"We were thrilled to share our just published primary CAHtalyst Phase 3 data with ENDO 2024 attendees this past weekend," said Eiry W. Roberts, M.D., Chief Medical Officer at
CAHtalystTM Phase 3 Pediatric and Adult Data
In an oral presentation on
In a poster presentation on
CAHtalogTM Registry—Negative Impacts of Supraphysiologic Dosing in Patients with CAH
A real-world study explored the effects of high GC doses in pediatric and adult patients enrolled in the CAHtalog registry, highlighting the fluctuations in GC dose and androstenedione over time and the relationship between higher GC dose and negative clinical outcomes in patients with CAH (Poster #SUN-685). The findings included:
- Among 44 pediatric patients, 12 (27.3%) received a high GC dose (>15 mg/m2/day), that was associated with:
- Premature adiposity rebound starting at ~2 years of age (usual age is ~6 years)
- Early growth acceleration attributed to advanced bone age, followed by blunted pubertal growth
- In 69 patients (45 pediatric, 34 adult and 10 in both groups) with available comorbidity-related data, hypertensive diseases and metabolic complications were significantly more prevalent with high versus low GC doses
- In pediatric patients, short stature was more common with high versus low GC dose
- In 40 patients (27 pediatric, 14 adult and 1 in both groups) with ≥ 3 matched GC-androstenedione records, 92% had ≥ 1 transition in health state over the median 7-year observation period
- Higher GC dose with androstenedione < upper limit of normal (ULN) was the most common health state observed at the first recorded datapoint (48%), with only 3% maintaining that health state throughout the observation period
- Although 22% of patients presented with lower GC and androstenedione <ULN at the start of the observation period, none sustained this health state throughout the observation period; all patients (100%) had a higher GC dose and/or loss of androstenedione control at some point in their health state patient journey
- Limitations included absence of temporal context, variation in observational period and number of records per patient and blood draw timing
"Higher rates of overweight/obesity, hypertensive and metabolic comorbidities related to high glucocorticoid dosing and androgen excess were seen across all age groups in this study," said Oksana Lekarev, D.O., Associate Professor of
CAHtalogTM Registry—Natural History of CAH
The results of a longitudinal study were presented using medical records from the CAHtalog registry and provided insight into the natural history of classic CAH, including the height and weight trends that carry across pediatric and adult patient groups (Poster# SUN-417). Data were analyzed from 42 pediatric patients (55% female) and 32 adult patients (72% female) enrolled in the registry. Median duration of observation was 9 years in pediatric patients and 13 years in adults. The findings included:
- Pediatric patients had early growth acceleration followed by blunted pubertal growth. This trend was more pronounced in females, with mean height-for-age generally exceeding the 90th percentile at ages 4–10 years but dropping below 50th percentile at ages 13–17 years.
- Mean bone age-to-chronological age ratios were highest in females aged 5 years and males aged 7 years.
- The mean body mass index (BMI)-for-age consistently exceeded the 85th percentile (i.e., overweight or obese) in males aged ≥ 5 years and females aged ≥ 6 years.
- Across adult age groups in both sexes, median BMI met the threshold for overweight (≥ 25 kg/m2) or obesity (≥30 kg/m2).
- 83% of female patients (all ages) and 100% of male patients had a BMI ≥ 25 kg/m2
- 74% of female patients and 33% of males had a BMI ≥ 30 kg/m2
- Obesity, hypertension, fatigue, acne, and hyperlipidemia were common, particularly among adults. Among adults, the comorbidity of obesity (68%) was more prevalent than in the general population (42%).
Analyses of these real-world data highlight the limitations of current conventional GC therapies, which usually require supraphysiologic doses to manage adrenal androgen excess. High rates of comorbidities related to GC treatment and androgen excess indicate the challenges with current GC treatments in maintaining androgen control without causing adverse effects.
"CAHtalog Registry data reveals a persistent abnormal growth pattern in children, characterized by accelerated growth in early childhood and deceleration in adolescence, along with early obesity that was sustained into adulthood," said
Claims-Based Cohort Analysis—Disease- and GC-Related Comorbidities in CAH
A retrospective cohort study was conducted analyzing insurance claims from 2020-2022 within the Merative MarketScan commercial and Medicaid databases (Poster #SUN-437). The frequency of comorbidities related to adrenal androgen excess and/or supraphysiologic GC dosing was captured using International Classification of Diseases, 10th Revision (ICD-10) codes. Matching between the CAH and general population (GenPop) cohorts was based on age, sex, payer type, region and enrollment duration with a 1:5 ratio (CAH:GenPop). Compared with GenPop, CAH patients had significantly greater rates of multiple chronic conditions related to both excess adrenal androgens and supraphysiologic GC doses, including short stature, anxiety disorders, and diabetes.
- Top significant comorbidities in adults with CAH versus GenPop:
- Anxiety disorders—34% versus 26%
- Fatigue—27% versus 18%
- Depression—26% versus 19%
- Obesity—23% versus 13%
- Hirsutism/excess hair (female only)—11% vs 1%
- Top significant comorbidities in pediatric patients with CAH versus GenPop
- Obesity—14% versus 5%
- Fatigue—13% versus 6%
- Anxiety disorders—12% versus 8%
- Hirsutism/excess hair (female only)—11% versus 1%
- Acne—10% versus 6%
"These data show a statistically higher clinical burden of CAH compared with a matched control, with patients of all ages suffering comorbidities that result from high adrenal androgens, such as short stature and hirsutism, and from supraphysiologic GC dosing, such as cardiovascular disease, metabolic disorders, and bone loss,"
- (OR20-05): CAHtalyst: Results from the Randomized, Double-Blind, Placebo-Controlled Period of a Phase 3 Trial of Crinecerfont, a Corticotropin-Releasing Factor Type 1 Receptor (CRF1) Antagonist, in Adults with Classic Congenital Adrenal Hyperplasia
- (Poster #SUN-441): CAHtalyst: Results from the Randomized, Double-Blind, Placebo-Controlled Period of a Phase 3 Trial of Crinecerfont, a Corticotropin-Releasing Factor Type 1 Receptor (CRF1) Antagonist, in Children and Adolescents with Classic Congenital Adrenal Hyperplasia
- (Poster #SUN-685): Negative Impacts of Supraphysiologic Glucocorticoid Dosing in Patients with Classic Congenital Adrenal Hyperplasia: An Analysis of Data from the CAHtalog™ Registry
- (Poster #SAT-437): Disease- and Glucocorticoid-related Comorbidities in Classic Congenital Adrenal Hyperplasia: A Claims-Based Retrospective Cohort Analysis
- (Poster #SUN-417): Natural History of Classic Congenital Adrenal Hyperplasia: Results from Pediatric and Adult Patients in the CAHtalog Registry
- (Poster #MON-676, RF36-01): CHAMPAIN Study: Initial Results from a Phase II Study of Efficacy, Safety and Tolerability of Modified-Release Hydrocortisones: Chronocort® (Efmody®) versus Plenadren, in Primary Adrenal Insufficiency
- (Poster #SAT-427): Incidence of Adrenal Crisis in Congenital Adrenal Hyperplasia (CAH) Patients During a Prospective Monitored Long-Term Study of Modified-Release Hydrocortisone (MRHC) Capsules, (Efmody)
- (Poster #SAT-412): Morning Cortisol Levels in Patients with Established Primary Adrenal Insufficiency
About Congenital Adrenal Hyperplasia
Congenital adrenal hyperplasia (CAH) is a rare genetic condition that results in an enzyme deficiency that alters the production of adrenal hormones which are essential for life. Approximately 95% of CAH cases are caused by a mutation that leads to deficiency of the enzyme 21-hydroxylase. Severe deficiency of this enzyme leads to an inability of the adrenal glands to produce cortisol and, in approximately 75% of cases, aldosterone. If left untreated, CAH can result in salt wasting, dehydration, and even death.
Glucocorticoids (GCs) are currently used not only to correct the endogenous cortisol deficiency, but doses used are higher than cortisol replacement needed (supraphysiologic) to lower the levels of adrenocorticotropic hormone (ACTH) and adrenal androgens. However, glucocorticoid treatment at supraphysiologic doses has been associated with serious and significant complications of steroid excess, including metabolic issues such as weight gain and diabetes, cardiovascular disease, and osteoporosis. Additionally, long-term treatment with supraphysiologic GC doses may have psychological and cognitive impact, such as changes in mood and memory. Adrenal androgen excess has been associated with abnormal bone growth and development in pediatric patients, female health problems such as acne, excess hair growth and menstrual irregularities, testicular rest tumors in males, and fertility issues in both sexes.
To learn more about CAH, click here.
About Crinecerfont and the CAHtalystTM Studies
Crinecerfont is an investigational, oral, selective corticotropin-releasing factor type 1 receptor (CRF1) antagonist being developed to reduce and control excess adrenocorticotropic hormone (ACTH) and adrenal androgens through a glucocorticoid-independent mechanism for the treatment of congenital adrenal hyperplasia (CAH) due to 21-hydroxylase deficiency. Antagonism of CRF1 receptors in the pituitary has been shown to decrease ACTH levels, which in turn decreases the production of adrenal androgens and potentially the symptoms associated with CAH. Our data demonstrate that lowering adrenal androgen levels enables lower, more physiologic dosing of glucocorticoids and thus could potentially reduce the complications associated with exposure to greater than normal glucocorticoid doses in patients with CAH.
The CAHtalyst™ Pediatric and Adult Phase 3 global registrational studies are designed to evaluate the safety, efficacy, and tolerability of crinecerfont in children and adolescents, and adults respectively, with congenital adrenal hyperplasia due to 21-hydroxylase deficiency. The primary portions of the CAHtalyst Phase 3 studies have completed and enrollment is closed, while the open-label extension treatment portions of both studies are ongoing. Data from the CAHtalyst Pediatric and CAHtalyst Adult Phase 3 studies supported two New Drug Application submissions to the
To learn more about crinecerfont and the CAHtalyst studies, click here.
About the CAHtalog™ Registry
In 2021, the
About
(*in collaboration with AbbVie)
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Neurocrine Biosciences, Inc. Media: Linda Seaton, 1-858-617-7292, media@neurocrine.com; Investors: Todd Tushla, 1-858-617-7143, ir@neurocrine.com