Biora Therapeutics Achieves Positive Interim Results for Clinical Trial of BT-600, Advancing NaviCap Platform Development
Biora Therapeutics Achieves Positive Interim Results for Clinical Trial of BT-600, Advancing NaviCap Platform Development
Mean Plasma Tofacitinib Concentration
托法替尼血浆平均浓度
All pharmacokinetic endpoints were achieved, with a PK profile consistent with drug delivery and absorption in the colon
所有药代动力学终点均已达到,其PK分布与结肠中的药物递送和吸收一致
All NaviCap devices performed as intended and were well tolerated, with no safety signals observed
所有 NaviCap 设备均按预期运行且耐受性良好,未观察到安全信号
Multiple-ascending dose (MAD) portion of the trial is underway and progressing well
该试验的多递增剂量(MAD)部分正在进行中,进展顺利
SAN DIEGO, April 04, 2024 (GLOBE NEWSWIRE) -- Biora Therapeutics, Inc. (Nasdaq: BIOR), the biotech company that is reimagining therapeutic delivery, today shared additional positive interim results from the single-ascending dose (SAD) clinical trial of BT-600, which is a drug-device combination consisting of the orally administered NaviCap device that delivers a proprietary liquid formulation of tofacitinib to the colon. BT-600 is being developed for the potential treatment of patients with ulcerative colitis (UC). The SAD portion of the phase 1 randomized, double-blind, placebo-controlled clinical trial tested the tolerability and pharmacokinetics of BT-600 at 5 mg and 10 mg doses of tofacitinib, compared to placebo, in healthy adult participants.
圣地亚哥,2024年4月4日(GLOBE NEWSWIRE)——正在重新构想治疗的生物技术公司Biora Therapeutics, Inc.(纳斯达克股票代码:BIOR)今天分享了BT-600 的单升剂量(SAD)临床试验的更多积极中期结果。是一种药物器械组合,由口服的NaviCap设备组成,可向结肠输送托法替尼的专有液体配方。BT-600 正在开发用于潜在的溃疡性结肠炎 (UC) 患者的治疗。1 期随机、双盲、安慰剂对照临床试验的 SAD 部分测试了 BT-600 在健康成年参与者中与安慰剂相比,5 mg 和 10 mg 剂量的托法替尼的耐受性和药代动力学。
"We are extremely pleased with the interim trial results, some of which we shared during our recent quarterly call, that demonstrate the NaviCap platform's unique ability to achieve localized delivery to the colon, with a corresponding reduction in systemic drug exposure," said Ariella Kelman, MD, Chief Medical Officer of Biora Therapeutics. "Direct delivery of JAK inhibitors to the colon has potential for improved efficacy driven by increased colonic tissue exposure, while reducing toxicity risks related to systemic exposure. We believe this could lead to better outcomes for patients suffering from UC."
Biora Therapeutics首席医学官Ariella Kelman医学博士说:“我们对中期试验结果感到非常满意,我们在最近的季度电话会议上分享了其中一些结果,这些结果表明NaviCap平台具有实现结肠局部输送、相应减少全身药物暴露的独特能力。”“在结肠组织暴露增加的推动下,将JAK抑制剂直接输送到结肠有可能提高疗效,同时降低与全身暴露相关的毒性风险。我们相信,这可以为患有UC的患者带来更好的预后。”
According to the interim clinical data, all pharmacokinetic endpoints were met in all study participants. BT-600 was well tolerated with no serious adverse events. All devices performed as intended, with all participants receiving BT-600 showing systemic drug absorption. Tofacitinib was first detected in plasma at approximately six hours following administration, which is consistent with colonic delivery as opposed to absorption in the upper GI tract. The mean time to reach maximum concentration (Tmax) was 8–10 hours following administration of BT-600, versus 0.5-1.0 hours for conventional oral tofacitinib. Tofacitinib was present in fecal samples of all subjects, further confirming delivery of the drug in the colon.
根据临时临床数据,所有研究参与者都满足了所有药代动力学终点。BT-600 耐受性良好,没有严重的不良事件。所有设备均按预期运行,所有接受 BT-600 的参与者均显示全身药物吸收。托法替尼在给药后约六小时内首次在血浆中检出,这与结肠输送一致,而不是上消化道吸收。达到最大浓度的平均时间 (T最大值)给药 BT-600 后 8-10 小时,而传统口服托法替尼为 0.5-1.0 小时。托法替尼存在于所有受试者的粪便样本中,进一步证实了该药物在结肠中的输送。
Colonic delivery of BT-600 was associated with 3–4x lower systemic absorption of tofacitinib, with a maximum plasma concentration (Cmax) of 26 ng/mL for BT-600 at the 10 mg dose of tofacitinib, versus 88 ng/mL for conventionally administered oral tofacitinib at a 10 mg dose.
BT-600 的结肠输送可使托法替尼的全身吸收降低 3—4 倍,最大血浆浓度 (C)最大值) 在托法替尼剂量为 10 mg 时,BT-600 为 26 ng/mL,而常规口服托法替尼 10 mg 剂量为 88 ng/mL。
"Many IBD drugs could benefit from localized delivery—research shows that for JAK inhibitors, integrin inhibitors and TNF inhibitors, higher colon tissue concentrations correlate with better outcomes," said Adi Mohanty, Chief Executive Officer of Biora Therapeutics. "Our NaviCap platform represents a new therapeutic approach to UC and beyond. We continue to demonstrate that our localized delivery technology can enable higher colon tissue concentrations, without subjecting patients to high systemic drug levels, and results from the SAD portion of our clinical trial further confirm the platform's capability."
Biora Therapeutics首席执行官阿迪·莫汉蒂表示:“许多IBD药物可以从局部交付中受益——研究表明,对于JAK抑制剂、整合素抑制剂和肿瘤坏死因子抑制剂,较高的结肠组织浓度与更好的疗效相关。”“我们的 NaviCap 平台代表了一种治疗超声波及其他疾病的新治疗方法。我们继续证明,我们的本地化给药技术可以提高结肠组织浓度,而不会使患者承受较高的全身药物水平,而我们临床试验的SAD部分的结果进一步证实了该平台的能力。”
Highlights from the interim results can be found in the corporate presentation on Biora's website.
中期业绩的要点可以在Biora网站上的公司介绍中找到。
The multiple-ascending dose (MAD) portion of the trial, currently underway, will evaluate daily doses of BT-600 for 7 days at 5 mg and 10 mg tofacitinib or placebo. Final results are expected to be available in late Q2 2024.
该试验的多重递增剂量(MAD)部分目前正在进行中,将评估为期 7 天的 BT-600 每日剂量,分别为 5 mg 和 10 mg 托法替尼或安慰剂。最终结果预计将在2024年第二季度末公布。
Phase 1 Clinical Trial Design
The objectives of this phase 1 randomized, double-blind, placebo-controlled, single and multiple ascending dose (SAD/MAD) clinical trial are to evaluate the safety, pharmacokinetics and pharmacodynamics, including effects on colon tissue, of BT-600 when administered orally in healthy adult participants. The study, which is being conducted in the United States, consists of two parts. The first part is comprised of 24 participants receiving a single ascending dose of BT-600 with tofacitinib at 5 mg or 10 mg doses or placebo. The second part is comprised of 24 participants receiving multiple ascending-doses of BT-600 with tofacitinib at 5 mg or 10 mg doses or placebo daily for 7 days. The trial is listed at clinicaltrials.gov (NCT06275464).
1 期临床试验设计
这项 1 期随机、双盲、安慰剂对照、单次和多次递增剂量 (SAD/MAD) 临床试验的目标是评估 BT-600 在健康成年参与者中口服时的安全性、药代动力学和药效学,包括对结肠组织的影响。这项研究正在美国进行,由两部分组成。第一部分由 24 名参与者组成,他们接受单次递增剂量的 BT-600,托法替尼 5 mg 或 10 mg 剂量或安慰剂。第二部分由 24 名参与者组成,每天服用 5 mg 或 10 mg 剂量的多次递增剂量的 BT-600 或安慰剂,持续 7 天。该试验已在clinicaltrials.gov(NCT06275464)上列出。
About the NaviCap Targeted Oral Delivery Platform
Biora's NaviCap targeted oral therapeutics platform utilizes a novel approach that could improve patient outcomes by enabling delivery of therapeutics directly to the site of disease, increasing therapeutic levels in tissue while reducing systemic uptake. For the 1.8 million patients in the United States who suffer from inflammatory bowel disease (IBD), existing therapeutics offer less than ideal efficacy, likely because of the challenges with safely achieving sufficient drug levels in the affected tissues. Research has shown that targeted delivery of therapeutics has the potential to improve patient outcomes in IBD.
关于 NaviCap 定向口服给药平台
Biora的NaviCap靶向口服治疗平台采用了一种新方法,该方法可以将治疗直接送到疾病部位,提高组织中的治疗水平,同时减少全身吸收,从而改善患者的预后。对于美国180万患有炎症性肠病(IBD)的患者来说,现有疗法的疗效并不理想,这可能是因为在受影响的组织中安全地达到足够的药物水平方面存在挑战。研究表明,靶向治疗有可能改善IBD患者的预后。
The NaviCap platform uses an ingestible device designed for targeted delivery of therapeutics to improve treatment of IBD. Once swallowed, Biora's GItrac autolocation technology enables the device to autonomously identify targeted locations in the GI tract and release a therapeutic dose of up to 500μl. Studies in healthy volunteers have demonstrated accurate localization and delivery in a fasted state and demonstrated the device's ability to function in both fasted and fed states, making it potentially the first ingestible therapeutic delivery device that does not require fasting or other food restriction for use. A device function study in participants with active UC also demonstrated successful device performance in active UC patients.
NaviCap 平台使用专为靶向提供治疗而设计的可吸收设备,以改善 IBD 的治疗。一旦吞下,Biora的GitRac自动定位技术使该设备能够自主识别胃肠道中的目标位置,并释放高达500μl的治疗剂量。对健康志愿者的研究表明,在禁食状态下可以准确地定位和给药,并证明该设备能够在禁食和喂食状态下运行,这使其有可能成为第一款不需要禁食或其他食物限制即可使用的可摄入的治疗性递送设备。一项针对主动UC参与者的设备功能研究还表明,活跃UC患者的设备性能良好。
About Ulcerative Colitis
Ulcerative colitis (UC) is a chronic disease that causes inflammation and damage to the colon. Common symptoms include abdominal pain, increased bowel movements, stool urgency, and rectal bleeding. Despite the availability of advanced treatments for UC, including biologics, immunomodulators, and targeted synthetic small molecules, only about 40% of patients achieve clinical remission in induction trials. Surgical intervention is needed in approximately 20% of UC patients, with up to 10% of patients requiring surgical removal of the colon. About 1.5 million people are affected with UC in the United States alone, and ~40,000 new cases are diagnosed each year.
关于溃疡性结肠炎
溃疡性结肠炎(UC)是一种慢性疾病,会导致结肠发炎和损伤。常见症状包括腹痛、排便增多、便急和直肠出血。尽管有先进的UC治疗方法,包括生物制剂、免疫调节剂和靶向合成小分子,但只有大约40%的患者在诱导试验中实现临床缓解。大约20%的UC患者需要手术干预,其中多达10%的患者需要手术切除结肠。仅在美国,就有大约150万人受到UC的影响,每年诊断出约40,000例新发病例。
About Biora Therapeutics
Biora Therapeutics is reimagining therapeutic delivery. By creating innovative smart pills designed for targeted drug delivery to the GI tract, and systemic, needle-free delivery of biotherapeutics, the company is developing therapies to improve patients' lives.
关于 Biora Therapeu
Biora Therapeutics正在重新构想治疗方式。通过开发创新的智能药丸,专为胃肠道靶向药物输送以及生物治疗药物的系统性、无针输送而设计,该公司正在开发改善患者生活的疗法。
Biora is focused on development of two therapeutics platforms: the clinical-stage NaviCap targeted oral delivery platform, which is designed to improve outcomes for patients with inflammatory bowel disease through treatment at the site of disease in the gastrointestinal tract, and the preclinical-stage BioJet systemic oral delivery platform, which is designed to replace injection for better management of chronic diseases through needle-free, oral delivery of large molecules.
Biora专注于开发两个治疗平台:临床阶段的NaviCap靶向口服给药平台,旨在通过胃肠道疾病部位的治疗来改善炎症性肠病患者的预后;以及临床前阶段的BioJet全身口服给药平台,该平台旨在通过无针口服大分子来替代注射以更好地管理慢性病。
For more information, visit bioratherapeutics.com or follow the company on LinkedIn or Twitter.
欲了解更多信息,请访问bioratherapeutics.com或在LinkedIn或Twitter上关注该公司。
Safe Harbor Statement or Forward-Looking Statements
This press release contains "forward-looking statements" within the meaning of the "safe harbor" provisions of the Private Securities Litigation Reform Act of 1995, which statements are subject to substantial risks and uncertainties and are based on estimates and assumptions. All statements, other than statements of historical facts included in this press release, including statements concerning the progress and future expectations and goals of our research and development, preclinical, and clinical trial efforts including our BT-600 clinical trial execution and data timelines, are forward-looking statements. In some cases, you can identify forward-looking statements by terms such as "may," "might," "will," "objective," "intend," "should," "could," "can," "would," "expect," "forward," "believe," "design," "estimate," "predict," "potential," "plan," "target," or the negative of these terms, and similar expressions intended to identify forward-looking statements. These statements reflect our plans, estimates, and expectations, as of the date of this press release. These statements involve known and unknown risks, uncertainties and other factors that could cause our actual results to differ materially from the forward-looking statements expressed or implied in this press release. Such risks, uncertainties, and other factors include, among others, our ability to innovate in the field of therapeutics, our ability to make future filings and initiate and execute clinical trials on expected timelines or at all, our ability to obtain and maintain regulatory approval or clearance of our products on expected timelines or at all, our plans to research, develop, and commercialize new products, the unpredictable relationship between preclinical study results and clinical study results, our expectations regarding allowed patents or intended grants to result in issued or granted patents, our expectations regarding opportunities with current or future pharmaceutical collaborators or partners, our ability to raise sufficient capital to achieve our business objectives, and those risks described in "Risk Factors" and "Management's Discussion and Analysis of Financial Condition and Results of Operations" in our Annual Report on Form 10-K for the year ended December 31, 2023 filed with the SEC and other subsequent documents, including Quarterly Reports, that we file with the SEC.
安全港声明或前瞻性陈述
本新闻稿包含1995年《私人证券诉讼改革法》中 “安全港” 条款所指的 “前瞻性陈述”,这些陈述存在重大风险和不确定性,并基于估计和假设。除本新闻稿中包含的历史事实陈述外,所有陈述,包括与我们的研发、临床前和临床试验工作(包括我们的 BT-600 临床试验执行和数据时间表)的进展和未来预期和目标有关的声明,均为前瞻性陈述。在某些情况下,你可以通过诸如 “可能”、“可能”、“将”、“目标”、“打算”、“应该”、“可以”、“会”、“期望”、“向前”、“相信”、“设计”、“估计”、“潜力”、“计划”、“目标” 等术语来识别前瞻性陈述,或这些术语的否定词以及类似的表述旨在识别前瞻性陈述。这些声明反映了截至本新闻稿发布之日的计划、估计和预期。这些陈述涉及已知和未知的风险、不确定性和其他因素,这些因素可能导致我们的实际业绩与本新闻稿中表达或暗示的前瞻性陈述存在重大差异。此类风险、不确定性和其他因素包括:我们在治疗领域的创新能力、我们在未来提交申请以及按预期时间表启动和执行临床试验的能力、我们按预期时间表获得和维持监管部门批准或批准或批准的能力、我们研究、开发和商业化新产品的计划、临床前研究结果与临床研究结果之间不可预测的关系、我们对临床研究结果的预期允许的专利或意向授权导致专利的颁发或授予、我们对与当前或未来的制药合作者或合作伙伴合作机会的期望、我们筹集足够资金以实现业务目标的能力,以及我们向美国证券交易委员会提交的截至2023年12月31日年度的10-K表年度报告中 “风险因素” 和 “管理层对财务状况和经营业绩的讨论和分析” 中描述的风险,以及我们向美国证券交易委员会提交的其他后续文件,包括季度报告。
Biora Therapeutics expressly disclaims any obligation to update any forward-looking statements whether as a result of new information, future events or otherwise, except as required by law.
除非法律要求,否则Biora Therapeutics明确表示没有义务更新任何前瞻性陈述,无论是由于新信息、未来事件还是其他原因。
Investor Contact
Chuck Padala
Managing Director, LifeSci Advisors
IR@bioratherapeutics.com
(646) 627-8390
投资者联系人
查克·帕达拉
LifeSci Advisors董事总经理
IR@bioratherapeutics.com
(646) 627-8390
Media Contact
media@bioratherapeutics.com
媒体联系人
media@bioratherapeutics.com
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