Synthesis of [3H] and [2H6]AZD6642, an inhibitor of 5‐lipoxygenase activating protein (FLAP) |
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| Authors: | Åsa Lindelöf Cecilia Ericsson Roger Simonsson Göran Nilsson Gunnar Grönberg Charles S. Elmore |
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| Affiliation: | 1. Isotope Chemistry, Enabling Services, Drug Safety and Metabolism iMED, AstraZeneca Pharmaceuticals LP, M?lndal, Sweden;2. Structure Analysis & Separation Science, Medicinal Chemistry, Respiratory, Inflammation, and Autoimmune iMED, AstraZeneca Pharmaceuticals LP, M?lndal, Sweden |
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| Abstract: | An AstraZeneca effort to identify a 5‐lipoxygenase activating protein inhibitor with good drug‐like properties resulted in the identification of AZD6642. To further understand its drug metabolism and pharmacokinetic properties, it was required labeled with tritium. The tritiation of AZD6642 was effected by Ir‐catalyzed exchange chemistry to give an average of one tritium per molecule. Additionally, a stable isotope labeled version of AZD6642 was required to support bioanalytical studies. The synthesis originated from [2H6]acetone which was converted to the trimethylsilyl cyanide adduct and subsequently reduced to give 2‐(aminomethyl)‐[1,1,1,3,3,3‐2H6]propan‐2‐ol in good yield. Carbonylation to give an amide adduct resulted in an intermediate that was converted to the final compound in four steps. |
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| Keywords: | AZD6642 5‐lipoxygenase activating protein 3H Ir hydrogen‐isotope exchange |
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