Illumina HiSeq 2000 paired end sequencing; GSM3395770: 3744-MS-10: SD Rat Liver, 8 h, Vehicle (3 ml/kg saline); Rattus norvegicus; RNA-Seq

3744-MS-10: SD Rat Liver, 8 h, Vehicle (3 ml/kg saline)

In this study we tested the ability to predict organ injury from transcriptomics data in Sprague-Dawley rats at early time points after exposure to thioacetmide (8 and 24 hours). We selected thioacetamide, an organosulfur compound extensively used in animal studies as a hepatotoxin and carcinogen for its ability to cause acute liver damage. Overall design: We treated 30 Sprague-Dawley rats with saline solution (control), 25 mg/kg (low dose), and 100 mg/kg (high dose) to produce different degrees of injury. RNA samples for gene expression analysis were collected from the liver, kidney, and heart at 8 and 24 hours. Number of repicates were five.

In vivo transcriptomic responses to thioacetamide exposure in rat liver, kidney, and heart tissue

Submitted on 21-SEP-2018

Frozen whole kidney and heart samples were powdered in liquid nitrogen, since these organs are histologically heterogeneous. Total RNA was isolated from liver, powdered kidney, and powdered heart, using TRIzol Reagent (Thermo Fisher Scientific, Waltham, MA) and the direct-zol RNA MiniPrep kit (Zymo Research, Irvine, CA). The isolated RNA samples were then submitted to the Vanderbilt University Medical Center VANTAGE Core (Nashville, TN) for RNA quality determination and sequencing At least 200 ng of DNase-treated total RNA with high RNA integrity was used to generate poly-A-enriched mRNA libraries, using KAPA Stranded mRNA sample kits with indexed adaptors (Roche, Indianapolis, IN). Library quality was assessed using the 2100 Bioanalyzer (Agilent), and libraries were quantitated using KAPA library Quantification kits (Roche). Pooled libraries were subjected to 75-bp paired-end sequencing according to the manufacturer's protocol (Illumina HiSeq3000, San Diego, CA). Bcl2fastq2 Conversion Software (Illumina) was used to generate de-multiplexed Fastq files.

In vivo transcriptomic responses to thioacetamide exposure in rat liver, kidney, and heart tissue

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