GROWTH-INHIBITION OF HERPES-SIMPLEX VIRUS-1 IN THE CELLS EXPRESSING ABUNDANT 2.0-KILOBASE LATENCY-ASSOCIATED TRANSCRIPTS

To elucidate the function of the latency-associated transcript (LAT) o f herpes simplex virus type 1 (HSV-1) in productive infection and late ncy, we established a cell line stably expressing LAT (V24 cells). V24 cells expressed 2.0-kilobase RNA that corresponds to the major specie s of LAT in mouse and human sensory ganglia. When the cells were infec ted with HSV-1 at a low multiplicity of infection, the amount of the p rogeny virus was much smaller in V24 cells than in a control cell line not expressing LAT. Inefficient growth of HSV-I in V24 cells was also observed when viral replication was initiated by transfection with vi ral DNA.