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Infect. Immun., Apr 1996, 1335-1341, Vol 64, No. 4
DR Demuth, R Savary, E Golub and BJ Shenker
We have previously demonstrated that sonic extracts of Fusobacterium
nucleatum FDC 364 were capable of inhibiting human T-cell responses to
mitogens and antigens. The purified F. nucleatum immunosuppressive protein
(FIP) is composed of two subunits of 44 and 48 kDa. Furthermore, FIP
inhibits T-cell activation by arresting cells in the middle of the G(1)
phase of the cell cycle; the data available to date suggest that FIP
impairs the expression of the proliferating-cell nuclear antigen. To
initiate delineation of FIP structure-function relationships, molecular
cloning of the FIP gene was carried out. A DNA library of F. nucleatum FDC
364 was constructed by partial digestion of genomic DNA with Sau3A and
screened for the production of FIP with polyclonal antibody. Twelve
immunoreactive clones were identified. One of these clones contained a
3.1-kbp insert and was chosen for further study. Cell lysates were found to
contain an immunoreactive band that comigrated with the 44-kDa subcomponent
of the native FIP. Sequencing of the 3.1-kpb insert revealed the presence
of three open reading frames (ORFs). One ORF extends from nucleotides 415
to 1620, encodes 402 amino acids, and is preceded by a ribosome-binding
site. Deletion analysis and antibody elution analysis showed that this ORF
encodes the 44-kDa subunit (FipA) of native FIP. A second ORF is situated
upstream of fipA. However, Northern (RNA) analysis suggested that fipA is
not transcribed as part of an operon but transcribed from its own promotor.
Finally, the partially purified recombinant FipA protein was capable of
impairing T-cell activation in a manner consistent with the native protein.
These results indicate that the two components that form the native protein
are most probably distinct gene products and suggest that the 44-kDa FipA
polypeptide is sufficient to mediate the immunosuppressive activities of
the native protein complex.
Copyright © 1996, American Society for Microbiology
Identification and analysis of fipA, a Fusobacterium nucleatum immunosuppressive factor gene
Department of Pathology, University of Pennsylvania School of Dental Medicine, Philadelphia 19104-6002, USA.
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