TY - JOUR
T1 - Examination of the cell sensitizing gene orf43 of ICE R391 suggests a role in ICE transfer enhancement to recipient cells
AU - Armshaw, Patricia
AU - Pembroke, J. Tony
N1 - Publisher Copyright:
© FEMS 2014.
PY - 2015/2/1
Y1 - 2015/2/1
N2 - SXT/R391 family of ICEs have been found to express an unusual function that enhances bacterial cell death post-UV irradiation. Previous analysis of ICE R391 found four core SXT/R391 ICE genes to be involved-orf96, orf90, orf91 and orf43. These genes functioned as part of a UV-inducible pathway, where upon exposure to UV, the levels of the Orf43 protein, a TraV homolog which we propose naming TraVR391, were upregulated, resulting in increased cell sensitization. Here, we examined the effect of orf43 overexpression and found it led to host cell permeabilization. The inducing agent for orf43,UV irradiation, is also known to increase the ICE R391 extrachromosomal form and apparent conjugative transfer rate. We demonstrated, via conjugative transfer deicient mutants, that orf43 overexpression alone restored a small level of ICE R391 transfer to recipient cells via an unknown mechanism other than conjugation. TraV homologs have been reported to function in conjugative transfer. However, TraVR391 is the irst homolog to cause UV-associated cell sensitization. TraVR391 when overexpressed must contain a unique adaptation or function which results in cell lysis and decreased survival. A hypothesis for retaining such a detrimental effect may be in its role of enhancing ICE survival upon cell damage.
AB - SXT/R391 family of ICEs have been found to express an unusual function that enhances bacterial cell death post-UV irradiation. Previous analysis of ICE R391 found four core SXT/R391 ICE genes to be involved-orf96, orf90, orf91 and orf43. These genes functioned as part of a UV-inducible pathway, where upon exposure to UV, the levels of the Orf43 protein, a TraV homolog which we propose naming TraVR391, were upregulated, resulting in increased cell sensitization. Here, we examined the effect of orf43 overexpression and found it led to host cell permeabilization. The inducing agent for orf43,UV irradiation, is also known to increase the ICE R391 extrachromosomal form and apparent conjugative transfer rate. We demonstrated, via conjugative transfer deicient mutants, that orf43 overexpression alone restored a small level of ICE R391 transfer to recipient cells via an unknown mechanism other than conjugation. TraV homologs have been reported to function in conjugative transfer. However, TraVR391 is the irst homolog to cause UV-associated cell sensitization. TraVR391 when overexpressed must contain a unique adaptation or function which results in cell lysis and decreased survival. A hypothesis for retaining such a detrimental effect may be in its role of enhancing ICE survival upon cell damage.
KW - Cell escape mechanism
KW - SXT/R391-like elements
KW - Type IV secretion systems
KW - UV-sensitizing
UR - http://www.scopus.com/inward/record.url?scp=84954230605&partnerID=8YFLogxK
U2 - 10.1093/femsle/fnu057
DO - 10.1093/femsle/fnu057
M3 - Article
C2 - 25688065
AN - SCOPUS:84954230605
SN - 0378-1097
VL - 362
JO - FEMS Microbiology Letters
JF - FEMS Microbiology Letters
IS - 4
M1 - fnu057
ER -