KSHV gB associated RGD interactions promote attachment of cells by inhibiting the potential migratory signals induced by the disintegrin-like domain
Loading...
Date
2016-02-24
Access
Authors
Hussein, Hosni
Walker, Lia
Akula, Shaw M.
Journal Title
Journal ISSN
Volume Title
Publisher
Abstract
Background: Kaposi’s sarcoma-associated herpesvirus (KSHV) glycoprotein B (gB) is not only expressed on the
envelope of mature virions but also on the surfaces of cells undergoing lytic replication. Among herpesviruses,
KSHV gB is the only glycoprotein known to possess the RGD (Arg-Gly-Asp) binding integrin domain critical to
mediating cell attachment. Recent studies described gB to also possess a disintegrin-like domain (DLD) said to
interact with non-RGD binding integrins. We wanted to decipher the roles of two individually distinct integrin
binding domains (RGD versus DLD) within KSHV gB in regulating attachment of cells over cell migration.
Methods: We established HeLa cells expressing recombinant full length gB, gB lacking a functional RGD (gBΔR),
and gB lacking a functionally intact DLD (gBΔD) on their cell surfaces. These cells were tested in wound healing
assay, Transwell migration assay, and adhesion assay to monitor the ability of the RGD and DLD integrin recognition
motifs in gB to mediate migration and attachment of cells. We also used soluble forms of the respective gB
recombinant proteins to analyze and confirm their effect on migration and attachment of cells. The results
from the above studies were authenticated by the use of imaging, and standard biochemical approaches as
Western blotting and RNA silencing using small interfering RNA.
Results: The present report provides the following novel findings: (i) gB does not induce cell migration; (ii) RGD
domain in KSHV gB is the switch that inhibits the ability of DLD to induce cellular migration thus promoting
attachment of cells.
Conclusions: Independently, RGD interactions mediate attachment of cells while DLD interactions regulate
migration of cells. However, when both RGD and DLD are functionally present in the same protein, gB, the RGD
interaction-induced attachment of cells overshadows the ability of DLD mediated signaling to induce migration
of cells. Furthering our understanding of the molecular mechanism of integrin engagement with RGD and DLD motifs within gB could identify promising new therapeutic avenues and research areas to explore
Description
Citation
DOI
http://dx.doi.org/10.1186/s12885-016-2173-9