On July 26, 2024 Orano reported Half-year results reflect the deteriorated situation in Niger in an otherwise favorable dynamic 2024 financial outlook confirmed (Presentation, Orano, JUL 26, 2024, View Source;orano-2024-half-year-results.pdf?sfvrsn=a29c3931_6 [SID1234647176]).

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On July 26, 2024 Bristol-Myers Squibb reported second quarter 2024 results (Presentation, Bristol-Myers Squibb, JUL 26, 2024, View Source [SID1234646907]).

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On July 26, 2024 Xspray Pharma AB (publ) (Nasdaq Stockholm: XSPRAY) reported to have received a Complete Response Letter (CRL) from the U.S. Food and Drug Administration (FDA) regarding the New Drug Application (NDA) for Dasynoc, a novel treatment for chronic myeloid leukemia (CML) and acute lymphocytic leukemia (ALL) (Press release, Xspray, JUL 26, 2024, View Source [SID1234645158]). The updated NDA was sent to the FDA on January 31, 2024. In the CRL the FDA requests additional information pertaining to the labeling comprehension and the pre-approval inspection at the third party’s manufacturing site, which was conducted 10 to 19 of June, 2024. Importantly, the FDA does not request additional clinical studies, nor does it question any submitted stability or clinical data.

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To meet the FDA’s requirements, Xspray Pharma will work together with its third-party manufacturer to address the requests relating to the pre-approval inspection. In addition, the FDA has suggested a dialogue in the near term with Xspray to adapt the labeling strategy.

"We are encouraged that the FDA’s feedback confirms the stability and clinical data of Dasynoc. While the additional requests from the FDA were unexpected, we are confident in our ability to address these in a timely manner" said Per Andersson, CEO of Xspray Pharma. "This delay of the anticipated September launch is unfortunate as it impacts patients who do not have a viable treatment option when they are prescribed dasatinib and co-medicate with acid reducing agents. Our team remains dedicated to ensure that Dasynoc reaches patients as soon as possible, offering a valuable new treatment option for CML. Xspray welcomes the opportunity to work with the FDA to expedite the resubmission of the NDA. We will revert within the coming weeks with an updated time plan."

About Dasynoc
Dasynoc is an innovative treatment designed for chronic myeloid leukemia (CML) and acute lymphocytic leukemia (ALL). Dasynoc leverages the proven safety and efficacy of dasatinib along with distinct patient benefits driven by Xspray’s patented HyNap Technology.

Dasynoc offers bioequivalence at doses 30% less, which means patients are dosed lower. Additionally, bioavailability within patients may be more precise and predictable, ensuring patients get the benefit of their intended dose. Finally, it will be possible to prescribe Dasynoc freely with any acid reducing agent (ARA) including Proton Pump Inhibitors (PPIs), H2 antagonist or antacids.

Co-medication of both Tyrosine Kinase Inhibitors (TKIs) and ARAs is common as was recently highlighted at the American Society of Clinical Oncology (ASCO) (Free ASCO Whitepaper), demonstrating that 54% of CML patients, despite a warning, were prescribed a PPI. This is not without potential consequence, as a separate published study demonstrated 5-year overall survival was reduced by 15% in patients who took both a TKI with PPI.

On July 26, 2024 Bristol Myers Squibb reported results for the second quarter of 2024 (Press release, Bristol-Myers Squibb, JUL 26, 2024, View Source [SID1234645115]).

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"Our second quarter results reflect progress against our strategy to position BMS for long-term, sustainable growth," said Christopher Boerner, Ph.D., board chair and chief executive officer, Bristol Myers Squibb. "As we move into the second half of the year, we remain focused on prioritizing opportunities with the greatest growth potential and impact for patients, including the anticipated U.S. launch of KarXT. We’re also driving operational excellence throughout the company, becoming more agile and strengthening execution."

On July 26, 2024 Natera, Inc. (NASDAQ: NTRA), a global leader in cell-free DNA testing, reported a new study published in the Journal of Clinical Oncology highlighting the utility of its personalized and tumor-informed molecular residual disease (MRD) test, Signatera, for surveillance in Merkel cell carcinoma (MCC) (Press release, Natera, JUL 26, 2024, View Source [SID1234645114]).

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MCC is an aggressive skin cancer with high mortality and a recurrence rate of 40% within 5 years.1 MRD testing using a viral antibody is recommended by the National Comprehensive Cancer Network (NCCN)2, but this tumor marker is only present in 52% of patients and has several known limitations3-4. There is an unmet need for improved MRD testing technologies that are applicable to all patients, regardless of their viral status.

This prospective, multicenter, observational study included 319 patients with stage I-IV MCC. Signatera was used to assess ctDNA levels at the time of enrollment, and every 3 months during the surveillance period. Key findings include:

Signatera showed a test sensitivity of approximately 95% for detecting clinically evident disease at time of enrollment.
ctDNA positivity during surveillance was associated with up to 20 times higher risk of recurrence than persistently ctDNA-negative patients.
At 12 months of surveillance, the recurrence-free probability was 9% among patients with a positive ctDNA result at any time, compared with 91% for patients who remained ctDNA-negative.
"There is a strong need for highly accurate biomarkers in merkel cell carcinoma, an incredibly aggressive and rare form of skin cancer," said Lisa Zaba, M.D., Ph.D., associate professor of dermatology, director of the MCC multi-disciplinary clinic and member of the supportive oncodermatology group at the Stanford Cancer Center. "Our study shows that a tumor-informed MRD test can inform prognosis and guide surveillance in patients with MCC, regardless of tumor viral status."

"We are encouraged by the excellent performance of Signatera in this study, where high prognostic accuracy was demonstrated, and where we can see the significant clinical utility of MRD testing for detecting recurrence in MCC patients," said Angel Rodriguez, M.D., senior medical director at Natera and co-author of the study. "We are optimistic that Signatera will become a standard monitoring tool in this highly lethal cancer type, enabling clinicians to select patients with MRD who might benefit most from adjuvant therapy and better determine who may or may not need more frequent imaging with a high degree of confidence."

About Signatera

Signatera is a personalized, tumor-informed, molecular residual disease test for patients previously diagnosed with cancer. Custom-built for each individual, Signatera uses circulating tumor DNA to detect and quantify cancer left in the body, identify recurrence earlier than standard of care tools, and help optimize treatment decisions. The test is available for clinical and research use and is covered by Medicare for patients with colorectal cancer, breast cancer, ovarian cancer and muscle invasive bladder cancer, as well as for immunotherapy monitoring of any solid tumor. Signatera has been clinically validated across multiple cancer types and indications, with published evidence in more than 70 peer-reviewed papers.