The brain penetrant PPARγ agonist leriglitazone restores multiple altered pathways in models of X-linked adrenoleukodystrophy.
Laura Rodríguez-PascauAnna VilaltaMarc CerradaEstefania TraverSonja Forss-PetterIsabelle WeinhoferJan BauerStephan KempGuillem PinaSílvia PascualUwe MeyaPatricia L MusolinoJohannes BergerMarc MartinellPilar PizcuetaPublished in: Science translational medicine (2021)
X-linked adrenoleukodystrophy (X-ALD), a potentially fatal neurometabolic disorder with no effective pharmacological treatment, is characterized by clinical manifestations ranging from progressive spinal cord axonopathy [adrenomyeloneuropathy (AMN)] to severe demyelination and neuroinflammation (cerebral ALD-cALD), for which molecular mechanisms are not well known. Leriglitazone is a recently developed brain penetrant full PPARγ agonist that could modulate multiple biological pathways relevant for neuroinflammatory and neurodegenerative diseases, and particularly for X-ALD. We found that leriglitazone decreased oxidative stress, increased adenosine 5'-triphosphate concentration, and exerted neuroprotective effects in primary rodent neurons and astrocytes after very long chain fatty acid-induced toxicity simulating X-ALD. In addition, leriglitazone improved motor function; restored markers of oxidative stress, mitochondrial function, and inflammation in spinal cord tissues from AMN mouse models; and decreased the neurological disability in the EAE neuroinflammatory mouse model. X-ALD monocyte-derived patient macrophages treated with leriglitazone were less skewed toward an inflammatory phenotype, and the adhesion of human X-ALD monocytes to brain endothelial cells decreased after treatment, suggesting the potential of leriglitazone to prevent the progression to pathologically disrupted blood-brain barrier. Leriglitazone increased myelin debris clearance in vitro and increased myelination and oligodendrocyte survival in demyelination-remyelination in vivo models, thus promoting remyelination. Last, leriglitazone was clinically tested in a phase 1 study showing central nervous system target engagement (adiponectin increase) and changes on inflammatory biomarkers in plasma and cerebrospinal fluid. The results of our study support the use of leriglitazone in X-ALD and, more generally, in other neuroinflammatory and neurodegenerative conditions.
Keyphrases
- oxidative stress
- cerebral ischemia
- spinal cord
- blood brain barrier
- endothelial cells
- mouse model
- white matter
- resting state
- cerebrospinal fluid
- multiple sclerosis
- dna damage
- subarachnoid hemorrhage
- insulin resistance
- ischemia reperfusion injury
- metabolic syndrome
- induced apoptosis
- diabetic rats
- spinal cord injury
- functional connectivity
- gene expression
- dendritic cells
- traumatic brain injury
- clinical trial
- randomized controlled trial
- adipose tissue
- risk assessment
- high glucose
- signaling pathway
- pseudomonas aeruginosa
- peripheral blood
- immune response
- staphylococcus aureus
- replacement therapy
- lps induced
- combination therapy
- inflammatory response
- cognitive impairment
- skeletal muscle
- biofilm formation
- human health