TG Therapeutics Announces Schedule of Upcoming Presentations for BRIUMVI (Ublituximab) in Multiple Sclerosis at the 2024 Consortium of Multiple Sclerosis Centers Annual Meeting
TG Therapeutics Announces Schedule of Upcoming Presentations for BRIUMVI (Ublituximab) in Multiple Sclerosis at the 2024 Consortium of Multiple Sclerosis Centers Annual Meeting
NEW YORK, May 28, 2024 (GLOBE NEWSWIRE) -- TG Therapeutics, Inc. (NASDAQ: TGTX), today announced the schedule of upcoming presentations highlighting study designs for post-marketing studies being undertaken for BRIUMVI (ublituximab-xiiy) in patients with relapsing forms of multiple sclerosis (RMS), at the 2024 Consortium of Multiple Sclerosis Centers (CMSC) annual meeting, being held May 29 – June 1, 2024, in Nashville, Tennessee. Abstracts are now available online and can be accessed on the CMSC meeting website at www.mscare.org/2024 or by clicking on the following link: https://meridian.allenpress.com/ijmsc/article/26/s1/1/500896/Abstracts-from-the-38th-Annual-Meeting-of-the. Details for the upcoming BRIUMVI presentations are outlined below.
TG Therapeutics公司(纳斯达克股票代码:TGTX)宣布,将于2024年5月29日至6月1日在田纳西州纳什维尔举行的2024年多发性硬化中心联合会(CMSC)年会上,公布正在进行的关于BRIUMVI(ublituximab-xiiy)治疗复发型多发性硬化(MS)患者的后市场研究计划的研究设计。摘要现已在线上发布,可通过CMSC会议网站 (https://meridian.allenpress.com/ijmsc/article/26/s1/1/500896/Abstracts-from-the-38th-Annual-Meeting-of-the) 进行访问。具体的BRIUMVI演讲时间表详见下方。www.mscare.org/2024或者点击以下链接:https://meridian.allenpress.com/ijmsc/article/26/s1/1/500896/Abstracts-from-the-38th-Annual-Meeting-of-the下列是有关即将举行的 BRIUMVI 演讲的详情:
Poster Presentation Title: A Post-Marketing Study Evaluating the Presence and Concentration of BRIUMVI in Breast Milk (PROVIDE)
海报演讲名称:评估母乳中 BRIUMVI 的存在和浓度的后市场研究(PROVIDE)
- Presentation Date/Time: Thursday, May 30 at 5:15pm - 7:15 pm CST (6:15pm – 8:15pm ET)
- Session: Disease-Modifying Therapy - Exhibit Hall AB
- Abstract Number/Poster Number: Abstract #9567/DMT46
- Lead Author: Riley Bove, MD - UCSF Weill Institute of Neurosciences, Dept. of Neurology Univ. of California San Francisco, San Francisco, CA
- 演讲日/时间:2024年5月30日,晚上5:15 - 7:15 CST(晚上6:15 - 8:15 ET)
- 会议议题:治疗疾病模式 - AB展厅
- 摘要编号/海报编号:摘要 #9567 / DMT46
- 主要作者:Riley Bove, MD - UCSF威尔神经科学研究所,神经病学系,加利福尼亚大学旧金山分校,旧金山,加利福尼亚州
Poster Presentation Title: BRIUMVI Pregnancy Registry: A Prospective Study of Pregnancy and Infant Outcomes in Patients Treated with BRIUMVI
海报演讲名称:BRIUMVI 妊娠登记表:对接受 BRIUMVI 治疗患者的妊娠和婴儿结局的前瞻性研究
- Presentation Date/Time: Thursday, May 30 at 5:00pm - 7:00 pm CST (6:00pm – 8:00pm ET)
- Session: Disease-Modifying Therapy - Exhibit Hall AB
- Abstract Number/Poster Number: Abstract #9800/Late Breaker LB15
- Lead Author: Riley Bove, MD - UCSF Weill Institute of Neurosciences, Dept. of Neurology Univ. of California San Francisco, San Francisco, CA
- 演讲日/时间:2024年5月30日,晚上5:00 - 7:00 CST(晚上6:00 - 8:00 ET)
- 会议议题:治疗疾病模式 - AB展厅
- 摘要编号/海报编号:摘要 #9800 / 晚期破裂 LB15
- 主要作者:Riley Bove, MD - UCSF威尔神经科学研究所,神经病学系,加利福尼亚大学旧金山分校,旧金山,加利福尼亚州
Presentations will be available on the Publications page, located within the Pipeline section, of the Company's website at https://www.tgtherapeutics.com/publications/.
关于TG Therapeutics公司演示的内容,请访问公司网站的流水线部分页面。https://www.tgtherapeutics.com/publications/.
ABOUT THE ULTIMATE I & II PHASE 3 TRIALS
ULTIMATE I & II are two randomized, double-blind, double-dummy, parallel group, active comparator-controlled clinical trials of identical design, in patients with RMS treated for 96 weeks. Patients were randomized to receive either BRIUMVI, given as an IV infusion of 150 mg administered in four hours, 450 mg two weeks after the first infusion administered in one hour, and 450 mg every 24 weeks administered in one hour, with oral placebo administered daily; or teriflunomide, the active comparator, given orally as a 14 mg daily dose with IV placebo administered on the same schedule as BRIUMVI. Both studies enrolled patients who had experienced at least one relapse in the previous year, two relapses in the previous two years, or had the presence of a T1 gadolinium (Gd)-enhancing lesion in the previous year. Patients were also required to have an Expanded Disability Status Scale (EDSS) score from 0 to 5.5 at baseline. The ULTIMATE I & II trials enrolled a total of 1,094 patients with RMS across 10 countries. These trials were led by Lawrence Steinman, MD, Zimmermann Professor of Neurology & Neurological Sciences, and Pediatrics at Stanford University. Additional information on these clinical trials can be found at www.clinicaltrials.gov (NCT03277261; NCT03277248).
关于ULTIMATE I和II第3期试验
ULTIMATE I和II是两项随机、双盲、双哑、平行分组、活性对照临床试验,采用相同设计,治疗RMS患者96周。患者随机分配接收BRIUMVI还是活性对照剂teriflunomide,BRIUMVI以4个小时的静脉输注150毫克给药,第1次给药后2周以1小时给药450毫克,每24周以1小时给药450毫克,口服安慰剂每日给药;或者口服14毫克剂量的活性对照剂teriflunomide,按BRIUMVI相同的时间表给予静脉安慰剂。两项研究均招募了在前一年内至少经历一次复发、前两年内经历两次复发或前一年内具有T1钆 - 强化病变的患者。患者还必须在基线时具有0至5.5的扩展残疾状态量(EDSS)评分。ULTIMATE I和II试验在10个国家招募了1094例RMS患者。这些试验由斯坦福大学Zimmermann神经病学及神经科学和儿科教授Lawrence Steinman, MD主导。关于这些临床试验的其他信息可以在www.clinicaltrials.gov(NCT03277261;NCT03277248)上找到。
ABOUT BRIUMVI (ublituximab-xiiy) 150 mg/6 mL Injection for IV
BRIUMVI is a novel monoclonal antibody that targets a unique epitope on CD20-expressing B-cells. Targeting CD20 using monoclonal antibodies has proven to be an important therapeutic approach for the management of autoimmune disorders, such as RMS. BRIUMVI is uniquely designed to lack certain sugar molecules normally expressed on the antibody. Removal of these sugar molecules, a process called glycoengineering, allows for efficient B-cell depletion at low doses.
关于BRIUMVI(ublituximab-xiiy)150 mg/6 mL 静脉注射液请参见。
BRIUMVI是一种新型的单克隆抗体,靶向CD20表达的B细胞上的一种独特表位。使用单克隆抗体靶向CD20已被证明是一种治疗自身免疫性疾病,如RMS的重要方法。BRIUMVI的设计独具匠心,去除了抗体上通常表达的某些糖分子。去除这些糖分子,即一种称为糖基工程的过程,可在低剂量下实现高效的B细胞减少。
BRIUMVI is indicated for the treatment of adults with relapsing forms of multiple sclerosis (RMS), to include clinically isolated syndrome, relapsing-remitting disease, and active secondary progressive disease.
BRIUMVI适用于成年复发性多发性硬化(RMS)的治疗,包括临床隔离综合征、复发缓解性疾病和活动性继发性疾病。
A list of authorized specialty distributors can be found at www.briumvi.com.
授权专业经销商列表可在www.briumvi.com上找到www.briumvi.com.
IMPORTANT SAFETY INFORMATION
Contraindications: BRIUMVI is contraindicated in patients with:
重要安全信息
禁忌症:BRIUMVI对下列患者禁忌:
- Active Hepatitis B Virus infection
- A history of life-threatening infusion reaction to BRIUMVI
- B型肝炎病毒感染
- 曾经对BRIUMVI注射反应性严重
WARNINGS AND PRECAUTIONS
警告及注意事项
Infusion Reactions: BRIUMVI can cause infusion reactions, which can include pyrexia, chills, headache, influenza-like illness, tachycardia, nausea, throat irritation, erythema, and an anaphylactic reaction. In MS clinical trials, the incidence of infusion reactions in BRIUMVI-treated patients who received infusion reaction-limiting premedication prior to each infusion was 48%, with the highest incidence within 24 hours of the first infusion. 0.6% of BRIUMVI-treated patients experienced infusion reactions that were serious, some requiring hospitalization.
注射反应:BRIUMVI会引起注射反应,包括发热、寒战、头痛、类似流感的病症、心动过速、恶心、咽喉刺激、红斑和过敏反应。在进行多发性硬化临床试验中,如果BRIUMVI注射前使用限制注射反应的预处理可以减少注射反应的发生率,但是有48%的BRIUMVI患者仍然会发生注射反应,其中发病率最高的是首次注射后24个小时。0.6%的BRIUMVI患者经历了严重的注射反应,有些还需要住院治疗。
Observe treated patients for infusion reactions during the infusion and for at least one hour after the completion of the first two infusions unless infusion reaction and/or hypersensitivity has been observed in association with the current or any prior infusion. Inform patients that infusion reactions can occur up to 24 hours after the infusion. Administer the recommended pre-medication to reduce the frequency and severity of infusion reactions. If life-threatening, stop the infusion immediately, permanently discontinue BRIUMVI, and administer appropriate supportive treatment. Less severe infusion reactions may involve temporarily stopping the infusion, reducing the infusion rate, and/or administering symptomatic treatment.
在注射过程中和注射后至少一个小时观察治疗患者是否出现注射反应,除非注射反应和/或过敏反应已经在当前或任何先前的注射中观察到。告知患者注射反应可能会在注射后24小时内发生。注射前使用推荐的预处理减少注射反应的频率和严重程度。如果出现生命危险,立即停止注射,永久停止BRIUMVI,给予适当的支持性治疗。轻度注射反应可能涉及暂停注射、减慢注射速度和/或给予症状性治疗。
Infections: Serious, life-threatening or fatal, bacterial and viral infections have been reported in BRIUMVI-treated patients. In MS clinical trials, the overall rate of infections in BRIUMVI-treated patients was 56% compared to 54% in teriflunomide-treated patients. The rate of serious infections was 5% compared to 3% respectively. There were 3 infection-related deaths in BRIUMVI-treated patients. The most common infections in BRIUMVI-treated patients included upper respiratory tract infection (45%) and urinary tract infection (10%). Delay BRIUMVI administration in patients with an active infection until the infection is resolved.
感染:BRIUMVI治疗过的患者中报告了严重、危及生命或致死的细菌和病毒感染。在进行多发性硬化临床试验中,BRIUMVI治疗患者的感染总率为56%,而特里氟腺苷治疗患者的感染总率为54%。BRIUMVI治疗患者发生严重感染的比例为5%,而特里氟腺苷治疗患者为3%。BRIUMVI治疗患者中有三例感染相关死亡。BRIUMVI治疗患者中最常见的感染包括上呼吸道感染(45%)和尿路感染(10%)。建议BRIUMVI治疗患者,如果出现活动性感染,应延迟注射,直到感染解除。
Consider the potential for increased immunosuppressive effects when initiating BRIUMVI after immunosuppressive therapy or initiating an immunosuppressive therapy after BRIUMVI.
在免疫抑制治疗后或在使用BRIUMVI后开启免疫抑制治疗时,应考虑增加免疫抑制效应的可能性。
Hepatitis B Virus (HBV) Reactivation: HBV reactivation occurred in an MS patient treated with BRIUMVI in clinical trials. Fulminant hepatitis, hepatic failure, and death caused by HBV reactivation have occurred in patients treated with anti-CD20 antibodies. Perform HBV screening in all patients before initiation of treatment with BRIUMVI. Do not start treatment with BRIUMVI in patients with active HBV confirmed by positive results for HBsAg and anti-HB tests. For patients who are negative for surface premedantigen [HBsAg] and positive for HB core antibody [HBcAb+] or are carriers of HBV [HBsAg+], consult a liver disease expert before starting and during treatment.
在临床试验中治疗BRIUMVI的MS患者中发生了HBV复发。由于使用抗CD20抗体的患者已发生过暴发性肝炎、肝衰竭和死亡,因此在使用BRIUMVI治疗之前对所有患者进行HBV筛查。不要在已确认HBsAg和抗-Hb试验结果为阳性的患者中开始使用BRIUMVI治疗。对于表面前体抗原(HBsAg)阴性和Hb核抗体(HBcAb +)阳性或携带HBV(HBsAg +)的患者,在开始和治疗期间请咨询肝病专家。逐渐多灶性脑白质病(PML):
Progressive Multifocal Leukoencephalopathy (PML): Although no cases of PML have occurred in BRIUMVI-treated MS patients, JCV infection resulting in PML has been observed in patients treated with other anti-CD20 antibodies and other MS therapies.
虽然在BRIUMVI治疗的MS患者中没有出现PML病例,但使用其他抗CD20抗体和其他MS治疗方法治疗的患者已出现了因JCV感染而导致的PML。疫苗接种:
If PML is suspected, withhold BRIUMVI and perform an appropriate diagnostic evaluation. Typical symptoms associated with PML are diverse, progress over days to weeks, and include progressive weakness on one side of the body or clumsiness of limbs, disturbance of vision, and changes in thinking, memory, and orientation leading to confusion and personality changes.
如果怀疑PML,应暂停注射BRIUMVI并进行适当的诊断评估。与PML相关的典型症状因人而异,进展速度为数天至数周,并包括身体一侧的渐进性无力或肢体不协调、视觉障碍和思维、记忆和定向能力的改变,最终导致混乱和人格变化。在发现可疑症状时,可以通过进一步调查来早期诊断PML。在停止使用导致PML的其他MS药物后,与诊断时已有典型临床表现的患者相比,最初无症状的患者报道了更低的PML相关死亡率和发病率。
MRI findings may be apparent before clinical signs or symptoms; monitoring for signs consistent with PML may be useful. Further investigate suspicious findings to allow for an early diagnosis of PML, if present. Following discontinuation of another MS medication associated with PML, lower PML-related mortality and morbidity have been reported in patients who were initially asymptomatic at diagnosis compared to patients who had characteristic clinical signs and symptoms at diagnosis.
如果确诊为PML,应停止使用BRIUMVI治疗。
If PML is confirmed, treatment with BRIUMVI should be discontinued.
疫苗:应按照免疫接种指南给予所有免疫接种。对于活疫苗或减毒活疫苗,至少在BRIUMVI治疗开始前4周,并在可能的情况下至少在BRIUMVI治疗开始前2周接种。BRIUMVI可能会影响非活疫苗的有效性。虽然未研究在治疗期间或接受B细胞重建之后使用活病毒疫苗的安全性,但不推荐在治疗期间接种活病毒疫苗。
Vaccinations: Administer all immunizations according to immunization guidelines: for live or live-attenuated vaccines at least 4 weeks and, whenever possible at least 2 weeks prior to initiation of BRIUMVI for non-live vaccines. BRIUMVI may interfere with the effectiveness of non-live vaccines. The safety of immunization with live or live-attenuated vaccines during or following administration of BRIUMVI has not been studied. Vaccination with live virus vaccines is not recommended during treatment and until B-cell repletion.
疫苗接种:根据免疫规范,所有的疫苗接种都应在BRIUMVI的非活性疫苗接种前至少4周(对于活体或减毒活体疫苗)在可能的情况下至少提前2周进行。BRIUMVI可能会影响非活性疫苗的有效性。BRIUMVI的安全性在接种活体或减弱活体疫苗期间或之后尚未得到研究。在治疗期间以及b-细胞恢复之前不建议接种活病毒疫苗。
Vaccination of Infants Born to Mothers Treated with BRIUMVI During Pregnancy: In infants of mothers exposed to BRIUMVI during pregnancy, assess B-cell counts prior to administration of live or live-attenuated vaccines as measured by CD19+ B-cells. Depletion of B-cells in these infants may increase the risks from live or live-attenuated vaccines. Inactivated or non-live vaccines may be administered prior to B-cell recovery. Assessment of vaccine immune responses, including consultation with a qualified specialist, should be considered to determine whether a protective immune response was mounted.
接种BRIUMVI治疗期间母亲怀孕的婴儿:对于在怀孕期间接触了BRIUMVI的母亲的婴儿,在使用CD19衡量时,在注射活体或减弱活体疫苗之前评估b-细胞计数。+免疫球蛋白水平下降:与任何B细胞消耗性抗体治疗预期相同,观察到免疫球蛋白水平的降低。参与人数为514名的多发性硬化病人中,0.6%的BRIUMVI患者报道降低免疫球蛋白M(IgM)的情况,而对照组特里氟腺苷患者没有报道。在治疗期间,特别是在治疗期间和等待B细胞重建时,对于有机会或反复感染的患者,应监测量化血清免疫球蛋白水平。如果免疫球蛋白水平过低的患者发生严重的机会性感染或反复感染,或长期低免疫球蛋白血症需要静脉免疫球蛋白治疗,应考虑停止BRIUMVI治疗。
Fetal Risk: Based on data from animal studies, BRIUMVI may cause fetal harm when administered to a pregnant woman. Transient peripheral B-cell depletion and lymphocytopenia have been reported in infants born to mothers exposed to other anti-CD20 B-cell depleting antibodies during pregnancy. A pregnancy test is recommended in females of reproductive potential prior to each infusion. Advise females of reproductive potential to use effective contraception during BRIUMVI treatment and for 6 months after the last dose.
最常见的不良反应:RMS试验中最常见的不良反应(发生率至少为10%)是注射反应和上呼吸道感染。
Reduction in Immunoglobulins: As expected with any B-cell depleting therapy, decreased immunoglobulin levels were observed. Decrease in immunoglobulin M (IgM) was reported in 0.6% of BRIUMVI-treated patients compared to none of the patients treated with teriflunomide in RMS clinical trials. Monitor the levels of quantitative serum immunoglobulins during treatment, especially in patients with opportunistic or recurrent infections, and after discontinuation of therapy until B-cell repletion. Consider discontinuing BRIUMVI therapy if a patient with low immunoglobulins develops a serious opportunistic infection or recurrent infections, or if prolonged hypogammaglobulinemia requires treatment with intravenous immunoglobulins.
对于B细胞减少治疗中预计的,免疫球蛋白水平降低的情况需要警惕。参与人数为514名的多发性硬化病人中,0.6%的BRIUMVI患者报道降低免疫球蛋白M(IgM)的情况,而对照组特里氟腺苷患者没有报道。在治疗期间,特别是在治疗后和等待B细胞重建时,对于有机会或反复感染的患者,应监测量化血清免疫球蛋白水平,在B细胞重建之前应持续监测。如低免疫球蛋白血症需要,应考虑使用静脉免疫球蛋白制剂治疗。
Most Common Adverse Reactions: The most common adverse reactions in RMS trials (incidence of at least 10%) were infusion reactions and upper respiratory tract infections.
专业医生、药剂师或其他医疗保健专业人员如需了解BRIUMVI相关问题,请访问www.briumvi.com。
Physicians, pharmacists, or other healthcare professionals with questions about BRIUMVI should visit www.briumvi.com.
如需有关 BRIUMVI 的信息,请访问 www.briumvi.com。
ABOUT BRIUMVI PATIENT SUPPORT
BRIUMVI Patient Support is a flexible program designed by TG Therapeutics to support U.S. patients through their treatment journey in a way that works best for them. More information about the BRIUMVI Patient Support program can be accessed at www.briumvipatientsupport.com.
关于BRIUMVI患者支持。
BRIUMVI 患者支持是 TG Therapeutics 设计的灵活计划,旨在为美国的患者提供最好的治疗。有关 BRIUMVI 患者支持计划的更多信息,请访问www.briumvipatientsupport.com。
ABOUT MULTIPLE SCLEROSIS
Relapsing multiple sclerosis (RMS) is a chronic demyelinating disease of the central nervous system (CNS) and includes people with relapsing-remitting multiple sclerosis (RRMS) and people with secondary progressive multiple sclerosis (SPMS) who continue to experience relapses. RRMS is the most common form of multiple sclerosis (MS) and is characterized by episodes of new or worsening signs or symptoms (relapses) followed by periods of recovery. It is estimated that nearly 1 million people are living with MS in the United States and approximately 85% are initially diagnosed with RRMS.1,2 The majority of people who are diagnosed with RRMS will eventually transition to SPMS, in which they experience steadily worsening disability over time. Worldwide, more than 2.3 million people have a diagnosis of MS.1
多发性硬化
复发性多发性硬化(RMS)是中枢神经系统(CNS)的慢性脱髓鞘性疾病,包括患有复发缓解型多发性硬化(RRMS)和持续经历复发的继发性进行性多发性硬化(SPMS)的患者。RRMS是最常见的多发性硬化(MS)形式,其特征是新的或加重的体征或症状(复发)的发作,随后是恢复期。据估计,在美国有近100万人患有MS,大约有85%最初被诊断为RRMS。1,2诊断为RRMS的大多数人最终都会转变为SPMS,在SPMS中他们会随着时间的推移经历逐渐恶化的残疾。全世界有超过230万人被诊断患有多发性硬化症。1
ABOUT TG THERAPEUTICS
TG Therapeutics is a fully integrated, commercial stage, biopharmaceutical company focused on the acquisition, development and commercialization of novel treatments for B-cell diseases. In addition to a research pipeline including several investigational medicines, TG has received U.S. Food and Drug Administration (FDA) approval for BRIUMVI (ublituximab-xiiy), for the treatment of adult patients with relapsing forms of multiple sclerosis (RMS), to include clinically isolated syndrome, relapsing-remitting disease, and active secondary progressive disease, as well as approval by the European Commission (EC) and the Medicines and Healthcare Products Regulatory Agency (MHRA) for BRIUMVI to treat adult patients with RMS who have active disease defined by clinical or imaging features in Europe and the United Kingdom, respectively. For more information, visit www.tgtherapeutics.com, and follow us on X (formerly Twitter) @TGTherapeutics and on LinkedIn.
TG Therapeutics是一家完全集成、商业化阶段的生物制药公司,专注于收购、开发和商业化B细胞疾病的新型治疗方法。除了研究管线中包含几种调查药物外,TG还获得了美国食品和药品管理局的批准,使用BRIUMVI(ublituximab-xiiy)治疗复发性多发性硬化症的成人患者(RMS),包括临床分离综合征、复发缓解性疾病和活动性继发性疾病,以及欧洲委员会(EC)和药品和医疗保健产品监管局(MHRA)批准BRIUMVI用于治疗欧洲和英国分别具有临床或成像特征的RMS成人患者的活动性疾病。有关详细信息,请访问www.tgtherapeutics.com,并在X(前称Twitter)@TGTherapeutics上关注我们,并在
TG Therapeutics 是一家完全整合的商业阶段生物制药公司,致力于收购、开发和市场化用于b细胞疾病的新型治疗方法。除了研究流水线中包括多种试验性药物之外,TG 还获得了美国食品和药物管理局(FDA)批准 BRIUMVI(ublituximab-xiiy)治疗成年复发型多发性硬化(RMS),包括临床孤立综合征、复发缓解型疾病和活动性次进展型疾病,以及欧盟委员会(EC)和药品和保健品监管局(MHRA)的批准,用于治疗欧洲和英国分别有临床或影像特征定义的 RMS 成年患者。欲了解更多信息,请访问。www.tgtherapeutics.com,并关注我们的X(前称Twitter)账号@TGTherapeutics。与此同时您也可以在LinkedIn.
BRIUMVI is a registered trademark of TG Therapeutics, Inc.
BRIUMVI是tg therapeutics注册商标。
Cautionary Statement
This press release contains forward-looking statements that involve a number of risks and uncertainties. For those statements, we claim the protection of the safe harbor for forward-looking statements contained in the Private Securities Litigation Reform Act of 1995.
声明
本新闻发布包含涉及若干风险和不确定因素的前瞻性声明。对于这些声明,我们声称受到1995年《私人证券诉讼改革法》中前瞻性声明的免责保护。
Any forward-looking statements in this press release are based on management's current expectations and beliefs and are subject to a number of risks, uncertainties and important factors that may cause actual events or results to differ materially from those expressed or implied by any forward-looking statements contained in this press release. In addition to the risk factors identified from time to time in our reports filed with the U.S. Securities and Exchange Commission (SEC), factors that could cause our actual results to differ materially include the below.
本新闻发布中的任何前瞻性声明都是基于管理层的当前期望和信念,并且受到可能导致任何本新闻发布中包含的任何前瞻性声明的实际事件或结果与其中所表达或暗示的事件或结果不同的若干风险、不确定因素和重要因素的影响。除了我们向美国证券交易委员会(SEC)提交的报告中不时确定的风险因素外,可能导致我们的实际结果与此处包含的前瞻性声明不同的因素包括以下几点。
Such forward looking statements include but are not limited to statements regarding the results of the ULTIMATE I & II Phase 3 studies, the ENHANCE Phase 3b study, and BRIUMVI as a treatment for relapsing forms of multiple sclerosis (RMS). Additional factors that could cause our actual results to differ materially include the following: the risk that the data from the ULTIMATE I & II or ENHANCE trials that we announce or publish may change, or the product profile of BRIUMVI may be impacted, as more data or additional endpoints are analyzed; the risk that data may emerge from future clinical studies or from adverse event reporting that may affect the safety and tolerability profile and commercial potential of BRIUMVI; the risk that any individual patient's clinical experience in the post-marketing setting, or the aggregate patient experience in the post-marketing setting, may differ from that demonstrated in controlled clinical trials such as ULTIMATE I and II; the risk that BRIUMVI will not be commercially successful; our ability to expand our commercial infrastructure, and successfully market and sell BRIUMVI in RMS; the Company's reliance on third parties for manufacturing, distribution and supply, and a range of other support functions for our commercial and clinical products, including BRIUMVI, and the ability of the Company and its manufacturers and suppliers to produce and deliver BRIUMVI to meet the market demand for BRIUMVI; the failure to obtain and maintain requisite regulatory approvals, including the risk that the Company fails to satisfy post-approval regulatory requirements; the uncertainties inherent in research and development; and general political, economic and business conditions, including the risk that the ongoing COVID-19 pandemic could have on the safety profile of BRIUMVI and any of our other drug candidates as well as any government control measures associated with COVID-19 that could have an adverse impact on our research and development plans or commercialization efforts. Further discussion about these and other risks and uncertainties can be found in our Annual Report on Form 10-K for the fiscal year ended December 31, 2023 and in our other filings with the U.S. Securities and Exchange Commission.
这样的前瞻性声明包括但不限于关于ULTIMATE I & II Phase 3研究、ENHANCE Phase 30亿研究和BRIUMVI作为治疗复发形式的多发性硬化(RMS)的声明。可能会导致我们实际结果有所不同的额外因素包括:我们公布或公布的ULTIMATE I & II或ENHANCE试验的数据可能会发生变化,或者BRIUMVI的产品概况可能会受到更多数据或额外终点分析的影响;可能会从未来的临床研究或不良事件报告中出现数据,这些数据可能会影响BRIUMVI的安全性和耐受性配置文件和商业潜力;一个人的临床经验在后市场环境中,或在跟踪临床试验(例如,ULTIMATE I和II)中展示的经验总结中可能存在差异;BRIUMVI将无法获得商业成功;我们能够扩大我们的商业基础设施,并成功地在RMS中营销和销售BRIUMVI;对于我们的商业和临床产品,包括BRIUMVI,我们依赖第三方进行制造、分销和供应以及一系列其他支持功能,以满足BRIUMVI的市场需求,而公司及其制造商和供应商能够生产和交付BRIUMVI;未能获得和维持所需的监管批准,包括风险我们无法满足审批后监管要求的风险;研究和开发中固有的不确定性;以及一般的政治、经济和商业条件,包括持续的COVID-19大流行可能对BRIUMVI和我们其他药物候选人的安全性产生的风险和与COVID-19相关的任何政府控制措施可能对我们的研究和开发计划或商业化努力产生不利影响。有关这些和其他风险和不确定因素的进一步讨论,请参见我们的年度报告10-k报告,截至2023年12月31日的财年和我们向美国证券交易委员会的其他申报。
Any forward-looking statements set forth in this press release speak only as of the date of this press release. We do not undertake to update any of these forward-looking statements to reflect events or circumstances that occur after the date hereof. This press release and prior releases are available at www.tgtherapeutics.com. The information found on our website is not incorporated by reference into this press release and is included for reference purposes only.
此新闻稿中给出的任何前瞻性声明仅代表本新闻稿发布日期时的声明。我们不承诺更新任何这些前瞻性声明,以反映在此之后发生的事件或情况。此新闻稿和先前发布的新闻稿可在www.tgtherapeutics.com上找到。我们网站上的信息不被纳入此新闻稿的引用范围内,仅用于参考目的。
CONTACT:
联系人:
Investor Relations
Email: ir@tgtxinc.com
Telephone: 1.877.575.TGTX (8489), Option 4
投资者关系
电子邮件: ir@tgtxinc.com
电话:1.877.575.TGTX(8489),选项4
Media Relations:
Email: media@tgtxinc.com
Telephone: 1.877.575.TGTX (8489), Option 6
媒体关系:
克莉丝汀·沃勒 +1 (724) 514-1968
Christine.Waller@mylan.com
艾米·罗斯 +1 (212)
733-7410
Amy.rose@pfizer.com
梅利莎·特朗贝塔 +1 (724) 514-1813
Melissa.Trombetta@mylan.com
查克·特里亚诺 +1 (212)
733-3901
Charles.E.Triano@pfizer.com
电子邮件: media@tgtxinc.com
电话:1.877.575.TGTX(8489),选项6
1. MS Prevalence. National Multiple Sclerosis Society website. https://www.nationalmssociety.org/About-the-Society/MS-Prevalence. Accessed October 26, 2020. 2. Multiple Sclerosis International Federation, 2013 via Datamonitor p. 236.
1.选举作为董事的四位被提名人,其名称在附加的代理声明中列出,其任期将在2025年的股东年会上到期且在其继任者被选举和被确认前担任董事。MS患病率。国家多发性硬化症协会网站。https://www.nationalmssociety.org/About-the-Society/MS-Prevalence。2020年10月26日访问。特定形式2013年国际多发性硬化联盟通过。Datamonitor。第236页。