Your search keyword '"Balduini, C"' showing total 5 results

1. International collaboration as a tool for diagnosis of patients with inherited thrombocytopenia in the setting of a developing country.

Author

Glembotsky AC, Marta RF, Pecci A, De Rocco D, Gnan C, Espasandin YR, Goette NP, Negro F, Noris P, Savoia A, Balduini CL, Molinas FC, and Heller PG

Subjects

Adolescent, Adult, Aged, Algorithms, Argentina, Biomarkers blood, Child, Child, Preschool, DNA Mutational Analysis, Feasibility Studies, Female, Flow Cytometry, Fluorescent Antibody Technique, Genetic Predisposition to Disease, Health Services Accessibility, Heredity, Humans, Italy, Male, Middle Aged, Molecular Motor Proteins blood, Myosin Heavy Chains blood, Pedigree, Phenotype, Platelet Count, Platelet Function Tests, Predictive Value of Tests, Prognosis, Referral and Consultation, Thrombocytopenia blood, Thrombocytopenia congenital, Thrombospondin 1 blood, Young Adult, Cooperative Behavior, Developing Countries, Genetic Testing methods, Hematologic Tests methods, International Cooperation, Thrombocytopenia diagnosis

Abstract

Background: Inherited thrombocytopenias (ITs) are heterogeneous genetic disorders that frequently represent a diagnostic challenge. The requirement of highly specialized tests for diagnosis represents a particular problem in resource-limited settings. To overcome this difficulty, we applied a diagnostic algorithm and developed a collaboration program with a specialized international center in order to increase the diagnostic yield in a cohort of patients in Argentina., Methods: Based on the algorithm, initial evaluation included collection of clinical data, platelet size, blood smear examination and platelet aggregation tests. Confirmatory tests were performed according to diagnostic suspicion, which included platelet glycoprotein expression, immunofluorescence for myosin-9 in granulocytes and platelet thrombospondin-1 and molecular screening of candidate genes., Results: Thirty-one patients from 14 pedigrees were included; their median age was 32 (4-72) years and platelet count 72 (4-147)×10(9) L(-1). Autosomal dominant inheritance was found in nine (64%) pedigrees; 10 (71%) had large platelets and nine (29%) patients presented with syndromic forms. A definitive diagnosis was made in 10 of 14 pedigrees and comprised MYH9-related disease in four, while classic and monoallelic Bernard-Soulier syndrome, gray platelet syndrome, X-linked thrombocytopenia, thrombocytopenia 2 (ANKRD26 mutation) and familial platelet disorder with predisposition to acute myelogenous leukemia were diagnosed in one pedigree each., Conclusions: Adoption of an established diagnostic algorithm and collaboration with an expert referral center proved useful for diagnosis of IT patients in the setting of a developing country. This initiative may serve as a model to develop international networks with the goal of improving diagnosis and care of patients with these rare diseases., (© 2012 International Society on Thrombosis and Haemostasis.)

Published

2012

2. Management of bleeding and of invasive procedures in patients with platelet disorders and/or thrombocytopenia: Guidelines of the Italian Society for Haemostasis and Thrombosis (SISET).

Author

Tosetto A, Balduini CL, Cattaneo M, De Candia E, Mariani G, Molinari AC, Rossi E, and Siragusa S

Subjects

Blood Platelet Disorders drug therapy, Female, Humans, Italy, Male, Surgical Procedures, Operative methods, Thrombocytopenia drug therapy, Blood Platelet Disorders therapy, Thrombocytopenia therapy

Abstract

The optimal management of bleeding or its prophylaxis in patients with disorders of platelet count or function is controversial. The bleeding diathesis of these patients is usually mild to moderate: therefore, transfusion of platelet concentrates may be inappropriate, as potential adverse effects might outweigh its benefit. The availability of several anti-hemorrhagic drugs further compounds this problem, mainly because the efficacy/suitability of the various treatment options in different clinical manifestations is not well defined. In these guidelines, promoted by the Italian Society for Studies on Haemostasis and Thrombosis (Società Italiana per lo Studio dell'Emostasi e della Trombosi [SISET]), we aim at offering the best available evidence to help the physicians involved in the management of patients with disorders of platelet count or function. Literature review and appraisal of available evidence are discussed for different clinical settings and for different available treatments, including platelet concentrates (PC), recombinant activated factor VII, desmopressin, antifibrinolytics, aprotinin and local hemostatic agents.

Published

2009

3. 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

4. Autosomal dominant macrothrombocytopenia in Italy is most frequently a type of heterozygous Bernard-Soulier syndrome.

Author

Savoia A, Balduini CL, Savino M, Noris P, Del Vecchio M, Perrotta S, Belletti S, Poggi, and Iolascon A

Subjects

Adolescent, Adult, Aged, Bernard-Soulier Syndrome diagnosis, Bernard-Soulier Syndrome etiology, Child, Child, Preschool, DNA Mutational Analysis, Diagnosis, Differential, Family Health, Female, Flow Cytometry, Genes, Dominant, Genetic Linkage, Heterozygote, Humans, Infant, Italy epidemiology, Male, Middle Aged, Mutation, Missense, Pedigree, Platelet Glycoprotein GPIb-IX Complex genetics, Platelet Membrane Glycoproteins analysis, Thrombocytopenia diagnosis, Thrombocytopenia etiology, Bernard-Soulier Syndrome genetics, Thrombocytopenia genetics

Abstract

A form of autosomal dominant macrothrombocytopenia is characterized by mild or no clinical symptoms, normal platelet function, and normal megakaryocyte count. Because this condition has so far received little attention, patients are subject to misdiagnosis and inappropriate therapy. To identify the molecular basis of this disease, 12 Italian families were studied by linkage analysis and mutation screening. Flow cytometry evaluations of platelet membrane glycoproteins (GPs) were also performed. Linkage analysis in 2 large families localized the gene to chromosome 17p, in an interval containing an excellent candidate, the GPIbalpha gene. GPIbalpha, together with other proteins, constitutes the plasma von Willebrand factor (vWF) receptor, which is altered in Bernard-Soulier syndrome (BSS). In 6 of 12 families, a heterozygous Ala156Val missense substitution was identified. Platelet membrane GP studies were performed in 10 patients. Eight were distinguished by a reduction of GPs comparable to that found in a BSS heterozygous condition, whereas the other 2, without the Ala156Val mutation, had a normal content of platelet GPs. In conclusion, the current study provides evidence that most (10 of 12) patients with an original diagnosis of autosomal dominant macrothrombocytopenia shared clinical and molecular features with the heterozygous BSS phenotype. The remaining 2 affected subjects represented patients with "true" autosomal dominant macrothrombocytopenia; the GPIb/IX/V complex was normally distributed on the surface of their platelets. Thus, the diagnosis of heterozygous BSS must always be suspected in patients with inherited thrombocytopenia and platelet macrocytosis.

Published

2001

5. The gene for May-Hegglin anomaly localizes to a <1-Mb region on chromosome 22q12.3-13.1.

Author

Martignetti JA, Heath KE, Harris J, Bizzaro N, Savoia A, Balduini CL, and Desnick RJ

Subjects

Blood Platelet Disorders blood, Blood Platelet Disorders pathology, Female, Genes, Dominant genetics, Haplotypes genetics, Humans, Italy, Lod Score, Male, Microsatellite Repeats genetics, Pedigree, Polymorphism, Genetic genetics, Software, Blood Platelet Disorders genetics, Chromosome Mapping, Chromosomes, Human, Pair 22 genetics

Abstract

The May-Hegglin anomaly (MHA) is an autosomal dominant platelet disorder of unknown etiology. It is characterized by thrombocytopenia, giant platelets, and leukocyte inclusion bodies, and affected heterozygotes are predisposed to bleeding episodes. The MHA gene has recently been localized, by means of linkage analysis, to a 13.6-cM region on chromosome 22, and the complete chromosome 22 sequence has been reported. We recently performed a genome scan for the MHA gene in 29 members of a large, multigenerational Italian family, and we now confirm that the MHA locus is on chromosome 22q12. 3-13.1. The maximal two-point LOD score of 4.50 was achieved with the use of marker D22S283, at a recombination fraction of.05. Haplotype analysis narrowed the MHA critical region to 6.6 cM between markers D22S683 and D22S1177. It is of note that the chromosome 22 sequence allowed all markers to be ordered correctly, identified all the candidate genes and predicted genes, and specifically determined the physical size of the MHA region to be 0. 7 Mb. These results significantly narrow the region in which the MHA gene is located, and they represent the first use of chromosome 22 data to positionally clone a disease gene.

Published

2000