2012
DOI: 10.1016/j.jprot.2011.12.020
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Increased expression and phosphorylation of the two S100A9 isoforms in mononuclear cells from patients with systemic lupus erythematosus: A proteomic signature for circulating low-density granulocytes

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Cited by 21 publications
(18 citation statements)
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“…3B) highlighted that spots 1A and 11 corresponded to phosphorylated proteins and spots 2 and 1B to non-phosphorylated proteins. This result is in agreement with the identification of the S100A9 protein species recently obtained by Pavon et al on peripheral blood mononuclear cells from adults [18]. These authors reported a decrease in pI of 0.16 units between the non-phosphorylated long and short S100A9, due to the loss of Lys 4 in the short-form, and an identical pI decrease in phosphorylated long and short S100A9 with respect to the corresponding non-phosphorylated forms.…”
Section: S100 Familysupporting
confidence: 92%
“…3B) highlighted that spots 1A and 11 corresponded to phosphorylated proteins and spots 2 and 1B to non-phosphorylated proteins. This result is in agreement with the identification of the S100A9 protein species recently obtained by Pavon et al on peripheral blood mononuclear cells from adults [18]. These authors reported a decrease in pI of 0.16 units between the non-phosphorylated long and short S100A9, due to the loss of Lys 4 in the short-form, and an identical pI decrease in phosphorylated long and short S100A9 with respect to the corresponding non-phosphorylated forms.…”
Section: S100 Familysupporting
confidence: 92%
“…In support of the gene array analysis, high levels of calprotectin (S100A8/S100A9) were recently reported in a proteomic analysis of SLE PBMCs, in direct correlation with the presence of LDGs. These observations suggest a proteomic signature for circulating LDGs in lupus patients that requires further investigation [26]. Overall, based on the gene expression profile and the ultrastructural analysis of LDGs, it is possible that they represent a more immature granulocyte subset prematurely released from the marrow due to yet uncharacterized stimuli.…”
Section: Gene Array Analysis Of Ldgsmentioning
confidence: 99%
“…Now the research extends beyond rheumatism to diseases such as human immunodeficiency virus (HIV) infection, severe infections, tumors, and neonatal disorders where a significantly increased number of LDGs in PBMCs have been reported (Morisaki et al, 1992;Rodriguez et al, 2009;Lin et al, 2011;Cloke et al, 2012;Hoffmann et al, 2013;Ssemaganda et al, 2014). In the classical autoimmune disease of SLE, the LDG percentage in PBMCs was determined for 35 patients and 31 healthy controls, and the results indicated that the average percentage was 15% in SLE patents and 2% in healthy controls (Pavón et al, 2012). In another study, the LDG average percentage was 18% in 65 patients with SLE and 5% in 22 healthy controls (Denny et al, 2010).…”
Section: Discussionmentioning
confidence: 99%
“…Fluorescein isothiocyanate (FITC)-labeled anti-CD15 (Biolegend, Catalog: 301904) and phycoerythrin (PE)-labeled anti-CD14 (Biolegend, Catalog: 325606) antibodies were used for flow (Biolegend, Catalog: 401605, 400111) were used to calculate the amount of nonspecific staining. Lymphocytes, monocytes, and granulocytes were gated according to their forward and scatter characteristics as previously described (Denny et al, 2010;Pavón et al, 2012). Two color immunofluorescence analyses were performed on a Beckman Coulter Epics XL flow cytometer (Beckman Coulter, Inc., CA, USA).…”
Section: Pbmc Isolation and Ldg Measurementmentioning
confidence: 99%
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