Pharmacokinetic-pharmacodynamic correlation of imipenem in pediatric burn patients using a bioanalytical liquid chromatographic method

Santos, Silvia Regina Cavani Jorge; Sanches-Giraud, Cristina; Silva Júnior, Carlindo Vieira; Gomez, David Souza

doi:10.1590/S1984-82502015000200007

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Brazilian Journal of Pharmaceutical Sciences

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Articles • Braz. J. Pharm. Sci. 51 (2) • Apr-Jun 2015 • https://doi.org/10.1590/S1984-82502015000200007 copy

Pharmacokinetic-pharmacodynamic correlation of imipenem in pediatric burn patients using a bioanalytical liquid chromatographic method

Authorship SCIMAGO INSTITUTIONS RANKINGS

A bioanalytical method was developed and applied to quantify the free imipenem concentrations for pharmacokinetics and PK/PD correlation studies of the dose adjustments required to maintain antimicrobial effectiveness in pediatric burn patients. A reverse-phase Supelcosil LC18 column (250 x 4.6 mm 5 micra), binary mobile phase consisting of 0.01 M, pH 7.0 phosphate buffer and acetonitrile (99:1, v/v), flow rate of 0.8 mL/min, was applied. The method showed good absolute recovery (above 90%), good linearity (0.25-100.0 µg/mL, r²=0.999), good sensitivity (LLOQ: 0.25 µg/mL; LLOD: 0.12 µg/mL) and acceptable stability. Inter/intraday precision values were 7.3/5.9%, and mean accuracy was 92.9%. A bioanalytical method was applied to quantify free drug concentrations in children with burns. Six pediatric burn patients (median 7.0 years old, 27.5 kg), normal renal function, and 33% total burn surface area were prospectively investigated; inhalation injuries were present in 4/6 (67%) of the patients. Plasma monitoring and PK assessments were performed using a serial blood sample collection for each set, totaling 10 sets. The PK/PD target attained (40%T>MIC) for each minimum inhibitory concentration (MIC: 0.5, 1.0, 2.0, 4.0 mg/L) occurred at a percentage higher than 80% of the sets investigated and 100% after dose adjustment. In conclusion, the purification of plasma samples using an ultrafiltration technique followed by quantification of imipenem plasma measurements using the LC method is quite simple, useful, and requires small volumes for blood sampling. In addition, a small amount of plasma (0.25 mL) is needed to guarantee drug effectiveness in pediatric burn patients. There is also a low risk of neurotoxicity, which is important because pharmacokinetics are unpredictable in these critical patients with severe hospital infection. Finally, the PK/PD target was attained for imipenem in the control of sepsis in pediatric patients with burns.

Imipenem/quantification; Antibiotics/dosage; Pediatric patients/burn/antibiotics use; High Performance Liquid Chromatography/quantitative analysis; Drug plasma monitoring; PK/PD

Patient allocation	Gender	Age (yrs)	Weight (kg)	BMI (kg/m2)	TBSA (%)	CLcr (mL/min)	Inhalation injury	Endotracheal intubation	Vasoactive Drugs	Outcome
#1	M	09	30	17.1	30	207.4	(-)	(-)	(-)	Survivor
#2	F	06	25	19.4	75	185.4	(+)	(+)	(+)	Nonsurvivor
#3	M	02	12	14.8	15	682.0	(+)	(+)	(-)	Survivor
#4	M	01	16	25.0	28	702.2	(-)	(-)	(-)	Survivor
#5	M	08	40	23.7	45	388.1	(+)	(+)	(+)	Survivor
#6	M	03	16	17.7	36	372.8	(+)	(+)	(+)	Survivor
Patients	5M/1F	NAP	NAP	NAP	NAP	NAP	4/6	4/6	3/6	5/6
Median	NAP	7.0	27.5	21.5	33.0	377.8	NAP	NAP	NAP	NAP
Quartile 25-75%	NAP	2.3-8.0	16.0-37.5	17.3-23.7	28.9-45.0	246.9-608.5	NAP	NAP	NAP	NAP

Parameter	Unit	Confidence Limits
Linearity (n=3)	µg/mL	0.25-100.0
Linear regression (n=3 curves)		r²: 0.9974
LLOD: 0.12 µg/mL (n=10)	RSD	18.95
LLOQ: 0.25 µg/mL (n=10)	RSD	14.86
Recovery
Absolute (n=10) analite/IS	%	93.0/64.2
Relative (n=10) analite	%	144.9
Precision/within-day (n=9)	RSD (mean: 2.0)
80 µg/mL		5.3
40 µg/mL		6.7
1.0 µg/mL		5.8
Precision/between-day (n=27)	RSD (mean: 2.3)
80 µg/mL		6.5
40 µg/mL		7.2
1.0 µg/mL		8.3
Accuracy/within-day (n=9)	% (bias: 1.49%)
80 µg/mL		93.4
40 µg/mL		90.1
1.0 µg/mL		91.3
Accuracy/between-day (n=27)	% (bias: 1.65%)
80 µg/mL		95.2
40 µg/mL		94.7
1.0 µg/mL		91.7
Stability /thawing cycles	SE%
Cycle 1 (n=12)		6.6
Cycle 2 (n=12)		4.4
Cycle 3 (n=12)		3.5
Stability/ short term	SE%
40 µg/mL (n=3)		8.2
20 µg/mL (n=3)		7.9
0.6 µg/mL (n=3)		9.0
Stability/ post-preparative	SE%
40 µg/mL (n=3)		7.2
20 µg/mL (n=3)		7.3
0.6 µg/mL (n=3)		6.9

Parameters	Pharmacokinetics (10 sets)			PK/PD Correlation (10 sets) ¹³MIC values
Patient allocation	t_(1/2)β (h)	CL_T (mL/min.kg)	Vd^ss (L/kg)	0.5 mg/L	1 mg/L	2 mg/L	4 mg/L
#1 (set 1)	1.3	1.4	0.16	100	100	100	99
#1 (set 2)	0.5	2.4	0.10	70	61	53	36
#2	1.7	0.9	0.14	100	100	100	100
#3	0.8	3.8	0.26	100	104	90	63
#4 (set 1)	2.4	1.4	0.30	100	100	100	100
#4 (set 2)	1.6	13.1	1.78	100	94	74	34
#5 (set 1)	1.9	1.9	0.32	100	100	100	100
#5 (set 2)	4.8	6.4	2.68	100	100	100	100
#5 (set 3)	1.0	2.2	0.19	100	100	100	79
#6	0.4	5.5	0.17	91	85	78	65
Median	1.45	2.3	0.23	100	100	100	89
IQ (25/75%)	0.85-1.85	1.5-5.1	0.16-0.32	100-100	96-100	81-100	64-100
%TA (40%fT>MIC)	NAP	NAP	NAP	100%	100%	100%	80%

Universidade de São Paulo, Faculdade de Ciências Farmacêuticas Av. Prof. Lineu Prestes, n. 580, 05508-000 S. Paulo/SP Brasil, Tel.: (55 11) 3091-3824 - São Paulo - SP - Brazil
E-mail: bjps@usp.br

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[1] *Correspondence: S. R. C. J. Santos. Departamento de Fármácia. Faculdade de Ciências Farmacêuticas. Universidade de São Paulo. Av. Prof. Lineu Prestes, n.580, 05508-000 - São Paulo - SP, Brasil. E-mail: pharther@usp.br