Deciphering the genetics of primary angioedema with normal levels of C1 inhibitor

Επιστημονική δημοσίευση - Άρθρο Περιοδικού uoadl:3103633 32 Αναγνώσεις

Μονάδα:
Ερευνητικό υλικό ΕΚΠΑ
Τίτλος:
Deciphering the genetics of primary angioedema with normal levels of C1 inhibitor
Γλώσσες Τεκμηρίου:
Αγγλικά
Περίληψη:
The genetic alteration underlying the great majority of primary angioedema with normal C1 inhibitor (nl-C1-INH-HAE) cases remains unknown. To search for variants associated with nl-C1-INH-HAE, we genotyped 133 unrelated nl-C1-INH-HAE patients using a custom next-generation sequencing platform targeting 55 genes possibly involved in angioedema pathogenesis. Patients already diagnosed with F12 alterations as well as those with histaminergic acquired angioedema were excluded. A variant pathogenicity curation strategy was followed, including a comparison of the results with those of genotyping 169 patients with hereditary angioedema due to C1-inhibitor deficiency (C1-INH-HAE), and only filtered-in variants were studied further. Among the examined nl-C1-INH-HAE patients, carriers of neither the ANGPT1 p.Ala119Ser nor the KNG1 p.Met379Lys variant were found, whereas the PLG p.Lys330Glu was detected in four (3%) unrelated probands (one homozygote). In total, 182 different variants were curated, 21 of which represented novel mutations. Although the frequency of variants per gene was comparable between nl-C1-INH-HAE and C1-INH-HAE, variants of the KNG1 and XPNPEP1 genes were detected only in nl-C1-INH-HAE patients (six and three, respectively). Twenty-seven filtered variants in 23 different genes were detected in nl-C1-INH-HAE more than once, whereas 69/133 nl-C1-INH-HAE patients had compound heterozygotes of filtered variants located in the same or different genes. Pedigree analysis was performed where feasible. Our results indicate the role that alterations in some genes, like KNG1, may play in disease pathogenesis, the complex trait that is possibly underlying in some cases, and the existence of hitherto unrecognized disease endotypes. © 2020 by the authors.
Έτος δημοσίευσης:
2020
Συγγραφείς:
Loules, G.
Parsopoulou, F.
Zamanakou, M.
Csuka, D.
Bova, M.
González-Quevedo, T.
Psarros, F.
Porebski, G.
Speletas, M.
Firinu, D.
del Giacco, S.
Suffritti, C.
Makris, M.
Vatsiou, S.
Zanichelli, A.
Farkas, H.
Germenis, A.E.
Περιοδικό:
Journal of Clinical Medicine Research
Εκδότης:
MDPI
Τόμος:
9
Αριθμός / τεύχος:
11
Σελίδες:
1-8
Λέξεις-κλειδιά:
complement component C1s inhibitor; tranexamic acid, adult; angioneurotic edema; Article; comparative study; controlled study; DNA library; female; gene mutation; genetic association; genetic background; genotype; good clinical practice; high throughput sequencing; human; long term care; major clinical study; male; missense mutation; observational study; pathogenesis; pathogenicity; pathophysiology; protein protein interaction; Sanger sequencing
Επίσημο URL (Εκδότης):
DOI:
10.3390/jcm9113402
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