Autor: |
Degrossi, O., Ortiz, M., Degrossi, E., García del Río, H., Barreira, J., Messina, D., Kerzberg, E., Roldan, E., Montuori, E., Pérez Lloret, A. |
Zdroj: |
European Journal of Clinical Pharmacology; 1995, Vol. 48 Issue 6, p489-494, 6p |
Abstrakt: |
The activity of olpadronate labelled with technetium-99m(Tc) was monitored in plasma and urine samples after single oral (925 MBq Tc/10 mg, coadministered with 50 mg cold drug) and intravenous (925 MBq Tc/5 mg) administrations to two groups of patients with different rates of bone turnover. The first group comprised high bone turnover (HBTO) patients suffering from Paget's bone disease; the second group comprised patients with normal to low bone turnover (NBTO) having the diagnosis of rheumatoid arthritis and secondary osteoporosis. Kinetic variables were correlated with anthropomorphometric variables, biological markers of bone metabolism and plasma proteins. Data were also obtained after repeatedly dosing the HBTO patients. Additionally, Paget's bone and healthy bone (PB/HB) uptake before and after low-dose oral treatment were assessed by means of scintigraphy. Results showed that most of the kinetic variables did not differ between the two groups of patients, except for a greater V and smaller blood area under the curve AUC in the patients with HBTO. After a repeated-dose administration period, the blood AUC activity and Whole Body Retention (WBR) of the HBTO patients tended to be similar to those of the NBTO patients. In both groups, after oral dosing, the C was 20 times lower than the C after i.v. injection, and the oral bioavailability ranged from 3% to 4%. Finally, the plasma tβ ranged from 9 to 14 h. Correlation coefficients were obtained from multiple regression analysis; kinetic variables showed very low correlations with anthropomorphometric measurements. In contrast the V and WBR were significantly correlated with serum alkaline phosphatase levels and the V also with urine hydroxyproline levels. Plasma protein concentration was also correlated with excretion parameters such as CL and plasma tβ after an oral dose. Scintigraphic studies in the HBTO group allowed bone selectivity to be seen through skeletal drug uptake. The 15 Pagetic lesions analysed in the HBTO group showed a decrease in PB/HB ratio from 3.8 in the basal study to 2.7 after olpadronate administration for 30 days at the rate of 50 mg/day. In conclusion, the kinetic profile of Tc-labelled olpadronate, mainly AUC and WBR, showed a dependence upon bone metabolism and seemed unrelated to body size variables. HBTO patients showed a lower blood AUC but a higher V. Both variables may have been reflecting the fact that the drug binds selectively with calcified tissues and, in turn, with the target compartment. Scintigraphy confirmed the labelled-compound bone selectivity as a desirable feature for a bone-scanning agent. [ABSTRACT FROM AUTHOR] |
Databáze: |
Complementary Index |
Externí odkaz: |
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