Your search keyword '"Seri, Marco"' showing total 32 results

1. Exome sequencing in 116 patients with inherited thrombocytopenia that remained of unknown origin after systematic phenotype-driven diagnostic workup.

Author

Marconi C, Pecci A, Palombo F, Melazzini F, Bottega R, Nardi E, Bozzi V, Faleschini M, Barozzi S, Giangregorio T, Magini P, Balduini CL, Savoia A, Seri M, Noris P, and Pippucci T

Subjects

Humans, Exome Sequencing, Phenotype, Genotype, Genetic Testing methods, Thrombocytopenia diagnosis, Thrombocytopenia genetics

Abstract

Inherited thrombocytopenias (IT) are genetic diseases characterized by low platelet count, sometimes associated with congenital defects or a predisposition to develop additional conditions. Next-generation sequencing has substantially improved our knowledge of IT, with more than 40 genes identified so far, but obtaining a molecular diagnosis remains a challenge especially for patients with non-syndromic forms, having no clinical or functional phenotypes that raise suspicion about specific genes. We performed exome sequencing (ES) in a cohort of 116 IT patients (89 families), still undiagnosed after a previously validated phenotype-driven diagnostic algorithm including a targeted analysis of suspected genes. ES achieved a diagnostic yield of 36%, with a gain of 16% over the diagnostic algorithm. This can be explained by genetic heterogeneity and unspecific genotype-phenotype relationships that make the simultaneous analysis of all the genes, enabled by ES, the most reasonable strategy. Furthermore, ES disentangled situations that had been puzzling because of atypical inheritance, sex-related effects or false negative laboratory results. Finally, ES-based copy number variant analysis disclosed an unexpectedly high prevalence of RUNX1 deletions, predisposing to hematologic malignancies. Our findings demonstrate that ES, including copy number variant analysis, can substantially contribute to the diagnosis of IT and can solve diagnostic problems that would otherwise remain a challenge.

Published

2023

2. Dysregulation of oncogenic factors by GFI1B p32: investigation of a novel GFI1B germline mutation.

Author

Faleschini M, Papa N, Morel-Kopp MC, Marconi C, Giangregorio T, Melazzini F, Bozzi V, Seri M, Noris P, Pecci A, Savoia A, and Bottega R

Subjects

Carcinogenesis, Humans, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins metabolism, Repressor Proteins genetics, Germ-Line Mutation, Thrombocytopenia genetics

Abstract

GFI1B is a transcription factor essential for the regulation of erythropoiesis and megakaryopoiesis, and pathogenic variants have been associated with thrombocytopenia and bleeding. Analysing thrombocytopenic families by whole exome sequencing, we identified a novel GFI1B variant (c.648+5G>A), which causes exon 9 skipping and overexpression of a shorter p32 isoform. We report the clinical data of our patients and critically review the phenotype observed in individuals with different GFI1B variants leading to the same effect on the p32 expression. Since p32 is increased in acute and chronic leukemia cells, we tested the expression level of genes playing a role in various type of cancers, including hematological tumors and found that they are significantly dysregulated, suggesting a potential role for GFI1B in carcinogenesis regulation. Increasing the detection of individuals with GFI1B variants will allow us to better characterize this rare disease and determine whether it is associated with an increased risk of developing malignancies.

Published

2022

3. Immune cytopenias as a continuum in inborn errors of immunity: An in-depth clinical and immunological exploration.

Author

Zama D, Conti F, Moratti M, Cantarini ME, Facchini E, Rivalta B, Rondelli R, Prete A, Ferrari S, Seri M, and Pession A

Subjects

Child, Humans, Retrospective Studies, Anemia, Hemolytic, Autoimmune diagnosis, Common Variable Immunodeficiency, Purpura, Thrombocytopenic, Idiopathic diagnosis, Purpura, Thrombocytopenic, Idiopathic genetics, Thrombocytopenia

Abstract

Background: Immune thrombocytopenia (ITP), autoimmune hemolytic anemia (AIHA), and autoimmune neutropenia (AIN) are disorders characterized by immune-mediated destruction of hematopoietic cell lineages. A link between pediatric immune cytopenias and inborn errors of immunity (IEI) was established in particular in the combined and chronic forms., Objective: Aim of this study is to provide clinical-immunological parameters to hematologists useful for a prompt identification of children with immune cytopenias deserving a deeper immunological and genetic evaluation., Methods: We retrospectively collected 47 pediatric patients with at least one hematological disorder among which persistent/chronic ITP, AIHA, and AIN, aged 0-18 years at onset of immune cytopenias and/or immune-dysregulation. The cohort was divided into two groups (IEI+ and IEI-), based on the presence/absence of underlying IEI diagnosis. IEI+ group, formed by 19/47 individuals, included: common variable immune deficiency (CVID; 9/19), autoimmune lymphoproliferative syndrome (ALPS; 4/19), DiGeorge syndrome (1/19), and unclassified IEI (5/19)., Results: IEI prevalence among patients with ITP, AIHA, AIN, and Evans Syndrome was respectively of 42%, 64%, 36%, and 62%. In IEI+ group the extended immunophenotyping identified the presence of statistically significant (p < .05) specific characteristics, namely T/B lymphopenia, decrease in naїve T-cells%, switched memory B-cells%, plasmablasts%, and/or immunoglobulins, increase in effector/central memory T-cells% and CD21low B-cells%. Except for DiGeorge and three ALPS patients, only 2/9 CVID patients had a molecular diagnosis for IEI: one carrying the pathogenic variant CR2:c.826delT, the likely pathogenic variant PRF1:c.272C> and the compound heterozygous TNFRSF13B variants p.Ser144Ter (pathogenic) and p.Cys193Arg (variant of uncertain significance), the other one carrying the likely pathogenic monoallelic variant TNFRSF13B:p.Ile87Asn., Conclusion: The synergy between hematologists and immunologists can improve and fasten diagnosis and management of patients with immune cytopenias through a wide focused clinical/immunophenotypical characterization, which identifies children worthy of IEI-related molecular analysis, favouring a genetic IEI diagnosis and potentially unveiling new targeted-gene variants responsible for IEI phenotype., (© 2021 The Authors. Immunity, Inflammation and Disease published by John Wiley & Sons Ltd.)

Published

2021

4. Pathogenetic and clinical study of a patient with thrombocytopenia due to the p.E527K gain-of-function variant of SRC.

Author

Barozzi S, Di Buduo CA, Marconi C, Bozzi V, Seri M, Romano F, Balduini A, and Pecci A

Subjects

Gain of Function Mutation, Humans, Anemia, Leukopenia, Thrombocytopenia diagnosis, Thrombocytopenia genetics

Published

2021

5. Loss-of-function mutations in PTPRJ cause a new form of inherited thrombocytopenia.

Author

Marconi C, Di Buduo CA, LeVine K, Barozzi S, Faleschini M, Bozzi V, Palombo F, McKinstry S, Lassandro G, Giordano P, Noris P, Balduini CL, Savoia A, Balduini A, Pippucci T, Seri M, Katsanis N, and Pecci A

Subjects

Adolescent, Adult, Animals, Blood Platelets metabolism, CRISPR-Cas Systems, Child, Female, Follow-Up Studies, Hematopoiesis, Humans, Male, Megakaryocytes metabolism, Middle Aged, Pedigree, Prognosis, Receptor-Like Protein Tyrosine Phosphatases, Class 3 antagonists & inhibitors, Receptor-Like Protein Tyrosine Phosphatases, Class 3 genetics, Thrombocytopenia etiology, Thrombocytopenia genetics, Zebrafish, Blood Platelets pathology, Genetic Predisposition to Disease, Megakaryocytes pathology, Mutation, Thrombocytopenia pathology

Abstract

Inherited thrombocytopenias (ITs) are a heterogeneous group of disorders characterized by low platelet count that may result in bleeding tendency. Despite progress being made in defining the genetic causes of ITs, nearly 50% of patients with familial thrombocytopenia are affected with forms of unknown origin. Here, through exome sequencing of 2 siblings with autosomal-recessive thrombocytopenia, we identified biallelic loss-of-function variants in PTPRJ . This gene encodes for a receptor-like PTP, PTPRJ (or CD148), which is expressed abundantly in platelets and megakaryocytes. Consistent with the predicted effects of the variants, both probands have an almost complete loss of PTPRJ at the messenger RNA and protein levels. To investigate the pathogenic role of PTPRJ deficiency in hematopoiesis in vivo, we carried out CRISPR/Cas9-mediated ablation of ptprja (the ortholog of human PTPRJ ) in zebrafish, which induced a significantly decreased number of CD41 + thrombocytes in vivo. Moreover, megakaryocytes of our patients showed impaired maturation and profound defects in SDF1-driven migration and formation of proplatelets in vitro. Silencing of PTPRJ mutations presented as a nonsyndromic thrombocytopenia characterized by spontaneous bleeding, small-sized platelets, and impaired platelet responses to the GPVI agonists collagen and convulxin. These platelet functional defects could be attributed to reduced activation of Src family kinases. Taken together, our data identify a new form of IT and highlight a hitherto unknown fundamental role for PTPRJ in platelet biogenesis.PTPRJ mutations presented as a nonsyndromic thrombocytopenia characterized by spontaneous bleeding, small-sized platelets, and impaired platelet responses to the GPVI agonists collagen and convulxin. These platelet functional defects could be attributed to reduced activation of Src family kinases. Taken together, our data identify a new form of IT and highlight a hitherto unknown fundamental role for PTPRJ in platelet biogenesis., (© 2019 by The American Society of Hematology.)

Published

2019

6. ACTN1 mutations lead to a benign form of platelet macrocytosis not always associated with thrombocytopenia.

Author

Faleschini M, Melazzini F, Marconi C, Giangregorio T, Pippucci T, Cigalini E, Pecci A, Bottega R, Ramenghi U, Siitonen T, Seri M, Pastore A, Savoia A, and Noris P

Subjects

Adult, Aged, Blood Cell Count, Blood Platelets pathology, Child, DNA Mutational Analysis methods, Erythrocytes, Abnormal pathology, Female, Hematologic Diseases blood, Hematologic Diseases pathology, Humans, Male, Middle Aged, Mutation, Missense, Pedigree, Platelet Aggregation, Thrombocytopenia blood, Actinin genetics, Hematologic Diseases genetics, Mutation, Thrombocytopenia genetics

Abstract

The inherited thrombocytopenias (IT) are a heterogeneous group of diseases resulting from mutations in more than 30 different genes. Among them, ACTN1-related thrombocytopenia (ACTN1-RT; Online Mendelian Inheritance in Man: 615193) is one of the most recently identified forms. It has been described as a mild autosomal dominant macrothrombocytopenia caused by mutations in ACTN1, a gene encoding for one of the two non-muscle isoforms of α-actinin. We recently identified seven new unrelated families with ACTN1-RT caused by different mutations. Two of them are novel missense variants (p.Trp128Cys and p.Pro233Leu), whose pathogenic role has been confirmed by in vitro studies. Together with the 10 families we have previously described, our cohort of ACTN1-RT now consists of 49 individuals carrying ACTN1 mutations. This is the largest case series ever collected and enabled a critical evaluation of the clinical aspects of the disease. We concluded that ACTN1-RT is the fourth most frequent form of IT worldwide and it is characterized by platelet macrocytosis in all affected subjects and mild thrombocytopenia in less than 80% of cases. The risk of bleeding, either spontaneous or upon haemostatic challenge, is negligible and there are no other associated defects, either congenital or acquired. Therefore, ACTN1-RT is a benign form of IT, whose diagnosis provides affected individuals and their families with a good prognosis., (© 2018 British Society for Haematology and John Wiley & Sons Ltd.)

Published

2018

7. A new form of inherited thrombocytopenia due to monoallelic loss of function mutation in the thrombopoietin gene.

Author

Noris P, Marconi C, De Rocco D, Melazzini F, Pippucci T, Loffredo G, Giangregorio T, Pecci A, Seri M, and Savoia A

Subjects

Female, Humans, Male, Alleles, Genetic Diseases, Inborn genetics, Mutation, Thrombocytopenia genetics, Thrombopoietin genetics

Published

2018

8. Clinical and pathogenic features of ETV6-related thrombocytopenia with predisposition to acute lymphoblastic leukemia.

Author

Melazzini F, Palombo F, Balduini A, De Rocco D, Marconi C, Noris P, Gnan C, Pippucci T, Bozzi V, Faleschini M, Barozzi S, Doubek M, Di Buduo CA, Kozubik KS, Radova L, Loffredo G, Pospisilova S, Alfano C, Seri M, Balduini CL, Pecci A, and Savoia A

Subjects

Adolescent, Adult, Cell Transformation, Neoplastic genetics, Child, Child, Preschool, Core Binding Factor Alpha 2 Subunit genetics, Family, Humans, Infant, Infant, Newborn, Intercellular Signaling Peptides and Proteins, Middle Aged, Mutation, Nuclear Proteins genetics, Pedigree, Thrombocytopenia pathology, Young Adult, ETS Translocation Variant 6 Protein, Genetic Predisposition to Disease genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma etiology, Proto-Oncogene Proteins c-ets genetics, Repressor Proteins genetics, Thrombocytopenia genetics

Abstract

ETV6-related thrombocytopenia is an autosomal dominant thrombocytopenia that has been recently identified in a few families and has been suspected to predispose to hematologic malignancies. To gain further information on this disorder, we searched for ETV6 mutations in the 130 families with inherited thrombocytopenia of unknown origin from our cohort of 274 consecutive pedigrees with familial thrombocytopenia. We identified 20 patients with ETV6-related thrombocytopenia from seven pedigrees. They have five different ETV6 variants, including three novel mutations affecting the highly conserved E26 transformation-specific domain. The relative frequency of ETV6-related thrombocytopenia was 2.6% in the whole case series and 4.6% among the families with known forms of inherited thrombocytopenia. The degree of thrombocytopenia and bleeding tendency of the patients with ETV6-related thrombocytopenia were mild, but four subjects developed B-cell acute lymphoblastic leukemia during childhood, resulting in a significantly higher incidence of this condition compared to that in the general population. Clinical and laboratory findings did not identify any particular defects that could lead to the suspicion of this disorder from the routine diagnostic workup. However, at variance with most inherited thrombocytopenias, platelets were not enlarged. In vitro studies revealed that the maturation of the patients' megakaryocytes was defective and that the patients have impaired proplatelet formation. Moreover, platelets from patients with ETV6-related thrombocytopenia have reduced ability to spread on fibrinogen. Since the dominant thrombocytopenias due to mutations in RUNX1 and ANKRD26 are also characterized by normal platelet size and predispose to hematologic malignancies, we suggest that screening for ETV6, RUNX1 and ANKRD26 mutations should be performed in all subjects with autosomal dominant thrombocytopenia and normal platelet size., (Copyright© Ferrata Storti Foundation.)

Published

2016

9. SLFN14-related thrombocytopenia: identification within a large series of patients with inherited thrombocytopenia.

Author

Marconi C, Di Buduo CA, Barozzi S, Palombo F, Pardini S, Zaninetti C, Pippucci T, Noris P, Balduini A, Seri M, and Pecci A

Subjects

Adult, Aged, Amino Acid Substitution, Base Sequence, Blood Platelets pathology, DNA Mutational Analysis, Female, Humans, Male, Mean Platelet Volume, Mutation, Missense, Pedigree, Thrombocytopenia blood, Exome Sequencing, Blood Proteins genetics, Thrombocytopenia genetics

Published

2016

10. ACTN1-related thrombocytopenia: identification of novel families for phenotypic characterization.

Author

Bottega R, Marconi C, Faleschini M, Baj G, Cagioni C, Pecci A, Pippucci T, Ramenghi U, Pardini S, Ngu L, Baronci C, Kunishima S, Balduini CL, Seri M, Savoia A, and Noris P

Subjects

Actinin metabolism, Adolescent, Adult, Aged, Aged, 80 and over, Blood Platelets pathology, Case-Control Studies, Child, Child, Preschool, Female, Gene Expression, Genotype, Heterozygote, Humans, Male, Middle Aged, Pedigree, Platelet Count, Severity of Illness Index, Thrombocytopenia metabolism, Thrombocytopenia pathology, Thrombocytopenia physiopathology, Thrombopoiesis genetics, Thrombopoietin blood, Actinin genetics, Blood Platelets metabolism, Mutation, Missense, Phenotype, Thrombocytopenia genetics

Abstract

Inherited thrombocytopenias (ITs) are a heterogeneous group of syndromic and nonsyndromic diseases caused by mutations affecting different genes. Alterations of ACTN1, the gene encoding for α-actinin 1, have recently been identified in a few families as being responsible for a mild form of IT (ACTN1-related thrombocytopenia; ACTN1-RT). To better characterize this disease, we screened ACTN1 in 128 probands and found 10 (8 novel) missense heterozygous variants in 11 families. Combining bioinformatics, segregation, and functional studies, we demonstrated that all but 1 amino acid substitution had deleterious effects. The clinical and laboratory findings of 31 affected individuals confirmed that ACTN1-RT is a mild macrothrombocytopenia with low risk for bleeding. Low reticulated platelet counts and only slightly increased serum thrombopoietin levels indicated that the latest phases of megakaryopoiesis were affected. Given its relatively high frequency in our cohort (4.2%), ACTN1-RT has to be taken into consideration in the differential diagnosis of ITs., (© 2015 by The American Society of Hematology.)

Published

2015

11. Platelet diameters in inherited thrombocytopenias: analysis of 376 patients with all known disorders.

Author

Noris P, Biino G, Pecci A, Civaschi E, Savoia A, Seri M, Melazzini F, Loffredo G, Russo G, Bozzi V, Notarangelo LD, Gresele P, Heller PG, Pujol-Moix N, Kunishima S, Cattaneo M, Bussel J, De Candia E, Cagioni C, Ramenghi U, Barozzi S, Fabris F, and Balduini CL

Subjects

Adolescent, Adult, Case-Control Studies, Cell Size, Child, Child, Preschool, Diagnosis, Differential, Female, Hearing Loss, Sensorineural blood, Hearing Loss, Sensorineural classification, Hearing Loss, Sensorineural genetics, Humans, Infant, Male, Middle Aged, Molecular Motor Proteins genetics, Mutation, Myosin Heavy Chains genetics, Purpura, Thrombocytopenic, Idiopathic blood, Purpura, Thrombocytopenic, Idiopathic diagnosis, Thrombocytopenia classification, Thrombocytopenia congenital, Young Adult, Blood Platelets pathology, Thrombocytopenia blood, Thrombocytopenia genetics

Abstract

Abnormalities of platelet size are one of the distinguishing features of inherited thrombocytopenias (ITs), and evaluation of blood films is recommended as an essential step for differential diagnosis of these disorders. Nevertheless, what we presently know about this subject is derived mainly from anecdotal evidence. To improve knowledge in this field, we evaluated platelet size on blood films obtained from 376 patients with all 19 forms of IT identified so far and found that these conditions differ not only in mean platelet diameter, but also in platelet diameter distribution width and the percentage of platelets with increased or reduced diameters. On the basis of these findings, we propose a new classification of ITs according to platelet size. It distinguishes forms with giant platelets, with large platelets, with normal or slightly increased platelet size, and with normal or slightly decreased platelet size. We also measured platelet diameters in 87 patients with immune thrombocytopenia and identified cutoff values for mean platelet diameter and the percentage of platelets with increased or reduced size that have good diagnostic accuracy in differentiating ITs with giant platelets and with normal or slightly decreased platelet size from immune thrombocytopenia and all other forms of IT., (© 2014 by The American Society of Hematology.)

Published

2014

12. MYH9-related disease: a novel prognostic model to predict the clinical evolution of the disease based on genotype-phenotype correlations.

Author

Pecci A, Klersy C, Gresele P, Lee KJ, De Rocco D, Bozzi V, Russo G, Heller PG, Loffredo G, Ballmaier M, Fabris F, Beggiato E, Kahr WH, Pujol-Moix N, Platokouki H, Van Geet C, Noris P, Yerram P, Hermans C, Gerber B, Economou M, De Groot M, Zieger B, De Candia E, Fraticelli V, Kersseboom R, Piccoli GB, Zimmermann S, Fierro T, Glembotsky AC, Vianello F, Zaninetti C, Nicchia E, Güthner C, Baronci C, Seri M, Knight PJ, Balduini CL, and Savoia A

Subjects

Adult, Age of Onset, Amino Acid Substitution, Female, Genotype, Hearing Loss, Sensorineural complications, Hearing Loss, Sensorineural diagnosis, Humans, Italy, Linear Models, Male, Mutation, Phenotype, Risk Factors, Thrombocytopenia complications, Thrombocytopenia diagnosis, Thrombocytopenia genetics, Cataract genetics, Genetic Association Studies, Hearing Loss, Sensorineural genetics, Molecular Motor Proteins genetics, Myosin Heavy Chains genetics, Thrombocytopenia congenital

Abstract

MYH9-related disease (MYH9-RD) is a rare autosomal-dominant disorder caused by mutations in the gene for nonmuscle myosin heavy chain IIA (NMMHC-IIA). MYH9-RD is characterized by a considerable variability in clinical evolution: patients present at birth with only thrombocytopenia, but some of them subsequently develop sensorineural deafness, cataract, and/or nephropathy often leading to end-stage renal disease (ESRD). We searched for genotype-phenotype correlations in the largest series of consecutive MYH9-RD patients collected so far (255 cases from 121 families). Association of genotypes with noncongenital features was assessed by a generalized linear regression model. The analysis defined disease evolution associated to seven different MYH9 genotypes that are responsible for 85% of MYH9-RD cases. Mutations hitting residue R702 demonstrated a complete penetrance for early-onset ESRD and deafness. The p.D1424H substitution associated with high risk of developing all the noncongenital manifestations of disease. Mutations hitting a distinct hydrophobic seam in the NMMHC-IIA head domain or substitutions at R1165 associated with high risk of deafness but low risk of nephropathy or cataract. Patients with p.E1841K, p.D1424N, and C-terminal deletions had low risk of noncongenital defects. These findings are essential to patients' clinical management and genetic counseling and are discussed in view of molecular pathogenesis of MYH9-RD., (© 2013 WILEY PERIODICALS, INC.)

Published

2014

13. ANKRD26-related thrombocytopenia and myeloid malignancies.

Author

Noris P, Favier R, Alessi MC, Geddis AE, Kunishima S, Heller PG, Giordano P, Niederhoffer KY, Bussel JB, Podda GM, Vianelli N, Kersseboom R, Pecci A, Gnan C, Marconi C, Auvrignon A, Cohen W, Yu JC, Iguchi A, Miller Imahiyerobo A, Boehlen F, Ghalloussi D, De Rocco D, Magini P, Civaschi E, Biino G, Seri M, Savoia A, and Balduini CL

Subjects

5' Untranslated Regions genetics, Acute Disease, Family Health, Genetic Predisposition to Disease genetics, Humans, Intercellular Signaling Peptides and Proteins, Mutation, Leukemia, Myelogenous, Chronic, BCR-ABL Positive genetics, Leukemia, Myeloid genetics, Myelodysplastic Syndromes genetics, Nuclear Proteins genetics, Thrombocytopenia genetics

Published

2013

14. Mutations responsible for MYH9-related thrombocytopenia impair SDF-1-driven migration of megakaryoblastic cells.

Author

Pecci A, Bozzi V, Panza E, Barozzi S, Gruppi C, Seri M, and Balduini CL

Subjects

Cell Adhesion genetics, Cell Line, Chemotaxis genetics, Chromosome Breakage, Chromosome Disorders pathology, Collagen Type I metabolism, Cytoskeleton genetics, Extracellular Matrix metabolism, Humans, Megakaryocyte Progenitor Cells pathology, Molecular Motor Proteins genetics, Mutation genetics, Myosin Heavy Chains genetics, Thrombocytopenia genetics, Thrombocytopenia pathology, Thrombocytopenia physiopathology, Thrombopoiesis genetics, Transgenes genetics, Chemokine CXCL12 metabolism, Chromosome Disorders genetics, Chromosome Disorders physiopathology, Cytoskeleton metabolism, Megakaryocyte Progenitor Cells metabolism, Molecular Motor Proteins metabolism, Myosin Heavy Chains metabolism, Thrombocytopenia congenital

Abstract

MYH9-related disease (MYH9-RD) is an autosomal-dominant thrombocytopenia caused by mutations in the gene for the heavy chain of non-muscle myosin-IIA (NMMHC-IIA). Recent in vitro studies led to the hypothesis that thrombocytopenia of MYH9-RD derives from an ectopic platelet release by megakaryocytes in the osteoblastic areas of bone marrow (BM), which are enriched in type I collagen, rather than in vascular spaces. SDF-1-driven migration of megakaryocytes within BM to reach the vascular spaces is a key mechanism for platelet biogenesis. Since myosin-IIA is implicated in polarised migration of different cell types, we hypothesised that MYH9 mutations could interfere with this mechanism. We therefore investigated the SDF-1-driven migration of a megakaryoblastic cell line, Dami cells, on type I collagen or fibrinogen by a modified transwell assay. Inhibition of myosin-IIA ATPase activity suppressed the SDF-1-driven migration of Dami cells, while over-expression of NMMHC-IIA increased the efficiency of chemotaxis, indicating a role for NMMHC-IIA in this mechanism. Transfection of cells with three MYH9 mutations frequently responsible for MYH9-RD (p.R702C, p.D1424H, or p.R1933X) resulted in a defective SDF-1-driven migration with respect to the wild-type counterpart and in increased cell spreading onto collagen. Analysis of differential localisation of wild-type and mutant proteins suggested that mutant NMMHC-IIAs had an impaired cytoplasmic re-organisation in functional cytoskeletal structures after cell adhesion to collagen. These findings support the hypothesis that a defect of SDF-1-driven migration of megakaryocytes induced by MYH9 mutations contributes to ectopic platelet release in the BM osteoblastic areas, resulting in ineffective platelet production.

Published

2011

15. Mutations in ANKRD26 are responsible for a frequent form of inherited thrombocytopenia: analysis of 78 patients from 21 families.

Author

Noris P, Perrotta S, Seri M, Pecci A, Gnan C, Loffredo G, Pujol-Moix N, Zecca M, Scognamiglio F, De Rocco D, Punzo F, Melazzini F, Scianguetta S, Casale M, Marconi C, Pippucci T, Amendola G, Notarangelo LD, Klersy C, Civaschi E, Balduini CL, and Savoia A

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Ankyrin Repeat genetics, Child, Cohort Studies, Female, Gene Frequency, Humans, Inheritance Patterns genetics, Male, Middle Aged, Mutation physiology, Pedigree, Transcription Factors physiology, Young Adult, Family, Thrombocytopenia genetics, Transcription Factors genetics

Abstract

Until recently, thrombocytopenia 2 (THC2) was considered an exceedingly rare form of autosomal dominant thrombocytopenia and only 2 families were known. However, we recently identified mutations in the 5'-untranslated region of the ANKRD26 gene in 9 THC2 families. Here we report on 12 additional pedigrees with ANKRD26 mutations, 6 of which are new. Because THC2 affected 21 of the 210 families in our database, it has to be considered one of the less rare forms of inherited thrombocytopenia. Analysis of all 21 families with ANKRD26 mutations identified to date revealed that thrombocytopenia and bleeding tendency were usually mild. Nearly all patients had no platelet macrocytosis, and this characteristic distinguishes THC2 from most other forms of inherited thrombocytopenia. In the majority of cases, platelets were deficient in glycoprotein Ia and α-granules, whereas in vitro platelet aggregation was normal. Bone marrow examination and serum thrombopoietin levels suggested that thrombocytopenia was derived from dysmegakaryopoiesis. Unexplained high values of hemoglobin and leukocytes were observed in a few cases. An unexpected finding that warrants further investigation was a high incidence of acute leukemia. Given the scarcity of distinctive characteristics, the ANKRD26-related thrombocytopenia has to be taken into consideration in the differential diagnosis of isolated thrombocytopenias.

Published

2011

16. Heavy chain myosin 9-related disease (MYH9 -RD): neutrophil inclusions of myosin-9 as a pathognomonic sign of the disorder.

Author

Savoia A, De Rocco D, Panza E, Bozzi V, Scandellari R, Loffredo G, Mumford A, Heller PG, Noris P, De Groot MR, Giani M, Freddi P, Scognamiglio F, Riondino S, Pujol-Moix N, Fabris F, Seri M, Balduini CL, and Pecci A

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Case-Control Studies, Child, Child, Preschool, DNA Mutational Analysis, Female, Fluorescent Antibody Technique, Humans, Inclusion Bodies pathology, Italy, Male, Microscopy, Fluorescence, Middle Aged, Molecular Motor Proteins genetics, Mutation, Myosin Heavy Chains genetics, Neutrophils pathology, Predictive Value of Tests, Prospective Studies, Registries, Sensitivity and Specificity, Thrombocytopenia blood, Thrombocytopenia genetics, Thrombocytopenia pathology, Young Adult, Inclusion Bodies metabolism, Molecular Motor Proteins blood, Myosin Heavy Chains blood, Neutrophils metabolism, Thrombocytopenia diagnosis

Abstract

MYH9-related disease ( MYH9-RD) is an autosomal dominant thrombocytopenia with giant platelets variably associated with young-adult onset of progressive sensorineural hearing loss, presenile cataract, and renal damage. MYH9-RD is caused by mutations of MYH9 , the gene encoding for non-muscle heavy-chain myosin-9. Wild-type and mutant myosin-9 aggregate as cytoplasmic inclusions in patients' leukocytes, the identification of which by immunofluorescence has been proposed as a suitable tool for the diagnosis of MYH9-RD. Since the predictive value of this assay, in terms of sensitivity and specificity, is unknown, we investigated 118 consecutive unrelated patients with a clinical presentation strongly consistent with MYH9-RD. All patients prospectively underwent both the immunofluorescence assay for myosin-9 aggregate detection and molecular genetic analysis of the MYH9 gene. Myosin-9 aggregates were identified in 82 patients, 80 of which (98%) had also a MYH9 mutation. In the remaining 36 patients neither myosin-9 aggregates nor MYH9 mutations were found. Sensitivity and specificity of the immunofluorescence assay was evaluated to be 100% and 95%, respectively. Except for the presence of aggregates, we did not find any other significant difference between patients with or without aggregates, demonstrating that the myosin-9 inclusions in neutrophils are a pathognomonic sign of the disease. However, the identification of the specific MYH9 mutation is still of importance for prognostic aspects of MYH9-RD.

Published

2010

17. Position of nonmuscle myosin heavy chain IIA (NMMHC-IIA) mutations predicts the natural history of MYH9-related disease.

Author

Pecci A, Panza E, Pujol-Moix N, Klersy C, Di Bari F, Bozzi V, Gresele P, Lethagen S, Fabris F, Dufour C, Granata A, Doubek M, Pecoraro C, Koivisto PA, Heller PG, Iolascon A, Alvisi P, Schwabe D, De Candia E, Rocca B, Russo U, Ramenghi U, Noris P, Seri M, Balduini CL, and Savoia A

Subjects

Adult, Cataract genetics, Female, Genes, Dominant, Genotype, Hearing Loss, Sensorineural genetics, Humans, Infant, Kaplan-Meier Estimate, Male, Middle Aged, Nephritis genetics, Phenotype, Platelet Count, Protein Structure, Tertiary, Syndrome, Thrombocytopenia blood, Molecular Motor Proteins chemistry, Molecular Motor Proteins genetics, Mutation, Myosin Heavy Chains chemistry, Myosin Heavy Chains genetics, Thrombocytopenia genetics

Abstract

MYH9-related disease (MYH9-RD) is a rare autosomal-dominant disorder caused by mutations in MYH9, the gene for the heavy chain of nonmuscle myosin IIA (NMMHC-IIA). All patients present from birth with macrothrombocytopenia, but in infancy or adult life, some of them develop sensorineural deafness, presenile cataracts, and/or progressive nephritis leading to end-stage renal failure. No consistent correlations have been identified between the 27 different MYH9 mutations identified so far and the variable clinical evolution of the disease. We have evaluated 108 consecutive MYH9-RD patients belonging to 50 unrelated pedigrees. The risk of noncongenital manifestations associated with different genotypes was estimated over time by event-free survival analysis. We demonstrated that all subjects with mutations in the motor domain of NMMHC-IIA present with severe thrombocytopenia and develop nephritis and deafness before the age of 40 years, while those with mutations in the tail domain have a much lower risk of noncongenital complications and significantly higher platelet counts. We also evaluated the clinical course of patients with mutations in the four most frequently affected residues of NMMHC-IIA (responsible for 70% of MYH9-RD cases). We concluded that mutations at residue 1933 do not induce kidney damage or cataracts and cause deafness only in the elderly, those in position 702 result in severe thrombocytopenia and produce nephritis and deafness at a juvenile age, while alterations at residue 1424 or 1841 result in intermediate clinical pictures. These findings are relevant not only to patients' clinical management but also to the elucidation of the pathogenesis of the disease.

Published

2008

18. Congenital amegakaryocytic thrombocytopenia: clinical and biological consequences of five novel mutations.

Author

Savoia A, Dufour C, Locatelli F, Noris P, Ambaglio C, Rosti V, Zecca M, Ferrari S, di Bari F, Corcione A, Di Stazio M, Seri M, and Balduini CL

Subjects

Amino Acid Sequence, Amino Acid Substitution, Blood Platelets metabolism, Child, Child, Preschool, Female, Humans, Infant, Male, Molecular Sequence Data, Sequence Homology, Amino Acid, Thrombocytopenia pathology, Thrombopoietin genetics, Megakaryocytes pathology, Mutation genetics, Receptors, Thrombopoietin genetics, Thrombocytopenia congenital, Thrombocytopenia genetics

Abstract

Background and Objectives: Congenital amegakaryocytic thrombocytopenia (CAMT) is a rare, autosomal recessive disorder induced by mutations of the gene coding for thrombopoietin (TPO) receptor (c-MPL). Patients initially present with isolated thrombocytopenia that subsequently progresses into pancytopenia. Although the mechanisms leading to aplasia are unknown, the age of onset has been reported to depend on the severity of the c-MPL functional defect. To improve our knowledge in this field, we studied clinical and biological features of five new patients., Design and Methods: We diagnosed five CAMT patients, identified c-MPL mutations, including five novel alterations and investigated relationships between mutations and their clinical-biological consequences., Results: In all cases, platelet c-MPL and bone marrow colonies were reduced, while serum TPO levels were elevated. We also documented that the percentage of bone marrow cells expressing tumor necrosis factor-a and interferon-g was increased during pancytopenia as compared to in controls, suggesting that, as in other bone marrow failure diseases, these inhibitory cytokines contributed to the pancytopenia. Contrary to previously published data, we found no evidence of correlations between different types of mutations and the clinical course., Interpretation and Conclusions: These results suggest that therapies, such as hematopoietic stem cell transplantation, which are potentially curative although associated with a risk of treatment-related mortality, should not be postponed even in those CAMT patients whose c-MPL mutations might predict residual activity of the TPO receptor.

Published

2007

19. Dissecting clinical findings: platelet defects segregate independently of deafness and cataract in a family affected by an apparent syndromic form of macrothrombocytopenia.

Author

Gangarossa S, Seri M, Pecci A, Di Bari F, Cusano R, Balduini C, Gasparini P, and Savoia A

Subjects

Connexin 26, Connexins genetics, DNA Mutational Analysis, Family Health, Female, Genetic Predisposition to Disease genetics, Humans, Italy, Male, Mutation, Missense, Pedigree, Syndrome, Thrombocytopenia pathology, Cataract genetics, Deafness genetics, Thrombocytopenia genetics

Abstract

We studied a family with a suspected diagnosis of MYH9-related disease, which is one of the most common forms of autosomal dominant macrothrombocytopenias associated with hearing impairment, cataracts and nephritis. No mutation of the MYH9 gene was identified. Moreover, the A156V variant of the GPIbalpha gene, responsible for 30% of macrothrombocytopenias in Italy, was not detected in the family. Therefore, we hypothesized that the clinical symptoms were caused by mutations in different genes. The screening of the candidate genes for deafness and/or cataract allowed us to identify two variants, M34T and S19T, of the GJB2 gene in family members with hearing impairment. Because of the relatively common occurrence of inherited hearing loss and, at least in the Mediterranean area, of platelet macrocytosis, the two traits occurred by chance in the same family and mimicked the MYH9-related disease.

Published

2005

20. Defective expression of GPIb/IX/V complex in platelets from patients with May-Hegglin anomaly and Sebastian syndrome.

Author

Di Pumpo M, Noris P, Pecci A, Savoia A, Seri M, Ceresa IF, and Balduini CL

Subjects

Blood Platelet Disorders genetics, Blood Platelets pathology, Female, Flow Cytometry, Genetic Predisposition to Disease, Humans, Leukocytes metabolism, Leukocytes pathology, Male, Molecular Motor Proteins genetics, Mutation, Myosin Heavy Chains genetics, Nonmuscle Myosin Type IIA genetics, Syndrome, Thrombocytopenia pathology, Blood Platelet Disorders metabolism, Blood Platelet Disorders pathology, Blood Platelets metabolism, Platelet Glycoprotein GPIb-IX Complex metabolism, Thrombocytopenia metabolism

Abstract

Background and Objectives: May-Hegglin anomaly (MHA) and Sebastian syndrome (SBS) are inherited macrothrombocytopenias with D hle-like bodies in leukocytes. MHA-SBS are due to mutations of the gene (MYH9) for the heavy chain of non-muscle myosin IIA (NMMHC-IIA), the only myosin II expressed in platelets. The bleeding tendency is often more severe than expected on the basis of platelet count, but no abnormality of platelet function has been identified. To characterize platelet abnormalities deriving from MYH9 mutations better, we studied surface glycoproteins (GPs) in platelets from MHA-SBS patients., Design and Methods: Eight patients from 4 unrelated families were studied. Platelet surface GPs were studied by flow cytometry in both the whole platelet population and subpopulations of platelets identified according to their size., Results: Flow cytometry identified a defect of the GPIb/IX/V complex in the whole platelet population in 7 of 8 patients. Moreover, in all patients the subpopulation of large platelets had defective expression of this complex., Interpretation and Conclusions: These findings indicate that MYH9 mutations may be responsible for reduced surface expression of GPIb/IX/V. This defect could contribute to the bleeding tendency of these patients. The identification of a GPIb/IX/V defect in MHA-SBS platelets raises the question of the differential diagnosis from heterozygous Bernard-Soulier syndrome.

Published

2002

21. Immunocytochemistry for the heavy chain of the non-muscle myosin IIA as a diagnostic tool for MYH9-related disorders.

Author

Pecci A, Noris P, Invernizzi R, Savoia A, Seri M, Ghiggeri GM, Sartore S, Gangarossa S, Bizzaro N, and Balduini CL

Subjects

Case-Control Studies, Humans, Immunohistochemistry methods, Mutation, Myosin Heavy Chains genetics, Thrombocytopenia genetics, Blood Platelets chemistry, Leukocytes chemistry, Molecular Motor Proteins, Myosin Heavy Chains analysis, Nonmuscle Myosin Type IIA analysis, Thrombocytopenia diagnosis

Abstract

May-Hegglin anomaly (MHA), Sebastian syndrome (SBS) and Fechtner syndrome (FTNS) are autosomal-dominant macrothrombocytopenias with Döhle-like leucocyte inclusions. These diseases are due to mutations of the MHY9 gene, encoding the heavy chain of non-muscle myosin IIA (NMMHC-A). We investigated the NMMHC-A localization in blood cells from eight MHA, SBS or FTNS patients with known MYH9 mutations. All the patients showed an altered localization of NMMHC-A in granulocytes and platelets, suggesting that Döhle-like bodies are due to the aggregation of NMMHC-A in the cytoplasm. Therefore, immunocytochemistry for NMMHC-A is a simple and sensitive method to detect pathological phenotypes of granulocytes and platelets in the diagnosis of MYH9-related disorders.

Published

2002

22. Dysregulation of oncogenic factors by GFI1B p32: investigation of a novel GFI1B germline mutation

Author

Faleschini, Michela, Papa, Nicole, Morel-Kopp, Marie-Christine, Marconi, Caterina, Giangregorio, Tania, Melazzini, Federica, Bozzi, Valeria, Seri, Marco, Noris, Patrizia, Pecci, Alessandro, Savoia, Anna, Bottega, Roberta, Faleschini, Michela, Papa, Nicole, Morel-Kopp, Marie-Christine, Marconi, Caterina, Giangregorio, Tania, Melazzini, Federica, Bozzi, Valeria, Seri, Marco, Noris, Patrizia, Pecci, Alessandro, Savoia, Anna, and Bottega, Roberta

Subjects

Repressor Proteins, Carcinogenesis, GFI1B, thrombocytopenia, Proto-Oncogene Proteins, Humans, GFI1B, germline mutation, Article, Germ-Line Mutation

Abstract

GFI1B is a transcription factor essential for the regulation of erythropoiesis and megakaryopoiesis, and pathogenic variants have been associated with thrombocytopenia and bleeding. Analysing thrombocytopenic families by whole exome sequencing, we identified a novel GFI1B variant (c.648+5G>A), which causes exon 9 skipping and overexpression of a shorter p32 isoform. We report the clinical data of our patients and critically review the phenotype observed in individuals with different GFI1B variants leading to the same effect on the p32 expression. Since p32 is increased in acute and chronic leukemia cells, we tested the expression level of genes playing a role in various type of cancers, including hematological tumors and found that they are significantly dysregulated, suggesting a potential role for GFI1B in carcinogenesis regulation. Increasing the detection of individuals with GFI1B variants will allow us to better characterize this rare disease and determine whether it is associated with an increased risk of developing malignancies.

Published

2022

23. Mutations Identified in Thrombocytopenia THC2 Are Likely to Dysregulate ANKRD26 Expression

Author

Erica Valencic, Shinji Kunishima, Akihiro Iguchi, Anna Savoia, Silverio Perrotta, Felisa C. Molinas, Alessandro Pecci, Chiara Gnan, Carlo L. Balduini, Paula G. Heller, Seri Marco, Patrizia Noris, Brian Cannon, Gnan, Chiara, Patrizia, Nori, Felisa C., Molina, Shinji, Kunishima, Paula Graciela, Heller, Akihiro, Iguchi, Alessandro, Pecci, Erica, Valencic, Seri, Marco, Silverio, Perrotta, Carlo Luigi, Balduini, and Savoia, Anna

Subjects

Genetics, Untranslated region, Reporter gene, ANKRD26, Immunology, Luciferase assay, Wild type, Thrombocytopenia, 5'UTR, Promoter, Cell Biology, Hematology, Transfection, Biology, Biochemistry, Molecular biology, Luciferase, Gene, Thrombopoietin

Abstract

Abstract 708 Thrombocytopenia 2 (THC2, MIM 188000) is an autosomal dominant form of thrombocytopenia described for the first time in a large Italian family, which allowed us to map a locus on 10p11.1-p12. Since the recent identification of ANKRD26 (Pippucci et al, Am J Hum Genet 88:115, 2011), as the gene responsible for the disease, the screening led to recognition of 25 families (91 patients). Although most families were of Italian origin, patients were also from North America, Argentina, Senegal, Japan and Spain, indicating that the disease is distributed worldwide. Confirming recently published data (Noris et al, Blood 117:6673, 2011), this cohort showed that thrombocytopenia was moderate and bleeding tendency was usually mild. Most patients were characterized by deficiency of both glycoprotein Ia and a-granules but normal platelet aggregation in vitro. Bone marrow examination and serum thrombopoietin levels were indicative of dysmegakaryopoiesis. Moreover, there was evidence of leukemia risk in patients with ANKRD26 mutations. The 12 mutations identified so far are all localized in a short stretch of 22 nucleotides of the 5' untranslated region (5'UTR). The effect of three mutations was evaluated in a reporter gene assay with the luciferase gene under the control of the wild type and mutated 5'UTR. When constructs were transfected in K562 and undifferentiated DAMI cell lines, no significant difference in luciferase activity was observed. However, when the constructs were transfected in megakaryocytes obtained from differentiation of the DAMI cells, a significant increase in activity was reported, suggesting that the 5'UTR plays a regulatory role of the ANKRD26 expression during megakaryopoiesis (Pippucci et al, Am J Hum Genet 88:115, 2011). To further investigate the mechanisms responsible for the ANKRD26 expression, we tested the activity of a putative regulatory region (730 bp), containing 574 bp upstream of the transcription initiation site and the 5'UTR. The effect of two mutations (c.-128G>A and c.-116C>T) was evaluated in both orientations using a luciferase assay in HeLa cells. There was no significant difference between wild type and mutated inserts cloned in either sense or antisense orientation, though there was a slight transcriptional increase of the sense mutated constructs and a reduction of the antisense mutated sequences in comparison with the wild type inserts. In order to test the promoter region in a more suitable model, the same constructs were transfected in DAMI differentiated megakaryocytes. Whereas the antisense wild type and mutated constructs did not show any transcriptional activity, the sense mutated constructs generated a statistically significant increase of activity, suggesting that the mechanisms controlling the expression of ANKRD26 are different in the two cell lines. The role of 5'UTR was further investigated by testing a fragment (574 bp) in which 5'UTR was deleted. In megakaryocytes, this sequence generated a statistically significant increase of the luciferase activity compared to the 730 bp insert. On the contrary, the same constructs transfected in Hela cells resulted in a reduction of the luciferase activity. From these preliminary data we hypothesize that the 5'UTR region plays an important role inhibiting the ANKRD26 expression during megakaryopoiesis through the binding of factors, whose recognition sites are destroyed by mutations identified in patients. Consistent with this hypothesis, ANKRD26 is expressed in human CD34+ and BFU-E but hardly detectable in CD41+ cells. Disclosures: No relevant conflicts of interest to declare.

Published

2011

24. 5'UTR point substitutions and N-terminal truncating mutations of ANKRD26 in acute myeloid leukemia.

Author

Marconi, Caterina, Canobbio, Ilaria, Bozzi, Valeria, Pippucci, Tommaso, Simonetti, Giorgia, Melazzini, Federica, Angori, Silvia, Martinelli, Giovanni, Saglio, Giuseppe, Torti, Mauro, Pastan, Ira, Seri, Marco, and Pecci, Alessandro

Subjects

GENETIC mutation, MYELOID leukemia genetics, THROMBOCYTOPENIA, NUCLEOTIDES, GENETIC overexpression, BONE marrow transplantation

Abstract

Thrombocytopenia 2 (THC2) is an inherited disorder caused by monoallelic single nucleotide substitutions in the 5’UTR of the ANKRD26 gene. Patients have thrombocytopenia and increased risk of myeloid malignancies, in particular, acute myeloid leukemia (AML). Given the association of variants in the ANKRD26 5’UTR with myeloid neoplasms, we investigated whether, and to what extent, mutations in this region contribute to apparently sporadic AML. To this end, we studied 250 consecutive, non-familial, adult AML patients and screened the first exon of ANKRD26 including the 5’UTR. We found variants in four patients. One patient had the c.−125T>G substitution in the 5’UTR, while three patients carried two different variants in the 5’ end of the ANKRD26 coding region (c.3G>A or c.105C>G). Review of medical history showed that the patient carrying the c.−125T>G was actually affected by typical but unrecognized THC2, highlighting that some apparently sporadic AML cases represent the evolution of a well-characterized familial predisposition disorder. As regards the c.3G>A and the c.105C>G, we found that both variants result in the synthesis of N-terminal truncated ANKRD26 isoforms, which are stable and functional in cells, in particular, have a strong ability to activate the MAPK/ERK signaling pathway. Moreover, investigation of one patient with the c.3G>A showed that mutation was associated with strong ANKRD26 overexpression in vivo, which is the proposed mechanism for predisposition to AML in THC2 patients. These data provide evidence that N-terminal ANKRD26 truncating mutations play a potential pathogenetic role in AML. Recognition of AML patients with germline ANKRD26 pathogenetic variants is mandatory for selection of donors for bone marrow transplantation. [ABSTRACT FROM AUTHOR]

Published

2017

25. MYH9 related disease: four novel mutations of the tail domain of myosin-9 correlating with a mild clinical phenotype.

Author

Pecci, Alessandro, Panza, Emanuele, De Rocco, Daniela, Pujol-Moix, Nuria, Girotto, Giorgia, Podda, Luigi, Paparo, Carmelo, Bozzi, Valeria, Pastore, Annalisa, Balduini, Carlo L., Seri, Marco, and Savoia, Anna

Subjects

NEUTROPHILS, KIDNEY diseases, PHENOTYPES, DISEASE susceptibility, POLYCYSTIC kidney disease, MYOSIN, THROMBOCYTOPENIA

Abstract

MYH9-related disease ( MYH9-RD) is a rare autosomal dominant disorder caused by mutations in MYH9, the gene encoding the heavy chain of non-muscle myosin IIA. All patients present congenital macrothrombocytopenia and inclusion bodies in neutrophils. Some of them can also develop sensorineural deafness, presenile cataract, and/or progressive nephropathy leading to end-stage renal failure. We report four families, each with a novel mutation: two missense mutations, in exons 31 and 32, and two out of frame deletions in exon 40. They were associated with no bleeding diathesis, normal, or only slightly reduced platelet count and no extra-hematological manifestations, confirming that alterations of the tail domain cause a mild form of MYH9-RD with no clinically relevant defects. [ABSTRACT FROM AUTHOR]

Published

2010

26. ACTN1 mutations lead to a benign form of platelet macrocytosis not always associated with thrombocytopenia

Author

Caterina Marconi, Marco Seri, Roberta Bottega, Annalisa Pastore, Michela Faleschini, Federica Melazzini, Elena Cigalini, Tania Giangregorio, Alessandro Pecci, Tommaso Pippucci, Patrizia Noris, Ugo Ramenghi, Anna Savoia, Timo Siitonen, Faleschini, Michela, Melazzini, Federica, Marconi, Caterina, Giangregorio, Tania, Pippucci, Tommaso, Cigalini, Elena, Pecci, Alessandro, Bottega, Roberta, Ramenghi, Ugo, Siitonen, Timo, Seri, Marco, Pastore, Annalisa, Savoia, Anna, and Noris, Patrizia

Subjects

Adult, Blood Platelets, Male, 0301 basic medicine, medicine.medical_specialty, Erythrocytes, Platelet Aggregation, DNA Mutational Analysis, Autosomal dominant macrothrombocytopenia, Mutation, Missense, Erythrocytes, Abnormal, thrombocytopenia, Macrocytosis, Disease, 03 medical and health sciences, 0302 clinical medicine, ACTN1-related thrombocytopenia, ACTN1 gene, macrocytosis, mutations, Actinin, Aged, Blood Cell Count, Child, Female, Hematologic Diseases, Humans, Middle Aged, Pedigree, Thrombocytopenia, Mutation, Internal medicine, medicine, OMIM : Online Mendelian Inheritance in Man, Missense mutation, Gene, macrocytosi, Hematology, business.industry, medicine.disease, 030104 developmental biology, Immunology, Cohort, Abnormal, Missense, mutation, business, 030215 immunology

Abstract

The inherited thrombocytopenias (IT) are a heterogeneous group of diseases resulting from mutations in more than 30 different genes. Among them, ACTN1-related thrombocytopenia (ACTN1-RT; Online Mendelian Inheritance in Man: 615193) is one of the most recently identified forms. It has been described as a mild autosomal dominant macrothrombocytopenia caused by mutations in ACTN1, a gene encoding for one of the two non-muscle isoforms of alpha-actinin. We recently identified seven new unrelated families with ACTN1-RT caused by different mutations. Two of them are novel missense variants (p.Trp128Cys and p.Pro233Leu), whose pathogenic role has been confirmed by in vitro studies. Together with the 10 families we have previously described, our cohort of ACTN1-RT now consists of 49 individuals carrying ACTN1 mutations. This is the largest case series ever collected and enabled a critical evaluation of the clinical aspects of the disease. We concluded that ACTN1-RT is the fourth most frequent form of IT worldwide and it is characterized by platelet macrocytosis in all affected subjects and mild thrombocytopenia in less than 80% of cases. The risk of bleeding, either spontaneous or upon haemostatic challenge, is negligible and there are no other associated defects, either congenital or acquired. Therefore, ACTN1-RT is a benign form of IT, whose diagnosis provides affected individuals and their families with a good prognosis.

Published

2018

27. Loss-of-function mutations in PTPRJ cause a new form of inherited thrombocytopenia

Author

Caterina Marconi, Christian A. Di Buduo, Serena Barozzi, Carlo L. Balduini, Spencer U. McKinstry, Alessandro Pecci, Alessandra Balduini, Patrizia Noris, Paola Giordano, Nicholas Katsanis, Kellie LeVine, Marco Seri, Michela Faleschini, Tommaso Pippucci, Anna Savoia, Flavia Palombo, Giuseppe Lassandro, Valeria Bozzi, Marconi, Caterina, Di Buduo, Christian A, Levine, Kellie, Barozzi, Serena, Faleschini, Michela, Bozzi, Valeria, Palombo, Flavia, Mckinstry, Spencer, Lassandro, Giuseppe, Giordano, Paola, Noris, Patrizia, Balduini, Carlo L, Savoia, Anna, Balduini, Alessandra, Pippucci, Tommaso, Seri, Marco, Katsanis, Nichola, Pecci, Alessandro, LeVine, Kellie, and McKinstry, Spencer

Subjects

0301 basic medicine, Immunology, 030204 cardiovascular system & hematology, Biology, medicine.disease_cause, Biochemistry, inherited thrombocytopenia, ptprj, src signalling disruption, 03 medical and health sciences, 0302 clinical medicine, Megakaryocyte, medicine, Platelet, Exome sequencing, Loss function, gene identification, Thrombocytopenia, PTPRJ, Mutation, PTPRJ Gene, Convulxin, Cell Biology, Hematology, 030104 developmental biology, medicine.anatomical_structure, Cancer research, GPVI

Abstract

Inherited thrombocytopenias (ITs) are a heterogeneous group of disorders characterized by low platelet count that may result in bleeding tendency. Despite progress being made in defining the genetic causes of ITs, nearly 50% of patients with familial thrombocytopenia are affected with forms of unknown origin. Here, through exome sequencing of 2 siblings with autosomal-recessive thrombocytopenia, we identified biallelic loss-of-function variants in PTPRJ. This gene encodes for a receptor-like PTP, PTPRJ (or CD148), which is expressed abundantly in platelets and megakaryocytes. Consistent with the predicted effects of the variants, both probands have an almost complete loss of PTPRJ at the messenger RNA and protein levels. To investigate the pathogenic role of PTPRJ deficiency in hematopoiesis in vivo, we carried out CRISPR/Cas9-mediated ablation of ptprja (the ortholog of human PTPRJ) in zebrafish, which induced a significantly decreased number of CD41+ thrombocytes in vivo. Moreover, megakaryocytes of our patients showed impaired maturation and profound defects in SDF1-driven migration and formation of proplatelets in vitro. Silencing of PTPRJ in a human megakaryocytic cell line reproduced the functional defects observed in patients’ megakaryocytes. The disorder caused by PTPRJ mutations presented as a nonsyndromic thrombocytopenia characterized by spontaneous bleeding, small-sized platelets, and impaired platelet responses to the GPVI agonists collagen and convulxin. These platelet functional defects could be attributed to reduced activation of Src family kinases. Taken together, our data identify a new form of IT and highlight a hitherto unknown fundamental role for PTPRJ in platelet biogenesis.

Published

2019

28. A new form of inherited thrombocytopenia due to monoallelic loss of function mutation in the thrombopoietin gene

Author

Federica Melazzini, Giuseppe Loffredo, Tania Giangregorio, Tommaso Pippucci, Patrizia Noris, Caterina Marconi, Daniela De Rocco, Anna Savoia, Marco Seri, Alessandro Pecci, Noris, Patrizia, Marconi, Caterina, DE ROCCO, Daniela, Melazzini, Federica, Pippucci, Tommaso, Loffredo, Giuseppe, Giangregorio, Tania, Pecci, Alessandro, Seri, Marco, Savoia, Anna, and De Rocco, Daniela

Subjects

0301 basic medicine, Male, THPO gene, 030204 cardiovascular system & hematology, platelet genetic diseases, Loss of function mutation, 03 medical and health sciences, 0302 clinical medicine, Medicine, thrombopoietin, Humans, genetic disorders, platelets, Platelet, Thrombopoietin Gene, platelet genetic disease, Thrombopoietin, Alleles, platelet, business.industry, Genetic Diseases, Inborn, Hematology, Thrombocytopenia, 030104 developmental biology, Mutation, Cancer research, genetic disorder, Female, business

Abstract

Thrombopoietin (THPO) is an essential regulator of haemopoiesis that is required for the maintenance of haemopoietic progenitors and their differentiation into megakaryocytes (Mks). Moreover, it modulates the events that drive Mk maturation and allows the release of platelets into bone marrow sinusoids. THPO plays these roles by binding the MPL receptor, which is expressed in bone marrow stem cells, Mks, platelets and many other human cells. Until recently, no inherited THPO defect was known to cause thrombocytopenia or bone marrow aplasia. However, it was recently shown that microdeletions encompassing the THPO gene in chromosome 3 result in a complex clinical picture, including mild congenital thrombocytopenia. Moreover, a Micronesian family carrying the homozygous c.112C>T (p.Arg38Cys or p.Arg17Cys in the mature protein) missense mutation in THPO presents inherited bone marrow aplasia. No THPO mutation associated with isolated thrombocytopenia has been reported to date, but the application of whole exome sequencing (WES) in a cohort of patients with inherited thrombocytopenias (ITs) of unknown origin revealed that monoallelic changes in this gene identify a new form of IT. In fact, WES identified two unrelated individuals carrying the heterozygous variant c.91C>T (p. Arg31*), which is expected to result in mutant protein degradation and THPO haploinsufficiency.

Published

2017

29. Clinical and pathogenic features of ETV6-related thrombocytopenia with predisposition to acute lymphoblastic leukemia

Author

Serena Barozzi, Giuseppe Loffredo, Carlo L. Balduini, Chiara Gnan, Alessandra Balduini, Caterina Marconi, Michael Doubek, Lenka Radová, Christian A. Di Buduo, Federica Melazzini, Caterina Alfano, Anna Savoia, Daniela De Rocco, Valeria Bozzi, Tommaso Pippucci, Flavia Palombo, Marco Seri, Michela Faleschini, Katerina Stano Kozubik, Patrizia Noris, Šárka Pospíšilová, Alessandro Pecci, Melazzini, Federica, Palombo, Flavia, Balduini, Alessandra, DE ROCCO, Daniela, Marconi, Caterina, Noris, Patrizia, Gnan, Chiara, Pippucci, Tommaso, Bozzi, Valeria, Faleschini, Michela, Barozzi, Serena, Doubek, Michael, Di Buduo, Christian A., Kozubik, Katerina Stano, Radova, Lenka, Loffredo, Giuseppe, Pospisilova, Sarka, Alfano, Caterina, Seri, Marco, Balduini, Carlo L., Pecci, Alessandro, Savoia, Anna, De Rocco, Daniela, Di Buduo, Christian A, Stano Kozubik, Katerina, and Balduini, Carlo L

Subjects

0301 basic medicine, Fibrinogen, 0302 clinical medicine, hemic and lymphatic diseases, Medicine, Platelet, platelet disorders, inherited thrombocytopenia, Child, inherited thrombocytopenias, education.field_of_study, Hematology, Incidence (epidemiology), Nuclear Proteins, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Pedigree, 3. Good health, Cell Transformation, Neoplastic, Child, Preschool, Core Binding Factor Alpha 2 Subunit, Cohort, Intercellular Signaling Peptides and Proteins, medicine.drug, Adult, Platelets, medicine.medical_specialty, Adolescent, Platelet disorder, Population, Article, Young Adult, 03 medical and health sciences, Internal medicine, Humans, Family, Genetic Predisposition to Disease, education, Proto-Oncogene Proteins c-ets, business.industry, Infant, Newborn, Infant, Thrombocytopenia, Repressor Proteins, ETV6, 030104 developmental biology, Mutation, Immunology, business, 030215 immunology

Abstract

ETV6-related thrombocytopenia is an autosomal dominant thrombocytopenia that has been recently identified in a few families and has been suspected to predispose to hematologic malignancies. To gain further information on this disorder, we searched for ETV6 mutations in the 130 families with inherited thrombocytopenia of unknown origin from our cohort of 274 consecutive pedigrees with familial thrombocytopenia. We identified 20 patients with ETV6-related thrombocytopenia from seven pedigrees. They have five different ETV6 variants, including three novel mutations affecting the highly conserved E26 transformation-specific domain. The relative frequency of ETV6-related thrombocytopenia was 2.6% in the whole case series and 4.6% among the families with known forms of inherited thrombocytopenia. The degree of thrombocytopenia and bleeding tendency of the patients with ETV6-related thrombocytopenia were mild, but four subjects developed B-cell acute lymphoblastic leukemia during childhood, resulting in a significantly higher incidence of this condition compared to that in the general population. Clinical and laboratory findings did not identify any particular defects that could lead to the suspicion of this disorder from the routine diagnostic workup. However, at variance with most inherited thrombocytopenias, platelets were not enlarged. In vitro studies revealed that the maturation of the patients' megakaryocytes was defective and that the patients have impaired proplatelet formation. Moreover, platelets from patients with ETV6-related thrombocytopenia have reduced ability to spread on fibrinogen. Since the dominant thrombocytopenias due to mutations in RUNX1 and ANKRD26 are also characterized by normal platelet size and predispose to hematologic malignancies, we suggest that screening for ETV6, RUNX1 and ANKRD26 mutations should be performed in all subjects with autosomal dominant thrombocytopenia and normal platelet size.

Published

2016

30. ACTN1-related thrombocytopenia: Identification of novel families for phenotypic characterization

Author

Shinji Kunishima, Roberta Bottega, Simonetta Pardini, Caterina Marconi, Loretta Ngu, Patrizia Noris, Alessandro Pecci, Ugo Ramenghi, Michela Faleschini, Anna Savoia, Carlo Baronci, Gabriele Baj, Marco Seri, Carlo L. Balduini, Claudia Cagioni, Tommaso Pippucci, Bottega R, Marconi C, Faleschini M, Baj G, Cagioni C, Pecci A, Pippucci T, Ramenghi U, Pardini S, Ngu L, Baronci C, Kunishima S, Balduini CL, Seri M, Savoia A, Noris P, Bottega, Roberta, Marconi, Caterina, Faleschini, Michela, Baj, Gabriele, Cagioni, Claudia, Pecci, Alessandro, Pippucci, Tommaso, Ramenghi, Ugo, Pardini, Simonetta, Ngu, Loretta, Baronci, Carlo, Kunishima, Shinji, Balduini, Carlo L., Seri, Marco, Savoia, Anna, and Noris, Patrizia

Subjects

Proband, Adult, Blood Platelets, Male, medicine.medical_specialty, Heterozygote, Adolescent, Genotype, Immunology, Mutation, Missense, Gene Expression, medicine.disease_cause, Severity of Illness Index, Biochemistry, Thrombopoiesis, Inside BLOOD Commentary, Internal medicine, hemic and lymphatic diseases, Medicine, Missense mutation, Humans, Actinin, Child, Thrombopoietin, Aged, Genetics, Aged, 80 and over, inherited thrombocytopenias, Mutation, Hematology, business.industry, Platelet Count, Case-control study, Heterozygote advantage, Cell Biology, Middle Aged, Thrombocytopenia, Pedigree, Phenotype, Case-Control Studies, Child, Preschool, Female, business

Abstract

Inherited thrombocytopenias (ITs) are a heterogeneous group of syndromic and nonsyndromic diseases caused by mutations affecting different genes. Alterations of ACTN1, the gene encoding for α-actinin 1, have recently been identified in a few families as being responsible for a mild form of IT (ACTN1-related thrombocytopenia; ACTN1-RT). To better characterize this disease, we screened ACTN1 in 128 probands and found 10 (8 novel) missense heterozygous variants in 11 families. Combining bioinformatics, segregation, and functional studies, we demonstrated that all but 1 amino acid substitution had deleterious effects. The clinical and laboratory findings of 31 affected individuals confirmed that ACTN1-RT is a mild macrothrombocytopenia with low risk for bleeding. Low reticulated platelet counts and only slightly increased serum thrombopoietin levels indicated that the latest phases of megakaryopoiesis were affected. Given its relatively high frequency in our cohort (4.2%), ACTN1-RT has to be taken into consideration in the differential diagnosis of ITs.

Published

2015

31. Mutations in the 5' UTR of ANKRD26, the ankirin repeat domain 26 gene, cause an autosomal-dominant form of inherited thrombocytopenia, THC2

Author

Mariateresa Di Stazio, Marcella Ferraro, Carlo L. Balduini, Pamela Magini, Patrizia Noris, Francesca Punzo, Chiara Gnan, Saverio Scianguetta, Luca Dezzani, Samuele Gherardi, Daniela De Rocco, Tommaso Pippucci, Caterina Marconi, Valeria Bozzi, Giuseppe Loffredo, Nuria Pujol-Moix, Serena Barozzi, Giovanni Castegnaro, Anna Savoia, Giovanni Perini, Marco Seri, Silverio Perrotta, Alessandro Pecci, Pippucci T, Savoia A, Perrotta S, Pujol-Moix N, Noris P, Castegnaro G, Pecci A, Gnan C, Punzo F, Marconi C, Gherardi S, Loffredo G, De Rocco D, Scianguetta S, Barozzi S, Magini P, Bozzi V, Dezzani L, Di Stazio M, Ferraro M, Perini G, Seri M, Balduini CL, Pippucci, T, Savoia, A, Perrotta, Silverio, Pujol Moix, N, Noris, P, Castegnaro, G, Pecci, A, Gnan, C, Punzo, F, Marconi, C, Gherardi, S, Loffredo, G, De Rocco, D, Scianguetta, S, Barozzi, S, Magini, P, Bozzi, V, Dezzani, L, Di Stazio, M, Ferraro, M, Perini, G, Seri, M, Balduini, C. L., Pippucci, Tommaso, Savoia, Anna, Pujol Moix, Núria, Noris, Patrizia, Castegnaro, Giovanni, Pecci, Alessandro, Gnan, Chiara, Punzo, Francesca, Marconi, Caterina, Gherardi, Samuele, Loffredo, Giuseppe, DE ROCCO, Daniela, Scianguetta, Saverio, Barozzi, Serena, Magini, Pamela, Bozzi, Valeria, Dezzani, Luca, DI STAZIO, Mariateresa, Ferraro, Marcella, Perini, Giovanni, Seri, Marco, and Balduini, Carlo L.

Subjects

Untranslated region, Male, Five prime untranslated region, Molecular Sequence Data, Locus (genetics), Chromosome Disorders, autosomal-dominant thrombocytopenia, Haploinsufficiency, Biology, Genome, Conserved sequence, Genetic, Ankyrin Repeat, Base Sequence, Chromosome Breakage, Conserved Sequence, Female, Genetic Loci, Humans, Pedigree, Thrombocytopenia, Genes, Dominant, Mutation, Genetics, Genetics (clinical), Report, Genetics(clinical), Dominant, Gene, ANKRD26, Molecular biology, Chromosome Disorder, Genes, THC2, Chromosome breakage, Human

Abstract

THC2, an autosomal-dominant thrombocytopenia described so far in only two families, has been ascribed to mutations in MASTL or ACBD5. Here, we show that ANKRD26, another gene within the THC2 locus, and neither MASTL nor ACBD5, is mutated in eight unrelated families. ANKRD26 was also found to be mutated in the family previously reported to have an ACBD5 mutation. We identified six different ANKRD26 mutations, which were clustered in a highly conserved 19 bp sequence located in the 5' untranslated region. Mutations were not detected in 500 controls and are absent from the 1000 Genomes database. Available data from an animal model and Dr. Watson's genome give evidence against haploinsufficiency as the pathogenetic mechanism for ANKRD26-mediated thrombocytopenia. The luciferase reporter assay suggests that these 5' UTR mutations might enhance ANKRD26 expression. ANKRD26 is the ancestor of a family of primate-specific genes termed POTE, which have been recently identified as a family of proapoptotic proteins. Dysregulation of apoptosis might therefore be the pathogenetic mechanism, as demonstrated for another thrombocytopenia, THC4. Further investigation is needed to provide evidence supporting this hypothesis.

Published

2011

32. 5’UTR point substitutions and N-terminal truncating mutations of ANKRD26 in acute myeloid leukemia

Author

Silvia Angori, Mauro Torti, Giorgia Simonetti, Marco Seri, Ilaria Canobbio, Giuseppe Saglio, Caterina Marconi, Ira Pastan, Alessandro Pecci, Federica Melazzini, Giovanni Martinelli, Valeria Bozzi, Tommaso Pippucci, Marconi, Caterina, Canobbio, Ilaria, Bozzi, Valeria, Pippucci, Tommaso, Simonetti, Giorgia, Melazzini, Federica, Angori, Silvia, Martinelli, Giovanni, Saglio, Giuseppe, Torti, Mauro, Pastan, Ira, Seri, Marco, and Pecci, Alessandro

Subjects

0301 basic medicine, medicine.medical_specialty, Cancer Research, Myeloid, Chromosome Disorders, Biology, medicine.disease_cause, Transfection, lcsh:RC254-282, Inherited predisposition to leukemia, Germline, 03 medical and health sciences, Exon, Inherited thrombocytopenia, Internal medicine, hemic and lymphatic diseases, medicine, Familial predisposition, Coding region, Humans, Genetic Predisposition to Disease, RNA, Messenger, Acute myeloid leukemia, ANKRD26 gene, Hematology, Molecular Biology, Oncology, Letter to the Editor, Mutation, lcsh:RC633-647.5, Myeloid leukemia, Nuclear Proteins, Chromosome Breakage, lcsh:Diseases of the blood and blood-forming organs, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Thrombocytopenia, Leukemia, Myeloid, Acute, 030104 developmental biology, medicine.anatomical_structure, Cell Transformation, Neoplastic, Immunology, Cancer research, Intercellular Signaling Peptides and Proteins, 5' Untranslated Regions, HeLa Cells

Abstract

Thrombocytopenia 2 (THC2) is an inherited disorder caused by monoallelic single nucleotide substitutions in the 5’UTR of the ANKRD26 gene. Patients have thrombocytopenia and increased risk of myeloid malignancies, in particular, acute myeloid leukemia (AML). Given the association of variants in the ANKRD26 5’UTR with myeloid neoplasms, we investigated whether, and to what extent, mutations in this region contribute to apparently sporadic AML. To this end, we studied 250 consecutive, non-familial, adult AML patients and screened the first exon of ANKRD26 including the 5’UTR. We found variants in four patients. One patient had the c.−125T>G substitution in the 5’UTR, while three patients carried two different variants in the 5’ end of the ANKRD26 coding region (c.3G>A or c.105C>G). Review of medical history showed that the patient carrying the c.−125T>G was actually affected by typical but unrecognized THC2, highlighting that some apparently sporadic AML cases represent the evolution of a well-characterized familial predisposition disorder. As regards the c.3G>A and the c.105C>G, we found that both variants result in the synthesis of N-terminal truncated ANKRD26 isoforms, which are stable and functional in cells, in particular, have a strong ability to activate the MAPK/ERK signaling pathway. Moreover, investigation of one patient with the c.3G>A showed that mutation was associated with strong ANKRD26 overexpression in vivo, which is the proposed mechanism for predisposition to AML in THC2 patients. These data provide evidence that N-terminal ANKRD26 truncating mutations play a potential pathogenetic role in AML. Recognition of AML patients with germline ANKRD26 pathogenetic variants is mandatory for selection of donors for bone marrow transplantation. Electronic supplementary material The online version of this article (doi:10.1186/s13045-016-0382-y) contains supplementary material, which is available to authorized users.