Peripheral expression of brain-penetrant progranulin rescues pathologies in mouse models of frontotemporal lobar degeneration.
Marvin ReichMatthew J SimonBeate PolkeIñaki ParisGeorg WernerChristian SchraderLena SpiethSonnet S DavisSophie RobinsonGabrielly Lunkes de MeloLennart SchlaphoffKatrin BuschmannStefan A BerghoffTodd LoganBrigitte NuscherLis de WeerdDieter EdbauerMikael SimonsJung H SuhThomas SandmannMihalis S KariolisSarah L DeVosJoseph W LewcockDominik PaquetAnja CapellGilbert Di PaoloChristian HaassPublished in: Science translational medicine (2024)
Progranulin (PGRN) haploinsufficiency is a major risk factor for frontotemporal lobar degeneration with TAR DNA-binding protein 43 (TDP-43) pathology (FTLD- GRN ). Multiple therapeutic strategies are in clinical development to restore PGRN in the CNS, including gene therapy. However, a limitation of current gene therapy approaches aimed to alleviate FTLD-associated pathologies may be their inefficient brain exposure and biodistribution. We therefore developed an adeno-associated virus (AAV) targeting the liver (L) to achieve sustained peripheral expression of a transferrin receptor (TfR) binding, brain-penetrant (b) PGRN variant [AAV(L):bPGRN] in two mouse models of FTLD- GRN , namely, Grn knockout and GrnxTmem106b double knockout mice. This therapeutic strategy avoids potential safety and biodistribution issues of CNS-administered AAVs and maintains sustained concentrations of PGRN in the brain after a single dose. AAV(L):bPGRN treatment reduced several FTLD- GRN -associated pathologies including severe motor function deficits, aberrant TDP-43 phosphorylation, dysfunctional protein degradation, lipid metabolism, gliosis, and neurodegeneration in the brain. The potential translatability of our findings was tested in an in vitro model using cocultured human induced pluripotent stem cell (hiPSC)-derived microglia lacking PGRN and TMEM106B and wild-type hiPSC-derived neurons. As in mice, aberrant TDP-43, lysosomal dysfunction, and neuronal loss were ameliorated after treatment with exogenous TfR-binding protein transport vehicle fused to PGRN (PTV:PGRN). Together, our studies suggest that peripherally administered brain-penetrant PGRN replacement strategies ameliorate FTLD- GRN relevant phenotypes including TDP-43 pathology, neurodegeneration, and behavioral deficits. Our data provide preclinical proof of concept for the use of this AAV platform for treatment of FTLD- GRN and potentially other CNS disorders.
Keyphrases
- gene therapy
- binding protein
- resting state
- white matter
- amyotrophic lateral sclerosis
- functional connectivity
- cerebral ischemia
- stem cells
- mouse model
- blood brain barrier
- wild type
- poor prognosis
- endothelial cells
- inflammatory response
- multiple sclerosis
- oxidative stress
- spinal cord
- mesenchymal stem cells
- machine learning
- type diabetes
- adipose tissue
- bone marrow
- subarachnoid hemorrhage
- transcription factor
- artificial intelligence
- early onset
- amino acid
- small molecule
- long non coding rna
- fatty acid
- brain injury
- neuropathic pain
- data analysis
- single cell
- cell free
- pet ct