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Kinetics of Phase Transitions in Amorphous Carbamazepine: From Sub- Structural Relaxation to High-Temperature Decomposition. | LitMetric

Kinetics of Phase Transitions in Amorphous Carbamazepine: From Sub- Structural Relaxation to High-Temperature Decomposition.

Int J Mol Sci

Department of Physical Chemistry, Faculty of Chemical Technology, University of Pardubice, Studentská 573, 532 10 Pardubice, Czech Republic.

Published: June 2025


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Article Abstract

Thermokinetic characterization of amorphous carbamazepine was performed utilizing non-isothermal differential scanning calorimetry (DSC) and thermogravimetry (TGA). Structural relaxation of the amorphous matrix was described in terms of the Tool-Narayanaswamy-Moynihan model with the following parameters: Δ ≈ 200-300 kJ·mol, = 0.57, = 0.44. The crystallization of the amorphous phase was modeled using complex Šesták-Berggren kinetics, which incorporates temperature-dependent activation energy and degree of autocatalysis. The activation energy of the crystal growth was determined to be >320 kJ·mol at the glass transition temperature (). Owing to such a high value, the amorphous carbamazepine is stable at , allowing for extensive processing of the amorphous phase (e.g., self-healing of the quench-induced mechanical defects or internal stress). A discussion was conducted regarding the converse relation between the activation energies of relaxation and crystal growth, which is possibly responsible for the absence of sub- crystal growth modes. The high-temperature thermal decomposition of carbamazepine proceeds via multistep kinetics, identically in both an inert and an oxidizing atmosphere. A complex reaction mechanism, consisting of a series of consecutive and competing reactions, was proposed to explain the second decomposition step, which exhibited a temporary mass increase. Whereas a negligible degree of carbamazepine degradation was predicted for the temperature characteristic of the pharmaceutical hot-melt extrusion (~150 °C), the degradation risk during the pharmaceutical 3D printing was calculated to be considerably higher (1-2% mass loss at temperatures 190-200 °C).

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC12250088PMC
http://dx.doi.org/10.3390/ijms26136136DOI Listing

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