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Early-onset stroke and vasculopathy associated with mutations in ADA2.

ABSTRACT:

Background

We observed a syndrome of intermittent fevers, early-onset lacunar strokes and other neurovascular manifestations, livedoid rash, hepatosplenomegaly, and systemic vasculopathy in three unrelated patients. We suspected a genetic cause because the disorder presented in early childhood.

Methods

We performed whole-exome sequencing in the initial three patients and their unaffected parents and candidate-gene sequencing in three patients with a similar phenotype, as well as two young siblings with polyarteritis nodosa and one patient with small-vessel vasculitis. Enzyme assays, immunoblotting, immunohistochemical testing, flow cytometry, and cytokine profiling were performed on samples from the patients. To study protein function, we used morpholino-mediated knockdowns in zebrafish and short hairpin RNA knockdowns in U937 cells cultured with human dermal endothelial cells.

Results

All nine patients carried recessively inherited mutations in CECR1 (cat eye syndrome chromosome region, candidate 1), encoding adenosine deaminase 2 (ADA2), that were predicted to be deleterious; these mutations were rare or absent in healthy controls. Six patients were compound heterozygous for eight CECR1 mutations, whereas the three patients with polyarteritis nodosa or small-vessel vasculitis were homozygous for the p.Gly47Arg mutation. Patients had a marked reduction in the levels of ADA2 and ADA2-specific enzyme activity in the blood. Skin, liver, and brain biopsies revealed vasculopathic changes characterized by compromised endothelial integrity, endothelial cellular activation, and inflammation. Knockdown of a zebrafish ADA2 homologue caused intracranial hemorrhages and neutropenia - phenotypes that were prevented by coinjection with nonmutated (but not with mutated) human CECR1. Monocytes from patients induced damage in cocultured endothelial-cell layers.

Conclusions

Loss-of-function mutations in CECR1 were associated with a spectrum of vascular and inflammatory phenotypes, ranging from early-onset recurrent stroke to systemic vasculopathy or vasculitis. (Funded by the National Institutes of Health Intramural Research Programs and others.).

SUBMITTER: Zhou Q 

PROVIDER: S-EPMC4193683 | biostudies-literature | 2014 Mar

REPOSITORIES: biostudies-literature

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Early-onset stroke and vasculopathy associated with mutations in ADA2.

Zhou Qing Q   Yang Dan D   Ombrello Amanda K AK   Zavialov Andrey V AV   Toro Camilo C   Zavialov Anton V AV   Stone Deborah L DL   Chae Jae Jin JJ   Rosenzweig Sergio D SD   Bishop Kevin K   Barron Karyl S KS   Kuehn Hye Sun HS   Hoffmann Patrycja P   Negro Alejandra A   Tsai Wanxia L WL   Cowen Edward W EW   Pei Wuhong W   Milner Joshua D JD   Silvin Christopher C   Heller Theo T   Chin David T DT   Patronas Nicholas J NJ   Barber John S JS   Lee Chyi-Chia R CC   Wood Geryl M GM   Ling Alexander A   Kelly Susan J SJ   Kleiner David E DE   Mullikin James C JC   Ganson Nancy J NJ   Kong Heidi H HH   Hambleton Sophie S   Candotti Fabio F   Quezado Martha M MM   Calvo Katherine R KR   Alao Hawwa H   Barham Beverly K BK   Jones Anne A   Meschia James F JF   Worrall Bradford B BB   Kasner Scott E SE   Rich Stephen S SS   Goldbach-Mansky Raphaela R   Abinun Mario M   Chalom Elizabeth E   Gotte Alisa C AC   Punaro Marilynn M   Pascual Virginia V   Verbsky James W JW   Torgerson Troy R TR   Singer Nora G NG   Gershon Timothy R TR   Ozen Seza S   Karadag Omer O   Fleisher Thomas A TA   Remmers Elaine F EF   Burgess Shawn M SM   Moir Susan L SL   Gadina Massimo M   Sood Raman R   Hershfield Michael S MS   Boehm Manfred M   Kastner Daniel L DL   Aksentijevich Ivona I  

The New England journal of medicine 20140219 10

<h4>Background</h4>We observed a syndrome of intermittent fevers, early-onset lacunar strokes and other neurovascular manifestations, livedoid rash, hepatosplenomegaly, and systemic vasculopathy in three unrelated patients. We suspected a genetic cause because the disorder presented in early childhood.<h4>Methods</h4>We performed whole-exome sequencing in the initial three patients and their unaffected parents and candidate-gene sequencing in three patients with a similar phenotype, as well as t  ...[more]

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