Oral dosage form is the most preferred route for the treatment of various diseases and disorder but in the gut wall it offers various barriers for the drug delivery. On oral administration of conventional dosage forms drug normally dissolves in the gastro-intestinal fluids and is absorbed from these regions of the gastro-intestinal tract, which depends upon the physicochemical properties of the drug. It has a serious drawback in conditions where localized delivery of the drug in the colon is required or in conditions where a drug needs to be protected from the hostile environment of upper GIT. Dosage forms that deliver drugs in the colon rather than upper GIT has number of advantages. Oral delivery of drugs in the colon is valuable in the treatment of diseases of colon (colon cancer, ulcerative colitis, crohn's disease and inflammatory bowel disease) whereby high local concentration can be achieved while minimizing side effects. The colon is attracting interest as a site where poorly absorbed drug molecule may have an improved bioavailability. This region of the colon having a somewhat less hostile environment with less diversity and intensity of activity than the stomach and small intestine. Additionally, the colon has a long retention time and appears highly responsible to agents that enhance the absorption of poorly absorbed drugs. The simplest method for targeting of drugs to the colon is to obtain slower release rates or longer release periods by the application of thicker layers of conventional enteric coating or extremely slow releasing matrices. Further, drug targeting to colon would prove useful where intestinal delayed drug absorption is desired from therapeutic point of view in the treatment of diseases that have peak symptoms in the early morning such as nocturnal asthma, angina or arthritis.
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