On June 9, 2021 EORTC reported that studies were well-represented at this year’s ASCO (Free ASCO Whitepaper) conference, which took place from 4 – 8 June. Seven abstracts were accepted, four for oral presentation, two as posters, and one for online publication (Press release, EORTC, JUN 9, 2021, View Source [SID1234583742]). "This is an impressive confirmation of the high quality and clinical importance of our international, patient-centred, academic trials," said EORTC Director General Dr Denis Lacombe.

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Two oral presentations on Sunday described new results from trials in melanoma and in breast cancer. In the first, Professor Alexander Eggermont presented data from the Phase 3 double-blind KEYNOTE trial, which evaluated pembrolizumab vs. placebo in stage III cutaneous melanoma patients with complete resection of lymph nodes. A subgroup of patients in the trial who had had a recurrence or crossed over from placebo were evaluated and followed as integral part 2 of the protocol. For the 155 patients who crossed over from placebo the 3-Year PFS rate was about 32% and the median PFS was 8.5 months. The 1-Year PFS rate for rechallenged patients was 4 months. The outcome of Pembrolizumab after cross over is in line with previous findings. Treatment activity for re-challenged patients is low.

The second, from Dr Josephine Lopes Cardozo, presented findings on the outcome of patients with an ultra-low risk 70 gene signature in the MINDACT trial. Of the 6,693 breast cancer patients enrolled in the trial, genomic profiling revealed that 1,000 of them were at ultra-low risk of distant recurrence. These patients were followed up for over eight years and results showed the accuracy of the prognosis. They had a breast cancer specific survival of 99.6% regardless of their clinical risk status, and an eight-year distant metastasis-free interval of 97.6%. This result implies that they may be candidates for a further de-escalation of treatment, with a reduction in side effects, the researchers say.

Monday saw an oral presentation of a study on newly diagnosed glioblastoma from Dr Patrick Roth, in which 749 newly diagnosed patients were randomised to receive the standard postoperative treatment of radiotherapy plus temozolomide chemotherapy, or standard treatment plus marizomib. Marizomib is a novel pan-proteasome inhibitor that has had encouraging results in Phase I and II studies. Enrolment started in June 2018 and was intended to include 750 patients, but was halted in September 2020 on the recommendation of the independent data monitoring committee. Results showed that the addition of marizomib to standard treatment did not improve either progression-free or overall survival, and that adverse events, particularly psychiatric and neurotoxicities, were higher in those who received it.

Tuesday’s oral presentation was from Professor Silke Gillessen, who reported on a study of the use of enzalutamide alone or in combination with Radium 223 (RA223) in asymptomatic or mildly symptomatic castration-resistant prostate cancer patients, together with the effect of bone-protecting agents (BPAs). Skeletal fractures are a common adverse effect of systemic treatment for advanced prostate cancer, and as a result, BPAs have recently been recommended. 136 patients randomized after mandating BPAs are part of the safety analysis. At one year without BPA, those in the enzalutamide alone group had a 15.6% risk of fracture, and those in the combined group 37.1%, whereas for those who had received a BPA the risks were almost abolished – 2.6% and 2.7% respectively. The results confirm the importance of using BPAs in these patents, say the researchers.

Two posters from EORTC sarcoma trials also featured at the conference. In the first, Dr Rick Haas and colleagues reported on quality assurance results from the STRASS trial, which looked at the impact of the addition of neoadjuvant radiotherapy to surgery alone in patients with retroperitoneal sarcoma. Radiotherapy was the experimental treatment in the trial, and therefore a quality assurance analysis was important to identify and correct potential deviations from the protocol. The researchers found that over 75% of patients had compliant radiotherapy plans, and that this had significant benefit in terms of abdominal recurrence-free survival as well as overall survival as opposed to the non radiotherapy compliant group. The researchers believe that it is the first quality assurance evaluation of a Phase III sarcoma trial and shows the benefit of quality assurance analyses in radiotherapy.

In a second poster, Dr Roberta Sanfilippo and colleagues presented results from a Phase II trial of cabazitaxel in patients with metastatic or inoperable locally advanced dedifferentiated liposarcoma. The study was devised to examine whether capazitaxel demonstrated sufficient anti-tumour activity in these patients to warrant further investigation in a Phase III trial. Eligible patients were treated with cabazitaxel infusions over one hour every 21 days. Out of the 38 patients enrolled, 21 were progression-free after 12 weeks of treatment. The results of the trial confirm the activity of cabazitaxel, say the researchers, and merit further investigation.

Finally, an abstract published online reports on a mapping exercise carried out by Mrs. Claire Piccinin and colleagues, who set out to link items In the EORTC patient-reported outcomes library with their clinical adverse event equivalents. Analysis showed that the EORTC library provides broad coverage of the common terminology criteria for adverse events (CTCAE) symptomatic toxicities, along with other issues such as emotional wellbeing. Therefore, use of the EORTC library can be complementary to CTCAE and classifying patient-reported outcomes following the CTCAE clinical framework will facilitate the use of patient-reported outcomes in trials and clinical care in the future, they say.

"These studies, which have brought together researchers from countries worldwide, have the potential to improve patient care in a significant fashion and to inform practice. We hope that their presentation at the world’s largest oncology conference will contribute to advancing knowledge in oncology" said Dr Lacombe.

On June 8, 2021 CyGenica has reported that it has raised USD $1.4 million in a seed fund investment round, led by global venture capital investor SOSV (Press release, CyGenica, JUN 8, 2021, View Source [SID1234633831]).

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CyGenica’s disruptive technology addresses the problem of delivering large-molecule therapeutics into living cells without damaging them or triggering an adverse immune response.

The current investment seed round of USD 1.4 million was led by venture capital investor SOSV. Other investors participating in the round included the VOYAGER Health-Tech fund, David Rowan, founder of Voyagers.io, and angel investors Sharaf Yamand Sami Mikati.

CyGenica intends to utilize the investment to accelerate the development of its disruptive drug delivery technology for genome editing, seeking to be a key partner of biopharmaceutical companies in the advancement of cutting-edge therapeutics for cancer and rare diseases to improve patient’s health and quality of life.

"The challenge of delivering drugs for cancer and genetic therapies, be it genes/RNAs/CRISPRs across cell membranes without damaging the cells and triggering an adverse immune response remains a complex hurdle in the pharmaceutical industry. Our groundbreaking technology functions like a universal USB drive. It acts as a nanomachine which can deliver multitudes of cargoes carrying molecular information such as drugs and genetic therapeutics in an efficient, targeted manner without any toxicity and minimum immunogenicity. This will revolutionize drug delivery and lead to better patient outcomes," said Dr Nusrat Sanghamitra, Co-founder and CEO of CyGenica, talking about the latest development.

"This current financing round has brought a diversified international network on board. This will help de-risk our technology, expand our leadership team and take us significantly closer to our goal of enabling safe and targeted intracellular delivery of genetic therapies for cancer and rare diseases," Nusrat further said.

"I am delighted to be leading this investment because CyGenica has solved one of the most pressing problems in biotech: delivery. We are incredibly excited to be part of this revolution," said Bill Liao, Partner SOSV.

"Life-changing healthcare innovation isn’t only coming out of the established life-science hubs. The VOYAGERS Health-Tech Fund is particularly excited to support CyGenica, a remarkable company born in Odisha, India, with the potential to transform targeted drug delivery without the normal side effects that cancer and other patients have had to bear. The VOYAGERS community will do all we can to support Dr Nusrat Sanghamitra and her team in their important mission," said David Rowan, Founder of Voyagers.io.

On June 8, 2021 BeyondSpring Inc. (the "Company" or "BeyondSpring") (NASDAQ: BYSI), a global biopharmaceutical company focused on the development of innovative cancer therapies, reported a late-breaking poster presentation of the company’s lead asset plinabulin, a selective immunomodulating microtubule-binding agent (SIMBA), in combination with pegfilgrastim in breast cancer as part of the Phase 3 PROTECTIVE-2 chemotherapy-induced neutropenia (CIN) study, at the Federation of Clinical Immunology Societies (FOCIS) Annual Meeting being held from June 8-11, 2021 (Press release, BeyondSpring Pharmaceuticals, JUN 8, 2021, View Source;utm_medium=rss&utm_campaign=beyondspring-announces-a-late-breaking-poster-presentation-of-protective-2-phase-3-data-showing-plinabulin-in-combination-with-pegfilgrastim-reverses-the-immune-suppressive-effects-of-pegfilgrastim [SID1234585695]).

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BeyondSpring’s poster titled "Adding Plinabulin (Plin) to Pegfilgrastim (Peg) Reverses the Immune Suppressive Potential of Peg while Offering Superior Prevention of Chemotherapy Induced Neutropenia (CIN) versus Peg Alone)," will be presented on June 9, 2021 at 3:15 p.m. PDT and authors will be available at the poster reception on June 10, 2021 from 4:45 p.m. – 5:30 p.m. PDT (Poster number TH58). Plinabulin in combination with pegfilgrastim demonstrated a superior immune profile and CIN prevention outcomes for patients treated with plinabulin in combination with pegfilgrastim compared to pegfilgrastim alone in breast cancer patients dosed with TAC (Taxotere, doxorubicin, and cyclophosphamide) in PROTECTIVE-2 Phase 3 study. Compared to pegfilgrastim alone (n=110), the plinabulin and pegfilgrastim combination (n=111) showed decreased production of immature neutrophil band (p=0.0012), and decreased promyelocytes and myelocyte production (p=0.0488). Immature neutrophil band and promyelocytes and myelocytes are less functional defending against infection and have potentially deleterious immune suppression effects.

"Plinabulin has broad effects on the immune system and tumor microenvironment. We are excited to see that in addition to the well-demonstrated CIN prevention benefits, we also see that plinabulin can protect against some of the immune-suppressive side effects of pegfilgrastim," said Ramon Mohanlal M.D., Ph.D., Chief Medical Officer and Executive Vice President of Research and Development at BeyondSpring "Plinabulin is a pipeline-in-a-drug and we are seeing more evidence of this with every study, demonstrating that it can help patients with cancer, from side-effects to cancer treatment."

The Company has submitted New Drug Applications (NDA) for plinabulin in combination with pegfilgrastim as a treatment for the prevention of CIN for review in both the U.S. and China. The U.S. FDA accepted the NDA with Priority Review and assigned a Prescription Drug User Fee Act (PDUFA) action date of November 30, 2021.

About The Federation of Clinical Immunology Societies (FOCIS) Annual Meeting
The Federation of Clinical Immunology Societies (FOCIS) exists to improve human health through immunology by fostering interdisciplinary approaches to both understand and treat immune-based diseases. The Federation of Clinical Immunology Societies is a key forum where opinion leaders come together to chart the path to the next major breakthrough in disease therapy. Through FOCIS, researchers and clinicians share knowledge across traditional disease borders, and identify commonalities between treatments and therapies that are life-changing for those impacted by immune-mediated diseases. Initially established as a cross-disciplinary meeting, FOCIS held its first Annual Meeting in 2001. After two successful consecutive meetings, FOCIS incorporated as a 501(c)3 organization in 2003. Today, FOCIS has 58 Member Societies, representing roughly 65,000 clinician scientists.

About CIN
CIN remains a severely unmet medical need and is the primary cause for the 4D’s (Decrease, Delay, Discontinue dose and Downgrade regimen) that compromise carefully selected cancer treatment regimens. Treatment or prevention of CIN with G-CSF has been the standard of care since Neupogen was approved in 1991. The main benefit of G-CSF treatment, however, is in Week 2 after chemotherapy. Week 1 after chemotherapy is considered the "neutropenia vulnerability gap" where over 75% of CIN-related clinical complications occur, including febrile neutropenia, infection, hospitalization and death. Plinabulin is the first drug seeking FDA approval that has the potential to fill this gap. Combining plinabulin and G-CSF may maximize the protection of patients for the full cycle of chemotherapy, as demonstrated in the PROTECTIVE-2 Phase 3 registration study.

Each year in the U.S., 110,000 patients receiving chemotherapy are hospitalized after developing CIN, a severe side effect that increases the risk of infection with fever (also called FN). Due to the COVID-19 pandemic, the updated National Comprehensive Cancer Network (NCCN) guidelines expanded the use of prophylactic G-CSFs, including pegfilgrastim, from high-risk patients only (chemo FN rate >20%), to include intermediate-risk patients (FN rate between 10-20%), to reduce the number of hospital/ER visits related to CIN. The revision of the NCCN guidelines effectively increases the addressable market of patients to approximately 467,500 cancer patients in the U.S. annually.

About Plinabulin
Plinabulin, BeyondSpring’s lead asset, is a selective immunomodulating microtubule-binding agent (SIMBA). It is a novel, intravenous infused, patent-protected, NDA ready asset for CIN prevention indication and a Phase 3 anti-cancer candidate for non-small cell lung cancer (NSCLC). Plinabulin triggers the release of the immune defense protein, GEF-H1, which leads to two distinct effects: first is a durable anticancer benefit due to the maturation of dendritic cells resulting in the activation of tumor antigen-specific T-cells to target cancer cells, and the second is early-onset action in CIN prevention after chemotherapy by boosting the number of hematopoietic stem/progenitor cells (HSPCs). Plinabulin received breakthrough designation from both US and China FDA for CIN prevention indication. As a "pipeline in a drug," plinabulin is being broadly studied in combination with various immuno-oncology agents that could boost the effects of the PD-1/PD-L1 antibodies and re-sensitize PD-1/PD-L1 antibody resistant patients.

On June 8, 2021 Incyte (Nasdaq:INCY) reported that the U.S. Food and Drug Administration (FDA) has extended the review period for the supplemental New Drug Application (sNDA) for ruxolitinib (Jakafi) for the treatment of adult and pediatric patients 12 years and older with steroid-refractory chronic graft-versus-host disease (GVHD) (Press release, Incyte, JUN 8, 2021, View Source [SID1234584957]). The new Prescription Drug User Fee Act (PDUFA) target action date is September 22, 2021.

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The FDA extended the PDUFA action date to allow time to review additional data submitted by Incyte in response to the FDA’s information request. The submission of the additional information has been determined by the FDA to constitute a Major Amendment to the sNDA, resulting in an extension of the PDUFA goal date by three months.

"We remain confident in the data from the REACH3 trial supporting our sNDA submission for ruxolitinib and look forward to continued dialogue with the FDA throughout the remainder of the review process," said Steven Stein M.D., Chief Medical Officer, Incyte. "We will work closely with the agency and are dedicated to bringing this innovative treatment to patients with steroid-refractory chronic GVHD who urgently need new treatment options."

The sNDA was based on data from REACH3, a Phase 3 randomized, open-label, multicenter study comparing ruxolitinib with best available therapy (BAT) in adult and pediatric patients 12 years and older with steroid-refractory chronic GVHD.

About Jakafi (ruxolitinib)

Jakafi is a first-in-class JAK1/JAK2 inhibitor approved by the U.S. FDA for the treatment of polycythemia vera (PV) in adults who have had an inadequate response to or are intolerant of hydroxyurea, intermediate or high-risk myelofibrosis (MF), including primary MF, post-polycythemia vera MF and post-essential thrombocythemia MF in adults, and for the treatment of steroid-refractory acute GVHD in adult and pediatric patients 12 years and older.

Jakafi is marketed by Incyte in the U.S. and by Novartis as Jakavi (ruxolitinib) outside the U.S. Jakafi is a registered trademark of Incyte Corporation. Jakavi is a registered trademark of Novartis AG in countries outside the U.S.

On June 8, 2021 Philogen reported its participation at the CEO Roundtable Zoom Session organised by Goldman Sachs from June 8 to 29, 2021 (Press release, Philogen, JUN 8, 2021, View Source [SID1234584926]).

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Co-founder, CEO and CSO, Prof. Dario Neri has been invited to share and discuss all the dimensions of the unprecedented current market environment, compare notes on the ongoing global situation and key focuses for 2021 and beyond. Dario Neri to attend three roundtables on June 8, 17 and 29, 2021.