Defective B-cell proliferation and maintenance of long-term memory in patients with chronic granulomatous disease

Cotugno, Nicola; Finocchi, Andrea; Cagigi, Alberto; Matteo, Gigliola Di; Chiriaco, Maria; Cesare, Silvia Di; Rossi, Paolo; Aiuti, Alessandro; Douagi, Iyadh

doi:10.1016/j.jaci.2014.07.012

Cited by 41 publications

(30 citation statements)

References 41 publications

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“…The DN B cells are characteristic of immune senescence in HC [10] and are also associated with autoimmunity [32] and chronic diseases such as systemic lupus erythe-matosus, chronic granulomatous disease and HIV [4, 44, 45]. In agreement with previous reports, higher frequencies of DN B cells were observed before vaccination in old HC compared to young HC [10, 11].…”

Section: Discussionsupporting

confidence: 87%

Paradoxical aging in HIV: immune senescence of B Cells is most prominent in young age

Rinaldi

Pallikkuth

George

et al. 2017

Aging

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Combination antiretroviral therapies (cART) can lead to normal life expectancy in HIV-infected persons, and people aged >50 yrs represent the fastest growing HIV group. Although HIV and aging are independently associated with impaired humoral immunity, immune status in people aging with HIV is relatively unexplored. In this study influenza vaccination was used to probe age associated perturbations in the B cell compartment of HIV-negative “healthy controls” (HC) and virologically controlled HIV-infected participants on cART (HIV) (n=124), grouped by age as young (<40 yrs), middle-aged (40-59yrs) or old (≥60 yrs). H1N1 antibody response at d21 post-vaccination correlated inversely with age in both HC and HIV. Immunophenotyping of cryopreserved PBMC demonstrated increased frequencies of double negative B cells and decreased plasmablasts in old compared to young HC. Remarkably, young HIV were different from young HC but similar to old HC in B cell phenotype, influenza specific spontaneous (d7) or memory (d21) antibody secreting cells. We conclude that B cell immune senescence is a prominent phenomenon in young HIV in comparison to young HC, but distinctions between old HIV and old HC are less evident though both groups manifest age-associated B cell dysfunction.

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Section: Discussionsupporting

confidence: 87%

Paradoxical aging in HIV: immune senescence of B Cells is most prominent in young age

Rinaldi

Pallikkuth

George

et al. 2017

Aging

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“…Thus, NADPH oxidase or resultant ROS may be important for proper expression of TLR5 and TLR9 in neutrophils, with the absence of NADPH or ROS resulting in impaired responses to stimulation by these TLR ligands, and thereby less efficient phagocytosis . The NADPH oxidase system was further shown to be important in the context of TLR9 stimulation in B cells, with defects in long‐term antibody memory responses recently reported in CGD patients . The authors linked deficient ROS production in B cells to reduced frequencies of memory B cells in patients, with a milder phenotype seen in carriers of CGD mutations (Fig.…”

Section: Tlr Signaling In Cgdmentioning

confidence: 96%

Toll‐like receptor signaling in primary immune deficiencies

Maglione

Simchoni

Cunningham‐Rundles

2015

Annals of the New York Academy of Sciences

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Toll-like receptors (TLRs) recognize common microbial or host-derived macromolecules and have important roles in early activation of the immune system. Patients with primary immune deficiencies (PIDs) affecting TLR signaling can elucidate the importance of these proteins to the human immune system. Defects in interleukin-1 receptor-associated kinase (IRAK)-4 and myeloid differentiation factor 88 (MyD88) lead to susceptibility to infections with bacteria, while mutations in nuclear factor-κB essential modulator (NEMO) and other downstream mediators generally induce broader susceptibility to bacteria, viruses, and fungi. In contrast, TLR3 signaling defects are specific for susceptibility to herpes simplex virus type 1 (HSV-1) encephalitis. Other PIDs induce functional alterations of TLR signaling pathways, such as common variable immunodeficiency in which plasmacytoid dendritic cell (pDC) defects enhance defective responses of B cells to shared TLR agonists. Dampening of TLR responses is seen for TLRs 2 and 4 in chronic granulomatous disease (CGD) and X-linked agammaglobulinemia (XLA). Enhanced TLR responses, meanwhile, are seen for TLRs 5 and 9 in CGD, TLRs 4, 7/8, and 9 in XLA, TLRs 2 and 4 in hyper IgE syndrome, and for most TLRs in adenosine deaminase deficiency.

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“…9 There is evidence for ROS having an influence on the process of memory B cell formation, as there is a correlation between the amount of neutrophils with normal NOX2 activity and the percentage of memory B cells in CGD patients. 68,84 In contrast, circulating CD19…”

Section: Chronic Granulomatous Diseasementioning

confidence: 98%

“…61,[63][64][65][66] Moreover, ROS can modulate the interaction of B cells with CD4 þ T cells by promoting MHC II antigen presentation and influence the number of circulating memory B cells. [67][68][69] T cells T cells are often found in the vicinity of potent oxidative burst-mounting phagocytes. ROS influence T cell activation, modulate T cell receptor signaling pathways, suppress T cell proliferation, and downregulate their responsiveness.…”

Section: B Cellsmentioning

confidence: 99%

Reactive oxygen homeostasis – the balance for preventing autoimmunity

Kienhöfer

Boeltz

Hoffmann

2016

Lupus

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Being mainly known for their role in the antimicrobial defense and collateral damage they cause in tissues as agents of oxidative stress, reactive oxygen species were considered ''the bad guys'' for decades. However, in the last years it was shown that the absence of reactive oxygen species can lead to the development of immune-mediated inflammatory diseases. Animal models of lupus, arthritis and psoriasis revealed reactive oxygen species-deficiency as a potent driver of pathogenesis. On the contrary, in chronic stages oxidative stress can still contribute to progression of inflammation. It seems that a neatly adjusted redox balance is necessary to sustain an immune state that both prevents the development of overt autoimmunity and attenuates chronic stages of disease. Lupus (2016) 25, 943-954.

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Defective B-cell proliferation and maintenance of long-term memory in patients with chronic granulomatous disease

Cited by 41 publications

References 41 publications

Paradoxical aging in HIV: immune senescence of B Cells is most prominent in young age

Paradoxical aging in HIV: immune senescence of B Cells is most prominent in young age

Toll‐like receptor signaling in primary immune deficiencies

Reactive oxygen homeostasis – the balance for preventing autoimmunity

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