TDP-43 proteinopathies: a new wave of neurodegenerative diseases

Author:

de Boer Eva Maria Johanna,Orie Viyanti K,Williams Timothy,Baker Mark R,De Oliveira Hugo M,Polvikoski Tuomo,Silsby Matthew,Menon Parvathi,van den Bos MehdiORCID,Halliday Glenda M,van den Berg Leonard H,Van Den Bosch Ludo,van Damme PhilipORCID,Kiernan Matthew CORCID,van Es Michael A,Vucic SteveORCID

Abstract

Inclusions of pathogenic deposits containing TAR DNA-binding protein 43 (TDP-43) are evident in the brain and spinal cord of patients that present across a spectrum of neurodegenerative diseases. For instance, the majority of patients with sporadic amyotrophic lateral sclerosis (up to 97%) and a substantial proportion of patients with frontotemporal lobar degeneration (~45%) exhibit TDP-43 positive neuronal inclusions, suggesting a role for this protein in disease pathogenesis. In addition, TDP-43 inclusions are evident in familial ALS phenotypes linked to multiple gene mutations including the TDP-43 gene coding (TARDBP) and unrelated genes (eg, C9orf72). While TDP-43 is an essential RNA/DNA binding protein critical for RNA-related metabolism, determining the pathophysiological mechanisms through which TDP-43 mediates neurodegeneration appears complex, and unravelling these molecular processes seems critical for the development of effective therapies. This review highlights the key physiological functions of the TDP-43 protein, while considering an expanding spectrum of neurodegenerative diseases associated with pathogenic TDP-43 deposition, and dissecting key molecular pathways through which TDP-43 may mediate neurodegeneration.

Funder

National Health and Medical Research Council of Australia

Publisher

BMJ

Subject

Psychiatry and Mental health,Clinical Neurology,Surgery

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