<b>Impact of formulation and media composition on polymer based dispersions</b>

Pradnya Prakash Bapat (19977498)

31 October 2024

<p dir="ltr">Amorphous solid dispersions (ASDs) are being widely used as enabling formulations for poorly water soluble drugs. An ASD is a molecular level mixture of an amorphous drug and a polymer to form a single-phase homogeneous blend. The amorphous form of a drug provides a higher transient solubility compared to equilibrium crystalline solubility, whereby the presence of a polymer of appropriate properties aids in crystallization inhibition. Polymers also improve the release rate of the drug from the ASD relative to the release rate of neat amorphous drug, specifically for release regimens where both drug and polymer release congruently. Hydroxypropyl methylcellulose acetate succinate (HPMCAS)-based ASDs tend to show congruent release of drug and polymer across multiple drug loadings, providing a significant dissolution improvement even beyond the amorphous solubility of a drug. Enteric polymers such as HPMCAS have been studied extensively in terms of enteric coated tablets but haven’t been explored in as much detail when molecularly dispersed with a drug as in case of ASDs. Literature shows not all ASDs are able to improve bioavailability of drugs. Such a failure to provide bioavailability advantage via certain ASDs could come from a randomized drug and polymer selection in the preformulation stage of drug product development which could fundamentally arise from the lack of understanding of the release mechanisms of ASDs. Given that HPMCAS is one of the most popularly used polymers for spray drying of ASDs in the pharmaceutical industry, investigating the release mechanisms of HPMCAS-based ASDs is critical. In this study, some of the key formulation design factors, such as drug-polymer interactions, different grades of polymer as well as dissolution media factors such as buffer capacity that impact the release performance of HPMCAS-based ASDs have been investigated. The results from this study are expected to contribute to the fundamental understanding of the failure mechanisms of HPMCAS-based ASDs, reducing empirical screening of drugs during the preformulation stage of the product development and enhance the success rate of ASDs.</p>

Pharmaceutical sciences

Amorphous solid dispersions

dissolution

enteric polymers

Oral peptide delivery

drug-polymer interactions

Thermodynamic and Spectroscopic Studies on the Molecular Interaction of Doxorubicin (DOX) with Negatively Charged Polymeric Nanoparticles

Gaurav, Raval

26 November 2012

The aim of this study was to investigate the molecular interactions of the anti-cancer drug Doxorubicin (DOX) with poly(methacrylic acid) grafted starch nanoparticles (PMAA-g-St). In order to fully understand the DOX/PMAA-g-St system, we conducted in-depth studies on DOX dimer dissociation and DOX/PMAA-g-St binding interactions using various techniques such as isothermal titration calorimetry (ITC), dynamic light scattering (DLS), and fluorescence and absorption spectroscopy. Based on our experimental results, we developed a quantitative thermodynamic model with relevant parameters such as dissociation constant, Kd, as well as enthalpy of binding, ΔH, in order to explain DOX/PMAA-g-St interactions. In addition, we also studied the effect of environmental factors such as pH and NaCl on DOX self-association and DOX/PMAA-g-St complex formation. In conclusion, the combination of results obtained from various techniques as well as the multispecies equilibrium model, enables us to interpret quantitatively the data of drug loading onto and release from polymeric nanoparticles.

Doxorubicin

Isothermal Titration Calorimetry

Dynamic Light Scattering

Drug/Polymer Interactions

Electrostatic Interactions

Specific binding

Mechanism of binding

effect of sodium chloride

effect of pH

0491

0494

0495

0572

Thermodynamic and Spectroscopic Studies on the Molecular Interaction of Doxorubicin (DOX) with Negatively Charged Polymeric Nanoparticles

Gaurav, Raval

26 November 2012

The aim of this study was to investigate the molecular interactions of the anti-cancer drug Doxorubicin (DOX) with poly(methacrylic acid) grafted starch nanoparticles (PMAA-g-St). In order to fully understand the DOX/PMAA-g-St system, we conducted in-depth studies on DOX dimer dissociation and DOX/PMAA-g-St binding interactions using various techniques such as isothermal titration calorimetry (ITC), dynamic light scattering (DLS), and fluorescence and absorption spectroscopy. Based on our experimental results, we developed a quantitative thermodynamic model with relevant parameters such as dissociation constant, Kd, as well as enthalpy of binding, ΔH, in order to explain DOX/PMAA-g-St interactions. In addition, we also studied the effect of environmental factors such as pH and NaCl on DOX self-association and DOX/PMAA-g-St complex formation. In conclusion, the combination of results obtained from various techniques as well as the multispecies equilibrium model, enables us to interpret quantitatively the data of drug loading onto and release from polymeric nanoparticles.

Doxorubicin

Isothermal Titration Calorimetry

Dynamic Light Scattering

Drug/Polymer Interactions

Electrostatic Interactions

Specific binding

Mechanism of binding

effect of sodium chloride

effect of pH

0491

0494

0495

0572