c-Rel plays a key role in deficient activation of B cells from a non–X-linked hyper-IgM patient

Lu, Kristina T.; Sinquett, Frank L.; Dryer, Rebecca L.; Song, Charles H.; Covey, Lori R.

doi:10.1182/blood-2006-03-008839

Cited by 5 publications

(8 citation statements)

References 71 publications

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“…Interestingly, rescue from Fas induced apoptosis is normal in these cells, demonstrating the existence of distinct CD40 signaling pathways that are at least in part distinguished by the involvement of c-rel. A similar c-rel associated difference in CD40 signaling has been seen in patients with ectodermal dysplasia and hyperIgM syndrome due to mutations in the NF-κB essential modulator, NEMO, where c-Rel dependent IL4 responses are also impaired19. C-Rel is the only NF-kappaB family member with oncogenic activity and the gene is amplified in some B cell lymphomas.…”

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confidence: 62%

REL, encoding a member of the NF-κB family of transcription factors, is a newly defined risk locus for rheumatoid arthritis

et al. 2009

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mentioning

confidence: 62%

REL, encoding a member of the NF-κB family of transcription factors, is a newly defined risk locus for rheumatoid arthritis

et al. 2009

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“…Of the 27,000 genes assessed, 764 (p = 0.05) displayed differential expression of 1.6-fold or higher. Importantly, we were able to show that both the expression of c-Rel and CD23 ( FCER2 ), which had been previously identified as a bona fide c-Rel target, were decreased on the array [32]. However, there was no difference in the expression of pro-survival genes including Bcl-xL and thus the difference observed at the protein level was likely independent of a direct, c-Rel-specific affect on transcription (see Figure 1C).…”

Section: Resultsmentioning

confidence: 73%

“…Our previous analysis of c-Rel expression in Pt1 and control cells suggested that reduced c-Rel expression was due to translational or post-translational differences [32] . However, additional analyses using multiple primer pairs that targeted both the 5′ and 3′untranslated regions revealed that reduced c-Rel corresponded to a transcriptional defect that resulted in an approximate 3.5-fold decrease in RNA ( Figure 1A ).…”

Section: Resultsmentioning

confidence: 99%

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c-Rel Deficiency Increases Caspase-4 Expression and Leads to ER Stress and Necrosis in EBV-Transformed Cells

Sinquett

Covey

2011

PLoS ONE

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LMP1-mediated activation of nuclear factor of kappaB (NF-κB) is critical for the ligand independent proliferation and cell survival of in vitro EBV-transformed lymphoblastoid cell lines (LCLs). Previous experiments revealed that a majority of LMP1-dependent responses are regulated by NF-κB. However, the extent that individual NF-κB family members are required for these responses, in particular, c-Rel, whose expression is restricted to mature hematopoietic cells, remains unclear. Here we report that low c-Rel expression in LCLs derived from a patient with hyper-IgM syndrome (Pt1), resulted in defects in proliferation and cell survival. In contrast to studies that associated loss of NF-κB with increased apoptosis, Pt1 LCLs failed to initiate apoptosis and alternatively underwent autophagy and necrotic cell death. Whereas the proliferation defect appeared linked to a c-Rel-associated decrease in c-myc expression, identified pro-survival and pro-apoptotic targets were expressed at or near control levels consistent with the absence of apoptosis. Ultrastructural examination of Pt1 LCLs revealed a high level of cellular and ER stress that was further supported by gene expression profiling showing the upregulation of several genes involved in stress and inflammation. Apoptosis-independent cell death was accompanied by increased expression of the inflammatory marker, caspase-4. Using gene overexpression and siRNA knockdown we demonstrated that levels of c-Rel directly modulated expression of caspase-4 as well as other ER stress genes. Overall, these findings reveal the importance of c-Rel in maintaining LCL viability and that decreased expression results in ER stress and a default response leading to necrotic cell death.

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“…Although the precise molecular targets by which PTIP mediates its function in B cell signaling remain to be elucidated, we provide multiple lines of evidence in PTIP-deficient B-1a cells and activated B-2 B cells for deregulation of the classical NF-κB pathway. In addition to decreased cREL and increased IκBα at steady state and in response to anti-IgM, we find protein levels of a handful of NF-κB target genes to be decreased in PTIP-deficient B cells, including BCL2, BCLXL ( 27 , 28 ), NFATc1 ( 29 ), uPA, IRF4 ( 30 ), and CD23 ( 31 ). These findings indicate a requirement for PTIP in the classical NF-κB pathway and are in line with ( i ) the established role of the NF-κB pathway in B-1 cell development ( 15 , 24 , 25 , 32 ), ( ii ) evidence for a role of NF-κB downstream of pre-BCR signaling in small pre-B cells ( 28 , 33 – 36 ), and ( iii ) FO B-2 cell functionality including activation-induced proliferation, survival, antibody production, GC differentiation, and CSR ( 24 – 26 , 37 ).…”

Section: Discussionmentioning

confidence: 84%

PTIP chromatin regulator controls development and activation of B cell subsets to license humoral immunity in mice

Vanhee

Soria

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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SignificanceTo provide optimal host defense, the full spectrum of antibody-based immunity requires natural antibodies and immunization-induced antigen-specific antibodies. Here we show that the PTIP (Pax transactivation domain-interacting protein) chromatin regulator is induced by B cell activation to potentiate the establishment of steady-state and postimmune serum antibody levels. It does so by promoting activation-associated proliferation and differentiation of all the major B cell subsets, at least in part, through regulating the NF-κB pathway. With the genetic basis still unknown for a majority of patients with common variable immunodeficiency, further work investigating how PTIP controls cell signaling may generate valuable new insight for human health and disease.

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c-Rel plays a key role in deficient activation of B cells from a non–X-linked hyper-IgM patient

Cited by 5 publications

References 71 publications

REL, encoding a member of the NF-κB family of transcription factors, is a newly defined risk locus for rheumatoid arthritis

REL, encoding a member of the NF-κB family of transcription factors, is a newly defined risk locus for rheumatoid arthritis

c-Rel Deficiency Increases Caspase-4 Expression and Leads to ER Stress and Necrosis in EBV-Transformed Cells

PTIP chromatin regulator controls development and activation of B cell subsets to license humoral immunity in mice

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