Open-label extension study to evaluate the safety of long-term twice-monthly administration of somavaratan in adults with Growth Hormone Deficiency (GHD).

开始日期2016-02-11

申办/合作机构

Versartis, Inc.

EUCTR2015-002072-24-DE / Not yet recruiting临床2期

An Open-Label, Dose Finding, International Phase 2 Study with Once Monthly Subcutaneous Somavaratan (VRS-317) in Adult Growth Hormone Deficiency (GHD)Versartis International Trial in Adults with Long Acting Growth Hormone. The VITAL study - Versartis International Trial in Adults with Long Acting Growth Hormone (VITAL)

开始日期2015-10-22

申办/合作机构

Versartis, Inc.

100 项与 Somavaratan 相关的临床结果

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100 项与 Somavaratan 相关的转化医学

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100 项与 Somavaratan 相关的专利（医药）

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项与 Somavaratan 相关的文献（医药）

2021-06-26·World Journal of Clinical Cases

Growth hormone cocktail improves hepatopulmonary syndrome secondary to hypopituitarism: A case report

作者: Wang, Xi ; Nie, Min ; Mao, Jiang-Feng ; Wu, Xue-Yan ; Ji, Wen ; Zhang, Hong-Bing

BACKGROUNDMetabolic associated fatty liver disease frequently occurs in patients with hypopituitarism and growth hormone (GH) deficiency. Some patients may develop to hepatopulmonary syndrome (HPS). HPS has a poor prognosis and liver transplantation is regarded as the only approach to cure it.CASE SUMMARYA 29-year-old man presented with progressive dyspnea for 1 mo. At the age of 10 years, he was diagnosed with panhypopituitarism associated with pituitary stalk interruption syndrome. Levothyroxine and hydrocortisone were given since then. To achieve ideal height, he received GH treatment for 5 years. The patient had an oxygen saturation of 78% and a partial pressure of arterial oxygen of 37 mmHg with an alveolar-arterial oxygen gradient of 70.2 mmHg. Abdominal ultrasonography showed liver cirrhosis and an enlarged spleen. Perfusion lung scan demonstrated intrapulmonary arteriovenous right-to-left shunt. HPS (very severe) was our primary consideration. His hormonal evaluation revealed GH deficiency and hypogonadotropic hypogonadism when thyroid hormone, cortisol, and desmopressin were administrated. After adding with long-acting recombinant human GH and testosterone for 14 mo, his liver function and hypoxemia were improved and his progressive liver fibrosis was stabilized. He was off the waiting list of liver transplantation.CONCLUSIONClinicians should screen HPS patients' anterior pituitary function as early as possible and treat them primarily with GH cocktail accordingly.

2018-12-01·Oral Oncology2区 · 医学

Prophylactic versus reactive gastrostomy tube placement in advanced head and neck cancer treated with definitive chemoradiotherapy: A systematic review

2区 · 医学

Review

作者: Janna Z. Andrews ; Sewit Teckie ; Huma Chaudhry ; Shearwood McClelland ; Anuj Goenka

Although chemoradiotherapy (CRT) has improved disease outcomes in advanced head and neck cancer (aHNC), toxicity remains a major concern. Treatment interruptions and decreased quality of life (QOL) can occur due to malnutrition, secondary to mucositis, dysphagia and odynophagia. Gastrostomy tubes are used in many patients to improve nutrition during CRT. The optimal timing of PEG placement in patients with aHNC undergoing CRT remains controversial. Using the PubMed database, we performed a systematic review of published CRT series in aHNC to guide decision-making regarding optimal timing of percutaneous endoscopic gastrostomy (PEG) placement. We aimed to compare outcomes when patients are treated with prophylactic PEG (pPEG) versus reactive PEG (rPEG). Twenty-two studies examining the role of PEG placement in CRT for aHNC were reviewed. pPEG reduces the number of malnourished patients (defined as >10% of body weight), but average weight loss at various time points following treatment appears similar to patients with rPEG. pPEG is also associated with improved QOL at 6 months, and greater long term PEG dependence. Clinical and dosimetric parameters that correlate with malnutrition in patients without pPEG include advanced age, percent weight loss preceding treatment, and radiation dose to the pharyngeal constrictor muscles. Based on this evidence, our institutional strategy is to encourage pPEG in those patients deemed at greatest risk of becoming malnourished during the course of treatment, and to approach the remainder of patients with rPEG.

2016-03-01·The Journal of Clinical Endocrinology & Metabolism2区 · 医学

A Randomized Safety and Efficacy Study of Somavaratan (VRS-317), a Long-Acting rhGH, in Pediatric Growth Hormone Deficiency

2区 · 医学

Article

作者: Cleland, Jeffrey L. ; Bright, George M. ; Moore, Jerome A. ; Miller, Bradley S. ; Kletter, Gad B. ; Nguyen, Huong Jil ; Humphriss, Eric ; Moore, Wayne V. ; Rogers, Douglas ; Ng, David

AbstractContext:Somavaratan (VRS-317) is a long-acting form of recombinant human GH under development for children and adults with GH deficiency (GHD).Objectives:To determine the optimal somavaratan dose regimen to normalize IGF-1 in pediatric GHD and to evaluate safety and efficacy of somavaratan over 6 months.Design:Open-label, multicenter, single ascending dose study followed by 6-month randomized comparison of 3 dosing regimens.Setting:Twenty-five United States pediatric endocrinology centers.Patients:Naive-to-treatment, prepubertal children with GHD (n = 68).Intervention(s):Patients received single sc doses of somavaratan (0.8, 1.2, 1.8, 2.7, 4.0, or 6.0 mg/kg) during the 30-day dose-finding phase, then were randomized to somavaratan 1.15 mg/kg weekly, 2.5 mg/kg twice monthly, or 5.0 mg/kg monthly for 6 months.Main Outcome Measures:Safety, pharmacokinetics, pharmacodynamics, 6-month height velocity (HV).Results:Somavaratan pharmacokinetics was linearly proportional to dose; dose-dependent increases in the magnitude and duration of IGF-1 responses enabled weekly, twice-monthly or monthly dosing. A single dose of somavaratan sustained IGF-1 responses for up to 1 month. No somavaratan or IGF-1 accumulation occurred with repeat dosing. Mean annualized HVs for somavaratan administered monthly, twice monthly, or weekly (7.86 ± 2.5, 8.61 ± 2.7, and 7.58 ± 2.5 cm/y, respectively) were similar between groups. Adverse events were mostly mild and transient.Conclusions:Somavaratan demonstrated clinically meaningful improvements in HV and IGF-1 in prepubertal children with GHD, with no significant differences between monthly, twice-monthly, or weekly dosing.

项与 Somavaratan 相关的新闻（医药）

2023-03-02

·BioSpace

Press Release: Completed XTEND-Kids Phase 3 study strengthens potential of ALTUVIIIOTM to redefine expectations for treatment of children <12 years of age with hemophilia A

Completed XTEND-Kids Phase 3 study strengthenspotential of ALTUVIIIO™to redefineexpectations for treatment of children <12 years of age with hemophilia A Paris,March2, 2023. The XTEND-Kids phase 3 pivotal study evaluating the safety, efficacy and pharmacokinetics of ALTUVIIIO as once-weekly prophylaxis in previously treated patients <12 years of age with severe hemophilia A met its primary endpoint of safety, with no FVIII inhibitors detected in 74 children, with more than 50 children experiencing at least 50 exposure days, nearly a full year of treatment. The completion of XTEND-Kids represents the final milestone needed for regulatory submission in the EU. Karin Knobe, MD, PhD Therapeutic Area Head, Rare Diseases and Rare Blood Disorders, Sanofi “At Sanofi, we never settle. We work alongside patients, caregivers, and advocacy organizations to understand the needs of the hemophilia community and pursue first-in-class technologies to meet those needs. We strive for a future where every child with hemophilia can play without fear, travel free from a rigid treatment schedule, and pursue their dreams unencumbered by worry.” Hemophilia A is a rare, lifelong condition in which the ability of a person’s blood to clot properly is impaired, leading to excessive bleeds and spontaneous bleeds into joints that can result in joint damage and chronic pain, and potentially impact quality of life. The severity of hemophilia is determined by the level of clotting factor activity in a person’s blood, and there is a negative correlation between risk of bleeding and factor activity levels. ALUTVIIIO is a first-in-class, high-sustained FVIII therapy approved by the US Food and Drug Administration (FDA) for routine prophylaxis, on-demand treatment and control of bleeding episodes, and perioperative management of bleeding in adults and children in February 2023. Granted Breakthrough Therapy designation by the FDA in May 2022 – the first FVIII therapy to receive this designation—ALTUVIIIO also received Fast Track designation in February 2021 and Orphan Drug designation in 2017. The European Commission granted Orphan Drug designation in June 2019. AboutXTEND-Kids The XTEND-Kids study (NCT04759131) was an open-label, non-randomized interventional study of the safety, efficacy, and pharmacokinetics of once-weekly ALTUVIIIO in previously treated patients younger than 12 years of age with severe hemophilia A. Patients received once-weekly ALTUVIIIO prophylaxis (50 IU/kg) for 52 weeks which provided high-sustained FVIII levels throughout the weekly dosing interval with a median (IQR) annualized bleeding rate (ABR) of 0.00 (0.00, 1.02) and an estimated mean (95% CI) ABR of 0.89 (0.56 ; 1.42). The primary endpoint was the occurrence of inhibitor development (baseline to 52 weeks). No inhibitors were detected in this study. About ALTUVIIIO™ ALTUVIIIO [Antihemophilic Factor (Recombinant), Fc-VWF-XTEN Fusion Protein-ehtl] is a first-in-class high-sustained factor VIII therapy that is designed to extend protection from bleeds with once-weekly prophylactic dosing for adults and children with hemophilia A. ALTUVIIIO has a 3 to 4 fold longer half-life relative to standard and extended half-life factor VIII products, providing high-sustained factor activity levels throughout (≥40%) for most of the week and at 15% at the end of the dosing interval. ALTUVIIIO is the first factor VIII therapy that has been shown to break through the von Willebrand factor ceiling, which imposes a half-life limitation on earlier generation factor VIII therapies. ALTUVIIIO builds on the innovative Fc fusion technology by adding a region of von Willebrand factor and XTEN® polypeptides to extend its time in circulation. XTEN® is a registered trademark of Amunix Pharmaceuticals, Inc. About the XTEND Clinical Programs The XTEND clinical program is comprised of two Phase 3 trials in hemophilia A: XTEND-1 in people 12 years or older and XTEND-Kids in children younger than 12 years old. There is also an ongoing extension study (XTEND-ed). The Phase 3 XTEND-1 study (NCT04161495) was an open-label, non-randomized interventional study assessing the safety, efficacy, and pharmacokinetics of once-weekly ALTUVIIIO in people 12 years of age or older (n=159) with severe hemophilia A who were previously treated with factor VIII replacement therapy. The study consisted of two parallel treatment arms — the prophylaxis Arm A (n=133), in which patients who had received prior factor VIII prophylaxis were treated with once-weekly intravenous ALTUVIIIO prophylaxis (50 IU/kg) for 52 weeks, and the on-demand Arm B (n=26), in which patients who had received prior on-demand factor VIII therapy began with 26 weeks of on-demand ALTUVIIIO (50 IU/kg), then switched to once-weekly prophylaxis with ALTUVIIIO (50 IU/kg) for an additional 26 weeks. The primary efficacy endpoint of XTEND-1 was the mean annualized bleeding rate (ABR) in Arm A, and the key secondary endpoint was an intra-patient comparison of ABR during the ALTUVIIIO weekly prophylaxis treatment period versus the prior factor VIII prophylaxis ABR for a subset of participants in Arm A who had participated in a previous observational study (Study 242HA201/OBS16221). The XTEND-Kids study (NCT04759131) was an open-label, non-randomized interventional study of the safety, efficacy, and pharmacokinetics of once-weekly ALTUVIIIO in previously treated patients younger than 12 years of age with severe hemophilia A. Patients received once-weekly ALTUVIIIO prophylaxis (50 IU/kg) for 52 weeks. The primary endpoint was the occurrence of inhibitor development. About the Sanofi and Sobi collaboration Sobi and Sanofi collaborate on the development and commercialization of Alprolix® and Elocta®/Eloctate®. The companies also collaborate on the development and commercialization of efanesoctocog alfa, or ALTUVIIIO in the US. Sobi has final development and commercialization rights in the Sobi territory (essentially Europe, North Africa, Russia and most Middle Eastern markets). Sanofi has final development and commercialization rights in North America and all other regions in the world excluding the Sobi territory. About Sobi® Sobi is a specialised international biopharmaceutical company transforming the lives of people with rare and debilitating diseases. Providing reliable access to innovative medicines in the areas of haematology, immunology and specialty care, Sobi has approximately 1,600 employees across Europe, North America, the Middle East, Asia and Australia. In 2022, revenue amounted to SEK 18.8 billion. Sobi’s share (STO:SOBI) is listed on Nasdaq Stockholm. More about Sobi at sobi.com, LinkedIn and YouTube. About Sanofi We are an innovative global healthcare company, driven by one purpose: we chase the miracles of science to improve people’s lives. Our team, across some 100 countries, is dedicated to transforming the practice of medicine by working to turn the impossible into the possible. We provide potentially life-changing treatment options and life-saving vaccine protection to millions of people globally, while putting sustainability and social responsibility at the center of our ambitions. Sanofi is listed on EURONEXT: SAN and NASDAQ: SNY Media Relations Sandrine Guendoul | + 33 6 25 09 14 25 | sandrine.guendoul@sanofi.com Sally Bain | + 1 617 834 6026 | sally.bain@sanofi.com Evan Berland | +1 215 432 0234 | evan.berland@sanofi.com Kate Conway | + 1 508 364 4931 | kate.conway@sanofi.com Victor Rouault | + 33 6 70 93 71 40 | victor.rouault@sanofi.com Investor Relations Eva Schaefer-Jansen | + 33 7 86 80 56 39 | eva.schaefer-jansen@sanofi.com Arnaud Delépine | + 33 6 73 69 36 93 | arnaud.delepine@sanofi.com Corentine Driancourt | + 33 6 40 56 92 21 | corentine.driancourt@sanofi.com Felix Lauscher | + 1 908 612 7239 | felix.lauscher@sanofi.com Tarik Elgoutni| + 1 617 710 3587 | tarik.elgoutni@sanofi.com Nathalie Pham | + 33 7 85 93 30 17 | nathalie.pham@sanofi.com Sobi Contacts: Media Relations For Sobi Media contacts, click here. Investor Relations For details on how to contact the Sobi Investor Relations Team, click here. Sanofi Forward-Looking Statements This press release contains forward-looking statements as defined in the Private Securities Litigation Reform Act of 1995, as amended. Forward-looking statements are statements that are not historical facts. These statements include projections and estimates regarding the marketing and other potential of the product, or regarding potential future revenues from the product. Forward-looking statements are generally identified by the words “expects”, “anticipates”, “believes”, “intends”, “estimates”, “plans” and similar expressions. Although Sanofi’s management believes that the expectations reflected in such forward-looking statements are reasonable, investors are cautioned that forward-looking information and statements are subject to various risks and uncertainties, many of which are difficult to predict and generally beyond the control of Sanofi, that could cause actual results and developments to differ materially from those expressed in, or implied or projected by, the forward-looking information and statements. These risks and uncertainties include among other things, unexpected regulatory actions or delays, or government regulation generally, that could affect the availability or commercial potential of the product, the fact that product may not be commercially successful, the uncertainties inherent in research and development, including future clinical data and analysis of existing clinical data relating to the product, including post marketing, unexpected safety, quality or manufacturing issues, competition in general, risks associated with intellectual property and any related future litigation and the ultimate outcome of such litigation, and volatile economic and market conditions, and the impact that COVID-19 will have on us, our customers, suppliers, vendors, and other business partners, and the financial condition of any one of them, as well as on our employees and on the global economy as a whole. The risks and uncertainties also include the uncertainties discussed or identified in the public filings with the SEC and the AMF made by Sanofi, including those listed under “Risk Factors” and “Cautionary Statement Regarding Forward-Looking Statements” in Sanofi’s annual report on Form 20-F for the year ended December 31, 2022. Other than as required by applicable law, Sanofi does not undertake any obligation to update or revise any forward-looking information or statements. Attachment PDF

临床3期临床结果快速通道孤儿药突破性疗法

2022-11-11

·BioSpace

Sobi to present new data at the ASH 2022 Annual Meeting

STOCKHOLM, Nov. 11, 2022 /PRNewswire/ -- Sobi® will present new data at the 64th Annual Meeting of the American Society of Hematology (ASH) taking place from 10 to 13 December 2022. Sobi's commitment to developing innovative treatments for people living with rare diseases is highlighted in studies spanning several rare disorders, including haemophilia, paroxysmal nocturnal haemoglobinuria (PNH), cold agglutinin disease (CAD), immune thrombocytopenia (ITP) and primary haemophagocytic lymphohistiocytosis (pHLH). Results from the long-term extension study of Aspaveli®/Empaveli™ (pegcetacoplan) in adults with PNH will be presented, demonstrating robust and sustained improvements for approximately two years in key markers of disease across a broad population of PNH patients. In haemophilia A, new data on efanesoctocog alfa will be presented. Efanesoctocog alfa, an investigational new class of factor therapy for people with haemophilia A, has the potential to elevate standards of care by providing high sustained factor VIII activity into the near-normal range for the majority of the week with once-weekly prophylaxis. New data also will be presented from the REAL-HLH study, which is the first study describing the clinical characteristics, treatment patterns and treatment outcomes of a larger cohort of patients who received Gamifant® (emapalumab) in a real-world clinical setting. New information will also be presented supporting the role of Doptelet® (avatrombopag) in the treatment of ITP and describing the design of a study with Aspaveli/Empaveli for the treatment of CAD. "The breadth of data being presented at ASH this year showcases our ongoing commitment to providing innovative treatments for those affected by rare, ultra-rare and life-threatening conditions," said Anders Ullman, Head of Research & Development and Chief Medical Officer at Sobi. "We look forward to collaborating and connecting in person at this year's meeting." ADC Therapeutics to present new data on loncastuximab tesirine Sobi collaboration partner ADC Therapeutics will present eight abstracts at ASH. Multiple presentations will highlight the clinical utility of loncastuximab tesirine in diffuse large B-cell lymphoma. For more information please visit: ir.adctherapeutics.com/press-releases. Key Sobi data to be presented at ASH 2022 All abstracts can be accessed via the official ASH website. About efanesoctocog alfa (BIVV001) Efanesoctocog alfa is a novel and investigational recombinant factor VIII therapy with the potential to deliver near-normal factor activity levels for most of the week, extending bleed protection in a once-weekly dose for people with haemophilia A. Efanesoctocog alfa builds on the innovative Fc fusion technology by adding a region of von Willebrand factor and XTEN® polypeptides to potentially extend its time in circulation. It is the only therapy that has been shown to break through the von Willebrand factor ceiling, which is believed to impose a half-life limitation on current factor VIII therapies. Efanesoctocog alfa is currently under clinical investigation and its safety and efficacy have not been reviewed by any regulatory authority. Efanesoctocog alfa was granted orphan drug designation by the US Food & Drug Administration (FDA) in August 2017 and the European Commission in June 2019. The FDA has accepted for priority review the Biologics License Application for efanesoctocog alfa for the treatment of haemophilia A. The target action date for the FDA decision is 28 February 2023. Regulatory submission in the EU will follow availability of data from the ongoing XTEND-Kids paediatric study, expected in 2023. About the Sobi and Sanofi collaboration Sobi and Sanofi collaborate on the development and commercialisation of Alprolix® and Elocta®/Eloctate®. The companies also collaborate on the development and commercialisation of efanesoctocog alfa, an investigational factor VIII therapy with the potential to provide high sustained factor activity levels with once-weekly dosing for people with haemophilia A. Sobi has final development and commercialisation rights in the Sobi territory (essentially Europe, North Africa, Russia and most Middle Eastern markets). Sanofi has final development and commercialization rights in North America and all other regions in the world excluding the Sobi territory. About Aspaveli®/Empaveli™ Aspaveli/Empaveli (pegcetacoplan) is a targeted C3 therapy designed to regulate excessive activation of the complement cascade, part of the body's immune system, which can lead to the onset and progression of many serious diseases. It is approved as Aspaveli for the treatment of adults with paroxysmal nocturnal haemoglobinuria (PNH) who are anaemic after treatment with a C5 inhibitor for at least three months in the European Union and the United Kingdom and as Empaveli for treatment of adult patients with PNH in the United States and Saudi Arabia. Empaveli is also approved in Australia for treatment of adult patients with PNH who have an inadequate response to, or are intolerant of, a C5 inhibitor. About the Sobi and Apellis Collaboration Sobi and Apellis collaborate to develop and commercialize systemic Aspaveli/Empaveli. Sobi has exclusive ex-US commercialisation rights for systemic Aspaveli/Empaveli. Apellis has exclusive US commercialisation rights for systemic Empaveli. The companies have global co-development rights for systemic Aspaveli/Empaveli. About Doptelet® Doptelet (avatrombopag) is an orally administered thrombopoietin receptor agonist (TPO-RA) that mimics the biologic effects of TPO in stimulating the development and maturation of megakaryocytes, resulting in increased platelet count. It is approved by the European Medicines Agency and the US Food & Drug Administration for the treatment of severe thrombocytopenia in adult patients with chronic liver disease who are scheduled to undergo an invasive procedure and for the treatment of thrombocytopenia in adult patients with primary chronic immune thrombocytopenia (ITP) who have had an insufficient response to a previous treatment. Chronic ITP is a rare autoimmune bleeding disorder characterised by low number of platelets. The incidence of primary ITP in adults is 3.3/100 000 adults per year with a prevalence of 9.5 per 100 000 adults1. About Gamifant® Gamifant (emapalumab) is an anti-interferon gamma (IFNγ) monoclonal antibody that binds to and neutralises IFNγ. In the USA, Gamifant is indicated for the treatment of adult and paediatric (newborn and older) patients with primary haemophagocytic lymphohistiocytosis (HLH) with refractory, recurrent or progressive disease or intolerance with conventional HLH therapy. Primary HLH is a rare syndrome of hyperinflammation that usually occurs within the first year of life and can rapidly become fatal unless diagnosed and treated. The FDA approval is based on data from the phase 2/3 studies (NCT01818492 and NCT02069899). Gamifant is indicated for administration through intravenous infusion over one hour twice per week until haematopoietic stem cell transplantation (HSCT). About loncastuximab tesirine Loncastuximab tesirine (US brand name ZYNLONTA®) is a CD19-directed antibody-drug conjugate (ADC). Once bound to a CD19-expressing cell, ZYNLONTA is internalised by the cell, where enzymes release a pyrrolobenzodiazepine (PBD) payload. The potent payload binds to DNA minor groove with little distortion, remaining less visible to DNA repair mechanisms. This ultimately results in cell cycle arrest and tumour cell death. The US Food and Drug Administration (FDA) has approved ZYNLONTA (loncastuximab tesirine-lpyl) for the treatment of adult patients with relapsed or refractory (r/r) large B-cell lymphoma after two or more lines of systemic therapy, including DLBCL not otherwise specified, DLBCL arising from low-grade lymphoma and also high-grade B-cell lymphoma. The LOTIS-2 study included a broad spectrum of heavily pre-treated patients (median three prior lines of therapy) with difficult-to-treat disease, including patients who did not respond to first-line therapy, patients refractory to all prior lines of therapy, patients with double/triple hit genetics and patients who had stem cell transplant and CAR-T therapy prior to their treatment with ZYNLONTA. This indication is approved by the FDA under accelerated approval based on overall response rate and continued approval for this indication may be contingent upon verification and description of clinical benefit in a confirmatory study. ZYNLONTA is also being evaluated as a therapeutic option in combination studies in other B-cell malignancies and earlier lines of therapy. 1 Lambert et al. Blood 2017 Sobi® Sobi is a specialised international biopharmaceutical company transforming the lives of people with rare diseases. Providing sustainable access to innovative medicines in the areas of haematology, immunology and specialty care, Sobi has approximately 1,600 employees across Europe, North America, the Middle East and Asia. In 2021, revenue amounted to SEK 15.5 billion. Sobi's share (STO:SOBI) is listed on Nasdaq Stockholm. More about Sobi at sobi.com, LinkedIn and YouTube. Contacts Thomas Kudsk Larsen Head of Communication and Investor Relations thomas.kudsklarsen@sobi.com +44 7443 191 773 For details on how to contact the Sobi Investor Relations Team, please click here. For Sobi Media contacts, click here. The following files are available for download: View original content: SOURCE Swedish Orphan Biovitrum AB Company Codes: Bloomberg:SOBI@SS, ISIN:SE0000872095, RICS:SOBI.ST, Stockholm:SOBI

上市批准ASH会议孤儿药免疫疗法引进/卖出

2010-06-21

·BioSpace

Versartis, Inc. Presents Results of Three Studies at ENDO 2010

MOUNTAIN VIEW, CA--(Marketwire - June 20, 2010) - Versartis, Inc., an emerging biotechnology company developing novel therapeutics for patients with metabolic diseases and endocrine disorders, announced positive results of the company's VRS-317, a once monthly form of human growth hormone, today in San Diego at ENDO 2010: The 92nd Annual Meeting of the Endocrine Society. During the meeting, the company also introduced 9 new members of its VRS-317 Clinical Advisory Board (CAB), which now comprises 14 renowned growth deficiency endocrinologists. "The members of our original Clinical Advisory Board were instrumental in helping us to design key preclinical experiments, which have been completed, and also to design the Phase I study in growth hormone deficient adults for VRS-317, which will be initiated in the fourth quarter of 2010," said Jeffrey L. Cleland, Ph.D., Versartis Chief Executive Officer. "With our mutual commitment to improving the lives of these patients, Versartis and our original advisors were able to attract additional distinguished endocrinologists to our CAB." VRS-317 Growth Deficiency Clinical Advisory Board The newest members of the VRS-317 CAB: Barry Bercu, M.D., Professor of Pediatrics, University of South Florida College of Medicine Pinchas Cohen, M.D., Chief of Endocrinology, Mattel Children's Hospital, UCLA Paul Czernichow, M.D., Professor des Universites, Endocrinologie, Hospital Necker Enfants Malades Paul Desrosiers, M.D., Professor of Pediatrics, Arnold Palmer Hospital for Children Vera Popovic-Brkic, M.D., Ph.D., Institute of Endocrinology, University Clinical Center, Belgrade Sally Radovick, M.D., Division Director of Endocrinology, Johns Hopkins Medical Institutes Ed Reiter, M.D., Chair, Department of Pediatrics, Baystate Medical Center, Tufts University Steve Rosenthal, M.D., Associate Program Director, Pediatric Endocrinology, UCSF Christian Strasburger, M.D., Chief Endocrinology, Charité-Universitätsmedizin, Berlin Charter members of the VRS-317 CAB: Beverly Biller, M.D., Professor of Medicine, Harvard Medical School, Massachusetts General Hospital Gudmundur Johannsson, M.D., Professor of Medicine, Dept of Endocrinology, Gothenburg University Mark Kipnes, M.D., Executive Vice President, Medical Affairs, Cetero Research/DGD Research Ron Rosenfeld, M.D., Formerly of Lucille Packard Foundation and Oregon Health Sciences, Pediatric Endocrinology Paul Saenger, M.D., Professor of Pediatrics Emeritus, Albert Einstein College of Medicine Endocrine Society Meeting 2010 Sunday, June 20, 2010 "A Novel Human Growth Hormone XTEN Construct (VRS-317) for Monthly Administration: Long Half-life and Sustained In Vivo Potency" Poster Presentation, P2-353 1:30 - 3:30 pm VRS-317 consists of natural human growth hormone and a long tail of natural amino acids, referred to as XTEN, at the N and C termini of hGH. VRS-317 has been shown to sustain growth and pharmacodynamic (PD) responses in animals. Single doses of VRS-317 stimulated a sustained PD response in monkeys for one month and the terminal elimination half-life of VRS-317 in monkeys was 110 hr. Lipoatrophy studies indicated that VRS-317 is rapidly and near completely absorbed after subcutaneous injection and does not cause lipoatrophy in pigs or monkeys. A repeat dose (3 month) study in juvenile monkeys indicated that VRS-317 was safe and well tolerated up to 1.4 mg/kg every 28 days. Overall, these results suggest that a monthly dose of VRS-317 of approximately 0.5 mg/kg may provide a comparable growth response and safety pro daily hGH products in growth hormone deficient children. Commenting on the results presented today at ENDO, Paul Saenger, M.D., Professor of Pediatrics Emeritus, Albert Einstein College of Medicine, stated, "The preclinical efficacy and pharmacokinetic data suggested that the expected monthly dose of VRS-317 could be no more than 1.5 mg/kg in pediatric patients, providing a promising, long-acting rhGH treatment for children with growth hormone deficiency." Monday, June 21, 2010 "The Combination of a Long Acting GLP-1 Analog (E-XTEN; VRS-859) and Long Acting Glucagon (Gcg-XTEN; AMX-808) for Superior Weight Loss and Glycemic Control in Treatment of Type 2 Diabetes and Obesity" Oral Presentation OR24-4 11:15 am, Room 29ABC "A Monthly Dosed GLP-1 Analog for Treatment of Type 2 Diabetes Mellitus" Poster Presentation P3-517 1:30 - 3:30 pm XTEN is a novel hydrophilic sequence of natural amino acids and is expressed as a fusion protein with a therapeutically active peptide or protein. New compounds developed by Versartis using the XTEN technology are expected to provide improved therapeutic outcomes such as enhanced efficacy, fewer side effects, prolonged half-life (up to monthly dosing), as well as low cost production and enhanced stability. About Versartis Versartis, Inc. is a biotechnology company developing therapeutics for the treatment of metabolic diseases and endocrine disorders. The company's lead product candidates are VRS-859, a once monthly form of the GLP-1 analog, exenatide and VRS-317, a once monthly form of human growth hormone. Versartis is pursuing the development of new therapeutic proteins utilizing the Amunix Inc. novel half-life extension XTEN technology. Versartis, a joint venture company between Amunix, Inc. and Index Ventures, owns and develops the novel drug candidates in metabolic diseases and endocrinology that it has licensed from Amunix. Versartis has established preclinical proof-of-concept for three product candidates in its pipeline: exenatide and IL-1ra for diabetes, and hGH for growth hormone deficiency. Further information on Versartis can be found at . Contacts: Corporate Paul Westberg SVP Business Development Ph: 650 963-8585 Email: Email Contact Media Debra Bannister Corporate Communications Ph: 530 676-8001 Email: Email Contact

100 项与 Somavaratan 相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D11193	-	-	DB12421

研发状态

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适应症	最高研发状态	国家/地区	公司	日期
生长障碍	临床3期	日本	Versartis, Inc.	2015-08-08
生长障碍	临床3期	日本	Versartis, Inc.	2015-08-08
生长激素缺乏症	临床3期	日本	Versartis, Inc.	2015-08-08
生长激素缺乏症	临床3期	日本	Versartis, Inc.	2015-08-08

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT02719990 (CTgov)	临床2期	生长激素缺乏症	36	somavaratan	遞壓膚窪築願鏇壓襯艱(鏇淵齋齋繭網範鑰夢構) = 築鏇積遞網鹽選壓糧願構製膚蓋鏇觸膚餘壓鑰 (齋鏇鏇鹽齋艱構鏇夢鏇, 觸積餘繭築鬱齋範襯鹹 ~ 鹽艱積觸餘餘憲鹹鹽鹹) 更多	-	2023-04-13
NCT02339090 (VELOCITY \| Phase 3 study, CTgov)	临床3期	生长障碍 \| 生长激素缺乏症	138	Somavaratan (Somavaratan)	齋遞鬱構鏇憲鑰糧廠淵(遞膚觸齋構遞網觸襯醖) = 範獵壓簾膚願網鹽窪積獵衊衊鹹構艱壓製鏇艱 (襯齋壓築夢鏇憲選鑰餘, 餘網製選壓廠範衊構繭 ~ 遞構積獵範網鏇積廠淵) 更多	-	2022-12-30
				rhGH (rhGH)	齋遞鬱構鏇憲鑰糧廠淵(遞膚觸齋構遞網觸襯醖) = 壓廠觸鹽憲鬱鏇膚鏇簾獵衊衊鹹構艱壓製鏇艱 (襯齋壓築夢鏇憲選鑰餘, 醖範糧糧鬱鬱壓顧糧構 ~ 選選鹽餘製鬱壓築構鹽) 更多
NCT02339090 (VELOCITY, GlobeNewswire) 人工标引	临床3期	生长激素缺乏症	-	somavaratan	(鹹積窪選醖觸繭淵鬱遞) = 構憲淵鏇淵膚襯顧網構餘鏇獵觸願艱積糧鹽餘 (鏇鑰獵醖獵願積醖淵襯 ) 更多	不佳	2017-09-21
				Somatropin	(鹹積窪選醖觸繭淵鬱遞) = 遞觸衊夢鏇獵觸夢鬱選餘鏇獵觸願艱積糧鹽餘 (鏇鑰獵醖獵願積醖淵襯 ) 更多
NCT02068521 (ESPE2016)	临床2/3期	生长激素缺乏症	64	Somavaratan	(憲範糧選糧鹽醖齋壓鏇) = Related AE rates declined in Year 2 ( n =7). Related AEs were generally mild and transient, with no new types reported. 壓繭鹽築鑰壓鹽鹽鏇窪 (廠廠構網簾繭糧遞獵糧 )	-	2016-09-10
ESPE2015	N/A	生长激素缺乏症	63	VRS-317 2.5 mg/kg	(願艱獵選製觸構淵繭廠) = Only mild and transient drug-related AEs were observed (n=9 patients after 12 months; n =7 patients after 18 months). No new or unexpected AEs occurred. Injection site discomfort decreased with time on treatment, with only four subjects reporting discomfort after 18 months. 鑰餘鏇壓願繭製艱淵遞 (簾壓網夢襯範衊窪構繭 )	-	2015-10-01
				VRS-317 3.5 mg/kg