This is an excellent study on a novel
C. elegans model for FTDP-17 tauopathies, with an eventual bearing on AD. The worms were humanized for tau and overexpress either wild-type or mutant tau in isoform ¡§4R1N,¡¨ i.e., containing the four microtubule binding domains and one N-terminal insert, the most abundant isoform in human brain. The
C. elegans model excels in its simplicity and clarity of pathology, with the evident (for worms) rapidity of evolution (~9 days) and the very distinct behavioral and neuropathological defects.
It is amazing to see the cellular pathological defects, recapitulating what is observed in brain and spinal cord of transgenic mice overexpressing human tau-4R in neurons, reported by us (Spittaels et al, 1999; 2000) and others, and comprehensively discussed and referenced in this paper.
The study further highlights that the differences in phenotype caused by either wild-type tau or FTD-mutant tau are...
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This is an excellent study on a novel
C. elegans model for FTDP-17 tauopathies, with an eventual bearing on AD. The worms were humanized for tau and overexpress either wild-type or mutant tau in isoform ¡§4R1N,¡¨ i.e., containing the four microtubule binding domains and one N-terminal insert, the most abundant isoform in human brain. The
C. elegans model excels in its simplicity and clarity of pathology, with the evident (for worms) rapidity of evolution (~9 days) and the very distinct behavioral and neuropathological defects.
It is amazing to see the cellular pathological defects, recapitulating what is observed in brain and spinal cord of transgenic mice overexpressing human tau-4R in neurons, reported by us (Spittaels et al, 1999; 2000) and others, and comprehensively discussed and referenced in this paper.
The study further highlights that the differences in phenotype caused by either wild-type tau or FTD-mutant tau are minor, and this emphazises the problem and our lack of understanding of the actual molecular contribution of expressed and silent FTD-mutants to the actual clinical phenotype. Of some concern for correct molecular interpretation is the difference—or the lack of it—between wild-type and FTD mutant tau for parameters like survival (similar) and neuronal loss (same for all) as opposed to axonal tau-aggregates seen only for tau-V337M.
Equally amazing is how this model so clearly pinpoints the problems and questions that the ¡§mammalian¡¨ model builders have faced for years.
First, what is the role of tau-phosphorylation (normal or ¡§hyper¡¨) in causing the defects and in forming the tau aggregates? We expect and await evidence for an important role for GSK3b in this model, as in transgenic mice (Spittaels et al, 2000). Second, what is (or are) the actual molecular culprit(s), i.e., single molecules of misphosphorylated tau or small aggregates? Third, what is the exact time course of events, i.e., phosphorylation before or after (smaller) aggregates are formed? Fourth, what is the underlying mechanism of disturbed presynaptic transmission, i.e., simply disturbed axonal transport (Terwel et al, 2003)? How does this operate in C. elegans in terms of microtubular structure and stabilization by microtubule-associated proteins (MAPs), if any, and how are they counteracted by human tau?
Without exception, these are important questions that can and will be addressed and answered by further work in this model, which, thanks to its speed and ¡§transparency,¡¨ hopefully will improve mammalian modeling.
Finally, one cannot but be reminded of the amyloid side of neurodegeneration, where attention has finally shifted to the smaller cell-associated aggregated peptides, and away from large aggregates, i.e., the amyloid plaques that have been advocated too long as the major and even the initial problem. As clearly stated in this work, we have appreciated for some time now that for amyloid and tau, and indeed for any protein, ¡§¡K low-level aggregates are ¡K sufficient to disrupt neuronal function.¡¨ On the other hand, a chemical property, e.g., hydrophobic propensity to form b-sheets, that causes a neuronal defect by interfering with a given process is likely to lead also to self-aggregation. But all are separate phenotypic traits, i.e., different externalizations or embodiments of that single chemical property.
This should not be taken to imply that aggregates of amyloid or tau, or any protein, for that matter, are ¡§harmless.¡¨ They might be initially, and could be even beneficial by lowering the active concentration of the monomer. In the long run, excessive accumulation, be it intra- or extracellular, will trigger (auto)-destructive mechanisms that will kill neurons and eventually, the organism. This is the ¡§late phase¡¨ of disease as observed clinically in patients, as well as in transgenic mice and other models, and so elegantly demonstrated in the C. elegans model here. Evidently, without minimizing the importance of proper treatment of the ¡§late phase,¡¨ one hopes to obtain from models—any model—insight into the very early phases of neurodegeneration, to prevent, stall, curb, or even reverse dementia.
References:
Spittaels K, Van den Haute C, Van Dorpe J, Bruynseels K, Vandezande K, Laenen I, Geerts H, Mercken M, Sciot R, Van Lommel A, Loos R, Van Leuven F. Prominent axonopathy in the brain and spinal cord of transgenic mice overexpressing four-repeat human tau protein. Am J Pathol. 1999 Dec;155(6):2153-65. Abstract
Spittaels K, Van den Haute C, Van Dorpe J, Geerts H, Mercken M, Bruynseels K, Lasrado R, Vandezande K, Laenen I, Boon T, Van Lint J, Vandenheede J, Moechars D, Loos R, Van Leuven F.
Glycogen synthase kinase-3ƒÒ phosphorylates protein tau and rescues the axonopathy in the CNS of human four-repeat tau transgenic mice. J Biol Chem. 2000 Dec 29;275(52):41340-9. Abstract
Terwel D, Dewachter L, Van Leuven F. Axonal transport, protein tau and neurodegeneration in Alzheimer¡¦s disease. Neuromolecular Med. 2002;2(2):151-65. Review. Abstract
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