Enhancement of Rosuvastatin Calcium Bioavailability Applying Nanocrystal Technology and in-vitro, in-vivo evaluations.

Authors

  • Karthick Palani PSG College of Pharmacy
  • PETER CHRISTOPER GV
  • Sathesh Kumar Kesavan

Abstract

Objective: The objective of this study is to prepare efficient dosage form using nanocrystal technology and to compare with micro and marketed
formulations for its in-vitro and the in-vivo behavior. The nanocrystal technology has good potential to enhance the dissolution profile of poorly
soluble drugs by reducing particle size, increasing surface area, and also by raising the saturation solubility of the drug.
Methods: In this study, solubility of rosuvastatin calcium is increased by adopting nanocrystal technology. Rosuvastatin calcium nanocrystals was
formulated using various stabilizers like sodium lauryl sulfate, hydroxyl propyl cellulose, hydroxyl propyl methyl cellulose, poloxamer 188, tween 80,
poly vinyl pyrrolidine, by adopting two different methods top down and bottom up techniques. Formulations were compressed and physical parameters
of tablets evaluated dissolution studies were performed to evaluate release and pharmacokinetic studies were done to evaluate in-vivo behavior.
Results: Particle size obtained by employing top down method was found to be <749.04 nm (F-1 to F-7) whereas particle size obtained by following
bottom up method was higher than 2000 nm. The micronized particles possessed a size range of 61.51 μm, whereas nanoparticle formulations showed
particle size of 0.509 μm, 0.399 μm respectively. Differential scanning calorimetry studies showed good compatibility between drug and excipients.
Friability values ranging from 0.15±0.0565% to 0.59±0.0283% and disintegration time lies between 29±1.414 and 44±1.414 seconds for the prepared
formulations. The hardness of prepared tablets was between 3.0 and 4.5±0.707 kg/cm2 which are sufficient for maintaining the integrity of tablets.
Friability, disintegration time and hardness for the micronized formulation (M-1) were 0.875±0.0919%, 50±2.828 seconds, 3.5±0.707 kg/cm2,
which are higher than the values obtained for lyophilized nanocrystals in formulation. In-vitro studies have shown a 36% increase in dissolution of
nanocrystal formulation while in-vivo studies exhibited 1.87-fold increases in the bioavailability of rosuvastatin when compared to the micronized
dosage form.
Conclusion: Formulations containing different constituents were prepared by following bottom up and top down techniques and evaluated in-vitro,
in-vivo, observed significant differences between the formulations. The results proved that the bioavailability of rosuvastatin calcium has been
improved considerably by applying nanocrystal technology. In-vitro and in-vivo evaluations showed that solubility and bioavailability have been
enhanced considerably.

Keywords: Rosuvastatin calcium, Nanocrystal technology, Solubility, Bioavailability, Pharmacokinetics.

Downloads

Download data is not yet available.

References

Merisko Liversidge E. Nanocrystals, resolving pharmaceutical formulation issues associated with poorly water-soluble compounds. In: Marty JJ, editor. Particles. Vol. 18. Orlando: Marcel Dekker; 2002. p. 113-20.

Noyes AA, Whitney WR. The rate of solution of solid substances in their own solutions. J Am Chem Soc 1897;19(12):930-4.

Thassu D, Deleers M, Pathak Y. Nanoparticulate Drug Delivery Systems. 1st ed. New York: Publisher Informa Health Care; 2007.

Rabinow BE. Nanosuspensions in drug delivery. Nat Rev Drug Discov 2004;3(9):785-96.

Keck CM, Müller RH. Drug nanocrystals of poorly soluble drugs produced by high pressure homogenisation. Eur J Pharm Biopharm 2006;62:3-16.

Merisko-Liversidge E, Liversidge GG, Cooper ER. Nanosizing: a formulation approach for poorly-water-soluble compounds. Eur J Pharm Sci 2003;18(2):113-20.

Martin A, Bustamante P, Chun AH. Interfacial phenomenon. Physical Pharmacy. Maryland: Lippincott Williams & Wilkins; 1993. p. 362-92.

Sharma P, Garg S. Pure drug and polymer based nanotechnologies for the improved solubility, stability, bioavailability and targeting of anti-HIV drugs. Adv Drug Deliv Rev 2010;62(4-5):491-502.

Amidon GL, Lennernäs H, Shah VP, Crison JR. A theoretical basis for a biopharmaceutic drug classification: the correlation of in vitro drug product dissolution and in vivo bioavailability. Pharm Res 1995;12(3):413-20.

Crisp MT, Tucker CJ, Rogers TL, Williams RO 3rd, Johnston KP. Turbidimetric measurement and prediction of dissolution rates of poorly soluble drug nanocrystals. J Control Release 2007;117(3):351-9.

Jinno J, Kamada N, Miyake M, Yamada K, Mukai T, Odomi M, et al. Effect of particle size reduction on dissolution and oral absorption of a poorly water-soluble drug, cilostazol, in beagle dogs. J Control Release 2006;111(1-2):56-64.

Mauludin R, Müller RH, Keck CM. Development of an oral rutin nanocrystal formulation. Int J Pharm 2009;370(1-2):202-9.

Hecq J, Deleers M, Fanara D, Vranckx H, Amighi K. Preparation and characterization of nanocrystals for solubility and dissolution rate enhancement of nifedipine. Int J Pharm 2005;299(1-2):167-77.

Kesisoglou F, Panmai S, Wu Y. Nanosizing – oral formulation development and biopharmaceutical evaluation. Adv Drug Deliv Rev 2007;59(7):631-44.

Kocbek P, Baumgartner S, Kristl J. Preparation and evaluation of nanosuspensions for enhancing the dissolution of poorly soluble drugs. Int J Pharm 2006;312(1-2):179-86.

Kumar TR, Shitut NR, Kumar PK, Vinu MC, Kumar VV, Mullangi R, et al. Determination of rosuvastatin in rat plasma by HPLC: Validation and its application to pharmacokinetic studies. Biomed Chromatogr 2006;20(9):881-7.

Van Eerdenbrugh B, Van den Mooter G, Augustijns P. Top-down production of drug nanocrystals: nanosuspension stabilization, miniaturization and transformation into solid products. Int J Pharm 2008;364(1):64-75.

Patel B, Sheth A, Doshi N, Dave JB, Patel CN. Comparative in-vitro dissolution study of rosuvastatin calcium and telmisartan by RP-HPLC. J Chem Pharm Res 2010;2(3):237-43.

Choi JS, Li X. Enhanced diltiazem bioavailability after oral administration of diltiazem with quercetin to rabbits. Int J Pharm 2005;297(1-2):1-8.

Jain SK, Awasthi AM, Jain NK, Agrawal GP. Calcium silicate based microspheres of repaglinide for gastroretentive floating drug delivery: preparation and in vitro characterization. J Control Release 2005;107(2):300-9.

Published

01-03-2015

How to Cite

Palani, K., PETER CHRISTOPER GV, and S. K. Kesavan. “ in-Vivo Evaluations”. Asian Journal of Pharmaceutical and Clinical Research, vol. 8, no. 2, Mar. 2015, pp. 88-92, https://journals.innovareacademics.in/index.php/ajpcr/article/view/1965.

Issue

Vol 8 Issue 2 (March - April) 2015

Section

Original Article(s)

The publication is licensed under CC By and is open access. Copyright is with author and allowed to retain publishing rights without restrictions.