Illustration of USC researchers preparing dopamine-producing stem cell implants for early-stage Parkinson’s trial.
Illustration of USC researchers preparing dopamine-producing stem cell implants for early-stage Parkinson’s trial.
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USC researchers begin early trial of dopamine-producing stem cell implants for Parkinson’s

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Keck Medicine of USC researchers are testing an experimental approach to Parkinson’s disease that implants lab-grown, dopamine-producing cells into a movement-control region of the brain. The early-stage Phase 1 REPLACE trial involves up to 12 people with moderate to moderate-severe Parkinson’s disease, and the U.S. Food and Drug Administration has granted the study fast-track designation.

Parkinson’s disease is a progressive neurological condition linked to the loss of dopamine-producing brain cells, which can contribute to tremors, muscle stiffness and slowed movement. More than one million people in the United States are living with Parkinson’s disease, and about 90,000 new diagnoses are made each year. While existing treatments can ease symptoms, no therapy has been proven to slow the disease itself.

Researchers at Keck Medicine of USC are now testing whether replacing lost dopamine-producing cells could help restore dopamine signaling in the brain. The study is evaluating induced pluripotent stem cells (iPSCs)—stem cells created by reprogramming adult cells such as skin or blood cells—that are prepared in the lab to become dopamine-producing brain cells.

“If the brain can once again produce normal levels of dopamine, Parkinson’s disease may be slowed down and motor function restored,” said Brian Lee, MD, PhD, a Keck Medicine neurosurgeon and principal investigator. Xenos Mason, MD, a Keck Medicine neurologist and co-principal investigator who specializes in Parkinson’s disease, said the team believes the iPSCs “can reliably mature into dopamine-producing brain cells” and may help “jump-start” dopamine production.

During the procedure, surgeons create a small opening in the skull and use magnetic resonance imaging (MRI) guidance to implant the cells into the basal ganglia, a brain region involved in movement control. After surgery, participants are monitored closely for 12 to 15 months for changes in symptoms and for potential side effects, including dyskinesia—excess movements—or infection. Follow-up is expected to continue for up to five years.

Keck Medicine of USC is one of three U.S. sites participating in the Phase 1 REPLACE clinical trial. The therapy being studied, called RNDP-001, is produced by Kenai Therapeutics. The FDA has granted the trial fast-track designation, a regulatory status intended to help speed development and review of treatments for serious conditions.

Keck Medicine said the announcement of the study is informational and is not a call for participants.

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Early reactions on X to the Keck Medicine of USC's Phase 1 REPLACE trial of dopamine-producing stem cell implants for Parkinson’s disease consist primarily of neutral news shares linking to the article or related announcements, an official post expressing hope for new treatments, and investor interest highlighting potential biotech implications.

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Scientists in a lab celebrating conditional approval of iPS cell products for treating Parkinson's and heart disease.
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Health ministry panel conditionally approves iPS cell products

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A health ministry expert panel has conditionally approved two regenerative medicine products derived from induced pluripotent stem (iPS) cells for treating Parkinson's disease and severe heart disease. This marks a potential world first in commercializing Nobel Prize-winning stem cell technology. The approval, based on small-scale clinical trials confirming safety and presumed efficacy, requires post-market verification within seven years.

Doctors at Keck Medicine of USC are implanting lab-grown, dopamine-producing cells into the brains of people with Parkinson’s disease in an early-stage clinical trial that will enroll up to 12 participants across three U.S. sites.

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Scientists at the University of Southern California are starting a phase 2b clinical trial to test a microscopic stem cell implant aimed at restoring vision in patients with advanced dry age-related macular degeneration. The hair-thin patch seeks to replace damaged retinal cells, building on earlier research that showed safety and vision gains in some participants. Researchers hope it could offer a way to reverse vision loss where current treatments fall short.

An experimental gene therapy has demonstrated significant promise in slowing the progression of Huntington’s disease, a rare form of dementia, by about 75 percent in a late-stage trial. Researchers hailed the breakthrough as a major step forward, though challenges remain in delivery and regulatory approval. Efforts are underway to develop a more practical version of the treatment.

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Researchers are exploring CAR T-cell therapy to slow the advancement of amyotrophic lateral sclerosis (ALS) by targeting overactive immune cells in the brain. The approach aims to reduce neuron damage without curing the disease. Early studies suggest potential benefits for other neurodegenerative conditions as well.

Scientists at Tulane University and collaborating institutions have found that neurons release an enzyme called vertebrate lonesome kinase (VLK) outside cells to help switch on pain signals after injury. Removing VLK from pain-sensing neurons in mice sharply reduced post-surgical pain–like responses without impairing normal movement or basic sensation, according to a study in Science, suggesting a potential new route to more targeted pain treatments.

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SereNeuro Therapeutics has reported promising preclinical data for SN101, an induced pluripotent stem cell-based therapy for chronic osteoarthritis pain. The treatment uses engineered peripheral pain-sensing neurons that sequester inflammatory pain factors without transmitting pain signals, while releasing regenerative molecules that may help preserve cartilage, according to data presented at an International Society for Stem Cell Research symposium.

 

 

 

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