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Endocrine Abstracts (2020) 70 AEP627 | DOI: 10.1530/endoabs.70.AEP627

ECE2020 Audio ePoster Presentations Pituitary and Neuroendocrinology (217 abstracts)

Absolute oral bioavailability and absorption, metabolism, excretion of [14C]-Labeled paltusotine (CRN00808), an orally bioavailable, nonpeptide, selective, somatostatin receptor 2 (sst2) biased agonist for the treatment of acromegaly

Ajay Madan 1 , Rosa Luo 1 , Chris Ferrara-Cook 1 , R. Scott Struthers 1 , Sjoerd van Marle 2 & Alan Krasner 1


1Crinetics Pharmaceuticals Inc, San Diego, United States; 2PRA Health Sciences Research Martini, Groningen, Netherlands


Injected depot formulations of somatostatin peptide analogs are routinely used to treat acromegaly and neuroendocrine tumors (NETs). Paltusotine (CRN00808), a small molecule nonpeptide selective somatostatin receptor 2 (sst2) agonist, is being evaluated for efficacy and safety in patients with acromegaly. The current Phase 1 study (NCT04246749) was conducted in two Parts: In Part A, the absorption, metabolism, excretion, and mass balance of a single oral dose of 20 mg [14C]-paltusotine (3.0 MBq) oral solution was characterized in six healthy male subjects. Plasma, blood, urine, and feces were collected for up to 432 hours, and were analyzed for total radioactivity and paltusotine concentrations (plasma only). Metabolite profiling was conducted on the plasma, urine, and feces samples. In Part B, the absolute bioavailability of paltusotine was determined by administering a single oral dose of 20 mg paltusotine compared with a single micro-tracer intravenous (IV) bolus injection of 0.050 mg [14C]-paltusotine (0.0185 MBq) in five healthy male subjects. The IV dose was administered approximately 90 minutes after the oral dose. Plasma samples were collected for up to 144 hours and were analyzed for paltusotine and [14C]-paltusotine concentrations. Part A of the study show that >90% of radioactivity was recovered within 7 days of dosing. The primary route of excretion was the feces (89.9% of dose) with minimal excretion in the urine (3.9% of dose). Absorption of total [14C]-paltusotine-derived radioactivity in plasma was rapid (median Tmax = 1 hour), and the geometric mean of Cmax, AUC0-inf, and t1/2 were determined to be 189 ng-equivalents/ml, 3180 ng-equivalents.hr/ml, and 31 hours, respectively. The pharmacokinetic parameters of unchanged paltusotine in plasma were similar, suggesting that majority of the circulating drug-derived radioactivity is accounted for by unchanged paltusotine and there are no abundant circulating metabolites. Data from Part B of the study show that the mean oral bioavailability of paltusotine was 70% and the mean clearance and volume of distribution after IV administration were 5.3 l/h and 240 l, respectively. Treatment emergent adverse events associated with paltusotine were generally mild and transient, and consistent with those reported with other somatostatin agonists. In conclusion, results from this clinical trial in healthy volunteers confirm that paltusotine has excellent drug-like properties for chronic once-daily oral treatment of patients with acromegaly and NETs.

Volume 70

22nd European Congress of Endocrinology

Online
05 Sep 2020 - 09 Sep 2020

European Society of Endocrinology 

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