Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes

Background: Complement dysregulation has been documented in the molecular pathophysiology of COVID-19 and recently implicated in the relevant pediatric patient inflammatory responses. Aims: Based on our previous data in adults, we hypothesized that signatures of complement genetic variants would als...

Descripción completa

Detalles Bibliográficos
Autores principales: Gavriilaki, Eleni, Touloumenidou, Tasoula, Tsiftsoglou, Stefanos, Tragiannidis, Athanasios, Farmaki, Evangelia, Panagopoulou, Paraskevi, Michailidou, Elisavet, Koravou, Evdoxia, Koutra, Maria, Iosifidis, Ilias, Papadimitriou, Eleni, Papadopoulou-Alataki, Efimia, Papayanni, Penelope Georgia, Varelas, Christos, Papalexandri, Apostolia, Evangeliou, Athanasios, Galli-Tsinopoulou, Assimina, Zafeiriou, Dimitrios, Roilides, Emmanuel, Sakellari, Ioanna, Anagnostopoulos, Achilles
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Hematology. Published by Elsevier Inc. 2021
Materias:
311.Disorders of Platelet Number or Function: Clinical and Epidemiological
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8701696/
http://dx.doi.org/10.1182/blood-2021-149382
_version_ 1784621065203351552
author Gavriilaki, Eleni
Touloumenidou, Tasoula
Tsiftsoglou, Stefanos
Tragiannidis, Athanasios
Farmaki, Evangelia
Panagopoulou, Paraskevi
Michailidou, Elisavet
Koravou, Evdoxia
Koutra, Maria
Iosifidis, Ilias
Papadimitriou, Eleni
Papadopoulou-Alataki, Efimia
Papayanni, Penelope Georgia
Varelas, Christos
Papalexandri, Apostolia
Evangeliou, Athanasios
Galli-Tsinopoulou, Assimina
Zafeiriou, Dimitrios
Roilides, Emmanuel
Sakellari, Ioanna
Anagnostopoulos, Achilles
author_facet Gavriilaki, Eleni
Touloumenidou, Tasoula
Tsiftsoglou, Stefanos
Tragiannidis, Athanasios
Farmaki, Evangelia
Panagopoulou, Paraskevi
Michailidou, Elisavet
Koravou, Evdoxia
Koutra, Maria
Iosifidis, Ilias
Papadimitriou, Eleni
Papadopoulou-Alataki, Efimia
Papayanni, Penelope Georgia
Varelas, Christos
Papalexandri, Apostolia
Evangeliou, Athanasios
Galli-Tsinopoulou, Assimina
Zafeiriou, Dimitrios
Roilides, Emmanuel
Sakellari, Ioanna
Anagnostopoulos, Achilles
author_sort Gavriilaki, Eleni
collection PubMed
description Background: Complement dysregulation has been documented in the molecular pathophysiology of COVID-19 and recently implicated in the relevant pediatric patient inflammatory responses. Aims: Based on our previous data in adults, we hypothesized that signatures of complement genetic variants would also be detectable in pediatric patients exhibiting COVID-19 signs and symptoms. Methods: We prospectively studied consecutive pediatric patients from our COVID-19 Units (November 2020-March 2021). COVID-19 was confirmed by reverse-transcriptase polymerase chain reaction (RT-PCR). Patient data were recorded by treating physicians that followed patients up to discharge. DNA was obtained from peripheral blood samples. Probes were designed using the Design studio (Illumina). Amplicons cover exons of complement-associated genes (C3, C5, CFB, CFD,  CFH, CFHR1, CFI, CD46, CD55, MBL2, MASP1, MASP2, COLEC11, FCN1, FCN3 as well as ADAMTS13 and ΤHBD) spanning 15 bases into introns. We used 10ng of initial DNA material. Libraries were quantified using Qubit and sequenced on a MiniSeq System in a 2x150 bp run. Analysis was performed using the TruSeq Amplicon application (BaseSpace). Alignment was based on the banded Smith-Waterman algorithm in the targeted regions (specified in a manifest file). We performed variant calling with the Illumina-developed Somatic Variant Caller in germline mode and variant allele frequency higher than 20%. Both Ensembl and Refseq were used for annotation of the output files. A preliminary analysis (A) for the identification of variants of clinical significance was based on annotated ClinVar data, while a further and more selective analysis (B) was performed to identify missense complement coding variants that may biochemically contribute to the deregulation of innate responses during infection. This analysis was mainly based on the dbSNP and UniProt databases and available literature. Results: 1. In our preliminary analysis, patients exhibited heterogeneous variant profiles including pathogenic, benign, likely benign, and variants of unknown significance (median number of variants: 97, range: 61-103). We found a variant of ADAMTS13 (rs2301612, missense) in 39 patients. We also detected two missense risk factor variants, previously detected in complement-related diseases: rs2230199 in C3 (33 patients); and rs800292 in CFH (36 patients). Among them, 40 patients had a combination of these characterized variants. This combination was significantly associated with the presence of dyspnea (p=0.031) and cough (p=0.042). Furthermore, 27 patients had a pathogenic variant in MBL2 (rs1800450), and 7 a pathogenic deletion in FCN3 that have been previously associated with inflammatory syndromes. 2. The results of our further analysis are summarized in Figure. We identified common variants, some well represented by relatively high frequencies (>70%) (rs11098044 in CFI, rs1061170 in CFH and rs12711521 in MASP2) and others less abundant, but varying considerably between the hospitalized group, the non-admitted group and the MIS-C individuals (rs2230199 in C3, rs1065489 in CFH, rs12614 and rs641153 in CFB, rs1800450 in MBL2, rs2273346 and rs72550870 in MASP2, rs72549154 in MASP3 and rs7567833 in COLEC11, all highlighted in Figure in red).). Structurally, the majority of these common variants of interest encode charge reversal mutations. These may influence protein-protein interactions in complex formations that are important for complement activation and/or regulation. Conclusion: In pediatric COVID-19 we have detected a novel set of complement missense coding variants some of which have been implicated earlier in inflammatory syndromes and endothelial stress responses. Certain combinations of mutations of alternative and/or lectin pathway components may increase the threshold dynamics of complement consumption and therefore alter COVID-19 phenotypes. [Figure: see text] DISCLOSURES: Gavriilaki:  Alexion, Omeros, Sanofi Corporation: Consultancy; Gilead Corporation: Honoraria; Pfizer Corporation: Research Funding. Anagnostopoulos:  Abbvie: Other: clinical trials; Sanofi: Other: clinical trials ; Ocopeptides: Other: clinical trials ; GSK: Other: clinical trials; Incyte: Other: clinical trials ; Takeda: Other: clinical trials ; Amgen: Other: clinical trials ; Janssen: Other: clinical trials; novartis: Other: clinical trials; Celgene: Other: clinical trials; Roche: Other: clinical trials; Astellas: Other: clinical trials .
format Online
Article
Text
id pubmed-8701696
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher American Society of Hematology. Published by Elsevier Inc.
record_format MEDLINE/PubMed
spelling pubmed-87016962021-12-28 Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes Gavriilaki, Eleni Touloumenidou, Tasoula Tsiftsoglou, Stefanos Tragiannidis, Athanasios Farmaki, Evangelia Panagopoulou, Paraskevi Michailidou, Elisavet Koravou, Evdoxia Koutra, Maria Iosifidis, Ilias Papadimitriou, Eleni Papadopoulou-Alataki, Efimia Papayanni, Penelope Georgia Varelas, Christos Papalexandri, Apostolia Evangeliou, Athanasios Galli-Tsinopoulou, Assimina Zafeiriou, Dimitrios Roilides, Emmanuel Sakellari, Ioanna Anagnostopoulos, Achilles Blood 311.Disorders of Platelet Number or Function: Clinical and Epidemiological Background: Complement dysregulation has been documented in the molecular pathophysiology of COVID-19 and recently implicated in the relevant pediatric patient inflammatory responses. Aims: Based on our previous data in adults, we hypothesized that signatures of complement genetic variants would also be detectable in pediatric patients exhibiting COVID-19 signs and symptoms. Methods: We prospectively studied consecutive pediatric patients from our COVID-19 Units (November 2020-March 2021). COVID-19 was confirmed by reverse-transcriptase polymerase chain reaction (RT-PCR). Patient data were recorded by treating physicians that followed patients up to discharge. DNA was obtained from peripheral blood samples. Probes were designed using the Design studio (Illumina). Amplicons cover exons of complement-associated genes (C3, C5, CFB, CFD,  CFH, CFHR1, CFI, CD46, CD55, MBL2, MASP1, MASP2, COLEC11, FCN1, FCN3 as well as ADAMTS13 and ΤHBD) spanning 15 bases into introns. We used 10ng of initial DNA material. Libraries were quantified using Qubit and sequenced on a MiniSeq System in a 2x150 bp run. Analysis was performed using the TruSeq Amplicon application (BaseSpace). Alignment was based on the banded Smith-Waterman algorithm in the targeted regions (specified in a manifest file). We performed variant calling with the Illumina-developed Somatic Variant Caller in germline mode and variant allele frequency higher than 20%. Both Ensembl and Refseq were used for annotation of the output files. A preliminary analysis (A) for the identification of variants of clinical significance was based on annotated ClinVar data, while a further and more selective analysis (B) was performed to identify missense complement coding variants that may biochemically contribute to the deregulation of innate responses during infection. This analysis was mainly based on the dbSNP and UniProt databases and available literature. Results: 1. In our preliminary analysis, patients exhibited heterogeneous variant profiles including pathogenic, benign, likely benign, and variants of unknown significance (median number of variants: 97, range: 61-103). We found a variant of ADAMTS13 (rs2301612, missense) in 39 patients. We also detected two missense risk factor variants, previously detected in complement-related diseases: rs2230199 in C3 (33 patients); and rs800292 in CFH (36 patients). Among them, 40 patients had a combination of these characterized variants. This combination was significantly associated with the presence of dyspnea (p=0.031) and cough (p=0.042). Furthermore, 27 patients had a pathogenic variant in MBL2 (rs1800450), and 7 a pathogenic deletion in FCN3 that have been previously associated with inflammatory syndromes. 2. The results of our further analysis are summarized in Figure. We identified common variants, some well represented by relatively high frequencies (>70%) (rs11098044 in CFI, rs1061170 in CFH and rs12711521 in MASP2) and others less abundant, but varying considerably between the hospitalized group, the non-admitted group and the MIS-C individuals (rs2230199 in C3, rs1065489 in CFH, rs12614 and rs641153 in CFB, rs1800450 in MBL2, rs2273346 and rs72550870 in MASP2, rs72549154 in MASP3 and rs7567833 in COLEC11, all highlighted in Figure in red).). Structurally, the majority of these common variants of interest encode charge reversal mutations. These may influence protein-protein interactions in complex formations that are important for complement activation and/or regulation. Conclusion: In pediatric COVID-19 we have detected a novel set of complement missense coding variants some of which have been implicated earlier in inflammatory syndromes and endothelial stress responses. Certain combinations of mutations of alternative and/or lectin pathway components may increase the threshold dynamics of complement consumption and therefore alter COVID-19 phenotypes. [Figure: see text] DISCLOSURES: Gavriilaki:  Alexion, Omeros, Sanofi Corporation: Consultancy; Gilead Corporation: Honoraria; Pfizer Corporation: Research Funding. Anagnostopoulos:  Abbvie: Other: clinical trials; Sanofi: Other: clinical trials ; Ocopeptides: Other: clinical trials ; GSK: Other: clinical trials; Incyte: Other: clinical trials ; Takeda: Other: clinical trials ; Amgen: Other: clinical trials ; Janssen: Other: clinical trials; novartis: Other: clinical trials; Celgene: Other: clinical trials; Roche: Other: clinical trials; Astellas: Other: clinical trials . American Society of Hematology. Published by Elsevier Inc. 2021-11-23 2021-12-24 /pmc/articles/PMC8701696/ http://dx.doi.org/10.1182/blood-2021-149382 Text en Copyright © 2021 American Society of Hematology. Published by Elsevier Inc. All rights reserved. Since January 2020 Elsevier has created a COVID-19 resource centre with free information in English and Mandarin on the novel coronavirus COVID-19. The COVID-19 resource centre is hosted on Elsevier Connect, the company's public news and information website. Elsevier hereby grants permission to make all its COVID-19-related research that is available on the COVID-19 resource centre - including this research content - immediately available in PubMed Central and other publicly funded repositories, such as the WHO COVID database with rights for unrestricted research re-use and analyses in any form or by any means with acknowledgement of the original source. These permissions are granted for free by Elsevier for as long as the COVID-19 resource centre remains active.
spellingShingle 311.Disorders of Platelet Number or Function: Clinical and Epidemiological
Gavriilaki, Eleni
Touloumenidou, Tasoula
Tsiftsoglou, Stefanos
Tragiannidis, Athanasios
Farmaki, Evangelia
Panagopoulou, Paraskevi
Michailidou, Elisavet
Koravou, Evdoxia
Koutra, Maria
Iosifidis, Ilias
Papadimitriou, Eleni
Papadopoulou-Alataki, Efimia
Papayanni, Penelope Georgia
Varelas, Christos
Papalexandri, Apostolia
Evangeliou, Athanasios
Galli-Tsinopoulou, Assimina
Zafeiriou, Dimitrios
Roilides, Emmanuel
Sakellari, Ioanna
Anagnostopoulos, Achilles
Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes
title Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes
title_full Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes
title_fullStr Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes
title_full_unstemmed Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes
title_short Identification of Complement-Related Missense Variants in Pediatric Patients with Acute and Post COVID-19 Syndromes
title_sort identification of complement-related missense variants in pediatric patients with acute and post covid-19 syndromes
topic 311.Disorders of Platelet Number or Function: Clinical and Epidemiological
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8701696/
http://dx.doi.org/10.1182/blood-2021-149382
work_keys_str_mv AT gavriilakieleni identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT touloumenidoutasoula identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT tsiftsogloustefanos identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT tragiannidisathanasios identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT farmakievangelia identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT panagopoulouparaskevi identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT michailidouelisavet identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT koravouevdoxia identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT koutramaria identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT iosifidisilias identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT papadimitrioueleni identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT papadopouloualatakiefimia identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT papayannipenelopegeorgia identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT varelaschristos identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT papalexandriapostolia identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT evangeliouathanasios identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT gallitsinopoulouassimina identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT zafeirioudimitrios identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT roilidesemmanuel identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT sakellariioanna identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes
AT anagnostopoulosachilles identificationofcomplementrelatedmissensevariantsinpediatricpatientswithacuteandpostcovid19syndromes

Ejemplares similares