AI Article Synopsis

  • The study assessed SIGLEC1 (CD169) as a potential biomarker in multiple sclerosis (MS) and neuromyelitis optica spectrum disorder (NMOSD) by measuring its expression on monocytes in patients and healthy controls.
  • Elevated SIGLEC1 expression was found in a small percentage of MS (18.6%) and NMOSD (9.8%) patients, particularly those receiving interferon beta treatment, but not significantly linked to disease severity.
  • SIGLEC1 myeloid cells were primarily present in active MS lesions and various acute diseases, providing a tool for evaluating inflammation in CNS lesions.

Article Abstract

We aimed to evaluate SIGLEC1 (CD169) as a biomarker in multiple sclerosis (MS) and Neuromyelitis optica spectrum disorder (NMOSD) and to evaluate the presence of SIGLEC1 myeloid cells in demyelinating diseases. We performed flow cytometry-based measurements of SIGLEC1 expression on monocytes in 86 MS patients, 41 NMOSD patients and 31 healthy controls. Additionally, we histologically evaluated the presence of SIGLEC1 myeloid cells in acute and chronic MS brain lesions as well as other neurological diseases. We found elevated SIGLEC1 expression in 16/86 (18.6%) MS patients and 4/41 (9.8%) NMOSD patients. Almost all MS patients with high SIGLEC1 levels received exogenous interferon beta as an immunomodulatory treatment and only a small fraction of MS patients without interferon treatment had increased SIGLEC1 expression. In our cohort, SIGLEC1 expression on monocytes was-apart from those patients receiving interferon treatment-not significantly increased in patients with MS and NMOSD, nor were levels associated with more severe disease. SIGLEC1 myeloid cells were abundantly present in active MS lesions as well as in a range of acute infectious and malignant diseases of the central nervous system, but not chronic MS lesions. The presence of SIGLEC1 myeloid cells in brain lesions could be used to investigate the activity in an inflammatory CNS lesion.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8119413PMC
http://dx.doi.org/10.1038/s41598-021-89786-0DOI Listing

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