On June 27, 2022 Alaunos Therapeutics, Inc. ("Alaunos" or the "Company") (Nasdaq: TCRT), a clinical-stage oncology-focused cell therapy company, reported that the Company has extended its Cooperative Research and Development Agreement (CRADA) with the National Cancer Institute (NCI), an institute of the National Institutes of Health, using the Alaunos Sleeping Beauty technology through January 2025 (Press release, Alaunos Therapeutics, JUN 27, 2022, View Source [SID1234616291]).

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Under the terms of the CRADA, the NCI will work to generate proof of concept utilizing the Company’s proprietary non-viral Sleeping Beauty technology for personalized TCR-T cell therapy. In this setting, T-cell receptors (TCRs) that react to the patient’s tumor will be identified from the patient and used to generate a TCR-T cell therapy. This approach could potentially apply to a wide range of solid tumor cancer patients. Alaunos believes that the non-viral Sleeping Beauty technology could rapidly and cost effectively produce safe and potent TCR-T cell therapies without the complexity of gene editing or viral approaches. Research conducted under the CRADA will be led by Steven A. Rosenberg, M.D., Ph.D., Chief of the Surgery Branch at the NCI’s Center for Cancer Research.

"We are privileged to extend the productive collaboration with Dr. Rosenberg, a cell therapy pioneer. Dr. Rosenberg and the NCI are working to develop personalized cancer therapies using our novel TCR-T cell platform," commented Kevin S. Boyle, Sr., Chief Executive Officer of Alaunos. "Our collaboration reinforces our commitment to improving the lives of cancer patients with solid tumors. We look forward to continuing our collaborating with Dr. Rosenberg and his team to generate proof of concept in this personalized TCR-T approach."

Drew Deniger, Ph.D., Vice President, Research & Development at Alaunos added, "Having worked alongside Dr. Rosenberg for many years, I am confident that his team at the NCI will be successful in developing personalized TCR-T therapies using our non-viral Sleeping Beauty technology. As the world’s experts in Sleeping Beauty, we believe that our non-viral means of adding the TCR to T cells is well suited for a personalized approach, with potential to further increase the addressable population for TCR-T therapies."

On June 27, 2022 INOVIO (NASDAQ: INO), a biotechnology company focused on developing and commercializing DNA medicines to help protect people from infectious diseases and treat people with cancer and HPV-associated diseases, reported the appointment of Dr. Michael Sumner, MB BS, MBA, as Chief Medical Officer (CMO) (Press release, Inovio, JUN 27, 2022, View Source [SID1234616290]). Dr. Sumner will oversee INOVIO’s clinical-stage pipeline of DNA medicines, global clinical development, clinical operations and biostatistics efforts, as well as regulatory affairs, pharmacovigilance and medical affairs. He will serve on the company’s executive leadership team and will report to INOVIO’s President and Chief Executive Officer, Dr. Jacqueline Shea.

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INOVIO’s President and Chief Executive Officer, Jacqueline Shea, Ph.D., said, "INOVIO is pleased to welcome Dr. Sumner to INOVIO. An industry veteran and a member of the Royal College of Physicians, Dr. Sumner’s clinical development and medical affairs expertise and track record of helping guide companies through regulatory approval and commercialization make him an important addition to the INOVIO team."

Dr. Sumner joins INOVIO after serving as CMO of Orexo AB since 2013. He previously held numerous European- and US-based leadership roles at Novartis Pharmaceuticals, Aventis Behring, Novo Nordisk and Shire Pharmaceuticals. Dr. Sumner brings over 25 years of extensive pharmaceutical, medical and clinical experience driving numerous late-stage product approvals and supporting successful commercial products on a global basis across multiple therapeutic areas.

Dr. Sumner received his medical degree from the University of London, is a member of the Royal College of Physicians, and holds a Master of Business Administration from Henley Management College, UK.

"I am pleased to join INOVIO as CMO and look forward to working with the team to unlock the power of the DNA Medicines platform to address unmet medical need," said Dr. Sumner.

On June 27, 2022 Hoffmann-La Roche reported to invite you to an analyst event on Tuesday, 26 July 2022, to discuss Roche’s Diagnostics Division, in conjunction with the American Association for Clinical Chemistry (AACC) Annual Meeting and Clinical Lab Exposition in Chicago, Illinois (July 24-28, 2022) (Press release, Hoffmann-La Roche, JUN 27, 2022, View Source [SID1234616289]).

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AACC brings together the global leaders in clinical chemistry, molecular diagnostics and lab management, and is the largest dedicated exhibition of equipment, instruments and services for clinical laboratories in the world.

The Analyst Event will start with a presentation on the Diagnostics Division and on AACC highlights followed by a Q&A session.

On June 27, 2022 Bonnie J Addario Lung Cancer Foundation reported that Targeted therapy research was front and center at the 2022 American Society of Clinical Oncology (ASCO) (Free ASCO Whitepaper) Annual Meeting (Press release, Bonnie J Addario Lung Cancer Foundation, JUN 27, 2022, View Source [SID1234616288]). Data was presented from several studies detailing new targeted therapies and better understanding of how to treat non-small cell lung cancer (NSCLC) with various driver mutations . Following are some highlights from targeted therapy information presented at the meeting.

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KRAS
The first targeted therapy for NSCLC with a KRAS G12C mutation, Lumakras (sotorasib), was approved last year as an option for NSCLC that had already been treated with another therapy, such as chemotherapy. Although this was a breakthrough in making targeted therapy available for one of the most common NSCLC mutations, only a portion of KRAS G12C-positive NSCLC responded well to Lumakras (sotorasib) and identifying new treatment options will be beneficial to many patients.

Data from the KRYSTAL-1 trial showed that the newer KRAS G12C targeted therapy, adagrasib, led to promising rates and lengths of response when given as a treatment after other previous therapies. A larger clinical trial, KRYSTAL-12, is in progress to compare adagrasib to standard therapies. Positive results may lead to adabrasib being an additional targeted therapy option for KRAS G12C-positive NSCLC.
Data presented from the KRYSTAL-1 trial showed that adagrasib had promising results when treating brain metastasis. Importantly, data on the effectiveness of adagrasib for active and untreated brain metastasis was shared. This research is important since patients with this type of brain metastasis are often prevented from participating in clinical trials.
EGFR
Tagrisso (osimertinib)’s effectiveness has made it the standard of care first treatment for EGFR-positive NSCLC. But for many patients, resistance (where the cancer starts to grow or spread again while still being treated) is an issue. More treatment options are needed for EGFR-positive patients to help when Tagrisso (osimertinib) resistance happens.

Updated data was shared from the CHRYSALIS-2 trial, confirming that a combination of amivantamab and azertinib produced promising results in treating EGFR-positive NSCLC, even after progression on multiple other lines of therapy including Tagrisso (osimertinib). This combination is being compared to other therapies in larger clinical trials and may have promise as a future option.
Data from an early phase trial showed that telisotuzumab vedotin (Teliso-V), showed initial positive results in treating NSCLC that had c-MET overexpression after developing Tagrisso (osimertinib) resistance. Repeat biomarker testing (after resistance to targeted therapies occurs) may help identify new changes such as c-MET overexpression for which clinical trials may be an option.
EGFR-positive NSCLC with an exon 20 mutation does not respond as well to standard targeted therapies approved to treat NSCLC with the most common EGFR mutations. Specific targeted therapies for EGFR exon 20-positive NSCLC, Exkivity (mobocertinib) and Rybrevant (amivantamab-vmjw), were approved in 2021, but these drugs do not produce responses to the same degree as the other EGFR targeted therapies. Many people living with EGFR exon 20-positive NSCLC would benefit from additional treatment options.

A clinical trial of CLN-081 showed promising responses that occurred when it was used to treat NSCLC with an EGFR exon 20 mutation that had already been treated previously with multiple other therapies, including other EGFR targeted therapies. It may represent a future additional option for patients with NSCLC with an EGFR exon 20 mutation.
MET
Since 2020, two different targeted therapies have been approved for initial treatment of NSCLC with a MET exon 14 skipping mutation—Tabrecta (capmatinib) and Tepmetko (tepotinib). However, as with many targeted therapies, some tumors may not respond well to these drugs and resistance can develop. This underscores the need to continue researching new treatments for NSCLC with these mutations.

Data from the CHRYSALIS-2 trial revealed that amivantimab may be a future addition treatment option for NSCLC with a MET exon 14 skipping mutation. It showed promising rates and durations of responses, however the effectiveness may be higher for cancer that has not yet been treated with other MET exon 14 targeted therapies.
NTRK
Vitrakvi (larotrectinib) and Rozlytrek (entrectinib) are both approved initial targeted therapy options for cancers that have an NTRK fusion, including NSCLC. Understanding how well these drugs work long term for patients and under which situations they are most effective could help determine the best options for NTRK fusion-positive NSCLC.

Combined long-term follow-up data from two different clinical trials confirmed that Vitrakivi (larotrectinib) produces high rates of lasting response to treatment in NTRK fusion-positive NSCLC, even in patients with brain metastasis. Weight gain was noted as a physical side effect for a group of patients.
Biomarker Testing
Receiving comprehensive biomarker testing is important at diagnosis to determine if a NSCLC tumor has a mutation that would benefit from a targeted therapy. It is also beneficial at progression after being on targeted therapy to help pick the next best treatment option. Biomarker testing is often done using a tumor biopsy, however a liquid biopsy (simple blood sample) can be helpful when getting a tumor biopsy is difficult or does not work well. Understanding how biomarker testing using tissue biopsies and liquid biopsies compare can help inform treatment decisions-based on these different types of tests.

Data from the BFAST trial, a study looking to see if using only liquid biopsy biomarker testing would help identify ROS1-positive NSCLC that would benefit from the ROS-1 targeted therapy Rozlytrek (entrectinib), was shared. Researchers observed that overall, patients had slightly lower benefit from Rozlytrek (entrectinib) in this trial than expected. However, researchers believe that liquid biopsy is more likely to detect a mutation when the cancer is at a more advanced stage and thus patients in this trial had less benefit from therapy since they had more advanced cancer growth. This may indicate that tumor biopsy-based testing is better at diagnosis or with lower stage cancer and liquid biopsy may be best for repeat testing at progression or with higher stage cancer.

On June 27, 2022 Cepheid and BioGX reported a collaboration between the two companies to deliver a PCR test for Monkeypox that will run on the GeneXpert system (Press release, Cepheid, JUN 27, 2022, View Source [SID1234616287]). With a global installed base of over 40,000 GeneXpert systems in 180 countries, this test could be deployed quickly in multiple settings where actionable information is needed .

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According to the Centers for Disease Control and Prevention (CDC), monkeypox is rare and does not spread easily between people without close contact. While the threat of monkeypox to the general U.S. population remains low1, it is important for healthcare providers worldwide to have a preparedness plan. One of the key signs of infection with the virus is fever with development of a maculopapular rash, often appearing as small, raised spots. However, there are many other illnesses, such as chickenpox, measles, bacterial skin infections, syphilis, herpes, and medication-associated allergies that can present with similar symptoms. This underscores the need for a molecular test that can identify monkeypox. The World Health Organization recommends PCR as the preferred laboratory test for monkeypox, using an appropriate skin lesion sample2.

"Our FleXible Cartridge program gives Cepheid the ability to work with external partners to develop accurate tests quickly when the need arises," said David H. Persing, M.D., Ph.D., Cepheid’s EVP and Chief Scientific Officer. Beginning with Bacillus anthracis (Anthrax) and continuing with Mycobacterium tuberculosis, Influenza H1N1, Ebola virus and SARS-CoV-2 among others, Cepheid has a long history of quickly developing and delivering tests that address urgent public health issues as they emerge."

BioGX also has a successful track record of working with government agencies and diagnostic partners to quickly develop and manufacture at-scale molecular tests for detection of emerging pathogens.

"We previously collaborated on a project with the CDC to develop and manufacture a multiplex Monkeypox/Orthopoxvirus test for a GeneXpert-based study3, and now with Cepheid we are moving to the validation stage utilizing the FleXible cartridge," said Michael Vickery, Ph.D., BioGX’s EVP and Chief Scientific Officer. "Regional response teams need a PCR test that is fast and easy to implement when they suspect an outbreak due to a novel pathogen."

Product in development. Not for use in diagnostic procedures. Not reviewed by any regulatory body. Product in development is subject to change and specifications have not yet been established.