Blood dendritic cells in systemic lupus erythematosus exhibit altered activation state and chemokine receptor function

Gerl, Velia; Lischka, Alexandra; Panne, Daniel; Großmann, Patrick; Berthold, Rita; Hoyer, Bimba F.; Biesen, Robert; Bruns, Anne; Alexander, Tobias; Jacobi, Annett M.; Dörner, Thomas; Burmester, Gerd‐Rüdiger; Radbruch, Andreas; Hiepe, Falk

doi:10.1136/ard.2009.111021

Cited by 52 publications

(38 citation statements)

References 55 publications

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“…However, it is plausible that her facial palsy is a manifestation of underlying SLE. One of the suggested pathophysiological mechanisms of SLE involve immune dysregulation with potential activation of the disease process by infections which may also be the trigger for CN VII palsy 7. Potential mechanisms for CN VII palsy in SLE include autoimmune antibodies against neuronal antigen or inflammatory cytokines; both of which may be triggered by an infectious process, viral or bacterial.…”

Section: Discussionmentioning

confidence: 99%

Unusual aetiology of isolated lower motor neuron facial palsy: systemic lupus erythematosus presenting with cranial nerve palsy and nephritis

Kazzaz

El-Rifai

2013

BMJ Case Reports

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A 20-year-old woman presented with common cold symptoms was found to have a left-sided facial droop. On examination, peripheral facial nerve palsy was confirmed. Subsequent testing showed nephrotic range proteinuria and positive serologies including antinuclear antibody and anti-smith antibody. Kidney biopsy showed stage III lupus nephritis. Treatment with pulse steroids along with mycophenolate mofetil for her lupus nephritis resulted in concomitant improvement of her facial palsy.

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Section: Discussionmentioning

confidence: 99%

Unusual aetiology of isolated lower motor neuron facial palsy: systemic lupus erythematosus presenting with cranial nerve palsy and nephritis

Kazzaz

El-Rifai

2013

BMJ Case Reports

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“…pDCs are capable of rapidly producing large amount of type-I IFNs 200–1000 times more than other immune cell types upon microbial challenge [ 100 ]. From SLE patients, the bone marrow-derived pDCs exhibited activated phenotypes with higher expression of CD40 and CD86 and induced stronger T-cell proliferation [ 101 ], reduced ChemR23 chemokine receptor expression and enhanced migratory ability of pDCs, which are suggestive of an activated status of pDCs in SLE patients [ 102 ]. Apart from directly augmenting the functions of autoreactive T and B cells, type I-IFN also acts indirectly through promoting the differentiation of blood-derived monocytes and activation of mDC, which then up-regulates MHC-II and co-stimulatory molecules for autoreactive helper (Th) and cytotoxic (TC) T cell activation; and enhances BAFF and APRIL expression for promoting autoreactive B cell survival and proliferation.…”

Section: Tissue-resident Dendritic Cells (Dcs)mentioning

confidence: 99%

Tissue-resident dendritic cells and diseases involving dendritic cell malfunction

Chen

Wang

Yuan

et al. 2016

International Immunopharmacology

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Dendritic cells (DCs) control immune responses and are central to the development of immune memory and tolerance. DCs initiate and orchestrate immune responses in a manner that depends on signals they receive from microbes and cellular environment. Although DCs consist mainly of bone marrow-derived and resident populations, a third tissue-derived population resides the spleen and lymph nodes (LNs), different subsets of tissue-derived DCs have been identified in the blood, spleen, lymph nodes, skin, lung, liver, gut and kidney to maintain the tolerance and control immune responses. Tissue-resident DCs express different receptors for microbe-associated molecular patterns (MAMPs) and damage-associated molecular patterns (DAMPs), which were activated to promote the production of pro- or anti-inflammatory cytokines. Malfunction of DCs contributes to diseases such as autoimmunity, allergy, and cancer. It is therefore important to update the knowledge about resident DC subsets and diseases associated with DC malfunction.

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“…Crohn (Weigert et al, 2010), doença hepática não-alcólica (Kukla et al, 2010), doença desmielinizante autoimmune (Graham et al, 2009), lupus eritematoso (Gerl et al, 2010) e doença periodontal (Ozcan et al, 2014). Além disso, níveis séricos da adipocina chemerin estão aumentados em pacientes obesos Os modelos de obesidade que envolvem mudanças na dieta dos animais consistem em modificações da ração, seja enriquecida com gordura (high-fat), açúcares (high-sucrose) ou ambos (Naderali et al, 2001;Naderali et al, 2003).…”

Section: Discussionunclassified

“…Além disso, os níveis circulantes de chemerin estão aumentados em uma série de doenças, tais como colite ulcerativa e doença de Crohn (Weigert et al, 2010), doença hepática não-alcólica (Kukla et al, 2010), doença desmielinizante autoimmune (Graham et al, 2009) e lupus eritematoso (Gerl et al, 2010 in vitro e in vivo (Dang et al, 2002;Okazaki et al, 2002;Duque, Macoritto and Kremer, 2004).…”

Section: Adipocina Chemerinunclassified

“…Os níveis circulantes de chemerin estão aumentados em uma série de doenças (Graham et al, 2009;Weigert et al, 2010;Kukla et al, 2010;Gerl et al, 2010) e também, estão relacionados ao IMC (Bozaoglu et al, 2007;Stejskal et al, 2008;Dong et al, 2011). Por isso, com o objetivo de avaliar se a dieta hiperlipidêmica ou a infecção eram capazes de alterar os níveis de chemerin plasmático, foi determinado a concentração de chemerin em plasma sanguíneo nos animais dos diferentes grupos experimentais.…”

Section: Quantificação De Chemerin Em Plasma Sanguíneo De Animais Conunclassified

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Efeito da adipocina chemerin na reabsorção ósseoa em modelo experimental de doença periodontal e hiperlipidemia

Guerreiro¹

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Blood dendritic cells in systemic lupus erythematosus exhibit altered activation state and chemokine receptor function

Abstract: The phenotypic and migratory disturbances observed in SLE blood DCs could result in altered distribution of DCs in peripheral tissues, contributing to dysregulated immune responses and autoimmunity.

Cited by 52 publications

References 55 publications

Unusual aetiology of isolated lower motor neuron facial palsy: systemic lupus erythematosus presenting with cranial nerve palsy and nephritis

Unusual aetiology of isolated lower motor neuron facial palsy: systemic lupus erythematosus presenting with cranial nerve palsy and nephritis

Tissue-resident dendritic cells and diseases involving dendritic cell malfunction

Efeito da adipocina chemerin na reabsorção ósseoa em modelo experimental de doença periodontal e hiperlipidemia

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