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Curcuminoid by na b





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Curcuminoid


 
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Cyclodextrins
Curcurminoids form a more stable complex[disambiguation needed] with solutions which contain cyclodextrin towards hydrolytic degradations. The stability differs between size and characterzation of the cyclodextrins that are used. Dissolution of demethoxycurcumin, bisdemethoxycurcumin and curcumin are greatest in the hydroxypropyl--cyclodextrin (HPCD) cavity. The curcuminoids which have a substituent connected to the phenyl groups show more affinity for the HPCD compound. Degradation rate is depended on pH of the solution and how much protection the cyclodextrins provide the curcuminoids. The derivatives are usually more stable than curcumin against hydrolysis in cyclodextrin solution. No covalent bonds are synthesized between the cyclodextrins and the curcuminoids so they are easily released from the complex.
Micelles and nanoparticles
A drug design with curcuminoids in complex with micelles could be one solution of the insolubility of the curcuminoids. The curcuminoids would be in complex with the core of the micelles similar to the complex inside the cyclodextrins. The micelles are dissolved in a suitable solvent where the headgroups of the micelles interact with the solvent. Curcuminoids as loaded solid lipid nanoparticles (SLN) have been developed with great success by using microemulsion technique. The loading capacity, the mean particle size and size distribution are all factors that have to be considered when the effects of curcuminoids in different strength are observed because it could variate. The advantages of SLN are the possibilities of controlled drug release and drug targeting, protection of incorporated compound against chemical degradation, no biotoxicity of the carrier, avoidance of organic solvent and no problems with respect to large scale production. In vitro studies show a prolonged release of curcuminoids from the nanoparticle preparate up to 12 hours and the curcuminoids maintained their physical and chemical stability after 6 months of storage in the absence of light at room temperature. The sensitivity of curcurminoids to light and oxygen is greatly reduced by formulation of curcuminoids in SLN.
SLN
Cosmetics
SLN preparate has been developed for cosmetics where the curcuminoids are used in cream base. But there are some stability issues which have not been overcome yet, further studies need to be done to find a suitable formulation which can be carried out in order to prolong the stability of the curcuminoids. Nevertheless there have been improvements in formulation of some stable model cream preparations with SLN curcuminoids. It is suggested that most of the curcuminoids are incorporated at the SLN surface where they are diffused into the cream matrix until a steady state is reached. At this state the curcuminoids go from the cream to the dissolution medium. A possible burst release in creams containing curcuminoids have been reported where the curcuminoids are rapidly released in a sufficient amount from the cream into the skin and is followed by a controlled release. When SLN are prepared by microemulsion at a temperature with the range of 70-75C an oil-in-water microemulsion is spontaneously formed. The SLN are obtained immediately when they are dispersed in the warm microemulsion into cold water, with the help of a homogenizer. The cold water facilitates a rapid crystallization of the lipids and therefore prevents aggregation of the lipids. After freeze drying the yellow curcuminoids containing SLN were obtained and could easily be redispersed in water and the model cream. The SLN have uniform distribution and according to electron micrograph scan they had a spherical shape and smooth surface. It has been reported that increasing the lipid content over 5-10%(w/w) increased the mean particle size and broader size distribution in most common cases. That range should there for be ideal concentration for formulation of the SLN.
Incorporation
Incorporation is one thing that needs to be considered in formulation of SLN. Concentration of the lipid, emulsifier and co-emulsifier solution is a key factor on this conversion of the SLN. If the amount of emulsifier and co-emulsifier are increased but the lipid amount is constant the surface of the SLN which is formed will be too small to adsorb all the surfactant and co-surfactant molecules, and a formation of curcuminoids solution micelles will be created. This will then increase the water solubility of the curcuminoids and they could partition from the SLN into the micelles that were formed during a wash procedure. This will reduce the final incorporation efficacy on the surface of the SLN.
Anti-oxidant activity
The curcumin derivatives demethoxycurcumin and bisdemethoxycurcumin have, like curcurmin itself been tested for their antioxidant activities in vitro. Antioxidants can be used to extend the shelf life for food and maintain their safety, nutritional quality, functionality and palatability. Pure chemicals of curcumin and its derivatives are not available in the open market. Commercial curcumin contains 77% curcumin, 17% demethoxycurcumin and 3% bisdemethoxycurcumin from the herb Curcuma longa. Curcumin is mainly produced in industry as pigment by using turmeric oleoresin as the starting material which curcuminoids can be isolated from. After the isolation of the curcurminoids, the extract which is about 75% liquor mainly contains oil, resin and more curcuminoids which can be isolated further. This isolation method was used to demonstrate the antioxidant activities of curcuminoids, where they isolated pure curcuminoids from the main liquor. One research reported that curcumin was the strongest antioxidant, demethoxycurcumin the second strongest and bisdemethoxycurcumin the least effective. Curcuminoids nevertheless showed activity against oxidation. Curcuminoids act as a superoxide radical scavenger as well as singlet oxygen quencher and gives the antioxidant its effectiveness. Of the naturally accruing curcuminoids, one of the main metabolites of curcumin, tetrahydrocurcumin is the most potent antioxidant. The curcuminoids are capable of inhibiting damage to super coiled plasmid DNA by hydroxyl radicals. It was concluded that the derivatives of curcumin are good in trapping the 2,2-diphenyl-1-picryhydrazyl(DPPH) radical as efficiently as curcumin which is a well known antioxidant.
Anti-inflammatory activity
Anti-inflammatory effects of curcumin and its derivatives are because of the hydroxyl and phenol groups in the molecules. These groups are essential for inhibition of prostaglandin synthetase and leukotrienes synthesis. A system with conjugated double bonds or dienes is also believed to be responsible for the anti-inflammatory effect as well as antiparasitic activity. The diene system seems to make the compounds more lipophilic and therefore provide a better skin penetration which could be good for that kind of drug preparation.
Chemotherapeutic activity
Studies suggest that the bioavailability of curcumin and possibly its derivatives is greatest in the colon. The tissue in the gastrointestinal tract seems to be more exposed predominantly to unmetabolised curcumin than other tissues hence they could support clinical studies of curcumin as a colorectal cancer preventive agent. Demethoxycurcumin has recently been tested in colon cancer and it showed more effective inhibitation of cell division and apoptosis than curcumin. It is possible that the difference in apoptosis in vitro is connected to the degradation of the two chemicals and/or their stability.
References
^ a b c Pret-Almeida L, Cherubino APF, Alves RJ, Dufoss L, Glria MBA (October-November 2005). "Separation and determination of the physico-chemical characteristics of curcumin, demethoxycurcumin and bisdemethoxycurcumin". Food Research International 38 (8-9): 103944. http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6T6V-4GHRBYJ-9&_user=5915660&_coverDate=11%2F30%2F2005&_rdoc=1&_fmt=&_orig=search&_sort=d&view=c&_acct=C000068853&_version=1&_urlVersion=0&_userid=5915660&md5=31ef8e5c0d8983d74eb098289189a40f. 
^ a b Tomren MA, Msson M, Loftsson T, Tnnesen HH (June 2007). "Studies on curcumin and curcuminoids XXXI. Symmetric and asymmetric curcuminoids: stability, activity and complexation with cyclodextrin". Int J Pharm 338 (1-2): 2734. doi:10.1016/j.ijpharm.2007.01.013. PMID 17298869. http://linkinghub.elsevier.com/retrieve/pii/S0378-5173(07)00048-8. 
^ a b c d e f g h i j k l Tiyaboonchai W, Tungpradit W, Plianbangchang P (June 2007). "Formulation and characterization of curcuminoids loaded solid lipid nanoparticles". Int J Pharm 337 (1-2): 299306. doi:10.1016/j.ijpharm.2006.12.043. PMID 17287099. http://linkinghub.elsevier.com/retrieve/pii/S0378-5173(07)00012-9. 
^ a b c d e f g h i j Jayaprakasha GK, Rao LJ, Sakariah KK (2006). "Antioxidant activities of curcumin, demethoxycurcumin and bisdemethoxycurcumin". Food Chemistry 98 (4): 7204. http://portal.isiknowledge.com/portal.cgi?DestApp=WOS&Func=Frame. 
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