We propose to develop novel bioadhesive microspheres which will serve as
oral drug delivery systems for diseases of the gastrointestinal tract.
This project involves the correlation between in vitro bioadhesion
properties measured by using specialized tensile technique and in vivo
retention times as well as development of delivery systems for drugs used
in the treatment of inflammatory bowel diseases (IBDs), such as ulcerative
colitis and Crohn's disease. An important hypothesis to be tested include
the concept that protonated carboxyl groups are vital for bioadhesion, and
that these may function effectively on flexible chains such as swollen
hydrogel polymer as well as on more rigid chains on bioerodible
thermoplastic polymers. To address this issue, we plan to couple three
investigative approaches. First, we will conduct direct surface
characterization of the various microspheres to quantify the amount of
carboxyl groups or any other mucin specific ligands. These studies will be
done by using ESCA as well as ATIR. Second, an electrobalance will be used
to make direct in vitro measurements of the adhesive forces between
polymer microspheres and representative tissues of the GI tract, while
maintaining regional pH environments. Third, the direct in vivo evaluation
of adhesive, radio-opaque microspheres, retained beyond the normal time of
gastrointestinal transit, will be studied through serial X-ray imaging of
animals. Overall, the work will consist of the following phases: polymer
selection from a pool of synthetic and naturally-occurring polymers;
synthesis and characterization of the selected materials; preparation of
bioadhesive microspheres carrying barium sulfate, 5-aminosalicylic acid or
a combination thereof; bioadhesion studies in vitro; bioadhesion studies
in vivo: and in vivo delivery system efficiency tests.
No Sub Projects information available for 5R01GM047636-02
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