On September 2, 2021 Moderna, Inc. (Nasdaq: MRNA), a biotechnology company pioneering messenger RNA (mRNA) therapeutics and vaccines, reported its participation in the following upcoming virtual investor conferences (Press release, Moderna Therapeutics, SEP 2, 2021, View Source [SID1234587204]):

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Wells Fargo 2021 Virtual Healthcare Conference on Friday, September 10, 2021 at 10:00 a.m. ET
Morgan Stanley 19th Annual Global Healthcare Conference on Friday, September 10, 2021 at 11:45 a.m. ET
A live webcast of each presentation will be available under "Events and Presentations" in the Investors section of the Moderna website at investors.modernatx.com. A replay of each webcast will be archived on Moderna’s website for 30 days following the presentation.

On September 2, 2021 Civetta Therapeutics, LLC, a biotechnology company focused on developing a pipeline of therapies that target beta-propeller proteins, reported that Christopher D. Roberts, Ph.D., has been appointed as Chief Executive Officer (Press release, Civetta Therapeutics, SEP 2, 2021, View Source [SID1234587203]). Dr. Roberts, who most recently served as Chief Scientific Officer of Black Diamond Therapeutics, brings more than 20 years of leadership experience discovering and developing novel therapies for oncology, immunology, virology and other indications.

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"Civetta has developed a unique discovery platform designed to rigorously investigate, validate and drug beta-propeller proteins. Because propeller domains are ubiquitous and play critical functions in pathways that are known contributors to pathogenesis, they provide broad opportunity as therapeutic targets," said Dr. Roberts. "I’m impressed by the work the team has done advancing its lead programs and platform. I look forward to joining the Civetta team in the discovery and development of novel, first-in-class therapies that can help patients across a variety of disease areas, from cancer, inflammation and immunology to neurodegeneration and metabolic disease."

Cameron Wheeler, Ph.D., who was serving as Chief Executive Officer at Civetta and is a Partner in the Biotherapeutics Group at Deerfield Management Company, will continue to serve as chairman of Civetta’s board of directors.

"The team at Civetta has done great work taking the early insights into beta-propeller science made by our founders at the Broad Institute and the Dana-Farber Cancer Institute and advancing them, to better understand their role in a variety of diseases," said Dr. Wheeler. "We see broad potential for targeting beta-propeller proteins and we’re working to identify novel, near-term therapeutics and establish the leading beta-propeller targeting platform in the industry. Attracting top talent like Chris will continue to be critical as we accelerate and expand our programs and pipeline."

Prior to joining Black Diamond, Chris served as an Entrepreneur in Residence at SR One, the corporate venture capital arm of GlaxoSmithKline (GSK). Prior to SR One, Chris was the Vice President (VP) of Chemistry and Early Development at Syros Pharmaceuticals, Inc., a publicly traded biotechnology company focused on gene control and drugging transcription, where he built and led a variety of discovery and development functions and helped guide two oncology assets into clinical development. Prior to joining Syros, Chris held numerous positions of increasing responsibility at GSK, including VP and Head of the Host Defense Discovery Performance Unit, and also led multiple clinical development projects. He joined GSK as Senior Director of Hepatitis C Virus (HCV) Medicinal Chemistry via its acquisition of Genelabs Technologies. As a medicinal chemist at Genelabs, Chris was significantly involved in establishing Genelabs’ HCV research focus. His work has been extensively published.

Chris earned a Ph.D. in Organic Chemistry from the University of California, Riverside, and completed a post-doctoral fellowship at the University of Bern, Switzerland. He graduated with a B.A. in Chemistry from Whitworth University.

On September 2, 2021 The Jerome Canady Research Institute for Advanced Biological and Technological Sciences (JCRI-ABTS), in collaboration with US Medical Innovations, LLC (USMI), reported that they have discovered the mechanism using Canady Helios Cold Plasma (CHCP) to induce cell death in breast cancer (Press release, JCRI-ABTS, SEP 2, 2021, View Source [SID1234587202]).

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Recently accepted for publication in the International Journal of Molecular Sciences, the article "Canady Helios Cold Plasma Induces Breast Cancer Cell Death by Oxidation of Histone mRNA" described how research scientists at JCRI/ABTS treated four (4) breast cancer cell lines with Canady Helios Cold Plasma (CHCP) at different dosages and monitored the progress of apoptosis (cell death).

Jerome Canady, MD (CEO of USMI), stated "As we have proven, CHCP is a very promising adjuvant therapy to selectively combat many cancers, but our focus in this report is our work on breast cancer which affects over 3.5 million women in the US alone. Inhibition of cell proliferation, induction of apoptosis, and disruption of cell cycle were all observed during the early S-phase of the cell cycle. This news is auspicious because it shows CHCP treatment can be personalized for specific breast cancer types."

Canady Helios Cold Plasma or CHCP is a highly selective, non-thermal process developed by USMI for treating solid cancerous tumors during the surgical procedure. CHCP triggers both chemical and molecular changes in the cancer cells that cause significant stress and drastically decreases the cancer cell’s viability, leading to apoptosis. CHCP is proven to be safe and causes no thermal injury to normal tissue.

JCRI-ABTS and USMI have recently completed the first FDA-approved Phase I Clinical Trial to evaluate Cold Atmospheric Plasma for the treatment of cancer (IDE #190165). The clinical sites were Rush University Medical Center (Chicago, IL) and Sheba Medical Center (Ramat Gan, Israel)).

More information will be shared when Dr Canady presents at the annual Baird Global Healthcare Conference on September 14th at 10:15 AM ET.

On September 2, 2021 Sunovion Pharmaceuticals Inc. (Sunovion) reported that it has entered into an agreement with BIAL in which Sunovion has granted exclusive commercial license rights in Europe for apomorphine sublingual film (APL-130277) (Press release, Sunovion, SEP 2, 2021, View Source [SID1234587201]). APL-130277, approved as KYNMOBI (apomorphine hydrochloride) sublingual film in the U.S. and Canada, is a novel thin film formulation of apomorphine that dissolves under the tongue for the acute, intermittent treatment of OFF episodes in patients with Parkinson’s disease (PD). APL-130277 is currently in Phase 3 clinical development in Europe.

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By 2030, an estimated 10 million people worldwide will be living with PD.1 OFF episodes are the re-emergence or worsening of PD symptoms otherwise controlled with oral levodopa/carbidopa. These episodes may disrupt a person’s ability to perform everyday activities and are characterized, in part, by tremor, stiffness, slowed movement or other symptoms.

Under the terms of the agreement, BIAL will be responsible for submitting marketing applications consistent with marketing authorization procedures in Europe and have exclusive commercial rights to distribute and commercialize apomorphine sublingual film in the European Union (EU), the European Economic Area (EEA) as well as the United Kingdom. BIAL expects to submit a European marketing authorization application for apomorphine sublingual film by the end of 2021. Sunovion will receive an upfront payment and is entitled to receive certain milestone payments. Sunovion will supply KYNMOBI in all approved dose strengths to BIAL.

Sunovion continues to hold the exclusive commercial rights to KYNMOBI in North America and all other regions of the world outside of the EU, EEA as well as the United Kingdom. KYNMOBI is the first and only sublingual (under the tongue) therapy available for the on-demand treatment of PD OFF episodes in the U.S. and Canada.

ABOUT KYNMOBI

KYNMOBI (apomorphine hydrochloride) sublingual film, a novel formulation of apomorphine, a non-ergoline dopamine agonist, is the first and only sublingual therapy approved in the United States and Canada for the fast-acting, on-demand treatment of OFF episodes associated with Parkinson’s disease. In the U.S. and Canada KYNMOBI may be used up to five times a day.

Phase 3 clinical trial results, published in Lancet Neurology, demonstrated that patients with PD receiving KYNMOBI experienced significant improvements in motor symptoms at 30 minutes after dosing at week 12, with a mean reduction of 7.6 points, compared to placebo, on the Movement Disorder Society Unified Parkinson’s Disease Rating Scale (MDS-UPDRS) Part III score. Separation from placebo was seen as early as 15 minutes post-dose (first time point measured) and persisted up to 90 minutes (last time point measured). Additionally, a significantly higher percentage of people treated with KYNMOBI had a patient-rated full ON response within 30 minutes at week 12, compared with people receiving placebo. KYNMOBI was generally well-tolerated. Among the most frequently reported treatment-emergent adverse events in this study (occurring in more than 5 percent of patients and at a rate greater than placebo) were nausea, oropharyngeal reactions, somnolence and dizziness.

Important Safety Information (United States)

INDICATION

KYNMOBI (apomorphine hydrochloride) sublingual film is a prescription medicine used to treat short-term (acute), intermittent "off" episodes in people with Parkinson’s disease (PD).

It is not known if KYNMOBI is safe and effective in children.

IMPORTANT SAFETY INFORMATION FOR KYNMOBI (apomorphine hydrochloride) SUBLINGUAL FILM

Do not take KYNMOBI if you are taking certain medicines to treat nausea called 5HT3 antagonists, including ondansetron, granisetron, dolasetron, palonosetron, and alosetron. People taking ondansetron together with apomorphine, the active ingredient in KYNMOBI, have had very low blood pressure and lost consciousness or "blacked out."

Do not use KYNMOBI if you are allergic to apomorphine hydrochloride or to any of the ingredients in KYNMOBI. KYNMOBI also contains a sulfite called sodium metabisulfite. Sulfites can cause severe, life‐threatening allergic reactions in some people. An allergy to sulfites is not the same as an allergy to sulfa. People with asthma are more likely to be allergic to sulfites. Call your healthcare provider if you have hives, itching, rash, swelling of the lips, tongue and mouth, redness of your face (flushing), throat tightness, trouble breathing or swallowing.

Before starting KYNMOBI, tell your healthcare provider:

About all of your medical conditions, including if you:

have difficulty staying awake during the daytime
have liver problems
have dizziness
have kidney problems
have fainting spells
have heart problems
have low blood pressure
have had a stroke or other brain problems
have asthma
have a mental problem called a major psychotic disorder
are allergic to any medicines containing sulfites
drink alcohol
are pregnant or plan to become pregnant. It is not known if KYNMOBI will harm your unborn baby
are breastfeeding or plan to breastfeed. It is not known if KYNMOBI passes into your breast milk. You and your healthcare provider should decide if you will take KYNMOBI or breastfeed.
Tell your healthcare provider about all the medicines you take, including:

prescription medicines
over-the-counter medicines
vitamins
herbal supplements
KYNMOBI may affect the way other medicines work, and other medicines can affect how KYNMOBI works. Taking KYNMOBI with other medicines may cause serious side effects. If you take nitroglycerin under your tongue (sublingual) while using KYNMOBI, your blood pressure may decrease and cause dizziness. You should lie down before and after taking sublingual nitroglycerin.

KYNMOBI can cause serious side effects, including:

nausea and vomiting. Nausea is a common side effect of KYNMOBI. Nausea and vomiting can happen with KYNMOBI. Your healthcare provider may prescribe a medicine called an antiemetic, such as trimethobenzamide to help prevent nausea and vomiting.
sleepiness or falling asleep during the day. Sleepiness is a serious, and common side effect of KYNMOBI. Some people treated with KYNMOBI may get sleepy during the day or fall asleep without warning while doing everyday activities such as talking, eating, or driving a car.
dizziness. Dizziness is a serious, and common side effect of KYNMOBI. KYNMOBI may lower blood pressure and cause dizziness. Dizziness can happen when KYNMOBI treatment is started or when the KYNMOBI dose is increased. Do not get up too fast from sitting or after lying down, especially if you have been sitting or lying down for a long period of time.
mouth (oral) irritation. Mouth (oral) irritation is a common side effect of KYNMOBI. You should call your healthcare provider if you develop any of these signs or symptoms.

redness
mouth sores (ulceration)
dryness of the mouth, lips or tongue

swelling
pain
pain with swallowing
falls. The changes that can happen with PD, and the effects of some PD medicines, can increase the risk of falling. KYNMOBI may also increase your risk of falling.
hallucinations or psychotic-like behavior. KYNMOBI may cause or make psychotic-like behavior worse including hallucinations (seeing or hearing things that are not real), confusion, excessive suspicion, aggressive behavior, agitation, delusional beliefs (believing things that are not real), and disorganized thinking.
strong (intense) urges. Some people with PD have reported new or strong uncontrollable urges to gamble, increased sexual urges, increased urges to spend money (compulsive shopping), and other intense urges, while taking PD medicines, including KYNMOBI. If you or your family members notice that you have strong urges, talk to your healthcare provider. The strong urges may go away if your KYNMOBI dose is lowered or stopped.
high fever and confusion. KYNMOBI may cause a problem that can happen in people who suddenly lower their dose, stop using, or change their dose of KYNMOBI. Symptoms include:

very high fever
confusion

stiff muscles
changes in breathing and heartbeat
Do not stop taking KYNMOBI or change your dose unless you are told to do so by your healthcare provider.

heart problems. If you have shortness of breath, fast heartbeat, chest pain, or feel like you are going to pass out (faint) while taking KYNMOBI, call your healthcare provider or get emergency help right away.
tissue changes (fibrotic complications). Some people have had changes in the tissues of their pelvis, lungs, and heart valves when taking medicines called nonergot derived dopamine agonists like KYNMOBI.
prolonged painful erections (priapism). KYNMOBI may cause prolonged, painful erections in some people. If you have a prolonged and painful erection, you should call your healthcare provider or go to the nearest hospital emergency room right away.
The most common side effects of KYNMOBI include:

nausea
dizziness

sleepiness
mouth swelling, pain, or sores
You are encouraged to report negative side effects of prescription drugs to the FDA. Visit www.fda.gov/medwatch or call 1-800-FDA-1088.

Please see full Prescribing Information for KYNMOBI at View Source

About Parkinson’s Disease and OFF Episodes

By 2030, it is estimated that 1.2 million people in the U.S. and an estimated 10 million people worldwide will be living with Parkinson’s disease (PD).2 PD is a chronic, progressive neurodegenerative disease characterized by motor symptoms, including tremor at rest, rigidity and impaired movement, as well as significant non-motor symptoms, including cognitive impairment and mood disorders. It is the second most common neurodegenerative disease after Alzheimer’s disease,2 and the prevalence of PD is increasing as the world’s population ages.

OFF episodes are the re-emergence or worsening of PD symptoms otherwise controlled with oral levodopa/carbidopa. These episodes may disrupt a person’s ability to perform everyday activities, can cause anxiety and may be burdensome for patients, family and care partners. OFF episodes are experienced by nearly 60 percent of people with PD within the first four to six years of diagnosis, and may worsen in frequency and severity over the course of the illness.3

On September 2, 2021 Gamida Cell Ltd. (Nasdaq: GMDA), an advanced cell therapy company committed to cures for blood cancers and serious blood diseases, reported that company management will present its corporate highlights at the following virtual investor conferences in September (Press release, Gamida Cell, SEP 2, 2021, View Source [SID1234587200]):

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H.C. Wainwright 23rd Annual Global Investment Conference, September 13-15, 2021. Company presentation will be available to view on-demand beginning on September 13 at 7:00 a.m. ET.
Baird’s 2021 Global Healthcare Conference, September 14, 2021 with a presentation at 11:25 a.m. ET.
In the fourth quarter of 2021, Gamida Cell is targeting a BLA submission for omidubicel, the first potential approval of a cell therapy for blood cancer patients in need of an allogeneic bone marrow transplant. This submission is expected to occur by the end of the year, subject to a pre-BLA meeting with the U.S. Food and Drug Administration (FDA) planned for the fourth quarter. In the third quarter of 2021, the Company is planning an IND submission to support the initiation of a Phase 1/2 clinical study of cryopreserved, off-the-shelf GDA-201 in patients with follicular and diffuse large b-cell lymphomas.

A webcast of both conference presentations will be available on the "Investors & Media" section of Gamida Cell’s website at www.gamida-cell.com, and will be available for at least 14 days following the event.