A growing number of studies are exploring the role of perineuronal nets (PNNs) in Parkinson’s disease. PNNs are specialized structures in the brain’s extracellular matrix that limit synaptic plasticity, like a stabilizing "glue" between neurons. While this stabilization helps maintain brain function in adulthood, it also reduces the brain’s ability to rewire or adapt, which is important for learning and recovery after injury.
PNNs are especially important during brain development. They help close the "critical period" of heightened plasticity in childhood. Interestingly, while PNNs are degraded in adults, this plasticity can be partially restored. For example, PNN removal can promote recovery in stroke models
PNNs serve multiple functions: protecting neurons from oxidative stress and harmful molecules, regulating plasticity, and helping stabilize long-term memories. Abnormal changes in PNNs have been observed in aging and various neurological conditions, making them a promising target for therapeutic intervention.
In the cerebral cortex, PNNs are primarily found around inhibitory interneurons, particularly those that produce the protein parvalbumin. These interneurons help maintain a balance between excitatory and inhibitory signals in the brain. In Parkinson’s disease, where dopamine-producing neurons in the substantia nigra are lost, this balance is disrupted—suggesting that changes in PNNs may contribute to the disorder.
A recent study investigated the effects of temporarily reducing PNNs in the primary motor cortex (M1) of healthy adult mice using chondroitinase ABC (ChABC). This intervention caused temporary impairments in motor function, suggesting that PNNs contribute to motor stability. Using ChABC makes sense as perineuronal nets are composed of chondroitin sulfate proteoglycans, and ChABC is an enzyme that digests them. Chondroitinase treatment has been shown to allow adults' vision to be restored; moreover, there is some evidence that Chondroitinase could be used for the treatment of spinal injuries.
The researchers created a Parkinson’s disease mouse model by damaging one side of the midbrain of mice with 6-hydroxydopamine (6-OHDA). Two weeks after the lesion, PNN levels dropped in both hemispheres of the motor cortex but returned to normal within five weeks.
The researchers then applied ChABC to reduce PNNs again in the motor cortex and paired this with motor training. This combination improved motor recovery slightly in the Parkinsonian mice. The improvement was linked to an increase in parvalbumin interneurons surrounded by PNNs and a normalization of excitatory signals at their cell bodies. These findings suggest that PNNs respond dynamically—first to the injury and later to therapeutic intervention—and that manipulating them could help restore motor function.
In summary, perineuronal nets in the motor cortex appear to play a subtle but significant role in regulating movement. Modifying their structure could open new avenues for motor rehabilitation in Parkinson’s disease.
This study investigates whether acupuncture has any impact on long-term health outcomes, such as mortality, disease progression, or complications, in individuals newly diagnosed with Parkinson’s disease (PD) in South Korea. Indeed, it is unclear what constitutes an effective acupuncture session for Parkinson's disease, and individuals interested should receive at least one session every two months. It is commonly believed that in PD, reduced mobility due to tremors, postural imbalance, and rigidity likely contributes to poor circulation and decreased gastrointestinal motility, leading to bowel obstructions and impaired swallowing, which can, in turn, result in recurrent aspiration pneumonia. The benefits may arise from the fact that people with PD might find it easier to move.
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Les progrès réalisés dans la chimie médicinale des ASO ont amélioré leur profil pharmacodynamique, permettant ainsi une administration sûre et efficace au système nerveux central. Les thérapies ASO pour la SLA se sont rapidement développées au cours des deux dernières décennies, et les ASO ciblant SOD1, C9orf72 et ATXN2 sont actuellement en essais cliniques pour les formes familiales ou sporadiques de SLA.
Identifié par criblage in vitro, l'ASO ION363 développé par la société IONIS qui a aussi développé Tofersen, cible le 6e intron de FUS (SLA avec une mutation P525L).
ION363 réduit les taux de protéines de liaison à l'ARN insolubles et insolubles associées aux agrégats, telles que hnRNPA1 et ralentit la neurodégénérescence des motoneurones lombaires et la perte d'innervation de la jonction neuromusculaire.
The researchers specifically focused on molecules that could reduce or reverse stress granule formation, particularly those that act directly on stress granule proteins and may be useful as therapeutic agents. From the initial screening, lipoamide emerged as a novel, potent modulator of stress granules.
Once lipoamide was identified as a hit, the researchers sought to determine its effects in cells regarding specificity, potency, intracellular localization, and its effects on other cellular condensates.
The hippocampus, a small, seahorse-shaped structure buried deep within the brain, is best known for its role in memory formation and learning. It is an exceptionally vulnerable structure, with perfusion deficits often observed in diseases related to learning and memory. However, a brain affected by Alzheimer's disease tends to exhibit at least moderate cortical atrophy, including in the precuneus and posterior cingulate gyrus. It should be noted that the posterior cingulate gyrus is adjacent to the hippocampus.