TY - JOUR
T1 - The pharmacokinetics of 8‐methoxypsoralen following i.v. administration in humans [see comments]
AU - Billard, V.
AU - Gambus, PL
AU - Barr, J.
AU - Minto, CF
AU - Corash, L.
AU - Tessman, JW
AU - Stickney, JL
AU - Shafer, SL
PY - 1995/1/1
Y1 - 1995/1/1
N2 - 1. 8‐methoxypsoralen (8‐MOP) is a naturally occurring photoreactive substance which, in the presence of u.v. light, forms covalent adducts with pyrimidine bases in nucleic acids. For many years, 8‐MOP has been used in PUVA therapy for treatment of psoriasis. Recently, the drug has been found to inactivate effectively bacteria spiked into platelet concentrates. The purpose of this study was to determine the pharmacokinetics and safety of 8‐MOP administered intravenously in the bactericidal dosage range. 2. Eighteen volunteers were divided into three treatment groups to receive, respectively, 5, 10, and 15 mg 8‐MOP infused over 60 min. Frequent arterial samples were gathered, and the blood and plasma were assayed for 8‐MOP concentration. The pharmacokinetic parameters were determined by moment and compartmental population analysis, the latter performed with the program NONMEM. Haemodynamics, ventilatory pattern, and subjective effects were recorded throughout the study. 3. The intravenously administered 8‐MOP was well tolerated in all individuals, and no acute toxicity was observed. 4. The pharmacokinetics of 8‐MOP were best described by a three‐compartment mammillary model in which the volumes and clearances were proportional to weight. The mean pharmacokinetic parameters for the plasma concentrations were: V1 = 0.045 1 kg‐1, V2 = 0.57 1 kg‐1, V3 = 0.15 1 kg‐1, CL1 (systemic) = 0.010 1 kg‐1 min‐1, CL2 = 0.0067 1 kg‐1 min‐1, CL3 = 0.012 1 kg‐1 min‐1. The mean pharmacokinetic parameters for the blood concentrations were: V1 = 0.061 1 kg‐1, V2 = 1.15 1 kg‐1, V3 = 0.21 1 kg‐1, CL1 (systemic) = 0.015 1 kg‐1 min‐1, CL2 = 0.011 1 kg‐ 1 min‐1 and CL3 = 0.015 1 kg‐1 min‐1. 5. The plasma pharmacokinetic model described the observations with a median absolute error of 17%, and the blood pharmacokinetic model described the observations with a median absolute error of 18%. Analysis of the relative concentration of 8‐MOP between plasma and red blood cells suggested concentration‐ dependent partitioning. 6. The addition of 7.5 mg 8‐MOP to 300 ml platelet concentrate would produce bactericidal concentrations of 25 micrograms ml‐1. Simulations based upon our data show that intravenous administration of 7.5 mg over 60 min would result in systemic concentrations of 8‐MOP similar to those observed with conventional PUVA therapy. We conclude that the extensive safety history established in PUVA therapy will be applicable to this new application of 8‐MOP. 1995 The British Pharmacological Society
AB - 1. 8‐methoxypsoralen (8‐MOP) is a naturally occurring photoreactive substance which, in the presence of u.v. light, forms covalent adducts with pyrimidine bases in nucleic acids. For many years, 8‐MOP has been used in PUVA therapy for treatment of psoriasis. Recently, the drug has been found to inactivate effectively bacteria spiked into platelet concentrates. The purpose of this study was to determine the pharmacokinetics and safety of 8‐MOP administered intravenously in the bactericidal dosage range. 2. Eighteen volunteers were divided into three treatment groups to receive, respectively, 5, 10, and 15 mg 8‐MOP infused over 60 min. Frequent arterial samples were gathered, and the blood and plasma were assayed for 8‐MOP concentration. The pharmacokinetic parameters were determined by moment and compartmental population analysis, the latter performed with the program NONMEM. Haemodynamics, ventilatory pattern, and subjective effects were recorded throughout the study. 3. The intravenously administered 8‐MOP was well tolerated in all individuals, and no acute toxicity was observed. 4. The pharmacokinetics of 8‐MOP were best described by a three‐compartment mammillary model in which the volumes and clearances were proportional to weight. The mean pharmacokinetic parameters for the plasma concentrations were: V1 = 0.045 1 kg‐1, V2 = 0.57 1 kg‐1, V3 = 0.15 1 kg‐1, CL1 (systemic) = 0.010 1 kg‐1 min‐1, CL2 = 0.0067 1 kg‐1 min‐1, CL3 = 0.012 1 kg‐1 min‐1. The mean pharmacokinetic parameters for the blood concentrations were: V1 = 0.061 1 kg‐1, V2 = 1.15 1 kg‐1, V3 = 0.21 1 kg‐1, CL1 (systemic) = 0.015 1 kg‐1 min‐1, CL2 = 0.011 1 kg‐ 1 min‐1 and CL3 = 0.015 1 kg‐1 min‐1. 5. The plasma pharmacokinetic model described the observations with a median absolute error of 17%, and the blood pharmacokinetic model described the observations with a median absolute error of 18%. Analysis of the relative concentration of 8‐MOP between plasma and red blood cells suggested concentration‐ dependent partitioning. 6. The addition of 7.5 mg 8‐MOP to 300 ml platelet concentrate would produce bactericidal concentrations of 25 micrograms ml‐1. Simulations based upon our data show that intravenous administration of 7.5 mg over 60 min would result in systemic concentrations of 8‐MOP similar to those observed with conventional PUVA therapy. We conclude that the extensive safety history established in PUVA therapy will be applicable to this new application of 8‐MOP. 1995 The British Pharmacological Society
UR - http://www.scopus.com/inward/record.url?scp=0028808843&partnerID=8YFLogxK
U2 - 10.1111/j.1365-2125.1995.tb04557.x
DO - 10.1111/j.1365-2125.1995.tb04557.x
M3 - Article
C2 - 8554937
AN - SCOPUS:0028808843
SN - 0306-5251
VL - 40
SP - 347
EP - 360
JO - British Journal of Clinical Pharmacology
JF - British Journal of Clinical Pharmacology
IS - 4
ER -