Transgene Unveils myvacTM, an Individualized Immunotherapy against Solid Tumors

On September 24, 2018 Transgene (Paris:TNG) (Euronext Paris: TNG) a biotechnology company that designs and develops virus-based immunotherapies against cancers and infectious diseases, reported myvacTM, an individualized, viral vector-based immunotherapy against cancer that will enter clinical development in 2019 (Press release, Transgene, SEP 24, 2018, View Source [SID1234621824]).

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myvacTM, an individualized, MVA-based immunotherapy
myvacTM is designed to stimulate and educate the immune system of patients to recognize and destroy tumor cells. The personalized immunotherapy product is based on the mutations that are identified in the patient’s own tumor. These mutations are highly relevant targets since they lead to the expression of tumor neoantigens which are known to trigger a stronger immune response than "classic"2 tumor antigens.

Once administered to the patient, myvacTM triggers a cascade of immune responses against a variety of targets found in the cancer cells.

The neoantigens which are the basis for the myvacTM approach are identified by sequencing and selected using artificial intelligence algorithms, and then integrated into the genome of the viral vector (MVA).

myvacTM differs from autologous treatments since no biological material from the patient is used in the manufacturing process and as such is much easier to manufacture; it is a truly individualized approach that uses the information that is specific to the characteristics of each patient’s tumor.

Transgene has combined its expertise in viral vectors with highly innovative technologies to develop myvacTM.

myvacTM features several key advantages:

It is expected to deliver the benefits of an individualized treatment without the disadvantages of autologous approaches (Transgene does not modify the patient’s cells but integrates the neoantigen panel into the virus);
It is based on a viral strain (MVA) whose safety, tolerability, immunogenicity and efficacy have already been demonstrated in the clinic with TG4010 and TG4001;
The myvacTM viral vector (MVA) has repeatedly shown that it can induce a strong immune response from the patient against the tumor antigens incorporated in its viral genome as well as an enlargement of the antitumoral immune repertoire (epitope spreading);
An "all-in-one" formula, requiring neither adjuvant nor association of different peptides.
Éric Quéméneur, PhD, Executive VP, Chief Scientific Officer of Transgene, said: "With myvacTM, Transgene is at the forefront of innovation in cancer immunotherapy. Based on our know-how in virotherapy, we have successfully integrated sequences coding for neoantigens to create an individualized immunotherapy. By combining sequencing and artificial intelligence with the design of the virus, myvacTM marks the entry of viral vector-based approaches in the era of digital transformation. Importantly we have also set up an organization able to design and manufacture myvacTM for each patient in a timely and cost-competitive manner. The myvacTM innovation is a logical evolution of our expertise and a new therapeutic option that promises a major improvement over existing therapies. myvacTM is also the result of our policy of open innovation which is based on working with partners developing technologies that are complementary to our expertise allowing us to benefit from a multidisciplinary approach. We look forward to demonstrating the transformative potential of myvacTM in the clinical trials we plan to start in 2019."

myvacTM, an ambitious project expected to enter the clinic in 2019
myvacTM will be administered to patients with solid tumors. Two clinical trials are being set up in Europe and in the United States, including HPV-negative head and neck cancers and ovarian cancer. These trials are expected to start in 2019.
The first preclinical and translational results will be presented soon at immuno-oncology conferences.

Our innovative network combines bioengineering and digital transformation

To design myvacTM, Transgene and its collaborative network had to overcome many scientific and technical challenges. The network’s expertise covers all the required know-how:

Institut Curie (Cancer Immunotherapy Center, led by Professor Amigorena) is involved in the generation of translational data and the characterization of the mechanism of action;
HalioDx studies biomarkers to maximize the effectiveness of the therapy;
Traaser automates, secures and manages genomic data, including predictive algorithms provided by a recognized partner in artificial intelligence;
Transgene has developed a unique manufacturing pilot unit in France to vectorize neoantigens and provide myvacTM within a timeframe compatible with clinical treatment schemes.
This innovative project has obtained the labeling of the Biovalley France and Eurobiomed French competitiveness clusters.

Transgene holds the intellectual property of the myvacTM viral vector platform and is actively working on the translational development of this innovative technology.

Spectrum Pharmaceuticals Announces Release of Updated Poziotinib Data From MD Anderson Phase 2 Study in Non-Small Cell Lung Cancer Patients

On September 24, 2018 Spectrum Pharmaceuticals, Inc. (NasdaqGS: SPPI), a biotechnology company with fully integrated commercial and drug development operations with a primary focus in hematology and oncology, reported preliminary poziotinib data from the University of Texas, MD Anderson Cancer Center Phase 2 non-small cell lung cancer (NSCLC) study which were released today during an oral presentation at the IASLC 19th World Conference on Lung Cancer hosted by the International Association for the Study of Lung Cancer (Press release, Spectrum Pharmaceuticals, SEP 24, 2018, View Source [SID1234529537]). The MD Anderson study is the single largest data set of patients with an exon 20 mutation in EGFR or HER2.

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"There are currently no approved targeted therapies for this hard-to-treat population," said John Heymach, M.D., Ph.D., Chairman and Professor, Department of Thoracic/Head and Neck Medical Oncology, University of Texas, MD Anderson Cancer Center. "For this reason, it is especially exciting to observe that poziotinib is highly active, with a manageable safety profile, in these heavily pre-treated patients. The study is ongoing with nineteen EGFR patients remaining on treatment, six of which have been on drug for longer than a year. Poziotinib may offer a much needed option to NSCLC patients with exon 20 mutations in EGFR or HER2."

In the interim analysis presented at the WCLC, the following observations were made:

This phase II study demonstrates high anti-tumor activity for poziotinib in metastatic, heavily pretreated EGFR exon 20 mutant NSCLC, a group for which no targeted agents have proven effective to date (other than patients bearing T790M or S768I mutations) with best response of PR in 55% of evaluable patients (43% confirmed ORR to date; 19 patients remain on treatment).
Median PFS 5.5m; durable responses observed with 6 treated for >1year thus far.
Compares favorably to historical ORR rates of <8% approved TKIs and <19% for standard of care 2L agents (docetaxel, PD-1/PD-L1 inhibitors).
Significant activity also observed in HER2 exon 20-mutant NSCLC with initial responses observed in 50% (6/12) evaluable patients and median PFS 5.1m.
EGFR-related toxicities (including rash, diarrhea, & paronychia) were manageable and required dose reductions in 60%. Discontinuation due to poor tolerance was rare (3%).
Encouraging activity has prompted a confirmatory, international, multicenter study in EGFR and HER2 exon 20 mutant NSCLC patients which is currently enrolling (NCT03318939), including a first-line cohort, and development of a separate pan-tumor basket study.
The poziotinib NSCLC clinical program for patients with EGFR or HER2 exon 20 insertion mutations currently consists of a Phase 2 investigator-initiated study at The University of Texas, MD Anderson Cancer Center and a Phase 2 pivotal, Spectrum-sponsored, multi-center, global study (ZENITH20) with active sites in the United States and future centers planned in Canada and Europe. The overall poziotinib clinical development program is focused on four pillars, including previously treated NSCLC, first-line treatment of NSCLC, combination therapy and treatment of other solid tumors.

Following the oral presentation of data, Spectrum Pharmaceuticals will be hosting a live webcast featuring Dr. John Heymach.

Conference Call Details:

Monday, September 24, 2018 @ 4:30 p.m. Eastern/1:30 p.m. Pacific

Domestic: (877) 837-3910, Conference ID# 1993267
International: (973) 796-5077, Conference ID# 1993267

The conference call will also be webcast live. To access the webcast and additional documents related to the call, please visit the Investor Relations page of the Spectrum Pharmaceuticals website at View Source

For interested individuals unable to join the call, a replay will be available from September 24, 2018 @ 7:00 p.m. ET/4:00 p.m. PT through October 1, 2018, until 7:30 p.m. ET/4:30 p.m. PT.

Domestic Replay Dial-In: (855) 859-2056, Conference ID# 1993267
International Replay Dial-In: (404) 537-3406, Conference ID# 1993267

About Poziotinib

Poziotinib is a novel, orally available Epidermal Growth Factor Receptor Tyrosine Kinase Inhibitor (EGFR TKI) that inhibits the tyrosine kinase activity of EGFR as well as HER2 and HER4. Importantly this, in turn, leads to the inhibition of the proliferation of tumor cells that overexpress these receptors. Mutations or overexpression/amplification of EGFR family receptors have been associated with a number of different cancers, including non-small cell lung cancer (NSCLC), breast cancer, and gastric cancer. Spectrum received an exclusive license from Hanmi Pharmaceuticals to develop, manufacture, and commercialize worldwide, excluding Korea and China. Poziotinib is currently being investigated by Spectrum and Hanmi in several mid-stage trials in multiple solid tumor indications.

BLINCYTO® (blinatumomab) Approved In Japan For The Treatment Of Relapsed Or Refractory B-cell Acute Lymphoblastic Leukemia

On September 24, 2018 Amgen (NASDAQ:AMGN) reported that the Japanese Ministry of Health, Labour and Welfare has granted marketing approval for BLINCYTO (blinatumomab) for the treatment of relapsed or refractory B-cell acute lymphoblastic leukemia (ALL) (Press release, Amgen, SEP 24, 2018, View Source;p=RssLanding&cat=news&id=2368696 [SID1234529558]). BLINCYTO was developed in Japan by Amgen Astellas BioPharma K.K. (AABP), a joint venture between Amgen and Astellas Pharma Inc., a pharmaceutical company headquartered in Tokyo.

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"As proof-of-concept for our bispecific T cell engager technology, BLINCYTO has laid the groundwork for Amgen to deliver on our passion of addressing cancer by exploring numerous biologic pathways and therapeutic modalities," said David M. Reese, M.D., executive vice president of Research and Development at Amgen. "This innovation is a good example of how we provide new options to patients with serious illnesses like cancer. In bringing BLINCYTO to Japanese patients, we reinforce our commitment to deliver novel cancer therapies on behalf of patients worldwide."

BLINCYTO is the first-and-only bispecific T cell engager (BiTE) immunotherapy construct approved globally. It is also the first approved immunotherapy from Amgen’s BiTE platform, an innovative approach that helps the body’s immune system target cancer cells.

"Today’s approval of BLINCYTO marks a significant milestone that reinforces our commitment to addressing unmet medical needs of patients in Japan," said Steve Sugino, president and representative director, AABP. "As our first oncology treatment approved in the region, we are proud to provide a much-needed innovative treatment option for adults and children with relapsed or refractory B-cell ALL, one of the most aggressive B-cell malignancies."

Hitoshi Kiyoi, M.D., Ph.D., professor of internal medicine, Hematology and Oncology, Nagoya University Graduate School of Medicine said, "The standard therapy for relapsed or refractory B-cell ALL has not been established in Japan and therefore different chemotherapy regimens have been selected, depending on the condition and background of each patient. BLINCYTO is a much-needed and important new treatment option for patients with relapsed or refractory B-cell ALL, as demonstrated by the efficacy and survival benefit seen in the TOWER study."

The approval is based on data from multiple global studies, including the Phase 3 TOWER study and Japan Phase 1b/2 Horai study. In the TOWER study, BLINCYTO demonstrated a superior improvement in median overall survival (OS) versus standard of care (SOC) chemotherapy. Median OS was 7.7 months (95 percent CI: 5.6, 9.6) for BLINCYTO versus 4.0 months (95 percent CI: 2.9, 5.3) for SOC (HR for death=0.71; p=0.012). Safety results among subjects who received BLINCYTO were comparable to those seen in the previous Phase 2 studies of BLINCYTO in adult patients with Philadelphia chromosome-negative (Ph-) relapsed or refractory B-cell precursor ALL. In the TOWER study, major adverse reactions were pyrexia (39.0 percent), decrease in white blood cell count (14.6 percent), cytokine release syndrome (13.5 percent), febrile neutropenia (10.9 percent), headache (10.1 percent), elevated liver enzyme (10.1 percent) and decrease in platelet count (10.1 percent). In the Phase 1b/2 Horai study, BLINCYTO was administered to 35 Japanese adult and pediatric patients with relapsed or refractory B-cell precursor ALL. The safety results from the Horai study were comparable to those seen in the global studies, including TOWER. In the Horai study, major adverse reactions in adult patients were cytokine release syndrome (46.2 percent), pyrexia (46.2 percent), decrease in white blood cell count (38.5 percent) and decrease in platelet count (34.6 percent), and major adverse reactions in pediatric patients were elevated liver enzyme (66.7 percent), pyrexia (66.7 percent), cytokine release syndrome (55.6 percent) and abdominal pain (44.4 percent).

BLINCYTO is now approved in 57 countries, including the United States (U.S.), all member countries in the European Union (EU) and the European Economic Area, Canada and Australia.

About the TOWER Study
The TOWER study was a Phase 3, randomized, active-controlled, open-label study investigating the efficacy of BLINCYTO versus SOC chemotherapy in 405 adult patients with Ph- relapsed or refractory B-cell precursor ALL. The study enrolled a difficult-to-treat patient population which included patients with one or more relapses or refractory disease. In the BLINCYTO arm, this included 35 percent of patients that had relapsed post-allogenic hematopoietic stem cell transplant (alloHSCT) and excluded those with late first relapse (≥12 months after initial remission). Patients were randomized in a 2:1 ratio to receive BLINCYTO (n=271) or treatment with investigator choice of SOC chemotherapy (n=134). The determination of efficacy was based on OS. These results were published in The New England Journal of Medicine.1

About the Horai Study
The Horai study is a Phase 1b/2, single-arm, open-label study evaluating the safety and efficacy of BLINCYTO in Japanese adult and pediatric patients with relapsed or refractory B-cell precursor ALL. The primary endpoint for the Phase 1b portion was incidence of dose-limiting toxicities; the primary endpoint for the Phase 2 portion was complete remission or complete remission with partial hematologic recovery within 12 weeks of treatment with BLINCYTO. Secondary endpoints include duration of response, OS and relapse-free survival. An extension of the study is ongoing. For more information about this trial, please visit www.clinicaltrials.gov under trial identification number NCT02412306.

About ALL in Japan
ALL is a rapidly progressing cancer of the blood and bone marrow that occurs in both adults and children.2,3 Japan is reported to have approximately 5,000 ALL patients, and it is estimated that of these, there are around 520 patients with relapsed or refractory ALL annually.4-7 Adults with relapsed or refractory ALL typically have a very poor prognosis, with a median OS of three to five months.8 Prognosis for children with ALL who are refractory or experience a relapse is extremely poor, and post-relapse survival is only achieved in 40-50 percent of patients.9-11

About BiTE Technology
Bispecific T cell engager (BiTE) antibody constructs are a novel immune-oncology technology that can be engineered to target any tumor antigen expressed by any type of cancer. The modified antibodies are designed to kill malignant cells using the patient’s own immune system by bridging T cells to tumor cells. BiTE antibody constructs help connect the T cells to the targeted cell, with the intent of causing T cells to inject toxins which trigger cancer cell death (apoptosis). Amgen is developing BiTE antibody constructs to uniquely (or specifically) target numerous hematologic malignancies and solid tumors.

About BLINCYTO (blinatumomab)
BLINCYTO is a bispecific CD19-directed CD3 T cell engager (BiTE) immunotherapy that binds to CD19 expressed on the surface of cells of B-lineage origin and CD3 expressed on the surface of effector T cells. BLINCYTO was granted breakthrough therapy and priority review designations by the U.S. Food and Drug Administration (FDA) in 2014, and now carries full approval in the U.S. for the treatment of relapsed or refractory B-cell precursor ALL in adults and children. In the U.S., BLINCYTO is also approved under accelerated approval for the treatment of adults and children with B-cell precursor ALL in first or second complete remission with minimal residual disease (MRD) greater than or equal to 0.1 percent.

BLINCYTO is approved in the EU for the treatment of Ph- relapsed or refractory B-cell precursor ALL in adults and children.

Important Japan Product Information

Indication:
Relapsed or refractory B-cell acute lymphoblastic leukemia

Dosage and Administration:
In general, blinatumomab (Genetical Recombination) is administered as continuous intravenous infusion with the following dosing regimen for 28 days followed by a 14-day treatment-free interval. This constitutes one cycle and is repeated up to 5 cycles. After that, blinatumomab (Genetical Recombination) is administered with the following dosing regimen for 28 days followed by a 56-day treatment-free interval. This constitutes one cycle and is repeated up to 4 cycles. Of note, dose of BLINCYTO can be reduced as appropriate depending on patient’s condition.

Patients with a body weight of ≥45 kg: 9 μg/day on Days 1 to 7 of Cycle 1, then 28 μg/day.
Patients with a body weight of <45 kg: 5 μg/m2 (body surface area [BSA])/day on Days 1 to 7 of Cycle 1, then 15 μg/m2 (BSA)/day. The dose should not exceed the dose for patients with a body weight of ≥45 kg.
For more information, see the latest Japan Package Inserts.

Important Safety Information Regarding BLINCYTO (blinatumomab) U.S. Indication
BLINCYTO is indicated for the treatment of B-cell precursor acute lymphoblastic leukemia (ALL) in first or second complete remission with minimal residual disease (MRD) greater than or equal to 0.1% in adults and children. This indication is approved under accelerated approval based on MRD response rate and hematological relapse-free survival. Continued approval for this indication may be contingent upon verification and description of clinical benefit in the confirmatory trials.

BLINCYTO is indicated for the treatment of relapsed or refractory B-cell precursor acute lymphoblastic leukemia (ALL) in adults and children.

WARNING: CYTOKINE RELEASE SYNDROME and NEUROLOGICAL TOXICITIES

Cytokine Release Syndrome (CRS), which may be life-threatening or fatal, occurred in patients receiving BLINCYTO. Interrupt or discontinue BLINCYTO as recommended.
Neurological toxicities, which may be severe, life-threatening or fatal, occurred in patients receiving BLINCYTO. Interrupt or discontinue BLINCYTO as recommended.
Contraindications

BLINCYTO is contraindicated in patients with a known hypersensitivity to blinatumomab or to any component of the product formulation.

Warnings and Precautions

Cytokine Release Syndrome (CRS): CRS, which may be life-threatening or fatal, occurred in patients receiving BLINCYTO. The median time to onset of CRS is 2 days after the start of infusion. Closely monitor patients for signs and symptoms of serious adverse events such as fever, headache, nausea, asthenia, hypotension, increased alanine aminotransferase (ALT), increased aspartate aminotransferase (AST), increased total bilirubin (TBILI), and disseminated intravascular coagulation (DIC). The manifestations of CRS after treatment with BLINCYTO overlap with those of infusion reactions, capillary leak syndrome (CLS), and hemophagocytic histiocytosis/macrophage activation syndrome (MAS). In clinical trials of BLINCYTO, CRS was reported in 15% of patients with relapsed or refractory ALL and in 7% of patients with MRD-positive ALL. Interrupt or discontinue BLINCYTO as outlined in the PI.
Neurological Toxicities: Approximately 65% of patients receiving BLINCYTO in clinical trials experienced neurological toxicities. The median time to the first event was within the first 2 weeks of BLINCYTO treatment and the majority of events resolved. The most common (≥ 10%) manifestations of neurological toxicity were headache and tremor. Severe, life‐threatening, or fatal neurological toxicities occurred in approximately 13% of patients, including encephalopathy, convulsions, speech disorders, disturbances in consciousness, confusion and disorientation, and coordination and balance disorders. Manifestations of neurological toxicity included cranial nerve disorders. Monitor patients for signs or symptoms and interrupt or discontinue BLINCYTO as outlined in the PI.
Infections: Approximately 25% of patients receiving BLINCYTO in clinical trials experienced serious infections such as sepsis, pneumonia, bacteremia, opportunistic infections, and catheter-site infections, some of which were life-threatening or fatal. Administer prophylactic antibiotics and employ surveillance testing as appropriate during treatment. Monitor patients for signs or symptoms of infection and treat appropriately, including interruption or discontinuation of BLINCYTO as needed.
Tumor Lysis Syndrome (TLS), which may be life-threatening or fatal, has been observed. Preventive measures, including pretreatment nontoxic cytoreduction and on-treatment hydration, should be used during BLINCYTO treatment. Monitor patients for signs and symptoms of TLS and interrupt or discontinue BLINCYTO as needed to manage these events.
Neutropenia and Febrile Neutropenia, including life-threatening cases, have been observed. Monitor appropriate laboratory parameters (including, but not limited to, white blood cell count and absolute neutrophil count) during BLINCYTO infusion and interrupt BLINCYTO if prolonged neutropenia occurs.
Effects on Ability to Drive and Use Machines: Due to the possibility of neurological events, including seizures, patients receiving BLINCYTO are at risk for loss of consciousness, and should be advised against driving and engaging in hazardous occupations or activities such as operating heavy or potentially dangerous machinery while BLINCYTO is being administered.
Elevated Liver Enzymes: Transient elevations in liver enzymes have been associated with BLINCYTO treatment with a median time to onset of 3 days. In patients receiving BLINCYTO, although the majority of these events were observed in the setting of CRS, some cases of elevated liver enzymes were observed outside the setting of CRS, with a median time to onset of 19 days. Grade 3 or greater elevations in liver enzymes occurred in approximately 7% of patients outside the setting of CRS and resulted in treatment discontinuation in less than 1% of patients. Monitor ALT, AST, gamma-glutamyl transferase (GGT), and TBILI prior to the start of and during BLINCYTO treatment. BLINCYTO treatment should be interrupted if transaminases rise to > 5 times the upper limit of normal (ULN) or if TBILI rises to > 3 times ULN.
Pancreatitis: Fatal pancreatitis has been reported in patients receiving BLINCYTO in combination with dexamethasone in clinical trials and the post-marketing setting. Evaluate patients who develop signs and symptoms of pancreatitis and interrupt or discontinue BLINCYTO and dexamethasone as needed.
Leukoencephalopathy: Although the clinical significance is unknown, cranial magnetic resonance imaging (MRI) changes showing leukoencephalopathy have been observed in patients receiving BLINCYTO, especially in patients previously treated with cranial irradiation and antileukemic chemotherapy.
Preparation and administration errors have occurred with BLINCYTO treatment. Follow instructions for preparation (including admixing) and administration in the PI strictly to minimize medication errors (including underdose and overdose).
Immunization: Vaccination with live virus vaccines is not recommended for at least 2 weeks prior to the start of BLINCYTO treatment, during treatment, and until immune recovery following last cycle of BLINCYTO.
Risk of Serious Adverse Reactions in Pediatric Patients due to Benzyl Alcohol Preservative: Serious and fatal adverse reactions including "gasping syndrome," which is characterized by central nervous system depression, metabolic acidosis, and gasping respirations, can occur in neonates and infants treated with benzyl alcohol-preserved drugs including BLINCYTO (with preservative). When prescribing BLINCYTO (with preservative) for pediatric patients, consider the combined daily metabolic load of benzyl alcohol from all sources including BLINCYTO (with preservative) and other drugs containing benzyl alcohol. The minimum amount of benzyl alcohol at which serious adverse reactions may occur is not known. Due to the addition of bacteriostatic saline, 7-day bags of BLINCYTO solution for infusion with preservative contain benzyl alcohol and are not recommended for use in any patients weighing < 22 kg.
Adverse Reactions

The most common adverse reactions (≥ 20%) in clinical trial experience of patients with MRD-positive B-cell precursor ALL (BLAST Study) treated with BLINCYTO were pyrexia, infusion related reactions, headache, infections (pathogen unspecified), tremor, and chills. Serious adverse reactions were reported in 61% of patients. The most common serious adverse reactions (≥2%) included pyrexia, tremor, encephalopathy, aphasia, lymphopenia, neutropenia, overdose, device related infection, seizure, and staphylococcal infection.
The most common adverse reactions (≥ 20%) in clinical trial experience of patients with Philadelphia chromosome-negative relapsed or refractory B-cell precursor ALL (TOWER Study) treated with BLINCYTO were infections (bacterial and pathogen unspecified), pyrexia, headache, infusion-related reactions, anemia, febrile neutropenia, thrombocytopenia, and neutropenia. Serious adverse reactions were reported in 62% of patients. The most common serious adverse reactions (≥ 2%) included febrile neutropenia, pyrexia, sepsis, pneumonia, overdose, septic shock, CRS, bacterial sepsis, device related infection, and bacteremia.
Adverse reactions that were observed more frequently (≥ 10%) in the pediatric population compared to the adult population were pyrexia (80% vs. 61%), hypertension (26% vs. 8%), anemia (41% vs. 24%), infusion-related reaction (49% vs. 34%), thrombocytopenia (34% vs. 21%), leukopenia (24% vs. 11%), and weight increased (17% vs. 6%).
In pediatric patients less than 2 years old (infants), the incidence of neurologic toxicities was not significantly different than for the other age groups, but its manifestations were different; the only event terms reported were agitation, headache, insomnia, somnolence, and irritability. Infants also had an increased incidence of hypokalemia (50%) compared to other pediatric age cohorts (15-20%) or adults (17%).
Dosage and Administration Guidelines

BLINCYTO is administered as a continuous intravenous infusion at a constant flow rate using an infusion pump which should be programmable, lockable, non-elastomeric, and have an alarm.
It is very important that the instructions for preparation (including admixing) and administration provided in the full Prescribing Information are strictly followed to minimize medication errors (including underdose and overdose).

Epizyme Announces the U.S. Food and Drug Administration Lifts Partial Clinical Hold on Tazemetostat Clinical Program

On September 24, 2018 Epizyme, Inc. (NASDAQ: EPZM), a clinical-stage company developing novel epigenetic therapies, reported the U.S. Food and Drug Administration (FDA) has lifted the partial clinical hold that had paused U.S.-based enrollment of new patients in its tazemetostat clinical trials (Press release, Epizyme, SEP 24, 2018, View Source [SID1234529538]). Epizyme is now in the process of reopening enrollment in all of its company-sponsored trials in the U.S., including the follicular lymphoma (FL) EZH2 activating mutation cohort of its Phase 2 non-Hodgkin lymphoma trial.

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Epizyme’s formal response to the FDA included a comprehensive assessment of the risk of secondary malignancies, including T-cell lymphoblastic lymphoma (T-LBL) potentially associated with tazemetostat, which took into account both published literature and the company’s clinical experience to date. This followed a report of a single case of T-LBL in its tazemetostat pediatric study. Epizyme provided a thorough assessment of efficacy and safety data across all of its trials in hematological malignancies and solid tumors, in both adults and children, and convened a panel of external scientific and medical experts who reviewed and validated the findings.

"The Epizyme team has worked diligently to provide a comprehensive response back to the FDA, and through constructive dialogue, we successfully resolved the partial clinical hold. This allows us to turn our full attention to our key priorities: preparing for our first NDA submission for tazemetostat in epithelioid sarcoma and defining our registration path in FL," said Robert Bazemore, president and chief executive officer of Epizyme. "We, along with our investigators and the global experts we consulted to support our complete response, continue to believe in the positive benefit/risk of tazemetostat as we move forward in our clinical development program. We remain steadfast in our commitment to bringing this potential therapeutic option to cancer patients in need of safe and effective new treatments."

Epizyme will now engage with regulators in France and Germany to resolve the partial clinical holds and resume enrollment in those countries. The company is also working closely with its study partners to reach a similar resolution for their respective trials in which tazemetostat is being studied in combination with other therapies.

Investor Conference Call Notice
Company management plans to host a conference call and webcast at 8:30 a.m. EDT today to discuss the resolution of the partial clinical hold. To participate, please dial (877) 844-6886 (domestic) or (970) 315-0315 (international) and refer to conference ID 3499753. A live webcast will be available in the investor section of the company’s website at www.epizyme.com. The webcast also will be archived on the website for 60 days.

About the Tazemetostat Clinical Trial Program
Tazemetostat, a potent, selective, orally available, first-in-class EZH2 inhibitor, is currently being studied as a monotherapy in ongoing Phase 2 programs in certain molecularly defined solid tumors, including epithelioid sarcoma and other INI1-negative tumors; follicular lymphoma (FL); and combination studies in diffuse large B-cell lymphoma (DLBCL) and non–small cell lung cancer (NSCLC).

Takeda receives positive opinion from CHMP recommending ALUNBRIG ® (brigatinib) for the treatment of non-small cell lung cancer positive ALK in patients previously treated with crizotinib

On September 22, 2018 Takeda Pharmaceutical Company Limited ( TSE: 4502 ) reported that the Committee for Medicinal Products for Human Use (CHMP) of the European Medicines Agency (EMA) adopted a positive opinion, recommending full approval of ALUNBRIG (brigatinib) as part of a monotherapy for the treatment of adult patients with anaplastic lymphoma (ALK +) kinase positive, advanced non-small cell lung cancer (NSCLC) and previously treated with crizotinib. ALUNBRIG is a tyrosine kinase inhibitor (TKI), designed to target and inhibit the ALK mutation in NSCLC (Press release, Takeda, SEP 22, 2018, View Source [SID1234529524]). Approximately 3% to 5% of patients with NSCLC worldwide have the ALK mutation. If the opinion of the CHMP is confirmed and the European Commission approves the ALUNBRIG, it will be the only ALK inhibitor available in the European Union as a dose of one tablet per day, which can be taken with or without food.

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The Randomized Phase 2 ALTA trial was designed to investigate the efficacy and safety of ALUNBRIG in patients with locally advanced or metastatic ALK + NSCLC who presented progress with crizotinib. Patients were randomized to receive one of two ALUNBRIG regimens: ALUNBRIG 90 mg once daily (n = 112) or 180 mg once daily with induction from 7 days to 90 mg once daily (n = 110) .

"ALK + NSCLC is a serious, life-threatening disease that affects approximately 40,000 people worldwide each year, with many patients progressing or failing to respond to first-line treatment," said Stefania Vallone, president, Lung Cancer Europe . "For Europeans with ALK + NSCLC, there remains a significant need not met by new and effective treatment options."

"Although ALK inhibitors have shown tremendous growth over this period of treatment over the past decade, another targeted therapy option available for ALK + NSCLC treatment has been awaited with anticipation and anticipation," said Enriqueta Felip, MD, PhD, chief of the Thoracic Oncology Unit, Department of Oncology at the Vall d’Hebron University Hospital in Barcelona. "With a median progression free survival of 16.7 months and an overall survival of 34.1 months, ALUNBRIG demonstrated impressive results, representing new progress for ALK + NSCLC treatment in this setting."

"The ALTA trial established ALUNBRIG as a possible second-line treatment option for ALK + NSCLC, demonstrating significant efficacy with a manageable safety profile," said Jesús Gómez-Navarro, MD, vice president, chief of Clinical Research and Development in Oncology in Takeda. "With 16.7 months of progression-free median survival, the longest of any ALK inhibitors to be reported in this setting, ALUNBRIG offers great potential for patients who progressed with crizotinib. Today’s positive opinion brings us closer to the ultimate goal of advancing the treatment paradigm for the considerable number of critically ill ALK + patients treated with crizotinib who live in Europe.

As part of this submission, the CHMP also analyzed data from the first interim review of the Phase 3 ALTA-1L trial, which fulfilled its main objective as evidence of support. In ALTA-1L, treatment with ALUNBRIG resulted in a statistically and clinically significant improvement in progression-free survival (PFS) versus crizotinib, as assessed by an independent blind review committee. The safety profile associated with ALUNBRIG has generally been consistent with previous studies and with labeling approved in the USA and Canada.

The CHMP’s positive opinion on ALUNBRIG will now be reviewed by the European Commission, which has the authority to approve medicines for use in the 28 member states of the European Union, as well as in Norway, Liechtenstein and Iceland.

About the ALTA test

The Phase 2 ALTA (acronym for A LK in L ung Cancer T rial of AP26113) in adults is a multicenter, open, randomized, continuous, multi-center trial involving 222 patients with locally advanced or metastatic ALK + NSCLC who progressed on crizotinib. Patients received ALUNBRIG at a dose of 90 mg once daily (n = 112) or 180 mg once daily with induction of seven days at 90 gm once daily (n = 110). The confirmed objective response rate (ORT), evaluated by the investigator according to RECIST v1.1, was the primary endpoint. Additional major endpoints included ORT, independent response committee (IRR), duration of response (DOR), progression-free survival (PFS), intracranial ORT, intracranial DOR, safety and tolerability.

The results of the ALTA trial demonstrated that, of the patients who received the 180 mg dosing regimen, 56% achieved an objective response rate as measured by the investigator and 56% by the CRI assessment. The median DOR was 13.8 months, as assessed by the investigator, and 15.7 months for the IRC evaluation. The median SLP was 15.6 months, as assessed by the investigator, and 16.7 months by the IRC evaluation. In addition, of the patients with measurable brain metastases at baseline (n = 18), 67% achieved intracranial ORR due to CRI; the median duration of intracranial response was 16.6 months by the CRI assessment. Median overall survival was 34.1 months, as assessed by the investigator.

The most frequent (≥ 25%) adverse reactions reported in ALUNBRIG-treated patients on the 180 mg dosing regimen were increased aspartate aminotransferase (AST), hyperglycemia, hyperinsulinemia, anemia, increased creatine phosphokinase (CPK), nausea, increased lipase, decreased lymphocyte count, increased alanine aminotransferase (ALT), diarrhea, increased amylase, fatigue, cough, headache, increased alkaline phosphatase, hypophosphataemia, increased abnormal activated partial thromboplastin time (APTT), rash, vomiting, dyspnoea, hypertension, decreased blood cell count, myalgia, and peripheral neuropathy.

About the ALTA-1L test

The Phase 3 ALTA-1L (acronym for A LK in L ung Cancer T rial of Brig A tinibe in 1 to Linha) in adults is an open, randomized, continuous, multicenter, global trial involving 275 patients with locally advanced or metastatic ALK + NSCLC who did not receive prior treatment with an ALK inhibitor. Patients received ALUNBRIG at the dose of 180 mg once daily with induction from 7 days to 90 mg once daily, or crizotinib at the dose of 250 mg twice daily. Progression-free survival (SLP) evaluated by the Independent Review Committee (IRC) was the primary endpoint. Secondary endpoints included objective response rate (ORT) according to RECIST v1.1, intracranial ORT, intracranial SLP, overall survival (OS), safety, and tolerability. A total of approximately 198 SLP events were planned in the final analysis of the primary endpoint to demonstrate a minimum of six months of improvement of SLP over crizotinib. The assay was developed with two pre-specified intermediate analyzes for the primary endpoint – one in approximately 50% of the planned PFS events and one in approximately 75% of the planned events of the SLP.

About CPNPC ALK +

Non-small cell lung cancer (NSCLC) is the most common form of lung cancer, accounting for about 85% of the estimated 1.8 million new lung cancer cases diagnosed each year worldwide, according to the Organization World Health Organization. Genetic studies indicate that chromosomal rearrangements in anaplastic lymphoma (ALK) kinase are fundamental motivators in a subset of patients with NSCLC. About 3% to 5% of patients with metastatic NSCLC have a rearrangement in the ALK gene.

Takeda is committed to continuing research and development at CPNPC to enhance the lives of the approximately 40,000 patients diagnosed with this severe and rare form of lung cancer worldwide each year.

About ALUNBRIG (brigatinib)

ALUNBRIG is a cancer-fighting drug discovered by ARIAD Pharmaceuticals, Inc., which was acquired by Takeda in February 2017. In April 2017, ALUNBRIG received accelerated approval from the US Food and Drug Administration (FDA) for patients with ALK + metastatic NSCLC, which have progressed or are intolerant to crizotinib. This indication was approved from accelerated approval, based on the tumor response rate and duration of response. Continuous approval for this indication may be conditional upon verification and description of clinical benefits in a confirmatory trial. In July 2018, Health Canada approved ALUNBRIG for the treatment of adult patients with metastatic ALK + NSCLC, who progressed or who were intolerant of an ALK inhibitor (crizotinib). ALUNBRIG’s approvals by the FDA and Health Canada were based primarily on the results of the ALTA Phase 2 trial (acronym forThe LK in U UNG Cancer T rial of the P26113).

ALUNBRIG has received the Breakthrough Therapy (FDA) designation of the FDA for the treatment of patients with critically ill ALK + NSCLC whose tumors are resistant to crizotinib and has been granted the Orphan Drug Designation by the FDA for the treatment of ALK + NSCLC, ROS1 + NSCLC and CPNPC EGFR +.

The brigatinib clinical development program further enhances Takeda’s continued commitment to the development of innovative therapies for people living with ALK + NSCLC worldwide and healthcare professionals who treat this disease. The comprehensive program includes the following clinical trials:

Phase 1/2 trial, which was designed to assess ALUNBRIG’s safety, tolerability, pharmacokinetics and antitumor activity
A phase 2 ALTA pivotal trial investigating the efficacy and safety of ALUNBRIG in two dosing regimens in patients with locally advanced or metastatic ALK + NSCLC who progressed with crizotinib
Phase 3 ALTA-1L trial, a randomized, global trial evaluating the efficacy and safety of ALUNBRIG in relation to crizotinib in patients with locally advanced or metastatic ALK + NSCLC who did not receive prior treatment with an ALK inhibitor
Single-phase, multicenter, phase 2 study in Japanese patients with ALK + NSCLC, focusing on patients who progressed in alectinib
A single-arm global phase 2 study evaluating ALUNBRIG in patients with advanced ALK + NSCLC who progressed in alectinib or ceritinib
A global randomized phase 3 trial comparing the efficacy and safety of ALUNBRIG versus alectinib in participants with ALK + NSCLC who progressed in crizotinib
For more information on brigatinib’s clinical trials, visit www.clinicaltrials.gov .

IMPORTANT SAFETY INFORMATION (USA)

WARNINGS AND PRECAUTIONS

Interstitial lung disease (IPD) / pneumonia: fatal life-threatening pulmonary adverse events consistent with interstitial lung disease (IPD) / pneumonia occurred with ALUNBRIG. In the ALTA trial, IPD / pneumonia occurred in 3.7% of patients in the 90 mg group (90 mg once daily) and 9.1% of patients in the 90 → 180 mg group (180 mg once daily). once daily with induction from 7 days to 90 mg once daily). Adverse reactions consistent with IPD / pneumonia occurred earlier (in 9 days after ALUNBRIG started, median onset was 2 days) in 6.4% of patients, with grade 3 to 4 reactions occurring in 2.7%. Monitor for new or worsening respiratory symptoms (eg, dyspnoea, cough, etc.), particularly during the first week of ALUNBRIG. Discontinue ALUNBRIG in any patient with new or worsening respiratory symptoms and immediately assess whether there is an IPD / pneumonia or other causes of respiratory symptoms (eg, pulmonary embolism, tumor progression, and infectious pneumonia). For Grade 1 or 2 PID / pneumonia, restart ALUNBRIG with dosage reduction after recovering the initial level or permanently discontinuing ALUNBRIG. Permanently discontinue ALUNBRIG for grade 3 or 4 PID / pneumonia or recurrence of grade 1 or 2 IPD / pneumonia. restart the ALUNBRIG with reduction of the dosage, after recovering the initial level or interrupt ALUNBRIG permanently. Permanently discontinue ALUNBRIG for grade 3 or 4 PID / pneumonia or recurrence of grade 1 or 2 IPD / pneumonia. restart the ALUNBRIG with reduction of the dosage, after recovering the initial level or interrupt ALUNBRIG permanently. Permanently discontinue ALUNBRIG for grade 3 or 4 PID / pneumonia or recurrence of grade 1 or 2 IPD / pneumonia.

Hypertension: in ALTA, hypertension was reported in 11% of patients in the 90 mg group, who received ALUNBRIG, and 21% of patients in the 90 → 180 mg group. In general, grade 3 hypertension occurred in 5.9% of the patients. Check blood pressure before ALUNBRIG treatment. Monitor blood pressure after 2 weeks and at least monthly thereafter during treatment with ALUNBRIG. Discontinue use of ALUNBRIG for grade 3 hypertension despite optimal antihypertensive therapy. After resolution or improvement to grade 1 severity, restart ALUNBRIG at a reduced dosage. Consider stopping ALUNBRIG treatment for grade 4 hypertension or recurrence of grade 3 hypertension.

Bradycardia: bradycardia may occur with ALUNBRIG. At ALTA, heart rates below 50 beats per minute (bpm) occurred in 5.7% of the patients in the 90 mg group and 7.6% of the patients in the 90 → 180 mg group. Grade 2 bradycardia occurred in 1 (0.9%) patient in the 90 mg group. Monitor your heart rate and blood pressure during ALUNBRIG treatment. Monitor patients more often if it is not possible to avoid the concomitant use of medication known to cause bradycardia. For symptomatic bradycardia, discontinue ALUNBRIG and review the concomitant use of medicines for those known to cause bradycardia. If a concomitant medication known to cause bradycardia is identified and discontinued or the dosage adjusted, restart ALUNBRIG at the same dosage, after symptomatic bradycardia has subsided; Otherwise, reduce ALUNBRIG dosage after reduction of symptomatic bradycardia. Stop ALUNBRIG for life-threatening bradycardia if the contribution of a concomitant medication is not identified.

Visual disturbance: in ALTA, adverse reactions that caused visual disturbance, including blurred vision, diplopia and reduced visual acuity, were recorded in 7.3% of patients treated with ALUNBRIG in the 90 mg group and 10% of the patients in the 90 → 180 group mg. Grade 3 macular edema and cataract occurred in one patient in each case in the 90 → 180 mg group. Advise patients to report any visual symptoms. Discontinue ALUNBRIG and obtain an ophthalmologic evaluation in patients with new or worsening grade 2 or greater severity of visual symptoms. After grade 2 or 3 visual impairment is restored for grade 1 or initial plateau pain, restart ALUNBRIG at a reduced dosage..

Elevated creatine phosphokinase (CPK): in ALTA, elevated creatine phosphokinase (CPK) occurred in 27% of patients receiving ALUNBRIG in the 90 mg group and 48% of patients in the 90 mg → 180 mg group. The incidence of grade 3 or 4 CPK elevation was 2.8% in the 90 mg group and 12% in the 90 → 180 mg group. The reduction in CPK elevation was observed in 1.8% of patients in the 90 mg group and 4.5% in the 90 → 180 mg group. Advise patients to report any unexplained pain, tenderness, or muscle weakness. Monitor CPK levels during treatment with ALUNBRIG. Discontinue ALUNBRIG if CPK grade 3 or 4 is elevated. After resolving or restoring to grade 1 or the initial plateau, restart ALUNBRIG at the same dosage or at a reduced dosage.

Elevation of pancreatic enzymes: in ALTA, increased amylase occurred in 27% of patients in the 90 mg group and 39% in the 90 → 180 mg group. Lipase elevations occurred in 21% of the patients in the 90 mg group and 45% of the patients in the 90 → 180 mg group. Elevation of grade 3 or 4 amylase occurred in 3.7% of patients in the 90 mg group and 2.7% in the 90 → 180 mg group. Elevation of grade 3 or 4 lipase occurred in 4.6% of patients in the 90 mg group and 5.5% in the 90 → 180 mg group. Monitor lipase and amylase during treatment with ALUNBRIG. Discontinue use of ALUNBRIG if there is elevation of pancreatic enzymes to grade 3 or 4. After resolution or recovery to grade 1 or baseline, restart ALUNBRIG at the same dosage or with a reduced dosage.

Hyperglycemia: in ALTA, 43% of patients receiving ALUNBRIG experienced new or worsening hyperglycemia. Grade 3 hyperglycemia, based on the laboratory evaluation of fasting serum glucose levels, occurred in 3.7% of the patients. Two of 20 (10%) patients with diabetes or glucose intolerance at the initial level requested the start of insulin use while receiving ALUNBRIG. Analyze fasting serum glucose before ALUNBRIG starts and then monitor periodically. Initiate or optimize antihyperglycemic medications as needed. If adequate control of hyperglycaemia can not be achieved with optimal medical management,

Embryo-fetal toxicity : Based on its mechanism of action and findings in animals, ALUNBRIG can cause fetal injury when administered to pregnant women. There are no clinical data on the use of ALUNBRIG in pregnant women. Advise the pregnant women about the potential risk to the fetus. Advise women with reproductive capacity to use effective non-hormonal contraceptives during treatment with ALUNBRIG and for at least 4 months after the final dose. Advise men with reproductive partners to use effective contraceptives during treatment and for at least 3 months after the last dose of ALUNBRIG .

ADVERSE REACTIONS

Serious adverse reactions occurred in 38% of the patients in the 90 mg group and 40% of the patients in the 90 → 180 mg group. The most common serious adverse reactions were pneumonia (5.5% overall, 3.7% in the 90 mg group, and 7.3% in the 90 → 180 mg group) and IPD / pneumonia (4.6% in total , 1.8% in the 90 mg group and 7.3% in the 90 → 180 mg group). Fatal adverse reactions occurred in 3.7% of the patients and consisted of pneumonia (2 patients), sudden death, dyspnea, respiratory arrest, pulmonary embolism, bacterial meningitis and urosepsis (1 patient each).

The most common adverse reactions (≥25%) in the 90 mg group were nausea (33%), fatigue (29%), headache (28%) and dyspnoea (27%), and in the group of 90 → 180 mg (40%), diarrhea (38%), fatigue (36%), cough (34%) and headache (27%).

DRUG INTERACTIONS

CYP3A Inhibitors : Avoid the concomitant use of ALUNBRIG with strong inhibitors of CYP3A. Avoid grapefruit juice or grapefruit as fruit, as it may also increase plasma concentrations of brigatinib. If concomitant use of a strong inhibitor of CYP3A is unavoidable, reduce ALUNBRIG dosage.

CYP3A Inducers: Avoid the concomitant use of ALUNBRIG with strong CYP3A inducers.

CYP3A Substrates: Co-administration of ALUNBRIG with substrates of CYP3A, including hormonal contraceptives, may result in decreased concentrations and loss of efficacy of CYP3A substrates.

USE ON SPECIFIC GROUPS

Pregnancy: ALUNBRIG can harm the fetus. Advise women with reproductive capacity about the potential risk to the fetus.

Lactation: There are no data regarding the secretion of brigatinib in human milk or its effect on the suckling baby or milk production. Due to potential adverse reactions in lactating infants, advise women not to breastfeed during treatment with ALUNBRIG.

Men and women with reproductive capacity:

Contraception : advise women with reproductive potential to use effective non-hormonal contraceptives during ALUNBRIG treatment and for at least 4 months after final dosing. Advise men living with women in reproductive capacity to use effective contraceptives during treatment with ALUNBRIG and for at least 3 months after the final dosing.

Infertility : ALUNBRIG can cause fertility reduction in men.

Pediatric use: The safety and efficacy of ALUNBRIG in pediatric patients has not been established.

Geriatric Use: ALUNBRIG clinical studies did not include sufficient patients aged 65 years or older to determine whether they responded differently from younger patients. Of the 222 patients in the ALTA, 19.4% were 65 to 74 years and 4.1% of 75 years or older. No clinically relevant difference in safety or efficacy was observed between patients 65 years of age and older and younger patients.

Hepatic or renal impairment: no dosage adjustment is recommended for patients with mild hepatic impairment or mild or moderate renal impairment. The safety of ALUNBRIG in patients with moderate or severe hepatic impairment or severe renal impairment has not been studied.