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. 2016 Nov;221(11):1227-36.
doi: 10.1016/j.imbio.2016.06.012. Epub 2016 Jun 15.

A novel infection- and inflammation-associated molecular signature in peripheral blood of myasthenia gravis patients

Claudia Barzago  1 Josephine Lum  2 Paola Cavalcante  3 Kandhadayar Gopalan Srinivasan  4 Elisa Faggiani  5 Giorgia Camera  6 Silvia Bonanno  7 Francesca Andreetta  8 Carlo Antozzi  9 Fulvio Baggi  10 Raffaele Adolfo Calogero  11 Pia Bernasconi  12 Renato Mantegazza  13 Lucia Mori  14 Francesca Zolezzi  15
Affiliations
Free article

A novel infection- and inflammation-associated molecular signature in peripheral blood of myasthenia gravis patients

Claudia Barzago et al. Immunobiology. 2016 Nov.
Free article

Abstract

Myasthenia gravis (MG) is a T-cell dependent autoimmune disorder of the neuromuscular junction, characterised by muscle weakness and fatigability. Autoimmunity is thought to initiate in the thymus of acetylcholine receptor (AChR)-positive MG patients; however, the molecular mechanisms linking intra-thymic MG pathogenesis with autoreactivity via the circulation to the muscle target organ are poorly understood. Using whole-transcriptome sequencing, we compared the transcriptional profile of peripheral blood mononuclear cells from AChR-early onset MG (AChR-EOMG) patients with healthy controls: 178 coding transcripts and 229 long non-coding RNAs, including 11 pre-miRNAs, were differentially expressed. Among the 178 coding transcripts, 128 were annotated of which 17% were associated with the 'infectious disease' functional category and 46% with 'inflammatory disease' and 'inflammatory response-associated' categories. Validation of selected transcripts by qPCR indicated that of the infectious disease-related transcripts, ETF1, NFKB2, PLK3, and PPP1R15A were upregulated, whereas CLC and IL4 were downregulated in AChR-EOMG patients; in the 'inflammatory' categories, ABCA1, FUS, and RELB were upregulated, suggesting a contribution of these molecules to immunological dysfunctions in MG. Data selection and validation were also based on predicted microRNA-mRNA interactions. We found that miR-612, miR-3654, and miR-3651 were increased, whereas miR-612-putative AKAp12 and HRH4 targets and the miR-3651-putative CRISP3 target were downregulated in AChR-EOMG, also suggesting altered immunoregulation. Our findings reveal a novel peripheral molecular signature in AChR-EOMG, reflecting a critical involvement of inflammatory- and infectious disease-related immune responses in disease pathogenesis.

Keywords: Inflammation; Myasthenia gravis; Peripheral blood mononuclear cells; Viral infection; Whole-transcriptome sequencing; microRNAs.

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