Your search keyword '"Susanna, Barella"' showing total 5 results

1. The Problem of Borderline Hemoglobin A2 Levels in the Screening for β-Thalassemia Carriers in Sardinia

Author

Raffaella Origa, Maria Franca Desogus, Laura Manunza, Maria Elisabetta Paglietti, Franca Rosa Demartis, Maria Carla Sollaino, Arianna Ventrella, Susanna Barella, and Stefania Satta

Subjects

0301 basic medicine, Mutation, education.field_of_study, business.industry, Thalassemia, Population, KLF1, Hematology, General Medicine, medicine.disease_cause, Bioinformatics, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Hemoglobin A2, hemic and lymphatic diseases, Cohort, Immunology, Medicine, Allele, business, education, Gene, 030215 immunology

Abstract

Background: The increase in HbA2 is the most important parameter for the identification of thalassemia carriers. However, in routine screening for hemoglobinopathies, some cases are difficult to classify because the level of HbA2 is not typically elevated. In this work, we report the results of a molecular investigation on a cohort of subjects with borderline HbA2. Methods: All subjects with a β-thalassemia carrier partner and a borderline percentage level of HbA2 were investigated for the presence of a pathological mutation in the β-globin gene. All negative subjects were screened for both the KLF1 mutation and the presence of ααα/ or αααα/ alleles. The subjects with reduced MCV and/or MCH were also screened for deletional and nondeletional α-globin gene defects. Results: Various β-globin mutations and KLF1 gene defects are the most common genetic determinants responsible for this phenotype in our population. Conclusion: KLF1 mutations are important in a screening program for hemoglobinopathies. An increase in HbF in association with borderline HbA2 levels is a useful but not exclusive marker that suggests the investigation of this gene. On the basis of our findings, we are able to suggest the molecular procedure to use in a population characterized by a high prevalence of thalassemia carriers.

Published

2016

2. Contents Vol. 135, 2016

Author

Yunxiang Zhang, Ciprian Tomuleasa, Lihong Yang, Melissa Winfield, Maria Elisabetta Paglietti, Mounzer Agha, Dan Douer, Jianpin Zhou, Yanhui Jin, Alexandra Marculescu, Raffaella Origa, Xiaoli Cheng, Cheryl Tompkins, Arianna Ventrella, Giovanni Romanelli, Maria Carla Sollaino, Mingshan Wang, Sant-Rayn Pasricha, Jiong Hu, Müge Aydoğdu, Ruham Alshiekh-Nasany, Jing-Zhou Hou, Susanna Barella, Junmin Li, Rodolfo D. Cançado, Michael Boyiadzis, Ken Cheng, Paulo Caleb Junior Lima Santos, Anastasios Raptis, Xiaoyang Li, Edileide Correia, Ivana Gojo, Paula Fernanda Silva Fonseca, Stefania Satta, Alexandru Bardas, Claire Sheeran, Franca Rosa Demartis, Donald K. Bowden, Bhavana Bhatnagar, Anca Colita, Xiuping Hao, Druckerei Stückle, Jianqing Mi, Marly Maria Uellendahl Lopes, Laura Manunza, Hongming Zhu, C. Orban, Yingyu Wang, Kelly J. Norsworthy, Mary Guay, Antonio M. Esquinas, Weili Zhao, Maria Franca Desogus, Zeba N. Singh, Manuel Antonio Lescano, Roger E. Peverill, Haixiao Xie, Sidsel Christy Lindgaard, Stefan O. Ciurea, Annie Im, Satz Mengensatzproduktion, and Alina Tanase

Subjects

Hematology, General Medicine

Published

2016

3. Investigating the Alpha1NcoI Mutation

Author

Maria Elisabetta Paglietti, Maria Carla Sollaino, Raffaella Origa, Susanna Barella, and Maria Franca Desogus

Subjects

Genetics, medicine.medical_specialty, Molecular genetics, Mutation (genetic algorithm), medicine, Hematology, General Medicine, Alpha-thalassemia, Quantitative trait locus, Biology, medicine.disease

Published

2014

4. Investigating the alpha1(NcoI) mutation

Author

Maria Franca, Desogus, Maria Elisabetta, Paglietti, Maria Carla, Sollaino, Susanna, Barella, and Raffaella, Origa

Subjects

Adult, Glycated Hemoglobin, Male, alpha-Thalassemia, Mutation, Quantitative Trait Loci, Humans, Female

Published

2014

5. HbH disease in Sardinia: molecular, hematological and clinical aspects

Author

Maria Addis, Maria Antonietta Melis, Susanna Barella, N. Giagu, P. Massa, B. Aru, L Maccioni, Antonio Cao, Carlo Dessì, E. Paglietti, M. P. Turco, Renzo Galanello, and S. Cocco

Subjects

Adult, Genotype, Disease, Pathogenesis, Medicine, Humans, Clinical phenotype, Child, Genetics, Hemoglobin H, business.industry, Homozygote, Large series, Chromosome Mapping, Hematology, General Medicine, medicine.disease, Globins, Hemoglobinopathies, Hemoglobinopathy, Phenotype, Genes, Italy, business, Gene Deletion

Abstract

In this study we have defined the molecular basis and correlated the clinical phenotype with the alpha-globin genotype in a large series of patients of Sardinian descent with HbH disease. The most prevalent molecular defect was the deletion of 3 alpha-globin structural genes most commonly the (--/-alpha 3.7) genotype (83.6%) and rarely the (--/-alpha 4.2) genotype (1.4%), followed in decreasing order of incidence by the combination of deletion alpha zero-thalassemia and initiation codon mutation of the alpha 2-gene (--/alpha NcoI alpha = 9.8%), deletion alpha zero-thalassemia and pentanucleotide deletion of IVS-I of the alpha 2-globin gene, (--/alpha HphI alpha = 3.3%) deletion alpha zero-thalassemia and initiation codon mutation of the alpha 1-gene (--/alpha alpha NcoI = 1.3%), a homozygous state for initiation codon mutation of the alpha 2-gene (alpha Nco alpha/alpha NcoI alpha = 0.7%). Patients with the (--/alpha thal alpha) genotypes showed severer clinical and hematological features as compared to those with the (--/-alpha) or those with the (--/alpha alpha thal) genotypes. The single patient with the (alpha Nco alpha/alpha Nco alpha) genotype had a clinical phenotype intermediate between HbH disease and the alpha-thalassemia carrier status. This heterogeneity depends on the fact that the alpha 2-globin gene produces 2-3 times alpha-globin chains than the alpha 1-gene and the single remaining alpha 1-like globin gene in the -alpha 3.7 chromosome has a compensatory increase in the alpha-globin chain output. alpha-Globin gene mapping of HbH disease patients may be useful for predicting the clinical outcome and to improve genetic counseling.

Published

1992