Your search keyword '"positron emission tomography (PET)"' showing total 3 results

1. In Vivo Preclinical Assessment of β-Amyloid–Affine [ 11 C]C-PIB Accumulation in Aluminium-Induced Alzheimer's Disease-Resembling Hypercholesterinaemic Rat Model.

Author

Képes, Zita, Barkóczi, Alexandra, Szabó, Judit P., Kálmán-Szabó, Ibolya, Arató, Viktória, Jószai, István, Deák, Ádám, Kertész, István, Hajdu, István, and Trencsényi, György

Subjects

*ALZHEIMER'S disease, *DISEASE risk factors, *POSITRON emission tomography, *RATS, *ANIMAL disease models, *LDL cholesterol

Abstract

Aluminum (Al) excess and hypercholesterinaemia are established risks of Alzheimer's disease (AD). The aim of this study was to establish an AD-resembling hypercholesterinaemic animal model—with the involvement of 8 week and 48 week-old Fischer-344 rats—by Al administration for the safe and rapid verification of β-amyloid-targeted positron emission tomography (PET) radiopharmaceuticals. Measurement of lipid parameters and β-amyloid–affine [11C]C-Pittsburgh Compound B ([11C]C-PIB) PET examinations were performed. Compared with the control, the significantly elevated cholesterol and LDL levels of the rats receiving the cholesterol-rich diet support the development of hypercholesterinaemia (p ≤ 0.01). In the older cohort, a notably increased age-related radiopharmaceutical accumulation was registered compared to in the young (p ≤ 0.05; p ≤ 0.01). A monotherapy-induced slight elevation of mean standardised uptake values (SUVmean) was statistically not significant; however, adult rats administered a combined diet expressed remarkable SUVmean increment compared to the adult control (SUVmean: from 0.78 ± 0.16 to 1.99 ± 0.28). One and two months after restoration to normal diet, the cerebral [11C]C-PIB accumulation of AD-mimicking animals decreased by half and a third, respectively, to the baseline value. The proposed in vivo Al-induced AD-resembling animal system seems to be adequate for the understanding of AD neuropathology and future drug testing and radiopharmaceutical development. [ABSTRACT FROM AUTHOR]

Published

2022

2. Influence of apolipoprotein-E genotype on brain amyloid load and longitudinal trajectories.

Author

Lopresti, Brian J., Campbell, Elizabeth M., Yu, Zheming, Anderson, Stewart J., Cohen, Ann D., Minhas, Davneet S., Snitz, Beth E., Royse, Sarah K., Becker, Carl R., Aizenstein, Howard J., Mathis, Chester A., Lopez, Oscar L., Klunk, William E., and Tudorascu, Dana L.

Subjects

*POSITRON emission tomography, *GENOTYPES, *PET therapy, *AGE of onset, *ALZHEIMER'S disease

Abstract

To characterize the influence of apolipoprotein-E (APOE) genotype on cerebral Aβ load and longitudinal Aβ trajectories, 11C]Pittsburgh compound-B (PiB) positron emission tomography (PET) imaging was used to assess amyloid load in a clinically heterogeneous cohort of 428 elderly participants with known APOE genotype. Serial 11C]PiB data and a repeated measures model were used to model amyloid trajectories in a subset of 235 participants classified on the basis of APOE genotype. We found that APOE-ε4 was associated with increased Aβ burden and an earlier age of onset of Aβ positivity, whereas APOE-ε2 appeared to have modest protective effects against Aβ. APOE class did not predict rates of Aβ accumulation. The present study suggests that APOE modifies Alzheimer's disease risk through a direct influence on amyloidogenic processes, which manifests as an earlier age of onset of Aβ positivity, although it is likely that other genetic, environmental, and lifestyle factors are important. • APOE-ε4 is associated with increased Aβ burden compared with other APOE genotypes. • Age of onset of Aβ positivity in APOE-ε4+ antecedes other genotypes by > 15 years. • APOE-ε2+ is associated with reduced Aβ burden and a delayed age of onset. • Within-genotype variability suggests additional factors influence Aβ trajectories. [ABSTRACT FROM AUTHOR]

Published

2020

3. Fully automated production of [11C]PiB for clinical use on Trasis-AllinOne synthesizer module.

Author

Myburgh, Paul Josef, Moore, Michael David, Pathirannahel, Buddhika Liyana, Grace, Laura Rose, and Solingapuram Sai, Kiran Kumar

Subjects

*RADIOACTIVE tracers, *POSITRON emission tomography, *ALZHEIMER'S disease, *METHYL triflate, *SOLID phase extraction, *RADIOCHEMICAL purification

Abstract

Pittsburgh compound B ([11C]PiB) was the first broadly applied radiotracer with specificity for amyloid-β (Aβ) peptide aggregates in the brain and has since been established as the gold standard for positron emission tomography (PET) employed for clinical in vivo imaging of Aβ plaques, used for imaging applications of Alzheimer's disease (AD), related dementia, and other tauopathies. The use of [11C]PiB for routine PET studies is dependent on the production capabilities of each radiochemistry laboratory, subsequently a continuous effort is made to develop suitable and sustainable methods on a variety of auto synthesis platforms. Here we report a fully automated, multi-step radio synthesis, purification, and reformulation of [11C]PiB for PET imaging using the Trasis AllinOne synthesis unit, a commonly used commercial radiochemistry module. We performed three validation runs to evaluate the reproducibility and to verify that the acceptable criteria were met for the release of clinical-grade [11C]PiB using a Trasis AllinOne auto radiosynthesis unit. Solid phase supported radiolabeling was performed through the capture of precursor (6-OH-BTA-0) on a C18 solid phase extraction (SPE) cartridge and subsequent flushing of gaseous [11C]Methyl triflate(MeOTf) through the Sep-Pak for carbon-11 (11C) N-methylation. Starting with 92.5 GBq [11C]CO 2 , [11C]PiB synthesis was completed in approximately 25 min after cyclotron end of bombardment with an injectable dose >7.0 GBq at end of the synthesis. The radiopharmaceutical product met all quality control criteria and specifications for use in human studies. • Automated radiosynthesis of [11C]PiB on the Trasis AllinOne synthesis unit. • Synthesis of the N-methylating synthon, [11C]MeOTf on the same cassette. • [11C]PiB was obtained with high molar activity and radiochemical purity. • Procedure is potentially transferable to the production of [11C]PiB in commercial kit modules. • [11C]PiB produced meets all quality control specifications for human use. [ABSTRACT FROM AUTHOR]

Published

2023