SEATTLE, Dec. 10, 2024 (GLOBE NEWSWIRE) -- Atossa Therapeutics, Inc. (Nasdaq: ATOS) ("Atossa" or the "Company"), a clinical stage biopharmaceutical company developing innovative medicines in areas of significant unmet medical need in oncology with a focus on breast cancer, today announced that three posters involving pharmacokinetic and tolerability data from the Phase 2 EVANGELINE trial will be presented at the 2024 San Antonio Breast Cancer Symposium (SABCS 2024). EVANGELINE is a randomized Phase 2 non-inferiority study investigating (Z)-endoxifen as a neoadjuvant treatment for premenopausal women with estrogen receptor-positive (ER+)/HER2-negative breast cancer.
The first poster, "Neoadjuvant Z-Endoxifen for Premenopausal Estrogen Receptor (ER)+, Human Epidermal Receptor (HER2)- Breast Cancer (BC): Evaluation of the Pharmacokinetic (PK) Run-in for the EVANGELINE Study," discusses findings from the pharmacokinetic (PK) run-in phase of the trial. This phase evaluated (Z)-endoxifen monotherapy at 40 mg (data previously reported) and 80 mg (new data presented) doses, with and without goserelin (for ovarian function suppression or OFS). Findings include:
- Primary Endpoint Achieved: 50 percent of patients (3/6) in the group that received 80 mg of (Z)-endoxifen with goserelin met the target steady-state plasma concentrations (Css) of 500–1000 ng/mL. Approximately 38 percent of patients (3/8) in the 80 mg/day (Z)-endoxifen only group reached target Css levels. The average plasma Css level for all patients receiving 80mg/day of (Z)-endoxifen was 484 ng/mL. As previously reported, no patients in the 40 mg/day (Z)-endoxifen arm reached the target plasma Css level of 500 ng/mL.
- Tissue Penetration: Consistent with the recently updated trial protocol, tissue Css levels were evaluated in addition to plasma Css levels. The 80 mg/day dose, in both treatment arms, achieved tissue Css levels more than double that of plasma levels, surpassing the 500 ng/g target in 90 percent of patients—a level adequate to target PKCβ.
- Antitumor Activity: Substantial tumor suppression was observed across all dosing levels, with or without ovarian function suppression (OFS). The 4-week Ki-67 ≤10 percent response rate was generally above 85 percent across dose levels, with or without the presence of OFS.
- Safety and Tolerability: Overall, (Z)-endoxifen was well tolerated and target tissue Css levels were achieved without significant Grade 3–4 toxicities. Four gynecologic events were reported in the 80 mg groups, including one Grade 3 hemorrhagic cyst. These findings have informed protocol amendments to optimize dosing and tolerability.
The second poster, "Evaluation of Quality of Life (QOL) Measures in the EVANGELINE Study," focuses on patient-reported outcomes from (Z)-endoxifen treatment in patients enrolled onto the PK run-in. Findings include:
- Tolerability: The QOL data presented supports (Z)-endoxifen as generally well-tolerated. Most patient-reported side effects were low grade. Symptoms like hot flashes and reduced libido were reported as mildly to moderately bothersome. Amenorrhea and menstrual suppression were common but generally reported as manageable.
The third poster, "A Randomized Phase 2 Non-inferiority Trial of (Z)-endoxifen and Exemestane + Goserelin as Neoadjuvant Treatment for Premenopausal Women with ER+/HER2- Breast Cancer (EVANGELINE)," outlines the design and rationale for the randomized trial:
- Study Design: Based on adverse events reported in 80 mg/day groups, as well as the findings reported on (Z)-endoxifen tissue and plasma Css, overall tolerability, and antitumor activity, EVANGELINE is expected to proceed based on an amended protocol as a randomized trial that compares (Z)-endoxifen 40 mg/day plus OFS to exemestane plus OFS, using the 4-week Ki-67 reduction as the primary endpoint.
While tumor tissue (Z)-endoxifen levels were not tested at the 40 mg/day dose level, based on the ratio of plasma/tumor Css, (Z)-endoxifen tumor concentrations are expected to be >500 ng/g., meeting the required levels for PKCβ targeting.
- Next Steps: The process for trial initiation has begun and recruitment for this cohort is expected to begin in 2025, now that the PK run-in phase has been concluded.
"We are encouraged by the breadth of data being presented at SABCS, which collectively advances our understanding of (Z)-endoxifen's safety, efficacy, and impact on patient quality of life," said Steven Quay, M.D., Ph.D., Atossa's President and Chief Executive Officer. "Additionally, we believe we now have a clear plan for the randomized portion of the EVANGELINE trial, including a defined (Z)-endoxifen dose and study design. Our plan is to advance this arm of the study in 2025 as we seek to demonstrate the potential of (Z)-endoxifen to improve outcomes and provide a better tolerated option for premenopausal women with ER+/HER2- breast cancer."
A link to the poster presentations will be made available on Atossa Therapeutics' website at the time of the presentations on December 11. For additional information, please visit the SABCS website: .
About (Z)-Endoxifen
(Z)-endoxifen is one of the most potent Selective Estrogen Receptor Modulator (SERM) for estrogen receptor inhibition and may cause estrogen receptor degradation. It has also been shown to have efficacy in the setting of patients with tumor resistance to other hormonal treatments. In addition to its potent anti-estrogen effects, (Z)-endoxifen has been shown to target PKCβ1, a known oncogenic protein, at clinically attainable blood concentrations. Finally, (Z)-endoxifen appears to deliver similar or even greater bone agonistic effects while resulting in little or no endometrial proliferative effects compared with standard treatments, like tamoxifen.
Atossa is developing a proprietary oral formulation of (Z)-endoxifen that is encapsulated to bypass the stomach, as acidic conditions in the stomach convert a significant proportion of (Z)-endoxifen to the inactive (E)-endoxifen. Atossa's (Z)-endoxifen has been shown to be well tolerated in Phase 1 studies and in a small Phase 2 study of women with breast cancer. (Z)-endoxifen is currently being studied in five Phase 2 trials: one in healthy women with measurable breast density, one in women diagnosed with ductal carcinoma in situ, and three other studies including the EVANGELINE study and two I-SPY studies in women with ER+/HER2- breast cancer. Atossa's (Z)-endoxifen is protected by four issued U.S. patents and numerous pending patent applications.
About Atossa Therapeutics
Atossa Therapeutics, Inc. is a clinical-stage biopharmaceutical company developing innovative medicines in areas of significant unmet medical need in oncology with a focus on using (Z)-endoxifen to prevent and treat breast cancer. For more information, please visit .
FORWARD LOOKING STATEMENTS
This press release contains certain information that may constitute forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. We may identify these forward-looking statements by the use of words such as "expect," "potential," "continue," "may," "will," "should," "could," "would," "seek," "intend," "plan," "estimate," "anticipate," "believe," "design," "predict," "future," or other comparable words. All statements made in this press release that are not statements of historical fact, including statements regarding data related to the (Z)-endoxifen program, the safety, tolerability and efficacy of (Z)-endoxifen, the potential of (Z)-endoxifen as a breast cancer prevention and treatment agent, the expected design and enrollment of trials and timing of data and related publications, and the potential milestones and growth opportunities for the Company, are forward-looking statements. Forward-looking statements in this press release are subject to risks and uncertainties that may cause actual results, outcomes, or the timing of actual results or outcomes, to differ materially from those projected or anticipated, including risks and uncertainties associated with: macroeconomic conditions and increasing geopolitical instability; the expected timing of releasing data; any variation between interim or preliminary and final clinical results or analysis; actions and inactions by the FDA and foreign regulatory bodies; the outcome or timing of regulatory approvals needed by Atossa, including those needed to continue our planned (Z)-endoxifen trials; our ability to satisfy regulatory requirements; our ability to remain compliant with the continued listing requirements of the Nasdaq Stock Market; our ability to successfully develop and commercialize new therapeutics; the success, costs and timing of our development activities, including our ability to successfully initiate or complete our clinical trials, including our (Z)-endoxifen trials; our anticipated rate of patient enrollment; our ability to contract with third-parties and their ability to perform adequately; our estimates on the size and characteristics of our potential markets; our ability to successfully defend litigation and other similar complaints and to establish and maintain intellectual property rights covering our products; whether we can successfully complete our clinical trial of oral (Z)-endoxifen in women with mammographic breast density and our trials of (Z)-endoxifen in women with breast cancer, and whether the studies will meet their objectives; our expectations as to future financial performance, expense levels and capital sources, including our ability to raise capital; our ability to attract and retain key personnel; our anticipated working capital needs and expectations around the sufficiency of our cash reserves; and other risks and uncertainties detailed from time to time in Atossa's filings with the Securities and Exchange Commission, including without limitation its Annual Reports on Form 10-K and Quarterly Reports on 10-Q. Forward-looking statements are presented as of the date of this press release. Except as required by law, we do not intend to update any forward-looking statements, whether as a result of new information, future events or circumstances or otherwise.
Contact:
Michael Parks
VP, Investor and Public Relations
484-356-7105
michael.parks@atossainc.com
西雅图,2024年12月10日(GLOBE NEWSWIRE)——Atossa Therapeutics, Inc.(纳斯达克股票代码:ATOS)(“Atossa” 或 “公司”)是一家临床阶段的生物制药公司,在肿瘤学领域尚未得到满足的重大医疗需求领域开发以乳腺癌为重点的创新药物。该公司今天宣布,将发布三张海报,涉及EVANGELINE二期试验的药代动力学和耐受性数据在2024年圣安东尼奥乳腺癌研讨会(SABCS 2024)上。EVANGELINE 是一项随机的 2 期非劣势研究,研究 (Z)-内氧芬作为雌激素受体阳性 (ER+) /HER2 阴性乳腺癌的绝经前女性的新辅助疗法。
第一张海报 “用于绝经前雌激素受体(ER)+、人类表皮受体(HER2)——乳腺癌(BC)的新辅助Z-Endoxifen:EVANGELINE研究药代动力学(PK)运行评估” 讨论了该试验药代动力学(PK)试运行阶段的发现。该阶段评估了使用和不使用戈舍瑞林(用于卵巢功能抑制或OFS)剂量的(Z)-内氧芬单一疗法,剂量为40 mg(先前报告的数据)和80 mg(提供的新数据)。调查结果包括:
- 达到的主要终点:在接受80毫克(Z)-内昔芬和戈舍瑞林治疗的患者中,有50%(3/6)达到了500—1000 ng/mL的目标稳态血浆浓度(Css)。在仅限80毫克/天(Z)-内昔芬的组中,约有38%的患者(3/8)达到了目标Cs水平。所有接受80mg/天(Z)-内氧芬治疗的患者的平均血浆Cs水平为484 ng/mL。正如先前报道的那样,40毫克/天(Z)-内氧芬组中没有患者达到500 ng/mL的目标血浆Cs水平。
- 组织渗透:与最近更新的试验方案一致,除了血浆Css水平外,还评估了组织Css水平。两个治疗组每天80毫克的剂量使组织Cs水平达到血浆水平的两倍以上,超过了90%的患者500 ng/g的目标,这一水平足以靶向PKCβ。
- 抗肿瘤活性:无论是否有卵巢功能抑制(OFS),在所有剂量水平下均观察到肿瘤明显抑制。无论是否存在OFS,4周的Ki-67≤10%的反应率在所有剂量水平上通常都超过85%。
- 安全性和耐受性:总体而言,(Z)-内氧芬耐受性良好,靶组织Css水平达到了没有明显的3—4级毒性。在80 mg组中报告了四起妇科事件,包括一例3级出血性囊肿。这些发现为方案修订提供了依据,以优化剂量和耐受性。
第二张海报,“EVANGELINE研究中的生活质量评估(QOL)衡量标准”,重点介绍患者报告的参加Pk磨合的患者(Z)内氧芬治疗的结果。调查结果包括:
- 耐受性:所提供的QOL数据支持(Z)-内氧芬的耐受性总体良好。大多数患者报告的副作用是低度的。据报道,潮热和性欲减退等症状为轻度至中度困扰。闭经和月经抑制很常见,但通常报告是可以控制的。
第三张海报是 “(Z)-恩多昔芬和依西美坦+戈舍瑞林作为绝经前ER+/HER2-乳腺癌(EVANGELINE)女性新辅助治疗的随机2期非劣势试验” 概述了该随机试验的设计和理由:
- 研究设计:根据80mg/天组中报告的不良事件,以及报告的(Z)-内氧芬组织和血浆Css、总体耐受性和抗肿瘤活性的发现,EVANGELINE预计将根据修订后的方案进行随机试验,将4周的Ki-67降低量作为主要终点,将(Z)-内昔芬40毫克/天加OFS与依西美坦加OFS进行比较。
尽管根据血浆/肿瘤Cs的比例,肿瘤组织(Z)-内氧芬水平未在每天40毫克的剂量水平下进行测试,但根据血浆/肿瘤Cs的比例,(Z)-内昔芬肿瘤浓度预计为>500 ng/g。,达到靶向PKCβ的要求水平。
- 下一步:试验启动程序已经开始,由于Pk试用阶段已经结束,该队列的招募工作预计将于2025年开始。
Atossa总裁兼首席执行官史蒂芬·奎万博士说:“SABCS提供的广泛数据令我们感到鼓舞,这些数据共同增进了我们对(Z)-内氧芬的安全性、有效性以及对患者生活质量影响的理解。”“此外,我们认为我们现在已经为EVANGELINE试验的随机部分制定了明确的计划,包括确定的(Z)-内氧芬剂量和研究设计。我们的计划是在2025年推进这项研究,力求证明(Z)-内昔芬有可能改善预后,为患有ER+/HER2-乳腺癌的绝经前女性提供更好的耐受选择。”
海报演示的链接将在12月11日演示时在Atossa Therapeutics的网站上公布。欲了解更多信息,请访问SABCS网站:。
关于 (Z)-Endoxifen
(Z)-endoxifen 是抑制雌激素受体的最有效的选择性雌激素受体调节剂 (SERM) 之一,可能导致雌激素受体降解。它还被证明对其他激素治疗有耐药性的肿瘤患者具有疗效。除了具有强大的抗雌激素作用外,(Z)-内氧芬已被证明可以在临床上可达到的血液浓度下靶向PKCβ1(一种已知的致癌蛋白)。最后,与他莫昔芬等标准治疗相比,(Z)-内氧芬似乎具有相似甚至更大的骨激动作用,同时几乎没有或根本没有子宫内膜增生作用。
Atossa正在开发一种专有的(Z)-内氧芬口服制剂,该配方可封装以绕过胃部,因为胃中的酸性条件将很大一部分(Z)-内氧芬转化为非活性(E)-内氧芬。在1期研究和一项针对乳腺癌女性的小型2期研究中,Atossa(Z)-内昔芬的耐受性良好。(Z)-endoxifen目前正在五项2期试验中进行研究:一项针对乳房密度可测的健康女性,一项针对被诊断患有导管原位癌的女性,另外三项研究包括EVANGELINE研究和两项针对ER+/HER2-乳腺癌女性的I-SPY研究。Atossa的(Z)-内氧芬受四项已颁发的美国专利和大量待处理的专利申请的保护。
关于 Atossa Therapeutics
Atossa Therapeutics, Inc. 是一家处于临床阶段的生物制药公司,在肿瘤学中尚未满足的重大医疗需求领域开发创新药物,重点是使用(Z)-内氧芬预防和治疗乳腺癌。欲了解更多信息,请访问。
前瞻性陈述
本新闻稿包含某些可能构成1995年《私人证券诉讼改革法》所指的前瞻性陈述的信息。我们可以通过使用 “期望”、“潜在”、“继续”、“可能”、“将”、“应该”、“可以”、“将”、“寻求”、“打算”、“计划”、“估计”、“预测”、“相信”、“设计”、“预测”、“未来” 等词语来识别这些前瞻性陈述。本新闻稿中所有非历史事实陈述的陈述,包括与(Z)-内氧芬计划相关的数据、(Z)-内多昔芬的安全性、耐受性和有效性、(Z)-内多昔芬作为乳腺癌预防和治疗药物的潜力、试验的预期设计和注册以及数据和相关出版物的时间以及公司的潜在里程碑和增长机会的陈述,均为前瞻性陈述。本新闻稿中的前瞻性陈述受风险和不确定性的影响,可能导致实际结果、结果或实际结果或结果的时间与预测或预期存在重大差异,包括与宏观经济状况和地缘政治不稳定性加剧相关的风险和不确定性;预计发布数据的时间;中期、初步和最终临床结果或分析之间的任何差异;FDA和外国监管机构的行动和不作为;结果或时间Atossa所需的监管批准,包括继续我们计划中的(Z)-恩多昔芬试验所需的批准;我们满足监管要求的能力;我们遵守纳斯达克股票市场持续上市要求的能力;我们成功开发和商业化新疗法的能力;我们开发活动的成功、成本和时机,包括我们成功启动或完成临床试验,包括(Z)-恩多昔芬试验的能力;我们的预期的患者入院率;我们的能力与第三方签订的合同及其充分表现的能力;我们对潜在市场规模和特征的估计;我们成功地为诉讼和其他类似投诉进行辩护以及建立和维护涵盖我们产品的知识产权的能力;我们能否成功完成对乳腺密度成像女性进行口服(Z)-恩多昔芬的临床试验,以及我们在乳腺癌女性中对(Z)-内氧芬的试验,以及这些研究能否实现其目标;我们对未来财务的期望业绩、支出水平和资本来源,包括我们筹集资金的能力;我们吸引和留住关键人员的能力;我们对现金储备充足性的预期营运资金需求和预期;以及Atossa向美国证券交易委员会提交的文件中不时详述的其他风险和不确定性,包括但不限于其10-k表年度报告和10季度季度报告。前瞻性陈述截至本新闻稿发布之日发布。除非法律要求,否则我们无意更新任何前瞻性陈述,无论是由于新信息、未来事件或情况还是其他原因。
联系人:
迈克尔·帕克
投资者与公共关系副总裁
484-356-7105
michael.parks@atossainc.com
