Safety, Pharmacokinetic and Pharmacodynamic Evaluation of Teverelix for the Treatment of Hormone-Sensitive Advanced Prostate Cancer: Phase 2 Loading-Dose-Finding Studies

Carol M MacLean; Albertas Ulys; Feliksas Jankevičius; Žilvinas Saladžinskas; Steve van Os; Finn Larsen

doi:10.3390/medicina59040681

Safety, Pharmacokinetic and Pharmacodynamic Evaluation of Teverelix for the Treatment of Hormone-Sensitive Advanced Prostate Cancer: Phase 2 Loading-Dose-Finding Studies

Medicina (Kaunas). 2023 Mar 29;59(4):681. doi: 10.3390/medicina59040681.

Authors

Carol M MacLean¹, Albertas Ulys², Feliksas Jankevičius³, Žilvinas Saladžinskas⁴, Steve van Os¹, Finn Larsen¹

Affiliations

¹ Antev Ltd., London W1S 1DN, UK.
² National Cancer Institute, 08406 Vilnius, Lithuania.
³ Faculty of Medicine, Vilnius University, Ciurlionio 21, LT-03101 Vilnius, Lithuania.
⁴ Department of Surgery, Medical Academy, Hospital of Lithuanian University of Health Sciences, 50103 Kaunas, Lithuania.

Abstract

Background and objectives: Teverelix drug product (DP) is a gonadotropin-releasing hormone antagonist in development for the treatment of patients with prostate cancer in whom androgen deprivation therapy is indicated. The aim of this paper is to present the results of five Phase 2 studies that assessed the pharmacokinetics, pharmacodynamics, efficacy and safety of different loading dose regimens of teverelix DP. Methods: Five single-arm, uncontrolled clinical trials were conducted in patients with advanced prostate cancer. The five different loading dose regimens of teverelix DP tested were (a) a single 90 mg subcutaneous (SC) injection of teverelix DP given on 3 consecutive days (Days 0, 1 and 2); (b) a single 90 mg intramuscular (IM) injection of teverelix DP given 7 days apart (Days 0 and 7); (c) a single 120 mg SC injection of teverelix DP given on 2 consecutive days (Days 0 and 1); (d) 2 × 60 mg SC injections of teverelix DP given on 3 consecutive days (Days 0, 1 and 2), and (e) 2 × 90 mg SC injections of teverelix DP given on 3 consecutive days (Days 0, 1 and 2). The primary efficacy parameter was the duration of action of an initial loading dose regimen in terms of suppression of testosterone to below the castration level (0.5 ng/mL). Results: Eighty-two patients were treated with teverelix DP. Two regimens (90 mg and 180 mg SC on 3 consecutive days) had a mean duration of castration of 55.32 days and 68.95 days with >90% of patients having testosterone levels < 0.5 ng/mL at Day 28. The mean onset of castration for the SC regimens ranged from 1.10 to 1.77 days, while it was slower (2.4 days) with IM administration. The most common adverse event (AE) was injection site reaction. No AEs of severe intensity were reported. Conclusions: Teverelix DP is safe and well tolerated. Castrate levels of testosterone can be rapidly achieved following the subcutaneous injection of teverelix DP on 3 consecutive days. Streamlining of the administration of the loading dose and identifying a suitable maintenance dose will be investigated in future trials.

Keywords: androgen deprivation therapy; cardiovascular risk; castration; gonadotropin-releasing hormone agonist; gonadotropin-releasing hormone antagonist; luteinizing hormone-releasing hormone agonists; prostate cancer.

Publication types

Clinical Trial, Phase II

MeSH terms

Androgen Antagonists / therapeutic use
Gonadotropin-Releasing Hormone / therapeutic use
Humans
Leuprolide / adverse effects
Male
Prostatic Neoplasms* / drug therapy
Testosterone / therapeutic use

Substances

antarelix
Gonadotropin-Releasing Hormone
Leuprolide
Androgen Antagonists
Testosterone

Grants and funding

NA/Antev Ltd