A Randomized, Double-blinded, Clinical, Placebo-controlled Trial on the Effects of Therapy With Letrozole and hUman Choriongonadotropin in Male Hypogonadism Induced by Illicit Use of Anabolic Androgenic Steroids- The LUCAS Trial

Phase 4

Terminated

• Conditions: Hypogonadism; Hypogonadism, Male; Hypogonadotropic Hypogonadism
• Interventions: Drug: Placebo; Drug: Letrozole 2.5mg, hCG

• Registration Number: NCT05205837
• Lead Sponsor: Rigshospitalet, Denmark

Brief Summary

The overall objective of this randomized trial is to investigate the effects of treatment of AAS- induced male hypogonadism with combined therapy of letrozole and hCG compared with placebo on reproductive hormone levels, adherence to cessation of AAS use, fertility, cardiac function and quality of life.

Detailed Description

A randomized, double-blinded, clinical, placebo-controlled trial enrolling 60 male illicit AAS users with documented AAS-induced hypogonadism after a period \> 12 weeks of AAS cessation or a negative urine AAS doping test. Participants will be randomized to two study groups; 24 weeks of treatment with either tablet letrozole (femar®) initial dose of 2.5 mg each day versus tablet placebo. After an initial treatment period of four weeks, intramuscular injections with either hCG, initial dose 1500 IE twice weekly (letrozole group) or isotonic saline twice weekly (placebo group) will be added to therapy if plasma total testosterone level has not increased to target plasma level. Following 24 weeks of therapy, all participants will be observed for another 26 weeks without therapy. The study will have one trial center of recruitment: Department of Endocrinology, Rigshospitalet. Following participation in the study, all participants will be offered referral to an endocrine outpatient clinic if they still display clinical and biochemical signs of male hypogonadism.

A healthy group of 30 young lean eugonadal men, who have never used AAS, will be enrolled as control participants and undergo a screening visit and one visit including same procedures as the screening and randomization visits.

Study Timeline

• Study Start: 2021-11-24
• Study First Submitted: 2021-12-10
• Study First Submitted QC: 2022-01-12
• Study First Posted: 2022-01-25
• Primary Completion: 2023-08-15
• Study Completion: 2023-08-15
• Status Verified: 2024-02
• Last Update Submitted: 2024-02-14
• Last Update Posted: 2024-02-15

Recruitment & Eligibility

• Status: TERMINATED
• Sex: Male
• Target Recruitment: 8

Inclusion Criteria

• • Male sex

  • 18 - 50 years of age
  • Hypogonadism following observational period of a minimum of 12 weeks since AAS discontinuation OR hypogonadism with a urine sample negative for AAS analyses at screening visit: plasma total testosterone ≤ 10 nmol/L AND featuring at least one symptom of male hypogonadism using IIEF in terms of erectile function (IIEF: Q1 - Q5 + Q15; total score < 26) and/or sexual desire (IIEF: Q11 + Q12; total < 7) (1) and/or ADAM questionnaire (YES to three questions other than question 1 and 7) and/or regular use of medical treatment for erectile dysfunction.
  • Motivation for permanent AAS cessation

Exclusion Criteria

• Established cardiovascular disease

  • Established diabetes of any kind 384
  • Congenital hypogonadal conditions (cryptorchidism, Klinefelter's disease, Kallmann's disease etc.)
  • Previous established hypogonadal conditions due to other causes than illicit use of AAS
  • Current or previous treatment with testosterone on other indication than AAS-induced male hypogonadism
  • Abnormal puberty development (small testes, late or absent pubic hairing, late or absent deepening of voice, etc.)
  • Current or previous pituitary diseases including pituitary tumors
  • Current or previous tumors of the hypothalamus
  • Current or former testicular cancer
  • Current or previous prostate cancer
  • Current or previous breast cancer
  • Other cancers unless complete remission ≥ 5 year
  • Other concomitant disease or makes the patient unsuitable to participate in the study
  • Severely impaired liver function
  • Allergy or hypersensitivity to the active substance (letrozole) or excipients of Letrozol "Accord"® listed in Appendix D
  • Allergy or hypersensitivity to the active substance (hCG) or excipients of Brevactid® listed in Appendix D
  • Established Lapp lactase deficiency or glucose/galactose malabsorption
  • Severe venous phlebitis or current or previous venous thromboembolism
  • Inguinal hernia
  • treatment which according to the investigators' assessment
  • Simultaneous participation in another clinical study
  • Unable to follow treatment instructions in terms of study medication instructions
  • Ongoing criminal behavior in terms of violence or illicit distribution of drugs
  • Currently or in the foreseeable future included in anti-doping programs

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Active Comparator - placebo	Placebo	Intervention: Intramuscular injection - placebo Intervention: Drug: placebo
Active comparator - treatment	Letrozole 2.5mg, hCG	Intervention: intramuscular injection - hCG Intervention: Drug: Letrozole

Primary Outcome Measures

Name	Time	Method
Change in plasma total testosterone concentration after 24 weeks from baseline	24 weeks

Secondary Outcome Measures

Name	Time	Method
Change in basal plasma pituitary gonadotropins, LH and FSH, after 24 and 50 weeks from baseline	24 and 50 weeks
Change in sperm motility after 24 and 50 weeks from baseline	24 and 50 weeks
Change in questionnaire score IIEF (erectile function and libido) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score ADAM (hypogonadism) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score of Major Depression Inventory (MDI) (depression) from baseline and after 24 and 50 weeks	24 and 50 weeks
Number of participants who adhere to AAS cessation after 24 and 50 weeks from baseline	24 and 50 weeks
Change in secretion of plasma pituitary gonadotropins, LH and FSH, in response to GnRH stimulation after 24 and 50 weeks from baseline	24 and 50 weeks
Change in sperm acrosome reaction after 24 and 50 weeks from baseline	24 and 50 weeks
Change in sperm DNA fragmenting after 24 and 50 weeks from baseline	24 and 50 weeks
Change in testicular size assessed using ultrasound after 24 and 50 weeks	24 and 50 weeks
Change in total plasma testosterone concentration after 50 weeks from baseline	50 weeks
Change in plasma total testosterone secretion in response to hCG stimulation after 24 and 50 weeks from baseline	24 and 50 weeks
Change in sperm count after 24 and 50 weeks from baseline	24 and 50 weeks
Change in sperm morphology after 24 and 50 weeks from baseline	24 and 50 weeks
Change in questionnaire score of (GAD7) (anxiety) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score of Buss-Perry Aggression scale (BPA) (hostility and aggression) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score of COBRA (Cognitive complaints in bipolar disorder rating assessment) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score of the Health Assessment Short Form-36 questionnaire from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score of Body-Q 349 (Perception of own body) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in questionnaire score of the Inventory of Interpersonal Problems 32-item (IIP32) from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in myocardial function assessed by myocardial flow reserve (mL/min/gr) by Rb-82 PET from baseline and after 24 and 50 weeks	24 and 50 weeks
Change in cardiac systolic function assessed using left ventricular ejection fraction (LVEF) obtained using echocardiography and 24 and 50 weeks from baseline.	24 and 50 weeks
Change in cardiac systolic function assessed using left ventricular global longitudinal strain (GLS) obtained using echocardiography and 24 and 50 weeks from baseline.	24 and 50 weeks
Change in cardiac structure (left ventricular mass) obtained using echocardiography and 24 and 50 weeks from baseline.	24 and 50 weeks

Trial Locations

Locations (1)

Rigshospitalet; 🇩🇰 Copenhagen, Denmark