Abstract

The major goal of this proposal is to determine the cellular and molecular mechanisms responsible for activation of extracellular matrix genes in bladder fibrosis. Congenital and acquired obstructive uropathies, as the sequelae to neurologic lesions (myelomeningocele, tethered cord syndrome) or physical alteration (posterior urethral valves, benign prostatic hyperplasia, radiation therapy) can result in fibrosis of the bladder wall. The applicant has demonstrated that the terminal response is an accumulation of type III collagen in an abnormal location and an alteration in the ratio of types III to I collagen. To evaluate potential molecular control mechanisms responsible for bladder fibrosis, she will utilize a cell culture model system consisting of human bladder wall cells (detrusor smooth muscle cells and lamina propria fibroblasts) and bladder wall cells from mice which carry genetic mutations in the potential regulatory pathway proteins, transforming growth factor-beta (TGFB) and angiotensin. She will test the hypothesis that extracellular matrix changes in bladder wall cells are regulated by expression of transforming grow factor-beta via a cascade mechanism involving a positive feedback response of angiotensin. She will determine the role of these tissue factors in regulating cell growth (hyperplasia), cell enlargement (hypertrophy) and extracellular matrix gene and protein expression. These experiments will allow determination of the molecular and biochemical impact of each stimulus on a given cell type to determine further what role each cell type within the bladder wall contributes to the pathologic process. In vivo model of mice which have been genetically manipulated to produce less type I collagen or type III collagen, thereby producing a bladder model in which the normal type III: type I collagen ratio has been altered. Using length-tension studies and whole bladder cystometry on these genetically altered bladders; biochemical alterations will be correlated to physiologic functional properties (bladder compliance). We will initiate studies in vivo and in vitro to attempt to identify signaling molecules and transcription factors, which are part of the signaling pathways, which lead to bladder fibrosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK048215-07
Application #
6329394
Study Section
Special Emphasis Panel (ZRG4-UROL (01))
Program Officer
Mullins, Christopher V
Project Start
1993-09-30
Project End
2003-11-30
Budget Start
2000-12-01
Budget End
2001-11-30
Support Year
7
Fiscal Year
2001
Total Cost
$295,459
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Anatomy/Cell Biology
Type
Schools of Dentistry
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Wei, Wenjie; Howard, Pamela S; Macarak, Edward J (2013) Recombinant insulin-like growth factor-1 activates satellite cells in the mouse urethral rhabdosphincter. BMC Urol 13:62
Wei, Wenjie; Howard, Pamela S; Kogan, Barry et al. (2012) Urinary diversion results in marked decreases in proliferation and apoptosis in fetal bladder. J Urol 188:1306-12
Wei, Wenjie; Howard, Pamela S; Zderic, Steven A et al. (2008) Beta and gamma-sarcoglycans are decreased in the detrusor smooth muscle cells of the partially obstructed rabbit bladder. J Urol 179:2052-6
Wei, Wenjie; Howard, Pamela S; Kogan, Barry et al. (2007) Altered extracellular matrix expression in the diverted fetal sheep bladder. J Urol 178:1104-7
Stevenson, Karen; Kucich, Umberto; Whitbeck, Catherine et al. (2006) Functional changes in bladder tissue from type III collagen-deficient mice. Mol Cell Biochem 283:107-14
Macarak, Edward J; Schulz, Jake; Zderic, Stephen A et al. (2006) Smooth muscle trans-membrane sarcoglycan complex in partial bladder outlet obstruction. Histochem Cell Biol 126:71-82
Howard, Pamela S; Kucich, Umberto; Coplen, Douglas E et al. (2005) Transforming growth factor-beta1-induced hypertrophy and matrix expression in human bladder smooth muscle cells. Urology 66:1349-53
He, Yuling; Macarak, Edward J; Korostoff, Jonathan M et al. (2004) Compression and tension: differential effects on matrix accumulation by periodontal ligament fibroblasts in vitro. Connect Tissue Res 45:28-39
Howard, Pamela S; Renfrow, David; Schechter, Norman M et al. (2004) Mast cell chymase is a possible mediator of neurogenic bladder fibrosis. Neurourol Urodyn 23:374-82
Matsumoto, Seiji; Kogan, Barry A; Levin, Robert M et al. (2003) Response of the fetal sheep bladder to urinary diversion. J Urol 169:735-9

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