| dc.contributor.author |
Standing JF, Ongas MO, Ogwang C, Kagwanja N, Murunga S, Mwaringa S, Ali R, Mturi N, Timbwa M, Manyasi C, Mwalekwa L, Bandika VL, Ogutu B, Waichungo J, Kipper K, Berkley JA |
|
| dc.date.accessioned |
2024-08-07T08:50:40Z |
|
| dc.date.available |
2024-08-07T08:50:40Z |
|
| dc.date.issued |
2018-12 |
|
| dc.identifier.uri |
http://dx.doi.org/10.1002/cpt.1078 |
|
| dc.identifier.uri |
http://repository.kemri.go.ke:8080/xmlui/handle/123456789/849 |
|
| dc.description.abstract |
Infants and young children with severe acute malnutrition (SAM) are treated with
empiric broad-spectrum antimicrobials. Parenteral ceftriaxone is currently a second-line
agent for invasive infection. Oral metronidazole principally targets small intestinal
bacterial overgrowth. Children with SAM may have altered drug absorption, distribution,
metabolism, and elimination. Population pharmacokinetics of ceftriaxone and
metronidazole were studied, with the aim of recommending optimal dosing. Eighty-one
patients with SAM (aged 2-45 months) provided 234 postdose pharmacokinetic samples
for total ceftriaxone, metronidazole, and hydroxymetronidazole. Ceftriaxone protein
binding was also measured in 190 of these samples. A three-compartment model
adequately described free ceftriaxone, with a Michaelis-Menten model for concentration
and albumin-dependent protein binding. A one-compartment model was used for both
metronidazole and hydroxymetronidazole, with only 1% of hydroxymetronidazole
predicted to be formed during first-pass. Simulations showed 80 mg/kg once daily of
ceftriaxone and 12.5 mg/kg twice daily of metronidazole were sufficient to reach
therapeutic targets. |
en_US |
| dc.language.iso |
en |
en_US |
| dc.publisher |
Clin Pharmacol Ther. |
en_US |
| dc.title |
Dosing of Ceftriaxone and Metronidazole for Children With Severe Acute Malnutrition. |
en_US |
| dc.type |
Article |
en_US |