Author: Coudereau, Rémy; Waeckel, Louis; Cour, Martin; Rimmele, Thomas; Pescarmona, Rémi; Fabri, Astrid; Jallades, Laurent; Yonis, Hodane; Gossez, Morgane; Lukaszewicz, Anneâ€Claire; Argaud, Laurent; Venet, Fabienne; Monneret, Guillaume
Title: Emergence of immunosuppressive LOXâ€1+ PMNâ€MDSC in septic shock and severe COVIDâ€19 patients with acute respiratory distress syndrome Cord-id: wyggm522 Document date: 2021_4_28
ID: wyggm522
Snippet: Myeloidâ€derived suppressor cells (MDSC) are a heterogeneous population of immature myeloid cells with immunosuppressive properties. In cancer patients, the expression of lectinâ€type oxidized LDL receptor 1 (LOXâ€1) on granulocytic MDSC identifies a subset of MDSC that retains the most potent immunosuppressive properties. The main objective of the present work was to explore the presence of LOXâ€1+ MDSC in bacterial and viral sepsis. To this end, whole blood LOXâ€1+ cells were phenotypical
Document: Myeloidâ€derived suppressor cells (MDSC) are a heterogeneous population of immature myeloid cells with immunosuppressive properties. In cancer patients, the expression of lectinâ€type oxidized LDL receptor 1 (LOXâ€1) on granulocytic MDSC identifies a subset of MDSC that retains the most potent immunosuppressive properties. The main objective of the present work was to explore the presence of LOXâ€1+ MDSC in bacterial and viral sepsis. To this end, whole blood LOXâ€1+ cells were phenotypically, morphologically, and functionally characterized. They were monitored in 39 coronavirus diseaseâ€19 (COVIDâ€19, viral sepsis) and 48 septic shock (bacterial sepsis) patients longitudinally sampled five times over a 3 wk period in intensive care units (ICUs). The phenotype, morphology, and immunosuppressive functions of LOXâ€1+ cells demonstrated that they were polymorphonuclear MDSC. In patients, we observed the significant emergence of LOXâ€1+ MDSC in both groups. The peak of LOXâ€1+ MDSC was 1 wk delayed with respect to ICU admission. In COVIDâ€19, their elevation was more pronounced in patients with acute respiratory distress syndrome. The persistence of these cells may contribute to long lasting immunosuppression leaving the patient unable to efficiently resolve infections.
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