Clinical Validation of a Non-Invasive Diagnostic Test for Adrenal Insufficiency using Comparative Pharmacodynamic Equivalence in a Patient Population Salivary Test of Adrenal Response to Liquid Intranasal Tetracosactide - Study 3 (STARLIT-3)

开始日期2024-10-28

申办/合作机构

Sheffield Childrens Hospital NHS Foundation Trust

NCT06471829 / Recruiting临床2期

A Phase II, Multi-site, Open-label, Dose-titration Trial to Investigate the Safety, Tolerability, Pharmacokinetics, and Efficacy of Lu AG13909 in Adults With Cushing's Disease

This trial will evaluate the effects of Lu AG13909 in adult participants with Cushing's disease (CD). Cushing's disease is a rare and serious disorder where the body makes too much of a hormone called cortisol. The main goals of this trial are to learn about
1. the effect of Lu AG13909 on cortisol levels.
2. the safety and tolerability of Lu AG13909.
3. the pharmacokinetic parameters of Lu AG13909 (how the drug is absorbed, distributed, and processed by the body).

开始日期2024-06-19

申办/合作机构

H. Lundbeck A/S

NCT06363513 / Not yet recruitingN/AIIT

The Efficacy of Aescin in Combination With Micronized Purified Flavonoid Fraction (MPFF) in the Early Control of Bleeding From Acute Internal Hemorrhoids, A Randomized Controlled Trial

Hemorrhoidal disease, characterized by symptomatic enlargement and distal displacement of anal cushions, has been a subject of recognition and management for centuries. The etymology of "hemorrhoid" is traced back to the Greek words haima (blood) and rhoos (flow). Prevalent in over 20% of the population across various life stages, this anorectal condition impacts both genders. The multifaceted development of the disease incorporates theories encompassing abnormal dilation of hemorrhoidal plexuses, distension of arteriovenous anastomoses, prolapse of anal pads, and a myriad of genetic, anatomical, dietary, and lifestyle factors. Manifestations range from venous distension to bleeding and thrombosis, with classification based on location (internal/external/combined) and degree of prolapse (grade 1-4).
Upon comprehensive history-taking and examinations, including digital rectal and proctoscope assessments, a definitive diagnosis is established, leading to the treatment phase. Although outpatient procedures demonstrate efficacy, patients may persist with pain and discomfort. Medical intervention assumes significance for stages 1 and 2, incorporating approaches such as rubber-band ligation, injection sclerotherapy, and dietary modifications. Micronized Purified Flavonoid Fraction (MPFF), integral to hemorrhoid treatment, has been scrutinized for its ability to mitigate pathogenic processes culminating in acute bleeding. The stagnation of blood in vascular plexuses prompts an inflammatory response, activating white cells and increasing vessel wall permeability. MPFF's flavonoid compounds are posited to alleviate bleeding by augmenting venous tone, reducing stasis, inhibiting inflammatory mediators, and enhancing lymphatic drainage[8]. Multiple trials substantiate MPFF's efficacy in ceasing bleeding, alleviating symptoms, and preventing hemorrhoid relapse.
Aescin, a saponin mixture found in Aesculus hippocastanum (horse chestnut). The primary active component, β-aescin, contributes to the plant's medicinal attributes. Experimental investigations in animal models underscore its anti-edematous, anti-inflammatory, and venotonic properties, attributed to molecular mechanisms facilitating ion entry into channels and elevating venous tension. While the therapeutic benefits of aescin for hemorrhoids are acknowledged, the absence of randomized control trials impedes the conclusive validation of its efficacy. In the realm of diverse treatment options, this proposed randomized controlled trial aims to assess the comparative effectiveness of combining aescin with MPFF versus MPFF alone in managing hemorrhoid-related symptoms. The study aspires to furnish valuable insights for refining therapeutic strategies in the management of hemorrhoids and enhancing patient outcomes.

开始日期2024-04-01

申办/合作机构

Chiang Mai University

100 项与 ACTH receptor 相关的临床结果

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100 项与 ACTH receptor 相关的转化医学

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0 项与 ACTH receptor 相关的专利（医药）

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项与 ACTH receptor 相关的文献（医药）

2024-11-01·The Lancet Diabetes & Endocrinology

Aberrant hormone receptors regulate a wide spectrum of endocrine tumors

Review

作者: Louiset, Estelle ; Lefebvre, Hervé ; Kamenický, Peter ; Bourdeau, Isabelle ; Chasseloup, Fanny ; Lacroix, André ; Lopez, Antoine-Guy

Aberrant G-protein coupled receptor (GPCR) expression is highly prevalent in cortisol-secreting primary bilateral macronodular adrenal hyperplasia (PBMAH) and unilateral adenomas. The aberrant expression of diverse GPCRs and their ligands play an important role in the over-function of various endocrine tumours. Examples include aberrant expression of MC2R, 5-HT4R, AVPR1A, LHCGR, and GnRHR in primary aldosteronism; GCGR, LHCGR, and 5-HT4R in phaeochromocytomas and paragangliomas; TRHR, GnRHR, GIPR, and GRP101 in pituitary somatotroph tumours; AVPR2, D2DR, and SSTR5 in pituitary corticotroph tumours; GLP1R, GIPR, and somatostatin receptors in medullary thyroid carcinoma; and SSTRs, GLP1R, and GIPR in other neuroendocrine tumours. The genetic mechanisms causing the ectopic expression of GIPR in cortisol-secreting PBMAHs and unilateral adenomas have been identified, but distinct mechanisms are implicated in other endocrine tumours. Development of functional imaging targeting aberrant GPCRs should be useful for identification and for specific therapies of this wide spectrum of tumours. The aim of this review is to show that the regulation of endocrine tumours by aberrant GPCR is not restricted to cortisol-secreting adrenal lesions, but also occurs in tumours of several other organs.

2024-08-01·Clinical Endocrinology

Severe adrenal insufficiency in six neonates with normal newborn screening for CAH

Article

作者: Geckinli, Bilge ; Demir, Senol ; Guran, Tulay ; Ucar, Ahmet ; Ozcabi, Bahar ; Kurt, Ilknur ; Karagozlu, Selen ; Bulus, Derya ; Eser, Metin ; Ersoy, Aysenur ; Kahveci, Ahmet ; Guran, Omer

AbstractBackgroundNewborn screening (NBS) reduces the risk of mortality in congenital adrenal hyperplasia (CAH), mainly due to the salt‐wasting form of 21‐hydroxylase deficiency. There is limited knowledge regarding the results of NBS in non‐CAH primary adrenal insufficiency (non‐CAH PAI).Patients and MethodsClinical and NBS for CAH data of neonates who were diagnosed with non‐CAH PAI between January and December 2022 were examined.ResultsPatients (n = 6, 4 females) were presented with severe hyperpigmentation (n = 6), hypoglycemia (n = 4), hyponatremia (n = 3), hyperkalemia (n = 1), respiratory distress syndrome (n = 1) between 3rd hour to 2 months of life. All had normal NBS results. The median first‐tier 17‐hydroxyprogesterone (17OHP) concentration in NBS for CAH was 0.14 ng/mL (range; 0.05−0.85). Molecular studies revealed biallelic mutations in the MC2R (n = 4; 3 homozygous, 1 compound heterozygous), MRAP (n = 1) and STAR (n = 1) genes. Glucocorticoid with or without mineralocorticoid replacement was initiated once the diagnosis of non‐CAH PAI was established.ConclusionNeonates with non‐CAH PAI have always normal NBS due to persistently low 17OHP, even when these newborn infants are severely symptomatic for adrenal insufficiency. Clinicians should be alert for signs of adrenal insufficiency in neonates, even if the patient has a ‘normal’ screening for CAH, so as not to delay diagnosis and treatment. This fact should be kept in mind particularly in countries where these conditions are more common than elsewhere.

2024-08-01·Neuropeptides

Effects of an herbal adaptogen feed-additive on feeding-related hypothalamic neuropeptides in chronic cyclic heat-stressed chickens

Article

作者: Ardakani, Maryam Afkhami ; Greene, Elizabeth S ; Dridi, Sami

Heat stress (HS) is a global serious issue in the poultry industry with numerous adverse effects, including increased stress, depressed feed intake (FI), poor growth performance and higher mortality. Herbal adaptogens, plant extracts considered as stress response modifiers, are metabolic regulators that improve an organism's ability to adapt to and minimize damage from environmental stresses. Previously, we showed that herbal adaptogen supplementation increased FI and body weight (BW) of broiler (meat-type) chickens reared under HS conditions. Therefore, we hypothesized that these effects may be mediated through modulation of hypothalamic feeding-related neuropeptides. Male Cobb 500 chicks were reared in 12 environmental chambers with three diets: a corn-soybean-based diet (C) and two herbal adaptogen-supplemented diets at 500 g/1000 kg (NR-PHY-500) and 1 kg/1000 kg (NR-PHY-1000). Broilers in 9 chambers were exposed to chronic cyclic HS (35 °C for 8 h/day) from d29 to d42, while 3 chambers were maintained at 24 °C (thermoneutral, TN) for all 42 days. Hypothalamic samples were collected on d42 from each group, both before the onset of HS (Pre-HS) that day and after 3 h of HS (post-HS). Hypothalamic expressions of neuropeptide Y (NPY) receptors Y4 and Y7, Corticotropin-releasing hormone (CRH), orexin receptor 1 (ORXR1), melanocortin receptors (MC1R, MC4R, and MC5R), visfatin and neurosecretory protein GL (NPGL) genes were significantly upregulated by adaptogen supplementation. The hypothalamic expression of MC2R was affect by period, with a significant upregulation during post-HS phase. There was a significant period by treatment interaction for hypothalamic orexin and adiponectin expression. The hypothalamic expression of NPY, Y1, Y2, Y5, Y6, proopiomelanocortin (POMC), cocaine and amphetamine regulated transcript (CART), agouti-related peptide (AgRP), ORXR2, AdipR1/2, MC3R, and ghrelin was not affected by diet supplementation nor by HS exposure. In conclusion, these findings suggest that in-feed supplementation of adaptogen might improve FI and growth via modulation of hypothalamic feeding-related neuropeptides in heat-stressed broilers.

项与 ACTH receptor 相关的新闻（医药）

2024-08-05

·GlobeNewswire-Health Care

OMass Therapeutics Selected by Fierce Biotech as a “Fierce 15” Winner for 2024

PRESS RELEASE OMass Therapeutics Selected by Fierce Biotech as a “Fierce 15” Winner for 2024 Oxford, United Kingdom – 5th August 2024 – OMass Therapeutics (‘OMass’ or ‘the Company’), a biotechnology company identifying medicines against highly validated target ecosystems such as membrane proteins or intracellular complexes, today announces that it has been named by Fierce Biotech as one of 2024’s ‘Fierce 15’ biotechnology companies. The annual Fierce 15 companies are selected for being the most innovative and promising biotechnology companies in the industry and highlights OMass as one of the most ambitious and successful next generation biopharma companies. Ros Deegan, Chief Executive Officer at OMass Therapeutics, commented: “OMass is redefining drug discovery for previously intractable targets by fundamentally innovating the process and it is an incredible honour to be recognised by Fierce Biotech as one of the Fierce 15. Over the past year OMass made significant progress in translating the outputs of our proprietary platform into an exciting pipeline of novel drugs including advancing the development of our lead program, an insurmountable antagonist of the MC2 receptor for Congenital Adrenal Hyperplasia towards the clinic. This recognition is a testament to the dedication and hard work of our team and underlines our progress so far as well as our ambition to become a fully integrated pharma company bringing to market medicines that meaningfully improve patient lives.” Originally spun out of Oxford University, OMass has industrialised the groundbreaking research by the highly-awarded Oxford-based scientist, Professor Dame Carol Robinson. The Company is a world leader in the application of native mass spectrometry (MS) to drug discovery and has selected a number of high-value targets and is developing potent small molecule drugs with high therapeutics potential against these. Its proprietary platform, OdyssION™, integrates novel biochemistry techniques, with next-generation native MS, and custom chemistry, to allow for the interrogation of protein interactions within their native ecosystem while avoiding the confounding complexity of the cell demonstrated in its in-house pipeline. OMass has already made significant progress with its portfolio of highly-validated, yet intractable or inadequately drugged targets. OMass’ lead programme is an insurmountable antagonist of the GPCR MC2 receptor for Congenital Adrenal Hyperplasia which is expected to complete IND-enabling studies in 2025. OMass additionally has a novel immunology portfolio including a SLC15A4 antagonist for lupus, a GPR65 agonist for the treatment of Inflammatory Bowel Disease, and inhibitors of cGAS for inflammatory disorders. OMass’s goal is to ultimately evolve into a fully integrated biopharma company that can take products to market whilst continuing to discover medicines in high unmet need indications within rare and immunological diseases. The Company will also explore collaborations and partnerships both in and outside of its core focus to ensure its platform is maximally exploited to the benefit of patients. OMass has recently expanded its facilities and team, moving into purpose designed facilities on Advance Research Cluster Oxford, recruiting key executives and team members bringing its headcount to 57, and, notably, attracting Boston-based Industry-leader James (Jim) Geraghty as independent chair of its Board of Directors, bringing US and international experience from Genzyme and as NED and chair of multiple listed biotechs. “For the past 22 years, we have evaluated hundreds of companies for inclusion in the ‘Fierce 15’ special report. Our selection process considers various factors, including technological robustness, strategic partnerships, venture support and market positioning,” said Ayla Ellison, Editor-in-Chief, Fierce Life Sciences and Healthcare. “This report highlights innovation and creativity amid intense competition.” -ENDS- For further information, please contact: OMass Therapeutics ICR Consilium Rosamond Deegan, Chief Executive OfficerPhone: +44 (0) 1235 527589Email: ros.deegan@omass.comSue Charles / Suki Virji / Kumail WaljeePhone: +44 (0)20 3709 5700 Email: omass@icrhealthcare.com About OMass Therapeutics OMass Therapeutics is a biotechnology company discovering medicines against highly- validated target ecosystems, such as membrane proteins or intracellular complexes. The company’s unique OdyssION™ technology platform comprises novel biochemistry techniques, next-generation native mass spectrometry, and custom chemistry. This allows OMass to interrogate not just the target, but also the interaction of the target with its native ecosystem, separate from the confounding complexity of the cell. The result is cell-system fidelity with cell-free precision. OMass is advancing a pipeline of small molecule therapeutics in rare diseases and immunological conditions, that target solute carriers, complex-bound proteins, and GPCRs. Headquartered in Oxford, UK, OMass has raised over $160M (£129M) from a top-tier international investor syndicate, including Syncona, Oxford Science Enterprises, GV, Northpond Ventures, Sanofi Ventures and British Patient Capital. To learn more, please visit www.omass.com. Follow us on LinkedIn and X. About Fierce Biotech Fierce Biotech is the biotech industry’s daily monitor, providing the latest news, articles, and resources related to clinical trials, drug discovery, FDA approval, FDA regulation, patent news, pharma news, biotech company news and more. More than 300,000 top biotech professionals rely on Fierce Biotech for an insider briefing on the day’s top stories.

2024-07-02

·BioSpace

Lilly Inks Radiopharma Deal With Radionetics, Secures Right to Buy Biotech

Pictured: Eli Lilly biotechnology center in California/iStock, JHVEPhoto Eli Lilly on Monday signed a strategic partnership with Radionetics Oncology, which not only provides the pharma with a pipeline of promising cancer radiotherapeutics but also gives it the exclusive right to buy the San Diego biotech down the line. The agreement includes a $140 million upfront payment from Lilly as well as the potential right to acquire Radionetics for $1 billion. The companies did not provide specific details or a timeline for the potential buyout but said that it would occur “upon the conclusion of an exercise period.” Jacob Van Naarden, president of Lilly oncology, in a statement said that the partnership with Radionetics gives the pharma “access to novel GPCR targets” and the robust discovery capabilities of the biotech. Radionetics focuses on the development small molecule radiopharmaceuticals. The biotech targets GPCRs, a large family of membrane proteins that help transmit signals from outside the cell inside. According to its website, GPCRs represent a “vast and largely unexplored” class of targets for radiopharmaceuticals. Radionetics contends it leverages a “vast knowledge of GPCR biology” combines it with its platform’s “unrivaled proficiency” in designing small molecule drugs, resulting in highly selective radiopharma therapies. The approach “uniquely pairs the power of radiopharmaceuticals with the precision of small molecule targeting to novel GPCRs,” COO Brett Ewald said in a statement. Radionetics’ GPCR-targeting drug development technology has resulted in its lead candidate 68Ga-R8760, a gallium-based radioligand conjugate that targets the MC2R protein, which is highly expressed in the rare cancer adrenocortical carcinoma. The biotech kicked off the Phase I study of 68Ga-R8760 in October 2023 and announced plans to launch clinical programs in breast and lung cancer. For Lilly, Monday’s partnership with Radionetics continues its recent investment spree in the radiopharma space. In October 2023, the pharma snapped up Point Biopharma for $1.4 billion. The acquisition, closed in December 2023, gave Lilly ownership of PNT2002, Point’s lead asset and an investigational radioligand therapy for metastatic castration-resistant prostate cancer. At the time, Van Naarden said that the Point acquisition signaled the “beginning of our investment in developing multiple meaningful radioligand medicines for hard-to-treat cancers.” In May 2024, Lilly partnered with Aktis Oncology for $60 million upfront and the promise of $1.1 billion in royalties. The deal gave Lilly worldwide rights to develop certain radiopharma therapies and diagnostics discovered by Aktis based on specific targets. Tristan Manalac is an independent science writer based in Metro Manila, Philippines. Reach out to him on LinkedIn or email him at tristan@tristanmanalac.com or tristan.manalac@biospace.com.

并购临床1期

2024-06-05

·GlobeNewswire-Health Care

Crinetics Announces Positive Initial Findings at ENDO 2024 for Atumelnant in Two Ongoing, Open-Label Studies for the Treatment of Congenital Adrenal Hyperplasia (CAH) and ACTH-Dependent Cushing’s Syndrome (ADCS)

100% of Participants (n=6) With CAH Maintained Androstenedione (A4) Below the Upper Limit of Normal at all Time Points on Atumelnant (80 mg) CAH Participants Achieved More Than a 90% Reduction of A4 and 97% Reduction of 17-OHP on Atumelnant (80 mg), Beginning at Two Weeks and Sustained Through 12 Weeks In the ADCS Trial, Atumelnant (80 mg) Normalized 24-hr Urinary Free Cortisol Levels for 100% of Participants (n=5) During Treatment Management to Host Investor Conference Call Today at 4:30 PM ET and Onsite KOL Event at ENDO for Investors and Analysts at 6:00 PM ET June 03, 2024 -- Crinetics Pharmaceuticals, Inc. (Nasdaq: CRNX) today announced initial findings from the development program of its second clinical product candidate, atumelnant* (CRN04894), a novel, once-daily oral adrenocorticotropic hormone (ACTH) receptor antagonist. The results, presented at the Endocrine Society’s annual meeting (ENDO2024), include initial data from the Phase 1b/2a, open-label study in participants with ACTH-dependent Cushing’s syndrome (ADCS) conducted in collaboration with the National Institutes of Health, and the Phase 2 open-label TouCAHn study in participants with congenital adrenal hyperplasia (CAH). “Despite knowing about ACTH’s pivotal role in the endocrine stress response for nearly a century, no other ACTH antagonist drug candidates have been developed and studied in humans. Achieving physiologically normal hormone levels is critical for people living with CAH and ADCS, and today’s data show an impressive ability of atumelnant to reduce key disease drivers like A4 or cortisol to healthy levels,” said Scott Struthers, Ph.D., founder and chief executive officer of Crinetics. “These data also reinforce the strength of our in-house discovery engine and our ability to purposefully design medicines with groundbreaking mechanisms of action like atumelnant, the second novel drug candidate in our pipeline to have demonstrated remarkable results in clinical studies.” *Proposed international nonproprietary name under review In this initial analysis of this Phase 2 trial (TouCAHn), people with classic CAH were treated with once-daily, oral atumelnant and assessed for safety and efficacy. The trial continues to enroll three treatment cohorts: 80 mg once daily (n=9), 40 mg once daily (n=9) and 120 mg once daily (n=6). Data presented at ENDO (n=10) reflect a cutoff date of May 21, 2024. Available data for 80 mg includes: n=4 at 12 weeks of treatment, with two additional participant’s data up to six weeks of treatment. For 40 mg, available data was with n=4 for two weeks of treatment. The TouCAHn study is ongoing, with topline results from the complete study expected in the second half of 2024. Baseline biomarker levels for subjects in Cohort 1 were: Androstenedione (A4) mean: 838 ng/dL 17-hydroxyprogesterone (17-OHP) mean: 9,880 ng/dL Initial results from Cohort 1: Atumelnant resulted in profound, rapid and sustained reductions in key adrenal steroids that are hallmarks of CAH. 100% of participants had A4 levels below the upper limit of normal (ULN) at two weeks with atumelnant, which was sustained through 12 weeks. A4 reductions, a potential endpoint in registrational trials, from the baseline mean were: 91% at two weeks (n=6) 93% at six weeks (n=6) 96% at 12 weeks (n=4) 17-OHP changes in serum levels from the baseline mean were: 97% at two weeks (n=6) 95% at six weeks (n=6) 94% at 12 weeks (n=4) Two-week data from the first four patients in Cohort 2 (40 mg atumelnant once daily) are also presented at ENDO2024. No severe or serious treatment emergent adverse events have been observed to date, and no participants have discontinued from the trial. All AEs to-date have been mild to moderate and transient. There were no significant changes in safety labs or electrocardiograms. The most common treatment-emergent adverse events included: fatigue (3), headache (2) and upper respiratory tract infection (2). “In CAH, androgen production can go into overdrive and have a profound effect on people living with this difficult-to-manage disease,” said Dr. Umasuthan Srirangalingam, consultant physician in endocrinology and diabetes at University College London Hospitals NHS Foundation Trust and TouCAHn investigator. “Atumelnant’s unique ability to inhibit ACTH directly at its receptor sets it apart from how we’ve historically pursued controlling androgen production through supra-physiological doses of glucocorticoids. It’s compelling to see initial Phase 2 results showing atumelnant dramatically reduced A4 and 17-OHP.” Initial data from five ACTH-dependent Cushing’s syndrome trial participants who completed 10 days of once- daily oral atumelnant treatment (80 mg) in this dose-finding study shows rapid and profound impact on cortisol: In all participants, 24h urine free cortisol was below the upper limit of normal during the treatment period even while receiving oral hydrocortisone replacement. UFC normalization has been recommended by the U.S. Food and Drug Administration as a primary endpoint for drugs that decrease cortisol levels in Cushing’s syndrome. All five participants (100%) experienced serum cortisol Two or more clinical symptoms improved in all patients. “This initial data showed atumelnant’s ability to rapidly reduce — and normalize — cortisol levels in people with ADCS,” said Dr. Lynnette Nieman, senior investigator, National Institutes of Health, and principal investigator of the Phase 1b/2a atumelnant trial. “As a clinician and investigator, I’ve witnessed the unmet needs in this patient population for 40 years. I am hopeful for further promising results as we continue our research on this drug candidate.” Atumelnant was generally well tolerated. Adverse events were mild to moderate, with the most frequently reported being headache, nausea and decreased appetite, consistent with symptoms of adrenal insufficiency. Predefined biochemical adrenal insufficiency (morning serum cortisol Atumelnant, our second investigational compound, is the first once-daily, oral adrenocorticotropic hormone (ACTH) receptor antagonist that acts selectively at the melanocortin type 2 receptor (MC2R) on the adrenal glands. Diseases associated with excess ACTH can have significant impact on physical and mental health. Atumelnant has exhibited strong binding affinity for MC2R in preclinical models and has demonstrated suppression of adrenally derived glucocorticoids and androgens that are under the control of ACTH. Data in a Phase 1 healthy volunteer study demonstrated pharmacologic proof-of-concept for atumelnant, with reductions in both serum cortisol levels and 24-hour urine free cortisol excretion in the presence of sustained, disease-like ACTH concentrations. Atumelnant is currently in Phase 2 studies for Congenital Adrenal Hyperplasia and ACTH-dependent Cushing’s syndrome. TouCAHn is an open-label, global, Phase 2 study designed to evaluate the efficacy, safety, and pharmacokinetics of atumelnant when administered up to 12 weeks in participants with CAH caused by 21-hydroxylase deficiency. The study is ongoing and aims to enroll up to 30 patients, aged 18-75, with classic CAH and on a stable dose of glucocorticoid replacement for at least 6 months. Key endpoints include early morning androstenedione (A4), 17-hydroxyprogesterone (17-OHP) levels and safety. The Phase 1b/2a, is the first-in-disease, open-label, multiple-ascending dose exploratory study to evaluate safety, tolerability, pharmacokinetics, and pharmacodynamic biomarker responses associated with atumelnant over a 10-day treatment period in participants with ACTH-dependent Cushing's syndrome. The study is being conducted in collaboration with the National Institutes of Health and led by Dr. Lynnette Nieman. Participants will receive oral atumelnant once daily for 10 days, followed by monitoring during four wash-out days. The study is ongoing and aims to enroll 18 people. The content in this release is the sole responsibility of Crinetics Pharmaceuticals, Inc. and does not necessarily represent the official views or imply endorsement of the National Institutes of Health. For more information about the study, please visit clinicaltrials.gov (NCT05804669). Crinetics Pharmaceuticals is a clinical stage pharmaceutical company focused on the discovery, development, and commercialization of novel therapeutics for endocrine diseases and endocrine-related tumors. Paltusotine, an investigational, first-in-class, oral somatostatin receptor type 2 (SST2) agonist, is in Phase 3 clinical development for acromegaly and in Phase 2 clinical development for carcinoid syndrome associated with neuroendocrine tumors. Crinetics is also developing atumelnant (CRN04894), an investigational, first-in-class, oral ACTH antagonist, that is currently completing Phase 2 clinical studies for the treatment of congenital adrenal hyperplasia and ACTH-dependent Cushing’s syndrome. All of the company’s drug candidates are orally delivered, small molecule new chemical entities resulting from in-house drug discovery efforts, including additional discovery programs addressing a variety of endocrine conditions such as hyperparathyroidism, polycystic kidney disease, Graves’ disease, thyroid eye disease, diabetes and obesity. The content above comes from the network. if any infringement, please contact us to modify.