Clinical trial to assess the safety and effectiveness of a study drug called CORT125134 in the treatment of Cushing's syndrome
- Conditions
- Endogenous Cushing’s SyndromeMedDRA version: 20.0Level: LLTClassification code 10011657Term: Cushings syndromeSystem Organ Class: 100000004860Therapeutic area: Body processes [G] - Physiological processes [G07]
- Registration Number
- EUCTR2016-000899-23-HU
- Lead Sponsor
- Corcept Therapeutics Incorporated
- Brief Summary
Not available
- Detailed Description
Not available
Recruitment & Eligibility
- Status
- ot Recruiting
- Sex
- All
- Target Recruitment
- 30
1. Is a male or female adult, 18–75 years of age
2. Has a diagnosis of endogenous Cushing’s syndrome confirmed by:
At least two of the following test criteria (Nieman 2008):
•Urinary free cortisol above the upper limit of normal (ULN) (50.0 µg/24 h) in at least 2, and up to 4, complete 24 hour collections within 3 weeks prior to Day 1 (baseline)
•Late-night salivary cortisol above the ULN (at least 2, and up to 4, collections using a salivette) within 3 weeks prior to Day 1 (baseline)
•Lack of cortisol suppression (>1.8 µg/dL serum cortisol) on either 1 mg overnight or 2-mg 48 hour dexamethasone suppression testing during screening or within 12 weeks before ICF is signed.
And
At least two of the following clinical signs and symptoms of Cushing’s syndrome:
•Facial characteristics of a Cushingoid appearance (moon facies, dorsocervical fat pad, plethora)
•Increased body weight or central obesity
•Proximal muscle weakness
•Low bone mass (dual energy X-ray absorptiometry [DXA] T < -1.0)
•Psychiatric symptoms (including depression or psychosis)
•Hirsutism and/or violaceous striae and/or acne
•Easy bruising
A patient with an adrenal lesion may alternatively qualify if there is
autonomous cortisol secretion based on dexamethasone suppression
testing (Fassnacht 2016) and supporting evidence of clinically significant
cortisol excess. Such a patient must have:
• Radiologically proven unilateral or bilateral adrenal disease (nodules,
hyperplasia)
• Lack of cortisol suppression (>5 µg/dL serum cortisol) on either 1-mg
overnight or 2-mg 48-hour dexamethasone suppression testing during
screening
• Low or suppressed ACTH (<10 pg/mL) to confirm ACTH-independency
• Presence of at least two comorbidities potentially related to cortisol
excess (eg, type 2 diabetes, hypertension, obesity, osteoporosis), of
which at least one is inadequately controlled by medical measures
3. Requires medical treatment of hypercortisolemia (i.e. those for whom surgery or radiation is contraindicated or has been refused)
Examples include, but are not limited to, patients with Cushing’s disease who are post-surgery and/or post-radiation for whom additional surgery is not recommended; de novo patients with Cushing’s disease who are not eligible for surgery due to comorbidities; and patients with ectopic ACTH-dependent Cushing’s syndrome in which the tumor cannot be localized or completely removed.
4. Meets at least one of the following criteria:
•Has type 2 diabetes mellitus as confirmed at screening visit with a fasting glucose >126 mg/dL and a 2-hour oral glucose tolerance test [oGTT] result for plasma glucose =200 mg/dL at 2 hours (Standards of Medical Care in Diabetes – 2015)
•Has impaired glucose tolerance (2-hour oGTT result for plasma glucose in the range of >140 mg/dL to <200 mg/dL) (Standards of Medical Care in Diabetes – 2015)
• Has hypertension (mean systolic BP of 130–170 mmHg and/or a mean diastolic BP of
85–110 mmHg) based on 24 hour ambulatory BP measurement (O’Brien 2013)
5. If taking antidiabetic medication, is on a stable dose (i.e. cannot start new medication or change dose within 4 weeks prior to the first dose of study drug)
6. If taking antihypertensive medication, is on a stable dose (i.e. cannot start new medication or change dose within 4 weeks prior to the screening ambulatory BP measurement)
7. Has potassium within the normal range (3.5–5.3 mEq/L) at screening or corrected to within the normal range by Day 1
1. Has a non-endogenous source of hypercortisolemia
2. Has pseudo-Cushing’s syndrome. Patients with known or suspected pseudo-Cushing’s syndrome based on medical history (such as patients with severe obesity, major depression, or a history of alcoholism) should undergo a dexamethasone-CRH/DDAVP stimulation test (Yanovski 1993, Giraldi 2007, Yanovski 1998) to rule-in or rule-out this possibility.
3. Has uncontrolled, clinically significant hypothyroidism or hyperthyroidism
4. Has poorly controlled hypertension, defined as systolic BP >170 mmHg or diastolic BP >110 mmHg at screening
5. Has Stage 4 renal failure (ie, glomerular filtration rate =29 mL/min)
6. Has elevated total bilirubin >1.5×ULN or elevated alanine aminotransferase (ALT) or aspartate aminotransferase (AST) >3×ULN
7. For patients with diabetes or abnormal oGTT at screening: Has
glycated hemoglobin (HbA1c) of >12% within 3 months of first dose of
study drug
8. Has a screening hemoglobin level of <9 g/dL
9. Has a clinically significant electrocardiogram (ECG) abnormality at screening, which, in the opinion of the Investigator, will make the patient an unsuitable candidate for the study
10. Has a confirmed screening QTcF interval >450 ms for males and >470 ms for females (using Fridericia’s correction) in the presence of a normal QRS interval (QRS <120 ms) or a history of additional risk factors for torsades de pointes
11. Is currently receiving chemotherapy for a tumor related to Cushing’s syndrome
12. Had radiation therapy for Cushing’s syndrome-related tumor within 1 year of screening period
13. Is planning surgery or radiation therapy for Cushing’s syndrome-related tumor during the study
14. Has used or plans to use any of the following treatments for Cushing’s syndrome, as specified:
•Adrenostatic medications: metyrapone, ketoconazole, fluconazole, aminoglutethimide, or etomidate from 4 weeks prior to baseline (Day 1) through the follow-up visit
•Adrenolytic medications:
oIn Group 1, any patients taking mitotane
oIn Group 2 only, patients with adrenocortical carcinomas taking mitotane whose dose has not been stable for at least 2 months prior to baseline (Day 1) or in whom increases in the mitotane dosage are expected through the end of dosing
•Neuromodulator drugs that act at the hypothalamic-pituitary level: serotonin antagonists (cyproheptadine, ketanserin, retanserin), dopamine agonists (bromocriptine, cabergoline), gamma-aminobutyric acid agonists (sodium valproate), and somatostatin receptor ligands (octreotide long-acting release [LAR], pasireotide LAR, lanreotide) from 8 weeks before baseline (Day 1) through the follow-up visit. Use of short-acting somatostatin analogs (octreotide, pasireotide) from 4 weeks prior to baseline (Day 1) through the follow-up visit.
•Mifepristone, from 6 weeks before baseline (Day 1) through the follow-up visit
15. Has started or increased (or plans to start or increase) the dose of an antidepressant medication (eg, selective serotonin reuptake inhibitors or tricyclic compound) from 6 weeks before baseline (Day 1) through the end of the study dosing period
16. Has started or increased (or plans to start or increase) the dose of a lipid-lowering drug from 4 weeks before baseline (Day 1) through the follow-up visit
17. Is lactating
18. Has an acute or unstable medical problem that could be aggravated by treatment with the investigational study drug
19. Has a history of hypersensitivity or severe reaction to
Study & Design
- Study Type
- Interventional clinical trial of medicinal product
- Study Design
- Not specified
- Primary Outcome Measures
Name Time Method
- Secondary Outcome Measures
Name Time Method