Your search keyword '"Bozzi V"' showing total 4 results

1. MYH9-Related Thrombocytopenia: Four Novel Variants Affecting the Tail Domain of the Non-Muscle Myosin Heavy Chain IIA Associated with a Mild Clinical Evolution of the Disorder.

Author

Zaninetti C, De Rocco D, Giangregorio T, Bozzi V, Demeter J, Leoni P, Noris P, Ryhänen S, Barozzi S, Pecci A, and Savoia A

Subjects

Adolescent, Adult, Aged, Amino Acid Substitution, Chromosome Breakage, Chromosome Disorders pathology, Female, Frameshift Mutation, Humans, Male, Middle Aged, Molecular Motor Proteins chemistry, Myosin Heavy Chains chemistry, Pedigree, Phenotype, Protein Domains, Protein Isoforms chemistry, Protein Isoforms genetics, Thrombocytopenia genetics, Thrombocytopenia pathology, Young Adult, Chromosome Disorders genetics, Molecular Motor Proteins genetics, Mutation, Myosin Heavy Chains genetics, Thrombocytopenia congenital

Abstract

MYH9 -related disease ( MYH9 -RD) is an autosomal-dominant thrombocytopenia caused by mutations in the gene for non-muscle myosin heavy chain IIA (NMMHC-IIA). Patients present congenital macrothrombocytopenia and inclusions of NMMHC-IIA in leukocytes, and have a variable risk of developing kidney damage, sensorineural deafness, presenile cataracts and/or liver enzymes abnormalities. The spectrum of mutations found in MYH9 -RD patients is limited and the incidence and severity of the non-congenital features are predicted by the causative MYH9 variant. In particular, different alterations of the C-terminal tail domain of NMMHC-IIA associate with remarkably different disease evolution. We report four novel MYH9 mutations affecting the tail domain of NMMHC-IIA and responsible for MYH9 -RD in four families. Two variants cause amino acid substitutions in the coiled-coil region of NMMHC-IIA, while the other two are a splicing variant and a single nucleotide deletion both resulting in frameshift alterations of the short non-helical tailpiece. Characterization of phenotypes of affected individuals shows that all of these novel variants are associated with a mild clinical evolution of the disease., Competing Interests: None., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2019

2. 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

3. 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

4. Megakaryocytes of patients with MYH9-related thrombocytopenia present an altered proplatelet formation.

Author

Pecci A, Malara A, Badalucco S, Bozzi V, Torti M, Balduini CL, and Balduini A

Subjects

Adult, Cell Differentiation, Cells, Cultured, Female, Heterozygote, Humans, Male, Point Mutation, Blood Platelets pathology, Megakaryocytes pathology, Molecular Motor Proteins genetics, Myosin Heavy Chains genetics, Stem Cells pathology, Thrombocytopenia genetics, Thrombocytopenia pathology

Abstract

MYH9-related disease (MYH9-RD) is an autosomal-dominant thrombocytopenia caused by mutations of MYH9, the gene for the heavy chain of myosin-IIA. Pathogenesis of thrombocytopenia of MYH9-RD is unknown. Recent studies in mice demonstrated that myosin-IIA is an inhibitor of proplatelet formation (PPF), and suggested that it could be involved in the suppression of PPF exerted by megakaryocyte adhesion to type I collagen, which regulates the timing of platelet release within bone marrow. However, the consequences on PPF of the heterozygous mutations causative of the MYH9-RD have never been investigated. We studied the in-vitro PPF by megakaryocytes obtained from four patients carrying the p.D1424N or the p.R1933X mutations. We demonstrated that MYH9-RD megakaryocytes completely lose the physiologic suppression of proplatelet extension exerted by interaction with type I collagen, thus supporting the hypothesis that a premature platelet release within bone marrow contributes to pathogenesis of MYH9-related thrombocytopenia. Moreover, proplatelets extended by MYH9-RD megakaryocytes presented a significant defect in branching in secondary processes (p=0.001) and formed a significantly lower number of proplatelet tips (p=0.005). Since platelets are assembled at the level of proplatelet tips, this defect could further contribute to pathogenesis of thrombocytopenia of MYH9-RD patients.

Published

2009