Your search keyword '"Steinberg-Shemer O"' showing total 43 results

1. PB0252 The Role of Hydroxychloroquine in the Management of Children with ITP and Positive Antinuclear Antibodies

Author

Brik-Simon, D., primary, Levinsky, Y., additional, Efros, O., additional, Amarilyo, G., additional, Rabinowicz, R., additional, Steinberg-Shemer, O., additional, Tirosh, I., additional, Izraeli, S., additional, Yacobovich, J., additional, and Gilad, O., additional

Published

2023

2. P818: NEXT GENERATION TARGETED SEQUENCING FOR ENHANCED GENOTYPING OF DIAMOND BLACKFAN ANEMIA IN ISRAEL

Author

Goldberg, T., primary, Steinberg-Shemer, O., additional, Dgany, O., additional, Noy-Lotan, S., additional, Krasnov, T., additional, Gilad, O., additional, Yacobovich, J., additional, and Tamary, H., additional

Published

2022

3. P835: GENETIC BACKGROUND AND CLINICAL CHARACTERISTICS OF CONGENITAL NEUTROPENIAS IN ISRAEL

Author

Steinberg-Shemer, O., primary, Yeshareem, L., additional, Noy-Lotan, S., additional, Dgany, O., additional, Krasnov, T., additional, Berger Pinto, G., additional, Bielorai, B., additional, Kuperman, A. A., additional, Laor, R., additional, Mandel-Shorer, N., additional, Ben Barak, A., additional, Levin, C., additional, Mahdi, A., additional, Miskin, H., additional, Revel-Vilk, S., additional, Levin, D., additional, Benish, M., additional, Zuckerman, T., additional, Wolach, O., additional, Pazgal, I., additional, Gilad, O., additional, Goldberg, T., additional, Yacobovich, J., additional, Izraeli, S., additional, and Tamary, H., additional

Published

2022

4. P817: SYNDROMES PREDISPOSING TO LEUKEMIA ARE A MAJOR CAUSE OF INHERITED CYTOPENIAS IN CHILDREN

Author

Gilad, O., primary, Dgany, O., additional, Noy -Lotan, S., additional, Krasnov, T., additional, Yacobovich, J., additional, Rabinowicz, R., additional, Goldberg, T., additional, Kuperman, A., additional, Abu-Quider, A., additional, Miskin, H., additional, Kapelushnik, N., additional, Mandel-Shorer, N., additional, Shimony, S., additional, Harlev, D., additional, Ben-Ami, T., additional, Adam, E., additional, Levin, C., additional, Aviner, S., additional, Elhasid, R., additional, Berger-Achituv, S., additional, Chaitman-Yerushalmi, L., additional, Kodman, Y., additional, Oniashvilli, N., additional, Hameiri- Grosman, M., additional, Izraeli, S., additional, Tamary, H., additional, and Steinberg-Shemer, O., additional

Published

2022

5. PS1269 AUTOIMMUNE NEUTROPENIA OF INFANCY- UNEXPECTED PREVALENCE OF PSEUDOMONAS SKIN INFECTIONS

Author

Yacobovich, J., primary, Dagan, N. Aviran, additional, Goldberg, T., additional, Steinberg-Shemer, O., additional, and Tamary, H., additional

Published

2019

6. Targeted next generation sequencing for the diagnosis of patients with rare congenital anemias

Author

Shefer Averbuch, N. Steinberg-Shemer, O. Dgany, O. Krasnov, T. Noy-Lotan, S. Yacobovich, J. Kuperman, A.A. Kattamis, A. Ben Barak, A. Roth-Jelinek, B. Chubar, E. Shabad, E. Dufort, G. Ellis, M. Wolach, O. Pazgal, I. Abu Quider, A. Miskin, H. Tamary, H. and Shefer Averbuch, N. Steinberg-Shemer, O. Dgany, O. Krasnov, T. Noy-Lotan, S. Yacobovich, J. Kuperman, A.A. Kattamis, A. Ben Barak, A. Roth-Jelinek, B. Chubar, E. Shabad, E. Dufort, G. Ellis, M. Wolach, O. Pazgal, I. Abu Quider, A. Miskin, H. Tamary, H.

Abstract

Background: Most patients with anemia are diagnosed through clinical phenotype and basic laboratory testing. Nonetheless, in cases of rare congenital anemias, some patients remain undiagnosed despite undergoing an exhaustive workup. Genetic testing is complicated by the large number of genes involved in rare anemias and the similarities in the clinical presentation of the different syndromes. Objective: We aimed to enhance the diagnosis of patients with congenital anemias by using targeted next-generation sequencing. Methods: Genetic diagnosis was performed by gene capture followed by next-generation sequencing of 76 genes known to cause anemia syndromes. Results: Genetic diagnosis was achieved in 13 out of 21 patients (62%). Six patients were diagnosed with pyruvate kinase deficiency, 4 with dehydrated hereditary stomatocytosis, 2 with sideroblastic anemia, and 1 with CDA type IV. Eight novel mutations were found. In 7 patients, the genetic diagnosis differed from the pretest presumed diagnosis. The mean lag time from presentation to diagnosis was over 13 years. Conclusions: Targeted next-generation sequencing led to an accurate diagnosis in over 60% of patients with rare anemias. These patients do not need further diagnostic workup. Earlier incorporation of this method into the workup of patients with congenital anemia may improve patients’ care and enable genetic counseling. © 2018 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd

Published

2018

7. Galectin-3 secreted by triple-negative breast cancer cells regulates T cell function.

Author

Raiter A, Barhum Y, Lipovetsky J, Menachem C, Elgavish S, Ruppo S, Birger Y, Izraeli S, Steinberg-Shemer O, and Yerushalmi R

Subjects

Humans, Animals, Female, Mice, Cell Line, Tumor, Tumor Microenvironment immunology, T-Lymphocytes metabolism, T-Lymphocytes immunology, Disease Models, Animal, Lymphocytes, Tumor-Infiltrating immunology, Lymphocytes, Tumor-Infiltrating metabolism, Galectins metabolism, Galectins genetics, Blood Proteins, Triple Negative Breast Neoplasms metabolism, Triple Negative Breast Neoplasms pathology, Triple Negative Breast Neoplasms immunology, Triple Negative Breast Neoplasms genetics, Galectin 3 metabolism, Galectin 3 genetics

Abstract

Triple-negative breast cancer (TNBC) is an aggressive subtype that accounts for 10-15 % of breast cancer. Current treatment of high-risk early-stage TNBC includes neoadjuvant chemo-immune therapy. However, the substantial variation in immune response prompts an urgent need for new immune-targeting agents. This requires a comprehensive understanding of TNBC's tumor microenvironment. We recently demonstrated that Galectin-3 (Gal-3) binding protein/Gal-3 complex secreted by TNBC cells induces immunosuppression, through inhibiting CD45 signaling in T cells. Here, we further investigated the interaction between secreted Gal-3 and T cells in TNBC. Using CRISPR/Cas9 gene editing of the TNBC MDA-MB-231 cell-line, we obtained Gal-3 negative (neg) clones. We studied these in an in-vitro model, co-cultured with peripheral blood mononuclear cells (PBMC) to imitate immune-tumor interaction, and in an in-vivo model, when implanted in mice. Gal-3 neg tumors in mice had decelerated tumor growth after PBMC inoculation. In contrast, the Gal-3 positive (pos) tumors continued growing despite PBMC inoculation, and tumor T regulatory cell (CD4/FoxP3+) infiltration increased. RNA sequencing of T cells from women with TNBC with elevated plasma levels of Gal-3 revealed significantly lower expression of oxidative phosphorylation genes than in T cells from healthy women. Similarly, in our in-vitro model, the decreased expression of oxidative phosphorylation genes and mitochondrial dysfunction resulted in a significant increase in CD8 intracellular reactive oxygen species. Consequently, T exhausted cells (CD8/PD1/Tim3/Lag3+) significantly increased in PBMC co-cultured with Gal-3 pos TNBCs. To conclude, we revealed a novel TNBC-related Gal-3 suppressor mechanism that involved upregulation of CD4 T regulatory and of CD8 T exhausted cells., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2025

8. Clinical and Laboratory Characteristics of Pediatric Patients With ACKR1/DARC-Associated Neutropenia.

Author

Oz-Alcalay L, Steinberg-Shemer O, Elron E, Dvori M, Elitzur S, Dgany O, Noy-Lotan S, Krasnov T, Tamary H, Brik-Simon D, Yacobovich J, and Gilad O

Subjects

Humans, Female, Male, Infant, Child, Child, Preschool, Polymorphism, Single Nucleotide, Adolescent, Follow-Up Studies, Prognosis, Infant, Newborn, Israel epidemiology, Neutropenia genetics, Neutropenia epidemiology, Duffy Blood-Group System genetics, Receptors, Cell Surface genetics

Abstract

Background: ACKR1/DARC-associated neutropenia (ADAN), resulting from homozygosity for a single nucleotide polymorphism (SNP) in the ACKR1/DARC gene (rs2814778), is a common cause of benign neutropenia that primarily affects individuals of African and Jewish Yemenite descent. We aimed to characterize ADAN in pediatric patients in Israel, given its ethnically diverse population., Procedure: We assessed children with isolated neutropenia treated during 2018-2023 at one pediatric center, for the ACKR1/DARC polymorphism, using Sanger sequencing or targeted next-generation sequencing., Results: Of 115 patients evaluated, 49 (42.6%) were diagnosed with ADAN; of these, 29 (59%) had absolute neutrophil counts in the severe range (0-0.5 × 10 9 /L) at diagnosis. The allele distribution revealed 37% of Muslim Arab and 61% of Jewish origin. Yemenite, Ethiopian, Mediterranean, Asian, and European ancestry were included; 59% had a family history of neutropenia. The median age at the first neutropenia detection was 1.2 years; 91.8% were identified during routine blood counts. The median absolute neutrophil count at diagnosis was 0.5 × 10 9 /L (interquartile range: 0.3). An increased susceptibility to infections was not found either before or during the median follow-up period of 2.5 years (interquartile range: 1.54) after the diagnosis of ADAN. In 34 patients (72.3%), neutrophil counts were in the normal range during febrile illnesses., Conclusions: We identified ADAN in individuals of variable ethnicities, almost half with severe neutropenia. We recommend testing for ADAN in all children with isolated neutropenia without severe infections. Homozygosity for the ACKR1/DARC rs2814778 SNP may obviate the need for further investigation, follow-up, or treatment in specific clinical scenarios., (© 2024 The Author(s). Pediatric Blood & Cancer published by Wiley Periodicals LLC.)

Published

2025

9. Erratum to : Characterization and genotype-phenotype correlation of patients with Fanconi anemia in a multi-ethnic population.

Author

Steinberg-Shemer O, Goldberg TA, Yacobovich J, Levin C, Koren A, Revel-Vilk S, Ben-Ami T, Kuperman AA, Zemer VS, Toren A, Kapelushnik J, Ben-Barak A, Miskin H, Krasnov T, Noy-Lotan S, Dgany O, and Tamary H

Published

2025

10. A Variable Clinical Presentation of Hemoglobin City of Hope.

Author

Brik Simon D, Filon D, Meiner V, Krasnov T, Noy-Lotan S, Dgany O, Gilad O, Goldberg T, Izraeli S, Yacobovich J, Tamary H, and Steinberg-Shemer O

Abstract

Hemoglobin City of Hope (Hb-COH), NC_000011.9(NM_000518.5):c.208G > A; NP_000509.1:p.(Gly70Ser), has rarely been described. The presentation ranges from asymptomatic heterozygosity to significant anemia in patients carrying an additional pathogenic variant in β-globin. To elucidate the clinical spectrum of Hb-COH, we analyzed 31 individuals carrying the variant, including, for the first time, homozygous individuals. Seven patients who were compound heterozygous for Hb-COH and an additional variant in β-globin, presented with mild-to-severe microcytic anemia and elevated hemoglobin-A2. Three (43%) of these also had elevated fetal hemoglobin, but none required blood transfusions. Seven patients coinherited Hb-COH with an -α 3.7 -deletion (NG_000006.1:g.34247_38050del), their presentation ranged from mild microcytic anemia to normal blood counts. Three homozygous and 14 heterozygous individuals for Hb-COH had normal blood counts. Most Hb-COH alleles whose origin was traceable were from Ashkenazi Jews (70.4%). To conclude, while isolated Hb-COH appears asymptomatic even in the homozygous state, it may cause significant anemia when coinherited with an additional pathogenic variant in β-globin. Understanding the full impact of Hb-COH is crucial for optimal patient management and for genetic counseling., (© 2024 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2024

11. Is less more? Intravenous immunoglobulin for pediatric immune thrombocytopenia.

Author

Elron E, Yacobovich J, Efros O, Tanous O, Levy-Mendelovich S, Shamba E, Steinberg-Shemer O, Goldberg T, Izraeli S, and Gilad O

Abstract

Objectives: Treatment of pediatric immune thrombocytopenia (ITP) is guided by the risk of bleeding. Intravenous immunoglobulin (IVIg) is one of the first-line therapy options for new-onset pediatric ITP. However, the exact optimal dose of IVIg has not been determined., Methods: This retrospective cohort study included all hospitalized children with newly diagnosed ITP receiving IVIg as first-line therapy during 2010-2020. We compared the safety and efficacy of two common IVIg dose regimens, 1 and 2 g/kg. Outcomes were short and long-term treatment responses and adverse events to the different doses., Results: A total of 168 children were included in our cohort. Eighty-two children were treated with 1 g/kg of IVIg and 86 with 2 g/kg. There was no difference in sustained response (platelet count > 20 × 10 9 , > 14 days) between the groups (74.3% vs 76.7%, respectively, p  = 0.72) and maximal platelet counts following treatment ( p  = 0.44). No difference was found regarding the percentage of chronic ITP between the two groups (24.4% in the 1 g/kg group as compared to 17.4% in the 2 g/kg group; p  = 0.34). Logistic regression analysis demonstrated there was no effect of the IVIg dose on treatment failure and development of chronic ITP. As anticipated, 47.7% of adverse events were in the 2 g/kg group and 32.9% in the 1 g/kg group, with borderline statistical significance ( p  = 0.06)., Conclusion: The initial treatment of newly diagnosed pediatric ITP using a 1 g/kg IVIg regimen may give comparable results to the double dose of 2 g/kg in attaining a prolonged safe hemostatic threshold, without impacting the incidence of chronic disease., Competing Interests: Sarina Levy-Mendelovich is a recipient of research grants from Novo Nordisk and Pfizer and has an Honorium from Roche and Pfizer. The other authors have no conflicts of interest relevant to this article to disclose., (© The Author(s), 2024.)

Published

2024

12. Genetic backgrounds and clinical characteristics of congenital neutropenias in Israel.

Author

Yeshareem L, Yacobovich J, Lebel A, Noy-Lotan S, Dgany O, Krasnov T, Berger Pinto G, Oniashvili N, Mardoukh J, Bielorai B, Laor R, Mandel-Shorer N, Ben Barak A, Levin C, Asleh M, Miskin H, Revel-Vilk S, Levin D, Benish M, Zuckerman T, Wolach O, Pazgal I, Brik Simon D, Gilad O, Yanir AD, Goldberg TA, Izraeli S, Tamary H, and Steinberg-Shemer O

Subjects

Humans, Male, Israel epidemiology, Female, Child, Child, Preschool, Adolescent, Genetic Predisposition to Disease, Adult, Hematopoietic Stem Cell Transplantation, Infant, Consanguinity, Glucose-6-Phosphatase genetics, Alleles, Registries, High-Throughput Nucleotide Sequencing, Young Adult, Phenotype, Genetic Association Studies, Neutropenia genetics, Neutropenia congenital, Neutropenia epidemiology, Neutropenia diagnosis, Mutation, Congenital Bone Marrow Failure Syndromes genetics, Congenital Bone Marrow Failure Syndromes diagnosis

Abstract

Background: Congenital neutropenias are characterized by severe infections and a high risk of myeloid transformation; the causative genes vary across ethnicities. The Israeli population is characterized by an ethnically diverse population with a high rate of consanguinity., Objective: To evaluate the clinical and genetic spectrum of congenital neutropenias in Israel., Methods: We included individuals with congenital neutropenias listed in the Israeli Inherited Bone Marrow Failure Registry. Sanger sequencing was performed for ELANE or G6PC3, and patients with wild-type ELANE/G6PC3 were referred for next-generation sequencing., Results: Sixty-five patients with neutropenia were included. Of 51 patients with severe congenital neutropenia, 34 were genetically diagnosed, most commonly with variants in ELANE (15 patients). Nine patients had biallelic variants in G6PC3, all of consanguineous Muslim Arab origin. Other genes involved were SRP54, JAGN1, TAZ, and SLC37A4. Seven patients had cyclic neutropenia, all with pathogenic variants in ELANE, and seven had Shwachman-Diamond syndrome caused by biallelic SBDS variants. Eight patients (12%) developed myeloid transformation, including six patients with an unknown underlying genetic cause. Nineteen (29%) patients underwent hematopoietic stem cell transplantation, mostly due to insufficient response to treatment with granulocyte-colony stimulating factor or due to myeloid transformation., Conclusions: The genetic spectrum of congenital neutropenias in Israel is characterized by a high prevalence of G6PC3 variants and an absence of HAX1 mutations. Similar to other registries, for 26% of the patients, a molecular diagnosis was not achieved. However, myeloid transformation was common in this group, emphasizing the need for close follow-up., (© 2024 The Authors. European Journal of Haematology published by John Wiley & Sons Ltd.)

Published

2024

13. Symptomatic corpus luteum hemorrhage in adolescent females with ITP.

Author

Yelak A, From A, Gilad O, Brik Simon D, Rubin S, Cohen M, Amarilyo G, Levin C, Bakry D, Izraeli S, Tamary H, Yacobovich J, and Steinberg-Shemer O

Subjects

Adolescent, Female, Humans, Hemoperitoneum etiology, Ovarian Diseases diagnosis, Ovarian Diseases etiology, Retrospective Studies, Corpus Luteum, Hemorrhage etiology, Hemorrhage diagnosis, Hemorrhage therapy, Purpura, Thrombocytopenic, Idiopathic complications, Purpura, Thrombocytopenic, Idiopathic therapy, Purpura, Thrombocytopenic, Idiopathic diagnosis

Abstract

Patients with immune thrombocytopenia (ITP) usually present with minor mucocutaneous bleeding. Corpus luteum hemorrhage (CLH) is generally asymptomatic but may, rarely, lead to severe intraperitoneal bleeding, mostly in patients with coagulation disorders. CLH causing intraperitoneal bleeding has only been described in few individuals with ITP. The objective of this retrospective observational study was to assess the clinical course and incidence of symptomatic CLH in adolescent females with newly diagnosed or chronic ITP. Additionally, a comprehensive literature review was conducted to scrutinize cases of pediatric female patients with ITP, complicated by CLH. We identified three patients with ITP and hemoperitoneum secondary to CLH. They presented with acute abdominal pain, had severe thrombocytopenia (platelet counts below 20 × 10 9 /L), and required blood transfusions as well as ITP-directed therapy. All the patients were hemodynamically stable and did not require emergency surgical intervention.  Conclusion: CLH could potentially pose a significant complication in the context of adolescent females with ITP, requiring a strong index of suspicion to direct expedient therapy. What is Known: • Immune thrombocytopenia is typically associated with minor bleeding tendency. • Corpus luteum hemorrhage is generally asymptomatic; however, in women with bleeding disorders, it has the potential to result in substantial intra-abdominal bleeding. What is New: • Corpus luteum hemorrhage leading to intra-abdominal bleeding is a potential severe complication of immune thrombocytopenia in adolescent females., (© 2024. The Author(s).)

Published

2024

14. Excellent response to treatment with hydroxychloroquine in pediatric patients with SLE-related immune thrombocytopenia.

Author

Brik-Simon D, Efros O, Levinsky Y, Amarilyo G, Tirosh I, Levy-Mendelovich S, Steinberg-Shemer O, Izraeli S, Yacobovich J, and Gilad O

Subjects

Adolescent, Humans, Female, Child, Male, Hydroxychloroquine therapeutic use, Retrospective Studies, Purpura, Thrombocytopenic, Idiopathic drug therapy, Lupus Erythematosus, Systemic complications, Lupus Erythematosus, Systemic drug therapy, Thrombocytopenia drug therapy

Abstract

Background: Pediatric immune thrombocytopenia (ITP) may precede systemic autoimmune disorders. In adolescent patients with ITP, routine screening for systemic lupus erythematosus (SLE) may be performed by testing for antinuclear antibody (ANA) titer. Hydroxychloroquine (HCQ) is a safe and effective immunomodulatory drug in patients with SLE but rarely used in ITP. We analyzed the platelet count response and safety of HCQ in treating pediatric patients with SLE-related ITP., Methods: A retrospective study including pediatric patients with ITP and definite or incomplete SLE, who were treated with HCQ during 2010-2021. SLE was defined by ANA titer ≥ 1:160 as measured by immunofluorescence and ≥10 points according to the 2019 EULAR/ACR 2019 classification criteria, while patients with incomplete SLE achieved a score < 10. Complete response (CR) of the platelet count was defined as platelet count > 100 × 10 9 /L; partial response (PR) as platelet count 30-100 × 10 9 /L and exceeding ≥ twice baseline counts., Results: Of the 17 patients included (median age 15.5 years; IQR 3.6), 15 (88.2%) were female, 13 had definite SLE, and four had incomplete SLE. HCQ was initiated at a median of 17 months after ITP diagnosis with a median platelet count of 38 × 10 9 /L (IQR 28). At 8 weeks, 8 (47.1%) patients responded, including 6 (35.3%) achieving CR. After one year, the overall response was 82.4%, with the remaining patients having stable platelet counts requiring no additional ITP therapy. The response was maintained at a median follow-up of 42 months. No adverse effects to HCQ were noted., Conclusion: Pediatric patients with SLE-related ITP may benefit from treatment with HCQ., (© 2024 The Authors. Pediatric Blood & Cancer published by Wiley Periodicals LLC.)

Published

2024

15. A Need for a Novel Survival Risk Scoring System for Intensive Care Admissions Due to Sepsis in Pediatric Hematology/Oncology Patients.

Author

Wittmann Dayagi T, Nirel R, Avrahami G, Amar S, Elitzur S, Fisher S, Gilead G, Gilad O, Goldberg T, Izraeli S, Kadmon G, Kaplan E, Krauss A, Michaeli O, Stein J, Steinberg-Shemer O, Tamary H, Tausky O, Toledano H, Weissbach A, Yacobovich J, Yanir AD, Zon J, Nahum E, and Barzilai-Birenboim S

Subjects

Child, Humans, Infant, Retrospective Studies, Prospective Studies, Prognosis, Intensive Care Units, Pediatric, Critical Care, Hospital Mortality, Neoplasms, Sepsis, Hematology

Abstract

Background: Children with hemato-oncological diseases or following stem cell transplantation (SCT) are at high risk for life-threatening infections; sepsis in this population constitutes a substantial proportion of pediatric intensive care unit (PICU) admissions. The current pediatric prognostic scoring tools to evaluate illness severity and mortality risk are designed for the general pediatric population and may not be adequate for this vulnerable subpopulation. Methods: Retrospective analysis was performed on all PICU admissions for sepsis in children with hemato-oncological diseases or post-SCT, in a single tertiary pediatric hospital between 2008 and 2021 ( n  = 233). We collected and analyzed demographic, clinical, and laboratory data and outcomes for all patients, and evaluated the accuracy of two major prognostic scoring tools, the Pediatric Logistic Organ Dysfunction-2 (PELOD-2) and the Pediatric Risk of Mortality III (PRISM III). Furthermore, we created a new risk-assessment model that contains additional parameters uniquely relevant to this population. Results: The survival rate for the cohort was 83%. The predictive accuracies of PELOD-2 and PRISM III, as determined by the area under the curve (AUC), were 83% and 78%, respectively. Nine new parameters were identified as clinically significant: age, SCT, viral infection, fungal infection, central venous line removal, vasoactive inotropic score, bilirubin level, C-reactive protein level, and prolonged neutropenia. Unique scoring systems were established by the integration of these new parameters into the algorithm; the new systems significantly improved their predictive accuracy to 91% ( p  = 0.01) and 89% ( p  < 0.001), respectively. Conclusions: The predictive accuracies (AUC) of the PELOD-2 and PRISM III scores are limited in children with hemato-oncological diseases admitted to PICU with sepsis. These results highlight the need to develop a risk-assessment tool adjusted to this special population. Such new scoring should represent their unique characteristics including their degree of immunosuppression and be validated in a large multi-center prospective study., Competing Interests: Declaration of Conflicting InterestsThe author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2024

16. Biallelic hypomorphic variants in CAD cause uridine-responsive macrocytic anaemia with elevated haemoglobin-A2.

Author

Steinberg-Shemer O, Yacobovich J, Noy-Lotan S, Dgany O, Krasnov T, Barg A, Landau YE, Kneller K, Somech R, Gilad O, Brik Simon D, Orenstein N, Izraeli S, Del Caño-Ochoa F, Tamary H, and Ramón-Maiques S

Subjects

Humans, Uridine, Hemoglobins, Spasms, Infantile genetics, Anemia, Anemia, Macrocytic

Abstract

Biallelic pathogenic variants in CAD, that encode the multienzymatic protein required for de-novo pyrimidine biosynthesis, cause early infantile epileptic encephalopathy-50. This rare disease, characterized by developmental delay, intractable seizures and anaemia, is amenable to treatment with uridine. We present a patient with macrocytic anaemia, elevated haemoglobin-A2 levels, anisocytosis, poikilocytosis and target cells in the blood smear, and mild developmental delay. A next-generation sequencing panel revealed biallelic variants in CAD. Functional studies did not support complete abrogation of protein function; however, the patient responded to uridine supplement. We conclude that biallelic hypomorphic CAD variants may cause a primarily haematological phenotype., (© 2023 The Authors. British Journal of Haematology published by British Society for Haematology and John Wiley & Sons Ltd.)

Published

2024

17. Cytopenias in pediatric kidney transplant recipients: preceding factors and clinical consequences.

Author

Regev-Sadeh S, Borovitz Y, Steinberg-Shemer O, Gilad O, Shoham S, and Yacobovich J

Subjects

Humans, Child, Immunosuppressive Agents adverse effects, Retrospective Studies, Renal Dialysis, Graft Rejection epidemiology, Graft Rejection etiology, Graft Rejection prevention & control, Transplant Recipients, Risk Factors, Kidney Transplantation adverse effects, Anemia drug therapy, Thrombocytopenia epidemiology, Thrombocytopenia etiology, Neutropenia epidemiology, Neutropenia etiology, Neutropenia drug therapy

Abstract

Background: Kidney trans plantation is associated with secondary complications, including the risk of developing posttransplant cytopenias. This study aimed to evaluate the characteristics, identify predictors, and assess the management and consequences of cytopenias in the pediatric kidney transplant population., Methods: This is a single-center retrospective analysis of 89 pediatric kidney transplant recipients. Possible factors preceding cytopenias were compared with the goal of recognizing predictors for posttransplant cytopenias. Posttransplant neutropenias were analyzed for the total study period and separately for the period beyond 6 months posttransplant (late neutropenias), to rule out confounding influences of induction and initial intensive therapy., Results: Sixty patients (67%) developed at least one episode of posttransplant cytopenia. All episodes of posttransplant thrombocytopenias were mild or moderate. Posttransplant infections and graft rejection were found to be significant predictors for thrombocytopenia (HR 6.06, 95% CI 1.6-22.9, and HR 5.82, 95% CI 1.27-26.6, respectively). A total of 30% of posttransplant neutropenias were severe (ANC ≤ 500). Pretransplant dialysis and posttransplant infections were significant predictors for late neutropenias (HR 11.2, 95% CI 1.45-86.4, and HR 3.32, 95% CI 1.46-7.57, respectively). Graft rejection occurred in 10% of patients with cytopenia, all following neutropenia, within 3 months from cytopenia appearance. In all such cases, mycophenolate mofetil dosing had been held or reduced prior to rejection., Conclusions: Posttransplant infections are substantial contributors to developing posttransplant cytopenias. Preemptive transplantation appears to reduce risk of late neutropenia, the accompanying reduction in immunosuppressive therapy, and the ensuing risk of graft rejection. An alternative response to neutropenia, possibly using granulocyte colony stimulating factor, may diminish graft rejection. A higher resolution version of the Graphical abstract is available as Supplementary information., (© 2023. The Author(s), under exclusive licence to International Pediatric Nephrology Association.)

Published

2023

18. Cellular and metabolic characteristics of pre-leukemic hematopoietic progenitors with GATA2 haploinsufficiency.

Author

Rein A, Geron I, Kugler E, Fishman H, Gottlieb E, Abramovich I, Giladi A, Amit I, Mulet-Lazaro R, Delwel R, Gröschel S, Levin-Zaidman S, Dezorella N, Holdengreber V, Rao TN, Yacobovich J, Steinberg-Shemer O, Huang QH, Tan Y, Chen SJ, Izraeli S, and Birger Y

Subjects

Child, Humans, Mice, Animals, Bone Marrow pathology, Hematopoietic Stem Cells metabolism, Cell Transformation, Neoplastic genetics, Cell Transformation, Neoplastic metabolism, GATA2 Transcription Factor genetics, GATA2 Transcription Factor metabolism, GATA2 Deficiency genetics, Myelodysplastic Syndromes pathology, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute metabolism

Abstract

Mono-allelic germline disruptions of the transcription factor GATA2 result in a propensity for developing myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML), affecting more than 85% of carriers. How a partial loss of GATA2 functionality enables leukemic transformation years later is unclear. This question has remained unsolved mainly due to the lack of informative models, as Gata2 heterozygote mice do not develop hematologic malignancies. Here we show that two different germline Gata2 mutations (TgErg/Gata2het and TgErg/Gata2L359V) accelerate AML in mice expressing the human hematopoietic stem cell regulator ERG. Analysis of Erg/Gata2het fetal liver and bone marrow-derived hematopoietic cells revealed a distinct pre-leukemic phenotype. This was characterized by enhanced transition from stem to progenitor state, increased proliferation, and a striking mitochondrial phenotype, consisting of highly expressed oxidative-phosphorylation-related gene sets, elevated oxygen consumption rates, and notably, markedly distorted mitochondrial morphology. Importantly, the same mitochondrial gene-expression signature was observed in human AML harboring GATA2 aberrations. Similar to the observations in mice, non-leukemic bone marrows from children with germline GATA2 mutation demonstrated marked mitochondrial abnormalities. Thus, we observed the tumor suppressive effects of GATA2 in two germline Gata2 genetic mouse models. As oncogenic mutations often accumulate with age, GATA2 deficiency-mediated priming of hematopoietic cells for oncogenic transformation may explain the earlier occurrence of MDS/AML in patients with GATA2 germline mutation. The mitochondrial phenotype is a potential therapeutic opportunity for the prevention of leukemic transformation in these patients.

Published

2023

19. Neonatal Thrombocytopenia: Differing Characteristics of NAIT Versus Non-NAIT.

Author

Zemer VS, Mousa K, Herscovici T, Steinberg-Shemer O, Bonstein L, and Yacobovich J

Subjects

Pregnancy, Infant, Female, Child, Humans, Infant, Newborn, Isoantibodies, Retrospective Studies, Platelet Count, Thrombocytopenia, Neonatal Alloimmune therapy, Thrombocytopenia, Neonatal Alloimmune epidemiology, Infant, Newborn, Diseases, Antigens, Human Platelet

Abstract

While neonatal alloimmune thrombocytopenia (NAIT) is the most common cause of severe neonatal thrombocytopenia good clinical predictors are lacking. We analyzed cases of neonatal thrombocytopenia in Schneider Children's Medical Center of Israel to pinpoint qualifiers of NAIT (NAIT+) in comparison to non-NAIT (NAIT-) thrombocytopenia. Patient and maternal data were retrospectively collected on all thrombocytopenic newborns undergoing a workup for NAIT in our tertiary center between 2001 and 2016. Among 26 thrombocytopenic neonates, the mean nadir in NAIT+ patients (25×10 9 /L) was significantly lower than NAIT- patients (64×10 9 /L) ( P <0.001). 61.5% of NAIT+ infants required treatment compared with 23% of non-NAIT ( P =0.015). NAIT+ patients also required more therapeutic modalities than infants with NAIT- thrombocytopenia. Human platelet antigen (HPA)-1a and HPA-5b alloantibodies most frequently caused NAIT. In summary, thrombocytopenia in NAIT+ was significantly more severe compared with NAIT- and more likely to require treatment. In addition, despite the varied ethnic population in Israel, the HPA alloantibodies found in our population were most similar to those common in Western countries. In the absence of rigorous prenatal screening options, we suggest platelet counts below 40 to 50×10 9 /L in a healthy newborn be considered most suggestive for NAIT and warrant urgent NAIT-specific analysis., Competing Interests: The authors declare no conflict of interest., (Copyright © 2023 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2023

20. [GENETIC PANELS FOR THE DIAGNOSIS OF RARE CONGENITAL HEMATOLOGICAL DISORDERS].

Author

Steinberg-Shemer O, Dgany O, and Tamary H

Subjects

Humans, Syndrome, Anemia congenital, Hematopoietic Stem Cell Transplantation

Abstract

Introduction: Genetic diagnosis of congenital hematological disorders is complicated by the overlap of the clinical and laboratory presentation across different diseases and the large number of genes involved in each syndrome. Nonetheless, an accurate genetic diagnosis is essential for directing the follow-up and treatment program of the patients, as well as for identifying asymptomatic family members, choosing a non-affected related donor for hematopoietic stem cell transplantation and for offering a prenatal diagnosis. In recent years, a novel method of targeted next generation sequencing using gene panels was developed. In our laboratory, gene panels were incorporated for the diagnosis of congenital hematological disorders, including inherited bone marrow failure syndromes and rare anemias, and for the detection of somatic variant in the bone marrow. It is of utmost importance that an in-depth analysis will include a correlation of the genetic variants with the clinical and laboratory presentation and with the family history. Here, we demonstrate the importance of performing a timely genetic diagnosis in patients with congenital hematological disorders.

Published

2023

21. Cerebral sinus venous thrombosis in children with inherited bleeding disorders: A case series.

Author

Sheikh IN, Srivaths L, Li E, Steinberg-Shemer O, Mandel-Shorer N, Kenet G, and Barg AA

Subjects

Child, Hemorrhage, Humans, Blood Coagulation Disorders therapy, Blood Coagulation Disorders, Inherited, Thrombosis, Venous Thrombosis etiology, von Willebrand Diseases therapy

Abstract

In patients with inherited bleeding disorders, thrombus development poses a challenge in balancing the management of thrombosis and bleeding. Pediatric antithrombotic therapy guidelines do not address the treatment of a thrombus in the setting of a bleeding disorder. We present a case series of four children with inherited bleeding disorders presenting with cerebral sinus venous thrombosis and bleeding, in order to summarize the different therapeutic approaches and outcomes of these patients., (© 2022 Wiley Periodicals LLC.)

Published

2022

22. Syndromes predisposing to leukemia are a major cause of inherited cytopenias in children.

Author

Gilad O, Dgany O, Noy-Lotan S, Krasnov T, Yacobovich J, Rabinowicz R, Goldberg T, Kuperman AA, Abu-Quider A, Miskin H, Kapelushnik N, Mandel-Shorer N, Shimony S, Harlev D, Ben-Ami T, Adam E, Levin C, Aviner S, Elhasid R, Berger-Achituv S, Chaitman-Yerushalmi L, Kodman Y, Oniashvilli N, Hameiri-Grosman M, Izraeli S, Tamary H, and Steinberg-Shemer O

Subjects

Child, Congenital Bone Marrow Failure Syndromes, Disease Susceptibility, Humans, Anemia, Aplastic genetics, Leukemia, Myelodysplastic Syndromes diagnosis, Myelodysplastic Syndromes genetics, Neutropenia congenital, Neutropenia genetics, Thrombocytopenia diagnosis, Thrombocytopenia genetics

Abstract

Prolonged cytopenias are a non-specific sign with a wide differential diagnosis. Among inherited disorders, cytopenias predisposing to leukemia require a timely and accurate diagnosis to ensure appropriate medical management, including adequate monitoring and stem cell transplantation prior to the development of leukemia. We aimed to define the types and prevalences of the genetic causes leading to persistent cytopenias in children. The study comprises children with persistent cytopenias, myelodysplastic syndrome, aplastic anemia, or suspected inherited bone marrow failure syndromes, who were referred for genetic evaluation from all pediatric hematology centers in Israel during 2016-2019. For variant detection, we used Sanger sequencing of commonly mutated genes and a custom-made targeted next-generation sequencing panel covering 226 genes known to be mutated in inherited cytopenias; the minority subsequently underwent whole exome sequencing. In total, 189 children with persistent cytopenias underwent a genetic evaluation. Pathogenic and likely pathogenic variants were identified in 59 patients (31.2%), including 47 with leukemia predisposing syndromes. Most of the latter (32, 68.1%) had inherited bone marrow failure syndromes, nine (19.1%) had inherited thrombocytopenia predisposing to leukemia, and three each (6.4%) had predisposition to myelodysplastic syndrome or congenital neutropenia. Twelve patients had cytopenias with no known leukemia predisposition, including nine children with inherited thrombocytopenia and three with congenital neutropenia. In summary, almost one third of 189 children referred with persistent cytopenias had an underlying inherited disorder; 79.7% of whom had a germline predisposition to leukemia. Precise diagnosis of children with cytopenias should direct follow-up and management programs and may positively impact disease outcome.

Published

2022

23. Characterization of Fanconi Anemia Patients with Head and Neck Squamous Cell Carcinoma: Israel Fanconi Registry.

Author

Tsur N, Frig O, Steinberg-Shemer O, Tamary H, Kurman N, Mizrachi A, and Popovtzer A

Subjects

Humans, Israel epidemiology, Registries, Squamous Cell Carcinoma of Head and Neck epidemiology, Squamous Cell Carcinoma of Head and Neck therapy, Fanconi Anemia complications, Fanconi Anemia epidemiology, Fanconi Anemia therapy, Head and Neck Neoplasms epidemiology, Head and Neck Neoplasms therapy

Abstract

Background: Recent studies show a high risk of developing malignancy in patients with Fanconi anemia. The most common solid tumor in this condition is head and neck squamous cell carcinoma (HNSCC) and there is often uncertainty and about disease behavior as well as chemotherapy and radiation response., Objectives: To describe and characterize HNSCC among Fanconi anemia patients on the Israeli Fanconi Registry., Methods: Our study population included patients in Israel's inherited bone marrow failure registry who were diagnosed with Fanconi anemia between1980 and 2016. Demographic, clinical, and laboratory data were collected from patient charts., Results: From the collected data, HNSCC was confirmed in 6/111 (5.4%) Fanconi anemia patients; 1 (17%) had classic HNSCC risk factors of tobacco abuse and 4 (56%) had undergone primary surgery. The 3 (50%) receiving concurrent chemoradiotherapy had mild side effects, while half developed metachronous primary malignancy, and all developed > 2 primary malignancies. The overall median survival of the patients in our study was 14 (0.5-57) months., Conclusions: Fanconi anemia patients have a very high risk of developing HNSCC. Proactive screening for malignancies is needed for the head and neck regions. We also found that chemoradiotherapy can be used safely in high-stage cancers.

Published

2022

24. Congenital thrombocytopenia associated with a heterozygous variant in the MEIS1 gene encoding a transcription factor essential for megakaryopoiesis.

Author

Steinberg-Shemer O, Orenstein N, Krasnov T, Noy-Lotan S, Marcoux N, Dgany O, Yacobovich J, Gilad O, Shabad E, Basel-Salmon L, and Tamary H

Subjects

Gene Expression Regulation, Humans, Myeloid Ecotropic Viral Integration Site 1 Protein genetics, Thrombopoiesis genetics, Thrombocytopenia genetics, Transcription Factors genetics

Abstract

The transcription factor MEIS1 (myeloid ectotrophic insertion site 1) is crucial for the maintenance of hematopoietic stem cells and for megakaryopoiesis. Germline variants in MEIS1 are associated with restless-leg syndrome, but were not previously shown to cause cytopenias. This is the first report of a patient with congenital thrombocytopenia associated with a sequence variant in MEIS1 , presenting with early onset severe thrombocytopenia and mild signs of bone marrow stress. Whole exome sequencing revealed a de novo monoallelic splice site variant in MEIS1 , NM&#95;002398.3:exon4:c.432 + 5 G > C, leading to a premature stop codon. We propose that heterozygous mutations in MEIS1 may cause congenital thrombocytopenia.

Published

2022

25. Pediatric myelodysplastic syndrome with inflammatory manifestations: Diagnosis, genetics, treatment, and outcome.

Author

Yanir AD, Krauss A, Stein J, Steinberg-Shemer O, Gilad O, Lotan SN, Dgany O, Krasnov T, Kodman Y, Feuerstein T, Mardoukh J, Fishman H, Geron I, Yacobovich J, Tamary H, Birger Y, Avrahami G, Izraeli S, and Birenboim SB

Subjects

Child, Humans, Mutation, Treatment Outcome, Trisomy, Hematopoietic Stem Cell Transplantation, Leukemia, Myelomonocytic, Juvenile diagnosis, Leukemia, Myelomonocytic, Juvenile genetics, Leukemia, Myelomonocytic, Juvenile therapy, Myelodysplastic Syndromes diagnosis, Myelodysplastic Syndromes genetics, Myelodysplastic Syndromes therapy

Abstract

Background: Inflammatory manifestations (IM) are well described in adult patients with myelodysplastic syndrome (MDS), but the presentation is highly variable and no standardized treatment exists. This phenomenon is rarely reported in children. As more pediatric patients are hematopoietic stem cell transplantation (HSCT) candidates, the role of anti-inflammatory treatment in relation to HSCT should be defined., Procedure: Here, we report a series of five children from a tertiary center. We describe the clinical presentation, molecular findings, and treatment options., Results: All patients presented with advanced MDS with blast percentages ranging 10-30%, all had severe IM. One patient had MDS secondary to severe congenital neutropenia, the other four patients had presumably primary MDS. All four were found to harbor a PTPN11 gene driver mutation, which is found in 35% of cases of juvenile myelomonocytic leukemia (JMML). The mutation was present in the myeloid lineage but not in T lymphocytes. Three had symptoms of Behcet's-like disease with trisomy 8 in their bone marrow. All patients were treated with anti-inflammatory medications (mainly systemic steroids) in an attempt to bring them to allogeneic HSCT in a better clinical condition. All demonstrated clinical improvement as well as regression in their MDS status post anti-inflammatory treatment. All have recovered from both MDS and their inflammatory symptoms post HSCT., Conclusion: Primary pediatric MDS with IM is driven in some cases by PTPN11 mutations, and might be on the clinical spectrum of JMML. Anti-inflammatory treatment may reverse MDS progression and improve the outcome of subsequent HSCT., (© 2021 Wiley Periodicals LLC.)

Published

2021

26. Cdan1 Is Essential for Primitive Erythropoiesis.

Author

Noy-Lotan S, Dgany O, Marcoux N, Atkins A, Kupfer GM, Bosques L, Gottschalk C, Steinberg-Shemer O, Motro B, and Tamary H

Abstract

Congenital dyserythropoietic anemia type I (CDA I) is an autosomal recessive disease characterized by moderate to severe macrocytic anemia and pathognomonic morphologic abnormalities of the erythroid precursors, including spongy heterochromatin. The disease is mainly caused by mutations in CDAN1 (encoding for Codanin-1). No patients with homozygous null type mutations have been described, and mouse null mutants die during early embryogenesis prior to the initiation of erythropoiesis. The cellular functions of Codanin-1 and the erythroid specificity of the phenotype remain elusive. To investigate the role of Codanin-1 in erythropoiesis, we crossed mice carrying the Cdan1 floxed allele (Cdan fl/fl ) with mice expressing Cre-recombinase under regulation of the erythropoietin receptor promoter (ErGFPcre). The resulting Cdan Δ Ery transgenic embryos died at mid-gestation (E12.5-E13.5) from severe anemia, with very low numbers of circulating erythroblast. Transmission electron microscopy studies of primitive erythroblasts (E9.5) revealed the pathognomonic spongy heterochromatin. The morphology of Cdan Δ Ery primitive erythroblasts demonstrated progressive development of dyserythropoiesis. Annexin V staining showed increases in both early and late-apoptotic erythroblasts compared to controls. Flow cytometry studies using the erythroid-specific cell-surface markers CD71 and Ter119 demonstrated that Cdan Δ Ery erythroid progenitors do not undergo the semi-synchronous maturation characteristic of primitive erythroblasts. Gene expression studies aimed to evaluate the effect of Cdan1 depletion on erythropoiesis revealed a delay of ζ to α globin switch compared to controls. We also found increased expression of Gata2 , Pu.1 , and Runx1 , which are known to inhibit terminal erythroid differentiation. Consistent with this data, our zebrafish model showed increased gata2 expression upon cdan1 knockdown. In summary, we demonstrated for the first time that Cdan1 is required for primitive erythropoiesis, while providing two experimental models for studying the role of Codanin-1 in erythropoiesis and in the pathogenesis of CDA type I., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Noy-Lotan, Dgany, Marcoux, Atkins, Kupfer, Bosques, Gottschalk, Steinberg-Shemer, Motro and Tamary.)

Published

2021

27. Incorporation of somatic panels for the detection of haematopoietic transformation in children and young adults with leukaemia predisposition syndromes and with acquired cytopenias.

Author

Noy-Lotan S, Krasnov T, Dgany O, Jeison M, Yanir AD, Gilad O, Toledano H, Barzilai-Birenboim S, Yacobovich J, Izraeli S, Tamary H, and Steinberg-Shemer O

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Humans, Infant, Male, Middle Aged, Young Adult, Cell Transformation, Neoplastic genetics, Genetic Predisposition to Disease, High-Throughput Nucleotide Sequencing, Leukemia, Myeloid, Acute genetics, Mutation, Myelodysplastic Syndromes genetics

Abstract

Detection of somatic mutations may help verify the diagnosis of myelodysplastic syndrome (MDS) in patients with persistent cytopenias or with MDS-predisposition syndromes, prior to the development of overt leukemia. However, the spectrum and consequences of acquired changes in paediatric patients have not been fully evaluated, and especially not in the context of an underlying syndrome. We incorporated a targeted next-generation-sequencing panel of 54 genes for the detection of somatic mutations in paediatric and young adult patients with inherited or acquired cytopenias. Sixty-five patients were included in this study, of whom 17 (26%) had somatic mutations. We detected somatic mutations in 20% of individuals with inherited MDS-predisposition syndromes, including in patients with severe congenital neutropenia and Fanconi anaemia, and with germline mutations in SAMD9L. Thirty-eight per cent of children with acquired cytopenias and suspected MDS had somatic changes, most commonly in genes related to signal transduction and transcription. Molecularly abnormal clones often preceded cytogenetic changes. Thus, routine performance of somatic panels can establish the diagnosis of MDS and determine the optimal timing of haematopoietic stem cell transplantation, prior to the development of leukaemia. In addition, performing somatic panels in patients with inherited MDS-predisposition syndromes may reveal their unique spectrum of acquired mutations., (© 2020 British Society for Haematology and John Wiley & Sons Ltd.)

Published

2021

28. Novel manifestations of immune dysregulation and granule defects in gray platelet syndrome.

Author

Sims MC, Mayer L, Collins JH, Bariana TK, Megy K, Lavenu-Bombled C, Seyres D, Kollipara L, Burden FS, Greene D, Lee D, Rodriguez-Romera A, Alessi MC, Astle WJ, Bahou WF, Bury L, Chalmers E, Da Silva R, De Candia E, Deevi SVV, Farrow S, Gomez K, Grassi L, Greinacher A, Gresele P, Hart D, Hurtaud MF, Kelly AM, Kerr R, Le Quellec S, Leblanc T, Leinøe EB, Mapeta R, McKinney H, Michelson AD, Morais S, Nugent D, Papadia S, Park SJ, Pasi J, Podda GM, Poon MC, Reed R, Sekhar M, Shalev H, Sivapalaratnam S, Steinberg-Shemer O, Stephens JC, Tait RC, Turro E, Wu JKM, Zieger B, Kuijpers TW, Whetton AD, Sickmann A, Freson K, Downes K, Erber WN, Frontini M, Nurden P, Ouwehand WH, Favier R, and Guerrero JA

Subjects

Biopsy, Blood Proteins genetics, Case-Control Studies, Cohort Studies, Cytoplasmic Granules metabolism, Diagnosis, Differential, Gene Frequency, Genetic Association Studies, Humans, Immune System physiology, Immune System Diseases blood, Immune System Diseases diagnosis, Immune System Diseases genetics, Immune System Diseases pathology, Mutation, Cytoplasmic Granules pathology, Genetic Heterogeneity, Gray Platelet Syndrome classification, Gray Platelet Syndrome genetics, Gray Platelet Syndrome immunology, Gray Platelet Syndrome pathology, Immune System pathology, Phenotype

Abstract

Gray platelet syndrome (GPS) is a rare recessive disorder caused by biallelic variants in NBEAL2 and characterized by bleeding symptoms, the absence of platelet α-granules, splenomegaly, and bone marrow (BM) fibrosis. Due to the rarity of GPS, it has been difficult to fully understand the pathogenic processes that lead to these clinical sequelae. To discern the spectrum of pathologic features, we performed a detailed clinical genotypic and phenotypic study of 47 patients with GPS and identified 32 new etiologic variants in NBEAL2. The GPS patient cohort exhibited known phenotypes, including macrothrombocytopenia, BM fibrosis, megakaryocyte emperipolesis of neutrophils, splenomegaly, and elevated serum vitamin B12 levels. Novel clinical phenotypes were also observed, including reduced leukocyte counts and increased presence of autoimmune disease and positive autoantibodies. There were widespread differences in the transcriptome and proteome of GPS platelets, neutrophils, monocytes, and CD4 lymphocytes. Proteins less abundant in these cells were enriched for constituents of granules, supporting a role for Nbeal2 in the function of these organelles across a wide range of blood cells. Proteomic analysis of GPS plasma showed increased levels of proteins associated with inflammation and immune response. One-quarter of plasma proteins increased in GPS are known to be synthesized outside of hematopoietic cells, predominantly in the liver. In summary, our data show that, in addition to the well-described platelet defects in GPS, there are immune defects. The abnormal immune cells may be the drivers of systemic abnormalities such as autoimmune disease., (© 2020 by The American Society of Hematology.)

Published

2020

29. Splenectomy in childhood for non-malignant haematologic disorders - long-term follow-up shows minimal adverse effects.

Author

Yacobovich J, Barzilai-Birenboim S, Steinberg-Shemer O, Stark P, Pazgal I, and Tamary H

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Follow-Up Studies, Humans, Iatrogenic Disease epidemiology, Infant, Male, Postoperative Complications epidemiology, Postoperative Complications etiology, Retrospective Studies, Hematologic Diseases epidemiology, Hematologic Diseases surgery, Splenectomy

Abstract

Splenectomy is considered therapeutic in various non-malignant haematologic diseases. Adverse events - specifically infections and thromboembolism - are not extensively documented in the paediatric population, maintaining the concern over risks-versus-benefits of the procedure. We studied a cohort of paediatric haematology patients undergoing splenectomy between 1977 and 2015 to determine short- and long-term complications. We summarised all the patients of the haematology clinic in our major Israeli tertiary centre undergoing splenectomy for therapeutic reasons, capturing infectious and thromboembolic events. The data of 103 patients, comprising 1657 follow-up years, were analysed. The cohort included 33 patients with transfusion-dependent thalassaemia, seven with non-transfusion-dependent thalassaemia, four with sickle-thalassaemia, 41 with hereditary spherocytosis, and 18 with immune thrombocytopenia. Standard presplenectomy vaccinations were noted in most. No typical cases of overwhelming postsplenectomy infection (OPSI) were identified, nor were typical OPSI bacteria isolated. Thalassaemics with central lines were most prone to infection and thrombosis. Beyond this subgroup, thrombotic events were anecdotal. This is the largest study to date to comprehensively analyse infectious and thrombotic complications of childhood splenectomy for the treatment of haematologic diseases. The use of splenectomy appears to be a relatively safe therapeutic option in paediatric patients with proper preoperative vaccination and follow-up care; use of central venous lines or catheters increase the risk in thalassaemic patients and should be avoided if possible., (© 2020 British Society for Haematology and John Wiley & Sons Ltd.)

Published

2020

30. Impact of Next-Generation Sequencing on the Diagnosis and Treatment of Congenital Anemias.

Author

Steinberg-Shemer O and Tamary H

Subjects

Anemia congenital, Genetic Counseling methods, Genetic Testing methods, Hemoglobinopathies diagnosis, Hemoglobinopathies genetics, High-Throughput Nucleotide Sequencing methods, Humans, Pathology, Molecular methods, Prenatal Diagnosis methods, Anemia diagnosis, Anemia genetics

Abstract

Congenital anemias are a wide spectrum of diseases including hypoproliferative anemia syndromes, dyserythropoietic anemias, sideroblastic anemias, red blood cell membrane and enzymatic defects, hemoglobinopathies, and thalassemia syndromes. The various congenital anemia syndromes may have similar clinical and laboratory presentations, making the diagnosis challenging. The traditional work-up, which includes a complete blood count, blood smears, bone marrow studies, flow cytometry, and the osmotic fragility test, does not always lead to the diagnosis. Specialized tests such as red blood cell enzyme activity and ektacytometry are not widely available. In addition, red blood cell transfusions may mask some of the laboratory characteristics. Therefore, genetic testing is crucial for accurate diagnosis of patients with congenital anemias. However, gene-by-gene testing is labor intensive because of the large number of genes involved. Thus, targeted next-generation sequencing using custom-made gene panels has been increasingly utilized, with a high success rate of diagnosis. Accurate genetic diagnosis is important for determining specific therapeutic modalities, as well as for avoiding splenectomy when contraindicated. In addition, molecular diagnosis can allow for genetic counseling and prenatal diagnosis in severe cases. We suggest a work-up scheme for patients with congenital anemias, including early incorporation of targeted next-generation sequencing panels.

Published

2020

31. Characterization and genotype-phenotype correlation of patients with Fanconi anemia in a multi-ethnic population.

Author

Steinberg-Shemer O, Goldberg TA, Yacobovich J, Levin C, Koren A, Revel-Vilk S, Ben-Ami T, Kuperman AA, Zemer VS, Toren A, Kapelushnik J, Ben-Barak A, Miskin H, Krasnov T, Noy-Lotan S, Dgany O, and Tamary H

Subjects

Fanconi Anemia Complementation Group A Protein genetics, Fanconi Anemia Complementation Group C Protein genetics, Genetic Association Studies, Humans, Israel, Mutation, Fanconi Anemia genetics

Abstract

Fanconi anemia (FA), an inherited bone marrow failure (BMF) syndrome, caused by mutations in DNA repair genes, is characterized by congenital anomalies, aplastic anemia, high risk of malignancies and extreme sensitivity to alkylating agents. We aimed to study the clinical presentation, molecular diagnosis and genotype-phenotype correlation among patients with FA from the Israeli inherited BMF registry. Overall, 111 patients of Arab (57%) and Jewish (43%) descent were followed for a median of 15 years (range: 0.1-49); 63% were offspring of consanguineous parents. One-hundred patients (90%) had at least one congenital anomaly; over 80% of the patients developed bone marrow failure; 53% underwent hematopoietic stem-cell transplantation; 33% of the patients developed cancer; no significant association was found between hematopoietic stem-cell transplant and solid tumor development. Nearly 95% of the patients tested had confirmed mutations in the Fanconi genes FANCA (67%), FANCC (13%), FANCG (14%), FANCJ (3%) and FANCD1 (2%), including twenty novel mutations. Patients with FANCA mutations developed cancer at a significantly older age compared to patients with mutations in other Fanconi genes (mean 18.5 and 5.2 years, respectively, P =0.001); however, the overall survival did not depend on the causative gene. We hereby describe a large national cohort of patients with FA, the vast majority genetically diagnosed. Our results suggest an older age for cancer development in patients with FANCA mutations and no increased incidence of solid tumors following hematopoietic stem-cell transplant. Further studies are needed to guide individual treatment and follow-up programs., (Copyright© 2020 Ferrata Storti Foundation.)

Published

2020

32. Congenital neutropenia with variable clinical presentation in novel mutation of the SRP54 gene.

Author

Goldberg L, Simon AJ, Rechavi G, Lev A, Barel O, Kunik V, Toren A, Schiby G, Tamary H, Steinberg-Shemer O, and Somech R

Subjects

Child, Preschool, Female, Humans, Infant, Male, Neutropenia genetics, Neutropenia metabolism, Pedigree, Prognosis, Proteomics, Exome Sequencing, Mutation, Neutropenia congenital, Neutropenia pathology, Signal Recognition Particle genetics

Abstract

Background: The SRP54 (signal recognition protein 54) is a conserved component of the ribonucleoprotein complex that mediates cotranslational targeting and translocation of proteins to the endoplasmic reticulum. In 2017, mutations in the gene have been described as a cause of congenital neutropenia with or without pancreatic insufficiency, and since then, only limited cases were added to the literature., Methods: Two patients with neutropenia underwent hematological, immunological, and genetic work-up, including lymphocyte phenotyping, immunoglobulins, and complement levels, antineutrophil and antinuclear antibodies, bone marrow FISH panel for myelodysplastic syndrome, whole-exome sequencing, and in silico proteomic analysis., Results: Clinical findings in the two families revealed a wide spectrum of immunological and clinical manifestations, ranging from mild asymptomatic neutropenia during febrile illnesses to severe neutropenia and life-threatening infection requiring leg amputation. Immunological and hematological work-up showed isolated neutropenia with normal lymphocyte subpopulations, immunoglobulin and complement levels, and negative autoimmune tests. Bone marrow aspirations showed variability ranging from normal myelopoiesis to myeloid maturation arrest at the promyelocytic stage, with normal FISH panel for myelodysplastic syndrome. Genetic analysis identified a novel, de novo, in-frame deletion in the SRP54 gene, c.342-344delAAC, p.T115del. In silico proteomic analysis suggested impaired SRP54 protein function due to reduced GTP activity and stability., Conclusions: We describe congenital neutropenia with variable clinical presentation in novel mutation of the SRP54 gene., (© 2020 Wiley Periodicals, Inc.)

Published

2020

33. Essential thrombocythemia A retrospective case series.

Author

Barg AA, Toren A, Tamary H, Yacobovich J, Steinberg-Shemer O, Gilad O, Goldstein G, Miskin H, Revel-Vilk S, Rosenbeg N, Kenet G, and Zemer VS

Subjects

Adolescent, Child, Child, Preschool, Female, Follow-Up Studies, Humans, Infant, Male, Retrospective Studies, Thrombocythemia, Essential therapy, Calreticulin genetics, Janus Kinase 2 genetics, Mutation, Receptors, Thrombopoietin genetics, Thrombocythemia, Essential genetics

Abstract

Background: Essential thrombocythemia (ET) is rare in children, and pediatric guidelines are lacking. Therefore, we aimed to evaluate ET diagnosis and treatment in a pediatric cohort., Procedure: Data of patients with ET from three hospitals were reviewed. Molecular diagnosis included JAK2V617F, CALR, and MPL mutations. Patients were evaluated for acquired von Willebrand syndrome (AVWS). Follow-up included clinical symptoms, adverse events, and treatment., Results: Twelve children (median age: 8 years, range 1-14.5) were included. Mean lag period between the first documentation of thrombocytosis until ET diagnosis was 36 months. Six patients were positive for JAK2V617F and two for CALR mutations. In six of nine patients, AVWS was diagnosed. At diagnosis, only 33% of patients started therapy with aspirin (n = 4) and hydroxyurea (n = 2). In three of eight untreated patients, therapy was added during follow-up. The cohort was followed for a median of 32.5 months (range: 4-108 months). Clinical follow-up disclosed vascular complications in 4 of 12 patients (deep vein thrombosis, n = 1; transient ischemic attack, n = 3). Two females experienced excessive bleeding; both were diagnosed with AVWS. Neither leukemia nor myelofibrosis evolved in our cohort., Conclusion: Increased awareness to pediatric ET is warranted, as delayed diagnosis is common. Compared to adults, AVWS may be more prevalent among children with ET., (© 2020 Wiley Periodicals, Inc.)

Published

2020

34. Alpha-Thalassemia Carrier due to -α3.7 Deletion: Not So Silent.

Author

Gilad O, Steinberg-Shemer O, Dgany O, Krasnov T, Noy-Lotan S, Tamary H, and Yacobovich J

Subjects

Adolescent, Child, Erythrocyte Indices, Heterozygote, Humans, Male, Mutation, alpha-Thalassemia, beta-Thalassemia

Abstract

Background/objective: Alpha-thalassemia is one of the most prevalent genetic diseases, with the -α3.7 deletion being the most common mutation. Molecular studies have suggested mechanisms to explain the mild phenotype of "silent carrier" heterozygotes. However, the correlation between the clinical laboratory picture and the -α3.7 heterozygous state remains unclear, thus we chose to investigate., Methods: We analyzed the medical files of 192 children evaluated for microcytosis at our tertiary center between 2007 and 2017 and diagnosed as heterozygotes for the -α3.7 deletion. Additional α-thalassemia mutations, iron deficiency anemia, and β-thalassemia were ruled out. Laboratory parameters were compared to age- and sex-matched reference values., Results: The -α3.7 carriers had significantly lower Hb and mean corpuscular volume (MCV) than the reference population, and significantly higher red blood cell counts across all age groups. The greatest reduction in Hb level appeared among male adolescents, while MCV was consistently 2 SDs lower than normal in most patients older than 2 years., Conclusion: Heterozygosity for the -α3.7 deletion was associated with clinically significant microcytosis and mild anemia in our pediatric population. In the absence of iron deficiency and β-thalassemia, this finding provides a diagnosis for mild microcytic anemia, making additional investigations of microcytosis unnecessary., (© 2020 S. Karger AG, Basel.)

Published

2020

35. Targeted next generation sequencing for the diagnosis of patients with rare congenital anemias.

Author

Shefer Averbuch N, Steinberg-Shemer O, Dgany O, Krasnov T, Noy-Lotan S, Yacobovich J, Kuperman AA, Kattamis A, Ben Barak A, Roth-Jelinek B, Chubar E, Shabad E, Dufort G, Ellis M, Wolach O, Pazgal I, Abu Quider A, Miskin H, and Tamary H

Subjects

Adolescent, Adult, Anemia blood, Anemia therapy, Anemia, Dyserythropoietic, Congenital diagnosis, Anemia, Dyserythropoietic, Congenital genetics, Anemia, Dyserythropoietic, Congenital therapy, Anemia, Hemolytic, Congenital diagnosis, Anemia, Hemolytic, Congenital genetics, Anemia, Hemolytic, Congenital Nonspherocytic diagnosis, Anemia, Hemolytic, Congenital Nonspherocytic genetics, Anemia, Sideroblastic diagnosis, Anemia, Sideroblastic genetics, Bone Marrow pathology, Child, Child, Preschool, Computational Biology, Erythrocyte Indices, Female, Genetic Predisposition to Disease, Genetic Testing, High-Throughput Nucleotide Sequencing, Humans, Hydrops Fetalis diagnosis, Hydrops Fetalis genetics, Male, Mutation, Pyruvate Kinase deficiency, Pyruvate Kinase genetics, Pyruvate Metabolism, Inborn Errors diagnosis, Pyruvate Metabolism, Inborn Errors genetics, Rare Diseases, Young Adult, Anemia congenital, Anemia diagnosis, Genetic Association Studies

Abstract

Background: Most patients with anemia are diagnosed through clinical phenotype and basic laboratory testing. Nonetheless, in cases of rare congenital anemias, some patients remain undiagnosed despite undergoing an exhaustive workup. Genetic testing is complicated by the large number of genes involved in rare anemias and the similarities in the clinical presentation of the different syndromes., Objective: We aimed to enhance the diagnosis of patients with congenital anemias by using targeted next-generation sequencing., Methods: Genetic diagnosis was performed by gene capture followed by next-generation sequencing of 76 genes known to cause anemia syndromes., Results: Genetic diagnosis was achieved in 13 out of 21 patients (62%). Six patients were diagnosed with pyruvate kinase deficiency, 4 with dehydrated hereditary stomatocytosis, 2 with sideroblastic anemia, and 1 with CDA type IV. Eight novel mutations were found. In 7 patients, the genetic diagnosis differed from the pretest presumed diagnosis. The mean lag time from presentation to diagnosis was over 13 years., Conclusions: Targeted next-generation sequencing led to an accurate diagnosis in over 60% of patients with rare anemias. These patients do not need further diagnostic workup. Earlier incorporation of this method into the workup of patients with congenital anemia may improve patients' care and enable genetic counseling., (© 2018 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2018

36. Labile plasma iron as an indicator of patient adherence to iron chelation treatment.

Author

Steinberg-Shemer O, Yacobovich J, Cohen M, Cabantchik IZ, and Tamary H

Subjects

Adolescent, Biomarkers, Blood Transfusion, Chelation Therapy, Child, Child, Preschool, Female, Ferritins blood, Humans, Iron Chelating Agents therapeutic use, Iron Overload drug therapy, Iron Overload etiology, Male, Prognosis, Sensitivity and Specificity, Transferrin metabolism, Treatment Outcome, Young Adult, Iron blood, Iron Overload blood, Iron Overload epidemiology, Medication Adherence

Abstract

Poor adherence of transfusion-dependent patients to chelation treatment is often the cause of persistent iron overload and ensuing morbidity. However, a tool to assess patient compliance with therapy is lacking in clinical practice. Labile plasma iron (LPI, the redox-active component of non-transferrin bound iron) has been studied as an indicator of systemic iron overload and of chelation efficacy, and may particularly reflect recent iron equilibrium. We considered the use of LPI as a potential indicator for recent chelation treatment in 18 transfusion-dependent pediatric patients. Samples were collected under chelation treatment or after a short interruption of the treatment, and LPI was measured by the FeROS assay (Aferrix, Tel Aviv, Israel). LPI was significantly higher after a short-term interruption of the chelation (median of 0.4 μM off-therapy [range:0-4] vs 0 μM on-therapy [range:0-2.8] (p < .001)). Conversely, serum iron, serum ferritin and calculated transferrin saturation were not significantly higher in the "off-therapy" samples compared to "on-therapy". In addition, in multivariate logistic regression analysis LPI was the variable most significantly associated with recent chelation treatment (p = .001). We conclude that LPI could serve as a useful indicator of compliance to chelation therapy., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

37. Gray platelet syndrome mimicking atypical autoimmune lymphoproliferative syndrome: the key is in the blood smear.

Author

Steinberg-Shemer O and Tamary H

Subjects

Autoimmune Lymphoproliferative Syndrome blood, Autoimmune Lymphoproliferative Syndrome pathology, Bone Marrow pathology, Consanguinity, Gray Platelet Syndrome blood, Gray Platelet Syndrome pathology, Humans, Siblings, Autoimmune Lymphoproliferative Syndrome diagnosis, Blood Platelets pathology, Gray Platelet Syndrome diagnosis

Published

2018

38. Mechanism for survival of homozygous nonsense mutations in the tumor suppressor gene BRCA1 .

Author

Seo A, Steinberg-Shemer O, Unal S, Casadei S, Walsh T, Gumruk F, Shalev S, Shimamura A, Akarsu NA, Tamary H, and King MC

Subjects

Adolescent, Adult, Breast Neoplasms pathology, Child, Child, Preschool, Female, Humans, Ovarian Neoplasms pathology, Pedigree, Alternative Splicing, BRCA1 Protein genetics, Breast Neoplasms genetics, Codon, Nonsense, Homozygote, Ovarian Neoplasms genetics

Abstract

BRCA1 is essential for repair of DNA double-strand breaks by homologous recombination, and hence for survival. Complete loss of its function is lethal during early embryonic development. Patients who are compound heterozygous for BRCA1 truncating mutations and missense alleles that retain some DNA repair capacity may survive, albeit with very high risk of early onset breast or ovarian cancer and features of Fanconi anemia. However, a mechanism enabling survival of patients homozygous for BRCA1 truncating mutations has not been described. We studied two unrelated families in which four children presented with multiple congenital anomalies and severe chromosomal fragility. One child developed T cell acute lymphocytic leukemia (ALL), and a second child developed neuroblastoma. Each of the four children was homozygous for a nonsense mutation in BRCA1 exon 11. Homozygosity for the nonsense mutations was viable thanks to the presence of a naturally occurring alternative splice donor in BRCA1 exon 11 that lies 5' of the mutations. The mutations did not affect the alternative splice site, but transcription from it produced an in-frame BRCA1 message with deletion of 3,309 bp. The translated BRCA1 protein was only 40% of normal length, but with intact N- and C-terminal sequences. These patients extend the range of BRCA1 -related phenotypes and illustrate how naturally occurring alternative splicing can enable survival, albeit with severe consequences, of otherwise lethal genotypes of an essential gene., Competing Interests: The authors declare no conflict of interest.

Published

2018

39. Whole-exome sequencing identifies an α-globin cluster triplication resulting in increased clinical severity of β-thalassemia.

Author

Steinberg-Shemer O, Ulirsch JC, Noy-Lotan S, Krasnov T, Attias D, Dgany O, Laor R, Sankaran VG, and Tamary H

Subjects

Exome genetics, Genotype, Humans, Male, Mutation genetics, Exome Sequencing methods, Young Adult, alpha-Globins metabolism, beta-Globins genetics, DNA Copy Number Variations genetics, alpha-Globins genetics, beta-Thalassemia genetics

Abstract

Whole-exome sequencing (WES) has been increasingly useful for the diagnosis of patients with rare causes of anemia, particularly when there is an atypical clinical presentation or targeted genotyping approaches are inconclusive. Here, we describe a 20-yr-old man with a lifelong moderate-to-severe anemia with accompanying splenomegaly who lacked a definitive diagnosis. After a thorough clinical workup and targeted genetic sequencing, we identified a paternally inherited β-globin mutation ( HBB :c.93-21G>A, IVS-I-110:G>A), a known cause of β-thalassemia minor. As this mutation alone was inconsistent with the severity of the anemia, we performed WES. Although we could not identify any relevant pathogenic single-nucleotide variants (SNVs) or small indels, copy-number variant (CNV) analyses revealed a likely triplication of the entire α-globin cluster, which was subsequently confirmed by multiplex ligation-dependent probe amplification. Treatment and follow-up was redefined according to the diagnosis of β-thalassemia intermedia resulting from a single β-thalassemia mutation in combination with an α-globin cluster triplication. Thus, we describe a case where the typical WES-based analysis of SNVs and small indels was unrevealing, but WES-based CNV analysis resulted in a definitive diagnosis that informed clinical decision-making. More generally, this case illustrates the value of performing CNV analysis when WES is otherwise unable to elucidate a clear genetic diagnosis., (© 2017 Steinberg-Shemer et al.; Published by Cold Spring Harbor Laboratory Press.)

Published

2017

40. Evaluating platelet function disorders in children with bleeding tendency - A single center study.

Author

Tanous O, Steinberg Shemer O, Yacobovich J, Zoldan M, Horovitz Y, Yaniv I, Rabizadeh E, Tamary H, Nakav S, and Lahav J

Subjects

Adenosine Diphosphate pharmacology, Adolescent, Arachidonic Acid pharmacology, Automation, Laboratory, Blood Platelets drug effects, Blood Platelets metabolism, Child, Child, Preschool, Epinephrine pharmacology, Female, Hemorrhage blood, Humans, Infant, Infant, Newborn, Male, Platelet Function Tests, Retrospective Studies, Severity of Illness Index, Blood Platelets pathology, Hemorrhage diagnosis, Platelet Aggregation drug effects

Abstract

Platelet function disorders (PFDs) are a common cause of mild bleeding tendency. However, they cannot be recognized by standard screening studies. The gold standard test for PFD is platelet aggregation, performed by light transmission aggregometry (LTA). A newer and less validated method is the closure time (CT), performed by the platelet function Analyzer 100 (PFA-100). Data regarding the validity of these tests in children are limited. The aim of this study was to evaluate the usefulness of LTA and PFA-100 for the diagnosis of pediatric patients with bleeding tendency. This retrospective study included patients one month-18 year old that had LTA tests performed at the coagulation laboratory of Rabin Medical Center between the years 2006-2015. Bleeding severity was assessed using a pediatric bleeding score. Patients were excluded from analysis if they had thrombocytopenia, thrombocytosis or coagulation factors deficiencies. One hundred and thirty-seven (137) patients were included in the analysis. The median age was 7.5 years (range one month-18 years). Most patients (93%) had a bleeding score of 2 or more. Abnormal LTA was found in 40% and prolonged CT in 23% of the patients. Abnormal LTA was significantly more common in patients with a bleeding score of 2 or more compared to patients with a lower bleeding scores (P = 0.04). No significant correlation was found between the bleeding severity and the number of agonists which induced abnormal responses (p = 0.52) or the CT (p = 0.35). Furthermore, no correlation was found between abnormal LTA and prolonged CT. To conclude, we were able to diagnose 40% of children who presented with bleeding tendency with platelet aggregation defects by LTA. Abnormal LTA was significantly more prevalent in patients with a bleeding score of 2 and above. In contrast, CT was not found to be sensitive as a screening tool for PFD. Therefore, our data extend the validity of the use of LTA for the evaluation of pediatric patients with bleeding tendency.

Published

2017

41. Diamond Blackfan Anemia: A Nonclassical Patient With Diagnosis Assisted by Genomic Analysis.

Author

Steinberg-Shemer O, Keel S, Dgany O, Walsh T, Noy-Lotan S, Krasnov T, Yacobovich J, Quarello P, Ramenghi U, King MC, Shimamura A, and Tamary H

Subjects

Adenosine Deaminase blood, Anemia, Diamond-Blackfan genetics, Female, Humans, Infant, Anemia, Diamond-Blackfan diagnosis, Mutation, Ribosomal Proteins genetics

Abstract

Diamond Blackfan anemia (DBA) is an inherited syndrome usually presenting with severe macrocytic anemia in infancy, paucity of erythroid precursors in the bone marrow, and congenital anomalies. We describe a child with mild, transfusion independent normocytic anemia whose diagnosis of DBA was established by identification of a novel de novo mutation disrupting normal splicing of the ribosomal protein RPL5. The diagnosis of DBA was confirmed by elevated erythrocyte adenosine deaminase levels and an abnormal ribosomal RNA profile. This case demonstrates the usefulness of genomic analysis in establishing the diagnosis of DBA in patients with a nonclassical presentation of the disease., Competing Interests: The authors declare no conflict of interest.

Published

2016

42. Anti-D treatment for pediatric immune thrombocytopenia: Is the bad reputation justified?

Author

Yacobovich J, Abu-Ahmed S, Steinberg-Shemer O, Goldberg T, Cohen M, and Tamary H

Subjects

Adolescent, Child, Child, Preschool, Humans, Infant, Purpura, Thrombocytopenic, Idiopathic drug therapy, Rho(D) Immune Globulin therapeutic use

Abstract

The purpose of this study was to assess the efficacy and side effect profile of the repeated use of anti-D for the treatment of pediatric immune thrombocytopenia (ITP) in a large pediatric hematology center. We performed a retrospective analysis of patient records for children (aged 4 months-18 years) treated for ITP at Schneider Children's Medical Center of Israel from 1995-2015. Demographic and clinical data, reported adverse events, and therapy response were extracted from written and electronic files for all patients having received anti-D. Therapy response was defined as time to platelet count >30 x 10(9)/L. Thirty-six patients received 170 treatments of anti-D at a dose of 75 μg/kg. The majority were previously treated with corticosteroids and/or intravenous immunoglobulin (IVIG). Minimal adverse events were recorded including fever (3.5%), vomiting (2.9%), and headaches (1.7%). Notably only 1/170 treatments required blood transfusion and no life-threatening events occurred. The average time to platelets >30 x 10(9)/L was 2.3 days, with a median of 1 day, range 1-12 days. Despite the reported severe adverse events in mainly elderly patients, the use of anti-D can be safe and effective in carefully chosen, low-risk pediatric patients with ITP., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

43. Targeted Application of Human Genetic Variation Can Improve Red Blood Cell Production from Stem Cells.

Author

Giani FC, Fiorini C, Wakabayashi A, Ludwig LS, Salem RM, Jobaliya CD, Regan SN, Ulirsch JC, Liang G, Steinberg-Shemer O, Guo MH, Esko T, Tong W, Brugnara C, Hirschhorn JN, Weiss MJ, Zon LI, Chou ST, French DL, Musunuru K, and Sankaran VG

Subjects

CRISPR-Cas Systems, Cell Differentiation, Cytokines metabolism, Embryonic Stem Cells cytology, Fetal Blood cytology, Genetic Techniques, Genetic Variation, Genome, Human, Hematopoietic Stem Cells cytology, Hemoglobins analysis, Humans, Mutation, Pluripotent Stem Cells cytology, Regenerative Medicine methods, Erythrocytes cytology, Stem Cells cytology

Abstract

Multipotent and pluripotent stem cells are potential sources for cell and tissue replacement therapies. For example, stem cell-derived red blood cells (RBCs) are a potential alternative to donated blood, but yield and quality remain a challenge. Here, we show that application of insight from human population genetic studies can enhance RBC production from stem cells. The SH2B3 gene encodes a negative regulator of cytokine signaling and naturally occurring loss-of-function variants in this gene increase RBC counts in vivo. Targeted suppression of SH2B3 in primary human hematopoietic stem and progenitor cells enhanced the maturation and overall yield of in-vitro-derived RBCs. Moreover, inactivation of SH2B3 by CRISPR/Cas9 genome editing in human pluripotent stem cells allowed enhanced erythroid cell expansion with preserved differentiation. Our findings therefore highlight the potential for combining human genome variation studies with genome editing approaches to improve cell and tissue production for regenerative medicine., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016