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MedNess: bite-size biopharma and medtech news

4th August, 2021

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MedNess This Week
HIGHLIGHTS
Onco-I-Analyse
Keytruda gets green light from the FDA in high-risk, early stage TNBC
On 26th July, the US FDA has approved Merck’s Keytruda (pembrolizumab) in combination with chemotherapy as neoadjuvant therapy followed by adjuvant monotherapy in high-risk, early-stage triple-negative breast cancer (TNBC) patients. FDA also converted accelerated approval in PD-L1+, 1L TNBC to regular approval. The approval is based on the pivotal Phase 3 KEYNOTE-522 study.
Background: Early stage TNBC is an area of high unmet need with poorer outcomes and survival. High-risk early stage TNBC is also associated with higher recurrence rates within 5 years with 30-40% recurring after neoadjuvant therapy and surgery. Chemotherapy is the only standard of care for high-risk early stage TNBC patients.
Details: Phase 3 KEYNOTE-522 is evaluating Keytruda as neoadjuvant therapy in combination with chemotherapy (carboplatin + paclitaxel followed by doxorubicin/epirubicin + cyclophosphamide) and continued as monotherapy adjuvant treatment vs. neoadjuvant chemotherapy followed by adjuvant placebo in 1,174 high-risk, previously untreated stage II/III TNBC patients.
In mid-July, Merck had announced that Keytruda arm demonstrated statistically significant improvements in the EFS, co-primary endpoint, compared to the chemotherapy arm during the fourth interim analysis. At a median follow-up of 39 months, Keytruda arm demonstrated a 37% risk reduction in EFS events (including disease progression, recurrence, second primary cancer, or death from any cause) compared to chemotherapy arm (p=0.00031).
The other primary endpoint of pCR was achieved (63% vs. 56%) during the first interim analysis. Follow-up for OS is ongoing.
Additionally, based on the confirmatory data from KEYNOTE-522, the accelerated approval of Keytruda + chemotherapy was converted to full approval for PD-L1+ (CPS ≥10), 1L TNBC as determined by an FDA-approved test. The accelerated approval, granted in November 2020, was based on the Phase 3 KEYNOTE-355 study.
Implications: The approval marks the first immunotherapy combination approved in this patient segment. The application was reviewed based on RTOR and Assessment Aid to accelerate the process and approval was granted 5 months ahead of the PDUFA.
The review saw months of delays by the FDA. In February, FDA deferred the regulatory decision which resulted in a CRL in March due to unavailability of mature EFS data.
Although, Keytruda has the first mover advantage, Roche’s Tecentriq is next in line with similar trial design. SVB Leerink analyst predict US sales of $300-500 million in early stage TNBC for checkpoint inhibitors.
Collated by : Shilpa Rawal, PhD
Drug Approvals
European Commission Approves Opdivo as Adjuvant Treatment for Esophageal or GEJ Cancer Patients with Residual Pathologic Disease Following Chemoradiotherapy
“We have demonstrated that the use of immunotherapy in earlier stages of cancer has the potential to prevent recurrence for certain patients,” said Ian M. Waxman, M.D., development lead, gastrointestinal cancers, Bristol Myers Squibb. “BMS was the first company to bring checkpoint inhibitors into the adjuvant setting for the treatment of patients with melanoma, and we are pleased to be the first to bring adjuvant therapy to patients in the EU with esophageal or gastroesophageal junction cancers who continue to face a high unmet need.”
Health Canada approves BRUKINSA® (Zanubrutinib) for the Treatment of Patients with Mantle Cell Lymphoma
“BRUKINSA was specifically designed by BeiGene scientists to provide deep and durable responses for patients with hematologic malignancies, while also reducing the frequency of certain off-target side effects seen with first-generation BTK inhibitors. Today’s approval in Canada for patients with MCL follows its approval for patients with WM earlier in the year, where Canada was the first country to grant approval for BRUKINSA in patients with WM,” said Jane Huang, M.D., Chief Medical Officer, Hematology, BeiGene. “We are excited to continue working with patients and physicians in Canada, as well as in other markets, as part of our broad clinical development program for BRUKINSA investigating eight indications in over 25 clinical trials, with more than 3,100 patients participating.”
 Click here for more Drug Approvals
Regulatory News

ERYTECH Granted U.S. FDA Fast Track Designation for Eryaspase in Hypersensitive ALL
“This is yet another significant milestone and meaningful inflection point in advancing our lead product candidate eryaspase, further supporting our recently announced intention to submit a BLA for eryaspase in hypersensitive ALL patients,” said Gil Beyen, CEO of ERYTECH. “We believe that the FDA’s Fast Track designation for eryaspase underscores its potential to address this high unmet medical need.”

Opdivo® (nivolumab) Monotherapy Post-Sorafenib HCC U.S. Indication Withdrawn
“We are disappointed by the position the Advisory Committee and the FDA have taken regarding the continued approval of Opdivo monotherapy as a treatment for HCC post-sorafenib. HCC is a complex and challenging disease, and for patients who are initially treated with sorafenib and either cannot tolerate treatment or whose disease progresses, immunotherapy is an important treatment option. For the past three and a half years, Opdivo monotherapy has been an important option that physicians have relied on to address this need and is currently the most commonly used therapy in the post-sorafenib setting,” said Jonathan Cheng, senior vice president and head of oncology development, Bristol Myers Squibb. “Opdivo helped usher in an entirely new way to treat patients with this disease. We continue to support the FDA’s accelerated approval program, which has been integral to enabling people with difficult to treat cancers to gain access to certain safe and effective new therapies sooner.”
 Click here for more Regulatory News
Trial Results
Positive Topline Results Announced from Ph 3 SEQUOIA Trial of BRUKINSA® (Zanubrutinib) vs Bendamustine + Rituximab in 1L CLL Patients; Primary Endpoint Met
“The combined clinical evidence from SEQUOIA, ALPINE1, the 205 trial2, and the AU-003 trial3 validates our confidence in BRUKINSA as a regimen which can offer improvements in treatment outcomes for hundreds of thousands of patients living with CLL,” said Jane Huang, M.D., Chief Medical Officer, Hematology at BeiGene. “We are pleased to see that at the interim analysis of the SEQUOIA trial, BRUKINSA significantly prolonged progression-free survival for treatment-naïve CLL patients, and that the demonstrated safety profile was consistent with what we have observed in its global development program with more than 2,300 patients treated with BRUKINSA to date.”
Ph3 KEYNOTE-355 Trial Met Primary Endpoint of OS in mTNBC patients Whose Tumors Expressed PD-L1 (CPS ≥10)
“In the fight against triple-negative breast cancer, the subtype with the worst survival prognosis, new options that can extend the lives of patients are urgently needed,” said Dr. Vicki Goodman, vice president, clinical research, Merck Research Laboratories. “These new overall survival results confirm that KEYTRUDA in combination with chemotherapy represents an important treatment option for certain patients with metastatic TNBC. We thank the patients and investigators who have allowed us to evaluate innovative treatment approaches, anchored by KEYTRUDA, across multiple settings and stages of TNBC.”
Click here for more Trial Results
Trial/Program Status
First Patient with Advanced HER2-Positive Breast Cancer Dosed with Zanidatamab + Tukysa® (Tucatinib) and Chemotherapy
“Recent clinical trials have demonstrated the benefit of combining tucatinib with trastuzumab and chemotherapy in patients with metastatic HER2-positive breast cancer,” said Neil Josephson, M.D., Interim Chief Medical Officer at Zymeworks. “Given the antitumor activity of zanidatamab observed across a range of HER2-overexpressing tumors and preclinical studies demonstrating improved anti-tumor activity of zanidatamab compared to trastuzumab, we believe the combination of zanidatamab with tucatinib and chemotherapy has the potential to be an impactful treatment for patients with advanced HER2-positive breast cancer, including those with brain metastases.” Josephson added, “this new study cohort complements our ongoing trials with zanidatamab in combination with other standard of care treatment regimens and supports our goal of establishing zanidatamab as the foundational therapy for HER2‑expressing cancers.”
First patients dosed in Ph 2 and 1/2 studies of XPOVIO® (selinexor) + approved therapies in patients with advanced melanoma and 1L myelofibrosis
"Despite recent advances in treatment options for both metastatic melanoma and myelofibrosis, far too many patients either do not respond or have short-lived responses to currently available treatment options, making the development of novel drug treatment approaches incredibly important for these diseases," said Sharon Shacham, PhD, MBA, Chief Scientific Officer of Karyopharm. "Substantial need remains for continued research into new druggable targets and identifying multiple targets and pathways that have the potential to be inhibited synergistically using combination approaches. We believe XPOVIO's oral administration, along with its novel mechanism of action, make it a promising treatment candidate for new, single and synergistic combination regimens across both hematologic and solid tumors."
Click here for more Trial Statuses
Collated by : Richa Tewari, PhD 
MedNess HealthIT
Skewed rate of immunization revealed the role of ethnicity and racial disparity in preventable deaths
A lower vaccination rate in the racial and ethnically minor populations is causing adults to succumb to preventable deaths, a recent study published in the American Journal of Preventive Medicine suggests. A staggering range of 12,000 to 61,000 adults die from influenza alone. According to the study authors Kosuke Kawai, ScD, and Alison Tse Kawai, ScD: “Unfortunately, as we observed for vaccines against influenza, pneumococcal, shingles, and Tdap, a combination vaccine that protects against tetanus, diphtheria, and pertussis, adults from racial and ethnic minorities have had lower rates of COVID-19 vaccine uptake.”
Using data analytics between 2010 to 2019, the study examined vaccination trends factoring in race/ethnicity/socioeconomic conditions towards vaccination and used the data source of National Health Interview Surveys (NHIS). Vaccine coverage was studied for the following diseases: influenza, pneumococcal disease, herpes zoster, and Tdap. Collected data represented demographics, health status, insurance coverage, healthcare access, and health behaviors from a nationally representative sample. All these factors were found to influence the decision of the subjects to get vaccinated or not. Interestingly, Affordable Care Act was able to marginally improve the disparity between the age group of 18-64, although people from 65 to above were showed no difference. Black and Latino populations were found to have lower rates of immunization compared to the whites.
Precision medicine gets a boost for cancer treatment by studying DNA tags
Tiny tags in the DNA molecules through methylation can help physicians and researchers to distinguish between healthy vs. damaged tissue. Liquid biopsy in cancer patients, as opposed to biopsy directly from the tumor tissue provides a wider array of information on the heterogeneity of the tumor cells within the host. In this process, cell-free DNA (cfDNA) is collected from the blood, which are naturally released in the patient body as a result of cell death. Researchers from Georgetown Lombardi Comprehensive Cancer Center are leveraging these phenomena, combined with genome sequencing and computational analysis for the collected DNA samples. The lead author of the study Megan Barefoot explains it in simple words: "Methylated cfDNA has opened a new and minimally invasive way to detect damage to cells in the body as there are often hundreds of methyl markers per cell that can mark, very specifically, where the cells came from, much like a barcode scanner at a grocery checkout tells the store the identity of a particular product. Combined biological and computational analyses make deciphering these methylation patterns/molecular barcodes possible so that researchers can trace the origins of cfDNA."
The study promises to indicate the origin of a specific cancer cell in a patient, and also the extent of tissue damage incurred by external medical intervention, such as radiation, chemotherapy, and immunotherapy. Given the affordable nature of these tests, the authors believe that this knowledge will aid many labs by becoming a standard procedure.
Collated by: Debarati Banik, PhD
MedNess Business
Onco-News
MD Anderson and Blueprint Medicines Announce Strategic Collaboration to Accelerate BLU-222 Development
“This collaboration highlights our commitment to rapidly advance innovative science and builds on our prior efforts – also supported by MD Anderson investigators – that led to two FDA-approved and breakthrough therapy-designated precision therapies for patients with cancer,” said Fouad Namouni, M.D., President of Research and Development at Blueprint Medicines. “By leveraging the power of MD Anderson’s expertise in translational research, we aim to reveal the broad potential of BLU-222 and optimize our clinical development strategy to bring treatment innovation to as many patients as possible.”
BridgeBio And BMS To Study BBP-398 + OPDIVO® (Nivolumab) In Advanced Solid Tumors With KRAS Mutations
“A Priority Of Ours Is To Develop Innovative Medicines That Target Tumor Intrinsic Mechanisms Including The MAPK Pathway,” Said Emma Lees, Senior Vice President, Oncology Research At Bristol Myers Squibb. “We Look Forward To Beginning The Clinical Exploration Of The Mechanistic Rationale And Therapeutic Benefit From Combining Robust MAPK Pathway Inhibition And PD-1 Blockade In KRAS Mutant NSCLC.”
Click here for more on mergers, acquisition, and business news
 
Collated by: Richa Tewari, PhD 
Editors' Desk
Richa Tewari, PhD
Oncology News
Shilpa Rawal, PhD
Onco I-Analyse
Arundithi Ananthanarayanan
MedNess Reviews
Divyaanka Iyer
Business Review
Debarati Banik
HealthIT
Darpan Chakraborty
Social Media Manager
Nisha Peter, PhD
Managing Editor
Abhi Dey
Consulting Editor
Rinki Saha
BioPharma News
Managing Editor
Shalini Roy Choudhury
Genes and Therapy
Managing Editor
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The sponsors do not have any influence on the nature or kind of the news/analysis reported in MedNess. The views and opinions expressed in this article are those of the authors and do not necessarily reflect the official policy or position of Medness. Examples of analysis performed within this article are only examples. They should not be utilized in real-world analytic products as they are based only on very limited and dated open source information. Assumptions made within the analysis are not reflective of the position of anyone volunteering or working for Medness. This blog is strictly for news and information. It does not provide medical advice, diagnosis or treatment nor investment suggestions. This content is not intended to be a substitute for professional medical advice, diagnosis, or treatment. Always seek the advice of your physician or another qualified health provider with any questions you may have regarding a medical condition. Never disregard professional medical advice or delay in seeking it because of something you have read on this website.
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Content Editors: Richa Tewari , Esha SehanobishRinki Saha ,  Shilpa Rawal, PhD ,  Debarati Banik  , Divyaanka Iyer , Arundithi Ananthanarayanan and Abhinav Dey 
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