Abstract

Basic errors in the structure and function of extracellular matrix (or its specialized form basement membrane) leads to a broad spectrum of problems related to developmental abnormalities and secondary complications in such diseases as diabetes mellitus where basement membrane thickening and dysfunction is observed. Our understanding of the cellula mechanisms underlying normal and abnormal basement membrane formation and the role of matrix components in signal transmission during development has been limited by a lack of appropriate in vitro and in vivo models to experimental approach these problems. In order to better approach these problems, we have developed an in vivo cellular model in which basement membrane formation can be experimentally induced between an epithelial bilayer and its formation related to 1) the process of cytodifferentiation and morphogenesis and 2) disease processes which lead to abnormalities in the structure and function of basement membranes. This model has been developed from the invertebrate, Hydra vulgaris which is structurally reduced to an epithelial bilayer with an intervening basement membrane (mesoglea). Building on previously published studies, we have defined experimental conditions in which 1) pellets generated from cells isolated from adult Hydra form an epithelial bilayer, deposit an intervening basement membrane, and subsequently reform an adult Hydra structure within 72-96 hr through the processes of cytodifferentiation and morphogenesis and 2) as related to the disease diabetes mellitus, development of this cell-aggregation-morphogenesis system in the presence of elevated glucose levels leads to an abnormal thickening of basement membrane within 72-96 hr time frame as opposed to months or years as required in mammalian animal model of diabetes. Utilizing this in vivo epithelial/basement membrane model system we propose to test hypotheses directed at the cellular mechanisms involved in the normal and abnormal development of basement membrane and the concomitant transmission of epithelial signal which are involved in tissue cytodifferentiation and morphogenesis. Using a combination of cellular and molecular biology approaches we propose to focus on the following specific aims in order to further develop this nonmammalian in vivo model for application to biomedical research: 1. To examine the process of normal basement membrane formation during development and determine the precise role of basement membrane protein domains in tissue cytodifferentiation and morphogenesis. 2. To examine cellular mechanisms by which elevated glucose levels lead to an abnormal thickening of basement membrane as observed in individuals with diabetes mellitus.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Research Project (R01)
Project #
5R01RR006500-03
Application #
2283225
Study Section
Special Emphasis Panel (SRC (BM))
Project Start
1990-09-30
Project End
1995-09-29
Budget Start
1992-09-30
Budget End
1995-09-29
Support Year
3
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Kansas
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
016060860
City
Kansas City
State
KS
Country
United States
Zip Code
66160

  Publications

Raval, P; Hsu, H H; Anderson, H C (1996) Osteoinductive ability of confluent Saos-2 cell correlates with enhanced expression of bone morphogenetic proteins. J Orthop Res 14:605-10
Yan, L; Pollock, G H; Nagase, H et al. (1995) A 25.7 x 10(3) M(r) hydra metalloproteinase (HMP1), a member of the astacin family, localizes to the extracellular matrix of Hydra vulgaris in a head-specific manner and has a developmental function. Development 121:1591-602
Zhang, X; Hudson, B G; Sarras Jr, M P (1994) Hydra cell aggregate development is blocked by selective fragments of fibronectin and type IV collagen. Dev Biol 164:10-23
Agbas, A; Sarras Jr, M P (1994) Evidence for cell surface extracellular matrix binding proteins in Hydra vulgaris. Cell Adhes Commun 2:59-73
Sarras Jr, M P; Yan, L; Grens, A et al. (1994) Cloning and biological function of laminin in Hydra vulgaris. Dev Biol 164:312-24
Zhang, X; Sarras Jr, M P (1994) Cell-extracellular matrix interactions under in vivo conditions during interstitial cell migration in Hydra vulgaris. Development 120:425-32
Sarras Jr, M P; Zhang, X; Huff, J K et al. (1993) Extracellular matrix (mesoglea) of Hydra vulgaris III. Formation and function during morphogenesis of hydra cell aggregates. Dev Biol 157:383-98
Sarras Jr, M P; Huff, J K; Palmiter-Thomas, P (1992) High molecular weight secretory products of the human pancreatic ductal epithelium and the effect of secretin on their discharge. Pancreas 7:132-43
Hudson, B G; Kalluri, R; Gunwar, S et al. (1992) The pathogenesis of Alport syndrome involves type IV collagen molecules containing the alpha 3(IV) chain: evidence from anti-GBM nephritis after renal transplantation. Kidney Int 42:179-87
Sarras Jr, M P; Meador, D; Zhang, X M (1991) Extracellular matrix (mesoglea) of Hydra vulgaris. II. Influence of collagen and proteoglycan components on head regeneration. Dev Biol 148:495-500

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