David A Katz1,2, Wei Liu3, Charles Locke3, Sandeep Dutta3, Katherine A Tracy3. 1. AbbVie Inc., 1 North Waukegan Road, North Chicago, IL, 60064, USA. david.a.katz@me.com. 2. , 222 West Merchandise Mart Plaza, Suite 1230, Chicago, IL, 60654, USA. david.a.katz@me.com. 3. AbbVie Inc., 1 North Waukegan Road, North Chicago, IL, 60064, USA.
Abstract
RATIONALE: Arginine vasopressin type 1B receptor (V1B) receptor antagonism is considered a potential therapeutic for diseases with hypothalamic-pituitary-adrenal (HPA) axis dysregulation. OBJECTIVES: The aim of the present study was to evaluate the safety and pharmacodynamics of ABT-436, a selective V1B antagonist, in healthy adults. METHODS:Healthy adults received daily oral doses of ABT-436 in two clinical trials. In a dose escalation trial, nine subjects received each of 100, 500, or 800 mg ABT-436, or placebo, in the morning for 7-14 days. In a crossover trial on two 7-day regimens, 20 subjects received200 mg ABT-436 each morning or each evening. Pharmacokinetics, measures of basal HPA axis activity, and safety were assessed in both trials. RESULTS:Mild gastrointestinal intolerance was more common with ABT-436 treatment, compared to placebo, and showed dose dependence. Mean increases and decreases of systolic blood pressure (at different times), and mean pulse increases, were observed in subjects who received 800 mg ABT-436. Mean decreases of plasma adrenocorticotrophic hormone (ACTH), serum cortisol, urine total glucocorticoids, and urine cortisol, compared to placebo, were observed following 7 daily doses of 500 and 800 mg ABT-436. Statistically significant mean differences of plasma ACTH, serum cortisol, and urine total glucocorticoids were observed between morning and evening regimens of 200 mg ABT-436. The largest observed differences were near the times of maximum post-dose ABT-436 plasma concentrations. CONCLUSIONS:ABT-436 regimens of 200-800 mg once daily (QD) for 7 days attenuated basal HPA axis activity. The results support further evaluation of ABT-436 for treatment of disorders in which HPA axis dysregulation may have an etiologic role.
RCT Entities:
RATIONALE: Arginine vasopressin type 1B receptor (V1B) receptor antagonism is considered a potential therapeutic for diseases with hypothalamic-pituitary-adrenal (HPA) axis dysregulation. OBJECTIVES: The aim of the present study was to evaluate the safety and pharmacodynamics of ABT-436, a selective V1B antagonist, in healthy adults. METHODS: Healthy adults received daily oral doses of ABT-436 in two clinical trials. In a dose escalation trial, nine subjects received each of 100, 500, or 800 mg ABT-436, or placebo, in the morning for 7-14 days. In a crossover trial on two 7-day regimens, 20 subjects received 200 mg ABT-436 each morning or each evening. Pharmacokinetics, measures of basal HPA axis activity, and safety were assessed in both trials. RESULTS: Mild gastrointestinal intolerance was more common with ABT-436 treatment, compared to placebo, and showed dose dependence. Mean increases and decreases of systolic blood pressure (at different times), and mean pulse increases, were observed in subjects who received 800 mg ABT-436. Mean decreases of plasma adrenocorticotrophic hormone (ACTH), serum cortisol, urine total glucocorticoids, and urine cortisol, compared to placebo, were observed following 7 daily doses of 500 and 800 mg ABT-436. Statistically significant mean differences of plasma ACTH, serum cortisol, and urine total glucocorticoids were observed between morning and evening regimens of 200 mg ABT-436. The largest observed differences were near the times of maximum post-dose ABT-436 plasma concentrations. CONCLUSIONS:ABT-436 regimens of 200-800 mg once daily (QD) for 7 days attenuated basal HPA axis activity. The results support further evaluation of ABT-436 for treatment of disorders in which HPA axis dysregulation may have an etiologic role.
Authors: Vladimir Coric; Howard H Feldman; Dan A Oren; Anantha Shekhar; Joseph Pultz; Randy C Dockens; Xiaoling Wu; Kimberly A Gentile; Shu-Pang Huang; Eileen Emison; Terrye Delmonte; Bernadette B D'Souza; Daniel L Zimbroff; Jack A Grebb; Andrew W Goddard; Elyse G Stock Journal: Depress Anxiety Date: 2010-05 Impact factor: 6.505
Authors: L van Londen; J G Goekoop; G M van Kempen; A C Frankhuijzen-Sierevogel; V M Wiegant; E A van der Velde; D De Wied Journal: Neuropsychopharmacology Date: 1997-10 Impact factor: 7.853
Authors: Wei Liu; David A Katz; Charles Locke; Dan Daszkowski; Yi Wang; Matthew J Rieser; Walid Awni; Gerard J Marek; Sandeep Dutta Journal: Clin Pharmacol Drug Dev Date: 2013-02-21
Authors: Heike E Künzel; Astrid W Zobel; Thomas Nickel; Nibal Ackl; Manfred Uhr; Annette Sonntag; Marcus Ising; Florian Holsboer Journal: J Psychiatr Res Date: 2003 Nov-Dec Impact factor: 4.791
Authors: Marcus Ising; Ulrich S Zimmermann; Heike E Künzel; Manfred Uhr; Alan C Foster; Susan M Learned-Coughlin; Florian Holsboer; Dimitri E Grigoriadis Journal: Neuropsychopharmacology Date: 2007-02-07 Impact factor: 7.853
Authors: Jeremy W Tomlinson; Elizabeth A Walker; Iwona J Bujalska; Nicole Draper; Gareth G Lavery; Mark S Cooper; Martin Hewison; Paul M Stewart Journal: Endocr Rev Date: 2004-10 Impact factor: 19.871
Authors: Megan L Ryan; Daniel E Falk; Joanne B Fertig; Beatrice Rendenbach-Mueller; David A Katz; Katherine A Tracy; Eric C Strain; Kelly E Dunn; Kyle Kampman; Elizabeth Mahoney; Domenic A Ciraulo; Laurie Sickles-Colaneri; Nassima Ait-Daoud; Bankole A Johnson; Janet Ransom; Charles Scott; George F Koob; Raye Z Litten Journal: Neuropsychopharmacology Date: 2016-09-23 Impact factor: 7.853