Abstract

The overall objective of the work proposed in this application and accomplished during the previous 16 years the grant has been active is to define and understand the mechanisms regulating GI adaptation. During the past 5 years, we have concentrated our studies on the adaptations that occur during normal development and in response to mucosal damage, specifically the process of healing. These studies have shown that polyamines are involved in both processes and that they are required for the healing of mucosal stress erosions. The current proposal describes studies directed towards elucidating the role of polyamines in the process of mucosal healing. The work is divided into 8 specific aims that involve studies utilizing the rat stress ulcer model or the IEC-6 culture system. Using the rat stress ulcer model, we will 1) determine the cellular and intracellular localization of ornithine decarboxylase (ODC) before and after damage; 2) determine whether polyamines are essential to healing by virtue of their ability to take part in protein cross-linking; and 3) determine whether the activity of transglutaminase (TGase) which catalyzes protein cross-linking is altered during injury or healing. Using both the stress ulcer model and IEC-6 cells in vitro, we will 4) determine the role of polyamines in the regulation of TGase activity, and 5) elucidate whether the control of TGase is at the transcriptional level. We then plan to use the IEC-6 cells to 6) establish a methodology for measuring cell migration in vitro, and 7) determine the role of polyamines, protein cross-linking and TGase in cell migration. finally, we will 8) use a variety of synthetically modified polyamine analogues to determine the structure- function relationships that are important for the polyamine involvement in healing, TGase activity and cell migration. This last specific aim will provide significant insight into the mechanism of action of polyamines at the molecular level. We know that mucosal healing involves both an early phase of cell migration and then cell division to replace lost cells. Our data indicate that polyamines are essential to both. The actual mechanisms involved in these processes, and especially in cell migration in the injured mucosa are virtually unstudied. Investigation of the role of polyamines in these processes should provide important information about this clinically significant event.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK037260-10
Application #
5210581
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
10
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Ray, Ramesh M; Patel, Anami; Viar, Mary Jane et al. (2002) RhoA inactivation inhibits cell migration but does not mediate the effects of polyamine depletion. Gastroenterology 123:196-205
Wang, J Y; Viar, M J; Li, J et al. (1998) Differences in transglutaminase mRNA after polyamine depletion in two cell lines. Am J Physiol 274:C522-30
Wang, J Y; Viar, M J; Li, J et al. (1997) Polyamines are necessary for normal expression of the transforming growth factor-beta gene during cell migration. Am J Physiol 272:G713-20
Santos, M F; Viar, M J; McCormack, S A et al. (1997) Polyamines are important for attachment of IEC-6 cells to extracellular matrix. Am J Physiol 273:G175-83
Santos, M F; McCormack, S A; Guo, Z et al. (1997) Rho proteins play a critical role in cell migration during the early phase of mucosal restitution. J Clin Invest 100:216-25
Wang, J Y; McCormack, S A; Johnson, L R (1996) Role of nonmuscle myosin II in polyamine-dependent intestinal epithelial cell migration. Am J Physiol 270:G355-62
Banan, A; Wang, J Y; McCormack, S A et al. (1996) Relationship between polyamines, actin distribution, and gastric healing in rats. Am J Physiol 271:G893-903
Mayorga-Wark, O; Dubinsky, W P; Schultz, S G (1996) Reversal of glibenclamide and voltage block of an epithelial KATP channel. Am J Physiol 271:C1122-30
Harari, Y; Grossie Jr, V B; Castro, G A (1996) Nutritional support for adaptation to radiation-induced suppression of mucosal immunity in the intestine of the rat. Radiat Res 145:754-61
Mayorga-Wark, O; Dubinsky, W P; Schultz, S G (1995) Reconstitution of a KATP channel from basolateral membranes of Necturus enterocytes. Am J Physiol 269:C464-71

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