Clinical Trial Details
— Status: Recruiting
Administrative data
| NCT number |
NCT04543253 |
| Other study ID # |
19-006003 |
| Secondary ID |
|
| Status |
Recruiting |
| Phase |
|
| First received |
|
| Last updated |
|
| Start date |
July 25, 2019 |
| Est. completion date |
December 2025 |
Study information
| Verified date |
November 2023 |
| Source |
Mayo Clinic |
| Contact |
Melinda Thomas |
| Phone |
507-293-6628 |
| Email |
thomas.melinda[@]mayo.edu |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Observational
|
Clinical Trial Summary
Cushing syndrome (CS) is an endocrine disorder caused by chronic exposure to glucocorticoid
(GC) excess. Endogenous CS has an estimated incidence of 0.2 to 5.0 cases per million per
year and prevalence of 39 to 79 cases per million in various populations. CS usually affects
young women, with a median age at diagnosis of 41.4 with a female-to-male ratio of 3:1.
Following a curative surgery for CS, patients develop adrenal insufficiency and require GC
replacement postoperatively until the hypothalamic-pituitary-adrenal (HPA) axis recovery
occurs. Factors, such as age, gender, BMI, subtypes of CS, duration of symptoms, clinical and
biochemical severity and postoperative GC dose have been reported to affect the HPA recovery
in small retrospective studies. Glucocorticoid withdrawal syndrome (GWS) is a withdrawal
reaction due to decrease in supraphysiological GC concentrations, which occurs after a
successful surgery of CS. Glucocorticoid withdrawal syndrome (GWS) is under-recognized entity
in patients undergoing curative surgery for endogenous Cushing syndrome.
In this study we aim to determine pre- and post-surgical predictors of the duration and
severity of glucocorticoid withdrawal in patients undergoing a curative surgery for cortisol
excess and assess the effect of MUSE intervention on GWS severity in patients undergoing
curative surgery for CS as compared to standard of care.
Description:
Specific Aim 1: To determine pre- and post-surgical predictors of the duration and severity
of glucocorticoid withdrawal in patients undergoing a curative surgery for cortisol excess
Specific Aim 2: To characterize the timing and recovery of hypercortisolism-induced signs and
symptoms, proximal myopathy and tissue accumulation of Advanced Glycation End products (AGEs)
in patients after a curative surgery Specific Aim 3: To assess the effect of MUSE
intervention on GWS severity in patients undergoing curative surgery for CS as compared to
standard of care
1. Selection of study subjects and medical records review. We will prospectively recruit
adult patients with CS of any three subtypes (pituitary, adrenal or ectopic CS) and MACS
undergoing a curative surgery, from the pituitary clinic. Investigator will discuss
participation in the study and obtain an informed consent. We will review data for any
potential risk factors through clinical interview and review of medical record. Data
will include demographics, behavioral factors (smoking and alcohol consumption), past
medical history (history of AI, psychiatric disorder and recent GC usage), GWS related
symptoms and signs (anorexia, nausea, emesis, lethargy, somnolence, arthralgia, myalgia,
fever, hypotension), and lab tests.
2. Subjects: We will enroll 100 consecutive subjects in this study who will participate in
this study for up to 2 years. Inclusion and exclusion criteria are as below. We plan to
have 50 subjects participate in the intervention arm with MUSE in one year, without
modifying other study procedures.
3. Step-by-Step methods:
- Patients will be identified by their clinician. Permission will be obtained from
the patient in order for one of the investigators to explain the study and obtain
informed written consent.
- Baseline history, physical examination, and the necessary baseline tests will be
performed based on standard of care and as considered necessary by the treating
physician.
- Medical record will be reviewed for demographic information, comorbidities, medical
therapy, imaging information and biochemical testing results
- We will use a scoring system to quantify biochemical severity, and to classify
clinical abnormalities as mild, moderate and severe ( based on existent laboratory
and clinical parameters).
- At baseline, all patients will be asked to complete the Cushing QoL questionnaire,
SF36 and AddiQol questionnaires (forms are attached in Document). Patients will
discuss the intervention with MUSE with the study investigator. If they agree to
participate in the intervention arm, they will be instructed on its use.
- At follow up, patients will complete AddQoL survey (weekly in the first 3 months,
every 4 weeks in the next 6 months, every 3 months in the next 12 months, and then
every 6 months until the end of the study) and SF36 survey (every 3 months) until
the end of the study. (In-person, through a paper survey or electronically using
external REDCap server (user name and password protected)).
- For patients in the intervention group, in addition to the above, at the time of
enrollment, the study coordinator will help set up the MUSE application on to iPad
or iPhone or Android phone (we will use generic login name and password without
protected health information included). The coordinator will also go over a few
helpful hints and discuss the homework log, which will need to be completed
throughout the course of the study. After the surgery, patients are asked to
complete the 3 minute 'focusing' exercise daily until 12 weeks after the surgery.
During this time frame we will download the data from our end on a weekly basis.
After 12 weeks, the frequency of the usage will be at the participant's discretion
although ongoing usage is encouraged and data download should continue. In
addition, we ask that patients bring iPad, iPhone or Android phone to each of the
clinical visit for an app interrogation.
- Patient will participate in the study until one of the following: 1) 2 years of
follow up completed, 2) patient withdraws consent, 3) HPA axis recovery is achieved
and patient weans off GC, 4) completion of the study by the principal investigator.
