Background

[PubMed]

Benzodiazepines, such as diazepam, are potent psychoactive drugs used for their sedative and anxiolytic properties (1, 2). There are two types of benzodiazepine receptors, which have been identified as the central and peripheral benzodiazepine receptors. The central benzodiazepine receptor (CBR) is found exclusively in the central nervous system on the membranes of neurons and is coupled to the γ-aminobutyric acid receptor/chloride channel (3). In contrast, the peripheral benzodiazepine receptor (PBR) is a mitochondrial protein found in brain and peripheral tissues (adrenal gland, heart, lung, kidney, and testis) (4, 5). The brain has lower levels of PBR than do the peripheral tissues. Both glial cells and macrophages contain high levels of PBR (6-8). Increased PBR expression after brain injury or neuroinflammation is associated with microglial activation, such as occurs with the neuronal damage accompanying several neurodegenerative diseases, including Alzheimer’s disease, Wernicke’s encephalopathy, multiple sclerosis, and epilepsy.

PBR has been studied in vivo by positron emission tomography (PET) using 1-(2-chlorophenyl)-N-[¹¹C]methyl-N-(1-methylpropyl)-3-isoquinoline carboxamide ([11C]PK11195), an isoquinoline carboxamide with specific PBR antagonistic activity (9). [¹¹C]PK11195 is being developed as a PET agent for the non-invasive study of microglia and macrophage activation in the brain, lung, and heart.

Synthesis

[PubMed]

In the report by Hashimoto et al. (10), [¹¹C]PK11195 was synthesized by alkylation of the desmethyl precursor with [¹¹C]methyl iodide, with subsequent separation by high-performance liquid chromatography. Radiochemical purity was greater than 99%, and total synthesis time was 23 min. The specific activity was 51.8 GBq/μmol (1.4 Ci/μmol) at the end of bombardment. No yield was reported.

Shah et al. (11) described the fully remotely controlled synthesis of [¹¹C]S-PK11195 from S-desmethyl-PK11195 and [¹¹C]R-PK11195 from R-desmethyl-PK11195 with [¹¹C]methyl iodide. The ¹¹C-labeled enantiomers were prepared with a reproducible radiochemical yield of 80% (decay-corrected) based on [¹¹C]methyl iodide. Total synthesis time was 45 min. Radiochemical purity was >99% with specific activities varying between 20 and 96 GBq/μmol (0.54 and 2.6 Ci/μmol) at the end of synthesis.

In Vitro Studies: Testing in Cells and Tissues

[PubMed]

In vitro autoradiographic studies of [³H]PK11195 binding produced K_d values of 20.4 ± 1.3, 14.3 ± 2.1, and 3.9 ± 0.4 nM for human high-grade glioma, low-grade glioma, and cortex, respectively (12). The PBR B_max values were 12.4 ± 0.7, 4.0 ± 2.0, and 0.79 ± 0.09 pmol/mg protein for human high-grade glioma, low-grade glioma, and cortex, respectively. The high-grade glioma showed a B_max 14.5 times higher than that in the cortex. There was also a significant difference between the K_d measured in the tumors and that in normal cortex. Le Fur et al. (9) reported that PBR binding sites in rat myocardial membranes were specific and saturable with a K_d of 1.4 nM and a B_max of 2.25 pmol/mg protein.

Animal Studies

Human Studies

[PubMed]

Charbonneau et al. (16) reported on PET studies in 7 healthy male volunteers after injection of 259-777 MBq (7-21 mCi) of [¹¹C]PK11195. Accumulation in the lung was high up to 10 min post injection. The radioactivity in the myocardium became detectable at 2 min. The radioactivity in the heart decreased for 20 min and remained constant at 75 min. Injection of excess unlabeled PK11195 (650 nmol/kg) 30 min after [¹¹C]PK11195 (0.94 nmol/kg) led to a rapid decrease (48%) in the radioactivity in the myocardium. In a different study (19), formation of plasma metabolites from [¹¹C]PK11195 was analyzed in 2 healthy controls and 3 stroke patients. At 5, 20, and 35 min after injection of [¹¹C]PK11195 (370 MBq or 1 mCi), 5%, 22% and 32% of the plasma activity, respectively, was attributable to at least two more polar metabolites. However, no metabolites were found in the hearts, lungs, and brains of mice that received injections of [¹¹C]PK11195 (10).

[¹¹C]PK11195 or R-[¹¹C]PK11195 PET has been used mainly for assessing microglia/macrophage activation as an indication of neuronal and tissue damage in various neurodegenerative disorders (such as Alzheimer’s disease, Wernicke’s encephalopathy, multiple sclerosis, lateral sclerosis, Huntington’s disease, HIV-associated dementia, and epilepsy), pulmonary diseases, and ischemic stroke [PubMed]. Most of these human studies used a reference tissue (cerebellum or other cortical regions) to measure the accumulation of radioactivity. Kropholler et al. (20) reported that a kinetic plasma (metabolite-corrected) input with a reversible two-tissue compartment model was best for analyzing R-[¹¹C]PK11195 kinetics in PET brain studies of 13 human subjects.

Hirvonen et al. (21) performed dynamic whole-body scans after injection of R-[¹¹C]PK11195 in five healthy subjects for radiation dosimetry measurement. The mean effective dose was 4.8 µSv/MBq and the highest equivalent organ doses were recorded in the kidneys (14.0 µSv/MBq), spleen (12.5 µSv/MBq) and small intestine (12.2 µSv/MBq).

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