Table 3.

Secondary pharmacokinetic parameters of miltefosine in Eastern African patients with VL treated with either miltefosine monotherapy or combination therapy

	Secondary parametera [median (range)]
Monotherapy (28 days miltefosine)	Total (n = 48)	Paediatricb (n = 19)	Adultb (n = 29)	Diff (%)c	P value
Initial half-life (days)	7.05 (4.02–10.9)	7.02 (4.02–8.45)	7.18 (5.35–10.9)	–2	0.258
Terminal half-life (days)	79.4 (49.9–103)	77.8 (54.9–95.6)	81.3 (49.9–103)	–4	0.073
AUC0–∞ (μg·day/mL)	713 (237–1482)	545 (314–1080)	812 (237–1482)	–33	0.006d
AUC0–28d (μg·day/mL)	423 (191–767)	352 (232–593)	497 (191–767)	–29	0.002d
Time > EC50 (days)	51.4 (30.5–77.1)	48.3 (36.3–62.4)	52.9 (30.5–77.1)	–9	0.024e
Time > EC90 (days)	27.0 (4.29–43.8)	22.1 (11.0–34.2)	27.8 (4.29–43.8)	–21	0.005d
Combination therapy (10 days miltefosine)	Total (n = 47)	Paediatricb (n = 22)	Adultb (n = 25)	Diff (%)c	P value
Initial half-life (days)	7.39 (5.41–10.3)	6.76 (5.58–9.00)	7.52 (5.41–10.3)	–12	0.031e
Terminal half-life (days)	78.5 (62.4–98.6)	76.7 (66.0–98.6)	79.7 (62.4–93.7)	–4	0.231
AUC0–∞ (μg·day/mL)	290 (70.1–496)	197 (136–496)	313 (70.1–483)	–37	0.004d
AUC0–10 (μg·day/mL)	87.9 (31.1–136)	69.5 (31.1–129)	95.9 (32.3–136)	–28	0.004d
Time > EC50 (days)	31.2 (14.2–46.9)	28.5 (23.1–43.0)	34.1 (14.2–46.9)	–16	0.013e
Time > EC90 (days)	8.98 (0–16.8)	3.17 (0–16.8)	9.93 (0–16.2)	–68	0.002d

^aTime > EC₅₀, time the miltefosine concentration was above the in vitro susceptibility value EC₅₀; Time > EC₉₀, time the miltefosine concentration was above the in vitro susceptibility value EC₉₀; P value, calculated based on Mann–Whitney U-test.

^bPaediatric defined as having an age <12 years and adult defined as having an age ≥12 years.

^cPercentage difference between the median adult and paediatric ([paediatric – adult]/adult) pharmacokinetic parameter.

^dBelow significance level of P < 0.01.

^eBelow significance level of P < 0.05.