2004
DOI: 10.1002/glia.20009
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Neuronal expression of CD22: Novel mechanism for inhibiting microglial proinflammatory cytokine production

Abstract: Although considered an immunologically privileged site, the central nervous system (CNS) can display significant inflammatory responses, which may play a pathogenic role in a number of neurological diseases. Microglia appear to be particularly important for initiating and sustaining CNS inflammation. These cells exist in a quiescent form in the normal CNS, but acquire macrophage-like properties (including active phagocytosis, upregulation of proteins necessary for antigen presentation, and production of proinf… Show more

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Cited by 156 publications
(119 citation statements)
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“…On the other hand, it has been noted that neurons are able to generate various molecules that are demonstrated to suppress inflammation, such as TREM2, CD22, CD200, CD59 and fractalkine (Hsieh et al 2009;Mott et al 2004;Ransohoff 2007;Singhrao et al 1999;Walker et al 2009). Interestingly, several of these molecules have been found to be deficient in AD.…”
Section: Neuronmentioning
confidence: 99%
“…On the other hand, it has been noted that neurons are able to generate various molecules that are demonstrated to suppress inflammation, such as TREM2, CD22, CD200, CD59 and fractalkine (Hsieh et al 2009;Mott et al 2004;Ransohoff 2007;Singhrao et al 1999;Walker et al 2009). Interestingly, several of these molecules have been found to be deficient in AD.…”
Section: Neuronmentioning
confidence: 99%
“…CD45 is also an inhibitory receptor for CD22, a molecule expressed by B cells and CNS neurons [38]! The higher levels of CD45 expressed by peripheral immune cells suggests that neurons have a greater potential to inhibit acutely infiltrating macrophages than CNS resident microglia!…”
Section: Is Microgliosis Another Name For Macrophage Infiltration Intmentioning
confidence: 99%
“…Remarkably, genes products that are involved in the proinflammatory response such as chemokine [C-C motif] ligand 2 (Ccl2 or MCP-1) 24 or prostaglandin E receptor 2 (EP2 or Ptger2) 25 were down-regulated, whereas anti-inflammatory associated genes such as Cd22 26 or protein tyrosine phosphatase, nonreceptor type 2 (Ptpn2) 27 were up-regulated in brains of EH mice. Inflammation processes in AD brains lead to both enhanced cytotoxicity as well as enhanced A␤ aggregation.…”
Section: Inflammationmentioning
confidence: 99%