Brain-specific Proteins Decline in the Cerebrospinal Fluid of Humans with Huntington Disease

Fang, Qiaojun; Strand, Andrew D.; Law, Wendy; Faça, Vítor Marcel; Fitzgibbon, Matthew; Hamel, Nathalie; Houle, Benoit; Liu, Xin; May, Damon; Poschmann, Gereon; Roy, Line; Stühler, Kai; Ying, Wantao; Zhang, Jiyang; Zheng, Zhao-Bin; Bergeron, John J.M.; Hanash, Sam; He, Fuchu; Leavitt, Blair R.; Meyer, Helmut E.; Qian, Xiaohong; McIntosh, Martin W.

doi:10.1074/mcp.m800231-mcp200

Cited by 82 publications

(81 citation statements)

References 51 publications

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“…The abnormal flow could also compromise the role of the CSF in clearing brain catabolites, raising the possibility of a defect in brain homeostasis in HD patients. In support of these observations, alterations in various factors and proteins have been detected in the CSF of HD patients (33). Such defects in brain clearance capacity could be deleterious and exacerbate the neuronal death observed in HD.…”

Section: Htt and Hap1 Regulate Trafficking To The Centrosome And Cilimentioning

confidence: 50%

Ciliogenesis is regulated by a huntingtin-HAP1-PCM1 pathway and is altered in Huntington disease

Keryer¹,

Pineda²,

Liot³

et al. 2011

J. Clin. Invest.

122

130

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IntroductionHuntington disease (HD) is an autosomal-dominant neurodegenerative disorder caused by the pathogenic expansion of the polyglutamine (polyQ) N-terminal stretch in the huntingtin protein (HTT; encoded by HTT). HD is characterized by the dysfunction and death of neurons in the brain, leading to devastating cognitive, psychiatric, and motor symptoms in patients. Studies in multiple cell and animal model systems support the notion that polyQ expansion in mutant Htt leads to the gain of new toxic functions and loss of the neuroprotective functions of the WT Htt (1).Although some of its functions are linked to transcriptional activities in health and disease, Htt is primarily a cytoplasmic protein that associates with microtubules (MTs) and vesicles. Htt regulates intracellular trafficking of various organelles, including vesicles, by interacting with the dynein/dynactin pathway (2-4). Htt facilitates MT-dependent transport by interacting directly with dynein (2) and indirectly via huntingtin-associated protein 1 (HAP1), which binds to the dynactin p150 Glued subunit (3,(5)(6)(7). In pathological situations, the Htt-HAP1-dynactin complex is altered, resulting in a reduction of vesicular transport in neurons (3). These findings show that Htt integrates vesicular transport by regulating the activity of specific protein complexes containing the dynein/dynactin and kinesin 1 complexes and adaptor proteins such as HAP1.With 2 patterns of axonemal MTs (9 + 0 in primary cilia and 9 + 2 in motile cilia), cilia are involved in sensory role, motility, and flow generation. Within the last 5 years, the importance of this

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Section: Htt and Hap1 Regulate Trafficking To The Centrosome And Cilimentioning

confidence: 50%

Ciliogenesis is regulated by a huntingtin-HAP1-PCM1 pathway and is altered in Huntington disease

Keryer¹,

Pineda²,

Liot³

et al. 2011

J. Clin. Invest.

122

130

View full text Add to dashboard Cite

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“…Nano-LC-MS profiling of enzymatically digested proteins using label-free quantification on high resolution mass spectrometers may provide alternative solutions. These strategies have already been used to identify new biomarkers in CSF with good results (15,27). In such approaches, very limited or no fractionation at all is usually performed on the sample because of the large number of analyses that must be performed (number of patients and technical replicates) and the intrinsic variability that may be introduced by the fractionation procedure itself.…”

Section: Discussionmentioning

confidence: 99%

In-depth Exploration of Cerebrospinal Fluid by Combining Peptide Ligand Library Treatment and Label-free Protein Quantification

Mouton-Barbosa

Roux‐Dalvai

Bouyssié

et al. 2010

Molecular & Cellular Proteomics

121

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Cerebrospinal fluid (CSF) is the biological fluid in closest contact with the brain and thus contains proteins of neural cell origin. Hence, CSF is a biochemical window into the brain and is particularly attractive for the search for biomarkers of neurological diseases. However, as in the case of other biological fluids, one of the main analytical challenges in proteomic characterization of the CSF is the very wide concentration range of proteins, largely exceeding the dynamic range of current analytical approaches. Here, we used the combinatorial peptide ligand library technology (ProteoMiner) to reduce the dynamic range of protein concentration in CSF and unmask previously undetected proteins by nano-LC-MS/MS analysis on an LTQ-Orbitrap mass spectrometer. This method was first applied on a large pool of CSF from different sources with the aim to better characterize the protein content of this fluid, especially for the low abundance components. We were able to identify 1212 proteins in CSF, and among these, 745 were only detected after peptide library treatment. However, additional difficulties for clinical studies of CSF are the low protein concentration of this fluid and the low volumes typically obtained after lumbar puncture, precluding the conventional use of ProteoMiner with large volume columns for treatment of patient samples. The method has thus been optimized to be compatible with low volume samples. We could show that the treatment is still efficient with this miniaturized protocol and that the dynamic range of protein concentration is actually reduced even with small amounts of beads, leading to an increase of more than 100% of the number of identified proteins in one LC-MS/MS run. Moreover, using a dedicated bioinformatics analytical work flow, we found that the method is reproducible and applicable for label-free quantification of series of samples processed in parallel. Molecular & Cellular Proteomics 9:1006 -1021, 2010.

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“…Inevitably they identified many proteins that were altered in HD CSF, but the majority of these disease-associated changes were in proteins which were said to be liver-specific. There was a rather sur-prising tendency for brain-derived proteins to decline in HD CSF, with the exception of neuroinflammatory markers [80]. These findings highlight the inconsistencies between proteomic techniques and the nature of such studies as hypothesis-generating engines for future targeted work in properly powered sample sets.…”

Section: Proteomic Approachesmentioning

confidence: 82%

“…ApoA is a glycoprotein associated with inhibition of food intake and regulation of body weight. All three were higher in HD patients compared to matched controls [61] but these changes were not independently replicated using a more quantitative assay -though Fang and colleagues had also found robust elevations of ApoA in HD CSF in their previous proteomic work [80].…”

Section: Proteomic Approachesmentioning

confidence: 99%

Cerebrospinal Fluid Biomarkers for Huntington’s Disease

Byrne¹,

Wild

2016

JHD

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Abstract. Cerebrospinal fluid (CSF) is enriched in brain-derived components and represents an accessible and appealing means of interrogating the CNS milieu to study neurodegenerative diseases and identify biomarkers to facilitate the development of novel therapeutics. Many such CSF biomarkers have been proposed for Huntington's disease (HD) but none has been validated for clinical trial use. Across many studies proposing dozens of biomarker candidates, there is a notable lack of statistical power, consistency, rigor and validation. Here we review proposed CSF biomarkers including neurotransmitters, transglutaminase activity, kynurenine pathway metabolites, oxidative stress markers, inflammatory markers, neuroendocrine markers, protein markers of neuronal death, proteomic approaches and mutant huntingtin protein itself. We reflect on the need for large-scale, standardized CSF collections with detailed phenotypic data to validate and qualify much-needed CSF biomarkers for clinical trial use in HD.

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Brain-specific Proteins Decline in the Cerebrospinal Fluid of Humans with Huntington Disease

Cited by 82 publications

References 51 publications

Ciliogenesis is regulated by a huntingtin-HAP1-PCM1 pathway and is altered in Huntington disease

Ciliogenesis is regulated by a huntingtin-HAP1-PCM1 pathway and is altered in Huntington disease

In-depth Exploration of Cerebrospinal Fluid by Combining Peptide Ligand Library Treatment and Label-free Protein Quantification

Cerebrospinal Fluid Biomarkers for Huntington’s Disease

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