TY - JOUR
T1 - Pharmacokinetics of orally administered melatonin in critically ill patients
AU - Mistraletti, Giovanni
AU - Sabbatini, Giovanni
AU - Taverna, Martina
AU - Figini, Maria Adele
AU - Umbrello, Michele
AU - Magni, Paolo
AU - Ruscica, Massimiliano
AU - Dozio, Elena
AU - Esposti, Roberto
AU - Demartini, Germana
AU - Fraschini, Franco
AU - Rezzani, Rita
AU - Reiter, Russel J.
AU - Iapichino, Gaetano
PY - 2010/3
Y1 - 2010/3
N2 - Critically ill patients exhibit reduced melatonin secretion, both in nocturnal peaks and basal daytime levels. Oral melatonin supplementation may be useful for known sedative and antioxidant properties. Its early enteral absorption and daily pharmacokinetics were determined in two cohorts of six high-risk patients in this prospective trial. During their third and fourth Intensive Care Unit (ICU) day, they underwent two different sets of repeated blood samples to detect serum melatonin levels through radio-immuno-assay. Cohort 1: samples taken at 20:00, 20:45, 21:30, 24:00, 03:00, 06:00, 14:00, 20:00 to describe the daily pharmacokinetics. Cohort 2: 20:00, 20:05, 20:10, 20:20, 20:30, 20:45 to study the early absorption. On ICU day 3, endogenous levels were measured, while the absorption of exogenous melatonin was determined on ICU day 4 after administration, at 20:00, of 3 mg melatonin. All basal levels were below the expected values. Following enteral administration, pharmacological levels were already reached in 5 min, with a serum peak after 16 min (half-absorption time: 3 min 17 s). The maximum serum level observed was 11040 pg/mL and the disappearance rate indicated a half-elimination time of 1 hr 34 min. Serum melatonin levels decreased significantly after midnight; pharmacological levels were maintained up to 10 hr following administration. No excessive sleepiness was reported in this patient group. Critically ill patients exhibited reduced melatonin secretion, as reported in the literature. Despite the critical illness, the oral bioavailability was satisfactory: serum levels after oral administration showed basically unchanged intestinal absorption, while disappearance rate was slower than reported elsewhere in healthy volunteers.
AB - Critically ill patients exhibit reduced melatonin secretion, both in nocturnal peaks and basal daytime levels. Oral melatonin supplementation may be useful for known sedative and antioxidant properties. Its early enteral absorption and daily pharmacokinetics were determined in two cohorts of six high-risk patients in this prospective trial. During their third and fourth Intensive Care Unit (ICU) day, they underwent two different sets of repeated blood samples to detect serum melatonin levels through radio-immuno-assay. Cohort 1: samples taken at 20:00, 20:45, 21:30, 24:00, 03:00, 06:00, 14:00, 20:00 to describe the daily pharmacokinetics. Cohort 2: 20:00, 20:05, 20:10, 20:20, 20:30, 20:45 to study the early absorption. On ICU day 3, endogenous levels were measured, while the absorption of exogenous melatonin was determined on ICU day 4 after administration, at 20:00, of 3 mg melatonin. All basal levels were below the expected values. Following enteral administration, pharmacological levels were already reached in 5 min, with a serum peak after 16 min (half-absorption time: 3 min 17 s). The maximum serum level observed was 11040 pg/mL and the disappearance rate indicated a half-elimination time of 1 hr 34 min. Serum melatonin levels decreased significantly after midnight; pharmacological levels were maintained up to 10 hr following administration. No excessive sleepiness was reported in this patient group. Critically ill patients exhibited reduced melatonin secretion, as reported in the literature. Despite the critical illness, the oral bioavailability was satisfactory: serum levels after oral administration showed basically unchanged intestinal absorption, while disappearance rate was slower than reported elsewhere in healthy volunteers.
KW - Critically ill
KW - Enteral absorption
KW - Intensive care
KW - Melatonin
KW - Oral bioavailability
KW - Pharmacokinetics
KW - Radio-immuno-assay
UR - http://www.scopus.com/inward/record.url?scp=75149198595&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=75149198595&partnerID=8YFLogxK
U2 - 10.1111/j.1600-079X.2009.00737.x
DO - 10.1111/j.1600-079X.2009.00737.x
M3 - Article
C2 - 20070489
AN - SCOPUS:75149198595
SN - 0742-3098
VL - 48
SP - 142
EP - 147
JO - Journal of pineal research
JF - Journal of pineal research
IS - 2
ER -