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ABSTRACT: Background
Haploinsufficiency of A20 (HA20) is caused by loss-of-function TNFAIP3 variants. Phenotypic and genetic features of HA20 remain uncertain; therefore, the clinical distinction between HA20 and Behçet's disease (BD) requires clarification.Methods
We have collected 12 Japanese BD-like families. Probands of these families were analyzed by whole exome sequencing (WES) and subsequent Sanger sequencing. Clinical features were compared between 54 HA20 patients (including previously reported and new cases) and 520 Japanese BD patients.Results
We identified c.1434C>A:p.(Cys478*) in one family and a 236?kb deletion at 6q23.3 containing TNFAIP3 in another family. Four HA20 patients in the two families presented with childhood-onset recurrent oral and genital ulcers and were initially diagnosed and treated as BD. Consistent with the clinical features of HA20, recurrent, refractory fever attacks (three of four patients), and digestive ulcers (two of the four patients) were observed. A comparison of clinical features between HA20 patients and cohorts of BD patients revealed several critical features specific to HA20. These were early-onset, familial occurrence, recurrent fever attacks, gastrointestinal involvement, and infrequent ocular involvement.Conclusions
We identified a novel nonsense variant and deletion of the entire TNFAIP3 gene in two unrelated Japanese HA20 families. Genetic screening of TNFAIP3 should be considered for familial BD-like patients with early-onset recurrent fevers.
SUBMITTER: Tsuchida N
PROVIDER: S-EPMC6549368 | biostudies-literature | 2019 Jun
REPOSITORIES: biostudies-literature
Tsuchida Naomi N Kirino Yohei Y Soejima Yutaro Y Onodera Masafumi M Arai Katsuhiro K Tamura Eiichiro E Ishikawa Takashi T Kawai Toshinao T Uchiyama Toru T Nomura Shigeru S Kobayashi Daisuke D Taguri Masataka M Mitsuhashi Satomi S Mizuguchi Takeshi T Takata Atsushi A Miyake Noriko N Nakajima Hideaki H Miyatake Satoko S Matsumoto Naomichi N
Arthritis research & therapy 20190604 1
<h4>Background</h4>Haploinsufficiency of A20 (HA20) is caused by loss-of-function TNFAIP3 variants. Phenotypic and genetic features of HA20 remain uncertain; therefore, the clinical distinction between HA20 and Behçet's disease (BD) requires clarification.<h4>Methods</h4>We have collected 12 Japanese BD-like families. Probands of these families were analyzed by whole exome sequencing (WES) and subsequent Sanger sequencing. Clinical features were compared between 54 HA20 patients (including previ ...[more]