The question is how to interpret the many findings in terms of pa

The question is how to interpret the many findings in terms of pathogenic mechanism at play in vivo, and thus in non-overexpression conditions. It remains uncertain whether the cleavage, phosphorylation and ubiquination of TDP-43 are important for pathogenicity or not. Propensity

of TDP-43 to aggregate, further enhanced by the presence of mutations, is an almost universal finding (Johnson et al., 2009; Nonaka et al., 2009; Zhang et al., 2009), although the most relevant model generated hitherto did not contain TDP-43-containing aggregates (Wegorzewska et al., 2009). Furthermore, the significance INCB024360 chemical structure of the depletion of TDP-43 from the nucleus (found in many but not in all studies) as an underlying ‘compartmental’ loss-of-function

mechanism needs to be established. Alternatively, the sequestering of TDP-43 in the cytoplasm may be the underlying gain-of-function mechanism. Does cytoplasmic TDP-43 gain a toxic biochemical function? Is the formation of aggregates, or one of the (oligomeric) species that are a step in the dynamics of this process, the mechanism of disease? Are essential cellular constituents trapped into these aggregates, resulting in an ‘unrelated’ loss of function? In summary, the finding of TDP-43 in ALS and FTLD neurons and the identification of TDP-43 mutations in familial ALS was a second leap forward in ALS research. It has drawn attention to the possible role of RNA processing in the pathogenic

mechanism of these diseases, even though the involvement of RNA in the mechanism itself ABT 737 remains to be demonstrated (Lemmens et al., 2010). Of major importance is of course the possible involvement of TDP-43 in sporadic ALS. It looks as if TDP-43 may play a role similar to α-synuclein in Parkinson’s disease (PD) and amyloid precursor protein (APP) in Alzheimer’s disease (AD). α-Synuclein mutations are a rare cause of familial PD, and α–synuclein-containing inclusions are seen in the sporadic form of click here PD. APP mutations are a rare cause of AD, but abnormally processed APP under the form of Aβ is a hallmark of sporadic AD. APP and α-synclein overexpression give rise to AD and PD in humans. This has not been observed for TDP-43 in ALS yet. Finally, it needs to be pointed out that, while TDP-43-containing aggregates are seen in the large majority of sporadic ALS patients, they were noted to be absent in many (Mackenzie et al., 2007; Robertson et al., 2007; Tan et al., 2007), but not all (Shan et al., 2009) studies on mutant SOD1 ALS. This may suggest that the mechanisms underlying mutant SOD1-induced motor neuron degeneration and that of sporadic ALS may be different. This still needs to be studied in depth but it has further fuelled the doubts about whether mutant SOD1 models are of use in studying sporadic ALS.

Leave a Reply

Your email address will not be published. Required fields are marked *

*

You may use these HTML tags and attributes: <a href="" title=""> <abbr title=""> <acronym title=""> <b> <blockquote cite=""> <cite> <code> <del datetime=""> <em> <i> <q cite=""> <strike> <strong>