Systemic autoimmune disease induced by dendritic cells that have captured necrotic but not apoptotic cells in susceptible mouse strains

Ma, Liang; Chan, Kwok–Wah; Trendell-Smith, Nigel J.; Wu, Adrian; Tian, Lei; Lam, Audrey Carmen; Chan, Albert; Lo, Chung Kwan; Chik, Stanley; Ko, King-Hung; To, Christina K. W.; Kam, Christy; Li, Xiaosong; Yang, Cuihong; Leung, Suet Yi; Ng, Mun-Hon; Stott, David I.; MacPherson, G. Gordon; Huang, Fang-Ping

doi:10.1002/eji.200535192

Cited by 59 publications

(69 citation statements)

References 40 publications

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“…Increased necrosis rates could play a central role in enhanced inflammatory responses in SLE [18]. Necrotic cell death stimulates macrophages [19] and dendritic cells [20] and leads to inflammation [15,18,21] and development of murine SLE [22]. We proposed that increased release of necrotic materials from T cells would activate macrophages and dendritic cells (DCs) and enhance their capacity to produce NO and IFN-α̣ in SLE [18].…”

Section: Introductionmentioning

confidence: 99%

“…We proposed that increased release of necrotic materials from T cells would activate macrophages and dendritic cells (DCs) and enhance their capacity to produce NO and IFN-α̣ in SLE [18]. Indeed, DCs exposed to necrotic, but not apoptotic, cells induce lupus like-disease in MRL mice and accelerate the disease of MRL/lpr mice [22]. These data suggest that principal mitochondrial functions are involved in T cell activation.…”

Section: Introductionmentioning

confidence: 99%

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Nitric oxide, mitochondrial hyperpolarization, and T cell activation☆

Nagy

Koncz

Fernández

et al. 2007

Free Radical Biology and Medicine

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T lymphocyte activation is associated with nitric oxide (NO) production that plays an essential role in multiple T cell functions. NO acts as a messenger, activating soluble guanyl cyclase and participating in the transduction signaling pathways involving cyclic GMP. NO modulates mitochondrial events that are involved in apoptosis and regulates mitochondrial membrane potential and mitochondrial biogenesis in many cell types, including lymphocytes. Mitochondrial hyperpolarization (MHP), an early and reversible event during both T lymphocyte activation and apoptosis, is regulated by NO. Here, we discuss recent evidence that NO-induced MHP represents a molecular switch in multiple T cell signaling pathways. Overproduction of NO in systemic lupus erythematosus (SLE) induces mitochondrial biogenesis and alters Ca 2+ signaling. Thus, while NO plays a physiological role in lymphocyte cell signaling, its overproduction may disturb normal T cell function, contributing to the pathogenesis of autoimmunity.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Nitric oxide, mitochondrial hyperpolarization, and T cell activation☆

Nagy

Koncz

Fernández

et al. 2007

Free Radical Biology and Medicine

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“…We have shown previously that IFN-c is a critical cytokine involved in lupus pathogenesis [40]. The imbalanced IL-2 versus IFN-c production therefore also reflects the dysregulated Teff functions.…”

Section: Discussionmentioning

confidence: 91%

“…We have also shown subsequently in vivo evidence demonstrating the therapeutic benefit of IL-2 treatment in the MRL/lpr mice by using attenuated Salmonella typhimurium as the gene carrier [39]. Since IL-2 is an essential growth factor for Treg differentiation and proliferation, we next examined the ability of MRL/lpr Teff to produce IL-2 and IFN-c, two Th1 cytokines known to be differentially implicated in lupus pathogenesis [5,40]. To exclude the possibility that the defective IL-2 secretion was a cell dilution effect due to the presence of a large number of abnormal CD4 -CD8 -double-negative T cells [11], purified Teff were used for the study.…”

Section: Defective Il-2 But Enhanced Ifn-c Il-15 and Il-15r Expressimentioning

confidence: 99%

Immunological mechanisms and clinical implications of regulatory T cell deficiency in a systemic autoimmune disorder: Roles of IL‐2 versus IL‐15

et al. 2008

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Regulatory T cell deficiency is evident in patients with lupus, but the casual relationship and underlying mechanism leading to Treg deficiency are unclear. We analyzed the Treg profile, induction and functions of Treg in a lupus mouse model. A characteristic agedependent biphasic change of Treg frequency was observed in the MRL/lpr mice, which developed a spontaneous lupus-like disease. After an early increase, Treg frequency in the peripheral lymphoid organs rapidly declined with age. Functionally, Treg from both young and old MRL/lpr mice were fully competent in suppressing the wild-type MRL/+ T effector cell (Teff) responses. Adoptive transfer of MRL/+ Treg markedly suppressed clinical disease in the MRL/lpr mice. We demonstrated that the reduced Treg frequency was a result of insufficient peripheral Treg expansion due to defective MRL/lpr Teff in IL-2 production, and the associated defects in dendritic cells, which could be fully restored by exogenous IL-2. In the absence of IL-2, MRL/lpr Teff but not MRL/lpr Treg were highly responsive to IL-15 and could expand rapidly due to enhanced IL-15R expression and IL-15 synthesis. These findings thus provide a clear causal relationship and immunological mechanism underlying Treg deficiency and systemic autoimmunity.

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“…Intravenous injection of BM-derived DCs pulsed with U1 snRNP-A protein into BALB/c and DBA-2×NZW F1 (H-2 d/u ) mice elicited autoreactive T cell and IgG anti-U1A responses [29]. Chronic maturation of tissue DCs could induce severe organ-specific autoimmune disease and systemic autoimmunity [30][31][32]. In addition, transfer of DCs, isolated from donors with acute autoimmune disease or propagated in vitro under conditions that induce maturation, generates a strong Th-1 response and eventually leads to autoimmune disease such as EAE and diabetes in mice [33][34].…”

Section: Discussionmentioning

confidence: 99%

Interaction between antigen presenting cells and autoreactive T cells derived from BXSB mice with murine lupus

Yang

et al. 2007

Cell Res

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npg Systemic lupus erythematosus (SLE) is a typical autoimmune disease involving multiple systems and organs. Ample evidence suggests that autoreactive T cells play a pivotal role in the development of this autoimmune disorder. This study was undertaken to investigate the mechanisms of interaction between antigen presenting cells (APCs) and an autoreactive T cell (ATL1) clone obtained from lupus-prone BXSB mice. ATL1 cells, either before or after γ-ray irradiation, were able to activate naive B cells, as determined by B cell proliferation assays. Macrophages from BXSB mice were able to stimulate the proliferation of resting ATL1 cells at a responder/stimulator (R/S) ratio of 1/2.5. Dendritic cells (DCs) were much more powerful stimulators for ATL1 cells on a per cell basis. The T cell stimulating ability of macrophages and B cells, but not DCs, was sensitive to γ-ray irradiation. Monoclonal antibodies against mouse MHC-II and CD4 were able to block DC-mediated stimulation of ATL1 proliferation, indicating cognate recognition between ATL1 and APCs. Our data suggest that positive feedback loops involving macrophages, B cells and autoreactive T cells may play a pivotal role in keeping the momentum of autoimmune responses leading to autoimmune diseases.

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Systemic autoimmune disease induced by dendritic cells that have captured necrotic but not apoptotic cells in susceptible mouse strains

Cited by 59 publications

References 40 publications

Nitric oxide, mitochondrial hyperpolarization, and T cell activation☆

Nitric oxide, mitochondrial hyperpolarization, and T cell activation☆

Immunological mechanisms and clinical implications of regulatory T cell deficiency in a systemic autoimmune disorder: Roles of IL‐2 versus IL‐15

Interaction between antigen presenting cells and autoreactive T cells derived from BXSB mice with murine lupus

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