Your search keyword '"Brussino, Alessandro"' showing total 4 results

1. A novel case of Greenberg dysplasia and genotype–phenotype correlation analysis for LBR pathogenic variants: An instructive example of one gene‐multiple phenotypes.

Author

Giorgio, Elisa, Sirchia, Fabio, Bosco, Martino, Sobreira, Nara Lygia M., Grosso, Enrico, Brussino, Alessandro, and Brusco, Alfredo

Abstract

Greenberg skeletal dysplasia is an autosomal recessive, perinatal lethal disorder associated with biallelic variants affecting the lamin B receptor (LBR) gene. LBR is also associated with the autosomal recessive anadysplasia‐like spondylometaphyseal dysplasia, and the autosomal dominant Pelger–Huët anomaly, a benign laminopathy characterized by anomalies in the nuclear shape of blood granulocytes. The LBR is an inner nuclear membrane protein that binds lamin B proteins (LMNB1 and LMNB2), interacts with chromatin, and exerts a sterol reductase activity. Here, we report on a novel LBR missense variant [c.1379A>G; p.(D460R)], identified by whole exome sequencing and causing Greenberg dysplasia in two fetuses from a consanguineous Moroccan family. We revised published LBR variants to propose a genotype–phenotype correlation in LBR associated diseases. The diverse phenotypes are correlated to the functional domain affected, the heterozygous or homozygous state of the variants, and their different impact on the residual protein function. LBR represents an instructive example of one gene presenting with two different patterns of inheritance and at least three different clinical phenotypes. [ABSTRACT FROM AUTHOR]

Published

2019

2. Spinocerebellar ataxia type 12 identified in two Italian families may mimic sporadic ataxia.

Author

Brussino, Alessandro, Graziano, Claudio, Giobbe, Dario, Ferrone, Marina, Dragone, Elisa, Arduino, Carlo, Lodi, Raffaele, Tonon, Caterina, Gabellini, Anna, Rinaldi, Rita, Miccoli, Sara, Grosso, Enrico, Bellati, Maria Cristina, Orsi, Laura, Migone, Nicola, and Brusco, Alfredo

Abstract

SCA12 is an autosomal dominant cerebellar ataxia characterized by onset in the fourth decade of life with action tremor of arms and head, mild ataxia, dysmetria, and hyperreflexia. The disease is caused by an expansion of ≥51 CAGs in the 5′ region of the brain- specific phosphatase 2 regulatory subunit B-beta isoform ( PPP2R2B) gene. SCA12 is very rare, except for a single ethnic group in India. We screened 159 Italian ataxic patients for SCA12 and identified two families that segregated an expanded allele of 57 to 58 CAGs, sharing a common haplotype. The age at onset, phenotype, and variability of symptoms were compatible with known cases. In one family, the disease was apparently sporadic due to possible incomplete penetrance and/or late age at onset. Our data indicate that SCA12 is also present in Italian patients, and its genetic testing should be applied to both sporadic and familial ataxias. © 2010 Movement Disorder Society [ABSTRACT FROM AUTHOR]

Published

2010

3. A previously undiagnosed case of Gerstmann-Sträussler-Scheinker disease revealed by PRNP gene analysis in patients with adult-onset ataxia.

Author

Cagnoli, Claudia, Brussino, Alessandro, Sbaiz, Luca, Di Gregorio, Eleonora, Atzori, Cristiana, Caroppo, Paola, Orsi, Laura, Migone, Nicola, Buffa, Carlo, Imperiale, Daniele, and Brusco, Alfredo

Abstract

Ataxia is a frequently reported symptom in prion diseases (PD) and it is characteristic of Gerstmann-Sträussler-Scheinker syndrome (GSS), a genetic PD mainly related to the P102L mutation in the PRNP gene. Our aim was to screen for the P102L and other six known PRNP gene mutations (P105L, A117V, Y145X, E200K, D202N, and V210I) a group of 206 consecutive patients diagnosed with adult-onset cerebellar ataxia of unknown origin. The patients, negative for the most common acquired and genetic forms, were analyzed using a combination of restriction endonuclease digestion and pyrosequencing; eight, affected by ataxia and cognitive dysfunction, were also sequenced for the PRNP gene. One patient resulted to be heterozygous for the P102L mutation. Retrospectively, the clinical picture was consistent with a 'classical' GSS phenotype. In conclusion, the screening for the P102L mutation, or even the sequencing of the PRNP gene should be taken in consideration in patients with late-onset ataxia (>50 years). © 2008 Movement Disorder Society [ABSTRACT FROM AUTHOR]

Published

2008

4. The (−16C > T) substitution in the PLEKHG4 gene is not present among European ADCA patients.

Author

Cagnoli, Claudia, Brussino, Alessandro, Di Gregorio, Eleonora, Brusco, Alfredo, Stevanin, Giovanni, Durr, Alexandra, and Brice, Alexis

Published

2007