 Simple: fixed-dose regimen

           all age groups
           single daily dose/
           single dose only
CLINICAL TRIALS ON ACTs

                                                   (ATS+PD)3

                                                                                    (ART+NTQ)1 VS
                          Parentral ATM vs QN
     ATS3+AQ3 VS                                                                    (DHA+PPQ)3
     (ART+PPQ)2
                                                                                     (ATS+PD)3 vs
                                                                                     ((ATM+LMF)3
CQ3 vs (CQ3+SP1) vs AQ3


                                                                              IV ART vs QN
                                  (ATS+PD)3 vs
                                                 (ART+NTQ)1 VS
                                  ((CQ)3                                      (ATM+LMF)3 VS
                                                 (DHA+PPQ)3
                                                               (ATS+PD)3 vs   (DHA+PP)Q3
                                                               ((ATM+LMF)3    ATS3+AQ3 VS
                                                                              (DHA+PPQ)3
EFFICACY COMBO VS FIXED REGIMEN

                                                                           N=352

Artesunate+amodiaquine (ATS3+AQ3) vs Artemisinin+piperaquine (ART+PPQ)2

    Pf: 93.8% vs 96.5%                                                             Pv:96.5% vs 100% (Tjitra E et al, 2005)
                                                                                   4
7
                                                                               3.5
6
                                                                                   3
5
                                                                               2.5
4
                                                                                   2

3
                                                                               1.5

2                                                                                  1

1                                                                              0.5


0                                                                                  0
     Day 0   Day 1   Day 2     Day 3    Day 7   Day 14   Day 21   Day 28               Day 0   Day 1   Day 2     Day 3    Day 7   Day 14   Day 21   Day 28

                             ATS3+AQ3    ART2+PPQ2                                                             ATS3+AQ3    ART2+PPQ2
Artemisinin/naphtoquine P. vivax,
      P. falciparum, P.mix phase III trial


       A Phase III randomized, open label, non-inferiority trial
of artemisinin plus naphtoquine (ARCO) versus dihydroartemisinin
plus piperaquine in adult uncomplicated malaria patients: A Multi-
                      centre study in Indonesia
Artemisinin/naphtoquine phase III trial
                    Study outline
 401 patients randomized
 Study duration: April 2007 – August 2008

 Treatment : single dose, F/U to 42 days
 Multicentre: 2 sites, 4 hospital
 :
Artemisinin/naphtoquine phase III trial
                         Conclusions
   The trial demonstrated non inferiority treatment study
   Arco vs Duocotecxin
       P. vivax 98,7% vs 97,3%
       P. falciparum 98,7% vs 97,1%
   Both new fixed-dose ACTs are confirmed very
    effective, safe and tolerate for treatment of any malaria in
    adults, and meet with the recent WHO recommendation for
    replacing ineffective drugs
ARTEMISININ FOR SEVERE MALARIA

ARTEMETHER                       QUININE DIHYDROCHLORIDE
   FCT= 35.5 hours               FCT= 37.4 hours

   PCT= 38.9 hours               PCT= 41.8 hours

   Regain consciousness=         Regain consciousness =
    32 hours                       62.8 hours
   CFR cerebral mal =            CFR cerebral mal = 71.4%
    37.5%                         Overall CFR= 23%
   Overall CFR= 13%
                     Tjitra E et al, MJI, 1996
SEAQUAMAT TRIAL
   Study design: Open label, multi centre,
    randomised, comparison of artesunate
    and quinine in severe falciparum
    malaria
   Study sites: 2003-2005
      Bangladesh

      Indonesia (Timika Hospital, Timika)

      India

      Myanmar
   Target sample size: 2,000 patients
   1400 enrolled as at February 2005
   Coordination: Wellcome Unit, Bangkok
RESULTS
                (SEAQUAMAT Group, Lancet, 2005)

   Trial stopped early (n=1461) by Safety Monitoring
    committee because clear benefit with artesunate

   Overall reduction in mortality with artesunate 34.7%
    (95%CI 19-48%) p=0.0002
       mortality quinine: 164/731 (22%)
       mortality artesunate: 107/730 (15%)

   Indonesian national policy change before the results
    published
   Australian policy change 2006
THE IMPORTANCE OF COOPERATION BETWEEN
        NEIGHBOURING COUNTRIES
     Many health problems are cross border
      (malaria, rabies, filaria, DHF etc)
   Limited resource: mutual cooperation important
   Potential for inefficiency if countries work alone
      Sharing expertise and facilities
      Cooperation on research projects
      Share results of individual research
      Cooperation to develop guidelines or policy
MASS BLOOD SURVEY-YASPEM
   Target             45.454 [3 kecamatan]
   Blood sample taken 37.974      83,48 %
   Results F            351        0,9 %
             V           517        1,4 %
             Mix          71        0,2 %
             Total       939        2,5 %
DROP OUT
   Adverse event 18 [1,9%]
   Hospitalized 6 [0,6%]
   Loss of follow up 8 [0,8%]
   Reject to take medicine 12 [1,3%]
SOME EXAMPLES OF POOR PRACTICE
•   Giving SP to patients with fever even though blood
    smear negative
•   Treating uncomplicated malaria with parenteral quinine
    or arthemeter im
•   Treating complicated malaria with chloroquine or ACT
•   Giving SP for P vivax malaria
•   Giving Primaquine 15 mg for 14 days for P falciparum
    malaria
•   Giving all available forms of treatment to the one
    patient
SOME EXAMPLES OF POOR PRACTICE                      (contd)

•   Using RDT to evaluate response to treatment
•   Giving transfusion to malaria patients with mild
    anaemia
•   Using steroids to treat cerebral malaria
•   Inadequate fluid for complicated malaria
•   Postponing haemodialysis for complicated malaria
    with acute renal failure
•   Unawareness of hypoglycemia in complicated malaria
•   Not giving ACT for 3 days
•    Giving inadequate doses of artesunate or arthemeter

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Malaria border area

  • 1. MALARIA DIAGNOSIS AND TREATMENT IN BORDER AREAS: WHAT SHOULD WE PAY ATTENTION TO? Asep Purnama TC Hillers Hospital, Maumere, NTT
  • 2. STRATEGIES  Prevention Vector control, Long Lasting Insecticide Net, Repellent etc  Accurate diagnosis  Prompt treatment with ACT  Partnership  Increase Coverage of Service Erna Tresnaningsih, Direktur Pemberantasan Penyakit Bersumber Binatang, Depkes RI Seminar Nasional Manajemen Malaria Terkini, Manhattan Hotel-Jakarta, 14 Juni 2008
  • 3. MALARIA DIAGNOSIS PROBLEMS
  • 4. Clinical responses to malaria infection vary widely
  • 5. CLINICAL MALARIA, BLOOD SAMPLE TAKEN & POSITIVE DIAGNOSIS IN INDONESIA 3,500,000 3,000,000 2,500,000 2,000,000 1,500,000 1,000,000 500,000 0 8 00 01 02 03 04 05 06 07 '0 20 20 20 20 20 20 20 20 ar M n- Ja  Not all Malaria cases are diagnosed by microscopist or RDT  Slide positive malaria cases don’t decrease significantly
  • 6. M ALARIA KLINIS DAN PE E M RIKSAAN SE DIAAN DARAH M ALARIA DI JAWA BALI TAHUN 2000-2004 1600000 Klinis Pem SD 1475704 1400000 1200000 1210530 1000000 998791 800000 756833 600000 480048 400000 200000 0 2000 2001 2002 2003 2004 MALARIA KLINIS DAN PEMERIKSAAN SEDIAAN DARAH MALARIA DI LUAR JAWA BALI TAHUN 2000-2004 1974882 2000000 1702508 1732557 1686176 Kl i ni s Pem SD 1800000 1522831 1600000 1400000 1200000 1000000 404714 389477 337583 348366 479441 800000 600000 400000 200000 0 2000 2001 2002 2003 2004
  • 7. S ED I A A N D A R A H M A L A R I A P OS I T I F D A N M A L A R I A P f D A N M I X D I J A WA B A L I TA H U N 2 0 0 0 - 2 0 0 4 120000 SD Positif Pf + mix 100000 80000 60000 40000 20000 0 2000 2001 2002 2003 2004 SED I A A N D A R A H M A LA R I A PO SI T I F D A N M A LA R I A Pf D A N M I X D I LU A R JA W A B A LI T A HU N 2 0 0 0 - 2 0 0 4 SD Posit if Pf + mix 200000 181315 155796 148478 150000 140769 132095 100000 50000 0 2000 2001 2002 2003 2004
  • 8. MALARIA DIAGNOSIS What should we pay attention to?  Prompt and accurate diagnosis is critical to the effective management of malaria  Based on microscopic diagnosis/RDT  Capacity building  Equipment (microscope, RDT)  Cost  Quality Control
  • 9. Survey of General Practitioner’s Knowledge, Attitude and Practice on Malaria in Sikka District, East Nusa Tenggara 2008 Jane Hidayat, Asep Purnama
  • 10. MALARIA TREATMENT PROBLEMS
  • 11. P. falsiparum : chloroquine resistance Countries with at least one study indicating chloroquine total failure rate > 20% Countries with at least one study indicating chloroquine total failure rate > 10% No recent data available
  • 12. P. falsiparum: Sulfadoxin-pyrimethamine resistance Countries with at least one study indicating sulfadoxine-pyrimethamine total failure rate > 20% Countries with at least one study indicating sulfadoxine-pyrimethamine total failure rate > 10% Sulfadoxine-pyrimethamine total failure rate < 10% No failure reported No recent data available
  • 13. P. vivax prophylactic or treatment failure P. vivax prophylactic or treatment failure
  • 14. Anti Malaria Drug Resistance In Indonesia, RESISTANCE OF PLASMODIUM TO MALARIA DRUGS IN INDONESIA 1978 - 2003
  • 17. COST
  • 18. MALARIA TREATMENT What should we pay attention to?  Artemisinin based Combination Treatment  Radical treatment is essential  Outcome focus on clinical cure, parasitological clearance, and blocking transmission  Monitoring therapeutic efficacy of antimalarial drugs based on clinical and parasitological responses (in- vivo 28 days)
  • 19. 74 countries have adopted ACTs Updated 1 Oct 2007 Continent Countries Drug Line Burundi, Cameroon, Congo, Côte d'Ivoire, Democratic Republic of Congo, Eq. AS + AQ 1st Guinea, Gabon, Ghana, Guinea, Liberia, Madagascar, Eritrea, Mali, Mauritania, Senegal, Sao Tomé & Principe (ST&P), Sierra Leone, Sudan (S), AFRICA Tchad, Zanzibar Angola, Benin, Botswana, Burkina Faso, Central African Republic, Comoros, AL 1st Ethiopia, Gambia, Guinea Bissau, Kenya, Malawi, Mozambique, Namibia, Niger, Nigeria, Rwanda, Uganda, S. Africa, Tanzania, Togo, Zambia, Zimbabwe Côte d'Ivoire, Djibouti, Gabon, Sudan (N), ST&P, Zanzibar AL 2nd Djibouti, Somalia, Sudan (N) AS + SP 1st Cambodia, Malaysia, Myanmar, Thailand AS + 1st MQ Bangladesh, Bhutan, Laos, Philippines, Solomon Islands, Sri Lanka, Vanuatu AL 1st ASIA Indonesia AS + AQ 1st Afghanistan, India, Iran, Pakistan, Saudi Arabia, Tajikistan, Yemen AS + SP 1st Viet Nam, China DP 1st Papua New Guinea AS + SP 2nd Iran, Saudi Arabia, AL 2nd SOUTH Ecuador, Peru AS + SP 1st AMERICA Bolivia, Colombia, Peru, Venezuela AS + 1st MQ Brazil, Colombia, Guyana, Suriname AL 1st
  • 20. INDONESIA’S TREATMENT POLICY Uncomplicated Pf Complicated Pf  ATS3+AQ3+PQ  QN parenteral-oral7+Dx7/Clin7  DHP3+PQ  Artemether im-AQ3+ATS3  QN7+DX7/Clin7+PQ  Artesunate iv-AQ3+ATS3 Uncomplicated Pv Prophylaxis  ATS3+AQ3+PQ14  Doxycycline  DHP3+PQ14 Outbreak containment (MFS)  QN7+PQ14  AQ3+ATS3+PQ1
  • 21. Since 2004 Artesunate-amodiaquine as the first line ACT for P.falciparum malaria (based on the African study Adjuik M et al, Lancet 2002).  Efficacy of Artesunate-amodiaquine varied between study sites 78-96% (Gasem H et al, 2004 ; Tjitra E et al, 2004; and Sutanto I et al, 2004; Setyoningrum E et al, 2005; Hasugian et al, CID 2006 ).  Utility of Artesunate-amodiaquine reported low (<50%) due to poor compliance and adherent events because of need to take large number of pills (personal communication)
  • 22. ASSESMENT OF CHLOROQUINE AND ARTESUNATE- AMODIAQUINE COMBINATION EFFICACY FOR THE TREATMENT OF UNCOMPLICATED FALCIPARUM MALARIA IN BELU DISTRICT, EAST NUSA TENGGARA Asep Purnama et al, IJIM 2006:38;327-31
  • 23. RESULTS  Due to an increase in the chloroquine treatment failure rate to 47,62%, recruitment was terminated prematurely  A total of 95 of the originally recruited 203 patients were enrolled in the study  Artesunate-amodiaquine showed superior 28-day cure rate  Chloroquine versus artesunate-amodiaquine was 22/42 [52,38%] versus 49/53 [92,45%]; p<0,01  However , efficacy of As+Aq was <95%, below than WHO standard
  • 24. ARTESUNATE - AMODIAQUINE VERSUS CHLOROQUINE FOR THE TREATMENT OF VIVAX MALARIA IN MAUMERE, EAST NUSA TENGGARA National Institute of Health Research and Development, MOH, Jakarta
  • 25. RESULTS  A prospective comparative clinical trial of efficacy, safety and tolerability of As+Aq versus chloroquine for treatment of uncomplicated vivax malaria with a 28-day follow up  Of a total 105 enrolled patients there were 100 patients could be analysed  The efficacies of As+Aq and Chloroquine were 88% and 40,8% on day 28 by ITT and 93,2% and 47,2% by PP, respectively  However , efficacy of As+Aq was <95%, below than WHO standard
  • 26. NEED ALTERNATIVE ACTs ATS3+AQ3 QN7+Dx7/Clind  Efficacy <95% (Papua 70-87%)  Efficacy ?  AR: nausea and vomiting  AR: dizziness, tinnitus  Compliance? (no of pills)  Poor compliance  Cost and accessibility?
  • 27. IMPROVING ACT COMPLIANCE CURE RATE  Effective: rapid  Tolerate: tasteless  Safe: risk groups (infancy broad spectrum  Practice : all species and pregnancy) adverse events single dose only  Simple: fixed-dose regimen all age groups single daily dose/ single dose only
  • 28. CLINICAL TRIALS ON ACTs (ATS+PD)3 (ART+NTQ)1 VS Parentral ATM vs QN ATS3+AQ3 VS (DHA+PPQ)3 (ART+PPQ)2 (ATS+PD)3 vs ((ATM+LMF)3 CQ3 vs (CQ3+SP1) vs AQ3 IV ART vs QN (ATS+PD)3 vs (ART+NTQ)1 VS ((CQ)3 (ATM+LMF)3 VS (DHA+PPQ)3 (ATS+PD)3 vs (DHA+PP)Q3 ((ATM+LMF)3 ATS3+AQ3 VS (DHA+PPQ)3
  • 29. EFFICACY COMBO VS FIXED REGIMEN N=352 Artesunate+amodiaquine (ATS3+AQ3) vs Artemisinin+piperaquine (ART+PPQ)2 Pf: 93.8% vs 96.5% Pv:96.5% vs 100% (Tjitra E et al, 2005) 4 7 3.5 6 3 5 2.5 4 2 3 1.5 2 1 1 0.5 0 0 Day 0 Day 1 Day 2 Day 3 Day 7 Day 14 Day 21 Day 28 Day 0 Day 1 Day 2 Day 3 Day 7 Day 14 Day 21 Day 28 ATS3+AQ3 ART2+PPQ2 ATS3+AQ3 ART2+PPQ2
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  • 38. Artemisinin/naphtoquine P. vivax, P. falciparum, P.mix phase III trial A Phase III randomized, open label, non-inferiority trial of artemisinin plus naphtoquine (ARCO) versus dihydroartemisinin plus piperaquine in adult uncomplicated malaria patients: A Multi- centre study in Indonesia
  • 39. Artemisinin/naphtoquine phase III trial Study outline  401 patients randomized  Study duration: April 2007 – August 2008  Treatment : single dose, F/U to 42 days  Multicentre: 2 sites, 4 hospital  :
  • 40. Artemisinin/naphtoquine phase III trial Conclusions  The trial demonstrated non inferiority treatment study  Arco vs Duocotecxin  P. vivax 98,7% vs 97,3%  P. falciparum 98,7% vs 97,1%  Both new fixed-dose ACTs are confirmed very effective, safe and tolerate for treatment of any malaria in adults, and meet with the recent WHO recommendation for replacing ineffective drugs
  • 41. ARTEMISININ FOR SEVERE MALARIA ARTEMETHER QUININE DIHYDROCHLORIDE  FCT= 35.5 hours  FCT= 37.4 hours  PCT= 38.9 hours  PCT= 41.8 hours  Regain consciousness=  Regain consciousness = 32 hours 62.8 hours  CFR cerebral mal =  CFR cerebral mal = 71.4% 37.5%  Overall CFR= 23%  Overall CFR= 13% Tjitra E et al, MJI, 1996
  • 42. SEAQUAMAT TRIAL  Study design: Open label, multi centre, randomised, comparison of artesunate and quinine in severe falciparum malaria  Study sites: 2003-2005  Bangladesh  Indonesia (Timika Hospital, Timika)  India  Myanmar  Target sample size: 2,000 patients  1400 enrolled as at February 2005  Coordination: Wellcome Unit, Bangkok
  • 43. RESULTS (SEAQUAMAT Group, Lancet, 2005)  Trial stopped early (n=1461) by Safety Monitoring committee because clear benefit with artesunate  Overall reduction in mortality with artesunate 34.7% (95%CI 19-48%) p=0.0002  mortality quinine: 164/731 (22%)  mortality artesunate: 107/730 (15%)  Indonesian national policy change before the results published  Australian policy change 2006
  • 44. THE IMPORTANCE OF COOPERATION BETWEEN NEIGHBOURING COUNTRIES  Many health problems are cross border (malaria, rabies, filaria, DHF etc)  Limited resource: mutual cooperation important  Potential for inefficiency if countries work alone  Sharing expertise and facilities  Cooperation on research projects  Share results of individual research  Cooperation to develop guidelines or policy
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  • 52. MASS BLOOD SURVEY-YASPEM  Target 45.454 [3 kecamatan]  Blood sample taken 37.974 83,48 %  Results F 351 0,9 % V 517 1,4 % Mix 71 0,2 % Total 939 2,5 %
  • 53. DROP OUT  Adverse event 18 [1,9%]  Hospitalized 6 [0,6%]  Loss of follow up 8 [0,8%]  Reject to take medicine 12 [1,3%]
  • 54. SOME EXAMPLES OF POOR PRACTICE • Giving SP to patients with fever even though blood smear negative • Treating uncomplicated malaria with parenteral quinine or arthemeter im • Treating complicated malaria with chloroquine or ACT • Giving SP for P vivax malaria • Giving Primaquine 15 mg for 14 days for P falciparum malaria • Giving all available forms of treatment to the one patient
  • 55. SOME EXAMPLES OF POOR PRACTICE (contd) • Using RDT to evaluate response to treatment • Giving transfusion to malaria patients with mild anaemia • Using steroids to treat cerebral malaria • Inadequate fluid for complicated malaria • Postponing haemodialysis for complicated malaria with acute renal failure • Unawareness of hypoglycemia in complicated malaria • Not giving ACT for 3 days • Giving inadequate doses of artesunate or arthemeter