An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations

An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations

Abstract Introduction The COPA syndrome is a newly recognized monogenic, autosomal dominant autoimmune disease presenting mostly presenting in childhood. Clinical features include inflammation of the lungs, kidneys, and joints. Approximately twenty-six patients with COPA syndrome worldwide have been...

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Main Authors: Anjali Patwardhan, Charles H. Spencer
Format: Article
Language:English
Published: BMC 2019-08-01
Series:Pediatric Rheumatology Online Journal
Subjects:
Autoimmunity
COPA syndrome
Interstitial lung disease
Arthritis
Pulmonary hemorrhage
Alveolitis
Online Access:http://link.springer.com/article/10.1186/s12969-019-0359-9
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spelling doaj-9914ca3a1179466ba2a51ef0df06fc3b2020-11-25T03:57:24ZengBMCPediatric Rheumatology Online Journal1546-00962019-08-0117111310.1186/s12969-019-0359-9An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutationsAnjali Patwardhan0Charles H. Spencer1University of Missouri School of MedicineUniversity of Mississippi Medical Center, Batson Children’s HospitalAbstract Introduction The COPA syndrome is a newly recognized monogenic, autosomal dominant autoimmune disease presenting mostly presenting in childhood. Clinical features include inflammation of the lungs, kidneys, and joints. Approximately twenty-six patients with COPA syndrome worldwide have been investigated all originating from eight families. Patients with this syndrome exhibit heterozygous monogenic missense mutations in the WD40 domain. This domain is a functionally-significant area of the alpha subunit of coatomer-associated protein (COPα) which encodes the coat protein complex I (COPI). The COPI dysfunction is also associated with autoantibody expansion. We report two patients with COPA syndrome. Methods All testing and molecular genetic analysis were performed after obtaining the informed consent of both the patient and parents. A retrospective chart review was carried out on both the patients. Demographic, clinical and laboratory findings were abstracted from outpatient and inpatient encounters. Pulmonary function tests (PFTs), chest computed tomography (CT) scans, and lung biopsy histopathology reports were also reviewed and summarized. Results The index case and the father of the child both demonstrated a unique inflammatory pulmonary, arthritis, and renal disease triad starting in early childhood including pulmonary hemorrhage. The two patients had a novel COPA mutation previously undescribed. Conclusions To date, only four pathological, genetic mutations have been reported that are compatible with COPA syndrome. We here report two patients with COPA syndrome within the same family with a novel COPA gene mutation different than the heterozygous monogenic missense mutations in the WD40 domain and distinct from the clinical phenotypes reported in the literature so far.http://link.springer.com/article/10.1186/s12969-019-0359-9AutoimmunityCOPA syndromeInterstitial lung diseaseArthritisPulmonary hemorrhageAlveolitis
collection DOAJ
language English
format Article
sources DOAJ
author Anjali Patwardhan
Charles H. Spencer
spellingShingle Anjali Patwardhan
Charles H. Spencer
An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations
Pediatric Rheumatology Online Journal
Autoimmunity
COPA syndrome
Interstitial lung disease
Arthritis
Pulmonary hemorrhage
Alveolitis
author_facet Anjali Patwardhan
Charles H. Spencer
author_sort Anjali Patwardhan
title An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations
title_short An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations
title_full An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations
title_fullStr An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations
title_full_unstemmed An unprecedented COPA gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known COPA gene mutations
title_sort unprecedented copa gene mutation in two patients in the same family: comparative clinical analysis of newly reported patients with other known copa gene mutations
publisher BMC
series Pediatric Rheumatology Online Journal
issn 1546-0096
publishDate 2019-08-01
description Abstract Introduction The COPA syndrome is a newly recognized monogenic, autosomal dominant autoimmune disease presenting mostly presenting in childhood. Clinical features include inflammation of the lungs, kidneys, and joints. Approximately twenty-six patients with COPA syndrome worldwide have been investigated all originating from eight families. Patients with this syndrome exhibit heterozygous monogenic missense mutations in the WD40 domain. This domain is a functionally-significant area of the alpha subunit of coatomer-associated protein (COPα) which encodes the coat protein complex I (COPI). The COPI dysfunction is also associated with autoantibody expansion. We report two patients with COPA syndrome. Methods All testing and molecular genetic analysis were performed after obtaining the informed consent of both the patient and parents. A retrospective chart review was carried out on both the patients. Demographic, clinical and laboratory findings were abstracted from outpatient and inpatient encounters. Pulmonary function tests (PFTs), chest computed tomography (CT) scans, and lung biopsy histopathology reports were also reviewed and summarized. Results The index case and the father of the child both demonstrated a unique inflammatory pulmonary, arthritis, and renal disease triad starting in early childhood including pulmonary hemorrhage. The two patients had a novel COPA mutation previously undescribed. Conclusions To date, only four pathological, genetic mutations have been reported that are compatible with COPA syndrome. We here report two patients with COPA syndrome within the same family with a novel COPA gene mutation different than the heterozygous monogenic missense mutations in the WD40 domain and distinct from the clinical phenotypes reported in the literature so far.
topic Autoimmunity
COPA syndrome
Interstitial lung disease
Arthritis
Pulmonary hemorrhage
Alveolitis
url http://link.springer.com/article/10.1186/s12969-019-0359-9
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