Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling

BACKGROUND: Knowledge of the genetic variation underlying Primary Immune Deficiency (PID) is increasing. Reanalysis of genome-wide sequencing data from undiagnosed patients with suspected PID may improve the diagnostic rate. METHODS: We included patients monitored at the Department of Infectious Dis...

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Autores principales: Mørup, Sara Bohnstedt, Nazaryan-Petersen, Lusine, Gabrielaite, Migle, Reekie, Joanne, Marquart, Hanne V., Hartling, Hans Jakob, Marvig, Rasmus L., Katzenstein, Terese L., Masmas, Tania N., Lundgren, Jens, Murray, Daniel D., Helleberg, Marie, Borgwardt, Line
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9302041/
https://www.ncbi.nlm.nih.gov/pubmed/35874679
http://dx.doi.org/10.3389/fimmu.2022.906328
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author Mørup, Sara Bohnstedt
Nazaryan-Petersen, Lusine
Gabrielaite, Migle
Reekie, Joanne
Marquart, Hanne V.
Hartling, Hans Jakob
Marvig, Rasmus L.
Katzenstein, Terese L.
Masmas, Tania N.
Lundgren, Jens
Murray, Daniel D.
Helleberg, Marie
Borgwardt, Line
author_facet Mørup, Sara Bohnstedt
Nazaryan-Petersen, Lusine
Gabrielaite, Migle
Reekie, Joanne
Marquart, Hanne V.
Hartling, Hans Jakob
Marvig, Rasmus L.
Katzenstein, Terese L.
Masmas, Tania N.
Lundgren, Jens
Murray, Daniel D.
Helleberg, Marie
Borgwardt, Line
author_sort Mørup, Sara Bohnstedt
collection PubMed
description BACKGROUND: Knowledge of the genetic variation underlying Primary Immune Deficiency (PID) is increasing. Reanalysis of genome-wide sequencing data from undiagnosed patients with suspected PID may improve the diagnostic rate. METHODS: We included patients monitored at the Department of Infectious Diseases or the Child and Adolescent Department, Rigshospitalet, Denmark, for a suspected PID, who had been analysed previously using a targeted PID gene panel (457 PID-related genes) on whole exome- (WES) or whole genome sequencing (WGS) data. A literature review was performed to extend the PID gene panel used for reanalysis of single nucleotide variation (SNV) and small indels. Structural variant (SV) calling was added on WGS data. RESULTS: Genetic data from 94 patients (86 adults) including 36 WES and 58 WGS was reanalysed a median of 23 months after the initial analysis. The extended gene panel included 208 additional PID-related genes. Genetic reanalysis led to a small increase in the proportion of patients with new suspicious PID related variants of uncertain significance (VUS). The proportion of patients with a causal genetic diagnosis was constant. In total, five patients (5%, including three WES and two WGS) had a new suspicious PID VUS identified due to reanalysis. Among these, two patients had a variant added due to the expansion of the PID gene panel, and three patients had a variant reclassified to a VUS in a gene included in the initial PID gene panel. The total proportion of patients with PID related VUS, likely pathogenic, and pathogenic variants increased from 43 (46%) to 47 (50%), as one patient had a VUS detected in both initial- and reanalysis. In addition, we detected new suspicious SNVs and SVs of uncertain significance in PID candidate genes with unknown inheritance and/or as heterozygous variants in genes with autosomal recessive inheritance in 8 patients. CONCLUSION: These data indicate a possible diagnostic gain of reassessing WES/WGS data from patients with suspected PID. Reasons for the possible gain included improved knowledge of genotype-phenotype correlation, expanding the gene panel, and adding SV analyses. Future studies of genotype-phenotype correlations may provide additional knowledge on the impact of the new suspicious VUSs.
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spelling pubmed-93020412022-07-22 Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling Mørup, Sara Bohnstedt Nazaryan-Petersen, Lusine Gabrielaite, Migle Reekie, Joanne Marquart, Hanne V. Hartling, Hans Jakob Marvig, Rasmus L. Katzenstein, Terese L. Masmas, Tania N. Lundgren, Jens Murray, Daniel D. Helleberg, Marie Borgwardt, Line Front Immunol Immunology BACKGROUND: Knowledge of the genetic variation underlying Primary Immune Deficiency (PID) is increasing. Reanalysis of genome-wide sequencing data from undiagnosed patients with suspected PID may improve the diagnostic rate. METHODS: We included patients monitored at the Department of Infectious Diseases or the Child and Adolescent Department, Rigshospitalet, Denmark, for a suspected PID, who had been analysed previously using a targeted PID gene panel (457 PID-related genes) on whole exome- (WES) or whole genome sequencing (WGS) data. A literature review was performed to extend the PID gene panel used for reanalysis of single nucleotide variation (SNV) and small indels. Structural variant (SV) calling was added on WGS data. RESULTS: Genetic data from 94 patients (86 adults) including 36 WES and 58 WGS was reanalysed a median of 23 months after the initial analysis. The extended gene panel included 208 additional PID-related genes. Genetic reanalysis led to a small increase in the proportion of patients with new suspicious PID related variants of uncertain significance (VUS). The proportion of patients with a causal genetic diagnosis was constant. In total, five patients (5%, including three WES and two WGS) had a new suspicious PID VUS identified due to reanalysis. Among these, two patients had a variant added due to the expansion of the PID gene panel, and three patients had a variant reclassified to a VUS in a gene included in the initial PID gene panel. The total proportion of patients with PID related VUS, likely pathogenic, and pathogenic variants increased from 43 (46%) to 47 (50%), as one patient had a VUS detected in both initial- and reanalysis. In addition, we detected new suspicious SNVs and SVs of uncertain significance in PID candidate genes with unknown inheritance and/or as heterozygous variants in genes with autosomal recessive inheritance in 8 patients. CONCLUSION: These data indicate a possible diagnostic gain of reassessing WES/WGS data from patients with suspected PID. Reasons for the possible gain included improved knowledge of genotype-phenotype correlation, expanding the gene panel, and adding SV analyses. Future studies of genotype-phenotype correlations may provide additional knowledge on the impact of the new suspicious VUSs. Frontiers Media S.A. 2022-06-30 /pmc/articles/PMC9302041/ /pubmed/35874679 http://dx.doi.org/10.3389/fimmu.2022.906328 Text en Copyright © 2022 Mørup, Nazaryan-Petersen, Gabrielaite, Reekie, Marquart, Hartling, Marvig, Katzenstein, Masmas, Lundgren, Murray, Helleberg and Borgwardt https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Mørup, Sara Bohnstedt
Nazaryan-Petersen, Lusine
Gabrielaite, Migle
Reekie, Joanne
Marquart, Hanne V.
Hartling, Hans Jakob
Marvig, Rasmus L.
Katzenstein, Terese L.
Masmas, Tania N.
Lundgren, Jens
Murray, Daniel D.
Helleberg, Marie
Borgwardt, Line
Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling
title Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling
title_full Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling
title_fullStr Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling
title_full_unstemmed Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling
title_short Added Value of Reanalysis of Whole Exome- and Whole Genome Sequencing Data From Patients Suspected of Primary Immune Deficiency Using an Extended Gene Panel and Structural Variation Calling
title_sort added value of reanalysis of whole exome- and whole genome sequencing data from patients suspected of primary immune deficiency using an extended gene panel and structural variation calling
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9302041/
https://www.ncbi.nlm.nih.gov/pubmed/35874679
http://dx.doi.org/10.3389/fimmu.2022.906328
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