Abstract
The intent of the present investigation is to develop and evaluate colon-specific coated tacrolimus solid dispersion pellet (SDP) that retards drug release in the stomach and small intestine but progressively releases in the colon. Tacrolimus-SDP was prepared by extrusion-spheronization technology and optimized by the micromeritic properties including flowability, friability, yields and dissolution rate. Subsequently, the pH-dependent layer (Eudragit L30D55) and time-dependent layer (Eudragit NE30D and L30D55) were coated on the SDP to form tacrolimus colon-specific pellets (CSP) using a fluidized bed coater. Under in vitro gradient pH environment, tacrolimus only released from CSP after changing pH to 6.8 and then quickly released in the phosphate buffer solution of pH 7.2. The Cmax of CSP was 195.68 ± 3.14 ng/mL at Tmax 4.5 ± 0.24 h where as in case of SDP, the Cmax was 646.16 ± 8.15 ng/mL at Tmax 0.5 ± 0.03 h, indicating the ability of CSP targeted to colon. The highest area under the curve was achieved 2479.58 ± 183.33 ng·h/mL for SDP, which was 2.27-fold higher than tacrolimus suspension. However, the best biodistribution performance was achieved from CSP. In conclusion, SDP combining of pH- and time-dependent approaches was suitable for targeted delivery of tacrolimus to colon.
Highlights
Ulcerative colitis (UC) is a type of inflammatory bowel disease related to the autoimmune system
We initially developed tacrolimus solid dispersion pellet (SDP) and optimized the formulation consisting of Eudragit NE30D and Eudragit L30D55 as time-dependent layer, and Eudragit L30D55 as pH-dependent layer for the tacrolimus colon-specific pellet (CSP) to achieve OCDDS
Prolonged mean residence time (MRT), reduced Cmax and trending toward a delayed Tmax were observed for colon-specific pellets (CSP). These results clearly indicated that the controllable release of tacrolimus from CSP successfully resulted in the targeted absorption in vivo
Summary
Ulcerative colitis (UC) is a type of inflammatory bowel disease related to the autoimmune system. The outbreak of acute UC has high mortality. The chronic UC generally deteriorates to colon cancer and eventually requires surgery (De Toni et al, 2015). The medicines of UC treatment include non-steroidal anti-inflammatory drugs, glucocorticoids, synthetic immunosuppressants and biologic agents (Park, Jeen, 2015). Tacrolimus is a type of macrolide lactone with potent immunosuppressive activity, which is used for organ rejection prophylaxis in liver, kidney and small intestine transplantation (Fang, Ma, Gui, 2015). It potentially inhibits calcineurin phosphatase activity and prevents the generation of nuclear factor of activated
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