Towards development of plasmacytoma cells-based expression systems utilizing alphavirus vectors: an NS0-VEE model.

Towards development of plasmacytoma cells-based expression systems utilizing alphavirus vectors: an NS0-VEE model. J Virol Methods. 2019 Sep 13;:113734 Authors: Keyer VV, Shevtsov AB, Zaripov MM, Baltabekova AZ, Ramanculov EM, Shustov AV Abstract Plasmacytoma (myeloma) cells have a large protein expression capacity, although their industrial use is confined to stable expression systems. Vectors derived from genomes of viruses from the genus Alphavirus allow obtaining of high yields of target proteins but their use is limited to transient expression. Little information has been published to date on attempts to combine the myeloma cells as hosts with alphaviruses as expression vectors. A plasmid construct which allows rescue of a model alphavirus Venezuelan equine encephalitis virus (VEE) upon transfection of a cell culture was created. Mutations in the capsid and nsP2 genes allow for less cytopathogenic propagation of the virus. A cDNA-copy of the genome was placed in a plasmid under the control of the CMV promoter for virus rescue following DNA transfection. Parameters for the virus rescue by electroporating of the infectious clone in murine myeloma cells (NS0) were optimized. The highest FFU counts (1.2 × 105 FFU per 10 ug DNA) were produced with 2 pulses (voltage 250 V, capacitance 960 u F) and the best electroporation buffer was selected from eight buffers. Self-sustained VEE infection was established in NS0 cultures wi...
Source: Journal of Virological Methods - Category: Virology Authors: Tags: J Virol Methods Source Type: research