Primary Immunodeficiency Diseases: An Update on the Classification from the International Union of Immunological Societies Expert Committee for Primary Immunodeficiency

Al‐Herz, Waleed; Bousfiha, Aziz; Casanova, Jean‐Laurent; Chapel, Helen; Conley, Mary Ellen; Cunningham‐Rundles, Charlotte; Etzioni, Amos; Fischer, Alain; Franco, José Luis; Geha, Raif S.; Hammarström, Lennart; Nonoyama, Shigeaki; Notarangelo, Luigi D.; Ochs, Hans D.; Puck, Jennifer M.; Roifman, Chaim M.; Seger, Reinhard; Tang, Mimi L.K.

doi:10.3389/fimmu.2014.00162

Cited by 464 publications

(556 citation statements)

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“…Other spectacular achievements have been made in the domain of therapy, including the first successful cases of hematopoietic stem cell transplantation in 1968 (118) and gene therapy in 2000 (119). Increasingly diverse clinical phenotypes, extending beyond infection and including various autoinflammatory, allergic, and autoimmune phenotypes, have been attributed to primary immunodeficiencies (120)(121)(122)(123)(124). Autoimmune phenotypes include systemic and organ-specific conditions such as the intriguingly related and occasionally allelic systemic lupus erythematosus and neurological Aicardi-Goutières syndrome, two type I interferonopathies (125).…”

Section: Primary Immunodeficiencies: a Success Storymentioning

confidence: 99%

Human genetic basis of interindividual variability in the course of infection

Casanova

2015

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

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156

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The key problem in human infectious diseases was posed at the turn of the 20th century: their pathogenesis. For almost any given virus, bacterium, fungus, or parasite, life-threatening clinical disease develops in only a small minority of infected individuals. Solving this infection enigma is important clinically, for diagnosis, prognosis, prevention, and treatment. Some microbes will inevitably remain refractory to, or escape vaccination, or chemotherapy, or both. The solution also is important biologically, because the emergence and evolution of eukaryotes alongside more rapidly evolving prokaryotes, archaea, and viruses posed immunological challenges of an ecological and evolutionary nature. We need to study these challenges in natural, as opposed to experimental, conditions, and also at the molecular and cellular levels. According to the human genetic theory of infectious diseases, inborn variants underlie life-threatening infectious diseases. Here I review the history of the field of human genetics of infectious diseases from the turn of the 19th century to the second half of the 20th century. This paper thus sets the scene, providing the background information required to understand and appreciate the more recently described monogenic forms of resistance or predisposition to specific infections discussed in a second paper in this issue.

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Section: Primary Immunodeficiencies: a Success Storymentioning

confidence: 99%

Human genetic basis of interindividual variability in the course of infection

Casanova

2015

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

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156

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“…Patients with known primary immunodeficiency disorders (PIDD) [6] who were receiving either intravenous immunoglobulin (IVIG) or subcutaneous immunoglobulin (SCIG) were enrolled during 2014-15 from the Pediatric Allergy and Immunology Clinic at Cardinal Glennon Children's Medical Center at Saint Louis University. Twenty-four subjects with PIDD were enrolled, which included X-linked agammaglobulinaemia (XLA, n 5 6), common variable immunodeficiency (CVID, n 5 9), specific antibody deficiency (SAD, n 5 7) and persistent hypogammaglobulinaemia in patients with severe combined immunodeficiency following transplantation (SCID, n 5 2).…”

Section: Patientsmentioning

confidence: 99%

Streptococcus pneumoniae antibody titres in patients with primary antibody deficiency receiving intravenous immunoglobulin (IVIG) compared to subcutaneous immunoglobulin (SCIG)

Knutsen

Leiva

Caruthers

et al. 2015

Clinical and Experimental Immunology

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SummaryIntravenous immunoglobulin (IVIG) and subcutaneous immunoglobulin (SCIG) are effective in the treatment of patients with primary antibody deficiency disorders (PAD). The purpose of this study was to evaluate Streptococcus pneumoniae (Spn) antibody titres to 14 serotypes in patients receiving IVIG compared to SCIG and to correlate Spn antibody levels to clinical outcome. The doses of immunoglobulin (Ig)G/kg/month were similar in both IVIG and SCIG groups. In 11 patients treated with IVIG, Spn antibody titres were ! 1Á3 lg/ml to 99Á4 6 2Á1% of the 14 serotypes at peak IVIG but decreased to 66Á9 6 19Á8% at trough IVIG. Loss of Spn titres ! 1Á3 lg/ml was most frequent for Spn serotypes 1, 4, 9V and 23. This correlated with lower Spn antibody titres to these serotypes at peak IVIG compared to the other serotypes. In 13 patients treated with SCIG, Spn antibody titres were protective to 58Á2 6 23Á3% of the serotypes 3-5 days after infusion, similar to trough IVIG. Similarly, the Spn serotypes with the least protective percentages were the same as the ones observed in trough IVIG. There were no annualized serious bacterial infections (aSBI) in either group. However, there were significantly decreased annualized other infections (aOI) in the SCIG group compared to the IVIG-treated group, 0Á8 6 0Á7 versus 2Á2 6 1Á2 infections/patient/year (P 5 0Á004). Breakthrough aOI did not correlate with protective or higher serum Spn antibody titres.

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“…Clinical data were collected from all IPH and CVID patients to record their clinical phenotypes as previously described by Chapel et al 2,5 These phenotypes are: 1) no disease-related complications (infections only); 2) autoimmune cytopenias; 3) polyclonal lymphoproliferation (granuloma/LIP/persistent unexplained lympadenopathy); and 4) unexplained persistent enteropathy. In addition, data were collected concerning the frequency and severity of infections and modes of treatment.…”

Section: Clinical Phenotypingmentioning

confidence: 99%

“…Remarkably, according to the primary immunodeficiency classification of the International Union of Immunological Societies (IUIS) these patients cannot be sufficiently classified within any of the subcategories of "Predominantly Antibody Deficiency". 5 In comparison, the International Classification of Diseases v10 (ICD10), 6 classifies IPH as "hypogammaglobulinemia not otherwise specified" with the same ICD10 code as CVID. Patients Patients with hypogammaglobulinemia who do not fulfill all the classical diagnostic criteria for common variable immunodeficiency (reduction of two immunoglobulin isotypes and a reduced response to vaccination) constitute a diagnostic and therapeutic dilemma, because information concerning the clinical and immunological characteristics of these patients with idiopathic primary hypogammaglobulinemia is not available.…”

Section: Introductionmentioning

confidence: 99%

Common variable immunodeficiency and idiopathic primary hypogammaglobulinemia: two different conditions within the same disease spectrum

et al. 2013

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ABSTRACTical practice, but information concerning the prevalence and the clinical and immunological characteristics is not available. It is important to obtain insight into the frequency and severity of the clinical complications of IPH, to clarify whether IPH is a clinically relevant antibody deficiency, and to develop appropriate treatment strategies. In addition, analysis of immunological parameters will enable the comparison of pathophysiological aspects of IPH and CVID.Therefore, we aimed to determine the position of IPH in the spectrum of idiopathic antibody deficiencies through clinical and immunological comparison with CVID. First, we recorded the patients with the clinical phenotypes as established by Chapel et al. 2,7 In addition, we performed flow cytometric immunophenotyping in order to analyze T-cell dependent and independent memory B-cell subset counts 8 and blood B-cell patterns, which are associated with differences in pathophysiological background. 9 Methods PatientsPeripheral blood samples and clinical data were collected for 44 CVID patients and 21 IPH patients. IPH was diagnosed if patients had a reduction of IgG at least 2 SD below the mean for age, an onset of the immunodeficiency after two years of age, exclusion of defined causes of hypogammaglobulinemia and if they did not fulfill the CVID diagnostic criteria with respect to a reduction of two immunoglobulin isotypes and/or a reduced response to vaccination. The group of CVID patients includes the 37 patients who were reported in our original description of the B-cell patterns. 9 In addition, we collected blood from 130 healthy age-matched controls and 26 cord blood samples. This study was approved by the Medical Ethics Committee of the Erasmus MC. Clinical phenotypingClinical data were collected from all IPH and CVID patients to record their clinical phenotypes as previously described by Chapel et al. 2,5 These phenotypes are: 1) no disease-related complications (infections only); 2) autoimmune cytopenias; 3) polyclonal lymphoproliferation (granuloma/LIP/persistent unexplained lympadenopathy); and 4) unexplained persistent enteropathy. In addition, data were collected concerning the frequency and severity of infections and modes of treatment. Pneumococcal polysaccharide vaccination responses were interpreted according to Borgers et al. 10 as an adequate response to half of the measured pneumococcal serotypes. Flow cytometric analysis and assignment of B-cell patternsSix-color flow cytometric immunophenotyping of peripheral blood was performed on a CantoII (BD Biosiences) and data were analyzed using FACS Diva software (BD Biosiences). The following monoclonal antibodies were used: CD19-PerCP-Cy5.5, CD19-PE-Cy7, CD19-APC (all SJ25C1), CD5-APC ( L17F12 ), CD45-PerCP (2D1), CD19-APC (SJ25C1), CD38-PE, CD38-APC and CD38-PE-Cy7 ( HB7), CD27-APC (L128), CD3-PerCP-Cy5.5 (SK7) and CD8-APC-Cy7 (SK1) (all from BD Biosciences), polyclonal IgD-FITC, IgD-PE and IgM-PE (all from Southern Biotechnologies), polyclonal IgG-FITC (Kallestad), IgA-FITC a...

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Primary Immunodeficiency Diseases: An Update on the Classification from the International Union of Immunological Societies Expert Committee for Primary Immunodeficiency

Cited by 464 publications

References 0 publications

Human genetic basis of interindividual variability in the course of infection

Human genetic basis of interindividual variability in the course of infection

Streptococcus pneumoniae antibody titres in patients with primary antibody deficiency receiving intravenous immunoglobulin (IVIG) compared to subcutaneous immunoglobulin (SCIG)

Common variable immunodeficiency and idiopathic primary hypogammaglobulinemia: two different conditions within the same disease spectrum

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