Skoči na glavni sadržaj

Arhiv za higijenu rada i toksikologiju, Vol. 66 No. 4, 2015.

Pregledni rad

https://doi.org/10.1515/aiht-2015-66-2679

Molecular basis of ALS and FTD: implications for translational studies

Rajka M. Liščić ; Institute for Medical Research and Occupational Health, Zagreb and Department of Anatomy and Neuroscience, School of Medicine, University of Osijek, Croatia

Puni tekst: engleski pdf 395 Kb

str. 285-290

preuzimanja: 531

citiraj

Sažetak

Amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) are neurodegenerative disorders, related by signs of deteriorating motor and cognitive functions, and short survival. The cause is unknown and no effective treatment currently exists. For ALS, there is only a drug Riluzole and a promising substance arimoclomol. The overlap between ALS and FTD occurs at clinical, genetic, and pathological levels. The majority of ALS cases are sporadic (SALS) and a subset of patients has an inherited form of the disease, familial ALS (FALS), with a common SOD1 mutation, also present in SALS. A few of the mutant genes identified in FALS have also been found in SALS. Recently, hexanucleotide repeat expansions in C9ORF72 gene were found to comprise the largest fraction of ALS- and FTD-causing mutations known to date. TAR DNA-binding protein 43 (TDP-43), encoded by the TARDBP gene, has been identified as the pathological protein of FALS, SALS and, less frequently, FTD. The less frequent TDP-43 pathology in other forms of familial FTD has been linked to a range of mutations in GRN, FUS/TLS, rarely VCP, and other genes. TDP-43 and FUS/TLS have striking structural and functional similarities, most likely implicating altered RNA processing as a major event in ALS pathogenesis. The clinical overlap of the symptoms of FTD and ALS is complemented by overlapping neuropathology, with intracellular inclusions composed of microtubule-associated protein tau, TDP-43 and less frequently FUS, or unknown ubiquitinated proteins. Furthermore, new therapeutic approaches continue to emerge, by targeting SOD1, TDP-43 or GRN proteins. This review addresses new advances that are being made in our understanding of the molecular mechanisms of both diseases, which may eventually translate into new treatment options.

Ključne riječi

dementia; FTLD; FUS/TLS; genetics; motor neuron disease; TDP-43; C9ORF72 nucleotide repeat expansions; TARDBP

Hrčak ID:

149580

URI

https://hrcak.srce.hr/149580

Datum izdavanja:

16.12.2015.

Podaci na drugim jezicima: hrvatski

Posjeta: 1.568 *