| Literature DB >> 21914160 |
Carrie A Morris1, Stephan Duparc, Isabelle Borghini-Fuhrer, Donald Jung, Chang-Sik Shin, Lawrence Fleckenstein.
Abstract
Artesunate (AS) is a clinically versatile artemisinin derivative utilized for the treatment of mild to severe malaria infection. Given the therapeutic significance of AS and the necessity of appropriate AS dosing, substantial research has been performed investigating the pharmacokinetics of AS and its active metabolite dihydroartemisinin (DHA). In this article, a comprehensive review is presented of AS clinical pharmacokinetics following administration of AS by the intravenous (IV), intramuscular (IM), oral or rectal routes. Intravenous AS is associated with high initial AS concentrations which subsequently decline rapidly, with typical AS half-life estimates of less than 15 minutes. AS clearance and volume estimates average 2 - 3 L/kg/hr and 0.1 - 0.3 L/kg, respectively. DHA concentrations peak within 25 minutes post-dose, and DHA is eliminated with a half-life of 30 - 60 minutes. DHA clearance and volume average between 0.5 - 1.5 L/kg/hr and 0.5 - 1.0 L/kg, respectively. Compared to IV administration, IM administration produces lower peaks, longer half-life values, and higher volumes of distribution for AS, as well as delayed peaks for DHA; other parameters are generally similar due to the high bioavailability, assessed by exposure to DHA, associated with IM AS administration (> 86%). Similarly high bioavailability of DHA (> 80%) is associated with oral administration. Following oral AS, peak AS concentrations (Cmax) are achieved within one hour, and AS is eliminated with a half-life of 20 - 45 minutes. DHA Cmax values are observed within two hours post-dose; DHA half-life values average 0.5 - 1.5 hours. AUC values reported for AS are often substantially lower than those reported for DHA following oral AS administration. Rectal AS administration yields pharmacokinetic results similar to those obtained from oral administration, with the exceptions of delayed AS Cmax and longer AS half-life. Drug interaction studies conducted with oral AS suggest that AS does not appreciably alter the pharmacokinetics of atovaquone/proguanil, chlorproguanil/dapsone, or sulphadoxine/pyrimethamine, and mefloquine and pyronaridine do not alter the pharmacokinetics of DHA. Finally, there is evidence suggesting that the pharmacokinetics of AS and/or DHA following AS administration may be altered by pregnancy and by acute malaria infection, but further investigation would be required to define those alterations precisely.Entities:
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Year: 2011 PMID: 21914160 PMCID: PMC3180444 DOI: 10.1186/1475-2875-10-263
Source DB: PubMed Journal: Malar J ISSN: 1475-2875 Impact factor: 2.979
Summary of AS pharmacokinetic results following IV AS administration.
| Subjects & Regimen | Cmax (ng/mL) | Clearance (L/kg/hr) | Volume (L/kg) | Half-life (min) | AUC (ng*hr/mL) | |
|---|---|---|---|---|---|---|
| [ | 12 Vietnamese adults with vivax malaria | 13685†a | 3.01 | 0.16 | 2.19 | 876† |
| [ | 17 healthy Vietnamese volunteers; subjects randomized into two groups, both receiving: | 3.0; 2.2 | 0.19; 0.16 | 2.6; 3.3 | 846; 1269† | |
| [ | 23 Vietnamese adults with uncomplicated falciparum malaria; subjects randomized into two groups, both receiving: | 16146; | 2.8; 2.1 | 0.22 | 3.2 | 1038; 1230† |
| [ | 30 healthy volunteers | 4797; 6128; 19420; 36100; 83340 | 1.3; 18; 1.3; 1.4; 1.6† | Vss: 0.092; 0.187; 0.106; 0.109; 0.165† | 7.2; 8.4; 14.4; 9.0; 12.6† | 386; 593; 1595; 3038; 6994† |
| [ | 28 paediatric Gabonese patients with severe malaria randomized into two groups | Group 1: 29677a | Group 1: | Group 1 Vss: 0.17†a | Group 1: 1.5a | Group 1: |
| [ | 17 adults with severe falciparum malaria in Thailand | 130+†a | 64a | Vss: | 13.2+†a | 49.2†a |
| [ | 26 adult uncomplicated falciparum malaria patients in Vietnam | 2.33a | 0.140a | 2.73 | 1146† | |
| [ | 30 parasitaemic adults with falciparum malaria | Group 1: | Group 1: | Group 1: | ||
Values given as mean unless otherwise specified.
†Units converted to uniform scale +The authors note that Cmax is likely underestimated and half-life overestimated due to the lack of usable data from six patients with extremely rapid AS elimination. a.Median
Summary of DHA pharmacokinetic results following IV AS administration.
| Subjects & Regimen | Cmax (ng/mL) | Tmax (min) | Clearance (L/kg/hr) | Volume (L/kg) | Half-life (min) | AUC (ng*hr/mL) | |
|---|---|---|---|---|---|---|---|
| [ | 12 Vietnamese adults with vivax malaria | 2192†a | 8a | 1.10 | 0.92 | 36.7 | 1845† |
| [ | 17 healthy Vietnamese volunteers; subjects randomized into two groups, both receiving: | 1507; 1678† | 9; 16 | 53; 47 | |||
| [ | 23 Vietnamese adults with uncomplicated falciparum malaria; subjects randomized into two groups, both receiving: | 2758; 2730†a | 7; 9a | 0.64; 0.48 | 0.8; 0.55 | 59; 50 | 2872; 3298† |
| [ | 30 healthy volunteers | 428; 802; 1286; 3148; 4744 | 9.6; 15; 9.6; 7.2; 24† | 1.3; 0.98; 1.1; 0.86; 0.82† | Vss: 1.734; 2.201; 1.860; 1.701; 2.403† | 57.6; 92.4; 69.0; 82.2; 128.4† | 385; 1082; 1850; 4886; 10410 |
| [ | 28 paediatric Gabonese patients with severe malaria randomized into two groups | Group 1: | Group 1: | Group 1: | Group 1 | Group 1: | Group 1: |
| [ | 17 adults with severe falciparum malaria in Thailand | 605†a | Tmax reached by 15 min | 5.6a | Vss: 1.9a | 20.4†a | 418†a |
| [ | 26 adult uncomplicated falciparum malaria patients in Vietnam | 2648†a | 9.0a | 0.75a | 0.76 | 40.2 | 2377† |
| [ | 30 parasitaemic adults with falciparum malaria | Group 1: | Group 1: | Group 1: | Group 1: | Group 1: 40.0 | Group 1: |
| Krishna | 34 Ghanaian children (8 months - 7 years) with moderate falciparum malaria | Groups 1 & 2: | Groups 1 & 2: | Groups 1 & 2: | Groups 1 & 2: | Groups 1 & 2: | Groups 1 & 2: |
Values given as mean unless otherwise specified.
†Units converted to uniform scale a. Median
Summary of AS pharmacokinetic results following IM AS administration.
| Subjects & Regimen | Cmax (ng/mL) | Tmax (min) | Clearance (L/kg/hr) | Volume (L/kg) | Half-life (min) | AUC (ng*hr/mL) | |
|---|---|---|---|---|---|---|---|
| [ | 11 Vietnamese adults with uncomplicated falciparum malaria | 884†a | 12a | 2.9 | 2.6 | 41 | 999† |
| [ | 9 Vietnamese adults with severe falciparum malaria | 2195†a | 2.84a | 1.09a | 30a | 856†a | |
| [ | 28 paediatric Gabonese patients with severe malaria randomized into two groups | Group 1: | Group 1: | Group 1: | Group 1 Vss/F: 2.07a | Group 1: | Group 1: |
Values given as mean unless otherwise specified.
†Units converted to uniform scale a. Median
Summary of DHA pharmacokinetic results following IM AS administration.
| Subjects & Regimen | Cmax (ng/mL) | Tmax (min) | Clearance (L/kg/hr) | Volume (L/kg) | Half-life (min) | AUC (ng*hr/mL) | |
|---|---|---|---|---|---|---|---|
| [ | 11 Vietnamese adults with uncomplicated falciparum malaria | 1166†a | 45a | 0.73 | 1.1 | 64 | 2474† |
| [ | 9 Vietnamese adults with severe falciparum malaria | 870†a | 35a | 1.18a | 1.79a | 52.7a | 1496†a |
| [ | 28 paediatric Gabonese patients with severe malaria randomized into two groups | Group 1: | Group 1: | Group 1: | Group 1: | Group 1: | Group 1: |
Values given as mean unless otherwise specified.
†Units converted to uniform scale a. Median
Artesunate Tmax values obtained following oral artesunate administration.
| Subjects | Regimen | Tmax (hours) | |
|---|---|---|---|
| [ | 15 healthy Cambodian male adults | 4 mg/kg AS once with mefloquine | 0.75a |
| [ | 8 healthy adults in Australia | 150 mg AS once | 0.65 (n = 6)a |
| [ | 20 healthy adult males in Australia | 200 mg/day × 3 days alone (Period 1); repeated with mefloquine after washout (Period 2) | Period 1/Day 1: 0.6b |
| [ | 6 healthy adults in Geneva | 200 mg AS once | 0.25 (5/6 subjects) |
| [ | 23 healthy Malaysian adults | 200 mg AS once with amodiaquine as fixed or non-fixed product | Fixed:0.26 |
| [ | 13 healthy adults in Africa | Mean dose: 4.26 mg/kg with (ACT) or without (AS only) amodiaquine as single dose | AS only: 0.62 |
| [ | 8 healthy male Thai adults | 300 mg AS (Guilin or Arenco formulation) | Guilin: 0.25a |
| [ | 10 healthy male Vietnamese adults | 200 mg AS once daily × 5 days | Day 1: 0.8a |
| [ | 12 healthy male Malaysian adults | 200 mg AS once | 0.66 ± 0.34 |
| [ | 11 male Thai adults with uncomplicated falciparum malaria | 200 mg AS once, followed by 100 mg 12 hours later, then 100 mg once daily for another 4 days | Acute: 0.5a |
| [ | 43 adults with uncomplicated falciparum malaria in Thailand | AS+mefloquine as fixed (200 mg AS) or nonfixed (4 mg/kg AS) combination | Fixed:0.833 (n = 19) |
| [ | 13 male and female adult patients in the DRC with acute uncomplicated falciparum malaria | 200 mg AS once daily × 3 days with amodiaquine | 1.4 (n = 10) |
| [ | 86 acute uncomplicated falciparum malaria patients from Malawi and Gambia | 1, 2, or 4 mg/kg AS with chlorproguanil and dapsone once daily × 3 days | 1 mg/kg: 1.08a |
| [ | 6 male Thai adults with uncomplicated falciparum malaria and 6 healthy male adults | 100 mg AS once | Healthy: 0.71 |
| [ | 57 children (2-14 years) with uncomplicated falciparum malaria in Gabon | AS dose (mg/kg/day) with pyronaridine | Group A:0.6 |
| [ | 40 children and adults with uncomplicated falciparum malaria in Pailin, Cambodia and 40 adults with uncomplicated falciparum malaria in Wang Pha, Thailand | At each site: | Thailand: |
Values given as mean unless otherwise specified.
a. Median b. Geometric mean
Artesunate half-life values following oral artesunate administration.
| Subjects | Artesunate regimen | Artesunate half-life (hours) | |
|---|---|---|---|
| [ | 10 healthy male Vietnamese adults | 200 mg once daily × 5 days | Day 1: 0.43a |
| [ | 12 healthy male Malaysian adults | 200 mg single dose | 0.49 |
| [ | 8 healthy male Thai adults | 300 mg AS (Guilin or Arenco formulation) | Guilin:0.53 |
| [ | 23 healthy Malaysian adults | 200 mg AS + amodiaquine as fixed or non-fixed product | Fixed:0.63 |
| [ | 86 acute uncomplicated falciparum malaria patients from Malawi and Gambia | 1, 2, or 4 mg/kg AS + chlorproguanil and dapsone once daily × 3 days | 1 mg/kg: 0.515b |
| [ | 11 male Thai adults with uncomplicated falciparum malaria | 200 mg AS once, followed by 100 mg 12 hours later, then 100 mg once daily × 4 days | Acute: 0.36a |
| [ | 6 male Thai adults with uncomplicated falciparum malaria and 6 healthy male adults | 100 mg AS once | Healthy: 0.41 |
| [ | 57 children (2-14 years) with uncomplicated falciparum malaria in Gabon | AS dose (mg/kg) with pyronaridine | Group A: 0.8 (n = 12) |
| [ | 40 children and adults with uncomplicated falciparum malaria in Pailin, Cambodia and 40 adults with uncomplicated falciparum malaria in Wang Pha, Thailand | At each site: | Thailand: |
Value given as mean unless otherwise specified.
a. Median b. Geometric mean
Artesunate and DHA AUC and Cmax values following oral artesunate administration.
| Subjects | Oral AS regimen | AUC (ng*hr/mL) | Cmax (ng/mL) | |
|---|---|---|---|---|
| [ | 10 healthy male Vietnamese adults | 200 mg once daily × 5 days | ASa | ASa |
| DHAa | DHA | |||
| [ | 12 healthy male Malaysian adults | 200 mg AS once | AS | AS |
| DHA | DHA | |||
| [ | 13 healthy adults in Africa | Mean dose: 4.26 mg/kg with (ACT) or without (AS only) amodiaquine single dose | AS | AS |
| DHA | DHA | |||
| [ | 8 healthy male Thai adults | 300 mg AS | AS | AS |
| DHA | DHA | |||
| [ | 8 healthy adults in Australia | 150 mg once | AS | ASa |
| DHA | DHAa | |||
| [ | 23 healthy Malaysian adults | 200 mg once with amodiaquine as fixed or non-fixed product | AS† | AS† |
| DHA† | DHA† | |||
| [ | 86 acute uncomplicated falciparum malaria patients from Malawi and Gambia | 1, 2, or 4 mg/kg AS with chlorproguanil and dapsone once daily × 3 days | ASb | ASb |
| DHAb | DHAb | |||
| [ | 21 children (5 - 13 years) with uncomplicated malaria in Uganda | 4 mg/kg once daily with amodiaquine × 3 days | AS | AS 51 (data pooled from all subjects) |
| DHAa | DHAa | |||
| [ | 43 adults with uncomplicated falciparum malaria in Thailand | 200 mg/day for fixed dose AS-mefloquine tablet (n = 20) or 4 mg/kg/day as nonfixed (n = 23) AS-mefloquine | AS | AS |
| DHA | DHA | |||
| [ | 6 male Thai adults with uncomplicated falciparum malaria and 6 healthy male adults | 100 mg AS once | AS | AS |
| DHA | DHA | |||
| [ | 57 children (2-14 years) with uncomplicated falciparum malaria in Gabon | AS dose (mg/kg) | AS | AS |
| Administered with pyronaridine | DHA | DHA | ||
| [ | 40 children and adults with uncomplicated falciparum malaria in Pailin, Cambodia and 40 adults with uncomplicated falciparum malaria in Wang Pha, Thailand | At each site: | AS†a | AS†a |
| DHA†a | DHA†a | |||
Values given as mean unless otherwise specified.
†Units converted to uniform scale a. Median b. Geometric mean
DHA half-life values obtained following artesunate administration.
| Subjects | Artesunate regimen | DHA half-life (hours) | |
|---|---|---|---|
| [ | 10 healthy male Vietnamese adults | 200 mg once daily × 5 days | 0.87 (from pooled data) |
| [ | 12 healthy male Malaysian adults | 200 mg single dose | 0.49 |
| [ | 20 male and female healthy Thai adults | 4 mg/kg once | 0.74a |
| [ | 13 healthy adults in Africa | Mean dose: 4.26 mg/kg with (ACT) or without (AS only) amodiaquine single dose | AS only:1.46 |
| [ | 8 healthy male Thai adults | 300 mg AS (Guilin or Arenco formulation) | Guilin: 1.77 |
| [ | 10 healthy Vietnamese males | 100 mg AS once | Half-life: 0.55b |
| [ | 6 healthy adults in Geneva | 200 mg AS once | 0.65 |
| [ | 23 healthy Malaysian adults | 200 mg once with amodiaquine as fixed or non-fixed product | Fixed:1.68 |
| [ | 20 healthy adult males in Australia | 200 mg/day × 3 days alone (Period 1); repeated with mefloquine after washout (Period 2) | Period 1/Day 1: 1.14 |
| [ | 15 healthy Cambodian male adults | 4 mg/kg once with mefloquine | 1.30b |
| [ | 12 healthy adults | 200 mg once | 0.68 |
| [ | 86 acute uncomplicated falciparum malaria patients from Malawi and Gambia | 1, 2, or 4 mg/kg AS with chlorproguanil and dapsone once daily × 3 days | 1 mg/kg: 0.779b |
| [ | 12 Vietnamese adult male vivax malaria patients | 100 mg single dose | 0.67 (n = 11) |
| [ | 26 Vietnamese adult patients with uncomplicated falciparum malaria | 100 mg single dose | 0.66 (n = 16) |
| [ | 21 children (5 - 13 years) with uncomplicated malaria in Uganda | 4 mg/kg once daily with amodiaquine × 3 days | 1.3a |
| [ | 24 children with uncomplicated falciparum malaria in Gabon | 4 mg/kg once daily for 3 days in one of two formulations (blister pack and fixed dose) of AS/mefloquine | Fixed dose: 0.9(n = 9)a |
| [ | 43 adults with uncomplicated falciparum malaria in Thailand | 200 mg/day for fixed dose AS-mefloquine tablet or 4 mg/kg/day as nonfixed AS-mefloquine | Fixed: 1.1 (n = 14) |
| [ | 11 male Thai adults with uncomplicated falciparum malaria | 200 mg AS once, followed by 100 mg 12 hours later, then 100 mg once daily × 4 days | Acute: 0.64a |
| [ | 24 pregnant Karen women in the 2nd and 3rd trimesters with uncomplicated falciparum malaria | 4 mg/kg once daily × 3 days with atovaquone plus proguanil | Half-life: 1.0 (n = 13)a |
| [ | 6 male Thai adults with uncomplicated falciparum malaria and 6 healthy male adults | 100 mg AS once | Healthy: 0.85 |
| [ | 8 Vietnamese adults with uncomplicated falciparum malaria and 10 healthy Vietnamese adults | 150 mg once | Healthy: 0.77 |
| [ | 26 2nd and 3rd trimester pregnant women with asymptomatic falciparum parasitaemia, the same women postpartum, and 25 non-pregnant asymptomatic, parasitaemic controls | 200 mg once | Pregnant: 1.28a |
| [ | 57 children (2-14 years) with uncomplicated falciparum malaria in Gabon | AS dose (mg/kg) | Group A:1.0 |
| [ | 40 children and adults with uncomplicated falciparum malaria in Pailin, Cambodia and 40 adults with uncomplicated falciparum malaria in Wang Pha, Thailand | At each site: | Thailand: |
Estimates from PopPK studies are described in the text. Values given as mean unless otherwise specified.
a. Median b. Geometric mean
Summary of AS pharmacokinetic results following rectal AS administration.
| Subjects & Regimen | Cmax (ng/mL) | Tmax (hours) | Half-life (hours) | AUC (ng*hr/mL) | |
|---|---|---|---|---|---|
| [ | 16 paediatric patients with uncomplicated falciparum malaria | 507; 561†a | 0.8; 1.0a | 0.9; 0.9a | 692; 1076†a |
| [ | 12 paediatric patients with uncomplicated falciparum malaria | 90† | 0.58 | ||
| [ | 12 healthy Malaysian adults | 448.5 | 1.43 | 0.95 | 796 |
Estimates from PopPK studies are described in the text. Values given as mean unless otherwise specified.
†Units converted to uniform scale a. Median
Summary of DHA pharmacokinetic results following rectal AS administration.
| Subjects & Regimen | Cmax (ng/mL) | Tmax (hours) | Clearance (L/kg/hr) | Volume (L/kg) | Half-life (hours) | AUC (ng*hr/mL) | |
|---|---|---|---|---|---|---|---|
| [ | 16 paediatric patients with uncomplicated falciparum malaria | 898; 1535†a | 1.5; 2.0a | 1.3; 1.8a | 2403; 5633†a | ||
| [ | 12 paediatric patients with uncomplicated falciparum malaria | 180† | 1.13 | ||||
| [ | 12 healthy Sudanese adults | 219.1† | 1.95 | 1.21 | 1185.17 | ||
| [ | 12 healthy Malaysian adults | 385.6† | 1.80 | AUC0-t | |||
| Krishna | 34 Ghanaian children (8 months - 7 years) with moderate falciparum malaria | Group 1: | Group 1: | Group 1: | Group 1: | Group 1: | Group 1: |
Estimates from PopPK studies are described in the text. Values given as mean unless otherwise specified
†Units converted to uniform scale a. Median