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Entera Bio to Conduct Conference Call on June 30 to Discuss Phase 2 Results for EB613 Positioned to be the First Oral Bone-Building Agent for the Treatment of Osteoporosis

BOSTON and JERUSALEM, June 28, 2021 (GLOBE NEWSWIRE) — Entera Bio Ltd. (NASDAQ: ENTX), a leader in the development of orally delivered large molecule therapeutics, today announced it will conduct a conference call to discuss results from its successfully completed Phase 2 clinical trial of EB613 for the treatment of osteoporosis. EB613 is an oral formulation of human parathyroid hormone (1–34), or PTH, and is positioned to be the first oral bone building (anabolic) product to treat osteoporosis patients.

Attendees on the call will include osteoporosis expert and Principal Investigator of the Phase 2 study Dr. Liana Tripto–Shkolnik, Sheba Medical Center, Institute of Endocrinology. Dr. Tripto–Shkolnik will provide context on the results of the study and the benefits of an oral drug to treat osteoporosis. Also on the call will be Entera CEO, Spiros Jamas; President of R&D, Phillip Schwartz; Chief Medical Officer, Art Santora; and CFO, Ramesh Ratan.

The conference call will take place on Wednesday, June 30, 2021 from 12–1pm EDT and will include a question–and–answer session. To participate on the live call, please dial (844) 467–6041 (US) or (409) 217–8787 (international) and provide the conference ID "5298499" five to ten minutes before the start of the call.

To access a live audio webcast of the presentation on the "Investor Relations" page of Entera's website, please click here. A replay of the webcast will be archived on Entera's website for approximately 45 days following the presentation.

About Entera Bio

Entera is a leader in the development of orally delivered large molecule therapeutics for use in areas with significant unmet medical need where adoption of injectable therapies is limited due to cost, convenience and compliance challenges for patients. The Company's proprietary, oral drug delivery technology is designed to address the technical challenges of poor absorption, high variability, and the inability to deliver large molecules to the targeted location in the body through the use of a synthetic absorption enhancer to facilitate the absorption of large molecules, and protease inhibitors to prevent enzymatic degradation and support delivery to targeted tissues. The Company's most advanced product candidates, EB613 for the treatment of osteoporosis and EB612 for the treatment of hypoparathyroidism are in Phase 2 clinical development. Entera also licenses its technology to biopharmaceutical companies for use with their proprietary compounds and, to date, has established a collaboration with Amgen Inc. For more information on Entera Bio, visit www.enterabio.com.

Forward Looking Statements

Various statements in this release are "forward–looking statements" under the securities laws. Words such as, but not limited to, "anticipate," "believe," "can," "could," "expect," "estimate," "design," "goal," "intend," "may," "might," "objective," "plan," "predict," "project," "target," "likely," "should," "will," and "would," or the negative of these terms and similar expressions or words, identify forward–looking statements. Forward–looking statements are based upon current expectations that involve risks, changes in circumstances, assumptions and uncertainties. Forward–looking statements should not be read as a guarantee of future performance or results and may not be accurate indications of when such performance or results will be achieved.

Important factors that could cause actual results to differ materially from those reflected in Entera's forward–looking statements include, among others: changes in our interpretation of the complete3–month biomarker data from the ongoing Phase 2 clinical trial of EB613, the timing of data readouts from the ongoing Phase 2 clinical trial of EB613, the full results of the Phase 2 clinical trial of EB613, which is still ongoing and our analysis of those full results, the FDA's interpretation and review of our results from and analysis of our Phase 2 trial of EB613, unexpected changes in our ongoing and planned preclinical development and clinical trials, the timing of and our ability to make regulatory filings and obtain and maintain regulatory approvals for our product candidates; a possible suspension of the Phase 2 clinical trial of EB613 for clinical or data–related reasons; the impact of COVID–19 on Entera's business operations including the ability to collect the necessary data from the Phase 2 trial of EB613; the potential disruption and delay of manufacturing supply chains, loss of available workforce resources, either by Entera or its collaboration and laboratory partners, due to travel restrictions, lay–offs or forced closures or repurposing of hospital facilities; impacts to research and development or clinical activities that Entera is contractually obligated to provide, such as those pursuant to Entera's agreement with Amgen; overall regulatory timelines, if the FDA or other authorities are closed for prolonged periods, choose to allocate resources to review of COVID–19 related drugs or believe that the amount of Phase 2 clinical data collected are insufficient to initiate a Phase 3 trial, or a meaningful deterioration of the current political, legal and regulatory situation in Israel or the United States; the availability, quality and timing of the data from the Phase 2 clinical trial of EB613 in osteoporosis patients; the ability to find a dose that demonstrates the comparability of EB613 to FORTEO in the ongoing Phase 2 clinical trial of EB613; the size and growth of the potential market for EB613 and Entera's other product candidates including any possible expansion of the market if an orally delivered option is available in addition to an injectable formulation; the scope, progress and costs of developing Entera's product candidates including EB612 and GLP–2; Entera's reliance on third parties to conduct its clinical trials; Entera's expectations regarding licensing, business transactions and strategic collaborations; Entera's operation as a development stage company with limited operating history; Entera's ability to continue as a going concern absent access to sources of liquidity; Entera's expectations regarding its expenses, revenue, cash resources, liquidity and financial condition; Entera's ability to raise additional capital; Entera's interpretation of FDA feedback and guidance and how such guidance may impact its clinical development plans; Entera's ability to obtain and maintain regulatory approval for any of its product candidates; Entera's ability to comply with Nasdaq's minimum listing standards and other matters related to compliance with the requirements of being a public company in the United States; Entera's intellectual property position and its ability to protect its intellectual property; and other factors that are described in the "Special Note Regarding Forward–Looking Statements," "Risk Factors" and "Management's Discussion and Analysis of Financial Condition and Results of Operations" sections of Entera's annual and current filings which are on file with the SEC and available free of charge on the SEC's website at http://www.sec.gov. Additional factors may be set forth in those sections of Entera's Annual Report on Form 20–F for the year ended December 31, 2020, filed with the SEC in the first quarter of 2021. In addition to the risks described above and in Entera's annual report on Form 20–F and current reports on Form 6–K and other filings with the SEC, other unknown or unpredictable factors also could affect Entera's results. There can be no assurance that the actual results or developments anticipated by Entera will be realized or, even if substantially realized, that they will have the expected consequences to, or effects on, Entera. Therefore, no assurance can be given that the outcomes stated in such forward–looking statements and estimates will be achieved.

All written and verbal forward–looking statements attributable to Entera or any person acting on its behalf are expressly qualified in their entirety by the cautionary statements contained or referred to herein. Entera cautions investors not to rely too heavily on the forward–looking statements Entera makes or that are made on its behalf. The information in this release is provided only as of the date of this release, and Entera undertakes no obligation, and specifically declines any obligation, to update or revise publicly any forward–looking statements, whether as a result of new information, future events or otherwise.


GLOBENEWSWIRE (Distribution ID 8271666)

The Globe and Mail’s Sophi.io Wins Digiday Media Award

TORONTO, June 28, 2021 (GLOBE NEWSWIRE) — Sophi.io, The Globe and Mail's artificial intelligence–based automation and prediction engine, won the 2021 Digiday Media Award for Best Publisher Platform, which recognizes technology that is most successful in helping publishers achieve their goals.

"AI is an essential technology for helping publishers add authentic value to stories "" extending their measure of success beyond page views and virality. For example, Sophi is able to provide data on how much each article on The Globe and Mail contributes to subscriber retention, acquisition, registration potential and advertising dollars. Additionally, to effectively deploy machine learning, around 10% of The Globe and Mail's workforce is now data scientists and engineers, hired to develop Sophi and grow the strategy even further," Digiday said.

The awards honour companies, technologies and campaigns that have stood out throughout the media over the past year. "This year, the competition was fierce and the programs robust. Innovation and big ideas expanded the playing field for many of the winners, even in a year when quarantines limited where and how people could work "" and play," according to Digiday.

Phillip Crawley, Publisher and CEO of The Globe and Mail, commented: "It's an honour to be chosen as the winner of Digiday's Media Award for Best Publisher Platform. We aren't often up against companies in both the media and marketing industries but our investments in Sophi have been driven by the understanding that our technology can directly drive performance and economic growth for companies across a large range of industries."

The other finalists in the Best Publisher Platform category were: Piano, Connatix, Insticator, Duration Media and Adapex LLC.

Sophi is an artificial–intelligence system that helps publishers identify and leverage their most valuable content. It has powerful predictive capabilities "" using natural language processing, Sophi Dynamic Paywall is a fully dynamic, real–time, personalized paywall engine that analyses both content and user behaviour to determine when to ask a reader for money or an email address, and when to leave them alone.

Sophi Site Automation autonomously curates digital content to find and promote the most valuable articles. It places 99% of the content on all of The Globe and Mail's digital pages, including its homepage and section pages. Sophi has been so successful that it is now being used for print laydown as well. Sophi is available to publishers across the globe to enable their content producers to focus on creating the best content possible.

Earlier this month, Sophi won the 2021 International News Media Association (INMA) Global Media Awards for Best in Show in North America and Best Use of Data to Automate or Personalize. Sophi has also won the Online Journalism Award (OJA) for Technical Innovation in the Service of Digital Journalism, handed out by the Online News Association (ONA), and both the World Digital Media Award and the North American Digital Media Award awarded by The World Association of News Publishers (WAN–IFRA) in the category of Best Digital News Start–up.

About Sophi.io

Sophi.io (https://www.sophi.io) is a suite of AI–powered optimization and prediction tools that helps content publishers make important strategic and tactical decisions. Sophi solutions range from Sophi Site Automation and Sophi for Paywalls to Sophi Analytics, a decision–support system for content publishers. Sophi is designed to improve the metrics that matter most to any business, such as subscriber retention and acquisition, engagement, recency, frequency and volume.


GLOBENEWSWIRE (Distribution ID 8271636)

Sol-Gel Announces Pipeline Update and Future Development Plans

  • Sol–Gel investigational SGT–510 was found to be more effective than roflumilast cream, 0.3%, in a human xenograft psoriasis animal model

  • Sol–Gel is developing tapinarof cream, 1%, aiming to offer product formulation innovations and increased affordability for patients compared to the brand expected to be launched
  • Our proof–of–concept study for SGT–210 (erlotinib gel) in palmoplantar keratoderma patients has been completed and indicated a possible modest improvement

  • Sol–Gel to host Conference Call today at 8:00 am U.S. EDT to discuss the data and provide a corporate update

NESS ZIONA, Israel, June 28, 2021 (GLOBE NEWSWIRE) — Sol–Gel Technologies, Ltd. (NASDAQ: SLGL), a clinical–stage dermatology company focused on identifying, developing and commercializing branded and generic topical drug products for the treatment of skin diseases, today announced positive pre–clinical data for SGT–510, its investigational topical roflumilast drug candidate and provided a corporate update.

The study was conducted at the Skin Research Laboratory, Rappaport Faculty of Medicine, Technion Institute of Technology, Haifa, Israel, under the supervision of Professor Amos Gilhar, M.D. Professor Gilhar has pioneered a human psoriasis xenograft mouse model, consisting of immunodeficient mice transplanted with healthy human skin, and used it to validate a number of approved topical and systemic dermatology products, including those sold by large pharmaceutical companies. For the study, the human xenograft animal model was induced with psoriasis by injection of activated allogeneic IL2–enriched peripheral blood mononuclear cells isolated from psoriatic patients. The mice were then treated with several topical agents and assessed for recovery after each intervention.

“Our model has been proven to predict efficacy for novel approaches in the treatment of psoriasis, providing very valuable information to the companies leveraging this assay," commented Professor Gilhar.

All tested articles were applied for 14 days either once or twice daily:

  • Nine (9) out of 10 animals fully recovered following a twice–daily application of dexamethasone (the positive control);
  • None (0) out of 10 recovered following a once–daily application of vehicle cream (the negative control);
  • Three (3) out of 10 animals recovered following a once–daily application of roflumilast cream, 0.3% that was formulated by Sol–Gel according to conventional methods of cream formulation;
  • Six (6) out of 10 animals fully recovered following once–daily application of SGT–510.

Based on these results, Sol–Gel filed a provisional patent application for its novel and non–obvious formulation of SGT–510. By the end of 2022, the Company expects to have head–to–head data against a formulation of roflumilast cream, 0.3% and expects to initiate Phase 2 work thereafter.

Mr. Mori Arkin, Executive Chairman of the Board of Sol–Gel, commented, "While this small study does not represent a formal statistical analysis, we are very pleased that these early–stage results, demonstrating 60% recovery after a once–daily application of SGT–510 in the human psoriasis xenograft mouse model, supported our predefined hypothesis and confirmed our expectations about formulation superiority using our approach. Given our expertise in formulation science and topical drug delivery, we believe that we have an advantage due to the patentability of SGT–510. It is our belief that if these results are corroborated by clinical studies, a patent, if granted, will provide us not only freedom to operate, but more importantly, intellectual property protection against generic entrants until expiry of our patent in 2040."

Mr. Arkin continued, "Due to the safety–limiting features of steroids, the prospect of an effective alternative to steroid medicine for the treatment of psoriasis, such as SGT–510, is significant and would fill a critical unmet need for these patients. Sol–Gel intends to develop SGT–510 in accordance with the 505(b)(2) regulatory pathway by only referencing the oral roflumilast brand DALIRESP . The rationale for this carefully planned regulatory strategy is to create a clear path to market, with no litigation requirement. We expect that all Orange Book–listed DALIRESP patents will have expired by the time of its New Drug Application (NDA) submission, and that no Paragraph IV certification with a consequent 30–month stay would be required. As we plan to develop more than one roflumilast product, including potential combination products, we may also utilize alternative regulatory strategies. Our deep involvement in topical generics along with the supportive view of independent intellectual property experts guides us to believe that there is a significant risk that present patents and patent applications for roflumilast 0.3% cream may be unable to prevent early genericization of the roflumilast products currently under development. Should this be the case, our innovative formulations of roflumilast, if approved by the FDA, would give us the opportunity to become a leading player in the multi–billion–dollar psoriasis and atopic dermatitis markets in the second half of the decade."

Mr. Arkin added, "Separately, we have made progress towards the development of our proprietary formulation of tapinarof cream, 1%, SGT–310. We plan to pursue a de–novo NDA via the 505(b)(1) regulatory pathway, with the goal of creating a second alternative to an investigational tapinarof cream, 1%, for which an NDA was already submitted to the FDA. According to this strategy, we plan to launch our tapinarof drug product worldwide no later than five years following the U.S. approval of the first tapinarof cream, aiming to increase affordability for patients compared to the brand expected to be launched. In addition, we intend to differentiate ourselves by offering tapinarof product formulation innovations for new indications. We have already been refining our strategy in line with best regulatory practices, and our drug product will be developed via our active pharmaceutical ingredient (API) manufacturing collaboration with Wavelength Pharmaceuticals, previously known as Perrigo API, a company with an impressive track record of FDA GMP compliance."

Mr. Arkin further added: "Our proof–of–concept (POC) study for SGT–210 (erlotinib gel) in six (6) palmoplantar keratoderma (PPK) patients has been completed and indicated modest improvement and a favorable safety profile. In this study, we used a very low concentration of erlotinib. We are now planning to test erlotinib at much higher concentrations in an animal model in the second half of 2021 and if successful, will conduct a second POC study on PPK patients in 2022. We remain optimistic about this program."

Management to Host Conference Call Today

Sol–Gel will host an investor conference call today at 8 AM U.S. EDT to discuss today's announcement, herein, and the strategy of the company following today's partnership news, announced separately.

To participate in the call, dial either the domestic or international number fifteen minutes before the conference call begins:

Domestic: 1–877–407–0784
International: 1–201–689–8560
Passcode: 13720829

The live conference call and replay can also be accessed by audio webcast here and also on the Investor Relations section of the Company's website, located at https://ir.sol–gel.com/investor–relations.

About Roflumilast

Roflumilast is a selective, long–acting inhibitor of Phosphodiesterase–4 (PDE4). It is the active ingredient in the Food and Drug Administration (FDA) approved medication, DALIRESP , which is as an oral treatment indicated in the U.S. as a therapy to reduce the risk of COPD exacerbations in patients with severe COPD associated with chronic bronchitis and a history of exacerbations.

A roflumilast cream 0.3% formulation is under investigation as a once–daily treatment of plaque psoriasis and positive Phase 3 results were recently reported.

About Tapinarof

Tapinarof is a novel, first–in–class, small–molecule topical therapeutic aryl hydrocarbon receptor (AhR)""modulating agent. It is in clinical development for the treatment of psoriasis and atopic dermatitis. The efficacy of tapinarof in psoriasis is attributed to its specific binding and activation of AhR, a ligand–dependent transcription factor, leading to the downregulation of proinflammatory cytokines, including interleukin 17, and regulation of skin barrier protein expression to promote skin barrier normalization.

About Erlotinib

Erlotinib is a tyrosine kinase receptor inhibitor which acts on the Epidermal Growth Factor Receptor (EGFR). It is the active pharmaceutical ingredient (API) in Tarceva which is used to orally treat non–small cell lung cancer, pancreatic cancer and several other types of cancer. Currently, there are no topical products of erlotinib, and erlotinib is not approved for plaque psoriasis.

About Wavelength Pharmaceuticals

Wavelength is a customer–focused backward–integrated world–class developer and manufacturer of Active Pharmaceutical Ingredients (APIs). It is the independent company of choice for pharmaceutical industry leaders that require advanced API solutions and reliable supply to gain sustainable competitive advantage. The company is on the same wavelength as its customers "" a partner in tune with the results required to best support their needs. Founded in Israel in 1987, with more than 280 customers in 50 countries, Wavelength produces more than 630 metric tons of commercial products every year, across a wide range of technologies including injectables, inhalables, highly potent, cytotoxic and controlled substances. Its cGMP–compliant facility is a first–class operation recognized for excellence in safety and environmental stewardship. Wavelength has achieved an exceptional track record for more than 30 years with all leading global regulatory authorities, including USFDA, EU–EMA, PMDA, TGA, KFDA, ANVISA and COFEPRIS. The company includes experts in complex chemistry, process development and scale–up, enzymatic reactions, crystalline forms and particle design, spray drying and other bioavailability–enhancing solutions. Wavelength offers end–to–end customized solutions to meet individual customer requirements, including full–spectrum API CDMO services from pre–clinical grams to multi–ton commercial scale "" always with uncompromising consistent quality, regulatory compliance and exceptional customer service.

About Sol–Gel Technologies

Sol–Gel is a clinical–stage dermatology company focused on identifying, developing and commercializing branded and generic topical drug products for the treatment of skin diseases. Sol–Gel leverages its proprietary microencapsulation technology platform for the development of TWYNEO under investigation for the treatment of acne vulgaris with an NDA filed with the FDA and a PDUFA goal date set for August 1, 2021; and EPSOLAY , under investigation for the treatment of inflammatory lesions of rosacea with an NDA filed with the FDA and a PDUFA goal date set for April 26, 2021. Both product candidates are exclusively licensed for U.S. commercialization with Galderma Holding SA. Action on the NDA for EPSOLAY has not yet been taken due to the inability of the FDA to conduct a pre–approval inspection of the production site of EPSOLAY as a result of COVID–19 travel restrictions. The Company's pipeline also includes SGT–210, an early–stage topical epidermal growth factor receptor inhibitor, erlotinib, under investigation for the treatment of palmoplantar keratoderma, and preclinical assets tapinarof and roflumilast. For additional information, please visit www.sol–gel.com.

Forward–Looking Statements

This press release contains "forward–looking statements" within the meaning Securities of the Private Litigation Reform Act of 1995. All statements contained in this press release that do not relate to matters of historical fact should be considered forward–looking statements. These forward–looking statements include information about possible or assumed future results of our business, financial condition, results of operations, liquidity, plans and objectives. In some cases, you can identify forward–looking statements by terminology such as "believe," "may," "estimate," "continue," "anticipate," "intend," "should," "plan," "expect," "predict," "potential," or the negative of these terms or other similar expressions, including statements regarding the timing for the initiation of a Phase I study for SGT–510, the intellectual property protection that would be provided by a patent for SGT–210, the anticipated status of patents at the time of an NDA submission for SGT–210, the timing of the launch of our tapinarof drug product and the timing of a test of erlotinib with a much higher concentrations in an animal model and a second POC study on PPK patients. Forward–looking statements are based on information we have when those statements are made or our management's current expectation and are subject to risks and uncertainties that could cause actual performance or results to differ materially from those expressed in or suggested by the forward–looking statements. Important factors that could cause such differences include, but are not limited to, the risk of a delay in receipt of approval, if any, of the NDA for TWNYEO, the risk of a further delay in receipt of approval, if any, of the NDA for EPSOLAY, the risk of a delay in the initiation of a Phase I study for SGT–510, the risk that a patent for SGT–210 will not provide the anticipated intellectual property protection, the risk that all Orange Book–listed DALIRESP patents will not have expired by the time of our NDA application for SGT–21 and that a consequent 30–month stay will required, the risk of a delay in the launch of our tapinarof drug product, the risk of a delay the timing of a test of erlotinib with a much higher concentrations in an animal model and the risk of a delay in a second POC study on PPK patients, risks relating to the effects of COVID–19 (coronavirus) as well as the following factors: (i) the adequacy of our financial and other resources, particularly in light of our history of recurring losses and the uncertainty regarding the adequacy of our liquidity to pursue our complete business objectives; (ii) our ability to complete the development of our product candidates; (iii) our ability to find suitable co–development partners; (iv) our ability to obtain and maintain regulatory approvals for our product candidates in our target markets, the potential delay in receiving such regulatory approvals and the possibility of adverse regulatory or legal actions relating to our product candidates even if regulatory approval is obtained; (v) our ability to commercialize our pharmaceutical product candidates; (vi) our ability to obtain and maintain adequate protection of our intellectual property; (vii) our ability to manufacture our product candidates in commercial quantities, at an adequate quality or at an acceptable cost; (viii) our ability to establish adequate sales, marketing and distribution channels; (ix) acceptance of our product candidates by healthcare professionals and patients; (x) the possibility that we may face third–party claims of intellectual property infringement; (xi) the timing and results of clinical trials that we may conduct or that our competitors and others may conduct relating to our or their products; (xii) intense competition in our industry, with competitors having substantially greater financial, technological, research and development, regulatory and clinical, manufacturing, marketing and sales, distribution and personnel resources than we do; (xiii) potential product liability claims; (xiv) potential adverse federal, state and local government regulation in the United States, Europe or Israel; and (xv) loss or retirement of key executives and research scientists. These and other important factors discussed in the Company's Annual Report on Form 20–F filed with the Securities and Exchange Commission ("SEC") on March 4, 2021 and our other reports filed with the SEC could cause actual results to differ materially from those indicated by the forward–looking statements made in this press release. Any such forward–looking statements represent management's estimates as of the date of this press release. Except as required by law, we undertake no obligation to update publicly any forward–looking statements after the date of this press release to conform these statements.

For further information, please contact:

Sol–Gel Technologies
Gilad Mamlok
Chief Financial Officer
+972–8–9313433
Investor relations
Irina Koffler
LifeSci Advisors
+1–917–734–7387
ikoffler@lifesciadvisors.com


GLOBENEWSWIRE (Distribution ID 8271138)