Formulation pre-screening of inhalation powders using computational atom-atom systematic search method

Vasuki Ramachandran; Darragh Murnane; Robert B. Hammond; Jonathan Pickering; Kevin J. Roberts; Majeed Soufian; Ben Forbes; Sara Jaffari; Gary P. Martin; Elizabeth Collins; Klimentina Pencheva

doi:10.1021/mp500335w

Formulation pre-screening of inhalation powders using computational atom-atom systematic search method

Vasuki Ramachandran, Darragh Murnane^*, Robert B. Hammond, Jonathan Pickering, Kevin J. Roberts, Majeed Soufian, Ben Forbes, Sara Jaffari, Gary P. Martin, Elizabeth Collins, Klimentina Pencheva

^*Corresponding author for this work

Institute of Pharmaceutical Science

Research output: Contribution to journal › Article › peer-review

45 Citations (Scopus)

Abstract

The synthonic modeling approach provides a molecule-centered understanding of the surface properties of crystals. It has been applied extensively to understand crystallization processes. This study aimed to investigate the functional relevance of synthonic modeling to the formulation of inhalation powders by assessing cohesivity of three active pharmaceutical ingredients (APIs, fluticasone propionate (FP), budesonide (Bud), and salbutamol base (SB)) and the commonly used excipient, α-lactose monohydrate (LMH). It is found that FP (-11.5 kcal/mol) has a higher cohesive strength than Bud (-9.9 kcal/mol) or SB (-7.8 kcal/mol). The prediction correlated directly to cohesive strength measurements using laser diffraction, where the airflow pressure required for complete dispersion (CPP) was 3.5, 2.0, and 1.0 bar for FP, Bud, and SB, respectively. The highest cohesive strength was predicted for LMH (-15.9 kcal/mol), which did not correlate with the CPP value of 2.0 bar (i.e., ranking lower than FP). High FP-LMH adhesive forces (-11.7 kcal/mol) were predicted. However, aerosolization studies revealed that the FP-LMH blends consisted of agglomerated FP particles with a large median diameter (∼4-5 μm) that were not disrupted by LMH. Modeling of the crystal and surface chemistry of LMH identified high electrostatic and H-bond components of its cohesive energy due to the presence of water and hydroxyl groups in lactose, unlike the APIs. A direct comparison of the predicted and measured cohesive balance of LMH with APIs will require a more in-depth understanding of highly hydrogen-bonded systems with respect to the synthonic engineering modeling tool, as well as the influence of agglomerate structure on surface-surface contact geometry. Overall, this research has demonstrated the possible application and relevance of synthonic engineering tools for rapid pre-screening in drug formulation and design.

Original language	English
Pages (from-to)	18-33
Number of pages	16
Journal	Molecular Pharmaceutics
Volume	12
Issue number	1
Early online date	7 Nov 2014
DOIs	https://doi.org/10.1021/mp500335w
Publication status	Published - 5 Jan 2015

Keywords

budesonide
de-agglomeration
fluticasone propionate
in silico formulation design
inhalation drug delivery
inter-particle interaction
laser diffraction
molecular and synthonic modeling
powder dispersion analysis
salbutamol
α-lactose monohydrate

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10.1021/mp500335w

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title = "Formulation pre-screening of inhalation powders using computational atom-atom systematic search method",

abstract = "The synthonic modeling approach provides a molecule-centered understanding of the surface properties of crystals. It has been applied extensively to understand crystallization processes. This study aimed to investigate the functional relevance of synthonic modeling to the formulation of inhalation powders by assessing cohesivity of three active pharmaceutical ingredients (APIs, fluticasone propionate (FP), budesonide (Bud), and salbutamol base (SB)) and the commonly used excipient, α-lactose monohydrate (LMH). It is found that FP (-11.5 kcal/mol) has a higher cohesive strength than Bud (-9.9 kcal/mol) or SB (-7.8 kcal/mol). The prediction correlated directly to cohesive strength measurements using laser diffraction, where the airflow pressure required for complete dispersion (CPP) was 3.5, 2.0, and 1.0 bar for FP, Bud, and SB, respectively. The highest cohesive strength was predicted for LMH (-15.9 kcal/mol), which did not correlate with the CPP value of 2.0 bar (i.e., ranking lower than FP). High FP-LMH adhesive forces (-11.7 kcal/mol) were predicted. However, aerosolization studies revealed that the FP-LMH blends consisted of agglomerated FP particles with a large median diameter (∼4-5 μm) that were not disrupted by LMH. Modeling of the crystal and surface chemistry of LMH identified high electrostatic and H-bond components of its cohesive energy due to the presence of water and hydroxyl groups in lactose, unlike the APIs. A direct comparison of the predicted and measured cohesive balance of LMH with APIs will require a more in-depth understanding of highly hydrogen-bonded systems with respect to the synthonic engineering modeling tool, as well as the influence of agglomerate structure on surface-surface contact geometry. Overall, this research has demonstrated the possible application and relevance of synthonic engineering tools for rapid pre-screening in drug formulation and design.",

keywords = "budesonide, de-agglomeration, fluticasone propionate, in silico formulation design, inhalation drug delivery, inter-particle interaction, laser diffraction, molecular and synthonic modeling, powder dispersion analysis, salbutamol, α-lactose monohydrate",

author = "Vasuki Ramachandran and Darragh Murnane and Hammond, {Robert B.} and Jonathan Pickering and Roberts, {Kevin J.} and Majeed Soufian and Ben Forbes and Sara Jaffari and Martin, {Gary P.} and Elizabeth Collins and Klimentina Pencheva",

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AU - Ramachandran, Vasuki

AU - Murnane, Darragh

AU - Hammond, Robert B.

AU - Pickering, Jonathan

AU - Roberts, Kevin J.

AU - Soufian, Majeed

AU - Forbes, Ben

AU - Jaffari, Sara

AU - Martin, Gary P.

AU - Collins, Elizabeth

AU - Pencheva, Klimentina

PY - 2015/1/5

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N2 - The synthonic modeling approach provides a molecule-centered understanding of the surface properties of crystals. It has been applied extensively to understand crystallization processes. This study aimed to investigate the functional relevance of synthonic modeling to the formulation of inhalation powders by assessing cohesivity of three active pharmaceutical ingredients (APIs, fluticasone propionate (FP), budesonide (Bud), and salbutamol base (SB)) and the commonly used excipient, α-lactose monohydrate (LMH). It is found that FP (-11.5 kcal/mol) has a higher cohesive strength than Bud (-9.9 kcal/mol) or SB (-7.8 kcal/mol). The prediction correlated directly to cohesive strength measurements using laser diffraction, where the airflow pressure required for complete dispersion (CPP) was 3.5, 2.0, and 1.0 bar for FP, Bud, and SB, respectively. The highest cohesive strength was predicted for LMH (-15.9 kcal/mol), which did not correlate with the CPP value of 2.0 bar (i.e., ranking lower than FP). High FP-LMH adhesive forces (-11.7 kcal/mol) were predicted. However, aerosolization studies revealed that the FP-LMH blends consisted of agglomerated FP particles with a large median diameter (∼4-5 μm) that were not disrupted by LMH. Modeling of the crystal and surface chemistry of LMH identified high electrostatic and H-bond components of its cohesive energy due to the presence of water and hydroxyl groups in lactose, unlike the APIs. A direct comparison of the predicted and measured cohesive balance of LMH with APIs will require a more in-depth understanding of highly hydrogen-bonded systems with respect to the synthonic engineering modeling tool, as well as the influence of agglomerate structure on surface-surface contact geometry. Overall, this research has demonstrated the possible application and relevance of synthonic engineering tools for rapid pre-screening in drug formulation and design.

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KW - in silico formulation design

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KW - powder dispersion analysis

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Formulation pre-screening of inhalation powders using computational atom-atom systematic search method

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Keywords

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