Atossa Therapeutics Shares Significant Progress in Tumor Treatment

Atossa Therapeutics Presents Promising Study Results

Atossa Therapeutics, Inc. (NASDAQ: ATOS), a leading clinical-stage biopharmaceutical entity focused on innovative breast cancer therapies, recently shared impactful findings from its Phase 2 Endocrine Optimization Pilot sub-study carried out within the I-SPY 2 TRIAL. This study specifically evaluated the effects of low-dose (Z)-endoxifen, administered at 10 mg daily, among 20 women diagnosed with stage II/III estrogen-receptor-positive (ER+), HER2-negative breast cancer.

Positive Outcomes from the Study

The results demonstrated significant achievements, indicating the feasibility of the treatment approach. Notably, 95 percent of participants managed to complete at least 75 percent of their planned dosing schedule, outperforming the initially established threshold.

Rapid Response Observed

Within three weeks of treatment, the median Ki-67, a crucial marker for tumor proliferation, showed a drastic reduction from 10.5 percent to 5 percent. An impressive 65 percent of the patients reached a Ki-67 level of 10 percent or below, with this suppression sustained through surgery.

Substantial Tumor Shrinkage

Moreover, tumor measurements reflected remarkable efficacy. The median functional tumor volume (FTV) showed a decrease of 77.7 percent from baseline to surgery, alongside a significant reduction of 36.8 percent in the longest tumor diameter observed prior to surgery. These imaging results speak volumes about the effectiveness of (Z)-endoxifen.

Safety Profile Highlights

On the safety front, the treatment was well tolerated among participants. Predominantly Grade 1 adverse events like vasomotor symptoms (hot flushes) and fatigue surfaced, with only three Grade 3 events reported that were unrelated to the medication. Notably, there were no severe Grade 4 or Grade 5 complications.

Pathologic Insights

Interestingly, no participants achieved a pathologic complete response (pCR). The residual cancer burden indicated moderate to extensive disease, aligning with earlier findings demonstrating that higher doses of (Z)-endoxifen are necessary for substantial pathologic clearance.

What This Means for Future Research

Dr. Steven Quay, M.D., Ph.D., President and CEO of Atossa Therapeutics, emphasized, "These results reveal that even at a low dosage, (Z)-endoxifen exhibits bioactivity, effectively reducing tumor proliferation and size, while maintaining an excellent safety record. Our focus will now shift to evaluating higher doses in ongoing trials to enhance pathological outcomes. This could ultimately change the landscape of breast cancer treatment."

Additionally, Atossa is conducting a supplementary cohort within the I-SPY 2 study, targeting a 40 mg daily dose of (Z)-endoxifen, in various combinations, with interim data expected in the near future.

About (Z)-Endoxifen

(Z)-endoxifen functions as a selective estrogen receptor modulator (SERM), known for not only inhibiting but potentially degrading estrogen receptors. This treatment option has demonstrated efficacy against tumors resistant to standard endocrine therapies. Importantly, it addresses significant limitations posed by conventional treatments, such as minimal endometrial activity and enhanced bone-protective effects compared to tamoxifen.

Atossa’s innovative oral formulation of (Z)-endoxifen includes enteric coating designed to optimize absorption and effectiveness. Clinical trials have indicated it is well tolerated among participants, which is promising for ongoing and future studies.

Continuing Development and Innovation

Atossa Therapeutics is dedicated to treating metastatic breast cancer, a domain where fresh therapeutic strategies are pivotal. Currently, the company is involved in multiple Phase 2 trials for (Z)-endoxifen, including studies for ductal carcinoma in situ (DCIS) and various presentations of ER+/HER2- breast cancer. Their research endeavors are backed by a robust intellectual property portfolio, underscoring a commitment to innovation in breast cancer treatment.

About Atossa Therapeutics

Atossa Therapeutics, Inc. (NASDAQ: ATOS) strives to revolutionize breast cancer care through cutting-edge research and patient-centric solutions. The company’s flagship candidate, (Z)-endoxifen, aims at various stages of breast cancer management, from prevention to advanced treatment. Atossa is resolutely pushing forward with its clinical programs to enhance patient outcomes while ensuring lasting value for shareholders.

Frequently Asked Questions

What recent results has Atossa Therapeutics shared?

Atossa announced promising results from a study evaluating low-dose (Z)-endoxifen in treating ER+ breast cancer.

How effective was the treatment in the study?

The treatment resulted in significant tumor shrinkage and favorable Ki-67 suppression among participants.

What safety concerns were raised during the study?

The treatment was well tolerated, with mostly mild adverse events reported.

What are the future plans for (Z)-endoxifen?

Atossa plans to evaluate higher doses and combinations of (Z)-endoxifen in new trials.

What distinguishes (Z)-endoxifen from other treatments?

(Z)-endoxifen is noted for its targeted action and reduced side effects compared to traditional therapies like tamoxifen.

About The Author

My name is Dylan Bailey, and I am 28 years old. I am an author and an expert on the stock market who specializes in publicly traded companies. Early fascination with the stock market inspired me to seek a finance degree and then delve deeply into the world of stocks. I have developed over the years my abilities to spot investment prospects, assess business performance, and analyze market trends.

My books and articles try to help regular investors understand the nuances of the stock market. Anyone can, in my opinion, make wise investment choices and succeed financially if they have the correct information and resources. In my writing, I combine in-depth research with practical insights and advice that can be put into action. This is done with the intention of assisting readers in navigating the constantly shifting landscape of publicly traded companies.

In addition to writing, I also host webinars and workshops, where I give presentations and share my knowledge with a wider audience. I also write for top financial journals and show up as a guest analyst on financial news shows. I like to travel, spend time with my family, and keep active by playing different sports when I'm not buried in market research.

My goal is to enable people to choose wisely and consciously in their investments, so taking charge of their financial futures. By my work, I hope to create a community of informed and self-assured investors prepared to take advantage of the chances presented by the stock market.

Contact Dylan Bailey privately here. Or send an email with ATTN: Dylan Bailey as the subject to contact@investorshangout.com.

About Investors Hangout

Investors Hangout is a leading online stock forum for financial discussion and learning, offering a wide range of free tools and resources. It draws in traders of all levels, who exchange market knowledge, investigate trading tactics, and keep an eye on industry developments in real time. Featuring financial articles, stock message boards, quotes, charts, company profiles, and live news updates. Through cooperative learning and a wealth of informational resources, it helps users from novices creating their first portfolios to experts honing their techniques. Join Investors Hangout today: https://investorshangout.com/

The content of this article is based on factual, publicly available information and does not represent legal, financial, or investment advice. Investors Hangout does not offer financial advice, and the author is not a licensed financial advisor. Consult a qualified advisor before making any financial or investment decisions based on this article. This article should not be considered advice to purchase, sell, or hold any securities or other investments. If any of the material provided here is inaccurate, please contact us for corrections.