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. 2016 Nov 7:7:466.
doi: 10.3389/fimmu.2016.00466. eCollection 2016.

Diagnostics of Primary Immunodeficiencies through Next-Generation Sequencing

Vera Gallo  1 Laura Dotta  2 Giuliana Giardino  1 Emilia Cirillo  1 Vassilios Lougaris  2 Roberta D'Assante  1 Alberto Prandini  2 Rita Consolini  3 Emily G Farrow  4 Isabelle Thiffault  4 Carol J Saunders  4 Antonio Leonardi  5 Alessandro Plebani  2 Raffaele Badolato  2 Claudio Pignata  1
Affiliations

Diagnostics of Primary Immunodeficiencies through Next-Generation Sequencing

Vera Gallo et al. Front Immunol. .

Abstract

Background: Recently, a growing number of novel genetic defects underlying primary immunodeficiencies (PIDs) have been identified, increasing the number of PID up to more than 250 well-defined forms. Next-generation sequencing (NGS) technologies and proper filtering strategies greatly contributed to this rapid evolution, providing the possibility to rapidly and simultaneously analyze large numbers of genes or the whole exome.

Objective: To evaluate the role of targeted NGS and whole exome sequencing (WES) in the diagnosis of a case series, characterized by complex or atypical clinical features suggesting a PID, difficult to diagnose using the current diagnostic procedures.

Methods: We retrospectively analyzed genetic variants identified through targeted NGS or WES in 45 patients with complex PID of unknown etiology.

Results: Forty-seven variants were identified using targeted NGS, while 5 were identified using WES. Newly identified genetic variants were classified into four groups: (I) variations associated with a well-defined PID, (II) variations associated with atypical features of a well-defined PID, (III) functionally relevant variations potentially involved in the immunological features, and (IV) non-diagnostic genotype, in whom the link with phenotype is missing. We reached a conclusive genetic diagnosis in 7/45 patients (~16%). Among them, four patients presented with a typical well-defined PID. In the remaining three cases, mutations were associated with unexpected clinical features, expanding the phenotypic spectrum of typical PIDs. In addition, we identified 31 variants in 10 patients with complex phenotype, individually not causative per se of the disorder.

Conclusion: NGS technologies represent a cost-effective and rapid first-line genetic approach for the evaluation of complex PIDs. WES, despite a moderate higher cost compared to targeted, is emerging as a valuable tool to reach in a timely manner, a PID diagnosis with a considerable potential to draw genotype-phenotype correlation. Nevertheless, a large fraction of patients still remains without a conclusive diagnosis. In these patients, the sum of non-diagnostic variants might be proven informative in future studies with larger cohorts of patients.

Keywords: genetic diagnosis; genotype–phenotype correlation; primary immunodeficiencies; targeted next-generation sequencing; whole exome sequencing.

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Figures

Figure 1
Figure 1
Flowchart of the filtering strategy. A schematic overview of the approach/clear-cut strategy used to filter variants identified through T-NGS or WES in order to identify potentially causative mutations.
See this image and copyright information in PMC

References

    1. Al-Herz W, Bousfiha A, Casanova I, Chatila TA, Conley ME, Cunningham-Rundles C, et al. Primary immunodeficiency diseases: an update on the classification from the International Union of Immunological Societies Expert Committee for primary immunodeficiency. Front Immunol (2014) 5:162.10.3389/fimmu.2014.00162 - DOI - PMC - PubMed
    1. Cirillo E, Giardino G, Gallo V, D’Assante R, Grasso F, Romano R, et al. Severe combined immunodeficiency-an update. Ann N Y Acad Sci (2015) 1356:90–106.10.1111/nyas.12849 - DOI - PubMed
    1. Parvaneh N, Casanova JL, Notarangelo LD, Conley ME. Primary immunodeficiencies: a rapidly evolving story. J Allergy Clin Immunol (2013) 131:314–24.10.1016/j.jaci.2012.11.051 - DOI - PubMed
    1. de Greef JC, Wang J, Balog J, den Dunnen JT, Frants RR, Straasheijm KR, et al. Mutations in ZBTB24 are associated with immunodeficiency, centromeric instability, and facial anomalies syndrome type 2. Am J Hum Genet (2011) 88:796–804.10.1016/j.ajhg.2011.04.018 - DOI - PMC - PubMed
    1. Ghosh S, Krux F, Binder V, Gombert M, Niehues T, Feyen O, et al. Array-based sequence capture and generation sequencing for the identification of primary immunodeficiencies. Scand J Immunol (2012) 75:350–4.10.1111/j.1365-3083.2011.02658.x - DOI - PubMed