Tsc2+/– mice develop tumors in multiple sites that express gelsolin and are influenced by genetic background
Hiroaki Onda, … , Henry B. Warren, David J. Kwiatkowski
Hiroaki Onda, … , Henry B. Warren, David J. Kwiatkowski
Published September 15, 1999
Citation Information: J Clin Invest. 1999;104(6):687-695. https://doi.org/10.1172/JCI7319.
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Article

Tsc2+/– mice develop tumors in multiple sites that express gelsolin and are influenced by genetic background

Abstract

Tuberous sclerosis (TSC) is an autosomal dominant genetic disorder in which benign hamartomas develop in multiple organs, caused by mutations in either TSC1 or TSC2. We developed a murine model of Tsc2 disease using a gene targeting approach. Tsc2-null embryos die at embryonic days 9.5–12.5 from hepatic hypoplasia. Tsc2 heterozygotes display 100% incidence of multiple bilateral renal cystadenomas, 50% incidence of liver hemangiomas, and 32% incidence of lung adenomas by 15 months of age. Progression to renal carcinoma, fatal bleeding from the liver hemangiomas, and extremity angiosarcomas all occur at a rate of less than 10%. The renal cystadenomas develop from intercalated cells of the cortical collecting duct and uniformly express gelsolin at high levels, enabling detection of early neoplastic lesions. The tumor expression pattern of the mice is influenced by genetic background, with fewer large renal cystadenomas in the outbred Black Swiss background and more angiosarcomas in 129/SvJae chimeric mice. The slow growth of the tumors in the heterozygote mice matches the limited growth potential of the great majority of TSC hamartomas, and the influence of genetic background on phenotype correlates with the marked variability in expression of TSC seen in patients.

Authors

Hiroaki Onda, Andreas Lueck, Peter W. Marks, Henry B. Warren, David J. Kwiatkowski

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Figure 6

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Loss of tuberin expression in Tsc2+/– lesions. (a) LOH PCR analysis. The...
Loss of tuberin expression in Tsc2+/– lesions. (a) LOH PCR analysis. The upper band (–) represents the targeted allele; the lower band (+), the wild-type allele. RC, renal carcinoma; C, cyst; LH, liver hemangioma; N, normal control tissue; LA, lung adenoma; RA, renal adenoma. Numbers 1–5 are the animal numbers. Those scored as showing LOH are RC1, LH2, C3, and RA5. (b) Immunolocalization of tuberin in mouse kidney cortex. Tuberin was expressed in intercalated cells (arrow), and to a lesser extent in principal cells, of cortical collecting ducts (CCD) and distal convoluted tubule (DCT). (c) Tuberin expression in intercalated cells of medullary collecting ducts (CD), localized to both the apical and basolateral poles (arrowheads). (d) Expression of gelsolin in a cystadenoma. Intercalated cells of adjacent collecting ducts that also express gelsolin are indicated by arrowheads. (e) Parallel section to b, showing absence of tuberin expression in a cystadenoma. Scale bars are 20 μm (b), 10 μm (c), and 40 μm (d and e).