Miniatura

Fitxers

661486.pdf (2.53 MB)
correction.PDF (69.07 KB)

Tipus de document

Article

Versió

Versió publicada

Data de publicació

2013-10-11

Llicència de publicació

cc-by (c) Paco Mercader, Sonia et al., 2013
Si us plau utilitzeu sempre aquest identificador per citar o enllaçar aquest document: https://hdl.handle.net/2445/124527

Gene expression profiling identifies molecular pathways associated with collagen VI deficiency and provides novel therapeutic targets

Títol de la revista

Autors

Director/Tutor

ISSN de la revista

Títol del volum

Recurs relacionat

https://doi.org/10.1371/journal.pone.0077430

Resum

Ullrich congenital muscular dystrophy (UCMD), caused by collagen VI deficiency, is a common congenital muscular dystrophy. At present, the role of collagen VI in muscle and the mechanism of disease are not fully understood. To address this we have applied microarrays to analyse the transcriptome of UCMD muscle and compare it to healthy muscle and other muscular dystrophies. We identified 389 genes which are differentially regulated in UCMD relative to controls. In addition, there were 718 genes differentially expressed between UCMD and dystrophin deficient muscle. In contrast, only 29 genes were altered relative to other congenital muscular dystrophies. Changes in gene expression were confirmed by real-time PCR. The set of regulated genes was analysed by Gene Ontology, KEGG pathways and Ingenuity Pathway analysis to reveal the molecular functions and gene networks associated with collagen VI defects. The most significantly regulated pathways were those involved in muscle regeneration, extracellular matrix remodelling and inflammation. We characterised the immune response in UCMD biopsies as being mainly mediated via M2 macrophages and the complement pathway indicating that anti-inflammatory treatment may be beneficial to UCMD as for other dystrophies. We studied the immunolocalisation of ECM components and found that biglycan, a collagen VI interacting proteoglycan, was reduced in the basal lamina of UCMD patients. We propose that biglycan reduction is secondary to collagen VI loss and that it may be contributing towards UCMD pathophysiology. Consequently, strategies aimed at over-expressing biglycan and restore the link between the muscle cell surface and the extracellular matrix should be considered.

Matèries

Expressió gènica, Genètica molecular humana, Distròfia muscular

Matèries (anglès)

Gene expression, Human molecular genetics, Muscular dystrophy

Citació

Col·leccions

Articles publicats en revistes (Biomedicina)
Articles publicats en revistes (Cirurgia i Especialitats Medicoquirúrgiques)
Articles publicats en revistes (IDIBAPS: Institut d'investigacions Biomèdiques August Pi i Sunyer)

Citació

PACO MERCADER, Sonia, KALKO, Susana, JOU, Cristina, RODRÍGUEZ, María angeles, CORBERA, Joan, MUNTONI, Francesco, FENG, Lucy, RIVAS, Eloy, TORNER RUBIES, Ferran, GUALANDI, Francesca, GOMEZ-FOIX, Anna m., FERRER, Anna, ORTEZ, Carlos ignacio, NASCIMENTO, Andrés, COLOMER OFERIL, Jaume, JIMÉNEZ MALLEBRERA, Cecilia. Gene expression profiling identifies molecular pathways associated with collagen VI deficiency and provides novel therapeutic targets. _PLoS One_. 2013. Vol. 8, núm. 10, pàgs. 1-15. [consulta: 24 de gener de 2026]. ISSN: 1932-6203. [Disponible a: https://hdl.handle.net/2445/124527]

Exportar metadades

JSON - METS

Compartir registre