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The Food and Drug Administration (FDA) has approved the Alzheimer’s drug lecanemab, sold under the brand name Leqembi, making the US the first country in the world to approve the breakthrough medication.

Sold by pharma-giants Eisai and Biogen, the drug showed ability to slow down the progression of Alzheimer’s and clear plaque believed to be responsible for the disease from the brain. 

In clinical trials, those who received the drug saw their mental condition deteriorate 27 percent less than the control group. 

The drug has been deemed a game-changer in the treatment of Alzheimer’s by some experts, as there are not many available options for slowing the disease available. Eisai announced it will be priced at $26,500 for a full year of treatment. 

Some experts have cast doubts over the drug’s effectiveness, though, and safety concerns were raised after three patients died in clinical trials. Last year, Biogen’s Alzheimer’s drug Aduhelm was widely criticized after receiving the FDA greenlight.

The FDA has approved Eisai's and Biogen's new Alzheimer's drug lecanemab for use in early and middle stage patients. It slowed the progression of the disease 27 percent over 18 months in clinical trials (file photo)

The FDA has approved Eisai’s and Biogen’s new Alzheimer’s drug lecanemab for use in early and middle stage patients. It slowed the progression of the disease 27 percent over 18 months in clinical trials (file photo)

‘Alzheimer’s disease immeasurably incapacitates the lives of those who suffer from it and has devastating effects on their loved ones,’ Dr Billy Dunn, who works in the FDA’s Center for Drug Evaluation and Research, said in a statement.

‘This treatment option is the latest therapy to target and affect the underlying disease process of Alzheimer’s, instead of only treating the symptoms of the disease.’ 

Development and research on the drug was carried out by the Tokyo, Japan-based firm Eisai. It partnered with the Biogen, from Cambridge, Massachusetts, for the marketing of it.

Upon approval, the FDA has recommended the drug to be used in patients that are in the early and middle stages on Alzheimer’s. This includes at least 1.5million of the 6.5million Americans diagnosed with the condition.

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Phase III clinical trials included 1,795 patients will early Alzheimer’s. Half of participants were given 10mg/kg of the drug every two weeks.  The other group was instead given a placebo.

Researchers measured the memory, judgement and problem solving ability of participants before the trial began and again at 18 months.

They found that those who were on the drug saw their cognitive state deteriorate at a pace 27 percent slower than the placebo. 

‘The trial data has shown that lecanemab has a small but measurable impact in slowing the progression of Alzheimer’s,’ Hillary Evans, chef executive of Alzheimer’s Research UK, said in a statement.

‘In practice, lecanemab’s benefits are likely to be measured in extra months rather than years. Yet as anyone affected by Alzheimer’s knows, this time can be precious.’

Regulators in the UK are expected to clear the drug for use this year. 

It did come with some dangers, though. One-in-eight participants who used lecanemab experienced brain swelling, compared to one-in-fifty members of the control group.

These cases were not symptomatic, though, according to the pair of firm’s behind the drug.

Micro-hemorrhages, or small spurts of bleeding on the brain, were twice as common in the lecanemab group than the placebo group – with 17 percent suffering the issue.

The drug’s label will also include cautions against using blood thinners while using lecanemab – a known risk for drugs that combat amyloid beta plaques on the brain.

Two of three patients who died in clinical trials after experiencing brain bleeding and swelling were also being treated with blood thinners.

Deaths occurred at the end of the trial, at a point where they knew they were being treated with the drug and not a placebo. 

The promising trials have many experts excited, though. There are currently no effective treatments for Alzheimer’s itself – and doctors will usually just help patients manage symptoms as they continue to decline.

Institute for Clinical and Economic Review, which assesses the value of medicine, said the value of the drug is between $8,500 to $20,600 per year. This makes the $26,500 price tag set by Eisai an oversell.

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Last year, the FDA approved Aduhelm for treatment of Alzheimer’s. The controversial approval was widely criticized by experts after dubious results in trials. 

That drug targeted amyloid plaques on the brain that had already formed. It is believed that the formation of these deposits on the brain are responsible for cognitive decline.

Lecanemab instead targets the proteins that form these plaque deposit before they clump together, making experts hopeful it will be more effective than its predecessor.

The Aduhelm debacle has left a sour taste in the mouth of some Americans, though.

A congressional investigation revealed last week that the approval process for the drug was ‘rife with irregularities’.

‘The findings in this report raise serious concerns about FDA’s lapses in protocol and Biogen’s disregard of efficacy and access in the approval process for Aduhelm,’ the report, prepared by the staffs of the House Committee on Oversight and Reform and House Committee on Energy and Commerce, concluded. 

How does lecanemab work? When will it be rolled out? And is it dangerous? 

What does it do?

Lecanemab is given to patients in the earliest stages of Alzheimer’s as an infusion once a fortnight.

It is designed to clear a build up of amyloid protein — toxic plaques in the brain that are thought to cause the cruel, memory-robbing disease.

The antibody treatment, which tells the immune system to clear amyloid from the brain, is made by Japanese and US pharmaceutical firms Eisai and Biogen.

What did trials show?

The Phase III trial of lecanemab evaluated the drug’s ability to reduce cognitive and functional decline among 1,795 patients with early Alzheimer’s.

Half of participants were given 10mg/kg of the drug bi-weekly, while the others were given a placebo.

Researchers measured all the participants’ memory, judgment, problem solving and judgement before they started taking the study and again 18 months later.

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Results showed those on lecanemab saw their mental condition decline 27 per cent less than those given the dummy treatment.

Lecanemab recipients also experienced a slower build up of amyloid in their brains, scans showed.

Results were presented at a medical conference in San Francisco and published in the prestigious New England Journal of Medicine. 

Is the drug dangerous? 

As well as promising results, the trial also flagged some safety concerns.

Brain swelling was spotted among 12.5 per cent of the lecanemab group, compared to 1.7 per cent in the placebo group.

While it showed up on scans, many of these cases were not symptomatic, Eisai and Biogen insisted.

Data also showed micro-haemorrhages in the brain, or mini brain bleeds, occurred among 17 per cent in the lecanemab group, compared to 8.7 per cent of the placebo group.

Pharmaceutical bosses insisted the figures fell within an expected range.

Two patients also died while taking lecanemab during the trial, in events currently being investigated.

However, Eisai and Biogen noted that all available safety information shows the therapy is not linked with an increased risk of death.

How is it different to similar drug Aduhelm?

Both Aduhelm and lecanemab — which are both made by Eisai and Biogen — are antibodies designed to remove amyloid deposits.

However, lecanemab targets amyloid which has not yet clumped together.

Aduhelm removes amyloid plaques that built up in the brain.

Aduhelm’s approval was a rare bright spot for Alzheimer’s patients, but critics have warned about the underwhelming results of the drug and highlighted its risks.

Isn’t there already drugs for Alzheimer’s?

There are currently no Alzheimer’s treatments available, with decades of trials repeatedly failing to produce a successful remedy.

Drugs are dished out to fight off tell-tale symptoms, however.

Almost 7million Americans have dementia — with up to three quarters of cases thought to be caused by Alzheimer’s disease.

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