The Spectrum of the Deficiency of Adenosine Deaminase 2: An Observational Analysis of a 60 Patient Cohort

Karyl S. Barron(National Institutes of Health), Ivona Aksentijevich(National Institutes of Health), Natalie Deuitch(National Institutes of Health), Deborah L. Stone(National Institutes of Health), Patrycja Hoffmann(National Institutes of Health), Ryan Videgar-Laird(National Institutes of Health), Ariane Soldatos(National Institutes of Health), Jenna Bergerson(National Institutes of Health), Camilo Toro(National Institutes of Health), Cornelia Cudrici(National Institutes of Health), Michele Nehrebecky(National Institutes of Health), Tina Romeo(National Institutes of Health), Anne Jones(National Institutes of Health), Manfred Boehm(National Institutes of Health), Jennifer A. Kanakry(National Institutes of Health), Dimana Dimitrova(National Institutes of Health), Katherine R. Calvo(National Institutes of Health Clinical Center), Hawwa Alao(National Institutes of Health), Devika Kapuria(National Institutes of Health), Gil Ben Yakov(National Institutes of Health), Dominique C. Pichard(National Institutes of Health), Londa Hathaway(National Institutes of Health), Alessandra Brofferio(National Institutes of Health), Elisa McRae(National Institutes of Health), Natalia Sampaio Moura(National Institutes of Health), Oskar Schnappauf(National Institutes of Health), Sofia Rosenzweig(National Institutes of Health), Theo Heller(National Institutes of Health), Edward W. Cowen(National Institutes of Health), Daniel L. Kastner(National Institutes of Health), Amanda K. Ombrello(National Institutes of Health)
Frontiers in Immunology
January 10, 2022
10.3389/fimmu.2021.811473
Cited by 88Open Access
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Abstract

The deficiency of adenosine deaminase 2 (DADA2) is an autosomal recessively inherited disease that has undergone extensive phenotypic expansion since being first described in patients with fevers, recurrent strokes, livedo racemosa, and polyarteritis nodosa in 2014. It is now recognized that patients may develop multisystem disease that spans multiple medical subspecialties. Here, we describe the findings from a large single center longitudinal cohort of 60 patients, the broad phenotypic presentation, as well as highlight the cohort's experience with hematopoietic cell transplantation and COVID-19. Disease manifestations could be separated into three major phenotypes: inflammatory/vascular, immune dysregulatory, and hematologic, however, most patients presented with significant overlap between these three phenotype groups. The cardinal features of the inflammatory/vascular group included cutaneous manifestations and stroke. Evidence of immune dysregulation was commonly observed, including hypogammaglobulinemia, absent to low class-switched memory B cells, and inadequate response to vaccination. Despite these findings, infectious complications were exceedingly rare in this cohort. Hematologic findings including pure red cell aplasia (PRCA), immune-mediated neutropenia, and pancytopenia were observed in half of patients. We significantly extended our experience using anti-TNF agents, with no strokes observed in 2026 patient months on TNF inhibitors. Meanwhile, hematologic and immune features had a more varied response to anti-TNF therapy. Six patients received a total of 10 allogeneic hematopoietic cell transplant (HCT) procedures, with secondary graft failure necessitating repeat HCTs in three patients, as well as unplanned donor cell infusions to avoid graft rejection. All transplanted patients had been on anti-TNF agents prior to HCT and received varying degrees of reduced-intensity or non-myeloablative conditioning. All transplanted patients are still alive and have discontinued anti-TNF therapy. The long-term follow up afforded by this large single-center study underscores the clinical heterogeneity of DADA2 and the potential for phenotypes to evolve in any individual patient.

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