Your search keyword '"severe combined immune deficiency"' showing total 140 results

1. Variable clinical presentation of hypomorphic DCLRE1C deficiency from childhood to adulthood.

Author

Hazar, Esra, Karaselek, Mehmet Ali, Kapakli, Hasan, Dogar, Oznur, Kuccukturk, Serkan, Uygun, Vedat, Artac, Hasibe, Fındık, Sıdıka, Sahin, Ali, Arslan, Sevket, Guner, Sukru, Reisli, Ismail, and Keles, Sevgi

Subjects

*HEMATOPOIETIC stem cell transplantation, *KILLER cells, *INTERFERON gamma, *B cells, *SEVERE combined immunodeficiency, *IMMUNODEFICIENCY

Abstract

Background: In this study, we aimed to report long‐term follow‐up of our pediatric and adult patients with DCLRE1C (DNA cross‐link repair 1C) hypomorphic mutation who were diagnosed leaky severe combined immunodeficiency (SCID). Methods: Eighteen patients (13 children and five adults), aged between 6 and 29 years were included. Clinical and immunological features, including immunoglobulin levels, T and B cells, natural killer cell subsets, regulator T (Treg) cell ratios/markers, and cytokines, were assessed before and after hematopoietic stem cell transplantation (HSCT) and compared with healthy controls. Results: Recurrent infections (78%) and skin manifestations (61%) such as granulomatous skin lesions, warts, and vitiligo were the most common clinical findings. Autoimmune diseases were observed in 33% and malignancy in 17%. Most patients had low serum IgA and B‐ and T‐cell lymphopenia at the first admission. Recent thymic emigrants (RTE), Tnaive, Bnaive, CD56dimCD16+ cell ratios were significantly lower in the patients than in control; however, follicular helper T TFH and Th1 [interferon gamma (IFN‐γ)] cell ratios were significantly higher than the control. Although, Treg ratio and its functional receptors tend to be high but not significant. Eleven patients (61.1%) were treated with HSCT. Median follow‐up times of transplant patients was 56 (9–67) months. Conclusion: Patients with hypomorphic DCLRE1C mutations may present with variable clinical and laboratory findings at different ages. Our study showed a helper T (Th)1‐dominant immune response before and after HSCT. Increased IFN‐γ and TFH cells ratio could be a reason of chronic inflammation and autoimmunity developing before and after HSCT. Long‐term follow‐up of these patients after HSCT will help to better understand the disease and its pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2024

2. Expanding the PRAAS spectrum: De novo mutations of immunoproteasome subunit β-type 10 in six infants with SCID-Omenn syndrome.

Author

van der Made, Caspar I., Kersten, Simone, Chorin, Odelia, Engelhardt, Karin R., Ramakrishnan, Gayatri, Griffin, Helen, Schim van der Loeff, Ina, Venselaar, Hanka, Rothschild, Annick Raas, Segev, Meirav, Schuurs-Hoeijmakers, Janneke H.M., Mantere, Tuomo, Essers, Rick, Esteki, Masoud Zamani, Avital, Amir L., Loo, Peh Sun, Simons, Annet, Pfundt, Rolph, Warris, Adilia, and Seyger, Marieke M.

Subjects

*PROTEOLYSIS, *SEVERE combined immunodeficiency, *GENETIC variation, *INFANTS, *STEM cell transplantation, *T cell receptors, BONE marrow examination

Abstract

Mutations in proteasome β-subunits or their chaperone and regulatory proteins are associated with proteasome-associated autoinflammatory disorders (PRAAS). We studied six unrelated infants with three de novo heterozygous missense variants in PSMB10 , encoding the proteasome β2i-subunit. Individuals presented with T-B-NK± severe combined immunodeficiency (SCID) and clinical features suggestive of Omenn syndrome, including diarrhea, alopecia, and desquamating erythematous rash. Remaining T cells had limited T cell receptor repertoires, a skewed memory phenotype, and an elevated CD4/CD8 ratio. Bone marrow examination indicated severely impaired B cell maturation with limited V(D)J recombination. All infants received an allogeneic stem cell transplant and exhibited a variety of severe inflammatory complications thereafter, with 2 peri-transplant and 2 delayed deaths. The single long-term transplant survivor showed evidence for genetic rescue through revertant mosaicism overlapping the affected PSMB10 locus. The identified variants (c.166G>C [p.Asp56His] and c.601G>A/c.601G>C [p.Gly201Arg]) were predicted in silico to profoundly disrupt 20S immunoproteasome structure through impaired β-ring/β-ring interaction. Our identification of PSMB10 mutations as a cause of SCID-Omenn syndrome reinforces the connection between PRAAS-related diseases and SCID. [Display omitted] This study highlights the identification of recurrent heterozygous de novo mutations in immunoproteasome subunit β2i (PSMB10) as a cause for SCID-Omenn syndrome. These variants are predicted to profoundly disrupt immunoproteasome structure and function, emphasizing its importance for lymphocyte development. Pathogenic variants in PSMB10 should be sought in SCID newborn screening. [ABSTRACT FROM AUTHOR]

Published

2024

3. Profile of 208 patients with inborn errors of immunity at a tertiary care center in South India.

Author

Bhattad, Sagar, Mohite, Rachna S., Singh, Neha, Kotecha, Udhaya, Jhawar, Prerna, Ramprakash, Stalin, Commondoor, Raghuram, Jayaram, Ananthvikas, Rayabarapu, Pranavchand, Kumar, Harish, Unni, Jeeson, Cyril, Gladys, Kumar, Suresh, Pachat, Divya, Jakka, Shrinivas, Makam, Adinarayana, Porta, Fulvio, and Ginigeri, Chetan

Subjects

*PRIMARY immunodeficiency diseases, *JOB'S syndrome, *AUTOIMMUNE diseases, *TERTIARY care, *AUTOINFLAMMATORY diseases, *SEROTHERAPY

Abstract

Primary immune deficiencies or inborn errors of immunity (IEI) are a heterogeneous group of disorders that predispose affected individuals to infections, allergy, autoimmunity, autoinflammation and malignancies. IEIs are increasingly being recognized in the Indian subcontinent. Two hundred and eight patients diagnosed with an IEI during February 2017 to November 2021 at a tertiary care center in South India were included in the study. The clinical features, laboratory findings including microbiologic and genetic data, and treatment and outcome details were analyzed. The diagnosis of IEI was confirmed in a total of 208 patients (198 kindreds) based on relevant immunological tests and/or genetic tests. The male-to-female ratio was 1.8:1. Of the 208 patients, 72 (34.6%) were < 1 yr, 112 (53.8%) were 1–18 years, and 24 (11.5%) were above 18 years. The most common IEI in our cohort was SCID (17.7%) followed by CGD (12.9%) and CVID (9.1%). We also had a significant proportion of patients with DOCK8 deficiency (7.2%), LAD (6.2%) and six patients (2.8%) with autoinflammatory diseases. Autoimmunity was noted in forty-six (22%) patients. Molecular testing was performed in 152 patients by exome sequencing on the NGS platform, and a genetic variant was reported in 132 cases. Twenty-nine children underwent 34 HSCT, and 135 patients remain on supportive therapy such as immunoglobulin replacement and/or antimicrobial prophylaxis. Fifty-nine (28.3%) patients died during the study period, and infections were the predominant cause of mortality. Seven families underwent prenatal testing in the subsequent pregnancy. We describe the profile of 208 patients with IEI, and to the best of our knowledge, this represents the largest data on IEI from the Indian subcontinent reported so far. [ABSTRACT FROM AUTHOR]

Published

2023

4. Normal IgH Repertoire Diversity in an Infant with ADA Deficiency After Gene Therapy

Author

Baloh, Carolyn H, Borkar, Samiksha A, Chang, Kai-Fen, Yao, Jiqiang, Hershfield, Michael S, Parikh, Suhag H, Kohn, Donald B, Goodenow, Maureen M, Sleasman, John W, and Yin, Li

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Pediatric, Biotechnology, Clinical Research, Stem Cell Research, Genetics, Gene Therapy, Hematology, Good Health and Well Being, Adenosine Deaminase, Agammaglobulinemia, Enzyme Replacement Therapy, Female, Genetic Therapy, Humans, Immunoglobulin Heavy Chains, Infant, Lymphocyte Count, Severe Combined Immunodeficiency, Severe combined immune deficiency, adenosine deaminase deficiency, gene therapy, B cell repertoire, immunoglobulin sequencing, Immunology

Abstract

PurposeAdenosine deaminase (ADA) deficiency causes severe combined immunodeficiency (SCID) through an accumulation of toxic metabolites within lymphocytes. Recently, ADA deficiency has been successfully treated using lentiviral-transduced autologous CD34+ cells carrying the ADA gene. T and B cell function appears to be fully restored, but in many patients' B cell numbers remain low, and assessments of the immunoglobulin heavy (IgHV) repertoire following gene therapy are lacking.MethodsWe performed deep sequencing of IgHV repertoire in peripheral blood lymphocytes from a child following lentivirus-based gene therapy for ADA deficiency and compared to the IgHV repertoire in healthy infants and adults.ResultsAfter gene therapy, Ig diversity increased over time as evidenced by V, D, and J gene usage, N-additions, CDR3 length, extent of somatic hypermutation, and Ig class switching. There was the emergence of predominant IgHM, IgHG, and IgHA CDR3 lengths after gene therapy indicating successful oligoclonal expansion in response to antigens. This provides proof of concept for the feasibility and utility of molecular monitoring in following B cell reconstitution following gene therapy for ADA deficiency.ConclusionBased on deep sequencing, gene therapy resulted in an IgHV repertoire with molecular diversity similar to healthy infants.

Published

2021

5. Inborn Errors of Immunity—the Sri Lankan Experience 2010–2022.

Author

Dasanayake, Dhanushka, Bustamante, Jacinta, Boisson–Dupuis, Stéphanie, Karunatilleke, Chandima, Thambyrajah, James, Puel, Anne, Chan, Koon Wing, Doffinger, Rainer, Lau, Yu-Lung, Casanova, Jean-Laurent, Kumararatne, Dinakantha, and de Silva, Rajiva

Subjects

*CHRONIC granulomatous disease, *SEVERE combined immunodeficiency, *IMMUNITY, *MEDICAL research, *NUCLEOTIDE sequencing, *AGAMMAGLOBULINEMIA

Abstract

Purpose: Inborn errors of immunity (IEI) are typically monogenic. Data from the Indian subcontinent are relatively scarce. This paper evaluates IEI diagnosed in Sri Lanka. Methods: Data of patients diagnosed with IEI from 2010 to 2022 at the Department of Immunology, Medical Research Institute, Colombo, Sri Lanka, were retrospectively analyzed. Results: Two hundred and six patients were diagnosed with IEI, with a prevalence of 0.94 per 100,000. The onset of disease was below 12 years in 84.9%, whereas in 10.9%, it was after 18 years. The male: female ratio was 1.78:1. Consanguinity was identified in 26.6%. IEI were found in all but one (bone marrow failure) of the 10 IUIS categories. Predominantly antibody deficiencies were the most common category among the nine identified (30.1%), followed by combined immune deficiencies with syndromic features (21.3%), immunodeficiencies affecting cellular and humoral immunity (19.9%), congenital defects of phagocyte number or function (13.1%), and defects in intrinsic and innate immunity (8.2%). Severe combined immune deficiency (SCID) was the commonest disease (14.6%), followed by chronic granulomatous disease (CGD) (10.6%) and X linked agammaglobulinemia (8.7%). Of the patients with a known outcome (n = 184), 51 died (27.7%). Mortality rates were high in SCID (83.3%), Omenn syndrome (OS) (100%), and CGD (31.8%) patients. Conclusion: IEI in Sri Lanka are diagnosed mainly in childhood. The low diagnosis rates suggest a need for educating clinicians regarding IEI in adulthood. The high mortality rates associated with some IEI indicate the need of transplant services in the country. [ABSTRACT FROM AUTHOR]

Published

2023

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

Author

Kohn, Donald B, Hershfield, Michael S, Puck, Jennifer M, Aiuti, Alessandro, Blincoe, Annaliesse, Gaspar, H Bobby, Notarangelo, Luigi D, and Grunebaum, Eyal

Subjects

Animals, Humans, Agammaglobulinemia, Severe Combined Immunodeficiency, Adenosine Deaminase, Hematopoietic Stem Cell Transplantation, Consensus, Enzyme Replacement Therapy, Genetic Therapy, Adenosine deaminase deficiency, enzyme replacement therapy, gene therapy, hematopoietic stem cell transplantation, lentivirus, severe combined immune deficiency, Pediatric, Stem Cell Research, Transplantation, Clinical Research, Stem Cell Research - Nonembryonic - Human, Regenerative Medicine, Hematology, Stem Cell Research - Nonembryonic - Non-Human, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Immunology, Allergy

Abstract

Inherited defects in adenosine deaminase (ADA) cause a subtype of severe combined immunodeficiency (SCID) known as severe combined immune deficiency caused by adenosine deaminase defects (ADA-SCID). Most affected infants can receive a diagnosis while still asymptomatic by using an SCID newborn screening test, allowing early initiation of therapy. We review the evidence currently available and propose a consensus management strategy. In addition to treatment of the immune deficiency seen in patients with ADA-SCID, patients should be followed for specific noninfectious respiratory, neurological, and biochemical complications associated with ADA deficiency. All patients should initially receive enzyme replacement therapy (ERT), followed by definitive treatment with either of 2 equal first-line options. If an HLA-matched sibling donor or HLA-matched family donor is available, allogeneic hematopoietic stem cell transplantation (HSCT) should be pursued. The excellent safety and efficacy observed in more than 100 patients with ADA-SCID who received gammaretrovirus- or lentivirus-mediated autologous hematopoietic stem cell gene therapy (HSC-GT) since 2000 now positions HSC-GT as an equal alternative. If HLA-matched sibling donor/HLA-matched family donor HSCT or HSC-GT are not available or have failed, ERT can be continued or reinstituted, and HSCT with alternative donors should be considered. The outcomes of novel HSCT, ERT, and HSC-GT strategies should be evaluated prospectively in "real-life" conditions to further inform these management guidelines.

Published

2019

7. T and NK Cells in IL2RG-Deficient Patient 50 Years After Hematopoietic Stem Cell Transplantation.

Author

Melsen, Janine E., van Ostaijen-ten Dam, Monique M., van den Akker, Erik B., Welters, Marij J. P., Heezen, Kim C., Pico-Knijnenburg, Ingrid, Kolijn, P. Martijn, Bredius, Robbert G. M., van Doorn, Remco, Langerak, Anton W., Schilham, Marco W., and Lankester, Arjan C.

Subjects

*HEMATOPOIETIC stem cell transplantation, *KILLER cells, *T cells, *BLOOD cells, *STEM cells

Abstract

The first successful European hematopoietic stem cell transplantation (HSCT) was performed in 1968 as treatment in a newborn with IL2RG deficiency using an HLA-identical sibling donor. Because of declining naive T and natural killer (NK) cells, and persistent human papilloma virus (HPV)-induced warts, the patient received a peripheral stem cell boost at the age of 37 years. NK and T cells were assessed before and up to 14 years after the boost by flow cytometry. The boost induced renewed reconstitution of functional NK cells that were 14 years later enriched for CD56dimCD27+ NK cells. T-cell phenotype and T-cell receptor (TCR) repertoire were simultaneously analyzed by including TCR Vβ antibodies in the cytometry panel. Naive T-cell numbers with a diverse TCR Vβ repertoire were increased by the boost. Before and after the boost, clonal expansions with a homogeneous TIGIT and PD-1 phenotype were identified in the CD27− and/or CD28− memory population in the patient, but not in the donor. TRB sequencing was applied on sorted T-cell subsets from blood and on T cells from skin biopsies. Abundant circulating CD8 memory clonotypes with a chronic virus-associated CD57+KLRG1+CX3CR1+ phenotype were also present in warts, but not in healthy skin of the patient, suggesting a link with HPV. In conclusion, we demonstrate in this IL2RG-deficient patient functional NK cells, a diverse and lasting naive T-cell compartment, supported by a stem cell boost, and an oligoclonal memory compartment half a century after HSCT. [ABSTRACT FROM AUTHOR]

Published

2022

8. Newborn Screening in the Diagnosis of Primary Immunodeficiency.

Author

Kobrynski, Lisa J.

Abstract

Newborn screening for severe combined immune deficiency (SCID) is the first inborn error of immunity (IEI) to be detected through population screening. It also represents the first newborn screening test to utilize molecular testing on DNA from newborn dried blood spots. Newborn screening for SCID has provided opportunities to measure the population prevalence of this disorder and evaluate the effect of early interventions on the overall outcomes in affected infants. The success of SCID newborn screening has increased interest in developing and implementing molecular testing for other clinically significant inborn errors of immunity. This methodology has been adapted to screen for another monogenic inborn defect, spinal muscle atrophy. Advances in the clinical care and new therapeutics for many inborn errors of immunity support the need for early diagnosis and prompt institution of therapies to reduce morbidity and mortality. Early diagnosis may also improve the quality of life for affected patients. This article provides an overview of newborn screening for SCID, recommended steps for follow-up testing and early intervention as well as long-term follow-up. Numerous challenges remain, including the development of clinical consensus regarding confirmatory and diagnostic testing, early interventions, and best practices for immune reconstitution in affected infants. [ABSTRACT FROM AUTHOR]

Published

2022

9. Case Report: Preimplantation Genetic Testing for X-Linked Severe Combined Immune Deficiency Caused by IL2RG Gene Variant.

Author

Ren, Jun, Peng, Cuiting, Zhou, Fan, Li, Yutong, Keqie, Yuezhi, Chen, Han, Zhu, Hongmei, Chen, Xinlian, and Liu, Shanling

Subjects

GENETIC testing, GENETIC variation, IMMUNODEFICIENCY, KILLER cells, FETUS, SINGLE nucleotide polymorphisms, BLOOD coagulation factor XIII, AMNIOTIC liquid

Abstract

Preimplantation genetic testing (PGT) has been increasingly used to prevent rare inherited diseases. In this study, we report a case where PGT was used to prevent the transmission of disease-caused variant in a SCID-X1 (OMIM:300400) family. SCID-X1 is an X-linked recessive inherited disease whose major clinical manifestation of immune deficiency is the significant reduction in the number of T-cells and natural killer cells. This family gave birth to a boy who was a hemizygous proband whose IL2RG gene was mutated (c.315T > A, p(Tyr105*), NM_000206.3, CM962677). In this case, Sanger sequencing for mutated allele and linkage analysis based on single-nucleotide polymorphism (SNP) haplotype via next-generation sequencing were performed simultaneously. After PGT for monogenic disorder, we detected the aneuploidy and copy number variation (CNV) for normal and female carrier embryos. Four embryos (E02, E09, E10, and E11) were confirmed without CNVs and inherited variants at the IL2RG gene. Embryo E02 (ranking 4BB) has been transferred after considering the embryo growth rate, morphology, and PGT results. Prenatal genetic diagnosis was used to detect amniotic fluid cells, showing that this fetus did not carry the variant of the IL2RG gene (c.315T > A). Ultimately, a healthy girl who had not carried disease-causing variants of SCID-X1 confirmed by prenatal diagnosis was born, further verifying our successful application of PGT in preventing mutated allele transmission for this SCID family. [ABSTRACT FROM AUTHOR]

Published

2022

10. Recommendations for Screening and Management of Late Effects in Patients with Severe Combined Immunodeficiency after Allogenic Hematopoietic Cell Transplantation: A Consensus Statement from the Second Pediatric Blood and Marrow Transplant Consortium International Conference on Late Effects after Pediatric HCT.

Author

Heimall, Jennifer, Buckley, Rebecca H, Puck, Jennifer, Fleisher, Thomas A, Gennery, Andrew R, Haddad, Elie, Neven, Benedicte, Slatter, Mary, Roderick, Skinner, Baker, K Scott, Dietz, Andrew C, Duncan, Christine, Griffith, Linda M, Notarangelo, Luigi, Pulsipher, Michael A, and Cowan, Morton J

Subjects

Humans, Severe Combined Immunodeficiency, Hematopoietic Stem Cell Transplantation, Consensus, Adolescent, Adult, Child, Child, Preschool, Infant, Infant, Newborn, Female, Male, Practice Guidelines as Topic, Allografts, Bone marrow transplantation, Long-term follow-up guidelines, Severe combined immune deficiency, Pediatric, Cancer, Rare Diseases, Transplantation, Pediatric Research Initiative, Regenerative Medicine, Hematology, Clinical Sciences, Immunology

Abstract

Severe combined immunodeficiency (SCID) is effectively treated with hematopoietic cell transplantation (HCT), with overall survival approaching 90% in contemporary reports. However, survivors are at risk for developing late complications because of the variable durability of high-quality immune function, underlying genotype of SCID, comorbidities due to infections in the pretransplantation and post-transplantation periods, and use of conditioning before transplantation. An international group of transplantation experts was convened in 2016 to review the current knowledge of late effects seen in SCID patients after HCT and to develop recommendations for screening and monitoring for late effects. This report provides recommendations for screening and management of pediatric and adult SCID patients treated with HCT.

Published

2017

11. Case Report: Preimplantation Genetic Testing for X-Linked Severe Combined Immune Deficiency Caused by IL2RG Gene Variant

Author

Jun Ren, Cuiting Peng, Fan Zhou, Yutong Li, Yuezhi Keqie, Han Chen, Hongmei Zhu, Xinlian Chen, and Shanling Liu

Subjects

preimplantation genetic testing, severe combined immune deficiency, IR2RG, haplotype, rare genetic disease, next generation sequencing, Genetics, QH426-470

Abstract

Preimplantation genetic testing (PGT) has been increasingly used to prevent rare inherited diseases. In this study, we report a case where PGT was used to prevent the transmission of disease-caused variant in a SCID-X1 (OMIM:300400) family. SCID-X1 is an X-linked recessive inherited disease whose major clinical manifestation of immune deficiency is the significant reduction in the number of T-cells and natural killer cells. This family gave birth to a boy who was a hemizygous proband whose IL2RG gene was mutated (c.315T > A, p(Tyr105*), NM_000206.3, CM962677). In this case, Sanger sequencing for mutated allele and linkage analysis based on single-nucleotide polymorphism (SNP) haplotype via next-generation sequencing were performed simultaneously. After PGT for monogenic disorder, we detected the aneuploidy and copy number variation (CNV) for normal and female carrier embryos. Four embryos (E02, E09, E10, and E11) were confirmed without CNVs and inherited variants at the IL2RG gene. Embryo E02 (ranking 4BB) has been transferred after considering the embryo growth rate, morphology, and PGT results. Prenatal genetic diagnosis was used to detect amniotic fluid cells, showing that this fetus did not carry the variant of the IL2RG gene (c.315T > A). Ultimately, a healthy girl who had not carried disease-causing variants of SCID-X1 confirmed by prenatal diagnosis was born, further verifying our successful application of PGT in preventing mutated allele transmission for this SCID family.

Published

2022

12. DiGeorge Syndrome: Simultaneously Diagnosis of A Mother-Baby Pair With Great Clinical Variability.

Author

Dokuzboy, Refika Sirma, Sarı, Fatma Nur, Beşer, Esra, Ayvaz, Deniz Çağdaş, and Dizdar, Evrim Alyamaç

Subjects

*DIGEORGE syndrome, *22Q11 deletion syndrome, *FLUORESCENCE in situ hybridization, *MOTHER-infant relationship, *SKELETAL abnormalities, *CRANIOFACIAL abnormalities

Abstract

We report a female infant with complete DiGeorge syndrome who has craniofacial and skeletal abnormalities, feeding problems, cardiac defect, hypocalcemia induced seizure, thymic aplasia, and severe combined immune deficiency. Her mother also had a partial type of disease and was diagnosed at the same time with her baby. FISH analysis of both mother and the infant revealed a deletion in 22q11.2. This family's findings indicate that 22q11 deletion syndrome is a genetic condition with wide interfamilial and intrafamilial variability in clinical expression. [ABSTRACT FROM AUTHOR]

Published

2022

13. Hematopoietic stem cell transplantation complicated with EBV associated hemophagocytic lymphohistiocytosis in a patient with DOCK2 deficiency.

Author

Aytekin, Elif Soyak, Çağdaş, Deniz, Tan, Çağman, Çavdarlı, Büşranur, Bilgiç, Işıl, and Tezcan, İlhan

Abstract

Background. Dedicator of cytokinesis 2 (DOCK2) deficiency is a rare autosomal recessive combined immunodeficiency presenting with very early onset, severe bacterial and viral infections. In DOCK2 deficiency; T, B and NK cell numbers are decreased and functions are impaired resulting in severe atrophy of secondary lymphoid tissues. The aim of this report is to provide information on clinical and laboratory features and hematopoietic stem cell transplantation (HSCT) outcomes of a DOCK2 deficient patient. The patient was diagnosed by using a targeted next generation sequencing primary immunodeficiency (PID) panel. Lymphocyte subsets were measured by flow-cytometry. Case. Here, we describe a patient with DOCK2 deficiency presented with severe combined immunodeficiency. He underwent HSCT without conditioning regimen before the genetic diagnosis and developed hemophagocytic lymphohistiocytosis(HLH) due to Epstein-Barr virus (EBV) infection. Conclusions. Genetic testing is necessery for early diagnosis of DOCK2 deficiency. The curative treatment should be HSCT soon after diagnosis. [ABSTRACT FROM AUTHOR]

Published

2021

14. 82 Newborn Screening for Severe Combined Immune Deficiency: The Canadian Landscape.

Author

Mudilage, Mithili, Kalashnikova, Tatiana, Muranyi, Andrew, Biggs, Catherine, Sinclair, Graham, Suresh, Sneha, Martin, Georgina, Antonishyn, Nick, Rubin, Tamar, Evans, Cherie, Kim, Vy, Kernohan, Kristin, Derfalvi, Beata, Wright, Nicola, and Pham-Huy, Anne

Subjects

*NEWBORN screening, *IMMUNODEFICIENCY, *T cell receptors

Published

2024

15. A systematic analysis of recombination activity and genotype-phenotype correlation in human recombination-activating gene 1 deficiency

Author

Lee, Yu Nee, Frugoni, Francesco, Dobbs, Kerry, Walter, Jolan E, Giliani, Silvia, Gennery, Andrew R, Al-Herz, Waleed, Haddad, Elie, LeDeist, Francoise, Bleesing, Jack H, Henderson, Lauren A, Pai, Sung-Yun, Nelson, Robert P, El-Ghoneimy, Dalia H, El-Feky, Reem A, Reda, Shereen M, Hossny, Elham, Soler-Palacin, Pere, Fuleihan, Ramsay L, Patel, Niraj C, Massaad, Michel J, Geha, Raif S, Puck, Jennifer M, Palma, Paolo, Cancrini, Caterina, Chen, Karin, Vihinen, Mauno, Alt, Frederick W, and Notarangelo, Luigi D

Subjects

Biomedical and Clinical Sciences, Immunology, Genetics, Rare Diseases, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Alleles, B-Lymphocytes, Child, Child, Preschool, Gene Order, Gene Rearrangement, Genetic Association Studies, Homeodomain Proteins, Humans, Immunoglobulin Heavy Chains, Infant, Infant, Newborn, Mutation, Phenotype, Severe Combined Immunodeficiency, T-Lymphocytes, V(D)J Recombination, Recombination-activating gene 1, V(D)J recombination, severe combined immune deficiency, Omenn syndrome, autoimmunity, genotype-phenotype correlation, immune repertoire, Allergy

Abstract

BackgroundThe recombination-activating gene (RAG) 1/2 proteins play a critical role in the development of T and B cells by initiating the VDJ recombination process that leads to generation of a broad T-cell receptor (TCR) and B-cell receptor repertoire. Pathogenic mutations in the RAG1/2 genes result in various forms of primary immunodeficiency, ranging from T(-)B(-) severe combined immune deficiency to delayed-onset disease with granuloma formation, autoimmunity, or both. It is not clear what contributes to such heterogeneity of phenotypes.ObjectiveWe sought to investigate the molecular basis for phenotypic diversity presented in patients with various RAG1 mutations.MethodsWe have developed a flow cytometry-based assay that allows analysis of RAG recombination activity based on green fluorescent protein expression and have assessed the induction of the Ighc locus rearrangements in mouse Rag1(-/-) pro-B cells reconstituted with wild-type or mutant human RAG1 (hRAG1) using deep sequencing technology.ResultsHere we demonstrate correlation between defective recombination activity of hRAG1 mutant proteins and severity of the clinical and immunologic phenotype and provide insights on the molecular mechanisms accounting for such phenotypic diversity.ConclusionsUsing a sensitive assay to measure the RAG1 activity level of 79 mutations in a physiologic setting, we demonstrate correlation between recombination activity of RAG1 mutants and the severity of clinical presentation and show that RAG1 mutants can induce specific abnormalities of the VDJ recombination process.

Published

2014

16. Clinical, Immunological, and Molecular Features of Severe Combined Immune Deficiency: A Multi-Institutional Experience From India

Author

Pandiarajan Vignesh, Amit Rawat, Rajni Kumrah, Ankita Singh, Anjani Gummadi, Madhubala Sharma, Anit Kaur, Johnson Nameirakpam, Ankur Jindal, Deepti Suri, Anju Gupta, Alka Khadwal, Biman Saikia, Ranjana Walker Minz, Kaushal Sharma, Mukesh Desai, Prasad Taur, Vijaya Gowri, Ambreen Pandrowala, Aparna Dalvi, Neha Jodhawat, Priyanka Kambli, Manisha Rajan Madkaikar, Sagar Bhattad, Stalin Ramprakash, Raghuram CP, Ananthvikas Jayaram, Meena Sivasankaran, Deenadayalan Munirathnam, Sarath Balaji, Aruna Rajendran, Amita Aggarwal, Komal Singh, Fouzia Na, Biju George, Ankit Mehta, Harsha Prasada Lashkari, Ramya Uppuluri, Revathi Raj, Sandip Bartakke, Kirti Gupta, Sreejesh Sreedharanunni, Yumi Ogura, Tamaki Kato, Kohsuke Imai, Koon Wing Chan, Daniel Leung, Osamu Ohara, Shigeaki Nonoyama, Michael Hershfield, Yu-Lung Lau, and Surjit Singh

Subjects

severe combined immune deficiency, India, hematopoietic stem cell transplantation, newborn screening, BCG, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundSevere Combined Immune Deficiency (SCID) is an inherited defect in lymphocyte development and function that results in life-threatening opportunistic infections in early infancy. Data on SCID from developing countries are scarce.ObjectiveTo describe clinical and laboratory features of SCID diagnosed at immunology centers across India.MethodsA detailed case proforma in an Excel format was prepared by one of the authors (PV) and was sent to centers in India that care for patients with primary immunodeficiency diseases. We collated clinical, laboratory, and molecular details of patients with clinical profile suggestive of SCID and their outcomes. Twelve (12) centers provided necessary details which were then compiled and analyzed. Diagnosis of SCID/combined immune deficiency (CID) was based on 2018 European Society for Immunodeficiencies working definition for SCID.ResultsWe obtained data on 277 children; 254 were categorized as SCID and 23 as CID. Male-female ratio was 196:81. Median (inter-quartile range) age of onset of clinical symptoms and diagnosis was 2.5 months (1, 5) and 5 months (3.5, 8), respectively. Molecular diagnosis was obtained in 162 patients - IL2RG (36), RAG1 (26), ADA (19), RAG2 (17), JAK3 (15), DCLRE1C (13), IL7RA (9), PNP (3), RFXAP (3), CIITA (2), RFXANK (2), NHEJ1 (2), CD3E (2), CD3D (2), RFX5 (2), ZAP70 (2), STK4 (1), CORO1A (1), STIM1 (1), PRKDC (1), AK2 (1), DOCK2 (1), and SP100 (1). Only 23 children (8.3%) received hematopoietic stem cell transplantation (HSCT). Of these, 11 are doing well post-HSCT. Mortality was recorded in 210 children (75.8%).ConclusionWe document an exponential rise in number of cases diagnosed to have SCID over the last 10 years, probably as a result of increasing awareness and improvement in diagnostic facilities at various centers in India. We suspect that these numbers are just the tip of the iceberg. Majority of patients with SCID in India are probably not being recognized and diagnosed at present. Newborn screening for SCID is the need of the hour. Easy access to pediatric HSCT services would ensure that these patients are offered HSCT at an early age.

Published

2021

17. Clinical, Immunological, and Molecular Features of Severe Combined Immune Deficiency: A Multi-Institutional Experience From India.

Author

Vignesh, Pandiarajan, Rawat, Amit, Kumrah, Rajni, Singh, Ankita, Gummadi, Anjani, Sharma, Madhubala, Kaur, Anit, Nameirakpam, Johnson, Jindal, Ankur, Suri, Deepti, Gupta, Anju, Khadwal, Alka, Saikia, Biman, Minz, Ranjana Walker, Sharma, Kaushal, Desai, Mukesh, Taur, Prasad, Gowri, Vijaya, Pandrowala, Ambreen, and Dalvi, Aparna

Subjects

IMMUNODEFICIENCY, HEMATOPOIETIC stem cell transplantation, DIAGNOSIS, NEWBORN screening, SYMPTOMS

Abstract

Background: Severe Combined Immune Deficiency (SCID) is an inherited defect in lymphocyte development and function that results in life-threatening opportunistic infections in early infancy. Data on SCID from developing countries are scarce. Objective: To describe clinical and laboratory features of SCID diagnosed at immunology centers across India. Methods: A detailed case proforma in an Excel format was prepared by one of the authors (PV) and was sent to centers in India that care for patients with primary immunodeficiency diseases. We collated clinical, laboratory, and molecular details of patients with clinical profile suggestive of SCID and their outcomes. Twelve (12) centers provided necessary details which were then compiled and analyzed. Diagnosis of SCID/combined immune deficiency (CID) was based on 2018 European Society for Immunodeficiencies working definition for SCID. Results: We obtained data on 277 children; 254 were categorized as SCID and 23 as CID. Male-female ratio was 196:81. Median (inter-quartile range) age of onset of clinical symptoms and diagnosis was 2.5 months (1, 5) and 5 months (3.5, 8), respectively. Molecular diagnosis was obtained in 162 patients - IL2RG (36), RAG1 (26), ADA (19), RAG2 (17), JAK3 (15), DCLRE1C (13), IL7RA (9), PNP (3), RFXAP (3), CIITA (2), RFXANK (2), NHEJ1 (2), CD3E (2), CD3D (2), RFX5 (2), ZAP70 (2), STK4 (1), CORO1A (1), STIM1 (1), PRKDC (1), AK2 (1), DOCK2 (1), and SP100 (1). Only 23 children (8.3%) received hematopoietic stem cell transplantation (HSCT). Of these, 11 are doing well post-HSCT. Mortality was recorded in 210 children (75.8%). Conclusion: We document an exponential rise in number of cases diagnosed to have SCID over the last 10 years, probably as a result of increasing awareness and improvement in diagnostic facilities at various centers in India. We suspect that these numbers are just the tip of the iceberg. Majority of patients with SCID in India are probably not being recognized and diagnosed at present. Newborn screening for SCID is the need of the hour. Easy access to pediatric HSCT services would ensure that these patients are offered HSCT at an early age. [ABSTRACT FROM AUTHOR]

Published

2021

18. Неонатален скрининг за първични имунни дефицити - предимства и обхват

Author

Маринова, М., Георгиева, А., Йорданова, В., Наумова, Е., and Кандиларова, С.

Abstract

Severe combined immune deficiency (SCID) is characterized by defects in the maturation and development of T lymphocytes. Infants with SCID are at risk of serious infections, failure to thrive and fatal outcome during the first 2 years of life. Early diagnosis of PID is crucial for the survival of affected patients as it makes possible timely therapeutic interventions. The method for detecting SCID routinely during the neonatal period is based on the quantification of T-cell receptor excision circles (TREC) in dry blood spot samples of newborns. TRECs are circular DNA molecules formed by rearrangement of T cell receptor genes during the normal process of T cell maturation in the thymus. SCID screening is routinely performed in mass neonatal screening programs in the USA, Israel and many European countries, and many countries worldwide are in process of implementation of SCID screening in their health programs. In Bulgaria is currently running a pilot study in order to obtain preliminary results which will help to approve and adapt the technology for Bulgaria’s conditions, and to evaluate the potential public benefits of starting a routine screening program for all Bulgarian newborns. [ABSTRACT FROM AUTHOR]

Published

2020

19. Neonatal Screening for Severe Combined Immune Deficiency in Russia: Glorious Future or Tomorrow’s Reality?

Author

Svetlana S. Deryabina, Irina A. Tuzankina, Elena V. Vlasova, Mikhail A. Bolkov, and Viktor N. Shershnev

Subjects

severe combined immune deficiency, primary immunodeficiency, neonatal screening, trec, krec, Pediatrics, RJ1-570

Abstract

Mass screening of newborns in Russia for five hereditary diseases does not meet the requirements of the world community for the neonatal screening program. Success in the development of laboratory diagnostic technologies and active introduction of achievements in genetics and molecular biology into medical practice allow for the revision of the list of nosologies included in the national neonatal screening program by replacing the disease or adding new nosologies. The article discusses the possibility of including genetic testing for severe combined immune deficiency in the Newborn Screening Program in Russia. The results from a retrospective study of markers of naive T- and B-lymphocytes (TREC and KREC) in the group of children with immuno-dependent pathology developed in the first year of life are discussed.

Published

2017

20. Survey of Infection Control Precautions for Patients with Severe Combined Immune Deficiency.

Author

Dergousoff, Brieanne A., Vayalumkal, Joseph V., and Wright, Nicola A. M.

Subjects

*INFECTION prevention, *IMMUNODEFICIENCY, *CHILD care costs, *PROTECTIVE clothing, *T cells

Abstract

Severe combined immune deficiency (SCID) is caused by an array of genetic disorders resulting in a diminished adaptive immune system due to impaired T lymphocytes. In these patients, active infection at the time of hematopoietic transplantation has been shown to increase morbidity and mortality. To prevent transmission of infections in SCID patients, standardized infection control precautions should be implemented. An online survey regarding SCID-specific protocols was distributed through several immunodeficiency organizations. Seventy-three responses were obtained, with the majority (55%) of responses from the USA, 15% from Canada, and the remainder from 12 other countries. Only 50% of respondents had a SCID-specific infection control protocol at their center, and while a majority of these centers had training for physicians, a small minority had training for other healthcare workers such as nursing and housekeeping staff. Significant variability of infection control practices, such as in-patient precautions, required personal protective equipment (PPE), diet restrictions, visitor precautions and discharge criteria, was found between different treatment centers. There is a paucity of evidence-based data regarding the safest environment to prevent infection in SCID patients. Institutional protocols may have significant impact on infection risk, survival, family well-being, child development and cost of care. From these results, it is evident that further multi-center research is required to determine the safest and healthiest environment for these children, so that evidence-based infection control protocols for patients with SCID can be developed. [ABSTRACT FROM AUTHOR]

Published

2019

21. Primary Immunodeficiency Disorders Among North Indian Children.

Author

Gupta, Devika, Thakral, Deepshi, Kumar, Prabin, Kabra, Sushil K., Lodha, Rakesh, Kumari, Rinkee, Mohanty, Supreet K., Chakraborty, Sushmita, Bagri, Narendra, and Mitra, Dipendra K.

Abstract

Objectives: To report the distribution pattern of various categories of primary immunodeficiency disorders (PIDs) in children from North India, frequency of warning signs and critical parameters for evaluation.Methods: In this retrospective study, 528 children below 18 y of age after clinical assessment and presentation suggestive of PID were further screened by immunophenotyping for immune cell markers by flow cytometry.Results: A total of 120 (23%) children were diagnosed with PID with median age at diagnosis being 2.5 y in males and 3.5 y in females and an average delay in diagnosis from onset of symptoms being approximately 5 y. Chronic lower respiratory tract infections, gastrointestinal symptoms like persistent diarrhea and failure to thrive were amongst the most common warning signs in these patients. PIDs were classified according to the International Union of Immunological Societies' (IUIS) criteria. The diagnosis of index study subjects included combined humoral and cellular immunodeficiency (29%), phagocytic defects (29%), followed by predominantly antibody deficiency (18%), innate immunity and dysregulation (17%) and other well-defined syndromes (7%). A family history of PID (23%), consanguineous marriage (8%) and previous sibling death (23%) were observed as major clinical predictors/clues for underlying PID. All children received prophylactic antibiotics and/or antifungals in addition to specific therapy for underlying immune deficiency.Conclusions: The field of PIDs in India remains largely unexplored and we are faced with various challenges in the diagnosis of PIDs due to lack of awareness as well as absence of equipped immunological laboratory support. The authors propose a methodical step-wise laboratory diagnostic approach that can facilitate early diagnosis and timely intervention of these mis/underdiagnosed disorders. [ABSTRACT FROM AUTHOR]

Published

2019

22. Severe Combined Immune Deficiency

Author

Chen, Harold, editor

Published

2012

23. T and NK cells in IL2RG-deficient patient 50 years after hematopoietic stem cell transplantation

Author

Janine E. Melsen, Monique M. van Ostaijen-ten Dam, Erik B. van den Akker, Marij J. P. Welters, Kim C. Heezen, Ingrid Pico-Knijnenburg, P. Martijn Kolijn, Robbert G. M. Bredius, Remco van Doorn, Anton W. Langerak, Marco W. Schilham, Arjan C. Lankester, and Immunology

Subjects

Adult, T-cell receptor repertoire, natural killer cells, Immunology, Papillomavirus Infections, Programmed Cell Death 1 Receptor, Infant, Newborn, Receptors, Antigen, T-Cell, T cells, Severe combined immune deficiency, Killer Cells, Natural, CD28 Antigens, SDG 3 - Good Health and Well-being, hematopoietic stem cell transplantation, Immunology and Allergy, Humans, Receptors, Immunologic, Warts, Interleukin Receptor Common gamma Subunit

Abstract

The first successful European hematopoietic stem cell transplantation (HSCT) was performed in 1968 as treatment in a newborn with IL2RG deficiency using an HLA-identical sibling donor. Because of declining naive T and natural killer (NK) cells, and persistent human papilloma virus (HPV)-induced warts, the patient received a peripheral stem cell boost at the age of 37 years. NK and T cells were assessed before and up to 14 years after the boost by flow cytometry. The boost induced renewed reconstitution of functional NK cells that were 14 years later enriched for CD56dimCD27+ NK cells. T-cell phenotype and T-cell receptor (TCR) repertoire were simultaneously analyzed by including TCR Vβ antibodies in the cytometry panel. Naive T-cell numbers with a diverse TCR Vβ repertoire were increased by the boost. Before and after the boost, clonal expansions with a homogeneous TIGIT and PD-1 phenotype were identified in the CD27− and/or CD28− memory population in the patient, but not in the donor. TRB sequencing was applied on sorted T-cell subsets from blood and on T cells from skin biopsies. Abundant circulating CD8 memory clonotypes with a chronic virus-associated CD57+KLRG1+CX3CR1+ phenotype were also present in warts, but not in healthy skin of the patient, suggesting a link with HPV. In conclusion, we demonstrate in this IL2RG-deficient patient functional NK cells, a diverse and lasting naive T-cell compartment, supported by a stem cell boost, and an oligoclonal memory compartment half a century after HSCT.

Published

2022

24. How We Manage Adenosine Deaminase-Deficient Severe Combined Immune Deficiency (ADA SCID).

Author

Kohn, Donald and Gaspar, H.

Subjects

*IMMUNODEFICIENCY, *ADENOSINE deaminase, *PATIENTS, *IMMUNITY, *DEAMINASES

Abstract

Adenosine deaminase-deficient severe combined immune deficiency (ADA SCID) accounts for 10-15% of cases of human SCID. From what was once a uniformly fatal disease, the prognosis for infants with ADA SCID has improved greatly based on the development of multiple therapeutic options, coupled with more frequent early diagnosis due to implementation of newborn screening for SCID. We review the various treatment approaches for ADA SCID including allogeneic hematopoietic stem cell transplantation (HSCT) from a human leukocyte antigen-matched sibling or family member or from a matched unrelated donor or a haplo-identical donor, autologous HSCT with gene correction of the hematopoietic stem cells (gene therapy-GT), and enzyme replacement therapy (ERT) with polyethylene glycol-conjugated adenosine deaminase. Based on growing evidence of safety and efficacy from GT, we propose a treatment algorithm for patients with ADA SCID that recommends HSCT from a matched family donor, when available, as a first choice, followed by GT as the next option, with allogeneic HSCT from an unrelated or haplo-identical donor or long-term ERT as other options. [ABSTRACT FROM AUTHOR]

Published

2017

25. Management of ADA-Deficient SCID Patient on Adagen During Pregnancy.

Author

Shams, Marissa and Kobrynski, Lisa

Subjects

*SEVERE combined immunodeficiency, *PREGNANCY, *BLOOD cell count

Abstract

We describe the management of a patient with ADA-deficient Severe Combined Immune Deficiency maintained on PEG-ADA treatment throughout her pregnancy. ADA-deficient SCID (ADA-SCID) is rare but accounts for approximately 15% of all SCID cases. As a result of improved outcomes with definitive treatment such as hematopoietic cell transplant (HCT) and now gene therapy, few patients remain on long-term therapy with weekly PEG-ADA enzyme replacement alone. Knowledge detailing the management of ADA-SCID patients on PEG-ADA replacement during pregnancy is valuable to clinical immunologists. [Extracted from the article]

Published

2019

26. Dynamics of the Artemis and DNA-PKcs Complex in the Repair of Double-Strand Breaks.

Author

Watanabe, Go and Lieber, Michael R.

Subjects

*PROTEIN kinases, *CATALYTIC domains, *METALLOENZYMES, *CELL cycle, *NUCLEASES

Abstract

[Display omitted] • Newly solved structures reveal unique protein dynamics for a nuclease and its regulatory protein kinase. • The structures provide insight relevant to metalloenzymes and structure-specific nucleases. The findings are relevant to normal immune function and inherited immunodeficiencies. Pathologic chromosome breaks occur in human dividing cells ∼10 times per day, and physiologic breaks occur in each lymphoid cell many additional times per day. Nonhomologous DNA end joining (NHEJ) is the major pathway for the repair of all of these double-strand breaks (DSBs) during most of the cell cycle. Nearly all broken DNA ends require trimming before they can be suitable for joining by ligation. Artemis is the major nuclease for this purpose. Artemis is tightly regulated by one of the largest protein kinases, which tethers Artemis to its surface. This kinase is called DNA-dependent protein kinase catalytic subunit (or DNA-PKcs) because it is only active when it encounters a broken DNA end. With this activation, DNA-PKcs permits the Artemis catalytic domain to enter a large cavity in the center of DNA-PKcs. Given this remarkably tight supervision of Artemis by DNA-PKcs, it is an appropriate time to ask what we know about the Artemis:DNA-PKcs complex, as we integrate recent structural information with the biochemistry of the complex and how this relates to other NHEJ proteins and to V(D)J recombination in the immune system. [ABSTRACT FROM AUTHOR]

Published

2022

27. Combating oncogene activation associated with retrovirus-mediated gene therapy of X-linked severe combined immunodeficiency

Author

B.E. Strauss and E. Costanzi-Strauss

Subjects

Retrovirus, Insertional mutagenesis, Severe combined immune deficiency, Gene therapy, Adverse event, Clinical trial, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

A successful gene therapy clinical trial that also encountered serious adverse effects has sparked extensive study and debate about the future directions for retrovirus-mediated interventions. Treatment of X-linked severe combined immunodeficiency with an oncoretrovirus harboring a normal copy of the gc gene was applied in two clinical trials, essentially curing 13 of 16 infants, restoring a normal immune system without the need for additional immune-related therapies. Approximately 3 years after their gene therapy, tragically, 3 of these children, all from the same trial, developed leukemia as a result of this experimental treatment. The current understanding of the mechanism behind this leukemogenesis involves three critical and cooperating factors, i.e., viral integration, oncogene activation, and the function of the therapeutic gene. In this review, we will explore the causes of this unwanted event and some of the possibilities for reducing the risk of its reoccurrence.

Published

2007

28. A New IL-2RG Gene Mutation in an X-linked SCID Identified through TREC/KREC Screening: a Case Report

Author

Maryam Nourizadeh, Stephan Borte, MohammadReza Fazlollahi, Lennart Hammarström, and Zahra Pourpak

Subjects

Interleukin-2 Receptor gamma Chain, Severe Combined Immune Deficiency, T-cell receptor excision circles, kappa-deleting recombination excision circles, Medicine

Abstract

Severe combined immunodeficiency (SCID) represents a rare group of primary immunodeficiency disorders (PIDs), with known or unknown genetic alterations. Here, we report a new interleukin 2 receptor, gamma chain (IL-2RG) mutation in an Iranian SCID newborn.The patient was a 6-day old boy with a family history of PID. The child was screened using a molecular-based analysis for the assessment of T cell receptor excision circles (TRECs) and kappa-deleting recombination excision circles (KRECs). Moreover, a complete immunological evaluation and gene sequencing was performed.Results showed undetectable TREC but a high level of KREC copy numbers. Flow cytometric data indicated low numbers of T and NK cells, but elevated number of B cells. A novel substitution in IL2RG: c.675 C>A, leading to p.225 Ser>Arg was found. Based on the functional analysis, the mutation is predicted to be damaging. The patient was diagnosed as a T B+ NK X-linked SCID.

Published

2015

29. Current status of ex vivo gene therapy for hematological disorders: a review of clinical trials in Japan around the world.

Author

Tani, Kenzaburo

Abstract

Gene therapies are classified into two major categories, namely, in vivo and ex vivo. Clinical trials of human gene therapy began with the ex vivo techniques. Based on the initial successes of gene-therapy clinical trials, these approaches have spread worldwide. The number of gene therapy trials approved worldwide increased gradually starting in 1989, reaching 116 protocols per year in 1999, and a total of 2210 protocols had been approved by 2015. Accumulating clinical evidence has demonstrated the safety and benefits of several types of gene therapy, with the exception of serious adverse events in several clinical trials. These painful experiences were translated backward to basic science, resulting in the development of several new technologies that have influenced the recent development of ex vivo gene therapy in this field. To date, six gene therapies have been approved in a limited number of countries worldwide. In Japan, clinical trials of gene therapy have developed under the strong influence of trials in the US and Europe. Since the initial stages, 50 clinical trials have been approved by the Japanese government. In this review, the history and current status of clinical trials of ex vivo gene therapy for hematological disorders are introduced and discussed. [ABSTRACT FROM AUTHOR]

Published

2016

30. Normal IgH repertoire diversity in an infant with ADA deficiency after gene therapy

Author

John W. Sleasman, Carolyn H. Baloh, Maureen M. Goodenow, Kai-Fen Chang, Samiksha A Borkar, Li Yin, Michael S. Hershfield, Jiqiang Yao, Donald B. Kohn, and Suhag Parikh

Subjects

0301 basic medicine, Adenosine Deaminase, Genetic enhancement, Immunology, Somatic hypermutation, Article, 03 medical and health sciences, 0302 clinical medicine, Clinical Research, Agammaglobulinemia, medicine, Genetics, Immunology and Allergy, Humans, Enzyme Replacement Therapy, Lymphocyte Count, B cell, Pediatric, Severe combined immunodeficiency, B cell repertoire, biology, adenosine deaminase deficiency, Infant, Hematology, Gene Therapy, Genetic Therapy, medicine.disease, Severe combined immune deficiency, Stem Cell Research, Adenosine deaminase deficiency, 030104 developmental biology, medicine.anatomical_structure, Good Health and Well Being, Immunoglobulin class switching, immunoglobulin sequencing, biology.protein, Female, Severe Combined Immunodeficiency, Antibody, IGHV@, Immunoglobulin Heavy Chains, 030215 immunology, Biotechnology

Abstract

PURPOSE: Adenosine deaminase (ADA) deficiency causes severe combined immunodeficiency (SCID) through an accumulation of toxic metabolites within lymphocytes. Recently, ADA deficiency has been successfully treated using lentiviral-transduced autologous CD34+ cells carrying the ADA gene. T and B cell function appears to be fully restored but in many patients’ B cell numbers remain low and assessments of the immunoglobulin heavy (IgHV) repertoire following gene therapy are lacking. METHODS: We performed deep sequencing of IgHV repertoire in peripheral blood lymphocytes from a child following lentivirus-based gene therapy for ADA deficiency and compared to the IgHV repertoire in healthy infants and adults. RESULTS: After gene therapy, Ig diversity increased over time as evidenced by V, D, and J gene usage, N-additions, CDR3 length, extent of somatic hypermutation, and Ig class-switching. There was emergence of predominant IgHM, IgHG, and IgHA CDR3 lengths after gene therapy indicating successful oligoclonal expansion in response to antigens. This provides proof of concept for the feasibility and utility of molecular monitoring in following B cell reconstitution following gene therapy for ADA deficiency. CONCLUSION: Based on deep sequencing, gene therapy resulted in an IgHV repertoire with molecular diversity similar to healthy infants.

Published

2021

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

Author

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

Subjects

0301 basic medicine, Oncology, Allergy, Adenosine Deaminase, medicine.medical_treatment, Genetic enhancement, Hematopoietic stem cell transplantation, Regenerative Medicine, 0302 clinical medicine, Adenosine deaminase, lentivirus, Stem Cell Research - Nonembryonic - Human, Agammaglobulinemia, Immunology and Allergy, Pediatric, biology, Hematopoietic Stem Cell Transplantation, Hematology, Enzyme replacement therapy, Adenosine deaminase deficiency, Stem Cell Research - Nonembryonic - Non-Human, Development of treatments and therapeutic interventions, medicine.symptom, medicine.medical_specialty, Consensus, Immunology, Asymptomatic, Lentiviru, Article, 03 medical and health sciences, Gene therapy, Clinical Research, Internal medicine, medicine, Animals, Humans, Enzyme Replacement Therapy, Transplantation, Newborn screening, Severe combined immunodeficiency, 5.2 Cellular and gene therapies, business.industry, Genetic Therapy, Stem Cell Research, Severe combined immune deficiency, medicine.disease, 030104 developmental biology, biology.protein, Severe Combined Immunodeficiency, business, 030215 immunology

Abstract

Inherited defects in adenosine deaminase (ADA) cause a subtype of severe combined immunodeficiency (SCID) known as severe combined immune deficiency caused by adenosine deaminase defects (ADA-SCID). Most affected infants can receive a diagnosis while still asymptomatic by using an SCID newborn screening test, allowing early initiation of therapy. We review the evidence currently available and propose a consensus management strategy. In addition to treatment of the immune deficiency seen in patients with ADA-SCID, patients should be followed for specific noninfectious respiratory, neurological, and biochemical complications associated with ADA deficiency. All patients should initially receive enzyme replacement therapy (ERT), followed by definitive treatment with either of 2 equal first-line options. If an HLA-matched sibling donor or HLA-matched family donor is available, allogeneic hematopoietic stem cell transplantation (HSCT) should be pursued. The excellent safety and efficacy observed in more than 100 patients with ADA-SCID who received gammaretrovirus- or lentivirus-mediated autologous hematopoietic stem cell gene therapy (HSC-GT) since 2000 now positions HSC-GT as an equal alternative. If HLA-matched sibling donor/HLA-matched family donor HSCT or HSC-GT are not available or have failed, ERT can be continued or reinstituted, and HSCT with alternative donors should be considered. The outcomes of novel HSCT, ERT, and HSC-GT strategies should be evaluated prospectively in "real-life" conditions to further inform these management guidelines.

Published

2019

32. A New IL-2RG Gene Mutation in an X-linked SCID Identified through TREC/KREC Screening: a Case Report.

Author

Nourizadeh, Maryam, Borte, Stephan, Fazlollahi, Mohammad Reza, Hammarström, Lennart, Pourpak, Zahra, and Fazlollahi, MohammadReza

Subjects

*INTERLEUKIN-2, *GENETIC mutation, *SEVERE combined immunodeficiency, *T cell receptors, *FLOW cytometry

Abstract

Severe combined immunodeficiency (SCID) represents a rare group of primary immunodeficiency disorders (PIDs), with known or unknown genetic alterations. Here, we report a new interleukin 2 receptor, gamma chain (IL-2RG) mutation in an Iranian SCID newborn. The patient was a 6-day old boy with a family history of PID. The child was screened using a molecular-based analysis for the assessment of T cell receptor excision circles (TRECs) and kappa-deleting recombination excision circles (KRECs). Moreover, a complete immunological evaluation and gene sequencing was performed. Results showed undetectable TREC but a high level of KREC copy numbers. Flow cytometric data indicated low numbers of T and NK cells, but elevated number of B cells. A novel substitution in IL2RG: c.675 C>A, leading to p.225 Ser>Arg was found. Based on the functional analysis, the mutation is predicted to be damaging. The patient was diagnosed as a T B+ NK X-linked SCID. [ABSTRACT FROM AUTHOR]

Published

2015

33. Congenital defects in V(D)J recombination.

Author

de Villartay, Jean-Pierre

Subjects

SEVERE combined immunodeficiency, CONGENITAL disorders, GENE rearrangement, GENETIC recombination, DNA repair, B cells, GENETIC mutation

Abstract

Introduction or background: The V(D)J recombination is a DNA rearrangement process that generates the diversity of T and B lymphocyte immune repertoire. It proceeds through the generation of a DNA double-strand break (DNA-DSB) by the Rag1/2 lymphoid-specific factors, which is repaired by the non-homologous end joining (NHEJ) DNA repair pathway. V(D)J recombination also constitutes a checkpoint in the lymphoid development. Sources of data: V(D)J recombination defect results in severe combined immune deficiency (SCID) with a lack of T and B lymphocytes. Areas of agreement: The V(D)J recombination represents one of the few programmed molecular events leading to DNA-DSBs that strictly relies on NHEJ. Two NHEJ factors, Artemis and XLF/Cernunnos, were identified through the molecular studies of SCID patients. Mutations in PRKDC and DNA Ligase IV genes also result in SCID. Growing points: Studies in mice have demonstrated that XLF/Cernunnos is dispensable for V(D)J recombination in lymphoid cells but not for the repair of genotoxic-induced DNA-DSBs, which raises the question of the implication of Rag1/2 factors in the DNA repair phase of V(D)J recombination. Areas timely for developing research: New factors of NHEJ, such as PAXX, are being identified. Patients with NHEJ deficiency (XRCC4) without immune deficiency were recently reported. We, therefore, may not have yet the complete picture of DNA-DSB repair in the context of V(D)J recombination. [ABSTRACT FROM AUTHOR]

Published

2015

34. Identification of Patients with RAG Mutations Previously Diagnosed with Common Variable Immunodeficiency Disorders.

Author

Buchbinder, David, Baker, Rebecca, Lee, Yu, Ravell, Juan, Zhang, Yu, McElwee, Joshua, Nugent, Diane, Coonrod, Emily, Durtschi, Jacob, Augustine, Nancy, Voelkerding, Karl, Csomos, Krisztian, Rosen, Lindsey, Browne, Sarah, Walter, Jolan, Notarangelo, Luigi, Hill, Harry, and Kumánovics, Attila

Subjects

*RECOMBINATION activating genes, *GENETIC mutation, *IMMUNODEFICIENCY, *BIOMARKERS, *NUCLEOTIDE sequence, *LYMPHOPENIA, *DIAGNOSIS

Abstract

Purpose: Combined immunodeficiency (CID) presents a unique challenge to clinicians. Two patients presented with the prior clinical diagnosis of common variable immunodeficiency (CVID) disorder marked by an early age of presentation, opportunistic infections, and persistent lymphopenia. Due to the presence of atypical clinical features, next generation sequencing was applied documenting RAG deficiency in both patients. Methods: Two different genetic analysis techniques were applied in these patients including whole exome sequencing in one patient and the use of a gene panel designed to target genes known to cause primary immunodeficiency disorders (PIDD) in a second patient. Sanger dideoxy sequencing was used to confirm RAG1 mutations in both patients. Results: Two young adults with a history of recurrent bacterial sinopulmonary infections, viral infections, and autoimmune disease as well as progressive hypogammaglobulinemia, abnormal antibody responses, lymphopenia and a prior diagnosis of CVID disorder were evaluated. Compound heterozygous mutations in RAG1 (1) c256_257delAA, p86VfsX32 and (2) c1835A>G, pH612R were documented in one patient. Compound heterozygous mutations in RAG1 (1) c.1566G>T, p.W522C and (2) c.2689C>T, p. R897X) were documented in a second patient post-mortem following a fatal opportunistic infection. Conclusion: Astute clinical judgment in the evaluation of patients with PIDD is necessary. Atypical clinical findings such as early onset, granulomatous disease, or opportunistic infections should support the consideration of atypical forms of late onset CID secondary to RAG deficiency. Next generation sequencing approaches provide powerful tools in the investigation of these patients and may expedite definitive treatments. [ABSTRACT FROM AUTHOR]

Published

2015

35. The Expanding Spectrum of Human coronin 1A deficiency.

Author

Moshous, Despina and Villartay, Jean-Pierre

Abstract

Since the first discovery of coronin in the amoeba Dictyostelium discoideum, remarkable insights have been gained regarding the structure and function of coronins, highly conserved from yeast to humans. It has been speculated that coronins have evolved from actin-binding molecules in lower eukaryotes to regulators of various cellular processes in mammals. Indeed, coronins are not only involved in cytokinesis, cell motility, and other actin-related processes but they are also implicated in immune homeostasis and calcium-calcineurin signaling. Most strikingly, coronin 1 deficiencies give rise to immune deficiencies in mice and humans that are characterized by severe T lymphocytopenia. Whereas complete absence of coronin 1A is associated with severe combined immunodeficiency in humans, hypomorphic mutations lead to a profound defect in naïve T cells, expansion of oligoclonal memory T cells, and exquisite susceptibility to EBV-associated B cell lymphoproliferation. Recent publications show that coronin 1A also plays a role in natural killer cell cytotoxic function and in neurobehavioral processes. It can be expected that future identification of coronin 1A-deficient patients will further extend the phenotypic spectrum thereby increasing our knowledge of this fascinating molecule. [ABSTRACT FROM AUTHOR]

Published

2014

36. Clinical, Immunological, and Molecular Features of Severe Combined Immune Deficiency: A Multi-Institutional Experience From India

Author

Prasad Taur, Manisha Madkaikar, Kirti Gupta, Madhubala Sharma, Deepti Suri, Johnson Nameirakpam, Anit Kaur, Alka Khadwal, Aparna Dalvi, Sagar Bhattad, Anjani Gummadi, Sreejesh Sreedharanunni, Michael S. Hershfield, Ranjana W. Minz, Sandip Bartakke, Tamaki Kato, Biman Saikia, Deenadayalan Munirathnam, Komal Singh, Harsha Prasada Lashkari, Fouzia Na, Amita Aggarwal, Raghuram Cp, Ramya Uppuluri, Ankit Mehta, Yu-Lung Lau, Ankita Singh, Neha Jodhawat, Surjit Singh, Revathi Raj, Stalin Ramprakash, Mukesh Desai, Yumi Ogura, Koon Wing Chan, Amit Rawat, Kaushal Sharma, Vijaya Gowri, Aruna Rajendran, Ankur Kumar Jindal, Ananthvikas Jayaram, Daniel Leung, Biju George, Rajni Kumrah, Shigeaki Nonoyama, Priyanka Kambli, Sarath Balaji, Kohsuke Imai, Pandiarajan Vignesh, Osamu Ohara, Anju Gupta, Ambreen Pandrowala, and Meena Sivasankaran

Subjects

lcsh:Immunologic diseases. Allergy, Male, 2019-20 coronavirus outbreak, Pediatrics, medicine.medical_specialty, DCLRE1C, medicine.medical_treatment, Immunology, India, Hematopoietic stem cell transplantation, Immune system, medicine, Humans, Immunology and Allergy, BCG, Original Research, Newborn screening, newborn screening, business.industry, Infant, medicine.disease, Early infancy, hematopoietic stem cell transplantation, severe combined immune deficiency, Primary immunodeficiency, Female, Severe Combined Immunodeficiency, Age of onset, lcsh:RC581-607, business

Abstract

BackgroundSevere Combined Immune Deficiency (SCID) is an inherited defect in lymphocyte development and function that results in life-threatening opportunistic infections in early infancy. Data on SCID from developing countries are scarce.ObjectiveTo describe clinical and laboratory features of SCID diagnosed at immunology centers across India.MethodsA detailed case proforma in an Excel format was prepared by one of the authors (PV) and was sent to centers in India that care for patients with primary immunodeficiency diseases. We collated clinical, laboratory, and molecular details of patients with clinical profile suggestive of SCID and their outcomes. Twelve (12) centers provided necessary details which were then compiled and analyzed. Diagnosis of SCID/combined immune deficiency (CID) was based on 2018 European Society for Immunodeficiencies working definition for SCID.ResultsWe obtained data on 277 children; 254 were categorized as SCID and 23 as CID. Male-female ratio was 196:81. Median (inter-quartile range) age of onset of clinical symptoms and diagnosis was 2.5 months (1, 5) and 5 months (3.5, 8), respectively. Molecular diagnosis was obtained in 162 patients - IL2RG (36), RAG1 (26), ADA (19), RAG2 (17), JAK3 (15), DCLRE1C (13), IL7RA (9), PNP (3), RFXAP (3), CIITA (2), RFXANK (2), NHEJ1 (2), CD3E (2), CD3D (2), RFX5 (2), ZAP70 (2), STK4 (1), CORO1A (1), STIM1 (1), PRKDC (1), AK2 (1), DOCK2 (1), and SP100 (1). Only 23 children (8.3%) received hematopoietic stem cell transplantation (HSCT). Of these, 11 are doing well post-HSCT. Mortality was recorded in 210 children (75.8%).ConclusionWe document an exponential rise in number of cases diagnosed to have SCID over the last 10 years, probably as a result of increasing awareness and improvement in diagnostic facilities at various centers in India. We suspect that these numbers are just the tip of the iceberg. Majority of patients with SCID in India are probably not being recognized and diagnosed at present. Newborn screening for SCID is the need of the hour. Easy access to pediatric HSCT services would ensure that these patients are offered HSCT at an early age.

Published

2021

37. RAG1 Reversion Mosaicism in a Patient with Omenn Syndrome.

Author

Crestani, Elena, Choo, Sharon, Frugoni, Francesco, Lee, Yu, Richards, Stephanie, Smart, Joanne, and Notarangelo, Luigi

Subjects

*RECOMBINATION activating genes, *SEVERE combined immunodeficiency, *MOSAICISM, *CONSANGUINITY, *GENETIC mutation, *HETEROZYGOSITY, *JUVENILE diseases

Abstract

Purpose: To identify mechanisms of disease in a child born to consanguineous parents, who presented with Omenn syndrome (OS) and was found to carry a heterozygous RAG1 mutation in peripheral blood DNA. Methods: Mutation analysis was performed on whole blood and buccal swab DNA. Recombination activity of the mutant RAG1 protein and diversity of T cell repertoire were tested. Results: Apparent heterozygosity for a novel, functionally null RAG1 mutation in peripheral blood DNA from a patient with OS was shown to be secondary to true somatic reversion. Analysis of T cell repertoire demonstrated expression of various TCRBV families, but an overall restricted pattern. Conclusions: This is the first case of true somatic reversion of a RAG1 mutation in a patient with OS. The reversion event likely occurred at a stage where only a limited pool of T cell progenitors capable of performing V(D)J recombination could be generated. This work emphasizes the importance of performing functional studies to investigate the significance of novel genetic variants, and to consider somatic reversion as a possible disease modifier in SCID. [ABSTRACT FROM AUTHOR]

Published

2014

38. Omenn Sendromlu Bir Olgu.

Author

ÇALKAVUR, Sebnem, YALAZ, Mehmet, KÜTÜKÇÜLER, Necil, ÖZKINAY, Ferda, KANSOY, Savas, and KÜLTÜRSAY, Nilgün

Abstract

The Omenn syndrome is a form of severe combined immune deiciency that is inherited autosomal recessively and characterized by growth retardation, erythrodermia, lymphadenopathy, hepatosplenomegaly and severe recurrent infections. Although circulating T lymphocytes on the lymphocyte panel are normal, their functions are abnormal. On the other hand, circulating B lymphocytes are decreased or absent. Our case was a baby girl who was born to the second pregnancy of a 29-year-old mother on the 37th gestational week. She had a history of a sister's death on the 51st day of life due to Omenn syndrome. There was no consanguinity between parents. Her physical examination was normal expect generalized exfoliative erythrodermia. Routine laboratory investigations revealed eosinophilia. X-ray, echocardiography, abdominal and transfontanel ultrasonography indings were normal. IgG was at the lowest boundaries of the normal values. IgA and IgM were low as well. While T lymphocytes were elevated, B lymphocytes were extremely low. The family had a history of a baby death with the homozygote RAG1 g.854C>T (p.Q248X) mutation and parents were heterozygote carriers of the same mutation. Our patient also had the same homozygote RAG1 g.854C>T mutation. Since the parents' immunoglobulin levels and lymphocyte panels were normal, haploidentical stem cell transplantation from the father was performed. Unfortunately our patient passed away due to pulmonary infection on the posttransplantation 12th day. Genetic counseling has a great signiicance as untreated Omenn syndrome is fatal but the disorder is treatable with appropriate bone marrow or umbilical cord blood stem cell transplantion. [ABSTRACT FROM AUTHOR]

Published

2013

39. Spectrum of primary immunodeficiency disorders in Sri Lanka.

Author

Rajiva de Silva, Nilhan, Gunewardena, Sepali, Rathnayake, Damayanthi, and Devika Wickramasingha, Geethani

Subjects

*IMMUNODEFICIENCY, *PRIMARY care, *IMMUNOGLOBULINS, *GENETIC mutation, *HEALTH promotion, *DIAGNOSIS, *THERAPEUTICS

Abstract

Background While primary immunodeficiencies (PID has been recognized in the west for decades, recognition has been delayed in the third world. This study attempts to detail the spectrum of PID, the therapy provided, and constraints in the diagnosis and treatment in a middle income country such as Sri Lanka. Methods Nine hundred and forty two patients with recurrent infections and features suggestive of immune deficiency, referred from the entire country in a 4 year period, to the sole immunology unit in Sri Lanka were included. The following tests were performed. Full blood counts, serum Immunoglobulin and complement C3 and C4 levels, functional antibody levels, enumeration of lymphocyte subsets, in vitro and in vivo T cell functional assays, nitroblue tetrazolium assay to diagnose chronic granulomatous disease, hair shaft assay to diagnose Griscelli syndrome. Sequencing of the common gamma chain to identify x linked severe combined immune deficiency, and X linked agammaglobulinemia was confirmed by assaying for Btk mutations by single sequence conformation polymorphism. HIV/AIDS was excluded in all patients. Results Seventy three patients were diagnosed with a primary immune deficiency. The majority (60.27%) had antibody deficiency. Common variable immune deficiency was the commonest (28.76%), followed by X linked agammaglobulinemia (XLA) (20.54%). Five patients had possible hyper IgM syndrome. Ten patients had severe combined immune deficiency (SCID), including 2 with x linked SCID, in addition to DiGeorge syndrome (2), ataxia telangiectasia (6), autosomal dominant hyper IgE syndrome (2), chronic granulomatous disease (4), leucocyte adhesion deficiency type 1 (2) and Griscelli syndrome (3). Patients with autoinflammatory, innate immune and complement defects could not be identified due to lack of facilities. Conclusions Antibody deficiency is the commonest PID, as in the west .IgA deficiency is rare. Autoinflammatory diseases, innate immune and complement deficiencies could not be identified due to lack of diagnostic facilities. Lack of awareness of PID among adult physicians result in delay in treatment of adult patients. While treatment of antibody deficiencies provided in state hospitals has extended life expectancy, there is no treatment available for severe T cell defects. [ABSTRACT FROM AUTHOR]

Published

2013

40. Effects of Conditioning Regimens and T Cell Depletion in Hematopoietic Cell Transplantation for Primary Immune Deficiency

Author

Triplett, Brandon M., Wang, Chong, Yang, Jie, Dallas, Mari, Hartford, Christine, Howard, Vanessa, Pillai, Asha, Shook, David, Srinivasan, Ashok, Laver, Joseph, and Leung, Wing

Subjects

*HEMATOPOIETIC stem cell transplantation, *IMMUNODEFICIENCY, *T cells, *ORGAN donors, *DISEASE relapse, *HEALTH outcome assessment

Abstract

This study analyzes the hematopoietic cell transplantation experience in patients with immune deficiency at a single institution. The objective is to comprehensively evaluate the short-term and long-term outcomes with various preparative regimens, donor grafts, and ex vivo manipulations to identify transplantation approaches that most likely favor early donor immune competency without generating excessive toxicity. Clinical outcomes were evaluated in 52 consecutive patients with immune deficiencies. Thirty-seven of the 52 patients (71%) survived with attenuation of their underlying disease. The use of a melphalan-based reduced-intensity conditioning preparative regimen and immunomagnetic CD3+ T cell depletion techniques (when T cell depletion was indicated) were associated with improved event-free survival. Survivors who received a preparative regimen other than a melphalan-based reduced-intensity regimen suffered from therapy-related morbidities or chronic/recurrent infections. Our findings indicate that melphalan-based reduced-intensity conditioning regimens and immunomagnetic CD3+ T cell depletion limit therapy-related toxicity, and demonstrate promising results for the early establishment of donor immune competency. [Copyright &y& Elsevier]

Published

2012

41. The genetic basis of severe combined immunodeficiency and its variants.

Author

Tasher, Diana and Dalal, Ilan

Subjects

IMMUNOLOGICAL deficiency syndromes, IMMUNODEFICIENCY, LYMPHOCYTES, T cell differentiation, GENETIC mutation, PHENOTYPES, GENETICS

Abstract

Severe combined immunodeficiency (SCID) syndromes are characterized by a block in T lymphocyte differentiation that is variably associated with abnormal development of other lymphocyte lineages (B and/or natural killer [NK] cells), leading to death early in life unless treated urgently by hematopoietic stem cell transplant. SCID comprises genotypically and phenotypically heterogeneous conditions, of which the genetic basis for approximately 85% of the underlying immunologic defects have been recently elucidated. A major obstacle in deciphering the pathogenesis of SCID syndromes is that different mutations in a single gene may give rise to distinct clinical conditions and that a similar clinical phenotype can result from mutations in different genes. Mutation analysis is now an important component of the complete evaluation of a patient with SCID since it has a dramatic impact on many aspects of this potentially life-threatening disease such as genetic counseling, prenatal diagnosis, modalities of treatment, and, eventually, prognosis. Dr Robert Good, one of the founders of modern immunology, described the SCID syndrome as "experiments of nature." By understanding the cellular and genetic basis of these immunodeficiency diseases and, eventually, normal immunity, we optimize the "bedside to research laboratory and back again" approach to medicine. [ABSTRACT FROM AUTHOR]

Published

2012

42. Gene therapy for primary adaptive immune deficiencies.

Author

Fischer, Alain, Hacein-Bey-Abina, Salima, and Cavazzana-Calvo, Marina

Subjects

IMMUNODEFICIENCY, GENE therapy, ADENOSINE deaminase deficiency, CLINICAL trials, GENE expression, WISKOTT-Aldrich syndrome, KILLER cells, T cell receptors

Abstract

Gene therapy has become an option for the treatment of 2 forms of severe combined immunodeficiency (SCID): X-linked SCID and adenosine deaminase deficiency. The results of clinical trials initiated more than 10 years ago testify to sustained and reproducible correction of the underlying T-cell immunodeficiency. Successful treatment is based on the selective advantage conferred on T-cell precursors through their expression of the therapeutic transgene. However, “first-generation” retroviral vectors also caused leukemia in some patients with X-linked SCID because of the constructs’ tendency to insert into active genes (eg, proto-oncogenes) in progenitor cells and transactivate an oncogene through a viral element in the long terminal repeat. These elements have been deleted from the vectors now in use. Together with the use of lentiviral vectors (which are more potent for transducing stem cells), these advances should provide a basis for the safe and effective extension of gene therapy’s indications in the field of primary immunodeficiencies. Nevertheless, this extension will have to be proved by examining the results of the ongoing clinical trials. [ABSTRACT FROM AUTHOR]

Published

2011

43. Immune deficiency and the lung.

Author

Woodsford, Mairi A.M., Spencer, David A., and Cant, Andrew J.

Subjects

IMMUNODEFICIENCY, LUNG infections, PNEUMONIA, ASPERGILLOSIS, BRONCHIECTASIS, CHRONIC granulomatous disease, IMMUNOGLOBULIN E, IMMUNOGLOBULIN M, EARLY diagnosis, HEALTH outcome assessment, PEDIATRICS

Abstract

Abstract: The lungs are particularly vulnerable to infection; respiratory infections are common presenting features of primary immune deficiency (PID). Warning signs include recurrent, severe or invasive infections and poor weight gain. Understanding immune defects helps target investigations and management. Particular patterns of infection point to particular PIDs. Congenital antibody deficiencies are most common and feature recurrent pneumonia and bronchiectasis. Fungal pneumonia is seen in chronic granulomatous disease, lung abscesses are seen in Hyper IgE syndrome, and interstitial pneumonia in SCID and Hyper IgM syndrome. Lymphocyte subset analysis and specific antibody responses to vaccinations are useful investigations in addition to immunological measurements. Early diagnosis and referral for treatment greatly improve outcome. [Copyright &y& Elsevier]

Published

2011

44. Clinical and genetic heterogeneity in Omenn syndrome and severe combined immune deficiency.

Author

Gruber, Tanja A., Shah, Ami J., Hernandez, Michelle, Crooks, Gay M., Abdel-Azim, Hisham, Gupta, Sudhir, McKnight, Sean, White, Drew, Kapoor, Neena, and Kohn, Donald B.

Subjects

*IMMUNOLOGICAL deficiency syndromes, *T cells, *GENETIC mutation, *GENES, *LYMPHOCYTES, *GENETICS

Abstract

OS has been described as a clinical phenotype in infants characterized by SCID, diffuse erythroderma, and other distinct features. The pathogenesis is secondary to autologous, auto-reactive T cells produced as rare escapees from the SCID blockade. Mutations in either the RAG1 or RAG2 gene that lead to partial recombinase activity are responsible for many of the patients with these clinical features. We report on two patients, one with an atypical phenotype of OS (absence of rash but presence of other typical features) who harbored a previously undescribed mutation in RAG1, and a second who had many of the classic features of OS but was found to have a mutation in the common gamma chain (γc) cytokine receptor gene. These cases highlight the clinical and genetic heterogeneity of OS. [ABSTRACT FROM AUTHOR]

Published

2009

45. A Non-Leaky Artemis-Deficient Mouse That Accurately Models the Human Severe Combined Immune Deficiency Phenotype, Including Resistance to Hematopoietic Stem Cell Transplantation

Author

Xiao, Zheng, Dunn, Elizabeth, Singh, Kanal, Khan, Imran S., Yannone, Steven M., and Cowan, Morton J.

Subjects

*HEMATOPOIETIC stem cells, *DNA repair, *GENE therapy, *T cells, *TRANSPLANTATION of organs, tissues, etc.

Abstract

Abstract: Two Artemis-deficient (mArt-/- ) mouse models, generated independently on 129/SvJ backgrounds, have the expected T-B-NK+ severe combined immune deficiency (SCID) phenotype but fail to mimic the human disease because of CD4+ T cell leakiness. Moreover, immune reconstitution after hematopoietic stem cell transplantation is achieved more readily in these leaky mouse models than in Artemis-deficient humans. To develop a more clinically relevant animal model, we backcrossed the mArt-/- mutation onto the C57Bl/6 (B6) background (99.9%), which resulted in virtually no CD4+ T cell leakiness compared with 129/SvJ mArt+/- mice (0.3% ± 0.25% vs 19.5% ± 15.1%, P < .001). The nonleaky mouse also was uniquely resistant to engraftment using allogeneic mismatched hematopoietic stem cells, comparable to what is seen in human Artemis deficiency. The genetic background also influenced Artemis-associated radiation sensitivity, with differing degrees of x-ray hypersensitivity evident in 129/SvJ and B6 backgrounds with both the mArt-/- and mArt+/- genotypes. Our results indicate that immunogenic and DNA repair phenotypes associated with Artemis deficiency are significantly altered by genetic background, which has important implications for the diagnosis and treatment of SCID. Moreover, the B6 mArt-/- mouse provides a more accurate model for the human disease and a more appropriate system for studying human Artemis deficiency and for developing improved transplantation and gene therapy regimens for the treatment of children with SCID. [Copyright &y& Elsevier]

Published

2009

46. Stem cell transplantation for primary immunodeficiencies: King Faisal Specialist Hospital experience from 1993 to 2006.

Author

Al-Ghonaium, A.

Subjects

*HEMATOPOIETIC stem cells, *IMMUNODEFICIENCY, *SEVERE combined immunodeficiency, *HLA histocompatibility antigens, *HOMOGRAFTS, *PROGNOSIS, *THERAPEUTICS

Abstract

Primary immunodeficiencies constitute a group of highly complex congenital disorders most of which are characterized by poor prognosis with high mortality and morbidity. Hematopoietic SCT became an established therapy for such disorders. The first clear-cut report of successful allogenic SCT in 1968 dealt with the treatment of a patient with primary immunodeficiency, that is, SCID and Wiskott–Aldrich syndrome. Starting with this pioneering experience in 1968, hundreds of SCID patients and hundreds of patients affected by other life-threatening forms of primary immunodeficiency throughout the world have benefited from SCT. Presently, hematopoietic SCT from an HLA-matched sibling donor confers at least 80% chance of cure for children affected by primary immunodeficiency and about a 70% chance of cure when a fully HLA-matched related donor is available. This high success rate is the consequence of better management of nutrition and the infection problem affecting these patients at the time of disease. Conversely, when a related HLA-mismatched donor is used, the survival rate is significantly lower than that of patients receiving SCT from either an HLA-matched sibling or a fully matched HLA-unrelated donor. Optimal results and outcome of SCT are highly dependent on early and correct diagnosis of these disorders. SCT should be applied early in the course of the disease to prevent irreversible complications from the primary disease and/or infection. We present the data on outcome for primary immunodeficiency transplantation at King Faisal Specialist Hospital from 1993 to 2006.Bone Marrow Transplantation (2008) 42, S53–S56; doi:10.1038/bmt.2008.115 [ABSTRACT FROM AUTHOR]

Published

2008

47. Clinical application of DNA microarrays: Molecular diagnosis and HLA matching of an Amish child with severe combined immune deficiency

Author

Strauss, Kevin A., Puffenberger, Erik G., Bunin, Nancy, Rider, Nicholas L., Morton, Mary C., Eastman, James T., and Morton, D. Holmes

Subjects

*MENNONITE children, *DNA microarrays, *IMMUNODEFICIENCY, *GENETIC polymorphisms

Abstract

Abstract: Amish and Mennonite children with severe combined immune deficiency (SCID) often die without treatment as a result of delayed diagnoses and prohibitive costs of therapy. In this detailed case report, we describe the novel use of DNA microarrays to improve the diagnosis and management of an Amish infant with SCID. Using 10,000 single nucleotide polymorphism (SNP) genotypes from the patient, her parents, and seven siblings, we identified the recombinase activating genes for diagnostic sequencing, and then characterized a novel pathogenic variant in RAG1 (c.2974A>G). The same genotype data were used to identify a sibling stem cell donor who was haplo-identical at human leukocyte antigen (HLA) and blood group (ABO) loci. Autozygosity and linkage analysis of SNP genotypes within a family narrows the search for SCID candidate genes and provides a relatively simple and inexpensive way to identify potential tissue donors among biological siblings. [Copyright &y& Elsevier]

Published

2008

48. Spectrum of primary immune deficiency at a tertiary care hospital.

Author

Verma, Sumit, Sharma, Pradeep, Sivanandan, Sindhu, Rana, Nidhi, Saini, Savita, Lodha, Rakesh, and Kabra, S.

Abstract

To report various primary immune deficiencies diagnosed in children at a tertiary care hospital, their clinical manifestations and laboratory profile. Case records of children diagnosed to have primary immunodeficiency disorders over a period of 24 months at a tertiary care hospital in northern India were evaluated. Twenty-seven children (M: F=3.5: 1) with mean age of 5.4 ± 4.6 yrs (2mo-16yr) were diagnosed to have primary immunodeficiency. Thirteen children had chronic granulomatous disease (CGD), 4 had severe combined immunodeficiency (SCID), 4 had hypogammaglobulinemia, 2 had Ataxia telangiectasia, and one each had DiGeorge syndrome, Wiskott Aldrich syndrome, hyper IgM syndrome and leukocyte adhesion defect. Common mode of presentation were recurrent/ persistent pneumonia in 19, recurrent/ persistent diarrhea in 10, deep seated abscesses in 8, allergy in 3, disseminated tuberculosis infection in 2, extensive fungal infections in 2 and 1 each of disseminated cytomegalovirus (CMV) infection, disseminated BCG disease, otitis media and meningitis. Family history of sibling deaths was elicited in 2 families. Infectious agents were isolated in 16 cases. From a single center 27 patients with primary immune deficiency could be identified by chart review, suggesting need for high index of suspicion for diagnosis of primary immune deficiency in India. Though the exact prevalence is not known there is need to make a registry to document the magnitude of problem of these disorders. [ABSTRACT FROM AUTHOR]

Published

2008

49. PULMONARY AND SYSTEMIC TOXICITY OF BLEOMYCIN ON SEVERE COMBINED IMMUNE DEFICIENCY MICE.

Author

Miyazawa, Hiroshi, Takiguchi, Yuichi, Hiroshima, Kenzo, Kurosu, Katsushi, Tada, Yuji, Kasahara, Yasunori, Sakao, Seiichiro, Tanabe, Nobuhiro, Tatsumi, Koichiro, and Kuriyama, Takayuki

Subjects

*BLEOMYCIN, *SEVERE combined immunodeficiency, *PULMONARY toxicology, *IMMUNOLOGICAL deficiency syndromes, *LYMPHOCYTES, *MACROPHAGES

Abstract

Severe combined immune deficiency (SCID) mice were more sensitive to systemic delivery of bleomycin (BLM) than the wild-type strain, and died from esophagitis. Lung injury in the SCID mice by its intratracheal injection, however, was of comparable degree but with less lymphocyte infiltration than that in the wild-type mice. Macrophages and lymphocytes increased transiently in bronchoalveolar lavage fluid of SCID mice, whereas their increase in wild-type was continuous. Unsustainable inflammation in the lung might reduce BLM-induced lung injury in BLM-sensitive SCID mice. [ABSTRACT FROM AUTHOR]

Published

2008

50. Long-term immune reconstitution and clinical outcome after stem cell transplantation for severe T-cell immunodeficiency.

Author

Mazzolari, Evelina, Forino, Concetta, Guerci, Sara, Imberti, Luisa, Lanfranchi, Arnalda, Porta, Fulvio, and Notarangelo, Luigi D.

Subjects

TRANSPLANTATION of organs, tissues, etc., QUALITY of life, PRESERVATION of organs, tissues, etc., BONE grafting

Abstract

Background: Currently, hematopoietic stem cell transplantation allows long-term survival in a high proportion of infants with congenital severe T-cell immunodeficiency. However, relatively little is known of their long-term quality of life. Objective: We sought to assess the long-term immune reconstitution and clinical status in children treated with stem cell transplantation for severe T-cell immunodeficiency. Methods: Immune function and clinical status have been analyzed in a cohort of 40 patients with severe T-cell immunodeficiency who are alive at a follow-up of at least 5 years after transplantation. Results: Most patients have attained normal T- and B-cell function. Weight and height were normal at last follow-up in most patients. Endocrine and severe neurologic abnormalities have been observed in 17.5% and 10% of the patients, respectively. Conclusions: These data indicate that with current management strategies, stem cell transplantation can lead to long-term survival and good quality of life in the majority of patients with severe T-cell immunodeficiency. Clinical implications: Prompt recognition of congenital severe T-cell immunodeficiency, followed by stem cell transplantation, allows excellent perspectives of long-term survival and good quality of life for these otherwise fatal disorders. [Copyright &y& Elsevier]

Published

2007