Reciprocal CD40 signals through p38MAPK and ERK-1/2 induce counteracting immune responses

Mathur, Ramkumar; Awasthi, Amit; Wadhone, Pallavi; Boppana, Ramanamurthy; Saha, Bhaskar

doi:10.1038/nm1045

Cited by 222 publications

(330 citation statements)

References 29 publications

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“…43 However, PSLinduced increase in IL-10 by LPS-stimulated macrophages may depend on ERK activity, because ERK activity leads to IL-10 production. 47,48 Furthermore, PSLs inhibited the rapid activation of p38 MAPK and may result in the subsequent slow enhancement of ERK activity in LPS-stimulated macrophages, because p38 MAPK and ERK cross-regulate each other such as the inhibition of one enhances the activation of the other. 47,49 Moreover, PSLs regulated the expression levels of IL-10 and IL-1b in the PB monocytes, the source of macrophage infiltrated in the ankle joints, and regulated the phosphorylation of p38, ERK and IkBa in the infiltrated macrophages in the synovium of the ankle joints of AA rats.…”

Section: Discussionmentioning

confidence: 99%

Phosphatidylserine-containing liposomes suppress inflammatory bone loss by ameliorating the cytokine imbalance provoked by infiltrated macrophages

Mei

Nakanishi

2011

Laboratory Investigation

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Phosphatidylserine (PS)-containing liposomes (PSLs) strongly inhibit inflammatory bone loss in adjuvant arthritic (AA) rats. This effect was attributed to the inhibition of osteoclastogenesis through the secretion of prostaglandin E 2 and transforming growth factor-b1 by osteoclast precursors after the phagocytosis of PSLs. However, infiltrated macrophages are considered to secrete anti-inflammatory mediators after phagocytosis of PSLs, which also contribute to inhibiting osteoclastogenesis. In the present study, we have attempted to elucidate the effects of PSLs on the phenotype of infiltrated macrophages during inflammatory bone loss. In AA rats, the ankle joints swelled with the infiltration of both macrophages and helper T cells into the synovium after a complete Freund's adjuvant injection. In the ankle joints of AA rats, approximately half of the infiltrated macrophages underwent a phenotypic change from interleukin (IL)-1b-producing to IL-10-producing cells after the phagocytosis of PSLs. In lipopolysaccharide (LPS)-stimulated macrophages, PSLs also significantly decreased IL-1b production, but increased IL-10 production. Moreover, PSLs inhibited the rapid activation of p38 mitogen-activated protein kinases (MAPK) and nuclear factor (NF)-kB, but enhanced the delayed activation of extracellular signal-regulated kinase (ERK) in LPS-stimulated macrophages. PSL-induced different influence on the activities of p38 MAPK and ERK is a likely underlying mechanism for phenotypic change of infiltrated macrophages after the phagocytosis of PSLs. This phenotypic change may be responsible for a significant decrease in the mean mRNA level of the receptor activator of NF-kB (RANK) and the RANK ligand (RANKL) in the ankle joint of PSL-treated AA rats, resulting in the inhibition of inflammatory bone loss.Laboratory Investigation (2011) 91, 921-931;

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Section: Discussionmentioning

confidence: 99%

Phosphatidylserine-containing liposomes suppress inflammatory bone loss by ameliorating the cytokine imbalance provoked by infiltrated macrophages

Mei

Nakanishi

2011

Laboratory Investigation

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“…As far as the role of IL-2 in experimental visceral leishmaniasis is concerned, during the early phase of infection, IL-2 induces both IFN-␥-and IL-10-secreting T cells, perhaps as a function of the available IL-2 concentration, but IL-10 suppresses the IL-12 production by the APCs by differential regulation of MAPKs (26), reduces IL-12R expression on T cells (B. Saha, unpublished observation), and impairs IFN-␥ responsiveness of macrophages, resulting in the suppression of IFN-␥-mediated amastigote elimination. Being residents of the IL-10-rich splenic microenvironment, these T cells do not proliferate and suppress the activation of the infiltrating naive T cells, a phenomenon reminiscent of infectious tolerance (27).…”

Section: Discussionmentioning

confidence: 99%

“…Being residents of the IL-10-rich splenic microenvironment, these T cells do not proliferate and suppress the activation of the infiltrating naive T cells, a phenomenon reminiscent of infectious tolerance (27). Thus, Leishmania exaggerates and exploits the host's IL-10-dependent autoregulatory or a feedback servo-mechanism that prevents excessive inflammation-mediated host-tissue pathology, but supports unhindered parasite growth (25,26). Such a mechanism may operate in those viral infections in which the viral IL-10 (28, 29) may skew the immune response in a similar way.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of IL-2 Induced IL-10 Production as a Principle of Phase-Specific Immunotherapy

Bodas

Jain

Awasthi

et al. 2006

The Journal of Immunology

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Leishmania donovani, a protozoan parasite, inflicts a fatal disease, visceral leishmaniasis. The suppression of antileishmanial T cell responses that characterizes the disease was proposed to be due to deficiency of a T cell growth factor, IL-2. We demonstrate that during the first week after L. donovani infection, IL-2 induces IL-10 that suppresses the host-protective functions of T cells 14 days after infection. The observed suppression is concurrent with increased CD4+glucocorticoid-induced TNF receptor+ T cells and Foxp3 expression in BALB/c mice, implicating IL-2-dependent regulatory T cell control of antileishmanial immune responses. Indeed, IL-2 and IL-10 neutralization at different time points after the infection demonstrates their distinct roles at the priming and effector phases, respectively, and establishes kinetic modulation of ongoing immune responses as a principle of a rational, phase-specific immunotherapy.

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“…FCM and RT-PCR detected the upregulated expression of CD40L after EBV infection. Other researchers reported that LMP1 plays a key role in B-cell transformation by EBV [15,16]. Although LMP1 is very similar to CD40 in terms of the signal transduction pathway and in the recruitment of TNF receptor-associated factor signaling molecules, it cannot entirely replace CD40 [17] because LMP1 and CD40 differ in some aspects.…”

Section: Figurementioning

confidence: 99%

Effects of Epstein-Barr virus infection on the development of multiple myeloma after liver transplantation

Ye-wei

Zhao

et al. 2012

Sci. China Life Sci.

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Reduced cellular immune function in patients after liver transplantation easily results in many types of viral infections, such as Epstein-Barr virus. Epstein-Barr virus is a γ-herpesvirus and is related to many malignant diseases, especially epithelial and lymph tumors. The abnormal interaction of cluster of differentiation 40 with cluster of differentiation 40 ligand and expression of cluster of differentiation 40 ligand are considered closely related to the development of myeloma cells. This study explored the influence and mechanism of Epstein-Barr virus infection on the phenotype and biological behavior of myeloma cells after liver transplantation. Flow cytometry was used to detect coexpression of cluster of differentiation 40 and cluster of differentiation 40 ligand in 10 samples of freshly isolated multiple myeloma cells. Cluster of differentiation 40 and cluster of differentiation 40 ligand were coexpressed in sample Nos. 5, 8, 9, and 10, particularly in sample No. 5. Western blot analysis was used to detect the expression of the Epstein-Barr virus antigens latent membrane protein 1 and Epstein-Barr virus nuclear antigen 2 in the multiple myeloma cell line RPMI 8226 infected with Epstein-Barr virus. The antigen expression indicated that Epstein-Barr virus can infect multiple myeloma virus cells in vitro. Reverse transcription-polymerase chain reaction revealed upregulated expression of cluster of differentiation 40 ligand on the infected RPMI 8226 cells, which may be involved in the anti-apoptosis activity of the infected cells. Confocal microscopy showed that pairs of molecules of cluster of differentiation 40, cluster of differentiation 40 ligand, and latent membrane protein 1 were colocalized on the surface of the infected cells. CXC chemokine receptor 4 was upregulated on the RPMI 8226 cells after Epstein-Barr virus infection. The migratory ability of the infected cells improved in the presence of the chemokine stromal cell-derived factor-1α. Anti-apoptosis and migration are known important biological characteristics of malignant cells. Our results indicate the involvement of Epstein-Barr virus in the origin and development of multiple myeloma. The risk of multiple myeloma increases when Epstein-Barr virus infects B cells in the germinal center, which may result in an anti-apoptosis effect of B cells and an improved ability to migrate from the germinal center to peripheral blood.

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Reciprocal CD40 signals through p38MAPK and ERK-1/2 induce counteracting immune responses

Cited by 222 publications

References 29 publications

Phosphatidylserine-containing liposomes suppress inflammatory bone loss by ameliorating the cytokine imbalance provoked by infiltrated macrophages

Phosphatidylserine-containing liposomes suppress inflammatory bone loss by ameliorating the cytokine imbalance provoked by infiltrated macrophages

Inhibition of IL-2 Induced IL-10 Production as a Principle of Phase-Specific Immunotherapy

Effects of Epstein-Barr virus infection on the development of multiple myeloma after liver transplantation

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