Primary immunodeficiency

Primary immunodeficiency

Abstract Primary immunodeficiency disorder (PID) refers to a large heterogeneous group of disorders that result from defects in immune system development and/or function. PIDs are broadly classified as disorders of adaptive immunity (i.e., T cell, B-cell or combined immunodeficiencies) or of innate...

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Main Authors: Christine McCusker, Julia Upton, Richard Warrington
Format: Article
Language:English
Published: BMC 2018-09-01
Series:Allergy, Asthma & Clinical Immunology
Online Access:http://link.springer.com/article/10.1186/s13223-018-0290-5
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spelling doaj-96af24707cbf47239c7d8a233af62ec02020-11-25T02:08:39ZengBMCAllergy, Asthma & Clinical Immunology1710-14922018-09-0114S211210.1186/s13223-018-0290-5Primary immunodeficiencyChristine McCusker0Julia Upton1Richard Warrington2McGill UniversityDivision of Immunology and Allergy, Hospital for Sick ChildrenUniversity of ManitobaAbstract Primary immunodeficiency disorder (PID) refers to a large heterogeneous group of disorders that result from defects in immune system development and/or function. PIDs are broadly classified as disorders of adaptive immunity (i.e., T cell, B-cell or combined immunodeficiencies) or of innate immunity (e.g., phagocyte and complement disorders). Although the clinical manifestations of PIDs are highly variable, many disorders involve an increased susceptibility to infection. Early consultation with a clinical immunologist is essential, as timely diagnosis and treatment are imperative for preventing significant disease-associated morbidity. PIDs should be suspected in patients with: recurrent sinus or ear infections or pneumonias within a 1 year period; failure to thrive; poor response to prolonged use of antibiotics; persistent thrush or skin abscesses; or a family history of PID. Patients with multiple autoimmune diseases should also be evaluated. Diagnostic testing often involves lymphocyte proliferation assays, flow cytometry, measurement of serum immunoglobulin (Ig) levels, assessment of serum specific antibody titers in response to vaccine antigens, neutrophil function assays, stimulation assays for cytokine responses, and complement studies. The treatment of PIDs is complex and generally requires both supportive and definitive strategies. Ig replacement therapy is the mainstay of therapy for B-cell disorders, and is also an important supportive treatment for many patients with combined immunodeficiency disorders. The disorders affecting the activity of the T-cell arm of the adaptive system, such as severe combined immunodeficiency, require immune reconstitution as soon as possible. The treatment of innate immunodeficiency disorders varies depending on the type of defect, but may involve antifungal and antibiotic prophylaxis, cytokine replacement, vaccinations and bone marrow transplantation. This article provides an overview of the major categories of PIDs and strategies for the appropriate diagnosis and management of these rare disorders.http://link.springer.com/article/10.1186/s13223-018-0290-5
collection DOAJ
language English
format Article
sources DOAJ
author Christine McCusker
Julia Upton
Richard Warrington
spellingShingle Christine McCusker
Julia Upton
Richard Warrington
Primary immunodeficiency
Allergy, Asthma & Clinical Immunology
author_facet Christine McCusker
Julia Upton
Richard Warrington
author_sort Christine McCusker
title Primary immunodeficiency
title_short Primary immunodeficiency
title_full Primary immunodeficiency
title_fullStr Primary immunodeficiency
title_full_unstemmed Primary immunodeficiency
title_sort primary immunodeficiency
publisher BMC
series Allergy, Asthma & Clinical Immunology
issn 1710-1492
publishDate 2018-09-01
description Abstract Primary immunodeficiency disorder (PID) refers to a large heterogeneous group of disorders that result from defects in immune system development and/or function. PIDs are broadly classified as disorders of adaptive immunity (i.e., T cell, B-cell or combined immunodeficiencies) or of innate immunity (e.g., phagocyte and complement disorders). Although the clinical manifestations of PIDs are highly variable, many disorders involve an increased susceptibility to infection. Early consultation with a clinical immunologist is essential, as timely diagnosis and treatment are imperative for preventing significant disease-associated morbidity. PIDs should be suspected in patients with: recurrent sinus or ear infections or pneumonias within a 1 year period; failure to thrive; poor response to prolonged use of antibiotics; persistent thrush or skin abscesses; or a family history of PID. Patients with multiple autoimmune diseases should also be evaluated. Diagnostic testing often involves lymphocyte proliferation assays, flow cytometry, measurement of serum immunoglobulin (Ig) levels, assessment of serum specific antibody titers in response to vaccine antigens, neutrophil function assays, stimulation assays for cytokine responses, and complement studies. The treatment of PIDs is complex and generally requires both supportive and definitive strategies. Ig replacement therapy is the mainstay of therapy for B-cell disorders, and is also an important supportive treatment for many patients with combined immunodeficiency disorders. The disorders affecting the activity of the T-cell arm of the adaptive system, such as severe combined immunodeficiency, require immune reconstitution as soon as possible. The treatment of innate immunodeficiency disorders varies depending on the type of defect, but may involve antifungal and antibiotic prophylaxis, cytokine replacement, vaccinations and bone marrow transplantation. This article provides an overview of the major categories of PIDs and strategies for the appropriate diagnosis and management of these rare disorders.
url http://link.springer.com/article/10.1186/s13223-018-0290-5
work_keys_str_mv AT christinemccusker primaryimmunodeficiency
AT juliaupton primaryimmunodeficiency
AT richardwarrington primaryimmunodeficiency
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