Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P43026 (
lipopolysaccharide
)
62,215
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Granzymes are serine proteases released by cytotoxic lymphocytes to induce apoptosis in virus-infected cells and tumor cells. Evidence is emerging that granzymes also play a role in controlling inflammation. Granzyme serum levels are elevated in patients with autoimmune diseases and infections, including sepsis. However, the function of extracellular granzymes in inflammation largely remains unknown. Here, we show that
granzyme K
(GrK) binds to Gram-negative bacteria and their cell-wall component
lipopolysaccharide
(
LPS
). GrK synergistically enhances
LPS
-induced cytokine release in vitro from primary human monocytes and in vivo in a mouse model of
LPS
challenge. Intriguingly, these extracellular effects are independent of GrK catalytic activity. GrK disaggregates
LPS
from micelles and augments
LPS
-CD14 complex formation, thereby likely boosting monocyte activation by
LPS
. We conclude that extracellular GrK is an unexpected direct modulator of
LPS
-TLR4 signaling during the antimicrobial innate immune response.
...
PMID:Granzyme K synergistically potentiates LPS-induced cytokine responses in human monocytes. 2471 7
Granzymes are serine proteases that, upon release from cytotoxic cells, induce apoptosis in tumor cells and virally infected cells. In addition, a role of granzymes in inflammation is emerging. Recently, we have demonstrated that extracellular
granzyme K
(GrK) potentiates
lipopolysaccharide
(
LPS
)-induced cytokine response from monocytes. GrK interacts with
LPS
, disaggregates
LPS
micelles, and stimulates
LPS
-CD14 binding and Toll-like receptor signaling. Here we show that human GrA also potentiates cytokine responses in human monocytes initiated by
LPS
or Gram-negative bacteria. Similar to GrK, this effect is independent of GrA catalytic activity. Unlike GrK, however, GrA does not bind to
LPS
, has little influence on
LPS
micelle disaggregation, and does not augment
LPS
-CD14 complex formation. We conclude that GrA and GrK differentially modulate
LPS
-Toll-like receptor signaling in monocytes, suggesting functional redundancy among cytotoxic lymphocyte proteases in the anti-bacterial innate immune response.
...
PMID:Granzymes A and K differentially potentiate LPS-induced cytokine response. 2802 41
