Horizon Discovery’s SMARTvector shRNA Technology Deployed in Celyad’s Successful IND Filing for Next-Generation CAR-T Cell Therapy, CYAD-02

On July 8, 2019 Horizon Discovery Group plc (LSE: HZD) ("Horizon"), a company driving the application of gene editing and gene modulation within the global life science market, reported that Celyad (Euronext Brussels and Paris, and Nasdaq: CYAD), a clinical-stage biopharmaceutical company focused on the development of CAR-T cell-based therapies, received FDA Acceptance of Investigational New Drug (IND) application for the autologous NKG2D based CAR-T cell therapy CYAD-02 that deploys Horizon’s optimized SMARTvector shRNA technology (Press release, Horizon Discovery, JUL 8, 2019, View Source [SID1234537405]). The Phase 1 trial will be the first CAR-T cell therapy to employ the SMARTvector platform. Horizon will receive an undisclosed milestone payment for the successful IND filing.

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Celyad has been investigating the use of shRNAs to support the clinical development of its CAR-T cell platform. The FDA approved IND application involves CYAD-02, a next generation CAR-T cell therapy in which shRNA is employed to suppress two genes. Celyad has pre-clinical data indicating that this improves in vivo engraftment and efficacy of CYAD-02.

A Phase 1 dose-escalation trial evaluating the safety and clinical activity of CYAD-02 is planned for early 2020 and will involve a preconditioning chemotherapy (CyFlu) in patients with relapse/refractory (r/r) acute myeloid leukemia (AML) or myelodysplastic syndromes (MDS).

Terry Pizzie, Chief Executive Officer, Horizon Discovery Group plc, commented: "We see great potential for shRNA technology in the optimization of next-generation cell therapies. The success of this IND filing is testament to the strength of our relationship with Celyad, and the powerful combination of Horizon’s SMARTvector shRNA platform with Celyad’s CAR-T expertise."

Filippo Petti, Chief Executive Officer, Celyad, said: "Over the past few years Celyad has made great strides in evaluating our NKG2D-based CAR-T therapy for the treatment of relapsed/refractory acute myeloid leukemia and myelodysplastic syndrome. The FDA approval for the CYAD-02 IND application will allow us to evaluate new therapies in this difficult to treat population and the inclusion of an optimized shRNA developed using Horizon’s SMARTvector technology represents the output of a strong collaboration. We look forward to a continued successful relationship."

Provectus Provides Update on GI Tumor Program for Investigational Cancer Drug PV-10

On July 8, 2019 Provectus (OTCQB: PVCT) reported an update on the Company’s gastrointestinal (GI) tumor clinical development program for its lead investigational cancer drug PV-10, which is administered percutaneously when targeting primary or metastatic tumors of the liver, such as hepatocellular carcinoma (HCC), metastatic neuroendocrine tumors (mNET), and metastatic uveal melanoma (mUM) (Press release, Provectus Biopharmaceuticals, JUL 8, 2019, View Source [SID1234537404]). Intratumoral injection of oncolytic immunotherapy PV-10 can yield immunogenic cell death in solid tumor cancers that results in tumor-specific reactivity in circulating T cells.1-5

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The Company’s oncology drug development strategy includes:

Further demonstrating PV-10’s activity in non-T cell and T cell inflamed and low and high tumor mutation burden tumor types,
Further demonstrating the T cell response generated by PV-10 treatment, and
Contrasting and comparing PV-10 treatment – activity and induced immune response – with that of checkpoint inhibitor (CI) and other drug classes in monotherapy and combination therapy settings.
Provectus believes this strategy should quicken the advancement of single-agent PV-10 along a pathway-to-approval in solid tumor cancer indications where there is high unmet need, limited activity from other therapies, and the opportunity to further display a functional immune response from PV-10 treatment, such as for mNET (NCT02693067).

Provectus also believes this approach should permit the Company to develop and advance a combination therapy involving a CI or other drug class along a pathway-to-approval in an indication where there is high unmet need, limited activity from standard of care (SOC) treatment, and the opportunity to display how PV-10 augments clinical response to existing or emerging SOCs, such as for mUM (i.e., combination therapy with anti-CTLA-4 and anti-PD-1 agents) (NCT00986661).

Update #1 (mNET): The Company plans to present further lesion-level (i.e., local) efficacy, preliminary patient-level (i.e., systemic) efficacy, further clinical and biomarker outcome, and preliminary T cell response data from single-agent PV-10 treatment of mNET at a regional annual scientific meeting in the third quarter of 2019 and a global GI-focused medical conference in the first quarter of 2020.

Update #2 (mNET): Investigators and researchers collaborating with Provectus plan to present the design of a Phase 2 mNET study combining PV-10 and an agent from a class of CI drugs at the abovementioned scientific meeting. The Company would seek partial or total sponsored-financial support for this trial.

Update #3 (mNET): The Company is exploring possible collaboration with another group of investigators to develop a Phase 2 mNET study design of PV-10 and an agent from another class of CI drugs. The Company would also seek partial or total sponsored-financial support for this trial.

Dominic Rodrigues, Vice Chair of Provectus’ Board of Directors stated, "We believe PV-10 monotherapy treatment of metastatic neuroendocrine tumors has yielded encouraging clinical data of single-agent drug activity that include both local and systemic disease control. Checkpoint inhibitor drugs have thus far shown limited or no monotherapy activity in this non-T cell inflamed and low tumor mutation burden tumor type. While we believe single-agent PV-10 can help fill this unmet medical need, we also think there is a meaningful rationale to combine a tumor-specific immunotherapy like PV-10 with a non-specific immunotherapy like a checkpoint inhibitor drug for this patient population."

Update #4 (mUM): The Company plans to present preliminary lesion- and patient-level efficacy data from PV-10 treatment of mUM at a global immuno-oncology-focused medical conference in the fourth quarter of 2019. mUM patients have received PV-10 monotherapy and PV-10 in combination with two CI drugs, anti-CTLA-4 and anti-PD-1 agents.

Mr. Rodrigues added, "Currently, there is no consensus on standard of care for the treatment of metastatic uveal melanoma. Treatment varies from medical center to medical center. In working with current and prospective principal investigators, we feel strongly that the combination of PV-10 with an anti-CTLA-4 agent and an anti-PD-1 agent, an approach that appears to leverage the unique clinical characteristics of each drug and drug candidate, may benefit this patient population who are in dire need of better therapeutic solutions."

Update #5 (HCC): Provectus has extended its long-standing scientific research relationship with the laboratory of Shari Pilon-Thomas, PhD at Moffitt Cancer Center in Tampa, Florida. A key aim of her new research initiative is to elucidate PV-10’s mechanism of action (MOA) in HCC, where the MOA hypothesis is the release of damage associated molecular patterns (DAMPs) from PV-10 treatment. Dr. Pilon-Thomas’ team have previously elucidated PV-10’s DAMP pathway in both a murine model of and clinical work on cutaneous melanoma.2

Ajay Maker, MD and his team at the University of Illinois at Chicago have previously elucidated a comparable DAMP pathway for PV-10 in colon cancer.3

PV-10, a lysosome-targeting treatment, may trigger several different pathways to achieve the death of cancer. Aru Narendran, MD, PhD and his team at the University of Calgary in Alberta, Canada have shown that PV-10 treatment leads to poly-ADP ribose polymerase (PARP) cleavage and tumor cell apoptosis in refractory neuroblastoma cell lines.5 Dr. Narendran’s team is currently pursuing the hypothesis of a third distinct PV-10-mediated cancer cell death pathway through an ongoing scientific research initiative with the Company.

Update #6 (HCC): As of the first quarter of 2019, an analysis of six patients who have received PV-10 monotherapy treatment for HCC displayed a median overall survival of 2.5 years (mean 3.1 years; range 0-8.3+ years).

Mr. Rodrigues concluded, "Dr. Pilon-Thomas and past and present team members at Moffitt Cancer Center have undertaken a significant amount of consequential translational research on PV-10 treatment, ranging from melanoma and breast cancer to monotherapy and combination therapy. This work has resulted in a critical understanding of the drug candidate’s underlying medical science and the publication of seminal journal articles. Recent failures by OPDIVO and KEYTRUDA to meet primary overall survival endpoints in their respective clinical trials for the treatment of hepatocellular carcinoma highlight the importance of our new mechanism of action study of PV-10 treatment for this disease, which may better help characterize a potential PV-10-checkpoint inhibitor drug combination solution."

About PV-10

PV-10 causes acute oncolytic destruction of injected tumors, releasing DAMPs and tumor antigens that initiate an immunologic cascade where local response by the innate immune system facilitates systemic anti-tumor immunity by the adaptive immune system. The DAMP release-mediated adaptive immune response activates lymphocytes, including CD8+ T cells, CD4+ T cells, and NKT cells, based on clinical and preclinical experience in multiple tumor types. T cell function can be further augmented by combining PV-10 with CI drugs.

PV-10 is undergoing clinical study for adult solid tumor cancers like melanoma and cancers of the liver (including metastatic neuroendocrine tumors and metastatic uveal melanoma) and preclinical study for pediatric cancers like neuroblastoma5, Ewing sarcoma, rhabdomyosarcoma, and osteosarcoma.

Orphan drug designation status has been granted to PV-10 by the U.S. Food and Drug Administration for the treatments of metastatic melanoma in 2006, hepatocellular carcinoma in 2011, neuroblastoma in 2018, and ocular melanoma (including uveal melanoma) in 2019.

PV-10 is an injectable formulation of rose bengal disodium (RB) (4,5,6,7-tetrachloro-2’,4’,5’,7’-tetraiodofluorescein disodium salt), which is a small molecule halogenated xanthene and PV-10’s active pharmaceutical ingredient. PV-10 drug product is a bright rose red solution containing 10% w/v RB in 0.9% saline for injection, which is supplied in single-use glass vials containing 5 mL (to deliver) of solution and administered without dilution to solid tumors via intratumoral injection.

Provectus’ intellectual property includes a family of US and international patents that protect the process by which pharmaceutical grade RB and related xanthenes are produced, reducing the formation of previously unknown transhalogenated impurities that exist in commercial grade RB in uncontrolled amounts. The requirement to control these impurities is in accordance with International Conference on Harmonisation (ICH) guidelines for the manufacturing of an injectable pharmaceutical. US patent numbers are 8,530,675, 9,273,022, and 9,422,260, with expirations ranging from 2030 to 2031.

Arrowhead Pharmaceuticals to Participate in Roth RNA Revolution Conference

On July 8, 2019 Arrowhead Pharmaceuticals Inc. (NASDAQ: ARWR) reported that Bruce Given, M.D., Arrowhead’s chief operating officer and head of R&D, and Vincent Anzalone, CFA, Arrowhead’s vice president of investor relations, will participate in panel discussions at the Roth RNA Revolution Conference on July 17, 2019 (Press release, Arrowhead Pharmaceuticals, JUL 8, 2019, View Source [SID1234537402]).

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Y-mAbs Announces Successful Pre-BLA Meeting with FDA for Naxitamab

On July 8, 2019 -mAbs Therapeutics, Inc. (the "Company" or "Y-mAbs") (Nasdaq: YMAB) a late-stage clinical biopharmaceutical company focused on the development and commercialization of novel, antibody-based therapeutic products for the treatment of cancer, reported that it has completed a successful Type B Pre-Biologics License Application ("Pre-BLA") meeting with the U.S. Food and Drug Administration ("FDA") regarding a potential pathway for FDA approval of naxitamab for the treatment of patients with relapsed/refractory high-risk neuroblastoma (Press release, Y-mAbs Therapeutics, JUL 8, 2019, View Source [SID1234537400]).

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At the meeting, the Company reached alignment with the FDA on an Accelerated Approval Pathway for naxitamab along with a rolling BLA submission. The Company expects to submit the Clinical/Safety portion and the non-Clinical portion of the BLA in November 2019. For the CMC portion, the Company believes it will have sufficient data from the process performance qualification ("PPQ") batches to complete the CMC portion in early 2020. However, Y-mAbs is still investigating possibilities for accelerating the submission of the CMC portion, and hope to comply with the FDA requirements at an earlier time.

Under naxitamab’s breakthrough therapy designation ("BTD"), the compound qualifies for a Rolling BLA, which enables individual modules of the application to be submitted by the Company and reviewed by the FDA on a rolling basis, rather than waiting for all sections to be completed before submission. The rolling application process will provide the Company with the opportunity for ongoing communications with the FDA, and, during this rolling process, the Company anticipates that it will be able to address any substantial matters raised by the FDA.

Based on the previously announced efficacy data from Study 12-230 in relapsed/refractory high-risk neuroblastoma patients at Memorial Sloan Kettering Cancer Center ("MSK"), the FDA determined that efficacy data from all 37 patients of the Company’s multicenter Study 201 would not be required for the BLA filing. The FDA advised the Company that the available data for the first group of patients treated outside MSK in Study 201 would be sufficient for the BLA filing. The first group consists of 24 patients, of which 11 were evaluable prior to the pre-BLA meeting and showed an overall response rate ("ORR") of 73%, including 55% complete responses ("CR"), as assessed by the investigators. The Company intends to announce the complete dataset for Study 201 once the data becomes available.

"The positive outcome of the Pre-BLA meeting will be consequential for high-risk neuroblastoma patients waiting to get access to this new outpatient treatment with encouraging data," stated Thomas Gad, Founder, Chairman, President and Head of Business Development and Strategy.

Dr. Claus Moller, Chief Executive Officer, continued, "We are pleased to see that the clinical data previously generated at MSK was able to be replicated at other sites. We believe that an ORR of 73% may place naxitamab in a strong position in the market for the treatment of high-risk neuroblastoma."

Bausch Health Companies Inc. Will Release Second-Quarter 2019 Financial Results On August 6

On July 8, 2019 Bausch Health Companies Inc. (NYSE/TSX: BHC) ("Bausch Health") reported that it will release its second-quarter 2019 financial results on Tuesday, Aug. 6, 2019 (Press release, Valeant, JUL 8, 2019, View Source [SID1234537399]). Bausch Health will host a conference call and live web cast at 8:00 a.m. EDT to discuss the results and provide a business update. All materials will be made available on the Investor Relations section of the Bausch Health website prior to the start of the call.

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Conference Call Details

Date:

Tuesday, Aug. 6, 2019

Time:

8:00 a.m. EDT

Webcast:

View Source

Participant Event Dial-in:

+1 (888) 317-6003 (United States)

+1 (412) 317-6061 (International)

+1 (866) 284-3684 (Canada)

Participant Passcode:

2275809

Replay Dial-in:

+1 (877) 344-7529 (United States)

+1 (412) 317-0088 (International)

+1 (855) 669-9658 (Canada)

Replay Passcode:

10132759 (replay available until Aug. 13, 2019)