Staphylococcus aureus protein A binding to osteoblast tumour necrosis factor receptor 1 results in activation of nuclear factor kappa B and release of interleukin-6 in bone infection.
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Claro T, Widaa A, McDonnell C, Foster TJ, O'Brien FJ, Kerrigan SW, Staphylococcus aureus protein A binding to osteoblast tumour necrosis factor receptor 1 results in activation of nuclear factor kappa B and release of interleukin-6 in bone infection., Microbiology (Reading, England), 159, Pt 1, 2013, 147-54
Abstract
Staphylococcusaureus
is the major pathogen among the staphylococci and the most common
cause of bone infections. These infections are mainly characterized by bone destruction and
inflammation, and are often debilitating and very difficult to treat. Previously we demonstrated that
S.aureus
protein A (SpA) can bind to osteoblasts, which results in inhibition of osteoblast
proliferation and mineralization, apoptosis, and activation of osteoclasts. In this study we used
small interfering RNA (siRNA) to demonstrate that osteoblast tumour necrosis factor receptor-1
(TNFR-1) is responsible for the recognition of and binding to SpA. TNFR-1 binding to SpA results
in the activation of nuclear factor kappa B (NF
k
B). In turn, NF
k
B translocates to the nucleus of the
osteoblast, which leads to release of interleukin 6 (IL-6). Silencing TNFR-1 in osteoblasts or
disruption of the
spa
gene in
S.aureus
prevented both NF
k
B activation and IL-6 release. As well
as playing a key role in proinflammatory reactions, IL-6 is also an important osteotropic factor.
Release of IL-6 from osteoblasts results in the activation of the bone-resorbing cells, the
osteoclasts. Consistent with our results described above, both silencing TNFR-1 in osteoblasts
and disruption of
spa
in
S.aureus
prevented osteoclast activation. These studies are the first to
demonstrate the importance of the TNFR-1–SpA interaction in bone infection, and may help
explain the mechanism through which osteoclasts become overactivated, leading to bone
destruction. Anti-inflammatory drug therapy could be used either alone or in conjunction with
antibiotics to treat osteomyelitis or for prophylaxis in high-risk patients
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Author's Homepage: http://people.tcd.ie/tfoster
Type of material: Journal Article

