Development of paracetamol-caffeine co-crystals to improve compressional, formulation and in vivo performance

Sumera Latif; Nasir Abbas; Amjad Hussain; Muhammad Sohail Arshad; Nadeem Irfan Bukhari; Hafsa Afzal; Sualeha Riffat; Zeeshan Ahmad

doi:10.1080/03639045.2018.1435687

Development of paracetamol-caffeine co-crystals to improve compressional, formulation and in vivo performance

Drug Dev Ind Pharm. 2018 Jul;44(7):1099-1108. doi: 10.1080/03639045.2018.1435687. Epub 2018 Feb 15.

Authors

Sumera Latif¹, Nasir Abbas¹, Amjad Hussain¹, Muhammad Sohail Arshad², Nadeem Irfan Bukhari¹, Hafsa Afzal¹, Sualeha Riffat³, Zeeshan Ahmad⁴

Affiliations

¹ a University College of Pharmacy, University of the Punjab , Lahore , Pakistan.
² b Department of Pharmacy , Bahaudin Zakiria University , Multan , Pakistan.
³ c University of Veterinary and Animal Sciences , Lahore , Pakistan.
⁴ d Leicester School of Pharmacy, De Montfort University , Leicester , UK.

PMID: 29385849
DOI: 10.1080/03639045.2018.1435687

Abstract

Paracetamol, a frequently used antipyretic and analgesic drug, has poor compression moldability owing to its low plasticity. In this study, new co-crystals of paracetamol (PCM) with caffeine (as a co-former) were prepared and delineated. Co-crystals exhibited improved compaction and mechanical behavior. A screening study was performed by utilizing a number of methods namely dry grinding, liquid assisted grinding (LAG), solvent evaporation (SE), and anti-solvent addition using various weight ratios of starting materials. LAG and SE were found successful in the screening study. Powders at 1:1 and 2:1 weight ratio of PCM/CAF by LAG and SE, respectively, resulted in the formation of co-crystals. Samples were characterized by PXRD, DSC, and ATR-FTIR techniques. Compressional properties of PCM and developed co-crystals were analyzed by in-die heckle model. Mean yield pressure (Py), an inverse measure of plasticity, obtained from the heckle plots decreased significantly (p < .05) for co-crystals than pure drug. Intrinsic dissolution profile of co-crystals showed up to 2.84-fold faster dissolution than PCM and physical mixtures in phosphate buffer pH 6.8 at 37 °C. In addition, co-crystals formulated into tablets by direct compression method showed better mechanical properties like hardness and tensile strength. In vitro dissolution studies on tablets also showed enhanced dissolution profiles (∼90-97%) in comparison to the tablets of PCM prepared by direct compression (∼55%) and wet granulation (∼85%) methods. In a single dose sheep model study, co-crystals showed up to twofold increase in AUC and C_max. A significant (p < .05) decrease in clearance as compared to pure drug was also recorded. In conclusion, new co-crystals of PCM were successfully prepared with improved tabletability in vitro and in vivo profile. Enhancement in AUC and C_max of PCM by co-crystallization might suggest the dose reduction and avoidance of side effects.

Keywords: Paracetamol; bioavailability; caffeine; co-crystals; in vitro dissolution; intrinsic dissolution rate; tabletability.

MeSH terms

Acetaminophen / chemistry*
Animals
Caffeine / chemistry*
Chemistry, Pharmaceutical / methods
Crystallization / methods
Hardness / drug effects
Powders / chemistry
Sheep
Solubility / drug effects
Tablets / chemistry
Tensile Strength / drug effects

Substances

Powders
Tablets
Acetaminophen
Caffeine