T and B‐cell signaling in activated PI3K delta syndrome: From immunodeficiency to autoimmunity

Preite, Silvia; Gómez-Rodríguez, Julio; Cannons, Jennifer L.; Schwartzberg, Pamela L.

doi:10.1111/imr.12790

Cited by 54 publications

(49 citation statements)

References 181 publications

(376 reference statements)

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“…Mechanistically, these mutations function either by disrupting the inhibitory contacts of p110 with p85 or by increasing the affinity of p110δ for the plasma membrane, promoting its interaction with PIP 2 53 . Consistent with the known functions of PI3K signaling, APDS mutations result in enhanced activation of the Akt and mTOR kinase pathways and decreased activity of the FOXO1 transcription factor in T cells 50 . These changes are associated with increased T cell effector function and enhanced migration out of secondary lymphoid organs.…”

Section: Lessons From Activated Pi3kδ Syndromesupporting

confidence: 52%

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Control of T lymphocyte fate decisions by PI3K signaling

Murter

Kane

2020

F1000Res

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Virtually all aspects of T and B lymphocyte development, homeostasis, activation, and effector function are impacted by the interaction of their clonally distributed antigen receptors with antigens encountered in their respective environments. Antigen receptors mediate their effects by modulating intracellular signaling pathways that ultimately impinge on the cytoskeleton, bioenergetic pathways, transcription, and translation. Although these signaling pathways are rather well described at this point, especially those steps that are most receptor-proximal, how such pathways contribute to more quantitative aspects of lymphocyte function is still being elucidated. One of the signaling pathways that appears to be involved in this “tuning” process is controlled by the lipid kinase PI3K. Here we review recent key findings regarding both the triggering/enhancement of PI3K signals (via BCAP and ICOS) as well as their regulation (via PIK3IP1 and PHLPP) and how these signals integrate and determine cellular processes. Lymphocytes display tremendous functional plasticity, adjusting their metabolism and gene expression programs to specific conditions depending on their tissue of residence and the nature of the infectious threat to which they are responding. We give an overview of recent findings that have contributed to this model, with a focus on T cells, including what has been learned from patients with gain-of-function mutations in PI3K as well as lessons from cancer immunotherapy approaches.

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Section: Lessons From Activated Pi3kδ Syndromesupporting

confidence: 52%

“…Facilitating the understanding of APDS, a mouse model of active PI3K (Pik3cd E1020K/+ ) reproduces many aspects of this disease 45 – 49 . Clinical and cellular aspects of APDS have been reviewed extensively elsewhere 50 – 52 , so we will touch on a few highlights here.…”

Section: Lessons From Activated Pi3kδ Syndromementioning

confidence: 99%

Control of T lymphocyte fate decisions by PI3K signaling

Murter

Kane

2020

F1000Res

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“…PI3Kδ is a PI3K subunit exclusively expressed in leukocytes. Patients heterozygous for this mutation are now said to have "activated PI3Kδ syndrome, " or APDS, of which ∼200 patients have been described to date (88). Activated PI3Kδ syndrome is characterized by impaired T-and B-cell development and function, autoimmunity, and lymphoproliferation.…”

Section: Genetics Of Cvid Autoimmunitymentioning

confidence: 99%

Current Understanding and Recent Developments in Common Variable Immunodeficiency Associated Autoimmunity

Gereige

Maglione

2019

Front. Immunol.

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Common variable immunodeficiency (CVID) is the most prevalent symptomatic primary immunodeficiency and comprises a group of disorders with similar antibody deficiency but a myriad of different etiologies, most of which remain undefined. The variable aspect of CVID refers to the approximately half of patients who develop non-infectious complications in addition to heightened susceptibility to infection. The pathogenesis of these complications is poorly understood and somewhat counterintuitive because these patients that are defined by their immune futility simultaneously have elevated propensity for autoimmune disease. There are numerous aspects of immune dysregulation associated with autoimmunity in CVID that have only begun to be studied. These findings include elevations of T helper type 1 and follicular helper T cells and B cells expressing low levels of CD21 as well as reciprocal decreases in regulatory T cells and isotype-switched memory B cells. Recently, advances in genomics have furthered our understanding of the fundamental biology underlying autoimmunity in CVID and led to precision therapeutic approaches. However, these genetic etiologies are also associated with clinical heterogeneity and incomplete penetrance, highlighting the fact that continued research efforts remain necessary to optimize treatment. Additional factors, such as commensal microbial dysbiosis, remain to be better elucidated. Thus, while recent advances in our understanding of CVID-associated autoimmunity have been exciting and substantial, these current scientific advances must now serve as building blocks for the next stages of discovery.

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“…Clinical hallmarks of the disease are recurrent sinopulmonary infections, severe or persistent viral infections, autoimmunity (e.g., cytopenia, arthritis, enteropathy) and chronic benign lymphoproliferation with increased risk of developing lymphomas [ 8 , 9 , 10 , 11 ]. APDS-1 patients display defects in both B- and T-cells: usual findings include lymphopenia, normal to elevated serum immunoglobulin M (IgM) levels, and reduced levels of immunoglobulin G (IgG) with impaired ability to produce antibodies against vaccines [ 12 , 13 , 14 , 15 ].…”

Section: Introductionmentioning

confidence: 99%

Activated Phosphoinositide 3-Kinase Delta Syndrome 1: Clinical and Immunological Data from an Italian Cohort of Patients

Tessarin

Rossi

Baronio

et al. 2020

JCM

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Activated phosphoinositide 3-kinase delta syndrome 1 (APDS-1) is a recently described inborn error of immunity caused by monoallelic gain-of-function mutations in the PIK3CD gene. We reviewed for the first time medical records and laboratory data of eight Italian APDS-1 patients. Recurrent sinopulmonary infections were the most common clinical feature at onset of disease. Seven patients presented lymphoproliferative disease, at onset or during follow-up, one of which resembled hemophagocytic lymphohistiocytosis (HLH). Genetic analysis of the PIK3CD gene revealed three novel mutations: functional testing confirmed their activating nature. In the remaining patients, the previously reported variants p.E1021K (n = 4) and p.E525A (n = 1) were identified. Six patients were started on immunoglobulin replacement treatment (IgRT). One patient successfully underwent hematopoietic stem cell transplantation (HSCT), with good chimerism and no GVHD at 21 months post-HSCT. APDS-1 is a combined immune deficiency with a wide variety of clinical manifestations and a complex immunological presentation. Besides IgRT, specific therapies targeting the PI3Kδ pathway will most likely become a valid aid for the amelioration of patients’ clinical management and their quality of life.

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T and B‐cell signaling in activated PI3K delta syndrome: From immunodeficiency to autoimmunity

Cited by 54 publications

References 181 publications

Control of T lymphocyte fate decisions by PI3K signaling

Control of T lymphocyte fate decisions by PI3K signaling

Current Understanding and Recent Developments in Common Variable Immunodeficiency Associated Autoimmunity

Activated Phosphoinositide 3-Kinase Delta Syndrome 1: Clinical and Immunological Data from an Italian Cohort of Patients

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