Inherited ARPC5 mutations cause an actinopathy impairing cell motility and disrupting cytokine signaling

Cristiane J Nunes-Santos ,Mohammad Gharagozlou,Nima Parvaneh,Valarie A Barr ,Raz Somech ,Marita Bosticardo ,Beáta Dérfalvi ,Anne Puel ,Brigette Boast ,Hye Sun Kuehn ,Stefania Pittaluga ,Mones Abu‐Asab ,Tomoki Kawai ,Ottavia M Delmonte ,Douglas B Kuhns ,Jean‐Laurent Casanova ,Julie E Niemela ,Lawrence E Samelson ,Sujin Hwang ,Jennifer Stoddard ,John Davies ,Luigi D Notarangelo ,Magda Carneiro‐Sampaio ,Mary Garofalo ,Danielle Fink ,Bertrand Boisson ,Thomas A Fleisher ,Sergio D Rosenzweig

doi:10.1038/s41467-023-39272-0

Inherited ARPC5 mutations cause an actinopathy impairing cell motility and disrupting cytokine signaling

Cristiane J Nunes-Santos , Mohammad Gharagozlou + Show 26 more

Open Access

https://doi.org/10.1038/s41467-023-39272-0

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Journal: Nature Communications	Publication Date: Jun 22, 2023
Citations: 5	License type: CC BY 4.0

#Early-onset Autoimmunity #Severe Infections + Show 8 more

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Abstract

We describe the first cases of germline biallelic null mutations in ARPC5, part of the Arp2/3 actin nucleator complex, in two unrelated patients presenting with recurrent and severe infections, early-onset autoimmunity, inflammation, and dysmorphisms. This defect compromises multiple cell lineages and functions, and when protein expression is reestablished in-vitro, the Arp2/3 complex conformation and functions are rescued. As part of the pathophysiological evaluation, we also show that interleukin (IL)−6 signaling is distinctively impacted in this syndrome. Disruption of IL-6 classical but not trans-signaling highlights their differential roles in the disease and offers perspectives for therapeutic molecular targets.

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