Wednesday, July 1, 2026
Synthetic stress hormone dexamethasone could reduce certain breast cancer metastases
Tuesday, June 30, 2026
Praxis Precision Medicines Announces FDA Acceptance and Priority Review of New Drug Application for Relutrigine in Patients with SCN2A and SCN8A DEEs
Praxis Precision Medicines, Inc. (NASDAQ: PRAX), a fully integrated, leading central nervous system (CNS) precision neuroscience biopharmaceutical company, today announced that the U.S. Food and Drug Administration (FDA) has accepted for priority review its New Drug Application (NDA) for relutrigine, for the treatment of SCN2A and SCN8A developmental and epileptic encephalopathies (DEEs). The FDA has set a target action date under the Prescription Drug User Fee Act (PDUFA) of September 27, 2026.
- FDA assigned PDUFA target action date of September 27, 2026
“Our first FDA acceptance of an NDA submission marks a significant milestone in our evolution to a commercial-stage company and an important step toward delivering innovative, precision neuroscience therapies to patients in need. SCN2A/8A DEEs have no currently approved targeted therapies and relutrigine, if approved, would be the first disease-modifying therapy for children suffering from these devastating and fatal conditions. We look forward to working closely with the FDA during the review process while continuing to advance our launch preparations,” said Marcio Souza, president and chief executive officer.
Relutrigine is also being investigated in broad DEEs through the EMERALD trial, which is expected to be completed by the end of 2026.
Monday, June 29, 2026
Elevar Therapeutics Announces FDA Acceptance for Review of New Drug Application for Lirafugratinib as Second-line Cholangiocarcinoma Treatment
Elevar Therapeutics, Inc., a majority-owned subsidiary of HLB Co., Ltd. and a fully integrated biopharmaceutical company dedicated to elevating treatment experiences and outcomes for patients who have limited or inadequate therapeutic options, today announced that the U.S. Food and Drug Administration (FDA) has completed its filing review of the New Drug Application (NDA) for lirafugratinib, an investigational therapy, for the treatment of patients with cholangiocarcinoma (CCA) with FGFR2 fusions or rearrangements who have received prior therapy. The FDA determined that the NDA is sufficiently complete to permit a substantive review and granted Priority Review, with a Prescription Drug User Fee Act (PDUFA) target action date of September 27, 2026.
- With Priority Review designation, FDA set a Sept. 27 PDUFA date for approval decision
- Lirafugratinib achieved a 46.5% ORR, in CCA patients with FGFR2 fusion and rearrangement
Priority Review designations are given to applications for medicines that, if approved, would lead to “significant improvements in the safety or effectiveness of the treatment” of a serious condition, according to the FDA. The Priority Review designation of the lirafugratinib NDA was supported by positive clinical data from the Phase 1/2 ReFocus trial (NCT04526106), which demonstrated a confirmed objective response rate (ORR) of 46.5% in the patients with the proposed indication. Its safety profile in the clinical data has been shown to be predictable and manageable through dose adjustments.
“Lirafugratinib has established a compelling clinical profile that differentiates it from existing treatment options,” said Dong-Gun Kim, chief executive officer of Elevar. “We are very pleased with the FDA’s priority review designation and focused on advancing the review process efficiently to bring this therapy to patients as quickly as possible.”
CCA, also known as bile duct cancer, is rare, with about 8,000 people in the U.S. diagnosed each year, according to the American Cancer Society.
Elevar Therapeutics continues to evaluate lirafugratinib in ongoing clinical development programs, including studies in other FGFR2-altered solid tumors. Any future indications will be subject to regulatory review and approval.
For more information about lirafugratinib, visit ElevarTX.com.
About Lirafugratinib
Lirafugratinib (RLY-4008) is a potent, selective, and oral small molecule inhibitor of FGFR2, a receptor tyrosine kinase that is frequently altered in certain cancers. FGFR2 is one of four members of the FGFR family, a set of closely related proteins with highly similar protein sequences and properties. Preclinically, lirafugratinib demonstrated FGFR2-dependent killing in cancer cell lines and induced regression in in vivo models with minimal inhibition of other targets, including other members of the FGFR family. In addition, lirafugratinib demonstrated strong activity against known clinical on-target resistance mutations in vitro and in vivo preclinical models. Lirafugratinib is currently being evaluated in a clinical trial to enroll additional patients with previously treated, advanced or metastatic solid tumors other than CCA harboring FGFR2 fusion or rearrangement, who have not been treated with prior FGFR inhibitors.
Saturday, June 27, 2026
How statins harm muscles—and how to stop it
University of British Columbia researchers and their collaborators at the University of Wisconsin-Madison have now pinpointed the cause. Their findings, published last week in Nature Communications, could pave the way for a new generation of statins without these side effects.
How statins affect muscle cells
The team used cryo-electron microscopy, a powerful imaging technique that reveals proteins at near-atomic detail, to capture how statins interact with a critical muscle protein called the ryanodine receptor (RyR1). This protein acts like a gatekeeper for calcium inside muscle cells, opening only when muscles need to contract. When statins bind to it, they force the gate open, causing calcium to leak continuously—a toxic effect that can damage muscle tissue.
"We were able to see, almost atom by atom, how statins latch onto this channel," said lead author Dr. Steven Molinarolo, a postdoctoral researcher in UBC's department of biochemistry and molecular biology. "That leak of calcium explains why some patients experience muscle pain or, in extreme cases, life-threatening complications."
Implications for future statin development
The study focused on atorvastatin, one of the most widely prescribed statins, but the findings suggest the effect may be common across the drug class. The researchers discovered that statins bind in a highly unusual way: Three molecules cluster together inside a pocket of the protein. The first molecule attaches when the channel is closed, priming it to open. Two more molecules then wedge in, forcing the channel wide open.
"This is the first time we've had a clear picture of how statins activate this channel," said Dr. Filip Van Petegem, senior author and professor at UBC's Life Sciences Institute. "It's a big step forward because it gives us a roadmap for designing statins that don't interact with muscle tissue."
By adjusting only those parts of the statin molecule that are responsible for the negative effects, scientists could preserve the part that lowers cholesterol while reducing the risk.
Thursday, June 25, 2026
Methamphetamine impairs dopamine uptake by targeting a protein modification
Tuesday, June 23, 2026
Polyphenol-rich diets associated with lower long-term cardiovascular disease risk
Dr. Yong Li, first author of the study, added, "This research provides strong evidence that regularly including polyphenol-rich foods in your diet is a simple and effective way to support heart health. These plant compounds are widely available in everyday foods, making this a practical strategy for most people."
The researchers note that while cardiovascular risk naturally increases with age, higher polyphenol intake was associated with a slower progression of risk over the 11-year follow-up period. They also emphasize the need for future dietary intervention studies to further validate these associations.
Wednesday, June 17, 2026
Polyphenol-rich diets associated with lower long-term cardiovascular disease risk
People who regularly consume
polyphenol-rich foods and drinks, such as tea, coffee, berries, cocoa, nuts,
whole grains and olive oil, may have better long-term heart health.
The research, led by King's
College London, found that those with higher adherence to polyphenol-rich
dietary patterns had lower predicted cardiovascular disease (CVD) risk.
Polyphenols are natural compounds
found in plants that are linked to various health benefits, including improved
heart, brain, and gut health.
The study, published today in BMC Medicine, followed
more than 3,100 adults from the TwinsUK cohort for over a decade, found that
diets rich in specific groups of polyphenols were linked to healthier blood
pressure and cholesterol profiles, contributing to lower CVD risk scores.
For the first time, the
researchers also analyzed a large number of metabolites in the urine that are
produced when the body breaks down polyphenols.
These biomarkers confirmed that
individuals with higher levels of polyphenol metabolites—especially those
derived from specific groups of polyphenols, flavonoids and phenolic acids—had
lower cardiovascular risk scores. They also had increased HDL cholesterol, also
know as "good" cholesterol.
The study used a newly developed
polyphenol dietary score (PPS) to capture intake of 20 key polyphenol-rich
foods commonly consumed in the U.K., ranging from tea and coffee to berries,
olive oil, nuts, and whole grains.
This score showed stronger
associations with cardiovascular health than estimates of total polyphenol
intake, likely because it captures overall dietary patterns rather than
individual compounds. This finding suggests that considering the whole diet
provides a more accurate picture of how polyphenol-rich foods work together to
support long-term heart health.
Professor Ana Rodriguez-Mateos,
senior author and Professor of Human Nutrition at King's College London, said,
"Our findings show that long-term adherence to polyphenol-rich diets can
substantially slow the rise in cardiovascular risk as people age. Even small,
sustained shifts towards foods like berries, tea, coffee, nuts, and whole
grains may help protect the heart over time."
Dr. Yong Li, first author of the
study, added, "This research provides strong evidence that regularly
including polyphenol-rich foods in your diet is a simple and effective way to
support heart health. These plant compounds are widely available in everyday
foods, making this a practical strategy for most people."
The researchers note that while
cardiovascular risk naturally increases with age, higher polyphenol intake was
associated with a slower progression of risk over the 11-year follow-up period.
They also emphasize the need for future dietary intervention studies to further
validate these associations.
https://link.springer.com/article/10.1186/s12916-025-04481-5
Tuesday, June 16, 2026
Lilly's announces results from Phase III clinical trial of Jaypirca
Eli
Lilly and Company announced results from the Phase 3 BRUIN CLL-322 clinical
trial of Jaypirca (pirtobrutinib), a non-covalent Bruton tyrosine kinase (BTK)
inhibitor, plus venetoclax and rituximab versus venetoclax and rituximab in
patients with relapsed or refractory chronic lymphocytic leukemia or small
lymphocytic lymphoma (CLL/SLL).
The study met its primary endpoint of independent review committee
(IRC)-assessed progression-free survival (PFS), demonstrating that the addition
of pirtobrutinib to a two-year venetoclax plus rituximab regimen reduced the
risk of disease progression or death by 45%.
These data will be highlighted in a late-breaking oral presentation at the 2026
European Hematology Association (EHA) Annual Meeting taking place in Stockholm,
Sweden, as well as featured in the meeting's press program.
"These results from BRUIN CLL-322 show that the addition of pirtobrutinib
as part of a time-limited regimen further enhanced an already effective
treatment and extended the duration of remission for patients with previously
treated CLL. Importantly, the study provides the first robust evidence for such
an approach in patients who received a prior BTK inhibitor," said Matthew
S. Davids, M.D., M.M.Sc., Chief of the Division of Lymphoma at Dana-Farber
Cancer Institute, who is the lead author on the study.
"Time-limited regimens are an important option in CLL care and provide
patients with meaningful treatment-free intervals. In the context of the modern
CLL treatment landscape, where many patients may only receive two lines of
therapy, these results speak to the potential benefits that improving
second-line therapy can have. Our study has the potential to establish a new
standard of care in this population."
BRUIN CLL-322 enrolled 639 relapsed or refractory patients, with 79.8% having
prior covalent BTK inhibitor exposure, who were randomized 1:1 to receive
pirtobrutinib plus venetoclax and rituximab (PVR, n=321) or venetoclax and
rituximab alone (VR, n=318). Patients in the PVR arm received three cycles of
pirtobrutinib and the first three cycles of rituximab before venetoclax was
introduced.
The efficacy results are based on a February 2, 2026 data cutoff. At a median
follow-up of 27.3 months, the primary endpoint of IRC-assessed PFS was
significantly improved with the addition of pirtobrutinib to VR compared to VR
alone (HR=0.55 [95% CI, 0.40-0.75]; p=0.0001). Median PFS in the PVR arm was
not reached (95% CI, 43.3-NE), versus 39.7 months (95% CI, 35.9-NE) in the VR
arm.
The PFS results were consistent across prespecified subgroups, including
patients with prior covalent BTK inhibitor exposure (PVR: not reached [95% CI,
41.5-NE] versus VR: 36.2 months [95% CI, 33.2-NE]), those who discontinued
prior covalent BTK inhibitor due to progressive disease (PVR: 43.3 months [95%
CI, 39.2-NE] versus VR: 33.2 months [95% CI, 28.3-37.5]), as well as those with
high-risk features such as unmutated IGHV, TP53 mutation and/or 17p deletion,
and/or complex karyotype. In an exploratory analysis of second-line patients
whose disease progressed after a first-line covalent BTK inhibitor, the median
PFS was not reached (95% CI, 30.1-NE) in the PVR arm and was 28.3 months (95%
CI, 20.5-NE) in the VR arm (HR=0.32 [95% CI, 0.14-0.73]), with 24-month PFS
rates of 88% (95% CI, 75.7-94.6) and 52% (95% CI, 34.7-66.2), respectively, and
consistent benefit was observed regardless of the specific prior covalent BTK
inhibitor received, said the company.
Overall survival (OS), a key secondary endpoint, was not yet mature at this
analysis (HR=0.89 [95% CI, 0.57-1.40]), and final testing of OS superiority is
planned at a future date. An additional secondary endpoint, time to next
treatment (TTNT), consistently favored the pirtobrutinib combination regimen.
The overall safety profile of this regimen in BRUIN CLL-322 was consistent with
the known safety profile of each medicine, with little additive toxicity
observed with the addition of pirtobrutinib to venetoclax and rituximab. Rates
of Grade =3 adverse events (AEs) were similar with PVR compared to VR (78.8%
versus 73.0%, respectively). Low rates of any grade atrial fibrillation/flutter
(3.5% versus 2.6%, respectively), hypertension (12.0% versus 7.4%,
respectively), and hemorrhage (14.2% versus 10.6%, respectively) were seen with
PVR versus VR.
Grade =3 clinical AEs of interest included neutropenia (50.3% versus 43.7%,
respectively) and tumor lysis syndrome (0.9% versus 3.9%, respectively) in the
PVR and VR arms. Discontinuation rates due to treatment-related AEs were
similar across the PVR and VR study arms (5.4% versus 5.1%, respectively). The
addition of pirtobrutinib to VR also allowed for downgrading of tumor lysis
risk, with 78% of high-risk patients downgraded to medium (n=20) or low risk
(n=18), and 61% of medium-risk patients downgraded to low risk.
"These remarkable findings support the potential addition of two years of
Jaypirca to a time-limited venetoclax-based regimen in relapsed or refractory
CLL," said Jacob Van Naarden, executive vice president and president of
Lilly Oncology.
"BRUIN CLL-322 enrolled a mostly covalent BTK inhibitor-pretreated
population, ensuring that these results have applicability to the modern CLL
treatment landscape where covalent BTK inhibitor use is now common.
Additionally, these data further strengthen the unique body of evidence for
Jaypirca across the CLL continuum, from monotherapy to combination therapy and
across multiple settings where CLL patients need effective treatment."
Lilly plans to submit results from the BRUIN CLL-322 study to global regulatory
authorities with the goal of further expanding Jaypirca's label. The company is
studying Jaypirca in CLL/SLL in multiple Phase 3 studies.
Alternative sweetener sorbitol linked to liver disease
The role of gut bacteria
For starters, although most of the research on sorbitol metabolism has focused on its production due to glucose overload in pathological settings such as diabetes, sorbitol can be naturally produced in the gut from glucose after eating, Patti said.
The enzyme that produces sorbitol has a low affinity for glucose, so glucose levels must be high for it to take effect. That is why sorbitol production has primarily been associated with diabetes, where blood glucose levels can become elevated. But, even in healthy settings, glucose levels in the gut become high enough after feeding to drive sorbitol production within the intestine, according to the team's zebrafish experiments.
"It can be produced in the body at significant levels," said Patti. "But if you have the right bacteria, turns out, it doesn't matter."
Sorbitol-degrading Aeromonas bacterial strains convert the sugar alcohol into a harmless bacterial byproduct. "However, if you don't have the right bacteria, that's when it becomes problematic. Because in those conditions, sorbitol doesn't get degraded and as a result, it is passed on to the liver," he said.
Once in the liver, it is converted to a derivative of fructose. It's important to determine if alternative sweeteners are providing a healthy alternative to table sugar, since people with diabetes and other metabolic disorders may be relying on them as "sugar-free" products.
Dietary habits and health implications
Gut bacteria do a good job of clearing sorbitol when it is present at modest levels, such as those found in fruit. But problems arise when sorbitol quantities become higher than what gut bacteria can degrade. This can occur when excessive amounts of glucose are consumed in the diet, which lead to high levels of glucose-derived sorbitol, or when dietary sorbitol itself is too high.
The more glucose and sorbitol consumed, then, even if someone has the friendly bacteria that clears it, those gut microbes may be overwhelmed with the task.
Avoiding both sugar and alternative sweeteners is increasingly complicated, as many foods are packed with multiple varieties of all the above. Patti was bemused to discover his own favorite protein bar was chock full of sorbitol.
The lab will need to do more research to understand the specific mechanisms for how bacteria clears sorbitol, but the basic idea that these sugar alcohols, called polyols, are harmlessly expelled, may not hold true. "We do absolutely see that sorbitol given to animals ends up in tissues all over the body," he said.
Bottom line: it's becoming more apparent that "there is no free lunch" when trying to find sugar alternatives, with many roads leading to liver dysfunction.
Monday, June 15, 2026
Drug developed for inherited bleeding disorder shows promising trial results
Study explores new treatment option
A study from Mass General Brigham tested the safety and efficacy of engasertib, a drug specifically designed to target the condition. This 75-participant, double-blind, placebo-controlled trial found engasertib was safe and decreased nosebleed frequency and duration.
Their results are published in the New England Journal of Medicine.
"HHT causes serious vascular abnormalities throughout the body, often leading to dangerous, abnormal blood vessels in the brain, lungs, and liver, which bring with them major complications including stroke, heart failure, and brain hemorrhage—yet an FDA-approved treatment doesn't exist," said co-lead principal investigator and first author Hanny Al-Samkari, MD, a Mass General Brigham hematologist and co-director of the Hereditary Hemorrhagic Telangiectasia Center of Excellence at Massachusetts General Hospital.
"This engasertib trial is a step toward a better life for these patients, and I'm thrilled we found it to be both safe and effective at decreasing bleeding in HHT."
How engasertib targets HHT
HHT's impact can be both pervasive and devastating. HHT mutates the activin receptor-like kinase 1 (ALK1) pathway, which normally controls new blood vessel formation and vascular maintenance. With these mutations come an excess of the protein AKT—which is the target of engasertib, an oral, once-daily AKT inhibitor developed by Vaderis Therapeutics.
To test the drug's safety and efficacy, 75 people with HHT were randomly split into three treatment groups to take 30 milligrams of engasertib, 40 milligrams of engasertib, or placebo once daily for 12 weeks. The trial was sponsored by Vaderis Therapeutics and was designed by the sponsor in collaboration with the investigators.
Results and future implications
At the end of 12 weeks, patients who received engasertib experienced fewer and shorter nosebleeds relative to the placebo group. Additionally, 61% of the 40-milligram group and 37% of the 30-milligram group reported feeling "much better" at the end of 12 weeks, while only 27% of the placebo group said the same.
The drug was deemed safe, with the most common side effect being a mild and reversible rash and serious adverse events not differing significantly between treatment and placebo groups.
The trial positions engasertib as a potential future treatment for patients with HHT, but bigger, longer studies are still needed to validate the findings.
Saturday, June 13, 2026
Eylea HD (aflibercept) Approved by FDA for the Treatment of Macular Edema Following Retinal Vein Occlusion (RVO) and for Monthly Dosing Across Approved Indications
Aflibercept is a combination of fluorouracil, leucovorin, and irinotecan,
Thursday, June 11, 2026
Ofirnoflast (HT-6184) Receives Orphan Drug Designation from U.S. FDA for Myelodysplastic Syndromes
Halia Therapeutics, Inc., a clinical-stage biopharmaceutical company pioneering therapies that target the root causes of inflammation-driven diseases, today announced that the U.S. Food and Drug Administration (FDA) has granted Orphan Drug Designation (ODD) to its investigational medicine ofirnoflast (HT-6184) for the treatment of Myelodysplastic Syndromes (MDS) — a group of bone marrow disorders characterized by ineffective blood cell production and a risk of progression to acute myeloid leukemia (AML).
The FDA grants Orphan Drug Designation to therapies intended for the treatment, prevention, or diagnosis of rare diseases or conditions that affect fewer than 200,000 people in the United States at the time of designation.
"This designation underscores the potential of our approach in Myelodysplastic Syndromes and supports our commitment to developing new treatment options for patients living with MDS," said David Bearss, PhD, Chief Executive Officer of Halia Therapeutics. "Ofirnoflast represents a first-in-class approach to modulating inflammasome biology, an upstream driver of inflammation, with the goal of restoring healthy bone marrow function."
Ofirnoflast is a selective NEK7 allosteric modulator designed to prevent the formation and promote the disassembly of the NLRP3 inflammasome, a central driver of chronic inflammation in multiple diseases. In MDS, inflammasome activation is increasingly recognized as a key contributor to ineffective hematopoiesis and bone marrow failure. By modulating NEK7, ofirnoflast aims to restore immune balance and improve blood-cell production without broad immunosuppression.
"Inflammasome biology represents a promising frontier for hematologic innovation," said Alan F. List, MD, member of Halia Therapeutics' Scientific Advisory Board and former President and CEO of Moffitt Cancer Center. "Ofirnoflast's approach is distinctive in that it seeks to modulate the underlying inflammatory drivers of MDS rather than just its downstream effects. This strategy has the potential to redefine how inflammation-linked bone marrow failure is treated."
Under the FDA's Orphan Drug Act, orphan-drug status provides several incentives, including tax credits for qualified clinical testing, exemption from FDA user fees, and potential for seven years of U.S. market exclusivity upon approval. The FDA also administers grant programs to support clinical research and advance the development of therapies for rare diseases.
About Myelodysplastic Syndromes (MDS)
Myelodysplastic Syndromes are a group of bone marrow disorders characterized by defective blood-cell formation, leading to anemia, infection risk, and bleeding complications. MDS primarily affects older adults and can progress to acute myeloid leukemia (AML). Current therapies, including hypomethylating agents and growth factors, often provide limited benefit and do not address the underlying inflammatory biology of the disease.
About Ofirnoflast (HT-6184)
Ofirnoflast (HT-6184) is Halia Therapeutics' lead investigational compound and a first-in-class NEK7 modulator that regulates activation of the NLRP3 inflammasome — an upstream molecular complex involved in chronic inflammation. The drug is currently being evaluated across multiple disease areas, including:
- Myelodysplastic Syndromes (MDS) – completed Phase 2 study evaluating safety and hematologic outcomes
- Obesity (in combination with semaglutide) – ongoing Phase 2 study targeting adipose inflammation and metabolic dysregulation
- Alzheimer's Disease – early-stage program focused on genetically at-risk populations
About Halia Therapeutics, Inc.
Halia Therapeutics is a clinical-stage biopharmaceutical company developing therapies that leverage genetic resilience to restore the body's natural ability to resolve inflammation. By targeting the NEK7–NLRP3 inflammasome axis, Halia's pipeline addresses a spectrum of chronic inflammatory and degenerative diseases, including hematologic disorders, metabolic disease, and neurodegeneration.
Monday, June 8, 2026
Genentech’s Fenebrutinib Shows Unprecedented Positive Phase III Results as the Potential First and Only BTK Inhibitor in Both Relapsing and Primary Progressive Multiple Sclerosis
Saturday, June 6, 2026
U.S. Food and Drug Administration Accepts Bristol Myers Squibb's New Drug Application for Iberdomide in Patients with Relapsed or Refractory Multiple Myeloma
Bristol Myers Squibb (NYSE: BMY) today announced that the U.S. Food and Drug Administration (FDA) has accepted a New Drug Application (NDA) for iberdomide combined with standard treatment (daratumumab + dexamethasone - IberDd) in patients with relapsed or refractory multiple myeloma (RRMM). Iberdomide is part of an investigational, new class of medicines called cereblon E3 ligase modulator (CELMoD) agents. The FDA has granted a Prescription Drug User Fee Act (PDUFA) date of August 17, 2026 for this indication.
- Iberdomide has the potential to be the first approved CELMoD agent
- The U.S. FDA has granted Breakthrough Therapy Designation and Priority Review for this indication and assigned a target action date of August 17, 2026
“The FDA’s acceptance of this application is a testament to the potential of iberdomide, in combination with anti-CD38 monoclonal antibodies, as a novel, potent, oral treatment option, with a manageable safety profile, for patients with multiple myeloma,” said Cristian Massacesi, executive vice president and chief medical officer, Bristol Myers Squibb. “Furthermore, our filing for iberdomide based on the MRD endpoint, underscores our commitment to pioneering new ways of advancing life-saving therapies for patients living with cancer.”
The filing was based on results from a planned analysis of MRD negativity rates in the Phase 3 EXCALIBER-RRMM study evaluating iberdomide as a treatment for RRMM patients. The EXCALIBER-RRMM trial is ongoing and patients continue to be evaluated for progression-free survival (PFS).
The FDA also granted Breakthrough Therapy designation for iberdomide based on these data.
This review is being conducted under the FDA’s Project Orbis initiative, which enables concurrent review by the health authorities in several other countries.