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Serum and Cerebrospinal Fluid Levels of Transthyretin in Lewy Body Disorders with and without Dementia

  • Walter Maetzler ,

    Contributed equally to this work with: Walter Maetzler, Youyong Tian, Stephanie Maria Baur

    walter.maetzler@uni-tuebingen.de

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Youyong Tian ,

    Contributed equally to this work with: Walter Maetzler, Youyong Tian, Stephanie Maria Baur

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany, Department of Neurology, Nanjing First Hospital of Nanjing Medical University, Nanjing, China

  • Stephanie Maria Baur ,

    Contributed equally to this work with: Walter Maetzler, Youyong Tian, Stephanie Maria Baur

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Tina Gauger,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Bartholomäus Odoj,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Benjamin Schmid,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Claudia Schulte,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Christian Deuschle,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Susanna Heck,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Anja Apel,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Arthur Melms,

    Affiliation Center of Neurology, General Neurology Department, University of Tuebingen, Tuebingen, Germany

  • Thomas Gasser,

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

  • Daniela Berg

    Affiliations Center of Neurology, Department of Neurodegeneration and Hertie Institute for Clinical Brain Research, University of Tuebingen, Tuebingen, Germany, DZNE, German Center for Neurodegenerative Diseases, Tuebingen, Germany

Abstract

Parkinson’s disease (PD) without (non-demented, PDND) and with dementia (PDD), and dementia with Lewy bodies (DLB) are subsumed under the umbrella term Lewy body disorders (LBD). The main component of the underlying pathologic substrate, i.e. Lewy bodies and Lewy neurites, is misfolded alpha-synuclein (Asyn), and - in particular in demented LBD patients - co-occurring misfolded amyloid-beta (Abeta). Lowered blood and cerebrospinal fluid (CSF) levels of transthyretin (TTR) - a clearance protein mainly produced in the liver and, autonomously, in the choroid plexus - are associated with Abeta accumulation in Alzheimer’s disease. In addition, a recent study suggests that TTR is involved in Asyn clearance. We measured TTR protein levels in serum and cerebrospinal fluid of 131 LBD patients (77 PDND, 26 PDD, and 28 DLB) and 72 controls, and compared TTR levels with demographic and clinical data as well as neurodegenerative markers in the CSF. Five single nucleotide polymorphisms of the TTR gene which are considered to influence the ability of the protein to carry its ligands were also analyzed. CSF TTR levels were significantly higher in LBD patients compared to controls. Post-hoc analysis demonstrated that this effect was driven by PDND patients. In addition, CSF TTR levels correlated negatively with CSF Abeta1–42, total tau and phospho-tau levels. Serum TTR levels did not significantly differ among the studied groups. There were no relevant associations between TTR levels and genetic, demographic and clinical data, respectively. These results suggest an involvement of the clearance protein TTR in LBD pathophysiology, and should motivate to elucidate TTR-related mechanisms in LBD in more detail.

Introduction

The term “Lewy body disorders (LBD)” subsumes the three entities Parkinson’s disease (PD) without dementia (PDND), PD with dementia (PDD), and dementia with Lewy bodies (DLB) [1]. In LBD, alpha-synuclein (Asyn)-positive Lewy bodies (LB) and Lewy neurites occur together with neurodegeneration [2].

Moreover, co-occurrence of amyloid-beta (Abeta) deposits with Asyn pathology is common, particularly in LBD patients with dementia [3], [4]. It is widely accepted that an Abeta1–42 production higher than its removal results in an enhanced presence of Abeta1–42 monomers, oligomers, insoluble fibrils and plaques in the central nervous system [5]. Age, ApoE genotype [6] as well as proteins and metabolites such as apolipoprotein E [7], apolipoprotein J (clusterin) [8], apolipoprotein A1 [9], uric acid [10], neprilysin [11], tau proteins [12], cystatin C [13], and transthyretin [14], [15] play a role in the neurotoxic aggregation of the usually soluble form of Abeta1–42. Similar mechanisms may lead to Asyn accumulation, at least for late onset PD although there is less evidence for this hypothesis [16].

The transthyretin (TTR) gene is located at chromosome 18q11 and consists of four exons [17]. TTR is mainly synthesized in the liver and the epithelial cells of the choroid plexus [18]. Recent results indicate that it is also a neuronal product up-regulated in Alzheimer’s disease (AD) [19]. It has binding sites for retinol binding protein (RBP), thyroxin and also for Abeta1–42 [20]. It can influence Abeta1–42 aggregation and destroy already formed Abeta1–42 fibrils by proteolytic cleavage of the peptides [21]. It has been suggested that TTR may be one of the major Abeta1–42-binding and -sequestering proteins in human cerebrospinal fluid (CSF) [14], [15]. Increased production of TTR in neurons exposed to Abeta1–42 toxicity, and reduced levels of the protein in blood [22], [23] and CSF [24][26] indicate an involvement of TTR (dys)function in clearance deficits as they occur in AD. In addition, there is very recent - at least indirect - evidence that TTR may be involved in Asyn clearance. Guerreiro and colleagues [27] observed highly increased levels of monomeric and oligomerized Asyn in the saliva of symptomatic heterozygous V30M TTR mutation carriers suffering from familial amyloidosis compared to healthy control individuals. Interestingly, Asyn levels in saliva of symptomatic TTR mutation carriers who underwent orthotropic liver transplantation (and, consecutively, had non-mutated TTR) were comparable with those of controls.

It has been demonstrated that not only the relatively rare mutations but also common variants of the TTR gene are differentially capable of altering the ability of TTR to carry and transport its ligands [28]. This has been shown in particular for the TTR single nucleotide polymorphisms (SNPs) rs13381522 and rs3764478 (both lie at the 5`end in the promoter region of the TTR gene), rs1800458 (located in exon 2, leads to a non-synonymous amino acid exchange of glycin to serin on position 26 of the TTR nucleotide sequence), rs723744 (localized in intron 3, does not result in amino acid differences), and rs36204272 (is intronic and spliced posttranslationally, should have no effect on the TTR protein) [15], [29][31]. As LBD patients obviously show neuronal and neural clearance deficits comparable to AD [16] and TTR seems to be critically involved in these mechanisms, we hypothesized that blood and CSF levels of TTR are altered in LBD patients and may be associated with clinical and demographic data, and that occurrence of the abovementioned SNPs are associated with these TTR levels.

Study Participants, Material and Methods

Ethics Statement

The study was approved by the ethics committee of the Medical Faculty, University of Tuebingen, Germany, and was performed according to the principles expressed in the Declaration of Helsinki. All participants gave their written informed consent. In case of compromised capacity of the participants to consent (MMSE <18 points), or another person was named to make decisions on behalf of the person, responsible persons consented on the behalf of the participant.

Study Participants

Demented DLB, PDD and non-demented LBD patients (PDND), and elderly neurodegeneratively healthy control individuals (HC) were recruited from the ward and the outpatient clinic of the Neurodegenerative Department of the University of Tuebingen. LBD patients were diagnosed based on clinical criteria by specialists in the field of neurodegenerative movement disorders (DB, TG, WM). All PD patients fulfilled the UKPDS Brain Bank criteria [32]. PDD patients, in addition, met the Diagnostic and Statistical Manual of Mental Disorders-IV (DSM-IV) criteria for dementia as well as core and associated clinical features proposed by Emre and colleagues [33]. All DLB patients fulfilled the McKeith criteria for clinical diagnosis of probable DLB [34]. Control individuals underwent spinal taps for exclusion of vascular events or inflammatory conditions. Any clinical sign for a neurodegenerative disorder led to exclusion from the study.

All individuals underwent demographic analysis and clinical testing including a Hoehn&Yahr (H&Y) staging and a Mini-Mental State Examination (MMSE). Table 1 provides an overview of demographic, clinical, and biochemical data of the groups.

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Table 1. Demographic, clinical, and routine biochemical data.

https://doi.org/10.1371/journal.pone.0048042.t001

Cerebrospinal Fluid and Serum Collection

CSF and serum collection as well as determination of routine diagnostic parameters were performed according to standardized protocols (for details see [35]). We only used samples specifically dedicated to this project from our biobank (http://www.hih-tuebingen.de/de/nd/biobank/for-researchers/), without any previous freeze-thaw cycle. Our biobank fulfills highest international standards with regard to collection, preparation and storage of biosamples. Samples for determination of TTR levels were centrifuged (CSF: 4000 g, 4°C, 10 min; blood: 2000 g, 4°C, 10 min) and stored at −80°C within 60 minutes after collection until analysis. Only samples of patients with normal routine CSF diagnostics were included in the study, slightly increased CSF albumin levels (up to 450 mg/L) were tolerated.

TTR, Abeta1–42, Total Tau and Phospho-tau Measurement

TTR levels in CSF and serum were measured using a laser nephelometric method with Ics Pab Prealbumin Reagent Test Kit on Beckman Coulter IMMAGE® Immunochemistry Systems according to manufacturer’s instructions (Beckman Coulter GmbH, Krefeld, Germany). Samples were run in triplicate. We observed within run precision of <2.0% coefficient of variation (CV), and total precision of <5% CV.

CSF Abeta1–42, total tau and phospho-tau levels were determined using commercially available ELISA kits (Innogenetics NV, Ghent, Belgium).

TTR and ApoE Genotyping

Genomic DNA was extracted using standard protocols. The coding sequence of the TTR gene was determined with Sanger-sequencing technique to identify the SNPs rs1800458 and rs36204272. SNPs rs13381522, rs3764478, and rs723744 which are located at the TTR intron or promoter region were analyzed by the SNaPshot method. Briefly, a PCR with specific SNaPshot primers was performed. After single base extension with fluorescent-labeled ddNTPs the SNaPshot product was analyzed by capillary gel electrophoresis with ABI Prism 3100 Genetic Analyzer sequencer (Applied Biosystems Life Technologies GmbH, Darmstadt, Germany). Fluorescence data were analyzed using Gene Mapper v3.5.

ApoE genotypes were obtained by PCR amplification of exon 4 of the ApoE gene, and subsequent digestion with enzyme HhaI according to [36]. All SNPs investigated were in Hardy-Weinberg equilibrium.

Data Analysis

Data were analyzed with JMP software (version 9.0.2, SAS). As dementia associated with LBD may per se be a relevant factor associated with TTR levels, PDD and DLB were not only considered as single groups but also comprised as a PDD/DLB group (see Table S1 for details). Demographic and clinical data were analyzed with the Wilcoxon signed rank test (LBD versus controls; presented as median and range) or Fishers exact test. As age was significantly different between LBD and controls and as there is some evidence that serum TTR may be associated with age [37], we corrected both serum and CSF TTR levels for this covariate using a regression model. The coefficient of determination (r2) was used as a measure for the proportion of response variation which was explained by the regressors in the model. Significance of each model effect was assessed by the likelihood ratio.

Differences were considered significant at p<0.05. Post-hoc analyses (TTR levels of PDND versus controls, PDND versus demented LBD, controls versus demented LBD) were corrected for multiple testing (see Table 2 and Table S1 for details).

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Table 2. Transthyretin values of the investigated cohorts.

https://doi.org/10.1371/journal.pone.0048042.t002

Results

TTR Levels and Demographic Variables

TTR values in CSF and serum were normally distributed, and did not correlate. They were not age-related, neither in CSF (controls, r2 = 0.02, p = 0.88; LBD patients, r2 = 0.01, p = 0.64) nor in serum (controls, r2 = 0.01, p = 0.19; LBD patients, r2 = 0.02, p = 0.11). CSF TTR values were approx. 18-fold lower than serum values (1.7 versus 30.1 mg/dl).

Gender did not differ significantly between LBD patients and controls. CSF TTR values were comparable between females and males (controls, p = 0.56; LBD patients, p = 0.59). Serum TTR levels were significantly higher in males than in females (controls, p = 0.03; LBD patients, p = 0.002) and were therefore calculated separately.

TTR Levels and LBD-associated Parameters

An overview is given in Table 2. CSF TTR values were significantly higher in LBD patients (1.73 mg/dl) compared to controls (1.58 mg/dl). The post-hoc analysis demonstrated that, within the LBD group, PDND patients accounted for this effect (1.80 mg/dl, r2 = 0.07, p = 0.008 compared to controls). Serum TTR levels were not significantly different between LBD patients and controls, and among LBD patients (see also Table S1).

CSF and serum TTR values were neither significantly associated with clinical parameters (age at onset of parkinsonism, duration of parkinsonism, Hoehn&Yahr stage, age at onset of dementia, duration of dementia, MMSE score), nor with ApoE status.

TTR Levels and Neurodegenerative Markers

There were weak but significant negative correlations between CSF TTR values and respective levels of CSF Abeta1–42 (r2 = 0.03, p = 0.02), CSF total tau (r2 = 0.03, p = 0.02) and CSF phospho-tau (r2 = 0.03, p = 0.03). No significant correlations were detectable between serum TTR values and neurodegenerative markers.

TTR Genotypes

None of the analyzed TTR SNPs (rs723744, rs13381522, rs3764478, rs1800458 and rs36204272) showed a significant association with LBD occurrence. In addition, no relevant associations of the SNPs with demographical, clinical and biochemical parameters were detectable (data not shown).

Discussion

In this study investigating TTR values in blood and CSF of LBD patients, CSF TTR levels were significantly higher in this cohort of patients compared to controls. The effect was mainly driven by non-demented LBD patients, explaining, as a diagnosis, approximately 7 percent of the variation in the CSF TTR levels. This makes it tempting to speculate that Asyn pathology alone (PDND patients rarely have marked additional brain pathology such as leucoaraiosis [38], [39] and Abeta1–42 pathology [4], [23], [40]) induces expression of central TTR. This observation may be explained by the known occurrence of oxidative stress in LBD [35], [41], as CSF TTR values have been observed to rise in response to oxidative stress [14]. In addition, an involvement of TTR in inflammatory processes - a common feature observed in brains of patients suffering from LBD - has also been suggested [42]. In the light of previous reports which mainly found decreased CSF TTR levels in disorders that are not primarily associated with inflammation (i.e., depression [43], AD [14], [24] and amyotrophic lateral sclerosis [44]), but increased levels in disorders typically associated with inflammatory processes (such as Guillain Barré syndrome and chronic inflammatory demyelinating polyneuropathy [45][47]) it may be interesting to focus in future studies on putative interaction pathways between inflammation and TTR in Asyn-associated pathology.

Actually it is not entirely clear whether (misfolded) Asyn is a target protein of TTR. The latter mainly functions as a transport protein, and is able to transfer e.g. Abeta1–42, as a misfolded peptide, from the neuron to the CSF [25]. A recent study also showed that Abeta1–42-stressed neurons increase the expression of TTR [48]. Thus it is intriguing to hypothesize that Asyn is also a target protein of TTR, and TTR may have an influence on Asyn-associated pathology. Indeed, indirect evidence for this suggestion comes from a recent study investigating levels of monomeric and oligomeric Asyn in saliva using MALDI-TOFTOF MSMS ion search and Western blotting [27]. In this study, symptomatic individuals with a heterozygous V30M mutation in TTR had much more intense Asyn-positive bands and a higher number of such bands at higher molecular mass (indicative of oligomeric forms of Asyn) than had control individuals and, most interestingly, TTR mutation carriers who underwent orthotropic liver transplantation. This strongly indicates that TTR is associated with clearance of (misfolded) Asyn.

Interestingly, demented LBD patients had relatively low CSF TTR levels, comparable to controls [49]. This is exciting in the light of recent studies demonstrating decreased CSF TTR levels in AD patients [14], [24], and the regular occurrence of Abeta1–42 pathology in demented LBD patients. Together with the observation that PDND patients have increased CSF TTR levels one may hypothesize that demented LBD patients face two driving forces with regard to TTR-associated pathways: Asyn pathology which goes along with increased TTR expression, and Abeta1–42 pathology associated with decreased TTR expression. Based on the abovementioned associations between TTR levels and amyloid pathology, one can also hypothesize that increased TTR levels in the brain protect against Abeta1–42 pathology. Indeed, there is accumulating evidence from in-vitro and in-vivo studies that TTR has beneficial direct and indirect effects on Abeta-associated pathology (reviewed in [14]).

Serum TTR levels were not significantly different between LBD patients and controls. Post-hoc analyses demonstrated slightly reduced TTR levels in demented compared to non-demented LBD patients. Although results did not survive correction for multiple testing, they may motivate to future, hypothesis-driven studies focusing on this particular aspect as decreased serum TTR levels have already been described in AD patients [22], [23], [50],, and are regarded as a biochemical marker for malnutrition [25], [51] and inflammation [52].

We found weak but significant negative correlations between CSF TTR levels and the three actually best-established neurodegenerative markers in CSF, i.e. Abeta1–42, total tau and phospho-tau. Together with the observed lack of such an association between peripheral TTR and these neurodegenerative markers, the observations may point to a specific interaction of central TTR with LBD-associated amyloid clearance. Higher CSF TTR levels were observed in non-demented LBD patients who regularly show relatively low CSF tau levels [53], [54]. This argues for an interaction of TTR with the specific neurodegenerative process (total tau) and axonal pathology (phospho-tau). The negative correlation between TTR and Abeta1–42 CSF levels is somehow counterintuitive and more difficult to explain as, in individuals with Abeta1–42 pathology, CSF Abeta1–42 is regularly low and tau parameters are high. Under physiological conditions, CSF TTR binds Abeta1–42 and keeps it soluble especially in CSF [25]. Decreased CSF TTR values may indicate that this dynamic equilibrium is affected, leading to accumulation and aggregation of Abeta1–42 proteins, amyloid formation, and neurotoxicity [15].

Analysis of SNPs that have been shown to influence binding capacity of TTR to amyloid did not add relevant information in this study. This may be due to sample size, but also to the fact that rather the absolute quantity of TTR than its function may be associated with LBD pathophysiology. Interestingly, we also did not find a significant association between demographic and clinical parameters (except the above reported, diagnosis of LBD and occurrence of dementia), and TTR values. This may indicate that TTR, although obviously involved in amyloidogenic and clearance pathways in LBD, cannot serve as a marker of disease progression and severity.

In conclusion, data presented in this study argue for a role of TTR in both Asyn- and Abeta1–42-associated LBD pathologies. The obvious interaction of centrally produced TTR with pathophysiological mechanisms in these neurodegenerative processes should motivate to more in-depth analyses.

Supporting Information

Table S1.

Post-hoc analyses of transthyretin levels between different groups

https://doi.org/10.1371/journal.pone.0048042.s001

(DOC)

Acknowledgments

The technical help of Siegfried Ebner is greatly appreciated.

Author Contributions

Conceived and designed the experiments: WM T. Gasser DB. Performed the experiments: YT SMB T. Gauger BO BS CS CD SH. Analyzed the data: WM AA AM. Contributed reagents/materials/analysis tools: WM AM T. Gasser DB. Wrote the paper: WM AA DB.

References

  1. 1. Lippa CF, Duda JE, Grossman M, Hurtig HI, Aarsland D, et al. (2007) DLB and PDD boundary issues: diagnosis, treatment, molecular pathology, and biomarkers. Neurology 68: 812–819.
  2. 2. Buchman AS, Shulman JM, Nag S, Leurgans SE, Arnold SE, et al. (2012) Nigral pathology and parkinsonian signs in elders without Parkinson disease. Ann Neurol 71: 258–266.
  3. 3. Braak H, Rub U, Jansen Steur EN, Del Tredici K, de Vos RA (2005) Cognitive status correlates with neuropathologic stage in Parkinson disease. Neurology 64: 1404–1410.
  4. 4. Maetzler W, Liepelt I, Reimold M, Reischl G, Solbach C, et al. (2009) Cortical PIB binding in Lewy body disease is associated with Alzheimer-like characteristics. Neurobiol Dis 34: 107–112.
  5. 5. Mawuenyega KG, Sigurdson W, Ovod V, Munsell L, Kasten T, et al. (2010) Decreased clearance of CNS beta-amyloid in Alzheimer's disease. Science 330: 1774.
  6. 6. Pankratz N, Byder L, Halter C, Rudolph A, Shults CW, et al. (2006) Presence of an APOE4 allele results in significantly earlier onset of Parkinson's disease and a higher risk with dementia. Mov Disord 21: 45–49.
  7. 7. Strittmatter WJ, Weisgraber KH, Huang DY, Dong LM, Salvesen GS, et al. (1993) Binding of human apolipoprotein E to synthetic amyloid beta peptide: isoform-specific effects and implications for late-onset Alzheimer disease. Proc Natl Acad Sci U S A 90: 8098–8102.
  8. 8. Ghiso J, Matsubara E, Koudinov A, Choi-Miura NH, Tomita M, et al. (1993) The cerebrospinal-fluid soluble form of Alzheimer's amyloid beta is complexed to SP-40,40 (apolipoprotein J), an inhibitor of the complement membrane-attack complex. Biochem J 293 (Pt 1): 27–30.
  9. 9. Roher AE, Maarouf CL, Sue LI, Hu Y, Wilson J, et al. (2009) Proteomics-derived cerebrospinal fluid markers of autopsy-confirmed Alzheimer's disease. Biomarkers 14: 493–501.
  10. 10. Maetzler W, Stapf AK, Schulte C, Hauser AK, Lerche S, et al. (2011) Serum and cerebrospinal fluid uric acid levels in lewy body disorders: associations with disease occurrence and amyloid-beta pathway. J Alzheimers Dis 27: 119–126.
  11. 11. Maetzler W, Stoycheva V, Schmid B, Schulte C, Hauser AK, et al. (2010) Neprilysin activity in cerebrospinal fluid is associated with dementia and amyloid-beta42 levels in Lewy body disease. J Alzheimers Dis 22: 933–938.
  12. 12. Arai H, Terajima M, Miura M, Higuchi S, Muramatsu T, et al. (1995) Tau in cerebrospinal fluid: a potential diagnostic marker in Alzheimer's disease. Ann Neurol 38: 649–652.
  13. 13. Maetzler W, Schmid B, Synofzik M, Schulte C, Riester K, et al. (2010) The CST3 BB genotype and low cystatin C cerebrospinal fluid levels are associated with dementia in Lewy body disease. J Alzheimers Dis 19: 937–942.
  14. 14. Li X, Buxbaum JN (2011) Transthyretin and the brain re-visited: is neuronal synthesis of transthyretin protective in Alzheimer's disease? Mol Neurodegener 6: 79.
  15. 15. Schwarzman AL, Gregori L, Vitek MP, Lyubski S, Strittmatter WJ, et al. (1994) Transthyretin sequesters amyloid beta protein and prevents amyloid formation. Proc Natl Acad Sci U S A 91: 8368–8372.
  16. 16. Deleidi M, Maetzler W (2012) Protein clearance mechanisms of alpha-synuclein and amyloid-beta as potential biomarker sources in Lewy body disorders. Int J Alzheimer's Disease doi:10.1155/2012/391438.
  17. 17. Tsuzuki T, Mita S, Maeda S, Araki S, Shimada K (1985) Structure of the human prealbumin gene. J Biol Chem 260: 12224–12227.
  18. 18. Schreiber G, Aldred AR, Jaworowski A, Nilsson C, Achen MG, et al. (1990) Thyroxine transport from blood to brain via transthyretin synthesis in choroid plexus. Am J Physiol 258: R338–345.
  19. 19. Li X, Masliah E, Reixach N, Buxbaum JN (2011) Neuronal production of transthyretin in human and murine Alzheimer's disease: is it protective? J Neurosci 31: 12483–12490.
  20. 20. Du J, Cho PY, Yang DT, Murphy RM (2012) Identification of beta-amyloid-binding sites on transthyretin. Protein Eng Des Sel 25: 337–345.
  21. 21. Costa R, Goncalves A, Saraiva MJ, Cardoso I (2008) Transthyretin binding to A-Beta peptide–impact on A-Beta fibrillogenesis and toxicity. FEBS Lett 582: 936–942.
  22. 22. Velayudhan L, Killick R, Hye A, Kinsey A, Guentert A, et al. (2012) Plasma transthyretin as a candidate marker for Alzheimer's disease. J Alzheimers Dis 28: 369–375.
  23. 23. Han SH, Jung ES, Sohn JH, Hong HJ, Hong HS, et al. (2011) Human serum transthyretin levels correlate inversely with Alzheimer's disease. J Alzheimers Dis 25: 77–84.
  24. 24. Gloeckner SF, Meyne F, Wagner F, Heinemann U, Krasnianski A, et al. (2008) Quantitative analysis of transthyretin, tau and amyloid-beta in patients with dementia. J Alzheimers Dis 14: 17–25.
  25. 25. Serot JM, Christmann D, Dubost T, Couturier M (1997) Cerebrospinal fluid transthyretin: aging and late onset Alzheimer's disease. J Neurol Neurosurg Psychiatry 63: 506–508.
  26. 26. Hansson O, Zetterberg H, Buchhave P, Londos E, Blennow K, et al. (2006) Association between CSF biomarkers and incipient Alzheimer's disease in patients with mild cognitive impairment: a follow-up study. Lancet Neurol 5: 228–234.
  27. 27. Guerreiro A, da Costa G, Gomes RA, Ribeiro-Silva C, Gilberto S, et al. (2012) alpha-Synuclein aggregation in the saliva of familial transthyretin amyloidosis: a potential biomarker. Amyloid 19: 74–80.
  28. 28. Ruano D, Macedo A, Soares MJ, Valente J, Azevedo MH, et al. (2007) Transthyretin: no association between serum levels or gene variants and schizophrenia. J Psychiatr Res 41: 667–672.
  29. 29. Cuenco KT, Friedland R, Baldwin CT, Guo J, Vardarajan B, et al. (2011) Association of TTR polymorphisms with hippocampal atrophy in Alzheimer disease families. Neurobiol Aging 32: 249–256.
  30. 30. Natunen T, Helisalmi S, Vepsalainen S, Sarajarvi T, Antikainen L, et al. (2012) Genetic analysis of genes involved in amyloid-beta degradation and clearance in Alzheimer's disease. J Alzheimers Dis 28: 553–559.
  31. 31. Olsson M, Norgren N, Obayashi K, Plante-Bordeneuve V, Suhr OB, et al. (2010) A possible role for miRNA silencing in disease phenotype variation in Swedish transthyretin V30M carriers. BMC Med Genet 11: 130.
  32. 32. Gibb WR, Lees AJ (1988) A comparison of clinical and pathological features of young- and old-onset Parkinson's disease. Neurology 38: 1402–1406.
  33. 33. Emre M, Aarsland D, Brown R, Burn DJ, Duyckaerts C, et al. (2007) Clinical diagnostic criteria for dementia associated with Parkinson's disease. Mov Disord 22: 1689–1707.
  34. 34. McKeith IG, Dickson DW, Lowe J, Emre M, O'Brien JT, et al. (2005) Diagnosis and management of dementia with Lewy bodies: third report of the DLB Consortium. Neurology 65: 1863–1872.
  35. 35. Maetzler W, Schmid SP, Wurster I, Liepelt I, Gaenslen A, et al. (2011) Reduced but not oxidized cerebrospinal fluid glutathione levels are lowered in Lewy body diseases. Mov Disord 26: 176–181.
  36. 36. Hixson JE, Vernier DT (1990) Restriction isotyping of human apolipoprotein E by gene amplification and cleavage with HhaI. J Lipid Res 31: 545–548.
  37. 37. Ritchie RF, Palomaki GE, Neveux LM, Navolotskaia O, Ledue TB, et al. (1999) Reference distributions for the negative acute-phase serum proteins, albumin, transferrin and transthyretin: a practical, simple and clinically relevant approach in a large cohort. J Clin Lab Anal 13: 273–279.
  38. 38. Bohnen NI, Muller ML, Kuwabara H, Constantine GM, Studenski SA (2009) Age-associated leukoaraiosis and cortical cholinergic deafferentation. Neurology 72: 1411–1416.
  39. 39. Bohnen NI, Muller ML, Zarzhevsky N, Koeppe RA, Bogan CW, et al. (2011) Leucoaraiosis, nigrostriatal denervation and motor symptoms in Parkinson's disease. Brain 134: 2358–2365.
  40. 40. Shirahama T, Skinner M, Westermark P, Rubinow A, Cohen AS, et al. (1982) Senile cerebral amyloid. Prealbumin as a common constituent in the neuritic plaque, in the neurofibrillary tangle, and in the microangiopathic lesion. Am J Pathol 107: 41–50.
  41. 41. Vicente Miranda H, Outeiro TF (2010) The sour side of neurodegenerative disorders: the effects of protein glycation. J Pathol 221: 13–25.
  42. 42. Santos SD, Lambertsen KL, Clausen BH, Akinc A, Alvarez R, et al. (2010) CSF transthyretin neuroprotection in a mouse model of brain ischemia. J Neurochem 115: 1434–1444.
  43. 43. Hatterer JA, Herbert J, Hidaka C, Roose SP, Gorman JM (1993) CSF transthyretin in patients with depression. Am J Psychiatry 150: 813–815.
  44. 44. Ryberg H, An J, Darko S, Lustgarten JL, Jaffa M, et al. (2010) Discovery and verification of amyotrophic lateral sclerosis biomarkers by proteomics. Muscle Nerve 42: 104–111.
  45. 45. Tumani H, Pfeifle M, Lehmensiek V, Rau D, Mogel H, et al. (2009) Candidate biomarkers of chronic inflammatory demyelinating polyneuropathy (CIDP): proteome analysis of cerebrospinal fluid. J Neuroimmunol 214: 109–112.
  46. 46. Zhang HL, Zhang XM, Mao XJ, Deng H, Li HF, et al. (2012) Altered cerebrospinal fluid index of prealbumin, fibrinogen, and haptoglobin in patients with Guillain-Barre syndrome and chronic inflammatory demyelinating polyneuropathy. Acta Neurol Scand 125: 129–135.
  47. 47. Chiang HL, Lyu RK, Tseng MY, Chang KH, Chang HS, et al. (2009) Analyses of transthyretin concentration in the cerebrospinal fluid of patients with Guillain-Barre syndrome and other neurological disorders. Clin Chim Acta 405: 143–147.
  48. 48. Buxbaum JN, Ye Z, Reixach N, Friske L, Levy C, et al. (2008) Transthyretin protects Alzheimer's mice from the behavioral and biochemical effects of Abeta toxicity. Proc Natl Acad Sci U S A 105: 2681–2686.
  49. 49. Riisoen H (1988) Reduced prealbumin (transthyretin) in CSF of severely demented patients with Alzheimer's disease. Acta Neurol Scand 78: 455–459.
  50. 50. Elovaara I, Maury CP, Palo J (1986) Serum amyloid A protein, albumin and prealbumin in Alzheimer's disease and in demented patients with Down's syndrome. Acta Neurol Scand 74: 245–250.
  51. 51. Carriere I, Dupuy AM, Lacroux A, Cristol JP, Delcourt C (2008) Biomarkers of inflammation and malnutrition associated with early death in healthy elderly people. J Am Geriatr Soc 56: 840–846.
  52. 52. Myron Johnson A, Merlini G, Sheldon J, Ichihara K (2007) Scientific Division Committee on Plasma Proteins IFoCC, et al (2007) Clinical indications for plasma protein assays: transthyretin (prealbumin) in inflammation and malnutrition. Clin Chem Lab Med 45: 419–426.
  53. 53. Mollenhauer B, Locascio JJ, Schulz-Schaeffer W, Sixel-Doring F, Trenkwalder C, et al. (2011) alpha-Synuclein and tau concentrations in cerebrospinal fluid of patients presenting with parkinsonism: a cohort study. Lancet Neurol 10: 230–240.
  54. 54. Shi M, Bradner J, Hancock AM, Chung KA, Quinn JF, et al. (2011) Cerebrospinal fluid biomarkers for Parkinson disease diagnosis and progression. Ann Neurol 69: 570–580.