Bhutani, Utkarsh and Ronghe, Anshaj and Majumdar, Saptarshi
(2018)
Piperine as a Placebo: Stability of Gelatin Capsules without a Cross-Linker.
ACS Applied Bio Materials, 1 (5).
pp. 1244-1253.
ISSN 2576-6422
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Abstract
Gelatin has been the biomaterial of choice for decades now. Its low cost, renewable, nontoxic and
biodegradable properties make it one of the most desirable materials for controlled release applications.
However, the usage of gelatin is limited by its poor mechanical/thermal stability and high water
solubility. Chemical cross-linkers and hydrophobic modifications of gelatin have solved this problem
but they lead to the problem of toxicity and/ or high processing cost. This research attempts to employ
a nontoxic hydrophobic drug molecule to curb early degradation of gelatin in an aqueous environment.
We report the design of non-cross-linked gelatin capsules with high dissolution resistance in an aqueous
medium. Piperine, a hydrophobic drug (Solubility: 40mg/L in water) was coated on the gelatin capsules
to enhance its stability in an aqueous environment. The hydrophobic piperine molecules repelled the
water molecules to intensify its dissolution resistance. This stabilization was used to control the release
of naproxen sodium, encapsulated inside the gelatin matrix. Piperine, in this case, acts as a placebo i.e
it has zero therapeutic effect but its presence was necessary to control the early degradation of gelatin
matrix. The deposition of piperine was done using the solvent evaporation method where ethanol was
used as the solvent. The wettability studies revealed the hydrophobic nature of surface after the
deposition of piperine while SEM analysis showed the presence of long cylindrical (fiber-like)
structures over the gelatin surface. Further investigation (FTIR/ATR and molecular dynamics) revealed
that the long fiber structures were due to the crystallization of piperine over the surface of gelatin. This
crystallization was triggered by the intermolecular association (hydrogen bond) of ethanol and piperine.
These observations enabled us to optimize the piperine loading protocol over the gelatin capsules that
helped in achieving a zero order naproxen release for 32 hours.
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