On May 26, 2021 NFlection Therapeutics, Inc., a clinical-stage biopharmaceutical company focused on the development of targeted therapies for rare disorders driven by aberrant activation of the RAS pathway (RASopathies), reported positive results from a 28-day, Phase 2a, multicenter, randomized, double-blind, parallel-group, vehicle-controlled clinical trial investigating the safety, tolerability, pharmacokinetics and pharmacodynamics of NFX-179 Gel in subjects with NF1 (Press release, NFlection Therapeutics, MAY 26, 2021, View Source [SID1234580652]). Topical application of NFX-179 Gel is designed to deliver a proprietary "soft" (metabolically labile) MEK inhibitor to cNF tumors to suppress the overactivation of the Ras/Raf/MEK/ERK pathway in these tumors while avoiding the systemic toxicities of orally administered MEK inhibitors, which have not been approved for this indication.

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In the trial, 48 subjects were randomized in a 1:1:1:1 ratio to receive once-daily NFX-179 Gel at 0.05%, 0.15%, or 0.5%, or placebo (vehicle), for 28 days. The primary endpoints were safety, tolerability and suppression of p-ERK, a key biomarker known to promote the growth of cNF tumors.

NFX-179 Gel was well tolerated. No serious adverse events were reported, and no adverse events were classified as related to NFX-179 Gel. All adverse events were mild to moderate and occurred at similar frequencies in the treatment and vehicle groups. Orally administered MEK inhibitors have common adverse effects of rash, diarrhea, peripheral edema and fatigue. Unlike systemic MEK inhibitors, which can cause severe acneiform rash, acneiform rash was not observed during treatment with NFX-179 Gel. Forty seven of the 48 subjects completed the trial; one subject withdrew from the trial due to COVID-19 infection.

NF1 subjects carry a mutation in the gene encoding neurofibromin 1, a tumor suppressor that suppresses the Ras/Raf/MEK/ERK pathway. The resulting overactivation of this pathway leads to increased levels of p-ERK, which drives the growth of cNF tumors. Treatment of cNF tumors with NFX-179 Gel for 28 days induced a dose-dependent suppression of p-ERK in the tumors. Compared to vehicle-treated lesions, tumors treated with 0.5% and 0.15% NFX-179 Gel showed a statistically significant suppression in p-ERK. A 47% reduction (p = 0.0001) in p-ERK was observed in tumors treated with 0.5% NFX-179 Gel, and a 26% reduction (p = 0.04) in p-ERK was observed in tumors treated with 0.15% NFX-179 Gel. The lowest dose group, 0.05% NFX-179 Gel, gave a 10% reduction of p-ERK that was not statistically different from vehicle (p = 0.4). In addition, exploratory secondary endpoints demonstrated a tumor size reduction despite limiting treatment to only 28 days. There was a 17% mean reduction in tumor volume from baseline in the 0.5% NFX-179 Gel group versus an 8% reduction in the vehicle group (p = 0.073). In a per-subject responder analysis, 22% of subjects in the 0.5% NFX-179 group had a 50% or greater mean reduction in tumor volume, versus 6% of subjects in the vehicle group (p = 0.051).

Dr. Guy Webster, Chief Medical Officer of NFlection, said, "We are very pleased with these data, which demonstrate that NFX-179 Gel is well tolerated and induces clinically meaningful levels of p-ERK suppression in cNF tumors. The strong p-ERK biomarker data, along with an unexpected early trend in cNF tumor volume reduction after only 28 days of treatment, support our hypothesis that NFX-179 Gel is an important novel therapy for NF1 patients. We look forward to progressing NFX-179 Gel to Phase 2b to determine the effect of longer treatment duration on cNF tumor regression, as well as to initiating trials testing NFX-179 Gel for the treatment of other cutaneous RASopathies."

"We are delighted that our partnership with NFlection is delivering such encouraging results," said Annette Bakker, Ph.D., President, Children’s Tumor Foundation. "It is really exciting to already observe tumor shrinkage in the 28-day Phase 2a study.

This study provides hope that the NFX-179 Gel could become a life-changing solution for the NF patients suffering with painful and often disfiguring cutaneous neurofibromas, for which no approved pharmacological therapies exist today."

About NFX-179 Gel
NFX-179 is an investigational mitogen-activated protein kinase kinase (MEK) inhibitor. NFX-179 is a "soft" (metabolically labile) drug, which, when formulated as NFX-179 Gel for topical application, is designed to concentrate at the dermal site of action but degrade in systemic circulation, thereby significantly reducing side effects compared to systemically available MEK inhibitors. NFlection is developing NFX-179 Gel for the treatment of RASopathies such as cutaneous neurofibromatosis type 1, immunosuppressant-mediated cutaneous squamous cell carcinoma, and congenital birthmarks.

About Cutaneous Neurofibromatosis Type 1
Cutaneous neurofibromas are tumors that grow from small nerves in the skin or just under the skin and appear as small or larger bumps typically beginning around the time of puberty. Individuals with NF1 commonly develop more cutaneous neurofibromas as they get older. They do not become malignant, but they may be disfiguring, itchy or painful when bumped. Despite their benign nature, they may cause significant problems (e.g., depression, isolation, etc.), and may require surgical removal.

On May 26, 2021 Oncopeptides AB (publ) (Nasdaq Stockholm: ONCO), a global biotech company focused on the development of therapies for difficult-to-treat hematological diseases, reported positive topline results from the head-to-head phase 3 OCEAN study evaluating the efficacy and safety of melphalan flufenamide versus pomalidomide in patients with relapsed refractory multiple myeloma (RRMM) (Press release, Oncopeptides, MAY 26, 2021, View Source [SID1234580651]). The randomized study was initiated in 2017 and includes 495 patients from more than 100 hospitals in 21 countries around the world.

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"Following the accelerated approval of Pepaxto in the U.S. earlier this year, the positive topline results from the OCEAN study marks another major milestone for Oncopeptides. It is very exciting news for patients and indicates that melphalan flufenamide has the potential to become part of the standard of care in relapsed refractory multiple myeloma", says Marty J Duvall, Chief Executive Officer at Oncopeptides AB. "By demonstrating that melphalan flufenamide is at least as efficacious as pomalidomide, we are now able to begin the preparation of a sNDA which could pave the way for a potential use of melphalan flufenamide in earlier lines of therapy in a substantially larger patient population."

The PFS, as assessed by the independent review committee, demonstrated a Hazard Ratio* favoring melphalan flufenamide of 0.817 (95% CI: 0.659-1.012, p=0.0640) for the primary endpoint and shows that melphalan flufenamide is non-inferior to pomalidomide. The Hazard Ratio for PFS as per investigator assessment was 0.790 (95% CI: 0.639-0.976). In both assessments, the median PFS for the melphalan flufenamide arm was more than 40% higher than for the pomalidomide arm. The Overall Response Rate for melphalan flufenamide was 32.1% vs. 26.5% for pomalidomide.

"The efficacy and safety data from the OCEAN study are very encouraging, and the results will be of importance in physicians’ treatment decisions for patients with relapsed and refractory multiple myeloma," says Pieter Sonneveld, MD, PhD, Professor of Hematology at the Erasmus University of Rotterdam, and Principal Investigator of the OCEAN study. "Melphalan flufenamide has a unique mode of action, which in addition with its tolerability profile, makes the drug an attractive treatment option for many patients."

Melphalan flufenamide and pomalidomide had similar discontinuation rates for adverse events, and the safety profile of melphalan flufenamide was in line with previous studies and consistent across age subgroups. The Company expects to present complete OCEAN data at an upcoming scientific congress.

"The outcome from the phase 3 OCEAN study is very good news for patients with relapsed refractory multiple myeloma", says Klaas Bakker, MD, PhD, Executive Vice President and Chief Medical Officer at Oncopeptides. "This head-to-head-comparison was a bold study with an optimal design for demonstrating melphalan flufenamide ‘s true isolated treatment effects. Based on these data, Oncopeptides intends to submit a supplementary New Drug Application to the US Food and Drug Administration FDA, in Q4 2021, given the OCEAN data clearly show that melphalan flufenamide may be an important therapeutic option for the increasing number of patients who need more treatment alternatives. I am truly looking forward to sharing these data with a broader audience."

Melphalan flufenamide is evaluated in a comprehensive clinical study program. In addition to the phase 3 OCEAN study, Oncopeptides is currently enrolling patients in the phase 3 LIGHTHOUSE study, with the aim to establish the efficacy and safety of a combination therapy with melphalan flufenamide plus daratumumab compared to daratumumab, based on the successful results from the ANCHOR study, presented at American Society of Hematology (ASH) (Free ASH Whitepaper) in December 2020.

Limitation of Use

PEPAXTO is not indicated and is not recommended for use as a conditioning regimen for transplant outside of controlled clinical trials.

To view the full prescribing information please visit View Source

About phase 3 OCEAN study

The phase 3 OCEAN study is a global, randomized, head-to-head, open-label study, evaluating the efficacy and safety of melphalan flufenamide and dexamethasone, versus pomalidomide and dexamethasone in patients with relapsed refractory multiple myeloma who have received 2-4 prior therapies. The patients have previously been treated with at least an immunomodulator agent, and a proteasome inhibitor. They have all developed resistance to their last line of therapy and to lenalidomide, the most used drug in multiple myeloma. The study was initiated in 2017 and includes 495 patients from more than 100 hospitals around the world. The primary efficacy endpoint is Progression Free Survival.

About Multiple Myeloma

Multiple myeloma is a cancer of plasma cells, a type of white blood cell which produces antibodies to help fight infection. Multiple myeloma causes cancer cells to accumulate in the bone marrow. Approximately 7 per 100,000 Americans per year are diagnosed with multiple myeloma, making it a rare disease. A growing subset of this population is becoming triple-class refractory. The number of patients diagnosed with multiple myeloma is growing and the number of cases diagnosed annually is expected to almost double in 20 years. The average age for diagnosis is 70 years of age, and there is currently no cure.

On May 26, 2021 Gracell Biotechnologies Inc. (NASDAQ: GRCL) ("Gracell"), a global clinical-stage biopharmaceutical company dedicated to discovering and developing highly efficacious and affordable cell therapies for the treatment of cancer, reported that it will host a key opinion leader (KOL) webinar on the challenges of treating High Risk Multiple Myeloma and a potential novel approach on Friday, June 11, 2021 at 8:00am Eastern Time (Press release, Gracell Biotechnologies, MAY 26, 2021, View Source;a-novel-approach-for-treatment-of-multiple-myeloma-301299911.html [SID1234580650]).

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The call will feature a presentation by Dr. Andrzej Jakubowiak, University of Chicago Medicine, who will give an overview on the current treatment landscape and unmet medical need in treating patients with high-risk multiple myeloma. Dr. Martina Sersch, Chief Medical Officer of Gracell, will present clinical data of GC012F, a BCMA/CD19 dual-targeting CAR-T therapy for multiple myeloma manufactured on Gracell’s proprietary FasTCAR overnight manufacturing platform.

Following the formal presentations, there will be a fireside chat moderated by Neil Canavan of LifeSci Advisors and Author of "The Cure Within" with Dr. Jakubowiak and members of the Gracell management team who will discuss various topics related to the FasTCAR technology platform and the lead clinical program GC012F, a BCMA/CD19 dual-targeting CAR-T therapy. FasTCAR is Gracell’s autologous CAR-T platform that tackles the most pressing challenges associated with autologous therapies, including lengthy manufacturing time, suboptimal manufacturing quality, high therapy cost, and poor T cell fitness.

A live Q&A session will follow the formal presentations and fireside chat.

To register for the event, please click here.

About the KOL

Andrzej Jakubowiak, M.D., Ph.D., is an internationally known expert on multiple myeloma, a cancer of the plasma cells in a patient’s bone marrow. He works closely with the Multiple Myeloma Research Consortium (MMRC) to bring the latest treatments to the patient’s bedside as quickly as possible.

Dr. Jakubowiak’s primary research focus is in the development of new drugs for the treatment of multiple myeloma. He is currently the lead investigator on a number of multi-site clinical trials for patients who are newly diagnosed, have relapsed, or have refractory (resistant to treatment) disease. Dr. Jakubowiak has received research funding and several grants from the MMRC. He is also the recipient of many honors, including the Myeloma Center of the Year award by the MMRC in 2008 and 2010.

A frequently invited lecturer, Dr. Jakubowiak has presented his research findings at medical meetings around the world. He has published more than 50 peer-reviewed articles as well as 14 book chapters. Additionally, he serves as an ad hoc reviewer for several scientific journals, including the Journal of Clinical Oncology, Blood and Leukemia and Lymphoma.

About GC012F

GC012F is a FasTCAR-enabled dual-targeting CAR-T product candidate that is currently being studied in an ongoing investigator-initiated Phase 1 trial across multiple centers in China for the treatment of MM. GC012F tackles MM by simultaneously targeting both malignant plasma cells expressing BCMA and early progenitor cells expressing CD19 in order to drive fast, deep and durable responses in MM patients.

About FasTCAR

CAR-T cells manufactured on Gracell’s proprietary FasTCAR platform appear younger, less exhausted and show enhanced proliferation, persistence, bone marrow migration and tumor cell clearance activities as demonstrated in preclinical studies. With overnight manufacturing, FasTCAR is able to significantly improve cell production efficiency which may result in meaningful cost savings, increasing the accessibility of cell therapies for cancer patients.

On May 26, 2021 TransThera Biosciences Co. Ltd. ( "TransThera" ), a clinical stage biotechnology company dedicated to developing innovative therapeutics across oncology, cardiovascular, and inflammatory diseases with major unmet medical needs globally and in China, reported that it has entered into a collaboration agreement with Roche to explore the combination of TT-00420 and atezolizumab for the treatment of patients in China with gastrointestinal ("GI") tract cancers (Press release, TransThera Biosciences, MAY 26, 2021, View Source [SID1234580649]). The Investigational New Drug application of the combination therapy has been recently approved by China National Medical Products Administration (NMPA).

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GI tract cancers represent one of the most challenging unmet medical needs in China. A lack of effective therapy calls for an emergent need for novel drug development. TT-00420, a unique small molecule kinase inhibitor, has demonstrated preliminary clinical benefits in Cholangiocarcinoma patients and other GI cancer patients in Phase I study. In addition to its targeted therapy attribute, TT-00420 also showed synergistic effect to modulate tumor microenvironment, rendering it a potential partner to checkpoint inhibitors for hard-to-treat solid tumors. Taken together, compelling pre-clinical and clinical data warrant the clinical development of TT-00420 in combination with atezolizumab.

"We are grateful to partner with Roche to tackle the challenge of GI tract cancers affecting people in China. GI cancers represent a huge unmet medical need and we are very excited about the potential of TT-00420 in this field. We are hoping to provide better options for GI cancer patients through the collaboration with Roche in the future", commented by Dr. Peng Peng, Vice President of TransThera in charge of the oncology pipeline development.

About TT-00420

TT-00420 is a highly innovative clinical stage spectrum-selective kinase inhibitor that exerts anti-tumor effects by targeting tumor cells and improving the tumor microenvironment. A large number of preclinical studies have found that TT-00420 has an excellent inhibitory effect on triple-negative breast cancer, cholangiocarcinoma and other malignant tumors. In September 2018, TT-00420 was approved by the US FDA for the first human clinical trial; in February 2019, it was approved by China’s NMPA for human clinical trials; and on November 7 of the same year, TT-00420 was granted the "Orphan Drug Designation" status (ODD) by FDA for the treatment of cholangiocarcinoma. On November 28, 2020, it was again approved by the US FDA targeting the clinical trial of new indication for cholangiocarcinoma. In March 2021, TransThera announced the completion of a phase I dose escalation clinical trial in China and the United States.

On May 26, 2021 Natera, Inc. (NASDAQ: NTRA), a pioneer and global leader in cell-free DNA testing, reported it will present new clinical data on its personalized and tumor-informed molecular residual disease (MRD) assay, Signatera, at the 2021 American Society of Clinical Oncology (ASCO) (Free ASCO Whitepaper) annual meeting, taking place June 4-8, 2021 (Press release, Natera, MAY 26, 2021, View Source [SID1234580648]). Two additional studies were presented at the 2021 American Association for Cancer Research (AACR) (Free AACR Whitepaper) annual meeting that took place April 9-14, 2021.

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At ASCO (Free ASCO Whitepaper), Natera will present four posters highlighting the use of Signatera in new indications including multiple myeloma. It will also unveil new colorectal cancer data from the CIRCULATE-Japan trial, the largest prospective MRD study to date.

"We are proud to share this wealth of new data with the larger oncology community," said Alexey Aleshin, M.D., Natera’s vice president of medical affairs, oncology. "The quality and quantity of these real-world data is a testament to the power of Signatera’s tumor-informed and personalized technology and to Natera’s commitment to pushing the boundaries of our understanding of MRD."

Details about the ASCO (Free ASCO Whitepaper) abstracts are as follows:

Abstract #8029 | Poster Presentation | Presenter: Binod Dhakal, M.D.

Personalized ctDNA analysis to detect minimal residual disease and identify patients at high risk of relapse with multiple myeloma

A retrospective study on the feasibility of using Signatera for MRD assessment in multiple myeloma. Archival bone marrow aspirates and formalin-fixed, paraffin-embedded (FFPE) slides from 28 patients taken at the time of diagnosis were used to design the custom MRD assay for that individual. Patients were serially monitored for a median of 92.4 months after autologous stem cell transplantation (AHCT). Despite the low quality of the samples, the MRD-positive patients had a significantly higher rate of relapse and poorer recurrence-free survival than those who had no detectable MRD after AHCT (HR 5.6, 95% CI: 1.8 – 17, p= 0.0003).

"The variability in sampling of bone marrow aspirates often provides an inaccurate estimate of marrow MRD. Further, serial monitoring of MRD status using bone aspiration is challenging due to the invasive nature of the procedure," said Dr. Binod Dhakal, associate professor of medicine, the Medical College of Wisconsin, and first author of the study. "We are encouraged by the data from this study as it shows that a sensitive ctDNA test can provide a non-invasive alternative that captures the spatial heterogeneity of multiple myeloma."

Abstract #3608 | Poster Presentation | Presenter: Hiroki Yukami, M.D.

Minimal residual disease by circulating tumor DNA analysis for colorectal cancer patients receiving radical surgery: An initial report from CIRCULATE-Japan

CIRCULATE-Japan is the largest prospective MRD study to date. Initial analysis from the first 400 early-stage (stage II-III) or relapsed colorectal cancer (CRC) patients in this observational study shows that Signatera’s tumor-informed approach has a pre-surgical detection rate of >94% across stage I-III CRC patients, and a post-surgical relapse detection rate of 92% with longitudinal sampling. These detection rates compare favorably to longitudinal results from tissue-naive approaches. Additionally, the failure rate of patient samples using Signatera was very low at <3%.

Abstract #3540 | Poster Presentation | Presenter: Tenna V. Henriksen, M.S.

Serial circulating tumor DNA analysis for assessment of recurrence risk, benefit of adjuvant therapy, growth rate and early relapse detection in patients with stage III colorectal cancer

This study serially monitors 168 stage III CRC patients using Signatera for 36 months after surgery, during and after adjuvant chemotherapy, and during surveillance. It demonstrates, for the first time, that the quantitative measurement of ctDNA levels provided by Signatera can be used to assess the growth rates of metachronous metastases. Patients may be classified as having either a slow- or fast-growing tumor based on the rate of increase of ctDNA. Those with fast-growing tumors (137% increase per month) had significantly poorer overall survival compared to those with slow-growing tumors (27% increase per month), underscoring the clinical utility of ctDNA quantitation in the management of stage III CRC.

Abstract #4103 | Poster Presentation | Presenter: Pashtoon Kasi, M.D., M.S.

Tumor-informed assessment of circulating tumor DNA and its incorporation into practice for patients with hepatobiliary cancers

This exploratory study establishes the feasibility of using a tumor-informed MRD test in a heterogeneous cohort of 113 patients with hepatocellular carcinoma, cholangiocarcinoma and gallbladder cancer. Detection rates pre- and post-surgery, during treatment, and surveillance, are reported and shown to correlate with disease stage.

Details about the AACR (Free AACR Whitepaper) abstracts are as follows:

Abstract #552 | Poster Presentation | Presenter: Jocelyn Chapman, M.D.

Circulating tumor DNA predicts disease recurrence in ovarian cancer patients

This study demonstrates the prognostic value of ctDNA in 70 patients with stage I-IV epithelial ovarian cancer (EOC), in comparison to blood biomarker CA-125. The presence of ctDNA was observed to be a strong predictor of relapse (p<0.0001), while CA-125 was not significantly associated with relapse-free survival (p=0.09). ctDNA detection preceded radiological relapse by a median of 10 months (p<0.05), while CA-125 had a lead time of approximately one month.

Abstract #569 | Poster Presentation | Presenter: Antony Tin, Ph.D.

Correlation of variant allele frequency and mean tumor molecules with tumor burden in patients with solid tumors

This poster compares two common measures of tumor burden in cfDNA — variant allele frequency (VAF) and mean tumor molecules (MTM) per mL of plasma. 13,218 plasma samples from 6,265 patients with a wide range of cancer types were analyzed, and discordances between trends in VAF and MTM per mL were observed in 8.8% of samples. These samples were derived from patients who had high total levels of cfDNA due to increased cell death from ongoing treatment. In these scenarios, MTM per mL, which accounts for total cfDNA levels, was found to be more reflective of clinical truth, as confirmed by imaging.

About Signatera
Signatera is a custom-built circulating tumor DNA (ctDNA) test for treatment monitoring and molecular residual disease (MRD) assessment in patients previously diagnosed with cancer. The test is available for both clinical and research use, and has been granted three Breakthrough Device Designations by the FDA for multiple cancer types and indications. The Signatera test is personalized and tumor-informed, providing each individual with a customized blood test tailored to fit the unique signature of clonal mutations found in that individual’s tumor. This maximizes accuracy for detecting the presence or absence of residual disease in a blood sample, even at levels down to a single tumor molecule in a tube of blood. Signatera is intended to detect and quantify how much cancer is left in the body, to detect recurrence earlier and to help optimize treatment decisions.

The Signatera test performance has been clinically validated in multiple cancer types including colorectal, non-small cell lung, breast, and bladder cancers. Signatera has been developed and its performance characteristics determined by Natera, the CLIA-certified laboratory performing the test. The test has not been cleared or approved by the US Food and Drug Administration (FDA). CAP accredited, ISO 13485 certified, and CLIA certified.