AAN 2026: Crexont linked to more on time in new Parkinson’s study

Trial shows longer symptom control and fewer daily fluctuations

Written by Marisa Wexler, MS |

An illustration of the brain with the letters AAN alongside, representing the American Academy of Neurology meeting.
  • Crexont is an extended-release formulation of levodopa and carbidopa used to treat Parkinson’s symptoms.
  • Switching to Crexont was linked to more good on time and less off time, as well as fewer motor fluctuations.
  • Interim study results suggest switching therapies may improve daily symptom control in Parkinson’s patients.

People with Parkinson’s disease who switch from other formulations of levodopa to Crexont may experience improvements in daily symptom control, according to new data from an ongoing clinical trial.

“Crexont substantially increased [good on] time, reduced [off time], and improved motor function in [Parkinson’s] patients across all therapy groups, confirming that switching patients from other levodopa-based therapies to Crexont offers meaningful improvements in symptom control through the day,” the researchers wrote.

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Findings presented at AAN highlight therapy switch

A team including scientists at Amneal Pharmaceuticals, the company that sells Crexont, presented the findings at the American Academy of Neurology (AAN) annual meeting, in a poster titled, “Switching to CREXONT Substantially Improves ‘Good On’ Time and Reduces Motor Fluctuations in Parkinson’s Disease: Interim Results from the Real-world ELEVATE-PD Phase Four Study.”

Parkinson’s is a neurological disease marked by the loss of brain cells that make a key signaling molecule called dopamine. Low dopamine levels disrupt normal brain signaling, ultimately leading to Parkinson’s symptoms.

Levodopa is a mainstay treatment for Parkinson’s that works by giving the brain more of the raw material it needs to make dopamine. It is often given in combination with other medications that help more levodopa reach the brain, such as carbidopa or COMT (catechol-o-methyl transferase) inhibitors.

Although levodopa can be effective for easing Parkinson’s symptoms, it may become less effective over time. This can lead to what is called off time, when symptoms aren’t well controlled between scheduled doses. Long-term use can also lead to dyskinesia, a side effect marked by uncontrolled, jerking movements.

Crexont is an extended-release formulation of levodopa and carbidopa designed to help maintain steady levels of the medication in the body, improve absorption, and extend its effects, which may allow for fewer daily doses. The therapy was approved in the U.S. in 2024.

Phase 4 study examines real-world use of Crexont

An ongoing, open-label Phase 4 clinical trial called ELEVATE-PD is evaluating the safety and efficacy of Crexont in people with Parkinson’s who switch to this new formulation from other levodopa-based therapies. At the AAN meeting, researchers presented interim data from the first 111 participants in the study.

Prior to entering ELEVATE-PD, most patients had been taking instant-release formulations of levodopa plus carbidopa. The study also included some patients taking levodopa plus COMT inhibitors, as well as those taking Rytary, another approved extended-release formulation of carbidopa and levodopa, sold by Amneal.

Upon entering the study, participants undergo a five-week period during which Crexont doses are adjusted, then receive treatment with the optimal dose for about a year.

The interim analyses indicated that patients switching to Crexont tended to experience a substantial increase in daily good on time, meaning periods when symptoms are well-controlled without problematic dyskinesia.

Switch linked to gains in daily symptom control

Specifically, data showed that daily good on time increased by more than three hours on average within six weeks of starting Crexont. Daily off time decreased by more than three hours on average. The researchers noted that these improvements were sustained, with longer continuous periods of symptom control reported during the day.

These improvements in daily symptom control were seen regardless of which treatment patients had been on before switching to Crexont. Analyses also showed that patients switching to Crexont experienced fewer motor fluctuations, and standard measures of motor symptom severity indicated an easing of symptoms. Safety data were in line with Crexont’s known profile.

“The longer duration of continuous [good on] intervals and reduced daily motor fluctuations after switching to Crexont provides patients with [Parkinson’s] greater uninterrupted time and predictability to perform their daily activities,” the researchers concluded. “Overall, switching patients with motor fluctuations from other levodopa-based therapies to Crexont offers meaningful improvements in symptom control throughout the day.”

Marisa Wexler, MS avatar

About the Author

Marisa Wexler, MS Marisa holds a Master of Science in cellular and molecular pathology from the University of Pittsburgh, where she studied novel genetic drivers of ovarian cancer. Her areas of expertise include cancer biology, immunology, and genetics, and she has worked as a science writing and communications intern for the Genetics Society of America.

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Donald L Stegemoller Jr avatar

Donald L Stegemoller Jr

Huge improvement with Crexont, better mobility and less downtime, very expensive though.

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Carole Ries avatar

Carole Ries

I switched from Rytary to Crexont and feel that I am “on” for most of the day.

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KD avatar

KD

Sure wish Crexont was more affordable.

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Jennifer White avatar

Jennifer White

I am still trying to find the right dose of Crexont. For me, the highest dose 87.5/350 causes dyskinesia and dystonia at the same time. I also get a little manic, talk too fast, and cry easily. The lower dose 70/280, doesn’t kick in for an hour or so, but the dyskinesia is less and my mood is more stable. My best results come when I take the 70/280 dose of Crexont with a half tablet of carbidopa /levodopa (sinimet). It seems to speed up the immediate release and increases my on time.
Also the slow release stage happens in the small intestine. Most pwp suffer from constipation which would seem to slow absorption. I would love to hear some success stories.

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Tina Fischer avatar

Tina Fischer

My Neurologist's PA gave me samples of Crexont (87.5/350) which I began to take Saturday March 28th, taking it 3 times daily. The first day I experienced a serious case of brain fog all day long. The next day it was gone. Over the next week or so I dealt with some nausea on and off, but I continued ta take it. During the first week of taking it, I began to feel more steady on my feet (better balance), and I realized on Friday April 17th that my feet are no longer freezing, which began about 6 months ago and I'm not shuffling my feet any longer. In fact, I can even march. The Parkinson's symptoms began in January 2019 and I was diagnosed in February 2020. I especially like that I only need it 3 times a day and I'm no longer having to deal with taking meds 4 times a day and dealing with timing my protein intake. My brain just feels so much better in less than a month. Thank you so much!! Tina

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