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http://dx.doi.org/10.4333/KPS.2011.41.4.239

Preparation and Characterization of Simvastatin Solid Dispersion using Aqueous Solvent  

Kim, Kwang-Hyeon (College of Pharmacy, Sahm Yook University)
Park, Jun-Bom (College of Pharmacy, Sahm Yook University)
Choi, Won-Jae (College of Pharmacy, Sahm Yook University)
Lee, Han-Seung (College of Pharmacy, Sahm Yook University)
Kang, Chin-Yang (College of Pharmacy, Sahm Yook University)
Publication Information
Journal of Pharmaceutical Investigation / v.41, no.4, 2011 , pp. 239-247 More about this Journal
Abstract
Simvastatin is an inhibitor of 3-hydroxy-3-methylglutaryl-coenzyme A (HMG-CoA) reductase, which catalyzes the conversion of HMG-CoA to mevalonate, an early and rate-limiting step in the biosynthesis of cholesterol. Simvastatin has good permeability, but it also has low solubility (BCS class II), which reduces its bioavailability. To overcome this problem, a solid dispersion is formed using a spray-dryer with polymeric material carrier to potentially enhance the dissolution rate and extend drug absorption. As carriers for solid dispersion, Gelucire$^{(R)}$44/14 and Gelucire$^{(R)}$ 50/13 are semisolid excipients that greatly improve the bioavailability of poorly-soluble drugs. To avoid any toxic effects of an organic solvent, we used aqueous medium to melt Tween$^{(R)}$ 80 and distilled water. The structural behaviors of the raw materials and the solid dispersion were analyzed by differential scanning calorimetry (DSC), powder X-ray diffraction (PXRD) and scanning electron microscopy (SEM). The DSC and PXRD data indicated that the crystalline structure of simvastatin was transformed to an amorphous structure through solid dispersion. Then, solid dispersion-based tablets containing 20 mg simvastatin were prepared with excipients. Dissolution tests were performed in distilled water and artificial intestinal fluid using the USP paddle II method. Compared with that of the commercial tablet (Zocor$^{(R)}$ 20 mg), the release of simvastatin from solid dispersion based-tablet was more efficient. Although the stability study is not complete, this solid dispersion system is expected to deliver poorly water-soluble drugs with enhanced bioavailability and less toxicity.
Keywords
Solid dispersion; Simvastatin; Zocor$^{(R)}$; Gelucire$^{(R)}$; Spray-dryer; Bioavailability;
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Times Cited By KSCI : 7  (Citation Analysis)
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1 Chae, G.S., Lee, J.S., Kim, S.H., Jeong, S.Y., Kim, M.S., Cho, S.H., Lee, H.B., Khang, G., 2002. Enhancement of the stability of BCNU using self-emulsifying drug delivery systems (SMEDDS) and in vitro antitumor activity of self-emulsified BCNU-loaded PLGA wafer, Int. J. Pharm., 231, 311-144.
2 Chiou, W.L., Riegelman, J.L., 1971. Pharmaceutical application of solid dispersion system, J. Pharm. Sci., 60, 1281-1301.   DOI
3 Chiou, W.L., Riegelman, S., 1969. Preparation and dissolution charateristics of several fast-release solid dispersions of griseofulvin, J. Pharm. Sci., 58, 1505-1510.   DOI
4 Craig, D.Q.M., 2002. The mechanism of drug release from solid dispersion in water-soluble polymers. Int, J, Pharm., 231, 131-144.   DOI
5 De Angelis, G., 2004. The influence of statin characteristics on their safety and tolerability. Int. J. Clin. Pract., 58, 945-955.   DOI
6 El-Zein, H., Riad, L., Elbary, A.A., 1998. Enhancement of carbamazepine dissolution - in vitro and in vivo evaluation, Int. J. Pharm., 168, 209-220.   DOI
7 FDA, Center for Drug Evaluation and Research 2000. Guidance for Industry: Waiver of in vivo bioavailability and bioequivalence studies for immediate-release solid oral dosage forms based on a biopharmaceutics classification system.
8 Fini, A., Moyano, J.R., Gines, J.M., Perez-Martinez, J.I., Rabasco, A.M., 2005. Diclofenac salts, II. solid dispersions in PEG6000 and Gelucire 50/13, Eur. J. Pharm. Biopharm., 60, 99-111.   DOI
9 Jeong, J.K., Kim, J.H., Khang, G., Rhee, J.M., Lee, H.B., 2002. Preparation and characterization of solid dispersion of ipriflavone with polyvinylpyrrolidone, J. Korean Pharm. Sci., 32(3), 173-179.   과학기술학회마을   DOI
10 Ahn, Y.S., Lee, H.Y., Hong, K.D., Jung, S.B., Cho, S.H., Rhee, J.M., Lee, H.B., Khang, G., 2004. Effect of types and mixing ratios of water-soluble polymers on in vitro release profile of solid dispersion for acyclovir, J. Kor. Pharm. Sci., 34(4), 289-297.
11 Ahn, Y.S., Lee, H.Y., Hong, K.D., Jung, S.B., Cho, S.H., Rhee, J.M., Lee, H.B., Khang, G., 2004. Preparation and in vitro test of solid dispersion using acyclovir and water soluble polymer, J. Korean Pharm. Sci., 34(3), 169-176.
12 Aiaraksinen, S., Karjalainen, M., Kivikero, N., Westermarck, S., Shevchenko, A., 2005. Excipient selection can significantly affect solic-state phase transformation in formulation during wet granulation. AAPS Pharm Sci Tech. 41, 311-322.
13 Anna, K., Nissim, G., 2006. Microemulsions as transdermal drug delivery vehicles. Adv. Colloid Interface Sci., 123-126, 369-385.   DOI
14 Bates, T.R., 1969. Dissolution characteristics of reserpine-polyvinylpyrrolidone co-precipitates, J. Pharm. Pharmacol., 21, 710-712.   DOI
15 Betageri, G.V., Makarla, K.R., 1995. Enhancement of dissolution of glyburide by solid dispersion and lyophilization techniques, Int. J. Pharm., 126, 155-160.   DOI
16 Brandari, K.H., Newa, M., Kim, J.A., Yoo, B.K., Woo, J.S., Lyoo, W.S., Lim, H.T., Choi, H.G., Yong, C.S., 2007. Preparation, characterization and evaluation of coenzyme Q10 binary solid dispersions for enhanced solubility and dissolution, Biol. Pharm. Bull., 30(6), 1171-1176.   DOI
17 Vilhelmsen, T., Eliasen, H., Schaefer, T., 2005. Effect of a melt agglomeration process on agglomerates containing solid dispersions, Int. J. Pharm., 303, 132-142.   DOI   ScienceOn
18 Yalkowsky, S.H., 1981. Techniques of Solubilization of Drugs, Marcel Dekker, Inc., pp. 15-157.
19 Yuksel, N., Karatas, A., Ozkan, Y., Savaser, A., Ozkan, S.A., Baykara, T., 2003. Enhanced bioavailability of piroxicam using Gelucire 44/14 and labrasol : in vitro and in vivo evaluation, Eur. J. Pharm. Biopharm., 56, 453-459.   DOI
20 Ro, H.S., Ko, W., Yang, H.O., Park, K.K., Cho, Y.H., Park, H.S., 1997. Effect of several solvent extracts from paeoniae radix on experimental hyperlipidemia in rats, J. Kor. Pharm. Sci., 27(2), 145-151.   과학기술학회마을
21 Storda, D., Kontoyannis, C.G., 2008. Identification and quantitative determination of atorvastatin calcium polymorph in tablets using FT-Raman spectroscopy, Talanta, 74, 1066-1070.
22 Bullen, W.W., Miller, R.A., Hayes, R.N., 1999. Development and validation of a high performance liquid chromatography tandem mass spectrometry assay for atorvastatin, ortho-hydroxy atorvastatin, and para-hydroxy atorvastatin in human, dog, and rat plasma, J. Am. Soc. Mass Spectrum., 10, 55-66.   DOI
23 Sah, H.K., Lee, K.S., Beak, M.S., 2006. Implementation of biopharmaceutics classification system concepts in developing dissolution tests, J. Kor. Pharm. Sci., 36(3), 161-167.   과학기술학회마을   DOI
24 Sekiguchi, K., Obi, N., 1961. Studies on absorption of eutectic mixture. I. A comparison of the behavior of eutectic mixtures of sulphathiazole and that of ordinary sulphathiazole in man, Chem. Pharm. Bull., 9, 866-872.   DOI
25 Sekiguchi, K., Obi, N., Ueda, Y., 1964. Studies on absorption of eutectic mixtures. I. Absorption of fused conglomerates of chloramphenicol and urea in rabbits, Chem. Pharm. Bull., 12, 134-144.   DOI   ScienceOn
26 Shibata, Y., Fujii, M., Sugamura, Y., Yoshikawa, R., Fujimoto, S., Nakanishi, S., Motosugi, Y., Koizumi, N., Yamada, M., Ouchi, K., Watanabe, Y., 2009. The preparation of a solid dispersion powder of indomethacin with crospovidone using a twinscrew extruder or kneader, Int. J. Pharm., 365, 53-60.   DOI
27 Tachibana, T., Nakamura A., 1965. A method for preparing an aqueous colloidal dispersion of organic materials by using water-soluble polymers : dispersion of beta-carotene by polyvinylpyrrolidone, Kolloid-Z. Polym., 203, 130-133.   DOI
28 Tran, P.H.L., Tran, H.T.T., Lee, B.J., 2008. Modulation of microenvironmental pH and crystallinity of ionizable telmisartan using alkalizers in solid dispersions for controlles release, J. Controlled Release., 129, 59-65.   DOI
29 Lee, J.W., 2006. The root of ambulatory care, Korea Med Pub, 16-21.
30 Lee, J.H., Ku, J., Park, J.S., Park, J.H., Ahn, S.I., Mo, J.H., Kim, Y.T., Rhee, J.M., Lee, H.B., Khang, G., 2008. Improved dissolution and characterization of solid dispersed atorvastatin calcium, J. Kor. Pharm. Sci., 38(2), 111-117.   과학기술학회마을   DOI
31 Leuner, C., Dressman, J., 2000. Improving drug solubility for oral delivery using solid dispersions (review article), Eur. J. Pharm. Biopharm., 50, 47-60.   DOI
32 Lindenberg, M., Kopp, S., Dressman, J.B., 2004. Classification of orally administered drugs on the World Health Organization model list of essential medicines according to the biopharmaceutics classification system, Eur. J. Pharm. Biopharm., 58, 265-278.   DOI
33 Lo, W.Y., Law, S.L., 1996. Dissolution behavior of griseofulvin solid dispersions using polyethylene glycol, talc, and their combination as dispersion carriers, Drug Dev. Ind. Pharm., 22, 231-236.   DOI
34 Mayersohn, M., Gibaldi, M., 1966. New method of solid-state dispersion for increasing dissolution rates, J. Pharm. Sci., 55, 1323-1324.   DOI
35 Noyes, A.A., Whitney, W.R., 1897. J. Am. Chem. Soc., 19, 930-934.   DOI
36 Ohara, T., Kitamura, S., Kitagawa, T., Terada, K., 2005. Dissolution mechanism of poorly water-soluble drug from extended release solid dispersion system with ethylcellulose and hydroxypropylmethylcellulose, Int. J. Pharm., 302, 95-102.   DOI
37 Oh, H.Y., 2004. Hyperlipidemia. in Handbook of Internal Medicine, 2nd ed., pp. 440-446.
38 Maggon, K., 2005. Best selling human medicines, Drug discovery Today, 10(11), 739-42.   DOI
39 Kang, B.K., Yoon, B.Y., Seo, K.S., Jeung, S.Y., Kil, H.J., Khang, G., Lee, H.B., Cho, S.H., 2003. Preparation of solid dosage form containing SMEDDS of simvastatin by micro encapsulation, J. Kor. Pharm. Sci., 33(2), 121-127.
40 Kang, B.K., Lee, J.S., Chon, S.K., Jeung, S.Y., Yuk, S.H., Khang, G., Lee, H.B., Cho, S.H., 2004. Development of self-microemulsifying drug delivery systems (SMEDDS) for oral bioavailability enhancement of simvastatin in beagle dogs, Int. J. Pharm., 274, 65-73.   DOI   ScienceOn
41 Kanig, J.L., 1964. Properties of fused mannitol in compressed tablets, J. Pharm. Sci., 53, 188-192.   DOI
42 Khang, G., Jeong, J.K., Rhee, J.M., Lee, H.B., 2001. Effect of hydrophilic polymers on solid dispersions of ipriflavone to improve bioavailability, Macromol. Chem. Symp., 14(3), 123-132.
43 Kim, M.S., Jin, S.J., Kim, J.S., Park, H.J., Song, H.S., Neubert, R.H.H., Hwang, S.J., 2008. Preparation, characterization and in vivo evaluation of amorphous atorvastatin calcium nanoparticles using supercritical antisolvent (SAS) process, Eur. J. Pharm. Biopharm., in press.
44 Kearney, A.S., Gabriel, D.L., Mehta, S.C., Radebaugh, G.W., 1994. Effect of polyvinylpyrrolidone on the crystallinity and dissolution rate of solid dispersions of the antiinflammatory Ci-987, Int. J. Pharm., 104, 169-174.   DOI
45 Koh, K.K., Quon, M.J., Rosenson, R.S., Chung, W.J., Han, S.H., 2008. Vascular and metabolic effects of treatment of combined hyperlipidemia : Focus on statins and fibrates, Int. J. Cardiol., 124, 149-159.
46 Lee, J.H., Kim, D.S., Kim, W., Park, J.H., Ahn, S.I., Kim, Y.T., Rhee, J.M., Khang, G., 2008. Improved dissolution of solid dispersed atorvastatin using spray-dryer, J. Kor. Pharm. Sci., 38(4), 249-254.   과학기술학회마을   DOI