Mechanisms of Th17 and Treg cell dysregulation in oral mucosal inflammation during HIV disease

Purpose: The goal of this study is to compare the transcriptomic profiles of healthy individuals and HIV+ patients on therapy Methods: Cells were pelleted from gingival mucosa. mRNA profiles were generated by Next-gen sequencing using the Illumina platform. Results: Comprehensive transcriptome data that showed underlying changes in the oral mucosal immune system of HIV+ patients on therapy. The transcriptome data of the pooled healthy controls are presented here. Conclusions: Our study represents the analysis of oral gingival transcriptomes. We conclude that RNA-seq based transcriptome characterization would expedite genetic network analyses and permit the dissection of complex biological functional alterations during chronic viral infections such as HIV infection. Overall design: Oral mucosal gingival cell mRNA profiles ex vivo of control (healthy) and HIV+ patients on therapy (HIV + cART)