Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
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Drug
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Target Concepts:
Gene/Protein
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Query: UMLS:C0037116 (
silicosis
)
1,822
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Chronic exposure to crystalline silica (CS) causes
silicosis
, an irreversible lung inflammatory disease that may eventually lead to lung cancer. In this study, we demonstrate that in K-ras(LA1) mice, CS exposure markedly enhances the lung tumour burden and genetic deletion of leukotriene B4 receptor-1 (
BLT1
(-/-)) attenuates this increase. Pulmonary neutrophilic inflammation induced by CS is significantly reduced in
BLT1
(-/-)K-ras(LA1) mice. CS exposure induces LTB4 production by mast cells and macrophages independent of inflammasome activation. In an air-pouch model, CS-induced neutrophil recruitment is dependent on LTB4 production by mast cells and
BLT1
expression on neutrophils. In an implantable lung tumour model, CS exposure results in rapid tumour growth and decreased survival that is attenuated in the absence of
BLT1
. These results suggest that the LTB4/
BLT1
axis sets the pace of CS-induced sterile inflammation that promotes lung cancer progression. This knowledge may facilitate development of immunotherapeutic strategies to fight
silicosis
and lung cancer.
...
PMID:Crystalline silica-induced leukotriene B4-dependent inflammation promotes lung tumour growth. 2592 88
The high affinity leukotriene B
4
receptor,
BLT1
mediates chemotaxis of diverse leukocyte subsets to the sites of infection or inflammation. Whereas the pathological functions of LTB
4
/
BLT1
axis in allergy, autoimmunity and cardiovascular disorders are well established; its role in cancer is only beginning to emerge. In this review, we summarize recent findings on LTB
4
/
BLT1
axis enabling distinct outcomes toward tumor progression. In a mouse lung tumor model promoted by
silicosis
-induced inflammation, genetic deletion of
BLT1
attenuated neutrophilic inflammation and tumor promotion. In contrast, in a spontaneous model of intestinal tumorigenesis, absence of
BLT1
led to defective mucosal host response, altered microbiota and bacteria dependent colon tumor progression. Furthermore,
BLT1
mediated CD8
+
T cell recruitment was shown to be essential for initiating anti-tumor immunity in number of xenograft models and is critical for effective PD1 based immunotherapy. BLT2 mediated chemotherapy resistance, tumor promotion and metastasis are also discussed. This new information points to a paradigm shift in our understanding of the LTB
4
pathways in cancer.
...
PMID:The yin and yang of leukotriene B
4
mediated inflammation in cancer. 2898 16
