The early stage of interaction between viruses and hosts is a detrimental step for successful virus replication and further infection. In order to understand the early stage of interaction during virus infection, the host transcriptome change in response to virus early infection was studied. Arabidopsis cDNA microarray was conducted to monitor host transcriptome change during the early stage of infection of Tobacco mosaic virus (TMV). A host gene, PAP85, with low expression level in most development stages but continuatively up-regulated in early stage of TMV infection was identified. Virus accumulation could be inhibited by down-regulation of PAP85. My data also indicated that TMV may adapt PAP85 to alter endoplasmic reticulum (ER) structure in facilitating the formation of virus replication complexes. A transcription factor (TF), WRKY6, which was up-regulated at 4 hour post virus infection was selected for further study. The WRKY6 TF was known to involve in plant resistance to pathogens in previous studies. TMV inoculation assay was conducted in WRKY6-overexpressed and -knockout protoplasts and plants. Although WRKY6 may not have the effect on the initial establishment of virus replication, WRKY6 plays both supportive and inhibitory roles in TMV accumulation. I also tried to understand whether histone modification are involved in early stage of virus infection. I performed mutant screening of histone acetyltransferase (HATs) and histone deacetylases (HDACs), and identified one of the HATs, HAC2, belonging to CBP family was required for TMV accumulation in Arabidopsis protoplasts. Combined these findings indicate that regulation of host gene expression, TF and histone modification are all involved in the early stage of virus-host interaction. Controlling these factors which are altered by virus infection in early stage may be a practicable and valid strategy in virus management.