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Inferring disease course from differential exon usage in the wide titinopathy spectrum

Di Feo, Maria Francesca; Oghabian, Ali; Nippala, Ella; Gautel, Mathias; Jungbluth, Heinz; Forzano, Francesca; Malfatti, Edoardo; Castiglioni, Claudia; Krey, Ilona; Gomez Andres, David; Brady, Angela F.; Iascone, Maria; Cereda, Anna; Pezzani, Lidia; Natera De Benito, Daniel; Nascimiento Osorio, Andres; Estévez Arias, Berta; Kurbatov, Sergei A.; Attie-Bitach, Tania; Nampoothiri, Sheela; Ryan, Erin; Morrow, Michelle; Gorokhova, Svetlana; Chabrol, Brigitte; Sinisalo, Juha; Tolppanen, Heli; Tolva, Johanna; Munell, Francina; Camacho Soriano, Jessica; Sanchez Duran, Maria Angeles; Johari, Mridul; Tajsharghi, Homa; Hackman, Peter; Udd, Bjarne; Savarese, Marco (2024)

 
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Ann_Clin_Transl_Neurol_-_2024_-_Di_Feo_-_Inferring_disease_course_from_differential_exon_usage_in_the_wide_titinopathy.pdf (723.1Kt)
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Di Feo, Maria Francesca
Oghabian, Ali
Nippala, Ella
Gautel, Mathias
Jungbluth, Heinz
Forzano, Francesca
Malfatti, Edoardo
Castiglioni, Claudia
Krey, Ilona
Gomez Andres, David
Brady, Angela F.
Iascone, Maria
Cereda, Anna
Pezzani, Lidia
Natera De Benito, Daniel
Nascimiento Osorio, Andres
Estévez Arias, Berta
Kurbatov, Sergei A.
Attie-Bitach, Tania
Nampoothiri, Sheela
Ryan, Erin
Morrow, Michelle
Gorokhova, Svetlana
Chabrol, Brigitte
Sinisalo, Juha
Tolppanen, Heli
Tolva, Johanna
Munell, Francina
Camacho Soriano, Jessica
Sanchez Duran, Maria Angeles
Johari, Mridul
Tajsharghi, Homa
Hackman, Peter
Udd, Bjarne
Savarese, Marco
2024

Annals of clinical and translational neurology
doi:10.1002/acn3.52189
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Julkaisun pysyvä osoite on
https://urn.fi/URN:NBN:fi:tuni-202410089154

Kuvaus

Peer reviewed
Tiivistelmä
Objective: Biallelic titin truncating variants (TTNtv) have been associated with a wide phenotypic spectrum, ranging from complex prenatal muscle diseases with dysmorphic features to adult-onset limb-girdle muscular dystrophy, with or without cardiac involvement. Given the size and complexity of TTN, reaching an unequivocal molecular diagnosis and precise disease prognosis remains challenging. Methods: In this case series, 12 unpublished cases and one already published case with biallelic TTNtv were collected from multiple international medical centers between November 2022 and September 2023. TTN mutations were detected through exome or genome sequencing. Information about familial and personal clinical history was collected in a standardized form. RNA-sequencing and analysis of TTN exon usage were performed on an internal sample cohort including postnatal skeletal muscles, fetal skeletal muscles, postnatal heart muscles, and fetal heart muscles. In addition, publicly available RNA-sequencing data was retrieved from ENCODE. Results: We generated new RNA-seq data on TTN exons and identified genotype–phenotype correlations with prognostic implications for each titinopathy patient (whether worsening or improving in prenatal and postnatal life) using percentage spliced in (PSI) data for the involved exons. Interestingly, thanks to exon usage, we were also able to rule out a titinopathy diagnosis in one prenatal case. Interpretation: This study demonstrates that exon usage provides valuable insights for a more exhaustive clinical interpretation of TTNtv; additionally, it may serve as a model for implementing personalized medicine in many other genetic diseases, since most genes undergo alternative splicing.
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  • TUNICRIS-julkaisut [22892]
Kalevantie 5
PL 617
33014 Tampereen yliopisto
oa[@]tuni.fi | Tietosuoja | Saavutettavuusseloste
 

 

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Kalevantie 5
PL 617
33014 Tampereen yliopisto
oa[@]tuni.fi | Tietosuoja | Saavutettavuusseloste