Abstract
BackgroundPancreatic neuritis is a histopathological hallmark of pancreatic neuropathy and correlates to abdominal neuropathic pain sensation in pancreatic adenocarcinoma (PCa) and chronic pancreatitis (CP). However, inflammatory cell subtypes that compose pancreatic neuritis and their correlation to the neuropathic pain syndrome in PCa and CP are yet unknown.MethodsInflammatory cells within pancreatic neuritis lesions of patients with PCa (n = 20) and CP (n = 20) were immunolabeled and colorimetrically quantified with the pan-leukocyte marker CD45, with CD68 (macrophages), CD8 (cytotoxic T-lymphocytes), CD4 (T-helper cells), CD20 (B-lymphocytes), NCL-PC (plasma cells), neutrophil elastase, PRG2 (eosinophils), anti-mast cell (MC) tryptase and correlated to pain sensation. Perineural mast cell subtypes were analyzed by double immunolabeling with MC chymase. Expression and neural immunoreactivity of protease-activated receptor type 1 (PAR-1) and type 2 (PAR-2) were analyzed in PCa and CP and correlated to pain status of the patients.ResultsIn PCa and CP, nerves were predominantly infiltrated by cytotoxic T-lymphocytes (PCa: 35% of all perineural inflammatory cells, CP: 33%), macrophages (PCa: 39%, CP: 33%) and MC (PCa: 21%, CP: 27%). In both entities, neuropathic pain sensation was associated with a specific increase of perineural MC (PCa without pain: 14% vs. PCa with pain: 31%; CP without pain: 19% vs. CP with pain: 34%), not affecting the frequency of other inflammatory cell subtypes. The vast majority of these MC contained MC chymase. PAR-1 and PAR-2 expression did not correlate to the pain sensation of PCa and CP patients.ConclusionPancreatic neuritis in PC and CP is composed of cytotoxic T-lymphocytes, macrophages and MC. The specific enrichment of MC around intrapancreatic nerves in neuropathic pain due to PCa and CP suggests the presence of MC-induced visceral hypersensitivity in the pancreas. Therefore, pancreatic and enteric neuropathies seem to share a similar type of neuro-immune interaction in the generation of visceral pain.
Highlights
Inflammation and cancer are intertwined in the generation, course and outcome of human malignancies
Later studies made the deciding contribution related to the importance of this targeted neural immune cell infiltration termed pancreatic neuritis in pancreatic cancer (PCa) and chronic pancreatitis (CP) patients: Increasing frequency and severity of pancreatic neuritis have been shown to bear a major correlation to the severity of abdominal pain sensation and neuroplastic alterations in PCa and CP patients [1,4,5]
We investigated the quantitative distribution of a large panel of leukocyte subset markers in PCa and CP tissue, including CD68, CD8, CD4 (T-helper cells), CD20 (B-lymphocytes), NCL-PC, neutrophil elastase, proteogylcan 2 / PRG2 and anti-mast cell (MC) tryptase and chymase within neural inflammatory clusters
Summary
Inflammation and cancer are intertwined in the generation, course and outcome of human malignancies. A specific and unique subtype of cancer-related inflammation is encountered around nerves in pancreatic tumours, especially in pancreatic cancer (PCa) and in the inflammatory pancreatic head tumour associated with chronic pancreatitis (CP). Both of these tumours frequently contain focal inflammatory cell clusters around intrapancreatic nerves [1,2]. Pancreatic neuritis is a histopathological hallmark of pancreatic neuropathy and correlates to abdominal neuropathic pain sensation in pancreatic adenocarcinoma (PCa) and chronic pancreatitis (CP). Inflammatory cell subtypes that compose pancreatic neuritis and their correlation to the neuropathic pain syndrome in PCa and CP are yet unknown
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