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An Unexpected pH Effect on the Stability of Moexipril Lyophilized Powder

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Abstract

Because of the limited stability of moexipril (RS-10085; 1) in aqueous solution, lyophilized parenteral formulations were evaluated as a function of pH in this study. In general, the lyophilized powder of 1 showed about two orders of magnitude less reactivity at 50°C than in aqueous solution at pH values below 3 or above 6. At pH 5.1, however, the lyophilized powder had maximum reactivity, with the rate actually comparable to that observed in aqueous solution. When the distribution of the two major products, diketopiperazine (DKP) 2 and ester hydrolysis analogue 3, was compared to the observed kinetics as a function of pH, it was clear that removal of water via lyophilization suppressed the spontaneous k 1 cyclization process, the spontaneous k 3 hydrolysis process, and the specific base-catalyzed k 4 hydrolysis process. The overall spontaneous k 2 cyclization process, however, was not affected by lyophilization. The latter result is accounted for by the increased equilibrium constant for the formation of the tetrahedral intermediate, To, as a result of lyophilization. This study demonstrates that stability data in solution can not be used for predicting the stability of moexipril in lyophilized powder form.

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Strickley, R.G., Visor, G.C., Lin, LH. et al. An Unexpected pH Effect on the Stability of Moexipril Lyophilized Powder. Pharm Res 6, 971–975 (1989). https://doi.org/10.1023/A:1015901731275

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  • DOI: https://doi.org/10.1023/A:1015901731275

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