Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
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Gene/Protein
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Target Concepts:
Gene/Protein
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Query: EC:3.1.1.53 (
sialidase
)
2,694
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mycoplasma alligatoris causes acute lethal primary infection of susceptible hosts. A genome survey implicated
sialidase
and hyaluronidase, potential promoters of
CD95
-mediated eukaryotic cell death, as virulence factors of M. alligatoris. We used immunofluorescence imaging and flow cytometry to examine the effects of M. alligatoris infection in vitro on
CD95
expression and apoptosis by alligator cardiac fibroblasts, a major cell type of a target organ of M. alligatoris infection in vivo. A uniform distribution of
CD95
in primary cultured cardiac, skeletal muscle, and embryonic fibroblasts was demonstrated by using polyclonal antibodies against the N or C terminus of mouse or human
CD95
. Anti-
CD95
antibodies reacted on Western blots of fibroblast lysates with a band with the predicted apparent molecular weight of
CD95
, but soluble
CD95
was not detected in plasma from control or M. alligatoris-infected alligators. The proportion of
CD95
-gated cardiac fibroblasts increased threefold (P<0.01) 48 h after inoculation with M. alligatoris. Infection induced morphological changes in cardiac fibroblasts, including translocation of
CD95
characteristic of apoptosis and an eightfold increase (P<0.16) in 5-bromo-2'-deoxyuridine (BrdU) incorporation measured in a terminal deoxynucleotide transferase dUTP nick end-labeling apoptosis assay. The proportion of BrdU-gated controls activated with agonistic immunoglobulin M against human
CD95
also increased threefold (P<0.03 for muscle). Heat-inactivated M. alligatoris and sterile M. alligatoris-conditioned culture supernatant had no effect. This is the first report of a
CD95
homolog in the class Reptilia and establishes a new model that can be used to test the direct bacterial interaction with upstream components of the
CD95
signal transduction pathway.
...
PMID:Mycoplasma alligatoris infection promotes CD95 (FasR) expression and apoptosis of primary cardiac fibroblasts. 1633 59
Mycoplasma alligatoris causes acute lethal cardiopulmonary disease of susceptible hosts. A survey of its genome implicated
sialidase
and hyaluronidase, synergistic regulators of hyaluronan receptor CD44-mediated signal transduction leading to apoptotic cell death, as virulence factors of M. alligatoris. In this study, after the existence of a CD44 homolog in alligators was established by immunolabeling primary pulmonary fibroblasts with monoclonal antibody IM7 against murine CD44, the
sialidase
inhibitor 2,3-didehydro-2-deoxy-N-acetylneuraminic acid (DANA) was used to examine the effects of
sialidase
on fibroblast apoptosis following in vitro infection with M. alligatoris. While their CD44 expression remained constant, infected cells exhibited morphologic changes characteristic of apoptosis including decreased size, rounding, disordered alpha-tubulin, and nuclear disintegration compared to untreated controls. DANA was a potent, non-toxic inhibitor of the
sialidase
activity, equivalent to about 1mU of Clostridium perfringens Type VI
sialidase
, expressed by M. alligatoris in the inoculum. Although DANA did not measurably reduce the proportion of infected fibroblasts labeled by a specific ligand of activated caspases, co-incubation with DANA protected (P<0.01) fibroblasts in a concentration-dependent fashion from the M. alligatoris-induced trends toward increased apoptosis receptor
CD95
expression, and increased 5-bromo-2'-deoxyuridine incorporation measured in a terminal dUTP nick end-labeling apoptosis assay. In contrast, incubation with 200-fold excess purified C. perfringens
sialidase
alone did not affect
CD95
expression or chromatin integrity, or induce fibroblast apoptosis. From those observations we conclude that interaction of its
sialidase
with hyaluronidase or another virulence factor(s) is necessary to elicit the pro-apoptotic effects of M. alligatoris infection.
...
PMID:Role of sialidase in Mycoplasma alligatoris-induced pulmonary fibroblast apoptosis. 1727 29
Protein modifications of death receptor pathways play a central role in the regulation of apoptosis. It has been demonstrated that O-glycosylation of TRAIL-receptor (R) is essential for sensitivity and resistance towards TRAIL-mediated apoptosis. In this study we ask whether and how glycosylation of
CD95
(Fas/APO-1), another death receptor, influences DISC formation and procaspase-8 activation at the
CD95
DISC and thereby the onset of apoptosis. We concentrated on N-glycostructure since O-glycosylation of
CD95
was not found. We applied different approaches to analyze the role of
CD95
N-glycosylation on the signal transduction: in silico modeling of
CD95
DISC, generation of
CD95
glycosylation mutants (at N136 and N118), modulation of N-glycosylation by deoxymannojirimycin (DMM) and
sialidase
from Vibrio cholerae (VCN). We demonstrate that N-deglycosylation of
CD95
does not block DISC formation and results only in the reduction of the procaspase-8 activation at the DISC. These findings are important for the better understanding of
CD95
apoptosis regulation and reveal differences between apoptotic signaling pathways of the TRAIL and
CD95
systems.
...
PMID:Modulation of the CD95-induced apoptosis: the role of CD95 N-glycosylation. 2162 44
