Consensus approach for the management of severe combined immune deficiency caused by adenosine deaminase deficiency

Kohn, Donald B.; Hershfield, Michael S.; Puck, Jennifer M.; Aiuti, Alessandro; Blincoe, Annaliesse; Gaspar, HB; Notarangelo, Luigi D.; Grunebaum, Eyal

doi:10.1016/j.jaci.2018.08.024

Cited by 113 publications

(104 citation statements)

References 88 publications

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“…Therapeutic small molecules and monoclonal antibodies are now revolutionizing care for many autoimmune diseases, taking the place of steroids because they have fewer systemic side effects. Gene therapy, accomplished by lentiviral addition of a cloned, correct copy of a gene into HSCs of a patient harboring a gene defect, has proven so successful for ADA SCID and X‐linked SCID that it is poised to become standard therapy . Similar gene addition trials are in progress for other PIDs.…”

Section: Evolution Of the Field Of Primary Immunodeficiencymentioning

confidence: 99%

“…Gene therapy, accomplished by lentiviral addition of a cloned, correct copy of a gene into HSCs of a patient harboring a gene defect, has proven so successful for ADA SCID and X-linked SCID that it is poised to become standard therapy. [14][15][16][17] Similar gene addition trials are in progress for other PIDs. Although low doses of chemotherapy appear to be required to make space in bone marrow niches for engraftment of corrected HSC, the difficulties with allogeneic HCT, rejection and GVHD, are avoided.…”

Section: E Voluti On Of the Field Of Primary Immunodeficien C Ymentioning

confidence: 99%

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Newborn screening for severe combined immunodeficiency and T‐cell lymphopenia

Puck

2018

Immunological Reviews

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133

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Summary The development of a T cell receptor excision circle (TREC) assay utilizing dried blood spots made possible universal newborn screening (NBS) for severe combined immunodeficiency (SCID) as a public health measure. Upon being flagged by an abnormal screening test in a SCID screening program, an infant can receive further diagnostic testing for SCID in the neonatal period, prior to onset of infectious complications, to pemit immediate institution of protective measures and definitive, life-saving treatment to establish a functional immune system. SCID screening is now the accepted standard of care in state public health departments across the USA, and it is being adopted in many countries. It has proven effective, with infants having this otherwise inapparent but serious, rare disorder achieving survival and immune reconstitution. In addition to bringing to attention infants with the primary screening target diseases, typical SCID and leaky SCID (due to hypomorphic mutations in known SCID genes), the newborn screening assay for insufficient TRECs in dried blood spots also reveals infants with non-SCID T lymphopenic conditions. Experience has accumulated regarding the range and limitations of diagnoses of newborns with low TRECs and low T cells. Previously unknown immune defects have been discovered, as well as conditions not formerly recognized to have low T cells in the neonatal period.

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Section: Evolution Of the Field Of Primary Immunodeficiencymentioning

confidence: 99%

Section: E Voluti On Of the Field Of Primary Immunodeficien C Ymentioning

confidence: 99%

Newborn screening for severe combined immunodeficiency and T‐cell lymphopenia

Puck

2018

Immunological Reviews

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133

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“…The first disease linked to a defect in adenosine deaminase function, severe combined immunodeficiency (SCID), was described in the 1970s. Extensive multidisciplinary research conducted over more than four decades elucidated its pathogenesis and led to the development of both enzyme replacement and gene therapy . Inspired by the experience with ADA1 deficiency, our goal is to review the discovery and characterization of ADA2 and its gene in humans and invertebrates, the discovery only 5 years ago of ADA2 deficiency in humans, and to update current understanding of its clinical heterogeneity.…”

Section: Introductionmentioning

confidence: 99%

“…Extensive multidisciplinary research conducted over more than four decades elucidated its pathogenesis and led to the development of both enzyme replacement and gene therapy. 8,9 Inspired by the experience with ADA1 deficiency, our goal is to review the discovery and characterization of ADA2 and its gene in humans and invertebrates, the discovery only 5 years ago of…”

Section: Introductionmentioning

confidence: 99%

Human adenosine deaminase 2 deficiency: A multi‐faceted inborn error of immunity

Moens

Hershfield

Arts

et al. 2018

Immunological Reviews

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Human adenosine deaminase 1 deficiency was described in the 1970s to cause severe combined immunodeficiency. The residual adenosine deaminase activity in these patients was attributed to adenosine deaminase 2. Human adenosine deaminase type 2 deficiency (DADA2), due to biallelic deleterious mutations in the ADA2 gene, is the first described monogenic type of small‐ and medium‐size vessel vasculitis. The phenotype of DADA2 also includes lymphoproliferation, cytopenia, and variable degrees of immunodeficiency. The physiological role of ADA2 is still enigmatic hence the pathophysiology of the condition is unclear. Preliminary data showed that in the absence of ADA2, macrophage differentiation is skewed to a pro‐inflammatory M1 subset, which is detrimental for endothelial integrity. The inflammatory phenotype responds well to anti‐TNF therapy with etanercept and that is the first‐line treatment for prevention of severe vascular events including strokes. The classic immunosuppressive drugs are not successful in controlling the disease activity. However, hematopoietic stem cell transplantation (HSCT) has been shown to be a definitive cure in DADA2 patients who present with a severe cytopenia. HSCT can also cure the vascular phenotype and is the treatment modality for patients’ refractory to anti‐cytokine therapies. In this review, we describe what is currently known about the molecular mechanisms of DADA2. Further research on the pathophysiology of this multifaceted condition is needed to fine‐tune and steer future therapeutic strategies.

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“…The enzyme ADA is involved in purine metabolism. A lack of ADA activity leads to the accumulation of toxic deoxyadenosine and dATP (within the cell), and thus the premature death of lymphocyte progenitor cells (Kohn et al, 2019). It is noteworthy that ADA is expressed ubiquitously; hence, ADA deficiency is associated with a number of additional, nonimmune features, such as lung and brain disease (Kohn et al, 2019).…”

Section: Gene Therapy For Ada Deficiencymentioning

confidence: 99%

Gene therapy for severe combined immunodeficiencies and beyond

Fischer

Hacein‐Bey‐Abina

2019

Journal of Experimental Medicine

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Ex vivo retrovirally mediated gene therapy has been shown within the last 20 yr to correct the T cell immunodeficiency caused by γc-deficiency (SCID X1) and adenosine deaminase (ADA) deficiency. The rationale was brought up by the observation of the revertant of SCIDX1 and ADA deficiency as a kind of natural gene therapy. Nevertheless, the first attempts of gene therapy for SCID X1 were associated with insertional mutagenesis causing leukemia, because the viral enhancer induced transactivation of oncogenes. Removal of this element and use of a promoter instead led to safer but still efficacious gene therapy. It was observed that a fully diversified T cell repertoire could be generated by a limited set (<1,000) of progenitor cells. Further advances in gene transfer technology, including the use of lentiviral vectors, has led to success in the treatment of Wiskott–Aldrich syndrome, while further applications are pending. Genome editing of the mutated gene may be envisaged as an alternative strategy to treat SCID diseases.

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Consensus approach for the management of severe combined immune deficiency caused by adenosine deaminase deficiency

Cited by 113 publications

References 88 publications

Newborn screening for severe combined immunodeficiency and T‐cell lymphopenia

Newborn screening for severe combined immunodeficiency and T‐cell lymphopenia

Human adenosine deaminase 2 deficiency: A multi‐faceted inborn error of immunity

Gene therapy for severe combined immunodeficiencies and beyond

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