Your search keyword '"Prasetyorini B"' showing total 13 results

1. Amplification of pvmdr1 Associated with Multidrug-Resistant Plasmodium vivax

Author

Suwanarusk, R., Chavchich, M., Russell, B., Jaidee, A., Chalfein, F., Barends, M., Prasetyorini, B., Kenangalem, E., Piera, K. A., Lek-Uthai, U., Anstey, N. M., Tjitra, E., Nosten, F., Cheng, Q., and Price, R. N.

Published

2008

2. In Vivo and In Vitro efficacy of chloroquine against Plasmodium malariae and P. ovale in Papua, Indonesia

Author

Seswantoro H., Russell, Barry, Ratcliff, A., Prasetyorini, B., Chalfein, Ferryanto, Marfurt, Jutta, Kenangalem, Enny, Wuwung, M., Piera, Kim A., Ebsworth, E. P., Anstey, Nicholas M., Tjitra, Emiliana, Price, Ric N., Seswantoro H., Russell, Barry, Ratcliff, A., Prasetyorini, B., Chalfein, Ferryanto, Marfurt, Jutta, Kenangalem, Enny, Wuwung, M., Piera, Kim A., Ebsworth, E. P., Anstey, Nicholas M., Tjitra, Emiliana, and Price, Ric N.

Abstract

Reports of potential drug-resistant strains of Plasmodium malariae in western Indonesia raise concerns that chloroquine resistance may be emerging in P. malariae and P. ovale. In order to assess this, in vivo and in vitro efficacy studies were conducted in patients with monoinfection in Papua, Indonesia. Consecutive patients with uncomplicated malaria due to P. ovale or P. malariae were enrolled in a prospective clinical trial, provided with supervised chloroquine treatment, and followed for 28 days. Blood from patients with P. malariae or P. ovale parasitemia greater than 1,000 per microliter underwent in vitro antimalarial drug susceptibility testing using a modified schizont maturation assay. Of the 57 evaluable patients in the clinical study (P. malariae, n = 46; P. ovale, n = 11), none had recurrence with the same species during follow-up. The mean parasite reduction ratio at 48 h was 86 (95% confidence interval [CI], 57 to 114) for P. malariae and 150 (95% CI, 54 to 245) for P. ovale (P = 0.18). One patient infected with P. malariae, with 93% of parasites at the trophozoite stage, was still parasitemic on day 4. In vitro drug susceptibility assays were carried out successfully for 40 isolates (34 infected with P. malariae and 6 with P. ovale). The P. malariae infections at trophozoite stages had significantly higher chloroquine 50% effective concentrations (EC50s) (median, 127.9 nM [range, 7.9 to 2,980]) than those initially exposed at the ring stage (median, 14.0 nM [range, 3.5 to 27.0]; P = 0.01). The EC50 for chloroquine in P. ovale was also higher in an isolate initially at the trophozoite stage (23.2 nM) than in the three isolates predominantly at ring stage (7.8 nM). Chloroquine retains adequate efficacy against P. ovale and P. malariae, but its marked stage specificity of action may account for reports of delayed parasite clearance times.

Published

2011

3. Determinants of In Vitro Drug Susceptibility Testing of Plasmodium vivax

Author

Russell, Bruce, Chalfein, Ferryanto, Prasetyorini, B., Kenangalem, Enny, Piera, Kim A., Suwanarusk, Rossarin, Brockman, Alan, Prayoga, Pak, Sugiarto, P., Cheng, Qi, Tjitra, Emiliana, Anstey, Nicholas M., Price, Erin P., Russell, Bruce, Chalfein, Ferryanto, Prasetyorini, B., Kenangalem, Enny, Piera, Kim A., Suwanarusk, Rossarin, Brockman, Alan, Prayoga, Pak, Sugiarto, P., Cheng, Qi, Tjitra, Emiliana, Anstey, Nicholas M., and Price, Erin P.

Abstract

In Papua, Indonesia, the antimalarial susceptibility of Plasmodium vivax (n = 216) and P. falciparum (n = 277) was assessed using a modified schizont maturation assay for chloroquine, amodiaquine, artesunate, lumefantrine, mefloquine, and piperaquine. The most effective antimalarial against P. vivax and P. falciparum was artesunate, with geometric mean 50% inhibitory concentrations (IC50s) (95% confidence intervals [CI]) of 1.31 nM (1.07 to 1.59) and 0.64 nM (0.53 to 0.79), respectively. In contrast, the geometric mean chloroquine IC50 for P. vivax was 295 nM (227 to 384) compared to only 47.4 nM (42.2 to 53.3) for P. falciparum. Two factors were found to significantly influence the in vitro drug response of P. vivax: the initial stage of the parasite and the duration of the assay. Isolates of P. vivax initially at the trophozoite stage had significantly higher chloroquine IC50s (478 nM [95% CI, 316 to 722]) than those initially at the ring stage (84.7 nM [95% CI, 45.7 to 157]; P < 0.001). Synchronous isolates of P. vivax and P. falciparum which reached the target of 40% schizonts in the control wells within 30 h had significantly higher geometric mean chloroquine IC50s (435 nM [95% CI, 169 to 1,118] and 55.9 nM [95% CI, 48 to 64.9], respectively) than isolates that took more than 30 h (39.9 nM [14.6 to 110.4] and 36.9 nM [31.2 to 43.7]; P < 0.005). The results demonstrate the marked stage-specific activity of chloroquine with P. vivax and suggest that susceptibility to chloroquine may be associated with variable growth rates. These findings have important implications for the phenotypic and downstream genetic characterization of P. vivax.

Published

2008

4. Amplification of pvmdr1 Associated with Multidrug-Resistant Plasmodium vivax

Author

Suwanarusk, Rossarin, Chavchich, M., Russell, B., Jaidee, A., Chalfein, Ferryanto, Barends, M., Prasetyorini, B., Kenangalem, Enny, Piera, Kim A., Lek-uthai, U., Anstey, Nicholas M., Tjitra, Emiliana, Nosten, F.., Cheng, Qi, Price, Ric N., Suwanarusk, Rossarin, Chavchich, M., Russell, B., Jaidee, A., Chalfein, Ferryanto, Barends, M., Prasetyorini, B., Kenangalem, Enny, Piera, Kim A., Lek-uthai, U., Anstey, Nicholas M., Tjitra, Emiliana, Nosten, F.., Cheng, Qi, and Price, Ric N.

Published

2008

5. In Vivo and In Vitro Efficacy of Chloroquine against Plasmodium malariae and P. ovale in Papua, Indonesia

Author

Siswantoro, H., primary, Russell, B., additional, Ratcliff, A., additional, Prasetyorini, B., additional, Chalfein, F., additional, Marfurt, J., additional, Kenangalem, E., additional, Wuwung, M., additional, Piera, K. A., additional, Ebsworth, E. P., additional, Anstey, N. M., additional, Tjitra, E., additional, and Price, R. N., additional

Published

2011

6. Amplification ofpvmdr1Associated with Multidrug‐ResistantPlasmodium vivax

Author

Suwanarusk, R., primary, Chavchich, M., additional, Russell, B., additional, Jaidee, A., additional, Chalfein, F., additional, Barends, M., additional, Prasetyorini, B., additional, Kenangalem, E., additional, Piera, K. A., additional, Lek‐Uthai, U., additional, Anstey, N. M., additional, Tjitra, E., additional, Nosten, F., additional, Cheng, Q., additional, and Price, R. N., additional

Published

2008

7. Determinants of In Vitro Drug Susceptibility Testing of Plasmodium vivax

Author

Russell, B., primary, Chalfein, F., additional, Prasetyorini, B., additional, Kenangalem, E., additional, Piera, K., additional, Suwanarusk, R., additional, Brockman, A., additional, Prayoga, P., additional, Sugiarto, P., additional, Cheng, Q., additional, Tjitra, E., additional, Anstey, N. M., additional, and Price, R. N., additional

Published

2008

8. In Vivo and In Vitro Efficacy of Chloroquine against Plasmodium malariae and P. ovale in Papua, Indonesia

Author

Siswantoro, H., Russell, B., Ratcliff, A., Prasetyorini, B., Chalfein, F., Marfurt, J., Kenangalem, E., Wuwung, M., Piera, K. A., Ebsworth, E. P., Anstey, N. M., Tjitra, E., and Price, R. N.

Abstract

Reports of potential drug-resistant strains of Plasmodium malariae in western Indonesia raise concerns that chloroquine resistance may be emerging in P. malariae and P. ovale. In order to assess this, in vivo and in vitro efficacy studies were conducted in patients with monoinfection in Papua, Indonesia. Consecutive patients with uncomplicated malaria due to P. ovale or P. malariae were enrolled in a prospective clinical trial, provided with supervised chloroquine treatment, and followed for 28 days. Blood from patients with P. malariae or P. ovale parasitemia greater than 1,000 per microliter underwent in vitro antimalarial drug susceptibility testing using a modified schizont maturation assay. Of the 57 evaluable patients in the clinical study (P. malariae, n = 46; P. ovale, n = 11), none had recurrence with the same species during follow-up. The mean parasite reduction ratio at 48 h was 86 (95% confidence interval [CI], 57 to 114) for P. malariae and 150 (95% CI, 54 to 245) for P. ovale (P = 0.18). One patient infected with P. malariae, with 93% of parasites at the trophozoite stage, was still parasitemic on day 4. In vitro drug susceptibility assays were carried out successfully for 40 isolates (34 infected with P. malariae and 6 with P. ovale). The P. malariae infections at trophozoite stages had significantly higher chloroquine 50% effective concentrations (EC50s) (median, 127.9 nM [range, 7.9 to 2,980]) than those initially exposed at the ring stage (median, 14.0 nM [range, 3.5 to 27.0]; P = 0.01). The EC50for chloroquine in P. ovale was also higher in an isolate initially at the trophozoite stage (23.2 nM) than in the three isolates predominantly at ring stage (7.8 nM). Chloroquine retains adequate efficacy against P. ovale and P. malariae, but its marked stage specificity of action may account for reports of delayed parasite clearance times.

Published

2010

9. In Vivoand In VitroEfficacy of Chloroquine against Plasmodium malariaeand P. ovalein Papua, Indonesia

Author

Siswantoro, H., Russell, B., Ratcliff, A., Prasetyorini, B., Chalfein, F., Marfurt, J., Kenangalem, E., Wuwung, M., Piera, K. A., Ebsworth, E. P., Anstey, N. M., Tjitra, E., and Price, R. N.

Abstract

ABSTRACTReports of potential drug-resistant strains of Plasmodium malariaein western Indonesia raise concerns that chloroquine resistance may be emerging in P. malariaeand P. ovale. In order to assess this, in vivoand in vitroefficacy studies were conducted in patients with monoinfection in Papua, Indonesia. Consecutive patients with uncomplicated malaria due to P. ovaleor P. malariaewere enrolled in a prospective clinical trial, provided with supervised chloroquine treatment, and followed for 28 days. Blood from patients with P. malariaeor P. ovaleparasitemia greater than 1,000 per microliter underwent in vitroantimalarial drug susceptibility testing using a modified schizont maturation assay. Of the 57 evaluable patients in the clinical study (P. malariae, n= 46; P. ovale, n= 11), none had recurrence with the same species during follow-up. The mean parasite reduction ratio at 48 h was 86 (95% confidence interval [CI], 57 to 114) for P. malariaeand 150 (95% CI, 54 to 245) for P. ovale(P= 0.18). One patient infected with P. malariae, with 93% of parasites at the trophozoite stage, was still parasitemic on day 4. In vitrodrug susceptibility assays were carried out successfully for 40 isolates (34 infected with P. malariaeand 6 with P. ovale). The P. malariaeinfections at trophozoite stages had significantly higher chloroquine 50% effective concentrations (EC50s) (median, 127.9 nM [range, 7.9 to 2,980]) than those initially exposed at the ring stage (median, 14.0 nM [range, 3.5 to 27.0]; P= 0.01). The EC50for chloroquine in P. ovalewas also higher in an isolate initially at the trophozoite stage (23.2 nM) than in the three isolates predominantly at ring stage (7.8 nM). Chloroquine retains adequate efficacy against P. ovaleand P. malariae, but its marked stage specificity of action may account for reports of delayed parasite clearance times.

Published

2010

10. In vitro and molecular characterisation of multidrug resistant Plasmodium vivax

Author

Suwanarusk, R., Bruce Russell, Chavchich, M., Chalfein, F., Kenangalem, E., Kosaisavee, V., Prasetyorini, B., Piera, K. A., Barends, M., Brockman, A., Lek-Uthai, U., Tjitra, E., Nosten, F., Anstey, N. M., Cheng, Q., and Price, R. N.

11. Efficacy and safety of artemisinin-naphthoquine versus dihydroartemisinin-piperaquine in adult patients with uncomplicated malaria: a multi-centre study in Indonesia

Author

Tjitra Emiliana, Hasugian Armedy R, Siswantoro Hadjar, Prasetyorini Budi, Ekowatiningsih Riyanti, Yusnita Endah A, Purnamasari Telly, Driyah Srilaning, Salwati Ervi, Yuwarni Eni, Januar Lidwina, Labora Joseph, Wijayanto Bambang, Amansyah Fajar, Dedang Tersila AD, and Purnama Asep

Subjects

Malaria, Artemisinin-naphthoquine, Dihydroartemisinin-piperaquine, Efficacy, Safety, Arctic medicine. Tropical medicine, RC955-962, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background A practical and simple regimen for all malaria species is needed towards malaria elimination in Indonesia. It is worth to compare the efficacy and safety of a single dose of artemisinin-naphthoquine (AN) with a three-day regimen of dihydroartemisinin-piperaquine (DHP), the existing programme drug, in adults with uncomplicated symptomatic malaria. Methods This is a phase III, randomized, open label using sealed envelopes, multi-centre, comparative study between a single dose of AN and a three-day dose of DHP in Jayapura and Maumere. The modified WHO inclusion and exclusion criteria for efficacy study were used in this trial. A total of 401 eligible adult malaria subjects were hospitalized for three days and randomly treated with AN four tablets single dose on day 0 or DHP three to four tablets single daily dose for three days, and followed for 42 days for physical examination, thick and thin smears microscopy, and other necessary tests. The efficacy of drug was assessed by polymerase chain reaction (PCR) uncorrected and corrected. Results There were 153 Plasmodium falciparum, 158 Plasmodium vivax and 90 P. falciparum/P. vivax malaria. Mean of fever clearance times were similar, 13.0 ± 10.3 hours in AN and 11.3 ± 7.3 hours in DHP groups. The mean of parasite clearance times were longer in AN compared with DHP (28.0 ± 11.7 hours vs 25.5 ± 12.2 hours, p = 0.04). There were only 12 PCR-corrected P. falciparum late treatment failures: seven in AN and five in DHP groups. The PCR uncorrected and corrected on day −42 of adequate clinical and parasitological responses for treatment of any malaria were 93.7% (95% Cl: 90.3–97.2) and 96.3% (95% Cl: 93.6–99.0) in AN, 96.3% (95% Cl: 93.5–99.0) and 97.3% (95% Cl: 95.0–99.6) in DHP groups. Few and mild adverse events were reported. All the abnormal haematology and blood chemistry values had no clinical abnormality. Conclusion AN and DHP are confirmed very effective, safe and tolerate for treatment of any malaria. Both drugs are promising for multiple first-line therapy policies in Indonesia.

Published

2012

12. Prevalence of Glucose 6-Phosphate Dehydrogenase Variants in Malaria-Endemic Areas of South Central Timor, Eastern Indonesia.

Author

Sulistyaningrum N, Arlinda D, Hutagalung J, Sunarno S, Oktoberia IS, Handayani S, Ekowatiningsih R, Yusnita EA, Prasetyorini B, Rizki A, Tjitra E, Na-Bangchang K, and Chaijaroenkul W

Subjects

Adult, Anemia, Hemolytic genetics, Child, Endemic Diseases, Female, Genetic Variation, Genotype, Glucosephosphate Dehydrogenase Deficiency epidemiology, Humans, Indonesia epidemiology, Male, Polymerase Chain Reaction, Polymorphism, Restriction Fragment Length, Sex Factors, Anemia, Hemolytic chemically induced, Antimalarials adverse effects, Glucosephosphate Dehydrogenase genetics, Glucosephosphate Dehydrogenase Deficiency genetics, Malaria, Falciparum drug therapy, Malaria, Vivax drug therapy, Primaquine adverse effects

Abstract

Primaquine is an effective anti-hypnozoite drug for Plasmodium vivax and Plasmodium ovale. However, it can trigger erythrocyte hemolysis in people with glucose 6-phosphate dehydrogenase (G6PD) deficiency. In a previous report from South Central Timor (SCT), Indonesia, we described the prevalence of Vanua Lava, Chatham, and Viangchan variants; in this study, other G6PD variants (Kaiping, Coimbra, Gaohe, Canton, and Mahidol) were subsequently analyzed. For clarity, all of these results are described together. The 381 DNA samples from the previous study during 2013-2014 were analyzed for G6PD variants by using PCR-restriction fragment length polymorphism (RFLP). The prevalence of G6PD deficiency in SCT was 6.3% (24/381 cases), including 4.2% (16/381 cases), 0.5% (2/381 cases), and 1.6% (6/381 cases) for Coimbra, Kaiping, and Vanua Lava variants, respectively. No other variants were found in this population. A significant association was found between ethnicity and the distribution of G6PD Kaiping in female subjects. A positive association was shown between G6PD activity and heterozygous females carrying Coimbra genotype, hemizygous males carrying Vanua Lava, Plasmodium falciparum infection in female subjects, and P. vivax infection in male subjects. Further molecular analysis of heterozygous females, particularly in malaria-endemic areas, is needed for mapping distribution of G6PD deficiency status in Indonesia.

Published

2020

13. Chloroquine resistant Plasmodium vivax: in vitro characterisation and association with molecular polymorphisms.

Author

Suwanarusk R, Russell B, Chavchich M, Chalfein F, Kenangalem E, Kosaisavee V, Prasetyorini B, Piera KA, Barends M, Brockman A, Lek-Uthai U, Anstey NM, Tjitra E, Nosten F, Cheng Q, and Price RN

Subjects

Animals, Genetic Variation, Humans, Indonesia, Inhibitory Concentration 50, Models, Biological, Parasitic Sensitivity Tests, Polymorphism, Genetic, Polymorphism, Single Nucleotide, Protozoan Proteins chemistry, Antimalarials pharmacology, Chloroquine pharmacology, Drug Resistance, Malaria, Vivax parasitology, Plasmodium vivax metabolism

Abstract

Background: Treatment failure of chloroquine for P. vivax infections has reached high levels in the eastern provinces of Indonesia, however, in vitro characterization of chloroquine resistance and its associated molecular profile have yet to be determined., Methods: Using a modified schizont maturation assay we investigated the in vitro chloroquine susceptibility profile and molecular polymorphisms of P. vivax isolates collected from Papua, Indonesia, where high levels of clinical chloroquine treatment failure have been reported, and from Thailand, where chloroquine treatment is generally effective., Results: The geometric mean chloroquine IC(50) for P. vivax isolates from Papua (n = 145) was 312 nM [95%CI: 237-411 nM] compared to 46.8 nM [95%CI: 34.7-63.1 nM] from Thailand (n = 81); p<0.001. Correlating with the known clinical efficacy of the area, a cut off for chloroquine resistance was defined as 220 nM, a level exceeded in 13.6% (11/81) of Thai isolates and 65% (94/145) of Papuan isolates; p<0.001. Several sequence polymorphisms in pvcrt-o and pvmdr1, and difference in pvmdr1 copy number were identified. A Y976F mutation in pvmdr1 was present in 96% (123/128) of Papuan isolates and 25% (17/69) of Thai isolates; p<0.001. Overall, the geometric mean chloroquine IC(50) in isolates with the Y976F mutation was 283 nM [95%CI: 211-379], compared to 44.5 nM [95%CI: 31.3-63.4] in isolates with the wild type; p< 0.001. Pvmdr1 amplification occurred in 23% (15/66) of Thai isolates compared to none (0/104) of Indonesian isolates (p<0.001), but was not associated with increased chloroquine resistance after controlling for geographical location., Conclusions: In vitro susceptibility testing of P. vivax discriminates between populations with differing levels of clinical efficacy of chloroquine. The pvmdr1 polymorphism at Y976F may provide a useful tool to highlight areas of emerging chloroquine resistance, although further studies defining its clinical correlates are needed.

Published

2007