Alison H. Harrill; Paul B. Watkins; Stephen Su; Pamela K. Ross; David E. Harbourt; Ioannis M. Stylianou; Gary A. Boorman; Mark W. Russo; Richard S. Sackler; Stephen C. Harris; Philip C. Smith; Raymond Tennant; Molly Bogue; Kenneth Paigen; Christopher Harris; Tanupriya Contractor; Timothy Wiltshire; Ivan Rusyn; David W. Threadgill

Mouse population-guided resequencing reveals that variants in CD44 contribute to acetaminophen-induced liver injury in humans

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Figure 4.

Haplotype association mapping of acetaminophen-induced liver injury in the mouse. Serum ALT at 4 h (A) and 24 h (B) after acetaminophen (300 mg/kg) treatment was used to identify genomic intervals significantly associated with liver injury. Peaks (numbered, see Table 1) indicate a significant logP association score at each 3-SNP marker window. Marker colors indicate chromosome number across the mouse genome.