TY - JOUR
T1 - Phosphated crosslinked guar for colon-specific drug delivery - II. In vitro and in vivo evaluation in the rat
AU - Gliko-Kabir, Irit
AU - Yagen, Boris
AU - Baluom, Muhammad
AU - Rubinstein, Abraham
PY - 2000/1/3
Y1 - 2000/1/3
N2 - Targeting of drugs to the colon, following oral administration, can be accomplished by the use of modified, biodegradable polysaccharides as vehicles. In a previous study, a crosslinked low swelling guar gum (GG) hydrogel was synthesized by reacting it with trisodium trimetaphosphate (STMP). In the present study the functioning of GG crosslinked products (GGP) as possible colon-specific drug carriers was analyzed by studying (a) the release kinetics of pre-loaded hydrocortisone from GGP hydrogels into buffer solutions with, or without GG degrading enzymes (α-galactosidase and β- mannanase) and (b) direct measurements of the polymers' degradation in the cecum of conscious rats. The effect of GG diet on α-galactosidase and β- mannanase activity in the cecum of the rat and GGP degradation was also measured. It was found that the product GGP-0.1 (loosely crosslinked with 0.1 equivalents of STMP) was able to prevent the release of 80% of its hydrocortisone load for at least 6 h in PBS, pH = 6.4. When a mixture of α- galactosidase and β-mannanase was added to the buffer solution, an enhanced hydrocortisone release was observed. In-vivo degradation studies in the rat cecum showed that despite the chemical modification of GG, it retained its enzyme-degrading properties in a crosslinker concentration-dependent manner. Eight days of GG diet prior to the study increased α-galactosidase activity in the cecum of the rat three-fold, compared to its activity without the diet. However, this increase in the enzyme activity was unable to improve the degradation of the different GGP products. The overall α-galactosidase activity in the rat cecum was found to be extracellular, while the activity of β-mannanase was found to be bacterial cell-wall associated. It is concluded that because CG crosslinked with STMP can be biodegraded enzymatically and is able to retard the release of a low water-soluble drug, this polymer could potentially be used as a vehicle for colon-specific drug delivery.
AB - Targeting of drugs to the colon, following oral administration, can be accomplished by the use of modified, biodegradable polysaccharides as vehicles. In a previous study, a crosslinked low swelling guar gum (GG) hydrogel was synthesized by reacting it with trisodium trimetaphosphate (STMP). In the present study the functioning of GG crosslinked products (GGP) as possible colon-specific drug carriers was analyzed by studying (a) the release kinetics of pre-loaded hydrocortisone from GGP hydrogels into buffer solutions with, or without GG degrading enzymes (α-galactosidase and β- mannanase) and (b) direct measurements of the polymers' degradation in the cecum of conscious rats. The effect of GG diet on α-galactosidase and β- mannanase activity in the cecum of the rat and GGP degradation was also measured. It was found that the product GGP-0.1 (loosely crosslinked with 0.1 equivalents of STMP) was able to prevent the release of 80% of its hydrocortisone load for at least 6 h in PBS, pH = 6.4. When a mixture of α- galactosidase and β-mannanase was added to the buffer solution, an enhanced hydrocortisone release was observed. In-vivo degradation studies in the rat cecum showed that despite the chemical modification of GG, it retained its enzyme-degrading properties in a crosslinker concentration-dependent manner. Eight days of GG diet prior to the study increased α-galactosidase activity in the cecum of the rat three-fold, compared to its activity without the diet. However, this increase in the enzyme activity was unable to improve the degradation of the different GGP products. The overall α-galactosidase activity in the rat cecum was found to be extracellular, while the activity of β-mannanase was found to be bacterial cell-wall associated. It is concluded that because CG crosslinked with STMP can be biodegraded enzymatically and is able to retard the release of a low water-soluble drug, this polymer could potentially be used as a vehicle for colon-specific drug delivery.
KW - α-Galactosidase
KW - β- Mannanase
KW - Colonic delivery
KW - Crosslinked guar
KW - Enzymes induction
KW - Guar diet
KW - Hydrocortisone
KW - Rat
UR - http://www.scopus.com/inward/record.url?scp=0033977611&partnerID=8YFLogxK
U2 - 10.1016/S0168-3659(99)00180-7
DO - 10.1016/S0168-3659(99)00180-7
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C2 - 10640586
AN - SCOPUS:0033977611
SN - 0168-3659
VL - 63
SP - 129
EP - 134
JO - Journal of Controlled Release
JF - Journal of Controlled Release
IS - 1-2
ER -