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Spring Bank制药公司提供公司更新和报告2017年第四季度和全年 [复制链接]

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发表于 2018-2-21 12:56 |只看该作者 |倒序浏览 |打印
Spring Bank Pharmaceuticals Provides Corporate Update and Reports Fourth Quarter and Full-Year 2017 Financial and Operational Results   
                             
                                       
                           

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                                                                                February 20, 2018 16:30 ET                                     | Source:  Spring Bank Pharmaceuticals, Inc.                                             
                                      

2017 highlighted by continued progress with global inarigivir clinical program for the treatment of chronic HBV and advancement of next-generation STING agonist candidate, SB 11285, towards the clinic

  

Multiple potential development catalysts and data read-outs expected in 2018

  

HOPKINTON, Mass., Feb.  20, 2018  (GLOBE NEWSWIRE) -- Spring Bank Pharmaceuticals, Inc. (Nasdaq:SBPH), a clinical-stage biopharmaceutical company developing novel therapeutics for the treatment of viral infections, inflammatory diseases and certain cancers, today announced its fourth quarter and full-year 2017 financial results and provided an update on recent developments.

  

“In 2017, we significantly advanced the development of both our RIG-I and STING platforms, entered into strategic partnerships and strengthened our balance sheet,” commented Martin Driscoll, president and chief executive officer of Spring Bank Pharmaceuticals. “With the positive initial top-line results announced from the ongoing Phase 2 ACHIEVE trial for our lead development candidate, inarigivir, we now have the most advanced clinical candidate for chronic hepatitis B and are excited to continue to lead the way in the development of a potential simple, safe and selective functional cure for this disease. We are also encouraged by the preclinical results for our next-generation STING agonist candidate, SB 11285, which lead us to believe that SB 11285 has the potential to be clinically administered intratumorally and intravenously for a variety of tumors at various anatomic sites. Our execution during 2017 has set the stage for what we believe could be a productive 2018 with numerous potential development catalysts.”

  

Mr. Driscoll continued, “We have multiple objectives that we are working towards in 2018. Our primary objective is to further advance our inarigivir global clinical development program, particularly our clinical trial collaboration with Gilead involving the co-administration of inarigivir with Gilead’s oral antiviral agents, tenofovir disoproxil fumarate (marketed by Gilead as Viread®) and tenofovir alafenamide (marketed by Gilead as Vemlidy®). We will continue to execute our broad inarigivir clinical development program by (1) completing the Part A monotherapy dose-finding segment of the ACHIEVE trial, (2) conducting additional formulation development work for SB 9225, our potential fixed-dose co-formulation product combining inarigivir with tenofovir disoproxil fumarate, and (3) pursuing additional combinatorial or “triplet” therapies combining inarigivir, an oral antiviral agent and/or a potential third product or product candidate with a differing mechanism of action. Depending on the results of the ACHIEVE study and additional co-administration clinical trials that we are conducting, it is our objective to enter into a global Phase 3 program with inarigivir in 2019. Finally, we plan to initiate a Phase 1b/2 clinical trial with our novel, next-generation STING agonist, SB 11285, in hepatocellular carcinoma late in the second half of 2018.”

  

Potential 2018 Milestones

  
  • Complete Part A inarigivir monotherapy segment of the ACHIEVE trial by end of 2018
    • The company remains on track to release top-line results from the third monotherapy cohort (100mg) of the ACHIEVE trial in mid-2018 and top-line results from the fourth monotherapy cohort (200mg) in late 2018.
  • Report data from the co-administration clinical trials of inarigivir with the oral antiviral agents Viread and/or Vemlidy
    • The company entered into a clinical supply and collaboration agreement with Gilead under which Gilead is funding and conducting a Phase 2 trial examining the co-administration of inarigivir (50mg) and Vemlidy in patients infected with chronic HBV. Gilead has initiated this clinical trial in Korea. Spring Bank anticipates interim results from this trial in the second half of 2018.
    • Spring Bank currently intends to initiate Part B of the ACHIEVE trial in mid-2018 to evaluate the co-administration of inarigivir (100mg) with Viread.
  • Continue to advance the development of SB 9225 (inarigivir + tenofovir disoproxil fumarate)
    • Spring Bank has conducted development work that indicates inarigivir and tenofovir disoproxil fumarate are compatible in the same formulation. The company is conducting additional formulation development work for SB 9225 with the objective to potentially include this fixed-dose combination product candidate in Phase 3 clinical trial(s) in 2019.
  • Advance the company’s proprietary, novel next-generation STING agonist candidate, SB 11285, into the clinic
    • The company plans to submit a clinical trial application for SB 11285 in the second half of 2018, and, if approved, initiate a Phase 1b/2 clinical trial in hepatocellular carcinoma later in the second half of 2018.
  • Explore additional strategic partnerships
    • The company plans to pursue additional HBV clinical trial collaboration opportunities, including a combinatorial or “triplet” therapy combining inarigivir, an oral antiviral agent and/or a potential third product or product candidate with a differing mechanism of action, such as a capsid inhibitor or siRNA compound.
    • Due to the substantial prevalence of chronic HBV and regulatory changes in China, the company plans to further examine strategic opportunities in that region.
  • Expand the Spring Bank STING agonist platform

    • The company is exploring additional delivery methods for its STING agonist platform, including nanoparticle formulations as well as further development of antibody-drug conjugates to be used with the company’s STING agonist product candidates.
  

2017 and Other Recent Accomplishments

  
  • Continued progress in the execution of the global Phase 2 ACHIEVE clinical trial for inarigivir in hepatitis B.
    • The first three cohorts of Part A of the ACHIEVE trial have been enrolled on a timely basis and Spring Bank remains on track to report top-line results for the third monotherapy cohort (100mg) in mid-2018. In March 2018, our chief medical officer, Nezam Afdhal, M.D., D.Sc., will be giving an oral presentation highlighting the combined results from the first two cohorts of Part A of the ACHIEVE trial, including the sequential Viread 12-week dosing period, at the Asian Pacific Association for the Study of the Liver (APASL) 2018 Annual Meeting (March 14-18, 2018). In April 2018, Professor Stephen Locarnini, the Principal Investigator of the Virology Core for the ACHIEVE trial and the Head, Research & Molecular Development, Victorian Infectious Diseases Reference Laboratory, will present additional virology results from the combined first two cohorts of Part A of the ACHIEVE trial, including the sequential Viread 12-week dosing period in an oral presentation at The European Association for the Study of the Liver (EASL) 2018 Annual Meeting (April 11-15, 2018). Also at EASL, Prof. Dr. Man-Fung Yuen, Principal Investigator of the ACHIEVE trial and Chair Professor of Gastroenterology and Hepatology, Li Shu Fan Medical Foundation Professor in Medicine, the University of Hong Kong, will deliver a poster presentation describing clinical results from the combined first two cohorts of Part A of the ACHIEVE trial.
    • Spring Bank advanced the development of SB 9225, a fixed-dose co-formulation product candidate combining inarigivir with tenofovir disoproxil fumarate.
  • Advanced SB 11285 for immuno-oncology

    • The company presented data from multiple preclinical studies that demonstrated SB 11285 as a highly potent anti-tumor agent with a durable anti-tumor response when administered by multiple routes in several tumor models.
    • Spring Bank initiated the IND-enabling toxicology program for SB 11285.
    • Spring Bank consummated an Evaluation Assessment Agreement with a major Antibody Drug Conjugate (ADC) biopharmaceutical company to examine the potential to conjugate the Spring Bank STING agonist compounds with proprietary antibodies for oncology.
    • Four Patent Cooperation Treaty (PCT) applications were published in January 2018 by the U.S. Patent and Trademark Office covering the Spring Bank STING agonist platform program.
  • Strengthened the balance sheet and extended the runway for the Company late into 2019 with financing activities that raised a total of $47M in 2017

  • Strengthened the board of directors with the addition of Christiana Bardon, M.D., one of the leading investors in the life sciences industry who has extensive expertise in the biopharma sector
  

Year-End and Fourth Quarter 2017 Financial Results

  
  • Cash Position: Cash, cash equivalents and marketable securities were $50.6 million as of December 31, 2017, compared to cash, cash equivalents and marketable securities of $25.5 million as of December 31, 2016. Net cash used in operating activities for the twelve months ended December 31, 2017 was $17.7 million, compared to $15.8 million for the same period in 2016. Spring Bank expects that its cash, cash equivalents and marketable securities as of December 31, 2017 will enable it to fund its operating expenses and capital expenditure requirements into the fourth quarter of 2019, but will not be sufficient to fund the initiation of any Phase 3 trial for inarigivir, which could occur earlier than the fourth quarter of 2019.
  • Operating Expenses: Total operating expenses for the year ended December 31, 2017 were $21.3 million, which consisted of $13.1 million of research and development (R&D) expenses and $8.2 million of general and administrative (G&A) expenses. Total operating expenses for the year ended December 31, 2016 were $19.8 million, which consisted of $14.0 million of R&D expenses and $5.8 million of G&A expenses. For the quarter ended December 31, 2017, operating expenses were $6.3 million, compared to $4.4 million for the quarter ended December 31, 2016.
  • Net loss: The company’s net loss for the year ended December 31, 2017 was $(27.7) million, or $(2.48) per share, compared to $(17.4) million for the year ended December 31, 2016, or $(2.39) per share. Net loss for the quarter ended December 31, 2017 was $(1.5) million, or $(0.11) per share, compared to net loss for the quarter ended December 31, 2016 of $(2.4) million, or $(0.28) per share.
  

Conference Call
Spring Bank will host a conference call and webcast at 8:30 a.m. EST tomorrow, Wednesday, February 21, 2018, to discuss its 2017 results and objectives for 2018. The conference call may be accessed by dialing (800) 289-0517 for U.S. callers and (323) 794-2423 for international callers and providing the conference ID 5789868. Additionally, a live, listen-only webcast of the conference call can be accessed by visiting the Investors & Media section of the company’s website at www.springbankpharm.com or by clicking here.  

  

A replay of the conference call will be available until March 7, 2018 by dialing 844-512-2921 for U.S. callers and 412-317-6671 for international callers and providing the conference ID 5789868.

  

A

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发表于 2018-2-21 13:01 |只看该作者
Spring Bank制药公司提供公司更新和报告2017年第四季度和全年财务和运营结果
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2018年2月20日16:30 ET |资料来源:Spring Bank Pharmaceuticals,Inc.

2017年随着全球慢性乙型肝炎治疗慢性乙型肝炎临床计划的持续进展以及下一代STING激动剂候选人SB 11285向诊所的发展

预计2018年将有多种潜在的开发催化剂和数据读取

马萨诸塞州霍普金顿,2018年2月20日(GLOBE NEWSWIRE) - 开发用于治疗病毒感染,炎症性疾病和某些癌症的新型疗法的临床阶段生物制药公司Spring Bank Pharmaceuticals,Inc.(纳斯达克股票代码:SBPH)今天宣布了其2017年第四季度和全年财务业绩,并提供了最新发展的最新情况。

“2017年,我们极大地推进了RIG-I和STING平台的开发,建立了战略合作伙伴关系,并加强了我们的资产负债表,”Spring Bank Pharmaceuticals总裁兼首席执行官Martin Driscoll评论道。 “由于我们的首席发展候选人Inarigivir正在进行的第二阶段ACHIEVE试验中宣布的积极的初步的一线结果,我们现在拥有最先进的慢性乙型肝炎临床候选人,并且很高兴能够继续领导发展这种疾病的潜在简单,安全和选择性功能治愈。我们也对下一代STING激动剂候选者SB 11285的临床前结果感到鼓舞,这导致我们相信SB 11285有可能在各种解剖部位对各种肿瘤进行瘤内和静脉内临床给药。我们在2017年的执行已经为我们认为2018年的高产能奠定了基础,其中有许多潜在的发展催化剂。“

Driscoll先生继续说:“我们有多个目标,我们正在努力实现2018年。我们的主要目标是进一步推进我们的inarigivir全球临床开发计划,特别是我们与Gilead的临床试验合作,涉及共同施用inarigivir和Gilead的口服抗病毒药物替诺福韦二吡呋酯富马酸盐(由Gilead以Viread?销售)和替诺福韦艾拉酚胺(由Gilead以Vemlidy?销售)。 (1)完成ACHIEVE试验的A部分单一疗法剂量发现部分,(2)为我们的潜在固定剂量共同制剂产品SB9225进行额外的制剂开发工作,我们将继续执行我们广泛的inarigivir临床开发计划(3)结合使用具有不同作用机制的瑞那韦尔,口服抗病毒剂和/或潜在的第三种产品或候选产品的追加组合或“三联”疗法。根据我们正在进行的ACHIEVE研究和其他共同施用临床试验的结果,我们的目标是在2019年与Inarigivir进入全球3期计划。最后,我们计划启动1b / 2期临床试验与我们的新型下一代STING激动剂SB 11285在2018年下半年晚期在肝细胞癌中的作用。“

2018年潜力里程碑

    到2018年底完成ACHIEVE试验的A部分inarigivir单一疗法部分
        该公司仍然准备在2018年年中发布ACHIEVE试验的第三个单一疗法队列(100mg)和2018年底第四个单一疗法队列(200mg)的最终结果。
    报告使用口服抗病毒药物Viread和/或Vemlidy的inarigivir联合行政临床试验数据
        该公司与Gilead签署了一项临床供应和合作协议,Gilead正在资助并开展第二阶段试验,研究慢性HBV感染患者联合应用inarigivir(50mg)和Vemlidy。 Gilead已经在韩国启动了这个临床试验。春季银行预计2018年下半年该试验的中期业绩。
        Spring Bank目前打算在2018年年中启动ACHIEVE试验的B部分,以评估与Viread联合使用inarigivir(100mg)的情况。
    继续推进SB 9225(inarigivir + tenofovir disoproxil富马酸盐)
        春季银行开展的研究工作表明,inarigivir和替诺福韦地索普西富马酸盐在相同配方中是相容的。该公司正在为SB 9225进行额外的配方开发工作,目标是在2019年可能将该固定剂量组合产品候选物纳入3期临床试验。
    推进该公司专有的新一代STING激动剂候选者SB 11285进入诊所
        该公司计划在2018年下半年提交SB 11285的临床试验申请,如获批准,将启动1b / 2期临床
该公司计划在2018年下半年提交SB 11285的临床试验申请,并且如果获得批准,将在2018年下半年启动肝细胞癌的1b / 2期临床试验。
    探索更多战略合作伙伴
        该公司计划寻求更多的HBV临床试验合作机会,包括联合使用inarigivir,口服抗病毒药物和/或具有不同作用机制的潜在第三种产品或候选产品的组合或“三联”疗法,如衣壳抑制剂或siRNA化合物。
        由于中国慢性HBV感染率和监管变化的实质性流行,该公司计划进一步研究该地区的战略机遇。
    展开Spring Bank STING激动剂平台
        该公司正在探索其STING激动剂平台的其他递送方法,包括纳米颗粒制剂以及进一步开发与公司的STING激动剂产品候选物一起使用的抗体 - 药物偶联物。

2017年和其他最近的成就

    在乙型肝炎疫苗全球第二阶段ACHIEVE临床试验中继续取得进展
        ACHIEVE试验A部分的前三个队列已经及时报名,春季银行仍然有望在2018年年中报告第三次单一疗法队列(100mg)的最终结果。 2018年3月,我们的首席医疗官Nezam Afdhal医学博士将进行口头报告,重点介绍ACHIEVE试验A部分前两个组合的结果,包括连续的Viread 12周给药期间,在亚太肝脏研究协会(APASL)2018年会(2018年3月14日至18日)举行。 2018年4月,ACHIEVE试验的病毒学核心首席研究员,维多利亚州传染病参考实验室研究与分子开发负责人Stephen Locarnini教授将提供来自A部分的前两个组合的额外病毒学结果ACHIEVE试验,包括在欧洲肝脏研究协会(EASL)2018年会(2018年4月11 - 15日)上口头报告的连续Viread 12周给药期。同样在EASL,ACHIEVE研究首席研究员,胃肠病学和肝病学讲座教授袁满芳教授,香港大学李树范医学基础医学教授将发表海报介绍临床结果来自ACHIEVE试验A部分的前两个合并队列。
        Spring Bank推进了SB 9225的开发,这是一种固定剂量的联合制剂候选产品,将inarigivir与富马酸替诺福韦二吡呋酯联合使用。
    先进的SB 11285免疫肿瘤学
        该公司提供了多项临床前研究的数据,证明SB 11285是一种高效抗肿瘤药物,在多种肿瘤模型中通过多种途径给药时具有持久的抗肿瘤反应。
        Spring Bank发起了针对SB 11285的IND启用毒理学计划。
        Spring Bank完成了与主要抗体药物偶联物(ADC)生物制药公司的评估评估协议,以检查将春季银行STING激动剂化合物与专有抗体用于肿瘤学的缀合的可能性。
        美国专利商标局于2018年1月发布了四项专利合作条约(PCT)申请,内容涉及Spring Bank STING激动剂平台项目。

    加强了资产负债表并延长了公司对2019年的跑道的筹资活动,2017年共筹集了4700万美元

    增加了董事会成员,加入了生命科学行业领先投资者之一的Christiana Bardon,他是生物制药行业的专家

2017年第四季度财务业绩

    截至2016年12月31日,现金,现金等价物和有价证券为5,060万美元,而截至2016年12月31日的现金,现金等价物和有价证券为25.5百万美元。截至12月31日止经营活动所用的现金净额2017年12月31日为1770万美元,而2016年同期为1580万美元。Spring Bank预计,截至2017年12月31日,其现金,现金等价物和有价证券将使其能够将其运营支出和资本支出需求2019年第四季度,但不足以资助启动任何第三阶段审判,这可能比2019年第四季度早。
营业费用:截至二零一七年十二月三十一日止年度的总营运开支为2,130万美元,其中包括研发(研发)开支1,310万美元及一般及行政(G&A)开支820万美元。截至二零一六年十二月三十一日止年度的总营运开支为1,980万美元,其中包括研发费用1,400万美元及并购开支580万美元。截至2017年12月31日止季度,营业费用为630万美元,而截至2016年12月31日的季度为440万美元。

    净亏损:公司截至2017年12月31日止年度的净亏损为27.7百万美元,或每股2.48美元,而截至2016年12月31日的年度为17.4百万美元, ) 每股。截至二零一七年十二月三十一日止季度的净亏损为$(150万)或$(0.11)每股,而截至二零一六年十二月三十一日止季度的净亏损为$ 240万或$(0.28)分享。

电话会议
Spring Bank将于2018年2月21日星期三美国东部时间上午8:30召开电话会议和网络直播,讨论2017年的结果和2018年目标。电话会议可通过拨打(800)289-0517美国(323)794-2423,并提供会议ID 5789868.此外,可以通过访问公司网站www.springbankpharm上的“投资者与媒体”部分查看电话会议的现场直播网络直播。 com或点击这里。

电话会议重播将于2018年3月7日前开始,美国电话用户拨打844-512-2921,国际电话用户拨打412-317-6671,并提供会议ID 5789868。

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发表于 2018-2-21 13:36 |只看该作者
2018年3月,我们的首席医疗官Nezam Afdhal医学博士将进行口头报告,重点介绍ACHIEVE试验A部分前两个组合的结果,包括连续的Viread 12周给药期间,在亚太肝脏研究协会(APASL)2018年会(2018年3月14日至18日)举行。 2018年4月,ACHIEVE试验的病毒学核心首席研究员,维多利亚州传染病参考实验室研究与分子开发负责人Stephen Locarnini教授将提供来自A部分的前两个组合的额外病毒学结果ACHIEVE试验,包括在欧洲肝脏研究协会(EASL)2018年会(2018年4月11 - 15日)上口头报告的连续Viread 12周给药期。同样在EASL,ACHIEVE研究首席研究员,胃肠病学和肝病学讲座教授袁满芳教授,香港大学李树范医学基础医学教授将发表海报介绍临床结果来自ACHIEVE试验A部分的前两个合并队列。

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发表于 2018-2-21 13:37 |只看该作者
期待亚肝会数据

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发表于 2018-2-21 15:43 |只看该作者
SB9225是一种联合制剂,看来吉利得对SB9200也是有信心

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发表于 2018-2-21 15:44 |只看该作者
兄弟姐妹们新年快乐

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发表于 2018-2-21 16:09 |只看该作者
回复 windu 的帖子

如果不能转阴,那有个卵用。只好再和rnai药组合试试

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才高八斗

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发表于 2018-2-21 17:31 |只看该作者
回复 windu 的帖子

在HBeAg阴性患者和更高的剂量SB9200是非常有前途.

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发表于 2018-2-22 08:46 |只看该作者

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发表于 2018-2-22 08:46 |只看该作者
本帖最后由 newchinabok 于 2018-2-22 08:50 编辑

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