ECE2014 Poster Presentations Pituitary Clinical (<emphasis role="italic">Generously supported by IPSEN</emphasis>) (108 abstracts)
Octreotide fluid crystal provides sustained octreotide bioavailability and similar IGF1 suppression to that of octreotide LAR (Sandostatin LAR): randomized, open-label, Phase I, repeat-dose study in healthy volunteers
John Roberts 1 , Margareta Linden 2 , Camilla Cervin 2 & Fredrik Tiberg 2,
1Novartis Pharmaceuticals Corporation, East Hanover, New Jersey, USA; 2Camurus AB, Lund, Sweden; 3Lund University, Lund, Sweden.
Background: Octreotide is the most widely used somatostatin analogue; however, the LAR formulation must be reconstituted prior to intramuscular injection. This Phase I study compared the pharmacokinetics and pharmacodynamics of octreotide Fluid Crystal (FC), a ready-to-use depot formulation for s.c. administration, vs octreotide LAR.
Methods: After a single dose of octreotide s.c. 200 μg, healthy adult male/female volunteers were randomized 1 week later to three injections of octreotide FC 30 mg/month (n=14) or octreotide LAR 30 mg/month (n=14). Blood samples for octreotide and IGF1 analyses were collected pre- and post-injection, and at pre-specified time points during the study. Adverse events were recorded.
Results: Octreotide FC exhibited a steady, rapid increase to peak concentrations (Cmax) followed by a slow, exponential decrease through day 28. After injection 3 (steady state): mean±S.D. Cmax=29.3±7.1 ng/ml, mean±S.D. AUC28d=3465±608h ng/ml, median (range) tmax=24 (2–24) h. Octreotide LAR exhibited a burst concentration peak and rapid decline to undetectable values, which rebounded by day 7, stabilized from day 10 and finally decreased around day 21. After injection 3 (steady state): mean±S.D. Cmax=1.8±0.6–ng/ml, mean±S.D. AUC28d=733±222h ng/ml, median (range) tmax=1 (0.5–360) h. Relative bioavailability (using AUC28d) of octreotide FC vs LAR was 487% (90% CI: 411–578). Octreotide FC provided more rapid and greater IGF1 suppression vs octreotide LAR after injection during weeks 1–2, but similar IGF1 levels were seen during weeks 3–4; AUC for IGF1 suppression was similar in both groups. Comparable injection-site and systemic tolerability was seen across both groups.
Conclusions: Octreotide FC provides greater octreotide bioavailability with a more rapid onset and similar duration of effect compared with octreotide LAR in healthy volunteers, and may offer enhanced convenience as medication as it may be supplied in a convenient, prefilled syringe with a thin needle. A Phase III study of octreotide FC in patients with acromegaly is planned.
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Endocrine Abstracts
ISSN 1470-3947 (print) | ISSN 1479-6848 (online)
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