Retrotransposon Insertion in the T-cell Acute Lymphocytic Leukemia 1 (Tal1) Gene Is Associated with Severe Renal Disease and Patchy Alopecia in Hairpatches (Hpt) Mice

Vishnu Hosur,Gregory A Cox,Bonnie L Lyons,Kimberly A Martin,Kenneth R Johnson,Lynn Alley,Leonard D Shultz,Lisa M Burzenski,Anoop Kavirayani,Melissa L Cox,Rebecca L Riding,Christine A Kozak

doi:10.1371/journal.pone.0053426

Vishnu Hosur, Gregory A Cox + Show 10 more

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Journal: PLoS ONE	Publication Date: Jan 2, 2013
Citations: 9	License type: CC BY 4.0

Affiliation: Jackson Laboratory

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“Hairpatches” (Hpt) is a naturally occurring, autosomal semi-dominant mouse mutation. Hpt/Hpt homozygotes die in utero, while Hpt/+ heterozygotes exhibit progressive renal failure accompanied by patchy alopecia. This mutation is a model for the rare human disorder “glomerulonephritis with sparse hair and telangiectases" (OMIM 137940). Fine mapping localized the Hpt locus to a 6.7 Mb region of Chromosome 4 containing 62 known genes. Quantitative real time PCR revealed differential expression for only one gene in the interval, T-cell acute lymphocytic leukemia 1 (Tal1), which was highly upregulated in the kidney and skin of Hpt/+ mice. Southern blot analysis of Hpt mutant DNA indicated a new EcoRI site in the Tal1 gene. High throughput sequencing identified an endogenous retroviral class II intracisternal A particle insertion in Tal1 intron 4. Our data suggests that the IAP insertion in Tal1 underlies the histopathological changes in the kidney by three weeks of age, and that glomerulosclerosis is a consequence of an initial developmental defect, progressing in severity over time. The Hairpatches mouse model allows an investigation into the effects of Tal1, a transcription factor characterized by complex regulation patterns, and its effects on renal disease.

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In 1979, the Mouse Mutant Stock Center of The Jackson Laboratory identified a novel spontaneous mutation causing skin abnormalities and progressive renal disease
Through Sanger and high throughput DNA sequencing (HTS), we identified an intracisternal A particle (IAP) insertion in intron 4 of the murine T-cell acute lymphocytic leukemia 1 (Tal1) locus
In this paper we show that an IAP retroviral insertion in Tal1 intron 4 is associated with the Hairpatches phenotype

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In 1979, the Mouse Mutant Stock Center of The Jackson Laboratory identified a novel spontaneous mutation causing skin abnormalities and progressive renal disease. HPT/LeJ, was developed to reduce the phenotypic variability found in the original segregating (C57BL/6J x C3HeB/FeJ-a/a) hybrid background. On the HPT/LeJ strain background, Hpt is semi-dominant, and is lethal in the homozygous state. Hpt/+ mice exhibit renal disease similar to a progressive membranous glomerulosclerosis with striking early abnormalities of the podocytes [1]. Our previous genetic linkage analysis localized Hpt to a broad region on Chromosome 4, linked to pintail (Pt) and brown (tyrosinase-related protein 1, Tyrp1) [1] In the current study, Hpt was mapped to a 6.7 Mb region of mouse Chromosome 4, containing 62 genes. Expression of the Tcell acute lymphocytic leukemia (Tal1) gene ( known as stem cell leukemia, Scl) was upregulated in the kidney and skin of Hpt/+

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