Early immune reconstitution in an infant with adenosine deaminase deficient severe combined immunodeficiency started on enzyme replacement therapy

Abstract

Severe Combined Immunodeficiency (SCID) due to adenosine deaminase (ADA) deficiency is an inborn error of immunity resulting in the accumulation of adenosine and deoxyadenosine leading to a T-B-NK-phenotype. Enzyme Replacement Therapy with Elapegademase-IvIr is typically used as a bridge prior to undergoing definitive treatment with HSCT or HSC-GT.We report a full-term female infant born to Caucasian parents. Immediate newborn course was unremarkable. She had two borderline newborn screens (NBS) for SCID. There was no consanguinity or family history of immunodeficiency. Physical exam was normal except for absent tonsils. She had profound lymphopenia (Absolute Lymphocyte Count of 210 cells/mL), and initial lymphocyte enumeration showed low CD3 cells (169/mL), decreased CD19 cells (6/mL) and CD16/56+ cells (26/mL) consistent with a T-B-NK- SCID. There was no maternal engraftment. Immunoglobulin studies showed normal IgG (325) with low IgM and IgA. Mitogen proliferation to phytohemagglutinin (PHA) was significantly low (10,200 CPM).A SCID genetics panel revealed two pathogenic variants in ADA (p.Glu319fs and p.Arg149Trp). Biochemical testing confirmed absent ADA activity and elevated total deoxyadenosine nucleotides (dAXP) of 40.3% in RBCs (normally undetectable), consistent with the diagnosis of ADA-SCID. She was promptly started on ERT twice weekly and developed full immune reconstitution of her T-cells, B-cells and NK-cells after 21 days. At that time, her dAXP remained elevated at 10%. Her T-cell function also normalized (PHA 239,562 CPM).We report an infant with ADA-SCID who had two borderline NBS results and developed full immune reconstitution 3 weeks after starting ERT. This is unusual since thymopoiesis typically requires 60–90 days for T-cell reconstitution. While B and NK immune reconstitution typically occurs early, early T-cell numbers lag behind, especially while dAXP levels remain measurable. Both genetic variants in this patient are severe, but somatic mosaicism with reversion of the Arg149Trp point mutation might account for rapid T-cell recovery; further T-cell analysis is planned to assess this possibility. This child is the first case of SCID diagnosed in North Carolina following a borderline NBS, as opposed to abnormal, reinforcing the utility of highly-sensitive TREC thresholds for identification of at-risk infants. [Display omitted] [Display omitted]