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Is there Artemisinin Resistance in Western Cambodia? Preliminary results, February 2008 Arjen Dondorp on behalf of the “Task Force on Antimalarial Drug Resistance in Cambodia”

31 march dundorp 1

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Is there Artemisinin Resistance in Western Cambodia?

Preliminary results, February 2008

Arjen Dondorp on behalf of the “Task Force on Antimalarial Drug Resistance in Cambodia”

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French Guiana 2002-2003; hypoxanthine uptake at 48 hours; no clinical data.Jambou et al. Lancet 2005; 366: 1960-63.

Artemether

S769N PfATPase6 mutation

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Cambodia 2001; hypoxanthine uptake at 48 hours.Jambou et al. Lancet 2005; 366: 1960-63.

Artesunate

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Antimalarial drug use in Western Cambodia

• 1955-9: DDT ± weekly mass drug administration

• 1960-61: Distribution of 77 tons of sea salt containing 0.05% pyrimethamine to a population of 20,000

• 1961-62: Distribution of 75 tons of salt containing 0.6% chloroquine

• Now: ACT (MAS3) first line treatment for uncomplicated falciparum malaria. However: substantial artesunate monotherapy use in the private sector

Verdrager 1986; Shunmay Yeung 2007

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ACT efficacy in Western Cambodia

• Coartem 28 day cure rate– Batambang 2002 (no food): 71.1% (but low day 7 blood levels)– Batambang 2003 (with food): 86.5%

• Artesunate-mefloquine 28 day cure rate– Batambang 2001: 96%– Pailin 2002: 86%– Batambang 2003: 92.4%– Pailin 2004: 90%– Trat province Thailand (just across the border) with a 2 days

regimen: 79%• Unconfirmed reports of prolonged parasite clearance

times (as PD measure for the artemisinins)

WHO 2007, TM&IH 2006;11:1800-07; Vijaykadga et al 2006

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Study site

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SCREENED: 92

INITIALLY ENROLLED: 43

ENROLLED: 40

EXCLUDED: 32 PARASiTAEMIA < 10,000/Ul

1 MIXED INFECTION

AS 2 MG/KG/DAY FOR 7 DAYS: 20

AS 4 MG/KG/DAY FOR 3 DAYSMQ 15&10 MG/KG/DAY DAY 3&4:

20

63 DAYS FOLLOW UP:20

63 DAYS FOLLOW UP: 1949 DAYS FOLLOW UP: 1

RECRUDESCENCE (Pf): 6 (30%)

(1 MIXED INFECTION)

REINFECTION (WITH MIXED Pf/Pv): 1

RECURRENT INFECTION (MIXED Pf/Pv):1

(genotyping follows)

RECURRENT INFECTION (Pv): 6

(1 MIXED INFECTION)

RECURRENT INFECTION (Pv): 7

(2 MIXED INFECTION)

CURE (FROM PRIMARY Pf INFECTION): 14

CURE(FROM PRIMARY Pf INFECTION): 19

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P (log-rank)=0.035

Genotyping will follow

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0 12 24 36 48 60 72 84 96 108

120

0.0001

0.001

0.01

0.1

1

10

100AS 2 mg/kgAS 4 mg/kg & MQ

time (hours)

para

sita

emia

as

% fr

om a

dmis

sion

(geo

met

ric m

ean)

parasite clearance curves (n=40)

0 12 24 36 48 60 72 84 96 108

120

0.001

0.01

0.1

1

10

100

1000black: AS7 (2mg/kg)red: MAS3 (4 mg/kg)green: relapse (all after AS7)

time (hours)

para

sita

emia

as

% fr

om a

dmis

sion

(indi

vidu

al d

ata)

FULLY SENSITIVE PARASITES

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Parasite reduction ratio at 48 hours

AS 2 mg/kg/dMedian (range): 114 (9-3956)

AS 4 mg/kg/d & MQMedian (range): 119 (10-1696)

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Parasite clearance time (hours)

AS 2 mg/kg/dMedian (range): 87 (42-120)

AS 4 mg/kg/d & MQMedian (range): 78 (36-114)

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0

10

20

30

40

104 105 106Prop

ortio

n (%

) par

asita

emic

at d

ay 3

(72h

)

Baseline parasitaemia (/uL)

50

Thai-Myanmar border, 2002-2006 n=1288

Cambodia-Thai border, 2007 Pailin; n=40 55% still parasitaemic at day 3

95%CI

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Gametocytocaemic during follow up: 8/40 (20%)(high compared to historical SMRU data (3%))

Arm Patient NoAdm.

P countGametocyte detection (Hour) PCT(Hour)

AS7(n=20) P002 25/1000 72 until 78 90

P013 2/1000 36 (once) 42

P022 9/1000 78 (once) 96

P035 4/1000 0 until 120 48MAS3(n=20) P015 7/1000 30 until 336 66

P027 24/1000 72 until 336 102

P029 9/1000 24 until 144 60

P034 3/1000 8 (once) 36

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No correlation PCT and IC50 (hypoxanthine uptake after 24 h)

Frederique Ariey, preliminary data

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• ‘Trophozoite inhibition assay’• Parasitemia/ 1000 red cells

and stage assessed• Parasite development assessed

in 200 asexual parasites• % trophozoites compared to

control well without drug.

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Kesinee Chotivanich, preliminary data

r2 =0.63

P=0.033

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Conclusions• Prolonged parasite clearance times confirmed,

with unacceptably high failure rate in AS7 arm• Not explained by inadequate drug levels;

variability in Cmax and AUC is considerable• No dose (or concentration)-response relationship

within current range of [AS]• Increased dose/ split dose? • No/ just 1 failure in MAS3 arm suggests continued

susceptibility to mefloquine• In vitro test under evaluation• Molecular marker?

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Acknowledgements

• Staff Pailin Referral Hospital• Mallika Imwong, Kesinee Chotivanich, Joel Tarning, Frederique

Ariey, Shunmay Yeung, Nick Day, Nick White• Staff of Mahidol - Oxford Tropical Medicine Research Unit • National Malaria Control Programme, Cambodia (Dr. Duong

Socheat)• Institut Pasteur, Pnomh Penh• AFRIMS, Bangkok• FHI, Bangkok• Li Ka Shing Foundation• WHO• Wellcome Trust

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Pailin, SW Cambodia

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Pailin clinical trial

• Inclusion:– Uncomplicated P. falciparum infection– Parasitaemia > 10,000/ uL– No mixed infection on light microscopy

• But 11/40 (28%) mixed Pf/Pv by PCR– No pregnancy– No previous antimalarial treatment (48H)

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Randomisation

• Artesunate 2 mg/kg bw per day for 7 days(AS7)

OR• Artesunate 4 mg/kg bw per day for 3 days

& mefloquine 15 and 10 mg/kg bw per day on day 3 and 4

(MAS3)

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Outcome measures

• Clinical and parasitological cure• Parasite clearance times• In vitro sensitivity tests• Molecular markers

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Molecular marker for artemisinin resistance?

• pfmdr1 mutation and copy no.• pfserca• pf mitochondrial DNA

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Single copy noMultiple copy no

Pfmdr1 copy no

$0

$0

$0

$0

$0

$1

$1

$1

$1

$1

$1

MaeSot06 Trat07 (n=32) Pailin06 (n=23) Pailin07 (n=40)

Freq

uenc

ies

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Pfserca SNP: full length sequence75 3132 3282 3580 3739 4068

89465464 759 847

pfserca mutation

0.00

0.20

0.40

0.60

0.80

1.00

1.20

I89T (n=17) 464(n=36) N465S(n=36) R759K (n=36) E847K (n=36)

Freq

uenc

ies

wild typemutant typeGap

SNP

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pf mitochondrial DNAcoxIII CoI CYTB

20474 1776772 2175

pf mitochondrial DNA (n=40)

0

0.1

0.2

0.3

0.4

0.5

0.6

0.7

0.8

0.9

A74T C204T G772A T1776C T2175C

Fre

qu

enci

es

wild type

mutant type

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0.1

1.0

10.0

100.0

1000.0

0 2 4 6 8 10 12

TIME (hr)

DHA

ARTS

ID=2, GROUP=AS7

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Dosing regimeEvery 12 hours for a week

daily

twice‐daily

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Molecular mechanisms of resistanceDrug Low to medium level

resistance High-level resistance

Chloroquine CRT; 76 CRT; 76 & othersMDR; 86, + others

Mefloquine, halofantrine, lumefantrine

MDR; amplification of wild-type gene

Pyrimethamine DHFR; 108 then 51 and 59 DHFR; 108 + 51 + 59 + 164

Cycloguanil, chlorcycloguanil DHFR; 16 + 108 DHFR; 108 + 51 + 59 + 164

Sulfonamides and sulfones DHPS; 436, 437, 540, 581, 614

Atovaquone None reported Cytochrome b; 133 ± 280

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DHA

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0 1 2 3 4 5 6 14 21 28 35 42 49 56 63

25

30

35

40

45

50

artesunate 2 mg/kg bs (for 7 days)artesunate 4 mg/kg bw (for 3 days) & mefloquine on day 4 and 5

Days after admission

Hae

mat

ocrit

(%, m

ean,

SD

)

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P. falciparum IC50 (ng/mL)Mean (95%CI)

Lab strain (TM267) 0.7 (0.5-0.9)

Isolates from

Pailin,Cambodia 13 (7-19)(N=9)

Mae Sot, Thailand 3.9 (0-16)(N=3)

Trophozoite inhibition IC50 (preliminary data)

Kesinee Chotivanich

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AS7 (2 mg/kg) MAS3 (4 mg/kg)DHA Mean % CV min max Mean % CV min max

Cmax (ng/mL) 802 75% 142 2780 1819 54% 771 4680AUC (hr*ng/mL) 1400 58% 482 4027 3543 29% 1708 5182C60min (ng/mL) 564 84% 6 1720 1103 71% 24 2570C90min (ng/mL) 469 60% 61 1100 1227 52% 141 2380C180min (ng/mL) 218 72 20 506 695 41% 211 1100

ARTS 20-300 foldCmax (ng/mL) 269 103% 28 897 411 91% 34 1620AUC (hr*ng/mL) 160 54% 53 340 317 48% 122 738C60min (ng/mL) 65 93% 0.3 244 252 141% 6 1620C90min (ng/mL) 27 80% 1.3 68 85 84% 3 260C180min (ng/mL) 6 131% 0 22 14 128% 0 54

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• Recrudescent P. falciparum infection:– N=6 (all in AS7 arm)

• Recrurrent P. falciparum infection:– N=1 (MAS3 arm; genotyping follows)

• Recurrent P. vivax infection:– N=13 (7 in AS7 arm; 6 in MAS3 arm)

• Recurrent mixed infection:– N=2 (1 in each arm, 1 included in total Pf recurrence;

1 still needs genotyping)

Summary of recurrent infections: