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Please use this identifier to cite or link to this item: https://hdl.handle.net/11055/1279
Title: T lymphocyte and monocyte subsets are dysregulated in type 1 diabetes patients with peripheral neuropathic pain
Authors: O’Brien JA
McGuire HM
Shinko D
Fazekas de St Groth B
Russo M 
Bailey D
Santarelli DM
Wynne K
Austin PJ
Keywords: CD27
Chronic pain
Diabetic neuropathy
FlowSOM
Immunophenotyping
MAPKAPK2
MK2
Mass cytometry
SPADE
Type 1 diabetes
Issue Date: 9-Jun-2021
Source: 15:100283.
Abstract: Diabetic neuropathic pain is a common and devastating complication of type 1 diabetes, but the mechanism by which it develops and persists is yet to be fully elucidated. This study utilised high-dimensional suspension mass cytometry in a pilot cohort to investigate differences in peripheral blood immunophenotypes between type 1 diabetes patients with (n ​= ​9) and without (n ​= ​9) peripheral neuropathic pain. The abundance and activation of several leukocyte subsets were investigated with unsupervised clustering approaches FlowSOM and SPADE, as well as by manual gating. Major findings included a proportional increase in CD4+ central memory T cells and an absolute increase in classical monocytes, non-classical monocytes, and mature natural killer cells in type 1 diabetes patients with pain compared to those without pain. The expression of CD27, CD127, and CD39 was upregulated on select T cell populations, and the phosphorylated form of pro-inflammatory transcription factor MK2 was upregulated across most populations. These results provide evidence that distinct immunological signatures are associated with painful neuropathy in type 1 diabetes patients. Further research may link these changes to mechanisms by which pain in type 1 diabetes is initiated and maintained, paving the way for much needed targeted treatments.
URI: https://hdl.handle.net/11055/1279
ISSN: 2666-3546
Appears in Collections:Scholarly and Clinical

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