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Design of an IV Formulation of an Unstable Prodrug Candidate for Prostate Cancer Treatment: Solution Chemistry of N-(glutaryl-hyp-ala-ser-cyclohexylglycyl-gln-ser-leu)-doxorubicin
Authors:Shyam B Karki  Varaporn Treemaneekarn  Drazen Ostovic  Maneesh Nerurkar  Örn Almarsson
Affiliation:1. Pharmaceutical Research and Development, Merck Research Laboratories, Merck &2. Co., Inc., West Point, Pennsylvania, USA;3. Amgen Inc., Thousand Oaks, California, USA;4. Nicholas Piramal Research CtR, 1 Nirlon Complex, Near NSE Complex, Goregaon, Mumbai, India;5. TransForm Pharmaceuticals Inc., Lexington, Massachusetts, USA
Abstract:ABSTRACT

The chemical degradation of N-(glutaryl-hyp-ala-ser-cyclohexylglycyl-gln-ser-leu)-doxorubicin (henceforth referred to as doxorubicin peptide conjugate 1) was studied in buffered aqueous solution. The pH-rate profile of degradation shows that the doxorubicin conjugate is most stable between pH 5 and 6. The dependence of log kobsd on pH in acidic medium is characteristic of specific acid-catalysis of the sugar hemiaminal of 1 (as in the case of doxorubicin). Isolation of degradates and structural determination shows that the degradation at lower pH values yields the water-insoluble aglycone doxorubicinone, supporting the mechanism of acid-catalyzed loss of the amino sugar. At pH higher than 5, a more complicated degradation pattern is observed, including the loss of the amino sugar and the aromatization of the saturated ring to give 7,8-dehydro-9,10-desacetyldoxorubicinone as one of the major products. Around the pH of maximum stability in solution, the rate of degradation of 1 is significantly greater than that for doxorubicin, which rules out the formulation of a room temperature solution product with a sufficiently long shelflife for market use. Design of a stable lyophilized formulation for sterile reconstitution based on the physicochemical properties of 1 is described.
Keywords:Doxorubicin peptide conjugate  Prodrug  Prostate cancer  Stability  Kinetics  Degradation  Preformulation  Lyophilization  IV formulation
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