Assessment of 18F-PBR-111 in the Cuprizone Mouse Model of Multiple Sclerosis

Abstract: The study aims to assess site assessment of the performance of 18F-PBR-111 as a neuroinflammation marker in the cuprizone mouse model of multiple sclerosis (MS). 18F-PBR-111 PET imaging has not been well evaluated in multiple sclerosis applications both in preclinical and clinical research. This study will help establish the potential utility of 18F-PBR-111 PET in preclinical MS research and future animal and future human applications.18F-PBR-111 PET/CT was conducted at 3.5 weeks (n = 7) and 5.0 weeks (n = 7) … Show more

“…Lastly, the work by Jewells et al utilizes novel in vivo detection of microglia through PET detection of 18-kDa translocator protein (TSPO) radiotracer in demyelinating mice model of MS [ 13 ]. TSPO, also called the peripheral benzodiazepine receptor (PBR), is highly expressed in activated microglia and a known prognostic factor in MS pathology.…”

“…TSPO, also called the peripheral benzodiazepine receptor (PBR), is highly expressed in activated microglia and a known prognostic factor in MS pathology. For this purpose, the Authors develop a specific 18F-PBR-111 radiotracer and demonstrated significant uptake after demyelination that was spatially correlated with positive histopathological staining of CD11b (activated microglia) and F4/80 (macrophages) [ 13 ]. This increase in uptake was greater when compared to control mice and located in the corpus callosum and striatum [ 13 ].…”

“…For this purpose, the Authors develop a specific 18F-PBR-111 radiotracer and demonstrated significant uptake after demyelination that was spatially correlated with positive histopathological staining of CD11b (activated microglia) and F4/80 (macrophages) [ 13 ]. This increase in uptake was greater when compared to control mice and located in the corpus callosum and striatum [ 13 ]. Therefore, PET 18F-PBR-111 could have potential as an in vivo imaging biomarker for MS neuroinflammation and an assessment of microglial activity.…”

Editorial of Special Issue “Multiple Sclerosis: From Diagnostic Biomarkers to Imaging and Clinical Predictors”

“…Lastly, the work by Jewells et al utilizes novel in vivo detection of microglia through PET detection of 18-kDa translocator protein (TSPO) radiotracer in demyelinating mice model of MS [ 13 ]. TSPO, also called the peripheral benzodiazepine receptor (PBR), is highly expressed in activated microglia and a known prognostic factor in MS pathology.…”

“…TSPO, also called the peripheral benzodiazepine receptor (PBR), is highly expressed in activated microglia and a known prognostic factor in MS pathology. For this purpose, the Authors develop a specific 18F-PBR-111 radiotracer and demonstrated significant uptake after demyelination that was spatially correlated with positive histopathological staining of CD11b (activated microglia) and F4/80 (macrophages) [ 13 ]. This increase in uptake was greater when compared to control mice and located in the corpus callosum and striatum [ 13 ].…”

“…For this purpose, the Authors develop a specific 18F-PBR-111 radiotracer and demonstrated significant uptake after demyelination that was spatially correlated with positive histopathological staining of CD11b (activated microglia) and F4/80 (macrophages) [ 13 ]. This increase in uptake was greater when compared to control mice and located in the corpus callosum and striatum [ 13 ]. Therefore, PET 18F-PBR-111 could have potential as an in vivo imaging biomarker for MS neuroinflammation and an assessment of microglial activity.…”

Editorial of Special Issue “Multiple Sclerosis: From Diagnostic Biomarkers to Imaging and Clinical Predictors”

Addressing Biological Questions with Preclinical Cancer Imaging