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Tuesday, June 14, 2022

FDA’s treatment of China-developed drugs spurs demands for multiregional clinical trials

 China’s emergence as an R&D powerhouse means that the country is quickly adding a number of drug candidates to the global pipeline. Despite more treatment options being a positive, Ben Hargreaves finds that this has raised issues over single-region clinical trials, leading to the FDA rejecting certain treatments and clarifying what is required for approval.

China’s ambition to become a leader in the biopharma industry has been clear in the last few years. The investment flowing into the sector is not limited to just the development of medicines, there has also been a focus on rapidly developing capability and capacity to manufacture both traditional pharmaceuticals and biologic medicines.

A representation of the country’s rapidly developing capability can be seen in the example of WuXi Biologics, which is a contract development and manufacturing organisation, that was created in 2015 and is now in the top five companies in terms of manufacturing capacity for biologics. Similar signs of growth can be seen in the amount of drugs, biologics and medical devices the country exports to the US. The US FDA notes that China ranks third among countries that export drugs and biologics to the country, with China also placing in first position for export of medical devices to the US.

The innovation that is happening within the Chinese biopharma ecosystem means that frequently Western pharma companies are looking to partner with Chinese firms to bring treatments to the US and Europe. Only last month, the US company Merck agreed to pay a potential $1.4 billion to partner on an immuno-oncology asset with Chinese firm, Sichuan Kelun Pharmaceutical. Merck is not alone, with a number of companies making deals to leverage the growing pipeline of therapeutic candidates developed in China, such as Bavarian Nordic’s agreement to progress a potential RSV vaccine developed by Nuance Pharma.

Evolving regulatory landscape

However, the developing commercial relationship between established pharma companies and China recently hit a snag: the US FDA has adopted a tougher approach to reviewing applications of treatments tested in China. Last month, the agency rejected two cancer therapies developed by Chinese pharma companies, after previously moving against Eli Lilly and Innovent Biologics’ immunotherapy, sintilimab.

The two treatments to be most recently rejected were Hutchmed’s surufatinib, and Coherus BioSciences and Shanghai Junshi Biosciences’ toripalimab. Coherus’ treatment was rejected on grounds related to the manufacturing process for the drug. More significant were the reasons for the rejection of sintilimab and surufatinib, as the FDA cited issues with the lack of clinical trial data gathered from outside of China.

Hutchmed had carried out two phase 3 trials in China and one bridging study in the US, but it was not enough to secure approval. Instead, in the complete response letter (CRL), the FDA requested a multi-region clinical trial to be completed for approval to be considered. Effectively, this will push back potential marketing approval for the treatment by years while the trial is completed. The FDA’s decision may not have been a surprise to Hutchmed, after the FDA also raised issue with Lilly’s application that relied on single-country clinical trials as the foundation for its request for approval.

Single-region concerns

The reasons behind the FDA’s decision to push back on single-country clinical trials were made explicit during the application process for Lilly’s sintilimab. Richard Pazdur, director of the FDA’s oncology centre of excellence, had an article published where he outlined concerns over drug applications being based on solely or predominantly data gathered from China-based clinical trials.

Underlining the importance of the FDA’s stance on the issue, Pazdur highlighted that there were at least 25 applications from China based on such data for treatments within oncology. As a senior member of the FDA, Pazdur’s comments can be taken as reflecting the position held by the FDA over similar applications and point towards the agency’s stance for future applications – later confirmed by the FDA’s rejection of Lilly’s and Hutchmed’s application.

Within the article, several key concerns were raised over the use of clinical trial data from a single foreign country. One significant factor centred on the generalisability of data gathered when applied to the US population, with intrinsic factors, such as genetic dissimilarity of populations, and extrinsic factors, such as difference in medical practice, raised as potential problems.

Pazdur noted, “The degree of regulatory flexibility in establishing the acceptability of data from a single country and its generalisability to a new population should be balanced against the drug’s innovation.”

Emphasising multiregional trials

The problem for Lilly’s sintilimab application is that there already exist a number of approved PD-1 treatments on the US market, making it difficult to suggest that the treatment represented an innovation. When asked, a spokesperson for Lilly refused a request for further information on the CRL it had received. However, the company had previously issued a statement on why it believed the treatment should have been approved: “We had hoped that sintilimab could have played a positive role for patients and the US healthcare system through an aggressive pricing strategy.”

The positioning of the treatment as one that could compete on pricing with existing treatments was enough to secure one vote when the treatment was put in front of the FDA’s oncology drug advisor committee, but was not enough to persuade the remaining 14 members to recommend the treatment for approval.

Within Pazdur’s piece, he pointed towards a pathway for future applications that focused on multiregional clinical trials, particularly hinting that those containing studies conducted in Africa and South America would be ‘strengthened.’ He explained that this was due to these regions being currently underrepresented in oncology multiregional clinical trials and would boost diversity thereby increasing the representation of racial and ethnic minorities.

After the rejection of Hutchmed’s treatment, despite the efforts to include a bridging trial, the FDA seems to have drawn a line in the sand, effectively requiring multiregional clinical trials unless the drug candidate is considered ground-breaking. With many treatments already progressing through towards an application the US, the question will be whether companies now pivot to establish multiregional trials, despite this adding time and expense to the drug development process.

https://pharmaphorum.com/market-access-2/fdas-treatment-of-china-developed-drugs-spurs-demands/

Evotec in Drug Discovery Collaboration with Janssen

Evotec SE (FRA:EVT)(MDAX/TecDAX)(ISIN:DE0005664809)(NASDAQ:EVO) announced today that the Company has entered a drug discovery collaboration with Janssen Pharmaceutica NV, one of the Janssen Pharmaceutical Companies of Johnson & Johnson ("Janssen"). Evotec's innovative TargetAlloMod platforms will be evaluated to discover first-in-class novel mode of action therapeutic candidates. The agreement was facilitated by Johnson & Johnson Innovation.

Under the agreement, Evotec and Janssen will jointly conduct screens on the identified targets and collaborate with hit identification and lead optimisation of the most promising chemical assets, leveraging Evotec's end-to-end integrated drug discovery and development platform.

https://www.biospace.com/article/releases/evotec-enters-a-drug-discovery-collaboration-with-janssen/

Clover in Phase 3 Trial of COVID-19 Booster After Inactivated, mRNA or Viral Vector Vaccines

 

  • Study to evaluate SCB-2019 (CpG 1018/Alum) as a heterologous booster in individuals previously vaccinated with CoronaVac™ (Sinovac Inactivated Vaccine), Comirnaty® (Pfizer mRNA Vaccine), and Vaxzevria® (AstraZeneca Viral Vector Vaccine)
  • Safety & immunogenicity data expected for key 3rd dose booster groups (CoronaVac™ and Comirnaty®) in Q3-2022 and the 4th dose booster group (CoronaVac™) in Q4-2022
  • Study to expand dataset supporting the potential use of SCB-2019 (CpG 1018/Alum) as a universal COVID-19 booster vaccine

Monday, June 13, 2022

Amylyx bags first approval for ALS drug Albrioza

 Amylyx Pharmaceuticals’ efforts to bring its amyotrophic lateral sclerosis therapy AMX0035 to market in the US have run into some roadblocks, so an approval by Health Canada is a welcome relief for the biotech.

Canada is the first country worldwide to approve the combination of orally active ingredients sodium phenylbutyrate and taurursodiol – as Albrioza – marking Amylyx’ transition from a development-stage to a commercial-stage company.

Albrioza is also the first new therapy for the devastating neurodegenerative disorder to be approved in Canada since Mitsubishi Tanabe’s Radicava (edaravone) in 2018.

It’s a vote of confidence in the drug after an FDA advisory committee voted against approval of the drug in the US by a narrow margin in March, and after the agency extended its review of the drug by three months to end-September.

Health Canada’s decision comes with some conditions attached, including that Albrioza staying on the market will depend on the outcome of the ongoing late-stage PHOENIX study in 600 patients, which is due to read out in 2024.

The green light comes on the back of the 137-patient phase 2 CENTAUR study, which showed a modest five-month survival benefit over placebo – a 44% lower risk of death over the duration of follow-up – as well as improvements in symptom scores for ALS patients that were borderline statistically significant.

Amylyx said it will launch Albrioza in Canada within the next six weeks, and will work with the pan-Canadian Pharmaceutical Alliance (pCPA) – which conducts price negotiations with manufacturers for government drug programmes – as well as federal, provincial and territorial governments on access.

In the US, the negative advisory committee vote was met with consternation by patient organisations, as ALS has only two approved therapies – oral riluzole and intravenous Radicava – which have limited efficacy.

“ALS is a devastating disease and can move with startling swiftness,” said Tammy Moore, chief executive of the ALS Society of Canada.

“It is incredibly important that all Canadians across the country are able to benefit from these and other innovations to come, as quickly as possible following regulatory approval. There is simply no time to wait with this disease.”

In ALS, which is also known as motor neurone disease, the nerve cells that control muscle function slowly die off. The two active ingredients in AMX0035 are thought to reduce neuronal death by regulating mitochondrial and endoplasmic reticulum pathways in nerve cells.

https://pharmaphorum.com/news/amylyx-bags-first-approval-for-als-drug-albrioza/

Alnylam: FDA OKs RNAi Therapeutic for Amyloidosis

  Alnylam Pharmaceuticals, Inc. (Nasdaq: ALNY), the leading RNAi therapeutics company, today announced that the U.S. Food and Drug Administration (FDA) approved AMVUTTRA™ (vutrisiran), an RNAi therapeutic administered via subcutaneous injection once every three months (quarterly) for the treatment of the polyneuropathy of hereditary transthyretin-mediated (hATTR) amyloidosis in adults. hATTR amyloidosis is a rare, inherited, rapidly progressive, and fatal disease with debilitating polyneuropathy manifestations, for which there are few treatment options. The FDA approval is based on positive 9-month results from the HELIOS-A Phase 3 study, where AMVUTTRA significantly improved the signs and symptoms of polyneuropathy, with more than 50 percent of patients experiencing halting or reversal of their disease manifestations.

Conference Call Information

Alnylam Management will discuss the FDA approval of AMVUTTRA via conference call on Tuesday, June 14, 2022, at 8:00 am ET. A webcast presentation will also be available on the Investors page of the Company’s website, www.alnylam.com. To access the call, please dial 1-877-312-7507 (domestic) or +1-631-813-4828 (international) five minutes prior to the start time and refer to conference ID 1084157. A replay of the call will be available beginning at 11:00 am ET on the day of the call. To access the replay, please dial 855-859-2056 (domestic) or +1-404-537-3406 (international) and refer to conference ID 1084157.

https://www.biospace.com/article/releases/alnylam-announces-fda-approval-of-amvuttra-vutrisiran-an-rnai-therapeutic-for-the-treatment-of-the-polyneuropathy-of-hereditary-transthyretin-mediated-amyloidosis-in-adults/

Transcript: Merck at Goldman Global Health Conference

 https://www.marketscreener.com/quote/stock/MERCK-CO-INC-13611/news/Transcript-Merck-Co-Inc-Presents-at-Goldman-Sachs-43rd-Annual-Global-Healthcare-Conference-J-40713533/

Becerra tests positive for COVID-19 twice in less than a month

 Health and Human Services (HHS) Secretary Xavier Becerra tested positive for COVID-19 on Monday, the agency announced, the second time he has been infected in less than a month.

“This morning in Sacramento, U.S. Health and Human Services Secretary Xavier Becerra tested positive for COVID-19 after taking an antigen test. He is fully vaccinated and boosted against COVID-19, and is experiencing mild symptoms. He will continue to perform his duties as HHS Secretary, working in isolation,” HHS spokeswoman Sarah Lovenheim said in a statement.

Becerra previously tested positive for COVID-19 on May 18 while traveling in Berlin ahead of the Group of Seven meetings for health ministers.

Last week, Becerra was in Los Angeles to participate in the Summit of the Americas with President Biden and Vice President Harris. HHS said Becerra is not considered a close contact of either.

Biden so far has avoided having a known case of the virus, but the White House has acknowledged it is possible he will be infected as well. The administration argues that tools such as vaccines, booster shots and treatments now exist that make the virus much more manageable.  \

Becerra is not the only official who tested positive following the summit. Canadian Prime Minister Justin Trudeau on Monday revealed he also tested positive for COVID-19 for the second time this year.

Reinfection is quickly becoming the primary driver of new cases in the United States, showing that immunity from previous infections is no longer able to provide the same level of protection against emerging variants and subvariants.

Infectious disease experts think a typical SARS-CoV-2 infection will likely become less dangerous over time, but the full implications and severity of multiple infections are still not clear.

https://thehill.com/policy/healthcare/3521555-health-secretary-becerra-tests-positive-for-covid-19-twice-in-less-than-a-month/