Background of the Invention Positron emission tomography (PET) is a non-invasive imaging technique that offers high spatial and temporal resolution and allows quantification of tracer concentrations in tissues.

The technique involves the use of radiotracers labelled with positron emitting radionuclides, which permit measurement of parameters regarding the physiology or biochemistry of a variety of living tissues.

Compounds can be labelled with positron or gamma emitting radionuclides. The most commonly used positron emitting (PET) radionuclides are"C,'8F,'50 and 13 N, which are accelerator produced, and have half lives of 20.4, 109.8, 2 and 10 minutes respectively. Due to their short half-lives"C, 150 and 3N labelled radiopharmaceuticals have to be use at the site of production and require the development of specific synthetic procedures.

"C (Ti/2=20. 4min) is an important neutron-deficient radionuclide for PET because it can substitute for non-radioactive carbon in any organic molecule without altering their biological and physiochemical properties. An important part of the elaboration of new procedures to incorporate PET radionuclides into molecules is the development and handling of new"C labelled precursors.

"C can be produced in the absence of the naturally occurring stable isotopes 12C and 13C, and with high yields on a small proton accelerator using the 14N (p, a)"C reaction in a target gas containing nitrogen (Christman, et al., 1975; Clark, et al., 1975 and Welch et al., 1968).

In the presence of oxygen trace (e. g. 0. 1% oxygen), the radiochemical species formed is ["C] carbon dioxide which is suitable for use directly as in the"C-carboxylation of Grignard reagents (organomagnesium halides). ["qcarbon dioxide can also be converted into a variety of secondary radiolabelled chemical entities such as high specific activity ["C] methyl iodide.

An important consideration for radiolabelling with carbon-11 is the maximization of specific activity of the radiolabelled compound, Isotopic dilution of [11C] carbon dioxide with atmospheric carbon dioxide (3.4 x 104 ppm) substantially reduces its specific activity and therefore limits the application of the resultant radiolabelled compound as a PET probe.

As an alternative method to using ["C] carbon dioxide for radiolabelling compounds, [11C] carbon monoxide may be used instead, as it is less prone to isotopic dilution with atmospheric carbon monoxide (0. 1 ppm). Methods for the production of [11C] carbon monoxide by reducing ["C] carbon dioxide using reducing metals at high temperatures are well known (Gmelins 1972; Clark, et al., 1975; Zeisler, et al., 1997). Zinc and molybdenum are the most widely used reducing agent for the ["C] carbon dioxide/carbon monoxide conversion.

However, it is difficult to trap"CO in the small volume of organic solvent in which most of the precursors for the production of radiolabelled compounds are soluble. Small volumes of solvent are required because this allows easy isolation of the radiolabelled product by means of preparative HPLC and increases the concentration of the starting materials in the reaction mixture, thereby forcing the reaction in the desired direction.

In 1978 Roeda, et al., described a method for the production of ["C] phosgene from ["C] carbon monoxide however, its practical use in the production of radiopharmaceuticals has been very limited due low yields and the lack of suitable equipment and methods to efficiently trap and react carbon monoxide.

Existing methods for the trapping of ['I qcarbon monoxide for the production of radiolabelled compounds rely on the use of high pressure or recirculation of ["C] carbon monoxide to maintain adequately high levels of ["C] carbon monoxide in solution (Kihlberg, et al., 1999; Hostetler, et al., 2002). This requires the use of dedicated automated robotic systems for the handling of ["C] carbon monoxide and specialised equipment.

Borane carbonyl (HgBCO) is the immediate precursor to boranocarbonates, such as the potassium salt K2 [H3BCO2] which were reported to release CO in water at elevated temperatures in 1967 (Malone et al., 1967; Malone et al., 1967a). Although yields of the solid, air stable K2 [H3BCO2], produced from the known methods of B2H6 + CO are good, it is not convenient to work under pressurised conditions with H3B. CO, as it is a pyrophoric gas (Carter, et al., 1965; Mayer, 1971). Alberto et al., (2001) found that by preparing H3B. CO from commercially available H3B. THF and reacting it in situ with an alcoholic solution of potassium hydroxide, K2 [H3BC02] could be produced at ambient pressures. This result was achieved by controlling the equilibrium of the two-way reaction between H3BCO and H3B. THF by selectively condensing the THF out of the reaction. The resultant K2 [H3BCO2] was then used as an in situ source of CO in aqueous solution and as a reducing agent.

It has now been found that radiolabelled H3B. CO can be used to release radiolabelled carbon monoxide in organic solvents, aqueous solvents and mixtures of organic and aqueous solvents in order to prepare radiolabelled compounds without the need for high pressure autoclaves or recirculation units.

Brief Summary of the Invention Accordingly, in a first aspect the invention provides a process for the preparation of radiolabelled H3B. CO comprising contacting H3B in a suitable solvent with carbon monoxide and a suitable base, characterised in that the carbon monoxide is radiolabelled.

Radiolabelled HgB. CO may be prepared by the reaction of borane (H3B) in a suitable solvent with radiolabelled carbon monoxide. Suitable solvents for this reaction are those which solubilize H3B and allow it to co-ordinate with free electron pairs of the oxygen, for example tetrahydrofuran (THF) and ethers such as diethyl ether and dioxane. THF is preferred as a solvent due to its physical characteristics of a high boiling point, a lower affinity towards water and its comparable low price.

Hydrides of other elements, such as aluminium gallium, indium and thallium hydride would also be expected to co-ordinate with radiolabelled carbon monoxide. However, the instability of aluminium hydride in solvents suitable for this reaction means that if an aluminium compound were to be used it would preferably be compounds such as Aids in THF or aluminium tri organyls.

Free solvent may be removed from the reaction by condensation or other suitable means such as a solid support. This achieves the advantage of shifting the equilibrium of the reaction towards increased production of radiolabelled H3B. CO.

The carbon monoxide used in the reaction may be labelled by any conventional method with any of the following isotopes"C, 13C, 14C,'50 or'80. Preferably"C is used.

Suitable solvents for use in the process of the invention include ethers such as diethyl ether and dioxane, and tetrahydrofuran. Preferably tetrahydrofuran is used. Suitable mixtures of solvents may also be used.

In a second aspect the invention provides the use of radiolabelled H3B. CO prepared according to the first aspect of the invention, as a donor of radiolabelled carbon monoxide in the manufacture by carbonylation of radiolabelled compounds.

In practice the second aspect of the invention may be carried out by using the radiolabelled H3B. CO prepared according to the first aspect of the invention in a coupling reaction as set out in Scheme 1 below, in which coupling reactions are typically carried out with a halide or a triflate (trifluoromethanesulfonate) with a nucleophile (alcohol, amine, thiol) or a organostannane, a base and a catalyst such as a palladium (0) catalyst to obtain esters, amides, ketones, aldehydes, carboxylic thioesters or by reacting a nitro component or an azido derivative to form isocyanate derivatives or condensing two nucleophiles in presence of selenium to synthesized carbamates, thiocarbamates, carbonates and ureas.

Suitable bases for use in the process of the invention include triethylamine (TEA), N- Methyidibutylamine (MDBA), M-Methyl-2, 2,6, 6-tetramethylpiperidine (N-MTMP) and N, N di- isopropyl-ethylamine (DIPEA). Suitable mixtures of bases may also be used.

The starting materials and reagents for use in the first and second aspects of the invention are available commercially or can be synthesised by well-know and conventional methods.

The reaction conditions used in the formation of non-radiolabelled H3B. CO can be sourced from Alberto et al., (2001), other reaction conditions such as the radiolabelling of CO and carbonylation reactions are well known.

["C] CO, prepared by reduction of ['C] CO2 with a reducing metal (commonly zinc or molybdenum), is trapped using conventional methods such as molecular sieves in liquid nitrogen or silica and is then carried into a solution of BH3THF using an inert gas carrier.

The ["C] borane carbonyl ( ["C] H3B. CO) complex thus formed is then carried through to a reaction chamber in which it is reacted with suitable components to construct the required compound using conventional coupling methods. Conventional coupling reaction often take place at elevated temperatures and the reaction chamber may be made of materials suitable for use in a microwave (such as glass).

In order to promote the formation of the ["C] borane carbonyl THF is removed from the reaction, typically by condensation. Coupling reactions are typically carried out reacting ["C] borane carbonyl with the appropriate starting materials and reagents as depicted in scheme 1. (1) Formation of radioactive * BH3CO BH3 in solvent radioactive CO removal of free solvent (II) Coupling reaction (a) when R1 and R2 are aryl, vinyl or alkyl ; X is I, Br, Cl or Off ; and Y is NH2, NHR, OH, SH or Sn (R3) 3 (with R3 = alkyl or aryl) radioactive BH3CO R1 * Zs or R1 s * R2 R1 X + lf-R2 R2 Pd (0), Base when Y is NH2, NHR, OH, SH ; when Y is-Sn (R3) 3 ZisNH, NR, OorS ° radloactiveBH3CO * R1-N+ R1-N--O Pd (0), Base o radioactive BH3CO * R1-N=N N R1-N--O Pd (0), Base or (b) when Xand Y are 0, N or S or (b) when Xand Y are 0, N or S and R1and R2are aryl or alkyl o 0 R1-X-H + H-Y-R2 BH, R1 8 zR2 v * v Se Scheme1 Suitable compounds for radiolabelling by this method are those which contain a carbonyl group (some examples are shown in Scheme 2). 0 amides& imides R ; NR R2 carboxylicacids RXoH 0 carboxylic thioesters R SR, carboxylic esters RAOR, ouzo JL N carbonates po'OR, isocyanates R 0 0 aldehyde R'''H ketones 0 0 ureas RNJ0NR, thiocarbamates RRtNXSRz 0 carbamates RR, N * OR, Scheme 2 Amides and imides can also contain lactams and carboxylic esters can also contain lactones.

In a third aspect the invention provides radiolabelled H3B. CO prepared in accordance with the first aspect of the invention.

In fourth aspect the invention provides radiolabelled compounds prepared by carbonylation in accordance with the second aspect of the invention.

Edidepride (N-((S)-1-Ethyl-pyrrolidin-2-ylmethyl)-3-iodo-5-methOxy-benz amide), FLB (5- bromo-N- ( (S)-l-ethyl-pyrrolidin-2-ylmethyl)-2, 3-dimethoxy-benzamide) and raclopride (3,5- dichloro-N- ( (S)-l-ethyl-pyrrolidin-2-ylmethyl)-2-hydroxy-6-methoxy-benza mide), which are all dopamine D2 ligands and PK11195 (1-(2-Chloro-phenyl)-isoquinoline-3-carboxylic acid), which is a benzodiazepine receptor ligand are commonly used PET ligands that contain carbonyl groups that can be labelled with ["C] CO.

In a fifth aspect the invention provides use of the radiolabelled compounds according to the fourth aspect of the invention in imaging techniques such as positron emission tomography, modified single photon emission tomography and autoradiography (classical and phosphor imaging plates).

In a sixth aspect the invention provides a composition comprising a radiolabelled compound in accordance with the fourth aspect of the invention and a pharmaceutically acceptable carrier or carriers, suitable for use in the above mentioned imaging techniques.

Detailed Description of the Invention The invention is further described through the following examples: Examples Abbreviation list : THF: Tetrahydrofuran TEA: Triethylamine DBU: 1, 8-Diazabicyclo [5.4. 0] undec-7-ene TMP: Tetramethylpiperidine DMF: Dimethylformamide DIPEA : NN-di-isopropyl-ethylamine MDBA: N-Methyldibutylamine N-MTMP: M-Methyl-2, 2,6, 6-tetramethylpiperidine Synthesis of ["C] N-benzyl-benzamide (I) 0 1 + H2N"" [,, qH3B'Co I * N advent Pd catalyst Base Example 1 Preparation of the reaction vial Palladium (II) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700/iL THF (degassed by bubbling N2 through it for few minutes). Then, iodobenzene (1.5 mg, 0.00735 mmol) and benzylamine (1.2 mg, 0.011 mmol) dissolved in 300 uL THF (degassed by bubbling N2 through it for few minutes) were added to the solution of palladium complex. TEA (1. 6, uL, 0.0088 mmol) was added, and the reaction vial was placed in the reaction-setup in a bath at-78°C.

Synthesis [11C] Carbon dioxide was produced by the 14N (p, a)"C nuclear reaction using a nitrogen gas target (containing 1% oxygen) pressurised to 150 psi and bombarded with 16 MeV protons using the General Electric Medical Systems PETtrace 200 cyclotron. Typically, the irradiation time was 30 minutes using a 40, uA beam current. After irradiation, ["C] carbon dioxide was trapped and concentrated on 4A molecular sieves. The trapped ["C] C02 was released from molecular sieves in a stream of nitrogen (30 mL/min) by heating them to 350°C. [11C] C02 was reduced on-line to ["C] carbon monoxide after passing through a quartz tube filled with zinc granular heated to 400°C. The produced ["C] carbon monoxide was transferred in our system set-up at 30 mL/min, where it was condensed on 4A molecular sieves at-196°C.

After 6 min delivery and trapping of the ["C] CO, the radioactive gas was then released at room temperature in a flow of nitrogen (6 mL/min) to bubble through a BH3. THF solution (1.5 mL of a 1, 0 M solution) in order to make the [11C] BH3. CO complex. This complex was carried with the flow of nitrogen through an empty vial cooled at-60°C to remove the THF, and finally through the reaction vial containing the reactants (cf. preparation of the reaction vial above) cooled at-78°C. The trapping process took approximately 6 min (when the radioactivity level measured in the reaction vial has reached a maximum). The delivery tubings were then removed and the reaction vial heated in an oven at 110°C for 10 min. The crude product was filtered through a 0. 45, um filter and analysed using analytical radio HPLC.

Analytical HPLC was performed using a Dionex system (SUMMIT HPLC system), equipped with a Dionex HPLC pump (Model P 680A LPG) with a 200, 1-il injection loop connected in series with a Phenomenex Sphereclone 5u ODS (2) column (250 x 4.60 mm, 5, um), a variable Dionex UVNIS detector (Type UVD 170U/340U) in series with a sodium iodide radiodetector of in-house design.

The desired end-product was identified by co-injection with a non-radioactive reference. The given yields of the product are based on the final radioactivity trapped in the reaction vial at EOS (End Of Synthesis).

The analytical HPLC showed the formation of the desired radiolabelled ["C] N- benzylbenzamide in Example 1 in approximately 1.7% yield.

Example 2 The synthesis of ["qN-benzyl-benzamide was carried out as described in Example 1 except that the palladium (II) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700 pL of a solution of THF: H20, 4: 1 (degassed by bubbling N2 through it for few minutes), the iodobenzene (1.5 mg, 0.00735 mmol) and benzylamine (1.2 mg, 0.011 mmol) were dissolved in 300, uL of a solution of THF: H20, 4: 1 (degassed by bubbling N2 through it for few minutes). The reaction vial was placed in the reaction-setup in a bath at 0°C and after the trapping of the ["C] BH3. CO the reaction vial was heated at 120°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired radiolabelled [11C] N-benzylbenzamide in approximately 7% yield.

Example 3 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 1 except that the palladium (li) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700 lit of a solution of THF + 2% H20 (degassed by bubbling N2 through it for few minutes), the iodobenzene (1.5 mg, 0.00735 mmol) and benzylamine (1.2 mg, 0.011 mmol) were dissolved in 300, uL of a solution of THF + 2% H20 (degassed by bubbling N2 through it for few minutes) and after the trapping of the ["C] BH3. CO, the reaction vial was heated at 120°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N- benzylbenzamide in approximately 30% yield.

Example 4 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 1 except that the palladium (li) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700 juL of a solution of THF + 1 % H2O (degassed by bubbling N2 through it for few minutes), the iodobenzene (1.5 mg, 0.00735 mmol) and benzylamine (1.2 mg, 0.011 mmol) were dissolved in 300, uL of a solution of THF + 1% H2O (degassed by bubbling N2 through it for few minutes) and after the trapping of the [CjBHg. CO the reaction vial was heated at 50°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N- benzylbenzamide in approximately 17% yield.

Example 5 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 4 except that after the trapping of the ["C] BH3. CO, the reaction vial was heated at 70°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["qN-benzylbenzamide in approximately 47% yield.

Example 6 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 4 except that after the trapping of the ["C] BH3. CO, the reaction vial was heated at 85°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N-benzylbenzamide in approximately 47% yield.

Example 7 The synthesis of ["qN-benzyl-benzamide was carried out as described in Example 4 except that after the trapping of the [11C] BH3. CO, the reaction vial was heated at 120°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired [11C] N-benzylbenzamide in approximately 47% yield.

Example 8 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 4 except that after the trapping of the [11C] BH3. CO, the reaction vial was heated at 140°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N-benzylbenzamide was approximately 28% yield.

Example 9 The synthesis of ["qN-benzyl-benzamide was carried out as described in Example 5 except that DBU (1. 3, uL, 0.0016 mmol) was used instead of TEA. The analysis of the HPLC chromatograms showed traces of the formation of the desired ["C] N-benzylbenzamide.

Example 10 The synthesis of [11C] N-benzyl-benzamide was carried out as described in Example 5 except that 2,2, 6,6-TMP (1. 7, uL, 0.009 mmol) was used instead of TEA. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N-benzylbenzamide in approximately 8% yield.

Example 11 The synthesis of [11C] N-benzyl-benzamide was carried out as described in Example 5 except that pyridine (0. 7 uL, 0.0088 mmol) was used instead of triethylamine and the reaction vial was heated from 40 to 80°C for 15 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired [11C] N- benzylbenzamide in approximately 28% yield.

Example 12 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 5 except that benzylamine (3.6 mg, 0.034 mmol) was used instead of TEA and the reaction vial was heated 90°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N-benzylbenzamide in approximately 20% yield.

Example 13 The synthesis of ["qN-benzyl-benzamide was carried out as described in Example 4 except that the palladium (II) diacetate, triphenylphosphine, iodobenzene and benzylamine benzylamine were dissolved in DMF, and after the addition of TEA the reaction vial was placed in the reaction-setup in a bath at-50°C. After the trapping of the [11C] Bug. CO the reaction vial was heated at 90°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired [11C] N- benzylbenzamide in approximately 23% yield.

Example 14 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 4 except that the palladium (II) diacetate, triphenylphosphine, iodobenzene and benzylamine benzylamine were dissolved in 1, 2-dichloroethane, and after the addition of TEA the reaction vial was placed in the reaction-setup in a bath at-20°C. After the trapping of the ["qBH3. CO the reaction vial was heated at 110°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired [11C] N-benzylbenzamide in approximately 12% yield.

Example 15 Preparation of the reaction vial Preparation of the reaction vial was carried out as described in Example 1 except that the palladium (II) diacetate (0.5mg, 0. 0022mmol) and triphenylphosphine (2.9 mg, 0. 11mmol) were dissolved in 700 ; j. L THF with 1 % H20 and the iodobenzene (1. 5mg, 0.00735 mmol) and benzylamine (1.2 mg, 0.011 mmol) were dissolved in 300 ; j. L degassed THF with 1 % H20.

Synthesis Synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 1 except that the produced [11C] CO was condensed onto a trap at-196 °C made from a 12-inch coil of <BR> <BR> 1/16"stainless steel tubing, 0. 040" i. d. , packed with carbonex 1000,45/60 mesh (Supelco).

After 6 min delivery and trapping of the ["C] CO, the radioactive gas was then released at room temperature and carried out through an empty vial in a flow of nitrogen (6 mL/min) into a reactor loaded with the BH3THF solution (1.5 mL of a 1.0 M solution in THF) in order to form the ["C] BH3 CO complex. The complex was then carried with the flow of nitrogen through an empty vial cooled at-78 °C, and finally through the reaction vial containing the reactants cooled at-78 °C. After 6 min of delivery of the ["C] BH3. COcomplex the tubings were removed and the reaction vial heated in an oven at a temperature o 95°C for 10 min.

The crude product was filtered through a 0. 45, um filter and analysed for radioactivity contentThe analysis of the HPLC chromatograms showed the formation of the desired ["qN-benzylbenzamide in approximately 47% yield.

Example 16 The synthesis of ["C] N-benzyl-benzamide was carried out as described in Example 15 except that the TEA was replaced with DIPEA (1. 53pL, 0. 0088 mmol) and the reaction vial containing the I"qBH3. COcomplex was heated in an oven at 90°C for 10 min, filtered and analysed for radioactivity content The analysis of the HPLC chromatograms showed the formation of the desired ["C] N-benzylbenzamide in approximately 91% yield Synthesis of ["C] phthalide SOH [11C] BH3*CO solvent Br Pd catalyst c Base 0 Example 17 Tetrakis (triphenylphosphine) palladium (0) (1.1 mg, 0. 95, umol) was dissolved in 500, uL of a solution of THF + 1 % H2O (degassed by bubbling N2 through it for few minutes). Then, a mixture of 2-bromobenzyl alcohol (1.1 mg, 0.006 mmol) and K2CO3 (5 mg, 0.036 mmol) were dissolved in 300, uL of THF + 1% H20 (degassed by bubbling N2 through it for few minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the ["C] BH3. CO as described in Example 1, the reaction was heated at 100°C for 4 min, filtered and analysed for radioactivity content The analysis of the HPLC chromatograms showed the formation of the desired ["C] phthalide in traces.

Example 18 Palladium (II) diacetate (0.8 mg, 0.0035 mmol) and triphenylphosphine (5 mg, 0.020 mmol) were dissolved in 700/iL of a solution of THF + 1 % H20 (degassed by bubbling N2 through it for few minutes). Then, a mixture of 2-bromobenzyl alcohol (2.2 mg, 0.012 mmol) and K2CO3 (5 mg, 0.036 mmol) were dissolved in 300, uL of THF + 1% H20 (degassed by bubbling N2 through it for few minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the [11C] BH3. CO as described in Example 1, the reaction was heated at 120°C for 5 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] phthalide in traces.

Example 19 Palladium (li) diacetate (0.8 mg, 0.0035 mmol) and triphenylphosphine (5 mg, 0.020 mmol) were dissolved in 700, uL of a solution of THF (degassed by bubbling N2 through it for few minutes). Then, a mixture of 2-bromobenzyl alcohol (2.2 mg, 0.012 mmol) and DBU (2. 0, uL, 0.014 mmol) was dissolved in 300, uL of THF (degassed by bubbling N2 through it for few minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the ["C] BH3. CO as described in Example 1, the reaction was heated at 110°C for 5 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["qphthalide in traces.

Example 20 Palladium (II) diacetate (0.8 mg, 0.0035 mmol) and triphenylphosphine (5 mg, 0.020 mmol) were dissolved in 700, uL of a solution of THF (degassed by bubbling N2 through it for few minutes). Then, a solution of 2-bromobenzyl alcohol (2.2 mg, 0.012 mmol) in 300, uL of THF (degassed by bubbling N2 through it for few minutes) was added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C.

After the trapping of the ["C] BH3. CO as described in Example 1, the reaction was heated at 120°C for 5 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] phthalide in approximately 40% yield.

Example 21 Palladium (li) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700, uL of a solution of THF + 1% H20 (degassed by bubbling N2 through it for few minutes). Then, a mixture of 2-bromobenzyl alcohol (2.2 mg, 0.012 mmol) and TEA (1. 9, uL, 0.014 mmol) were dissolved in 300 liL of THF + 1% H20 (degassed by bubbling N2 through it for few minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the [CJBHs. CO as described in Example 1, the reaction was heated at 90°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] phthalide in approximately 26% yield.

Example 22 Palladium (II) diacetate (1.0 mg, 0.0044 mmol) and triphenylphosphine (6 mg, 0.022 mmol) were dissolved in 700, uL of a solution ofTHF +1% H20 (degassed by bubbling N2 through it for few minutes). Then, a mixture of 2-bromobenzyl alcohol (2.2 mg, 0.012 mmol) and TEA (1. 9, uL, 0.014 mmol) were dissolved in 300, uL of THF + 1% H20 (degassed by bubbling N2 through it for few minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the ["C] BH3. CO as described in Example 1, the reaction was heated at 90°C for 8 min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] phthalide in approximately 20% yield.

Example 23 Palladium (li) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700/iL of a solution of THF with 1% H2O (degassed by bubbling N2 through it for few minutes). Then, a mixture of 2-bromobenzyl alcohol (1.37mg, 0.0073 mmol) and DIPEA (1. 53gL, 0.0088 mmol) were dissolved in 300, uL of THF with 1% H20 (degassed by bubbling N2 through it for few minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78C. The trapping of the ["C] BH3. CO complex was carried out as described in Example 15 and the reaction was heated at 95°C for 10min, filtered and analysed for radioactivity content. The analysis of HPLC chromatograms showed the formation of the desired ["qphthalide in approximately 40% yield.

Example 24 The synthesis of ["C] phthalide was carried out as described in Example 23 except that the reaction was heated at 95°C for 8min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] phthalide in approximately 89% yield min Synthesis of ["C] N-Methyinicotinamide 0 i CH3NH2 Pd (0) N H J ------------------- LJ N- 1CIBH3. CO, base, solvent N Example 25 Palladium (II) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 400, uL of a solution of THF with 1% H20 (degassed by bubbling N2 through it for 5 minutes). Then, a mixture of 3-iodopyridine (1.5mg, 0.0073 mmol) and DIPEA (1. 53pL, 0.0088 mmol) were dissolved in 600, uL of methylamine 2.0 M in solution in THF and then added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the ["C] BH3. CO as described in Example 15, the reaction was heated at 140 °C for 8min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] N-Methyinicotinamide in approximately 95% yield Synthesis of ["C] 6- [ (3-cyclobutyl-2, 3,4, 5-tetrahydro-1 H-3-benzazepin-7-yl) oxy]- N-methyinicotinamide (WO 2004/056369) \ carbonylation using [iC] BH9. C0 + N NH2Me + Pd (O) + DIPEA + THF + heat/P\ N N N /1, 0 /-0 Example 26 Palladium (lI) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700 uL of a solution of THF with 1% H20 (degassed by bubbling N2 through it for 5 minutes). Then, a mixture of 3-cyclobutyl-7- [ (5-iodo-2-pyridinyl) oxy] - 2,3, 4, 5-tetrahydro-1H-3-benzazepine (3. 1 mg, 0.0073 mmol), DIPEA (1. 5311L, 0.0088 mmol) and methylamine 2.0 M (0. 011 mol, 5. 48/iL solution in THF) were dissolved in 300 , uL of THF with 1 % H20 (degassed by bubbling N2 through it for 5 minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the [11C] BH3. CO as described in Example 15, the reaction was heated at 100 °C for 8min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] 6- [ (3-cyclobutyl- 2,3, 4, 5-tetrahydro-1 H-3-benzazepin-7-yl) oxy]-N-methyinicotinamide in approximately 6.5% yield.

Example 27 Palladium (II) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 400, uL of a solution of THF with 1% H20 (degassed by bubbling N2 through it for few minutes). Then, a mixture of 3-cyclobutyl-7- [ (5-iodo-2-pyridinyl) oxy] - 2,3, 4, 5-tetrahydro-1 H-3-benzazepine (1.6 mg, 0.00365 mmol), DIPEA (1. 53, uL, 0.0088 mmol) and methylamine 2.0 M (0. 011mmol, 5. 48, uL solution in THF) were dissolved in 300 , uL of THF with 1 % H20 (degassed by bubbling N2 through it for 5 minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C. After the trapping of the [11C] BH3. CO as described in Example 15, the reaction was heated at 140 °C for 8min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired ["C] 6- [ (3-cyclobutyl- 2,3, 4, 5-tetrahydro-1 H-3-benzazepin-7-yl) oxy]-N-methyinicotinamide in approximately 44.4% yield Example 28 Synthesis of ["C] (4- (1- {4- [4- (3-Piperidin-1-yl-propoxy)-phenyl]-piperazin-1-yl}-methanoyl )- benzonitrile (WO 2004/035556) joy NX i i carbonylation using ["C] BH,. CO N +pd (0) +DIPEA+THF+heat Ou Vin \ iso o . 2HCI i i Palladium (II) diacetate (0.5 mg, 0.0022 mmol) and triphenylphosphine (2.9 mg, 0.011 mmol) were dissolved in 700, uL of a solution of THF with 1 % H2O (degassed by bubbling N2 through it for 5 minutes). Then, a mixture of 1- (4- { [3- (1- piperidinyl) propyl] oxy} phenyl) piperazine (2.05mg, 0.0055 mmol), DIPEA (1. 86gel, 0.011 mmol) and 4-iodo-benzonitrile (0. 0036mol, 0. 85mg) were dissolved in 300, uL of THF with 1 % H20 (degassed by bubbling N2 through it for 5 minutes) and added to the solution of the palladium complex. The reaction vial was placed in the reaction-setup in a bath at-78°C.

After the trapping of the ["C] BH3. CO as described in Example 15, the reaction was heated at 140°C for 7min, filtered and analysed for radioactivity content. The analysis of the HPLC chromatograms showed the formation of the desired [ ["C] (4- (1- {4- [4- (3-Piperidin-1-yl- propoxy)-phenyl]-piperazin-1-yl}-methanoyl)-benzonitrile in approximately 30% yield.

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