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  • Primary immunodeficiencies

Observe warning signs and react!

    • Partner Content
    • RX
  • 3 minute read

Although most primary immunodeficiencies (PGDs) manifest in childhood, the disease is often not recognized until adulthood [1]. In this context, only early diagnosis can reduce morbidity and prevent deaths [2].

Immunodeficiencies arise as a result of dysfunction of the innate or adaptive immune system [2]. If the cause is a genetic defect, these are primary immunodeficiencies (PIDs), a rapidly growing group of over 400 immunodeficiencies, 200 of which have been identified only in the last decade [3].
The prevalence of PGD varies according to the type of disease, region, and population group [2]. In Switzerland, it is estimated to be 1:10000 – 1:500000 depending on the disease and region [4]. Thanks to diagnostic advances, the number of new PID diagnoses has risen sharply in recent years and recent epidemiological surveys suggest that the prevalence is significantly higher [2].

Antibody deficiency in over 50% of affected individuals

PGDs are divided into nine groups according to the components of the immune system affected(Table 1) [2]. Defects associated with decreased antibody production lead to antibody deficiency disease. They are by far the largest group and affect over half of PGD patients [2].

Table 1: Grouping of PGDs according to the affected component of the immune system. Adapted from [5].

Warning Signs: Also Think of PID in Autoimmunity

If the immune system’s defense function is impaired, infections become more frequent. Therefore, pathological susceptibility to infection is a major leading symptom of PID [2]. However, the identification of new genetic defects has enormously broadened the clinical picture in recent years and finally led to a paradigm shift: PID is no longer understood only as increased susceptibility to infections, but as a general malfunction of the immune system, which also includes disorders of immune regulation [3]. These include autoimmune and auto-inflammatory conditions such as skin eczema, chronic intestinal inflammation, allergies, and granulomas, and may be the sole symptom of PID [2].

10 warning signs of primary immunodeficiency in children

  • Four or more new onset ear infections within one year
  • Two or more severe sinusitis within one year
  • Two or more months under antibiotic therapy without noticeable effect
  • Two or more pneumonias within one year
  • No weight gain or no normal growth of the infant
  • Recurrent abscesses deep under the skin or in internal organs
  • Persistent thrush in the mouth or fungal infections of the skin
  • Need for intravenous antibiotics to eliminate infections.
  • Two or more deep-seated infections, including sepsis
  • Primary immunodeficiency in the family history

See Jeffrey Model Foundation:

http://downloads.info4pi.org/pdfs/10-Warning-Signs—Generic-Text–2-.pdf

ELVIS and GARFIELD for the detection of the warning signals

The enormous heterogeneity of symptoms and the difficult differentiation from other diseases cause a high diagnostic latency [2]. Detection of pathologic susceptibility to infection is difficult due to the lack of cutoff values, as is the differentiation of PID-associated immune dysregulation from other autoimmune diseases. To help physicians recognize important PGD warning signs, the acronyms ELVIS and GARFIELD were introduced(Table 2) [2].

Table 2: The acronyms ELVIS and GARFIELD facilitate the identification of pathological susceptibility to infection and immune dysregulation. Adapted from [2].

Early clarification reduces mortality

According to the European Society of Immunodeficiencies (ESID), the mortality risk of PGD increases by 1.7% with each year of diagnostic delay [2]. Early detection therefore plays an important role in preventing long-term damage. If warning signs of the ELVIS or GARFIELD scheme are present, a workup for PID is reasonable. This is also true in chronic diarrhea in infancy or early childhood, especially when failure to thrive is added [2]. More than half of PIDs are associated with antibody deficiency, which can also be detected in office-based practices by laboratory determination of serum immunoglobulins IgM, IgG, IgA, and IgE [2].

Conclusion

Although PID manifests in childhood, the majority of PID diagnoses occur in adults [1]. Early detection plays an important role in preventing long-term sequelae of PGD and reducing mortality [2]. To achieve this, pediatricians and family physicians should also be aware of the warning signs to identify PID [5]. The acronyms ELVIS and GARFILED can help you with this [2].

Literature

1. Amaya-Uribe, L., et al, Primary immunodeficiency and autoimmunity: a comprehensive review. Journal of autoimmunity, 2019. 99: p. 52-72.
Göschl, L., et al, Diagnostics and therapy of primary immunodeficiencies/”inborn errors of immunity “. Wiener klinische Wochenschrift Education, 2019. 14(1): p. 65-79.
3. Bucciol, G. and I. Meyts, Recent advances in primary immunodeficiency: from molecular diagnosis to treatment. F1000Research, 2020. 9.
4. https://www.immunschwaeche-schweiz.ch/de/?oid=1&lang=de. Last call: May 2021.
5. Douglas Paes Barreto, I.C., et al, Immunological deficiencies: more frequent than they seem to be. 2020.

This text was produced with the financial support of Takeda Pharma AG.

C-ANPROM/CH/CUVI/0009   06/2021

Post online since 20.07.2021

Partner
  • takeda_neu_4
Autoren
  • Dr. sc. ETH Jenny Thom
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