Constitutive reductions in mTOR alter cell size, immune cell development, and antibody production

Zhang, Shuling; Readinger, Julie A.; Dubois, Wendy; Janka-Junttila, Mirkka; Robinson, Richard; Pruitt, Margaret M.; Bliskovsky, Valery; Wu, Jing; Sakakibara, Kaori; Patel, Jyoti D.; Parent, Carole A.; Tessarollo, Lino; Schwartzberg, Pamela L.; Mock, Beverly A.

doi:10.1182/blood-2010-05-287821

Cited by 108 publications

(148 citation statements)

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“…Mice deficient for p85α or with inactive p110δ PI3K subunit show a similar phenotype to our Akt1 overexpressing mice resulting in a partial block at the pro-B-cell stage, reduced numbers of splenic B cells, and a strong reduction in peritoneal B1 cells [36,37]. A partial block in B-cell development and reduced B-cell proliferation was also found in mice with reduced mTOR levels [38]. Our results from Akt1 Tg mice seem contradictory to above findings, but the lower BCR signaling strength suggests that constitutively enhanced Akt1 signals induce a feedback that resets BCR responsiveness, "mimicking," at least in part, loss of PI3K signaling and, thereby, influencing B-cell maturation and function [13,14,39].…”

Section: Discussionmentioning

confidence: 57%

Constitutive Akt1 signals attenuate B‐cell receptor signaling and proliferation, but enhance B‐cell migration and effector function

Pierau

Simma

et al. 2012

Eur J Immunol

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Ligation of the BCR induces a complex signaling network that involves activation ofAkt, a family of serine/threonine protein kinases associated with B-cell development, proliferation, and tumor formation. Here, we analyzed the effect of enhanced Akt1 signals on B-cell maturation and function. Unexpectedly, we found that peripheral B cells overexpressing Akt1 were less responsive to BCR stimuli. This correlated with a decrease in Ca 2+ -mobilization and proliferation, in an impaired activation of Erk1/2 and mammalian target of rapamycin (mTOR) kinases and poor mobilization of NFATc1 and NF-κB/p65 factors. In contrast, activation of STAT5 and migration of B cells toward the chemokine SDF1α was found to be enhanced. Akt1 Tg mice showed an altered maturation of peritoneal and splenic B1 B cells and an enhanced production of IgG1 and IgG3 upon immunization with the T-cell independent Ag TNP-Ficoll. Furthermore, mice homozygous for Tg Akt1 showed a severe block in the maturation of B-cell precursors in BM and a strong enrichment of plasma cells in spleen. Altogether, our data reveal that enhanced Akt1 signals modify BCR signaling strength and, thereby, B-cell development and effector function.Keywords: B cell r NFAT r PKB/Akt r SDF1α r STAT5 IntroductionIn the BM B-cell progenitors develop through defined stages of differentiation to immature B cells giving rise to follicular B2 (FO) B cells, marginal zone (MZ), and B1 B cells. These processes are controlled by the signal intensity arising from the pre-BCR or mature BCR, which activate similar sets of signaling molecules. The most proximal signaling events upon BCR ligation include Correspondence: Prof. Ursula H. Bommhardt e-mail: ursula.bommhardt@med.ovgu.de activation of the protein tyrosine kinases Lyn and Syk. A prominent substrate of Syk is the adaptor protein SLP65/BLNK, which recruits Bruton's tyrosine kinase, phospholipase Cγ2, and further signal proteins into supramolecular complexes that trigger the activation of multiple signaling pathways. Activated phospholipase Cγ2 cleaves the membrane lipid phosphatidylinositol-4, 5-bisphosphate (PIP2) to generate diacylglycerol and inositol-1,4,5-trisphosphate (IP3), two second messengers affecting the * These authors contributed equally to this work. Eur. J. Immunol. 2012. 42: 3381-3393 activation of PKC family members, MAPK activation, and the release of Ca 2+ from intracellular stores, which finally leads to influx of extracellular Ca 2+ . Elevated intracellular Ca 2+ -levels induce the activity of serine/threonine-specific phosphatase calcineurin and, in turn, a set of Ca 2+ -regulated transcription factors, in particular of NFAT and NF-κB factors that control various gene expression programs [1].An important signaling cascade induced after BCR engagement encompasses the lipid kinase family of class I PI3Ks [2][3][4]. Mature peripheral B cells lacking a BCR could be rescued from apoptosis by the ectopic expression of a constitutively active catalytic subunit of PI3K, indicating that PI3K signals support the surv...

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Section: Discussionmentioning

confidence: 57%

Constitutive Akt1 signals attenuate B‐cell receptor signaling and proliferation, but enhance B‐cell migration and effector function

Pierau

Simma

et al. 2012

Eur J Immunol

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“…The cAMP pathway participates in the PI3K-AKT-mTOR axis, which is used by Tregs to control FOXP3 levels. 53,54 With their potential roles in reversing tumor immune evasion and promoting apoptosis, and due to the potential clinical cooperation between the cAMP pathway and the CY-Tregs pathway, cAMP analogs/PDE4B inhibitors and lowdose CY may be good candidate agents for lymphoma therapy. …”

Section: Western Blot Analysismentioning

confidence: 99%

Cyclic adenosine monophosphate involvement in low-dose cyclophosphamide-reversed immune evasion in a mouse lymphoma model

Dou

Liu

et al. 2012

Cell Mol Immunol

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Lymphoma cells mobilize many mechanisms to evade the immune system. There is substantial evidence that CD4 1 CD25 1 regulatory T cells (Tregs) play a key role in the control of immune evasion. Tregs can transfer cyclic adenosine monophosphate (cAMP) to effector T cells, suggesting an association between Tregs' immune-evasion role and the intracellular cAMP pathway. In this study, we used A20 B-cell lymphoma mice as aggressive tumor models to investigate the mechanism of the depletion of Tregs by low-dose cyclophosphamide (CY, 20 mg/kg). The tumor-bearing mice had longer survival times and slower tumor growth rates following treatment with CY, but its effects were temporary. Along with the depletion of Tregs by low-dose CY treatment, the expression of interleukin-2 (IL-2) in T effector cells increased, and intracellular cAMP concentrations in immune cells decreased. Our study demonstrates the ability of low-dose CY to reverse Tregs-mediated immune evasion in a mouse model. The changes in intracellular cAMP concentrations correlated with the upregulation of effector T cells and the downregulation of Tregs, indicating the close association of cAMP analogs and low-dose CY in the immune therapy of B-cell lymphoma.

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“…Sirolimus and everolimus engage FK binding proteins, forming a complex that inhibits mTOR. This inhibition prevents the translation of mRNA-encoding proteins needed to enter the cell cycle 68 (thus reducing T cell proliferation) and cytokine production 40,69 (Figure 1). Interestingly, engagement of the BCR activates PI3K, which beyond activation of NF-kBdependent transcription, also initiates a distinct signaling pathway involving the Akt and mTOR serine/threonine kinases.…”

Section: Mtor Inhibitorsmentioning

confidence: 99%

“…Homozygous knockin mice for hypomorphic mTOR showed decreased ability to produce antibodies. 69 To determine whether these effects were caused by a direct mTOR blockade in the B cells or only reflected T cell deficiency, the same group examined the humoral responses in mTOR conditional B cell knockout mice. 71 Mice with mTOR deleted in their B cell lineage produced fewer splenic germinal centers and also, exhibited a decrease in switched highaffinity antibody responses in contrast to their wild-type littermates.…”

Section: Mtor Inhibitorsmentioning

confidence: 99%

Effect of Immunosuppressive Drugs on Humoral Allosensitization after Kidney Transplant

Thaunat

Koenig

Leibler³

et al. 2016

JASN

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The negative effect of donor-specific antibodies on the success of solid transplant is now clearly established. However, the lack of effective treatment to prevent the development of antibody-mediated lesions deepens the need for clinicians to focus on primary prevention of de novo humoral allosensitization. Among the factors associated with the risk of developing de novo donor-specific antibodies, therapeutic immunosuppression is the most obvious parameter in which improvement is possible. Beyond compliance and the overall depth of immunosuppression, it is likely that the nature of the drugs is also crucial. Here, we provide an overview of the molecular effect of the various immunosuppressive drugs on B cell biology. Clinical data related to the effect of these drugs on de novo humoral allosensitization are also examined, providing a platform from which clinicians can optimize immunosuppression for prevention of de novo donor-specific antibody generation at the individual level.

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Constitutive reductions in mTOR alter cell size, immune cell development, and antibody production

Cited by 108 publications

References 51 publications

Constitutive Akt1 signals attenuate B‐cell receptor signaling and proliferation, but enhance B‐cell migration and effector function

Constitutive Akt1 signals attenuate B‐cell receptor signaling and proliferation, but enhance B‐cell migration and effector function

Cyclic adenosine monophosphate involvement in low-dose cyclophosphamide-reversed immune evasion in a mouse lymphoma model

Effect of Immunosuppressive Drugs on Humoral Allosensitization after Kidney Transplant

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