| Literature DB >> 27943061 |
Yangyang Yuan1, Dongyang Fan1, Sidong Zhu1, Jifang Yang1, Jigang Chen2.
Abstract
We have previously shown that non-structural protein p35, encoded by Scylla serrata reovirus (SsRV) S10, may act as a viroporin. To characterize the role of p35 protein in the modulation of cellular function, a yeast two-hybrid system was used to screen a cDNA library derived from S. serrata to find its interacting partner. Protein interactions were confirmed in vitro by GST pull-down. Full cDNAs of p35 interactors were cloned by the rapid amplification of cDNA ends. After two-hybrid library screening, we isolated partial cDNAs encoding hemocyanin, cryptocyanin, and TAX1BP1. Interaction of p35 with each of hemocyanin, cryptocyanin, and TAX1BP1 was confirmed by GST pull-down. The full-length cDNA fragments of hemocyanin, cryptocyanin, and TAX1BP1 were 2287, 2422, and 3437 bp, respectively, and they encoded three putative proteins with molecular masses of ~76.9, ~79.2, and ~107.2 kDa, respectively. This study casts new light on the function and physiological significance of p35 during the SsRV replication cycle.Entities:
Keywords: Cryptocyanin; Hemocyanin; Scylla serrata reovirus (SsRV); TAX1BP1; Yeast two-hybrid system
Mesh:
Substances:
Year: 2016 PMID: 27943061 DOI: 10.1007/s11262-016-1418-7
Source DB: PubMed Journal: Virus Genes ISSN: 0920-8569 Impact factor: 2.332