An in vivo pig model for testing novel PET radioligands targeting cerebral protein aggregates

Author:

Raval Nakul RaviORCID,Nasser Arafat,Madsen Clara AabyeORCID,Beschorner Natalie,Beaman Emily EufaulaORCID,Juhl MortenORCID,Lehel SzabolcsORCID,Palner MikaelORCID,Svarer Claus,Plavén-Sigray PontusORCID,Jørgensen Louise MøllerORCID,Knudsen Gitte MoosORCID

Abstract

AbstractPositron emission tomography (PET) has become an essential clinical tool for diagnosing neurodegenerative diseases with abnormal accumulation of proteins like amyloid-β or tau. Despite many attempts, it has not been possible to develop an appropriate radioligand for imaging aggregated α-synuclein in the brain for diagnosing, e.g., Parkinson’s Disease. Access to a large animal model with α-synuclein pathology would critically enable a more translationally appropriate evaluation of novel radioligands.We here establish a pig model with cerebral injections of α-synuclein preformed fibrils or brain homogenate from postmortem human brain tissue from individuals with Alzheimer’s disease (AD) or dementia with Lewy body (DLB) into the pig’s brain, using minimally invasive surgery and validated against saline injections. In the absence of a suitable α-synuclein radioligand, we validated the model with the unselective amyloid-β tracer [11C]PIB, which has a high affinity for β-sheet structures in aggregates. Gadolinium-enhanced MRI confirmed that the blood-brain barrier was intact. A few hours post-injection, pigs were PET scanned with [11C]PIB. Quantification was done with Logan invasive graphical analysis and simplified reference tissue model 2 using the occipital cortex as a reference region. After the scan, we retrieved the brains to confirm successful injection using autoradiography and immunohistochemistry.We found four times higher [11C]PIB uptake in AD-homogenate-injected regions and two times higher uptake in regions injected with α-synuclein-preformed-fibrils compared to saline. The [11C]PIB uptake was the same in non-injected (occipital cortex, cerebellum) and injected (DLB-homogenate, saline) regions. With its large brains and ability to undergo repeated PET scans as well as neurosurgical procedures, the pig provides a robust, cost-effective, and good translational model for assessment of novel radioligands including, but not limited to, proteinopathies.

Publisher

Cold Spring Harbor Laboratory

Reference50 articles.

1. Alstrup, A. K. O. , Munk, O. L. , and Landau, A. M. (2018). PET radioligand injection for pig neuroimaging. of Laboratory Animal … 44. Available at: http://sjlas.org/index.php/SJLAS/article/view/509.

2. Pathoanatomy of Parkinson’s disease

3. Developing a novel alpha‐synuclein positron emission tomography (PET) tracer for the diagnosis of synucleinopathies

4. Imaging HDACs In Vivo: Cross-Validation of the [11C]Martinostat Radioligand in the Pig Brain

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