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Literature DB >> 7495297

Analysis of the role of membrane polarity in polycystic kidney disease of transgenic SBM mice.

L Barisoni¹, M Trudel, N Chrétien, L Ward, J van Adelsberg, V D'Agati.

Abstract

Altered membrane polarity has been proposed as an important pathogenetic factor in the development of renal cysts in polycystic kidney disease. To determine whether this alteration in epithelial phenotype is a primary or secondary phenomenon, we examined the epithelial membrane polarity of SBM transgenic mice, in which epithelial proliferation mediated by the c-myc oncogene is an established primary event. Kidneys from 32 transgenic mice and 10 age-matched controls from fetal to adult age were immunostained with antibodies to Na,K-ATPase, fodrin, ankyrin, E-cadherin, and tubule segment-specific lectins. In normal control mice, Na,K-ATPase localization was apical in fetal kidneys but became translocated to the basolateral membrane at maturity. Early microcysts in fetal transgenic kidneys displayed similar (95 to 100%) apical Na,K-ATPase. In young and newborn transgenic mice (1 to 8 days of age), Na,K-ATPase localization was extremely heterogeneous. Noncystic tubules demonstrated either apical (mean 23 to 28%), basolateral (mean 48 to 58%), mixed (mean 4 to 15%), or absent (mean 10 to 13%) staining for Na,K-ATPase. Apical Na,K-ATPase was more frequently observed in early cysts (mean 55%) in young transgenic mice but became less prevalent in adult mice (mean 22%), where 30% of cysts had basolateral staining, 39% mixed patterns, and 9% absent staining. Macrocysts typically lost all Na,K-ATPase reactivity. At all ages, Na,K-ATPase colocalized well with cytoskeletal proteins ankyrin and fodrin. These heterogeneous patterns of Na,K-ATPase staining indicate that although altered cell polarity is frequent in early cystic epithelium of SBM mice, it is not a prerequisite to cystogenesis or progressive cyst enlargement. In conclusion, our results support the view that altered cystic membrane polarity is not a primary process, but represents the persistence of an immature epithelial phenotype characteristic of proliferative polycystic kidney disease epithelia.

Entities: Disease Gene Species

Mesh：

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Year: 1995 PMID： 7495297 PMCID： PMC1869945

Source DB: PubMed Journal: Am J Pathol ISSN： 0002-9440 Impact factor: 4.307

28 in total

1. C-myc as an inducer of polycystic kidney disease in transgenic mice.

Authors: M Trudel; V D'Agati; F Costantini
Journal: Kidney Int Date: 1991-04 Impact factor: 10.612

2. Ankyrin binding to (Na+ + K+)ATPase and implications for the organization of membrane domains in polarized cells.

Authors: W J Nelson; P J Veshnock
Journal: Nature Date: 1987 Aug 6-12 Impact factor: 49.962

3. Renal epithelial cyst formation and enlargement in vitro: dependence on cAMP.

Authors: R Mangoo-Karim; M Uchic; C Lechene; J J Grantham
Journal: Proc Natl Acad Sci U S A Date: 1989-08 Impact factor: 11.205

4. Epidermal growth factor (EGF) expression in the congenital polycystic mouse kidney.

Authors: S Horikoshi; S Kubota; G R Martin; Y Yamada; P E Klotman
Journal: Kidney Int Date: 1991-01 Impact factor: 10.612

5. Aberrant epithelial cell growth in autosomal dominant polycystic kidney disease.

Authors: P D Wilson
Journal: Am J Kidney Dis Date: 1991-06 Impact factor: 8.860

6. Linkage heterogeneity of autosomal dominant polycystic kidney disease.

Authors: W J Kimberling; P R Fain; J B Kenyon; D Goldgar; E Sujansky; P A Gabow
Journal: N Engl J Med Date: 1988-10-06 Impact factor: 91.245

7. Reversed polarity of Na(+) -K(+) -ATPase: mislocation to apical plasma membranes in polycystic kidney disease epithelia.

Authors: P D Wilson; A C Sherwood; K Palla; J Du; R Watson; J T Norman
Journal: Am J Physiol Date: 1991-03

6. Differential expression of E-cadherin, N-cadherin and beta-catenin in proximal and distal segments of the rat nephron.

Authors: Walter C Prozialeck; Peter C Lamar; Denah M Appelt
Journal: BMC Physiol Date: 2004-05-17

6 in total

Analysis of the role of membrane polarity in polycystic kidney disease of transgenic SBM mice.

1. C-myc as an inducer of polycystic kidney disease in transgenic mice.

2. Ankyrin binding to (Na+ + K+)ATPase and implications for the organization of membrane domains in polarized cells.

3. Renal epithelial cyst formation and enlargement in vitro: dependence on cAMP.

4. Epidermal growth factor (EGF) expression in the congenital polycystic mouse kidney.

5. Aberrant epithelial cell growth in autosomal dominant polycystic kidney disease.

6. Linkage heterogeneity of autosomal dominant polycystic kidney disease.

7. Reversed polarity of Na(+) -K(+) -ATPase: mislocation to apical plasma membranes in polycystic kidney disease epithelia.

8. Elevated c-myc protooncogene expression in autosomal recessive polycystic kidney disease.

9. The PKD1 gene produces a developmentally regulated protein in mesenchyme and vasculature.

10. A highly polymorphic DNA marker linked to adult polycystic kidney disease on chromosome 16.

1. C-myc-induced apoptosis in polycystic kidney disease is Bcl-2 and p53 independent.

Review 2. Cell adhesion molecules in chemically-induced renal injury.

3. Polycystic kidney disease in SBM transgenic mice: role of c-myc in disease induction and progression.

Review 4. Recent advances in understanding the pathogenesis of polycystic kidney disease: therapeutic implications.

5. Distinct roles and regulations for HoxD genes in metanephric kidney development.

6. Differential expression of E-cadherin, N-cadherin and beta-catenin in proximal and distal segments of the rat nephron.