Den 20 oktober, 2017 rapporterade Xspray Pharma att de har fått godkännande för ett sökt patent i USA. Patentet omfattar komposition avseende produktkandidaten HyNap-Dasa (Press release, Xspray, OCT 20, 2017, View Source [SID1234523284]). Det är Xsprays första produktpatent som godkänns på huvudmarknaden i USA. Bolaget har tidigare offentliggjort ett patentgodkännande i Japan och har pågående ansökningsärenden för motsvarande patent i USA, Japan och Europa..

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"Att vi nu får patent beviljat på vår viktigaste marknad bekräftar vårt innovativa arbete samt förbättrar vår kommande förhandlingsposition med tilltänkta partners." säger Per Andersson, vd för Xspray Pharma.

Xspray Pharma har erhållit godkännande ("notice of allowance") för ett patent i USA avseende produktkandidaten HyNap-Dasa som är tänkt för behandling av vissa cancerformer. Det är det första produktrelaterade patentet som beviljas för bolagets produktkandidat på den viktigaste marknaden, USA. Beskedet kommer i enlighet med bolagets plan att söka och erhålla patent för komposition och metod för samtliga tre produktkandidater under utveckling på de tre viktigaste marknaderna, USA, Europa och Japan.

"Vi satsar primärt på att lansera våra produktkandidater på den amerikanska marknaden. En väl fungerande patentstrategi fyller en viktig funktion och det här godkännandet visar att vi har en sådan", kommenterar Xsprays vd Per Andersson.

Xspray Pharmas aktier introducerades den 28 september på Nasdaq First North, efter en lyckosamt genomförd nyemission som tillförde bolaget 132 miljoner kronor före emissionskostnader. Planen är nu att använda kapitalet för att utveckla tre produktkandidater och blivande cancerläkemedel baserade på bolagets egenutvecklade teknologi, samt att introducera de första produkterna på den amerikanska marknaden under perioden 2020-2023.

ATOR-1015 (previously designated ADC-1015) is a bispecific immune activating antibody, developed for tumor-directed immunotherapy. The drug candidate binds to two different immunomodulating target proteins: the inhibitory checkpoint receptor CTLA-4, and the co-stimulatory receptor OX40. The OX40 binding part originates from ALLIGATOR-GOLD, and the CTLA-4 binding part was generated by FIND optimization of CD86, which is a natural binder to CTLA-4.

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ATOR-1015 is capable of binding individual T-cells simultaneously, thereby bringing those cells in close proximity, which may support the immune activating effect. It reduces the number of regulatory T-cells and activates effector T-cells. A strong immune activation is expected to be achieved primarily in environments where both target molecules are expressed at high levels, such as inside a tumor. Taken together, this results in an effective immune activation as well as localization of the effect to the tumor environment, the latter being expected to minimize immune-related side effects. The objective of ATOR-1015 is to be the first CTLA-4 and OX40-binding bispecific antibody to achieve a strong anti-tumor effect, either as a monotherapy or in combination with currently established immunotherapies such as PD-1 and PD-L1 blockers. ATOR-1015 is expected to be suitable for treating a large number of different forms of cancer.

Based on the promising results from concept validation and initial preclinical studies, cell line development, aimed at subsequent large-scale production for clinical trials, was initiated in January 2016. The program is currently in the second phase of production, process development, and is planned to be ready for clinical trials during 2018.

On October 19, 2017 Heidelberg Pharma – formerly WILEX AG – (ISIN DE000A11QVV0 / WKN A11QVV / Symbol WL6) reported that its relocation from Munich to Ladenburg and its name change from WILEX AG to Heidelberg Pharma AG have been successfully completed with its entry in the Mannheim commercial register on 18 October 2017 (Press release, Heidelberg Pharma, OCT 19, 2017, View Source [SID1234526972]). The Company’s shares will continue to be listed on the Regulated Market of the Frankfurt Stock Exchange’s Prime Standard under their old ISIN, German securities identification code (WKN) and symbol. Its subsidiary Heidelberg Pharma GmbH is now doing business as Heidelberg Pharma Research GmbH. The Annual General Meeting on 20 July 2017 adopted a resolution to change the name of the Company and relocate its headquarters from Munich to Ladenburg.

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"Our Company’s core business has been driven by the research and development activities of our subsidiary Heidelberg Pharma GmbH for some time. The renaming and relocation of the Company are part of our strategic realignment and the refinement of our business model," commented Dr. Jan Schmidt-Brand, CEO and CFO of Heidelberg Pharma AG. "In keeping with these changes, the Heidelberg Pharma companies now have a uniform, updated corporate identity, including a new corporate website."

Heidelberg Pharma is working to enhance its value by developing and licensing the proprietary ATAC technology platform, entering into project partnerships and building a proprietary ATAC portfolio. Clinical development of the first proprietary product candidate HDP-101 in multiple myeloma is expected to begin at the end of 2018.

The Company’s new website can be found at www.heidelberg-pharma.com.

On October 19, 2017 OncoSec Medical Incorporated ("OncoSec" or "Company") (NASDAQ:ONCS), a company developing DNA-based intratumoral cancer immunotherapies, reported updated Phase 2 clinical and immune monitoring data from patients treated with its investigational therapy, ImmunoPulse IL-12 as a monotherapy versus the combination of ImmunoPulse IL-12 and the approved anti-PD-1 therapy pembrolizumab (Press release, OncoSec Medical, OCT 19, 2017, View Source [SID1234521022]). These data were presented in an oral presentation at the 2017 9th World Congress of Melanoma – A Joint Meeting with the Society for Melanoma Research, and continue to support the rationale for the Company’s recently initiated global, open-label, Phase 2b registration directed trial, PISCES/KEYNOTE-695.

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The Phase 2 OMS-I100 monotherapy and Phase 2 OMS-I102 combination with pembrolizumab studies included 51 and 22* patients, respectively, with metastatic melanoma. The combination study patients were selected based on their baseline biomarker data, which predicted that patients would not respond to anti-PD-1 therapy. Monotherapy patients were treated with ImmunoPulse IL-12 alone and patients in the combination study also received pembrolizumab every 3 weeks per protocol. Fewer than 10% of patients in both studies reported treatment related serious adverse events (9.8% in the monotherapy and 8.7% in the combination studies). Data also demonstrate that ImmunoPulse IL-12 can trigger key immunologic events driving a cellular response leading to an inflamed tumor with increased TIL frequency whether as a monotherapy or combined with pembrolizumab, converting "cold" tumors to "hot", which were further enhanced with the addition of an anti-PD1 antibody.

*Includes one CR with non-evaluable RECIST lesions
Key Findings

OMS-I102 Combination with Pembrolizumab

50% (11/22) BORR observed at 24 weeks (42.9% [9/21] achieved RECIST v1.1 BORR).

41% (9/22) complete responders (CR), 9% (2/22) partial responders (PR), and 9% (2/22) stable disease (SD) for a total disease control rate of 59% (38.1% [8/21] achieved RECIST v1.1 durable CR).

Data demonstrate that the combination of ImmunoPulse IL-12 and pembrolizumab prime a coordinated innate and adaptive immune response, suggesting a synergistic relationship with anti-PD-1.

OMS-I100 Monotherapy

25-34.6% best overall response rate (BORR) by a modified "skin" RECIST.

Favorable safety profile (no life threatening or grade 4 AE).

In patients (n=26) treated with ImmunoPulse IL-12 on a 90-day cycle, there were 19.2% (5/26) complete responders (CR), 15.4% (4/26) partial responders (PR), and 34.6% (9/26) stable disease (SD) for a total disease control rate of 69.2%.

In the protocol addendum where patients (n=20) were treated with ImmunoPulse IL-12 on a 6-week cycle, there were 0 complete responders (CR), 25% (5/20) partial responders (PR), and 40% (8/20) stable disease (SD) for a total disease control rate of 65%.

"We are encouraged by the data from these analyses, which continue to show that ImmunoPulse IL-12 can prime the immune system to help improve patient response to anti-PD-1," said Dr. Alain Algazi, Lead Trial Investigator, Associate Professor, Department of Medicine (Hematology/Oncology), at the University of California San Francisco (UCSF) Helen Diller Family Comprehensive Cancer Center. "The complete response rates observed in the Phase 2 study assessing the combination of ImmunoPulse IL-12 and pembrolizumab in the predicted anti-PD-1 non-responder patient population provide compelling early evidence that the combination could lead to a clinically meaningful impact on patient outcomes."

"Collectively, these study findings reinforce the combination of ImmunoPulse IL-12 and pembrolizumab to address a significant unmet medical need in melanoma patients who are unlikely to respond to anti-PD-1 therapies," said Punit Dhillon, CEO and President of OncoSec. "We look forward to presenting additional data from our ongoing Phase 2 combination study at the upcoming 2017 Society for Immunotherapy of Cancer (SITC) (Free SITC Whitepaper) Annual Meeting, in addition to our global, open-label, registration directed phase 2b clinical trial, PISCES/KEYNOTE-695, which we anticipate reporting initial data in mid-2018."

The full-text abstract is available and can be viewed on the World Melanoma Congress – Joint Meeting with the Society of Melanoma Research website at View Source The presentation is available in the Publications section of OncoSec’s website.

About PISCES (Anti-PD-1 IL-12 Stage III/IV Combination Electroporation Study)

PISCES is a global, multicenter phase 2b, open-label trial of intratumoral plasma encoded IL-12 (tavokinogene telseplasmid or "tavo") delivered by electroporation in combination with intravenous pembrolizumab in patients with stage III/IV melanoma who have progressed or are progressing on either pembrolizumab or nivolumab treatment. The Simon 2-stage study of intratumoral tavo plus electroporation in combination with pembrolizumab will enroll approximately 48 patients with histological diagnosis of melanoma with progressive locally advanced or metastatic disease defined as Stage III or Stage IV. The primary endpoint will be the Best Overall Response Rate (BORR).

ATOR-1017 is an agonistic IgG4 antibody that activates the co-stimulatory receptor 4-1BB (CD137, TNFRSF9) (Company Pipeline, Alligator Bioscience, OCT 19, 2017, View Source [SID1234521032]). It was developed from Alligator´s human antibody library, ALLIGATOR-GOLD. In the development of ATOR-1017, Alligator has used their extensive expertise in the TNF receptor superfamily to develop a compound with a clear differentiation compared to other 4-1BB antibodies in development. Thus, ATOR-1017 has a unique target binding profile compared to the two 4-1BB antibodies currently in clinical development. In addition, its agonistic function is dependent on cross-linking by Fcγ receptors expressed by immune cells. The properties of the antibody directs the immune activation to the tumor area where 4-1BB as well as Fcγ receptors are highly expressed, resulting in a favorable safety-efficacy profile. ATOR-1017 therefore has the potential to be a best-in-class 4-1BB antibody in terms of risk-benefit profile.

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