Abstract
The deficiency of Adenosine Deaminase 2 (DADA2) is a new autoinflammatory disease characterised by an early onset vasculopathy with livedoid skin rash associated with systemic manifestations, CNS involvement and mild immunodeficiency.This condition is secondary to autosomal recessive mutations of CECR1 (Cat Eye Syndrome Chromosome Region 1) gene, mapped to chromosome 22q11.1, that encodes for the enzymatic protein adenosine deaminase 2 (ADA2). By now 19 different mutations in CECR1 gene have been detected.The pathogenetic mechanism of DADA2 is still unclear. ADA2 in a secreted protein mainly expressed by cells of the myeloid lineage; its enzymatic activity is higher in conditions of hypoxia, inflammation and oncogenesis. Moreover ADA2 is able to induce macrophages proliferation and differentiation; it’s deficiency is in fact associated with a reduction of anti-inflammatory macrophages (M2). The deficiency of ADA2 is also associated with an up-regulation of neutrophils-expressed genes and an increased secretion of pro-inflammatory cytokines. The mild immunodeficiency detected in many DADA2 patients suggests a role of this protein in the adaptive immune response; an increased mortality of B cells and a reduction in the number of memory B cells, terminally differentiated B cells and plasmacells has been described in many patients. The lack of the protein is associated with endothelium damage; however the function of this protein in the endothelial homeostasis is still unknown.From the clinical point of view, this disease is characterized by a wide spectrum of severity. Chronic or recurrent systemic inflammation with fever, elevation of acute phase reactants and skin manifestations (mainly represented by livedo reticularis) is the typical clinical picture. While in some patients the disease is mild and skin-limited, others present a severe, even lethal, disease with multi-organ involvement; the CNS involvement is rather common with ischemic or hemorrhagic strokes. In many patients not only the clinical picture but also the histopathologic features are undistinguishable from those of systemic polyarteritis nodosa (PAN). Of note, patients with an unusual phenotype, mainly dominated by clinical manifestations suggestive for an immune-disrective condition, have been described.Due to its rarity, the response to treatment of DADA2 is still anecdotal. While steroids can control the disease’s manifestations at high dosage, none of the common immunosuppressive drugs turned out to be effective. Biologic drugs have been used only in few patients, without a clear effectiveness; anti-TNF drugs are those associated to a better clinical response. Hematopoietic stem cells transplantation was effective in patients with a severe phenotype.
Highlights
The deficiency of Adenosine Deaminase 2 (DADA2) is a recently identified disease, gathered in the family of autoinflammatory diseases, mainly characterised by early-onset polyarteritis, hemorrhagic and ischemic strokes and hypogammaglobulinemia.In February 2014 two independent studies, one held by the American National Institutes of Health in Bethesda [1] and the other one by the Israeli Sharee Zedek Medical Center in Jerusalem [2], identified this new clinical entity, often familial, characterised by early onset livedoid rash associated with systemic inflammation
Some patients presented ischemic or haemorrhagic cerebral stroke, other vasculopathy-related manifestations, hepatosplenomegaly, peripheral neuropathy and mild immunodeficiency. In many cases both the clinical manifestations and the histological findings were consistent with the diagnosis of polyarteritis nodosa (PAN), with childhood-onset
The other patient described in this paper displayed a complete response to treatment with sirolimus; the authors assume that this drug may be of help in the control of the clinical manifestations related to ADA2deficiency, being able to reduce the M1 macrophage differentiation and the production of IL-6 [7]
Summary
The deficiency of Adenosine Deaminase 2 (DADA2) is a recently identified disease, gathered in the family of autoinflammatory diseases, mainly characterised by early-onset polyarteritis, hemorrhagic and ischemic strokes and hypogammaglobulinemia. 3 1 in heterozygosis Fever Skin: Livedo reticularis, urticarial rash CNS/PNS: ischemic and haemorrhagic strokes Visceral involvement: hepatomegaly, splenomegaly, portal hypertension Immune/hematologic system: Pancytopenia, hypogammaglobulinemia (100 %). 4 1 in heterozygosis Fever Skin: Livedo reticularis, ulcerations at extremities CNS/PNS: ischemic stroke, TIA, intracranial haemorrhage, polineuropathy Visceral involvement: bowel stenosis, oral aphtae Immune/hematologic system: hypogammaglobulinemia (100 %). 9 3 in heterozygosis Fever (100 %) Skin: Livedo reticularis (100 %), urticarial rash (33 %) CNS/PNS: ischemic stroke (100 %), haemorrhagic strokes (33 %) Visceral involvement: hepatomegaly (66 %), splenomegaly (100 %), portal hypertension (33 %) Immune/hematologic system: Pancytopenia (66 %), hypogammaglobulinemia (66 %).
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