FDA warns that emerging Omicron subvariant could make Evusheld obsolete

 AstraZeneca’s Covid-19 pre-exposure prophylactic Evusheld has managed to remain relevant for immunocompromised and other patients when many of its therapeutic peers haven’t with each new Omicron subvariant.

But that win streak may slowly come to a close as the FDA told healthcare providers on Monday that one of the emerging subvariants, BA.4.6, renders Evusheld almost completely useless.

Nationally, BA.4.6 currently makes up about 13% of new cases, compared to just 1% of cases at the beginning of July, according to the CDC. But in some regions, like in Iowa, Missouri, Kansas and Nebraska, the BA.4.6 subvariant makes up more than 20% of all Covid-19 cases.

AstraZeneca’s spokesperson told Endpoints News in a statement that in vitro data conducted by an FDA lab “showed that Evusheld is unlikely to be active against BA.4.6, which currently represents 6.2% of infections globally and growing slowly; it is not expected to become a dominant strain.”

Evusheld remains active against the dominant variant, BA.5, the spokesperson added, noting that the prophylactic “should continue to provide protection to the vast majority of intended recipients.”

If BA.4.6 spreads more nationally, and Evusheld can no longer be used, the blow would be a big one for for AstraZeneca, which saw the intramuscular injection pull in $914 million in the first half of 2022, and another $135 million last year.

If another subvariant takes over or BA.5 remains dominant, and Evusheld holds up, the commercial market awaits as federal funds dry up. HHS previously said that the remaining federal supply of Evusheld (about 750,000 courses of the 1.5 million ordered remain) could be gone by as soon as early 2023.

US expects to soon run out of government Covid-19 funds for vaccines, treatments

FDA on Monday also updated the Evusheld fact sheet to broaden the patient population that may benefit from it, especially among people with blood cancers regardless of treatment status, the spokesperson added.

https://endpts.com/another-one-bites-the-dust-fda-warns-that-emerging-omicron-subvariant-could-make-evusheld-obsolete/

Structure-based discovery of nonopioid analgesics acting through the α2A-adrenergic receptor

 ELISSA A. FINK HTTPS://ORCID.ORG/0000-0001-5531-1971JUN XU HTTPS://ORCID.ORG/0000-0002-1600-583XHARALD HÜBNER HTTPS://ORCID.ORG/0000-0002-7892-599XJOAO M. BRAZ HTTPS://ORCID.ORG/0000-0001-8955-0735PHILIPP SEEMANN HTTPS://ORCID.ORG/0000-0002-7575-2181CHARLOTTE AVETVERONICA CRAIK HTTPS://ORCID.ORG/0000-0001-5463-1199DOROTHEE WEIKERT HTTPS://ORCID.ORG/0000-0003-2259-9002MAXIMILIAN F. SCHMIDT HTTPS://ORCID.ORG/0000-0002-7055-2439[...]PETER GMEINER HTTPS://ORCID.ORG/0000-0002-4127-197X  

DOI: 10.1126/science.abn7065

A path to pain relief

The serious problems associated with opioid addiction have motivated the search for non-opioid pain-relief drugs. The α2A-adrenergic receptor (α2AAR) is a validated pain receptor and is targeted by dexmetadomine, a drug used in hospitals but unsuitable for broader use because it causes sedation and is not orally bioavailable. Fink et al. screened more than 300 million virtual molecules and identified agonists that bind α2AAR with reasonable affinity and are structurally unrelated to known agonists. Experimental structures of two of the compounds bound to α2AAR allowed optimization to improve potency. The optimized compounds were effective in a neuropathic pain model without causing sedation, making them promising leads for further development. —VV

Structured Abstract

INTRODUCTION

Epidemics of pain and opioid abuse underscore the need for new nonopioid therapeutics to treat pain. Many nonopioid receptors are involved in pain processing (nociception), but only a few have been validated therapeutically. Of particular interest is the α2A-adrenergic receptor (α2AAR), a G protein–coupled receptor (GPCR) whose activation in the central nervous system has pain-relieving effects. The known therapeutics targeting the α2AAR, like clonidine and dexmedetomidine, are known to be analgesic. They are also strongly sedating, which is important for the primary indication of dexmedetomidine. This, however, has restricted the use of these drugs to hospital settings and kept them from being used in broader patient populations.

RATIONALE

Because GPCRs, like α2AAR, can signal into the cell through multiple downstream effectors, we reasoned that agonists that were chemically dissimilar to the highly related dexmedetomidine, clonidine, and brimonidine might have different signaling and might be able to separate sedation from analgesia. We sought these chemotypes among a virtual library of more than 301 million diverse, readily accessible molecules in the ZINC15 library (http://zinc15.docking.org), few of which have been previously synthesized. We computationally docked each virtual molecule into the highly similar α2BAR binding site, prioritizing those that physically fit and that were chemically unrelated to the known drugs.

RESULTS

From the high-ranking docked compounds, we selected 48 for de novo synthesis and testing. Against the α2BAR used in the virtual docking screens, 30 molecules bound for a 63% hit rate, among the highest to date for docking campaigns. Seventeen further bound to α2AAR with binding constants in the low-nanomolar to low-micromolar concentration range. Several acted as full or partial agonists of α2AAR, activating the receptor. Among these was ‘9087 [mean effective concentration (EC50) of 52 nM]. Notably, the docking-derived agonists preferentially activated Gi, Go, and Gz G protein subtypes, which contrasts with known drugs, like dexmedetomidine and brimonidine, that activate a much broader set of G proteins and recruit β-arrestins. Thus, the new agonists activate a more selective set of cellular pathways than the known α2AAR drugs, something we had hoped for when prioritizing new chemotypes.

The structures of two of these agonists were experimentally determined in complex with the activated state of α2AAR. These experimental ligand geometries closely corresponded to computational predictions. They also templated the optimization of the initial docking hits and led to more potent analogs, including PS75 (EC50 4.8 nM). The physical features of these agonists allowed them to reach high brain concentrations after systemic dosing. In animal behavioral assays, six of these previously uncharacterized agonists relieved pain behaviors in neuropathic, inflammatory, and acute thermal nociception assays. Gene mutation and reversal of receptor binding with an α2AR antagonist confirmed that analgesia occurred primarily through α2AAR. Crucially, when compared with dexmedetomidine, none of the new compounds caused sedation, even at substantially higher doses than required for pain relief.

CONCLUSION

The separation of analgesic properties from sedation of the new agonists is important for further α2AAR drug development. The newly identified agonists, especially ‘9087 and PS75, overcome the sedation liability of the previously known drugs, and several are orally bioavailable. This makes them lead molecules for the development of nonopioid pain therapeutics.

https://www.science.org/doi/10.1126/science.abn7065

5 FDA decisions to watch in the fourth quarter

 Though 2022 has been a down year for the biotechnology sector, notable decisions from the Food and Drug Administration have provided a few bright spots.

Two gene therapies came to market, providing a lift for a field that’s been slowed by recent setbacks. The cancer drug Enhertu was approved for a newly defined tumor type known as “HER2-low.” The regulator also cleared a new medicine for ALS and a first-of-its-kind inflammatory disease drug.

The fourth quarter could yield some other medical milestones. An Alzheimer’s drug that unexpectedly succeeded in a large trial last week is under review. So are what could be the first treatment for a common form of vision loss, a closely watched HIV drug, and a type of anemia pill the FDA has already turned back twice.

Here are 5 FDA decisions to watch:

Covis’ Makena for prevention of preterm births

In the decade since the FDA made Makena available for the prevention of preterm births, the treatment has become a flashpoint in the debate over speedy drug approvals.

Makena was developed by AMAG Pharmaceuticals and granted accelerated approval in 2011 based on a study showing it reduced the risk of preterm births — which can jeopardize a baby’s health — in women with a history of delivering early.

A study meant to confirm Makena’s benefits took years to complete, however. When the results did arrive in 2019, Makena didn’t perform meaningfully better than a placebo.

Since then, the fate of Makena has been the subject of a fight between the FDA, AMAG and the drug’s current owner, Covis Pharma, which acquired AMAG in 2020. After an FDA advisory panel in 2019 recommended the regulator pull Makena from the market, the agency proposed doing so, arguing “the available evidence does not show Makena is effective” for its approved use.

Its developers, as well as some patient advocates and outside experts, have countered that doing so would be a mistake, claiming the drug still may help Black women at high risk of early births, who made up a larger portion of participants in the original trial than the confirmatory study.

A hearing on the issue has been delayed several times amid legal wrangling, extending the drug’s time on market while its benefit remains unclear. The FDA specifically cited the case as “an example of how lengthy and burdensome the withdrawal process may be” when a company disagrees with the agency, according to a report on accelerated approvals published last week by the U.S. Department of Health and Human Services.

The back-and-forth could come to a conclusion this quarter. A three-day hearing of an FDA advisory panel will begin on Oct. 17 and feature discussions on the available confirmatory evidence as well as “whether FDA should allow Makena to remain on the market.”

GSK’s daprodustat for anemia from kidney disease

GSK’s daprodustat is the third anemia drug of its kind to be reviewed by the FDA. If the rejections of the first two are any indication, daprodustat could have a tough time when the agency’s expert advisers meet to review it on Oct. 26.

Daprodustat is intended to be an oral alternative to injectable biologics like Epogen and Aranesp that boost red blood cell production and are used to treat anemia in patients with damaged kidneys. Those medicines have been standard treatments for years, but their use has been restricted because of the risk of heart problems.

GSK’s drug is also meant to increase red blood cell levels, but by tricking the body into thinking it’s in a low-oxygen environment. The approach is meant to be both safer and more convenient for patients, and has spawned daprodustat as well as drugs from FibroGen and Akebia Therapeutics. All three are approved in Japan, and FibroGen’s is cleared for use in Europe.

But none are available in the U.S., where regulators have taken a tougher stance. In a meeting last year, the FDA and its expert reviewers challenged claims that FibroGen’s drug is safer than its injectable competitors. The agency rejected that medicine and demanded another trial. It then did the same to Akebia’s treatment in March.

GSK believes it has a better case. Unlike its rivals, daprodustat didn’t perform worse than injectable drugs on measures of heart safety in the key studies supporting its application. There are still concerns, however. An editorial published in the New England Journal of Medicine alongside GSK’s two large studies flagged the risk of cancer, and questioned the drug’s benefit in patients who aren’t on dialysis, a group that makes up the majority of people with chronic kidney disease.

Apellis’ pegcetacoplan for geographic atrophy

People with the “wet” form of age-related macular degeneration, a leading cause of vision loss, have many effective treatment options. The estimated 5 million people across the globe with geographic atrophy — an irreversible eye disease that results from AMD — don’t. That could change if the FDA approves Apellis Pharmaceuticals’ pegcetacoplan later this year, however.

Pegcetacoplan is an injectable drug that blocks activation of the complement system, a part of the body’s innate immune response. In clinical testing, it’s shown the potential to slow growth of the lesions, or scar tissue, found in the eyes of people with geographic atrophy.

Yet Apellis doesn’t have a clear-cut case. The drug missed statistical significance in one of its two Phase 3 studies. Apellis also hasn’t yet proven that slowing lesion growth directly translates to improved vision. In August, the company reported patients in its late-stage trials didn’t experience a visual acuity benefit after two years of treatment.

Apellis executives have expressed confidence the drug’s benefit will become apparent with longer follow-up. “We have trouble imagining a scenario where lesion size doesn’t inevitably correlate with function,” wrote Evercore ISI analyst Umer Raffat, in a research note.

A green light from the FDA could yield a drug that Jefferies analysts estimate could generate as much as $6 billion in yearly sales at its peak. A rejection or delay, meanwhile, could cost Apellis a chance to be first to market, as Iveric Bio plans to file for approval of a similar drug early next year.

The FDA will make a decision by Nov. 26.

Mirati’s adagrasib for non-small cell lung cancer

For three years, analysts and investors have debated whether a cancer drug developed by Mirati Therapeutics, a small San Diego biotech, can top a rival one from Amgen that’s become the crown jewel of the larger company’s oncology business.

The two companies have traded clinical trial readouts showing their drugs can effectively shrink tumors driven to growth by mutations in a gene, called KRAS, that for decades was considered undruggable. Last spring, Amgen turned its positive data into a first-of-its-kind approval for its drug, now sold as Lumakras.

Now it’s Mirati’s turn in front of the FDA, as its drug adagrasib is under review with a decision deadline of Dec. 14. Should it win approval, Mirati would compete for market share with Amgen, which has the benefit of recent data confirming its drug beat chemotherapy in a larger study of patients with non-small cell lung cancer.

But Lumakras failed to show it could extend patients’ lives, leaving an opening for Mirati to do better. The company is currently enrolling a bigger trial that’s meant to confirm adagrasib’s benefit.

Gilead’s lenacapavir for HIV

By Dec. 27, Gilead Sciences should know whether its second attempt at getting a key HIV drug approved in the U.S. has succeeded.

The first try ended with an FDA rejection because of concerns about potential adverse interactions between the drug, known as lenacapavir, and the specific glass vials in which it was contained. Gilead said it has since addressed those manufacturing-related issues by using vials made from a different glass. The treatment won its first approval in Europe in September.

A similar outcome in the U.S. would bolster the commercial prospects for an important addition to Gilead’s arsenal of HIV medicines. Lenacapavir has a unique way of binding to the protein shell that surrounds the virus, and its benefits appear long-lasting. In a small study, an injection of the drug every six months, in combination with other antivirals, kept the virus in check for heavily pretreated patients who had developed resistance to multiple therapies.

Gilead has been evaluating potential combinations of lenacapavir and other drugs, including Merck & Co.’s islatravir, although that latter therapy has raised safety concerns over the last year. Gilead is also testing whether its drug works as a preventive treatment.

In a note to clients earlier this year, RBC Capital Markets analyst Brian Abrahams wrote that his team expects the FDA to approve lenacapavir for heavily pretreated HIV patients — a “relatively small indication” that could generate peak annual sales of about $200 million in the U.S.

But given lenacapavir’s various advantages, including the ability to be combined with other treatments and administered in multiple ways, the RBC team argues the drug could become “the backbone” of Gilead’s HIV franchise within several years and ultimately achieve more than $4 billion in yearly sales at its apex.

BONUS: Eisai and Biogen’s lecanemab for Alzheimer’s

Will lecanemab, an experimental Alzheimer’s drug that succeeded in a large clinical trial last week, become a backbone therapy for the neurodegenerative disease? Doctors and researchers aren’t yet sure, as only limited data have been disclosed by lecanemab’s developers, Eisai and Biogen.

They’ll get much more information Nov. 29, when the companies present fuller study results at a medical meeting in San Francisco. The results are likely to be pored over and debated, as they represent the first clearly positive data from a Phase 3 trial of a drug meant to treat Alzheimer’s underlying cause.

They’re also likely to help the FDA decide whether to approve lecanemab on an accelerated basis. Using data from an earlier study, Eisai filed an application earlier this year, and a decision is expected by Jan. 6 on the basis of the treatment’s ability to clear toxic plaques from the brain.

The new trial results were meant to confirm those preliminary findings. Now that they’re positive, Eisai has a stronger case and the FDA a potentially easier judgment call.

https://www.biopharmadive.com/news/5-fda-approval-decisions-fourth-quarter-2022/632732/

Inhibrx To Host Webcast on Regulatory Pathway for Rare Disease Therapy

 Inhibrx, Inc. (Nasdaq: INBX), a clinical-stage biopharmaceutical company dedicated to the development of therapeutics for oncology and rare diseases, announced today that it will host a live webcast presentation on Tuesday, October 4, 2022 at 5:30 a.m. PT to announce the regulatory pathway for INBRX-101 for the treatment of patients with alpha-1 antitrypsin deficiency, or AATD.

Investors may join via the web: https://app.webinar.net/8GArp0rQd3z or may listen to the call by dialing (1-877-870-4263). Please refer to Inhibrx, Inc. or confirmation code 10171898 when calling in. Following the webcast, the presentation may be accessed through a link on the investors section of Inhibrx's website at https://inhibrx.investorroom.com/events-and-presentations. The webcast will be available for 60 days following the event. Following the presentation, Inhibrx will update its corporate presentation within the "Investors" section of its website at www.inhibrx.com.

About INBRX-101 and AATD

INBRX-101 is a precisely engineered recombinant human AAT-Fc fusion protein designed to safely achieve and maintain levels of alpha-1 antitrypsin, or AAT, found in healthy individuals with the potential for a less frequent dosing interval compared to the weekly infusion interval of the currently available plasma-derived AAT therapies.

Alpha-1 antitrypsin deficiency, or AATD, is an inherited orphan disease affecting an estimated 100,000 patients in the United States. AATD is characterized by deficient levels of the AAT protein, which causes loss of lung tissue and function and decreased life expectancy.  Augmentation therapy with plasma-derived AAT is the current standard of care but does not maintain patients in the normal AAT range, requires frequent and inconvenient once-weekly IV dosing, and relies on plasma collection practices that might not be sustainable.

Data from the Phase 1 multiple ascending dose study of INBRX-101 at 40, 80 and 120 mg/kg IV every three weeks, showed the expected accumulation of functional AAT levels and the ability to achieve fully normal functional AAT levels in severely deficient AATD patients. Based on PK modeling, accumulation is expected to continue following subsequent doses and reach steady state after a total of approximately five to six consecutive doses, administered every three or four weeks.

Treatment was well tolerated with no severe or serious adverse events related to the study drug. Drug-related adverse events were predominantly mild and those few that were moderate in severity were all transient and reversible, with minimal or no symptomatic care. No safety-related or PK/PD-related signs of neutralizing anti-drug antibodies were observed.

In March 2022, the FDA granted orphan-drug designation for INBRX-101 for the treatment of AATD.

https://finance.yahoo.com/news/inhibrx-host-webcast-announce-regulatory-203000523.html

Adamis Reviewing Strategic Alternatives

 Adamis Pharmaceuticals Corporation (NASDAQ: ADMP), a specialty biopharmaceutical company primarily focused on developing and commercializing products in various therapeutic areas, including allergy, opioid overdose, respiratory and inflammatory disease, announced today that following the recently announced halting of the Company’s Phase 2/3 clinical trial examining the effects of Tempol in high risk subjects with early COVID-19 infection, it has initiated a process to explore a range of strategic and financing alternatives focused on maximizing stockholder value. Potential alternatives that may be explored or evaluated include a partnership or sale of one or both of the Company’s commercial products SYMJEPI® and ZIMHI®, a merger, sale, or reverse merger of the Company, and/or seeking additional financing.

As part of this process, the Company has engaged the investment bank Raymond James & Associates, Inc. to act as strategic advisor to assist the Company in evaluating certain alternatives. There can be no assurance that this strategic review process will result in the Company pursuing any transaction or that any transaction, if pursued, will be completed. The Company has not established a schedule for completion of this strategic review process, nor has it made any definitive decisions at this time related to strategic alternative transactions. If the Company is unable to complete a transaction, it may be required to seek bankruptcy protection or other alternatives for restructuring and resolving its liabilities. The Company does not expect to disclose or provide an update concerning developments related to this process until the Company enters in definitive agreements or arrangements with respect to a transaction or otherwise determines that other disclosure is necessary or appropriate. The Company is also reviewing and intends to pursue expense reduction alternatives and measures which may include, without limitation, employee headcount reductions and reduction or discontinuation of certain product development programs.

https://finance.yahoo.com/news/adamis-announces-review-strategic-alternatives-203000442.html

Oncternal: IND OKd for CAR-T B Cell Lymphoma Therapy

 Oncternal Therapeutics, Inc. (Nasdaq: ONCT), a clinical-stage biopharmaceutical company focused on the development of novel oncology therapies, today announced the receipt of a ‘Study May Proceed’ letter from the U.S. Food and Drug Administration (FDA), 30 days after submitting its Investigational New Drug (IND) application for a Phase 1/2 dose escalation study of ONCT-808, an autologous chimeric antigen receptor (CAR) T therapy targeting ROR1, in patients with aggressive B cell non-Hodgkin’s lymphoma (B NHL), including those who have failed previous CD19 CAR T treatment.

https://finance.yahoo.com/news/oncternal-therapeutics-receives-ind-clearance-203100312.html

UN urges Fed to pause interest rate hikes on global recession fears

 The Federal Reserve and other major central banks risk triggering a painful global recession followed by a period of stagnation with such aggressive interest rate increases, a United Nations agency warned Monday. 

In its annual report on the global economic outlook, the United Nations Conference on Trade and Development (UNCTAD) said the interest rate increases and austerity policies in wealthy nations represented an "imprudent gamble" that risked backfiring, particularly on lower-income nations. 

"There’s still time to step back from the edge of recession," UNCTAD Secretary-General Rebeca Grynspan said. "We have the tools to calm inflation and support all vulnerable groups. But the current course of action is hurting the most vulnerable, especially in developing countries and risks tipping the world into a global recession."

The agency estimated that a percentage point increase in the Fed's benchmark federal funds rate reduces the economic output in other wealthy nations by about 0.5%, and in poor countries by about 0.8% over the next three years. Lower-income nations will already see economic output tumbled by about $360 billion over the next three years as a result of the Fed's rate increases so far this year.

"Excessive monetary tightening could usher in a period of stagnation and economic instability," the UNCTAD said in a statement accompanying the report. "Any belief that they (central banks) will be able to bring down prices by relying on higher interest rates without generating a recession is, the report suggests, an imprudent gamble."

The Federal Reserve has embarked on one of the fastest courses in history to raise borrowing costs and slow the economy.

Officials last week approved a third consecutive 75-basis-point rate hike, lifting the federal funds rate to a range of 3.0% to 3.25% — near restrictive levels — and indicated that more super-sized increases are coming. 

There is a growing expectation on Wall Street that the Fed will trigger an economic downturn as it raises interest rates at the fastest pace in three decades to catch up with runaway inflation. 

Economic growth already contracted in the first two quarters of the year, with gross domestic product — the broadest measure of goods and services produced in a nation — contracting by 1.6% in the winter and 0.6% in the spring. 

The Federal Reserve has embarked on one of the fastest courses in history to raise borrowing costs and slow the economy. (Kevin Dietsch/Getty Images / Getty Images)

Fed chair Jerome Powell has all but conceded the central bank will tip the economy into a recession with its rapid rate hikes, warning that higher rates will cause economic "pain." 

"The chances of a soft landing are likely to diminish to the extent that policy needs to be more restrictive or restrictive for longer," Powell told reporters in Washington in September. "Nonetheless, we’re committed to getting inflation back down to 2%. We think a failure to restore price stability would mean far greater pain."

New government data released last week showed that the Fed's preferred inflation gauge, known as the Personal Consumption Expenditures (PCE) index, accelerated more than expected in August, suggesting that underlying inflationary pressures remain strong.

The PCE index showed core prices, excluding food and energy, climbed 0.6% from the previous month and rose 4.9% on an annual basis, according to the Commerce Department. 

https://www.foxbusiness.com/economy/un-urges-fed-pause-interest-rate-hikes-global-recession-fears