| Literature DB >> 31206565 |
Nina Schultz1, Shorena Janelidze1, Elin Byman1, Lennart Minthon1, Katarina Nägga1,2, Oskar Hansson1,3, Malin Wennström1.
Abstract
The biologically active pancreatic hormone peptide islet amyloid polypeptide (IAPP) regulates brain functions such as appetite and cognition. It also plays a role in clearance of amyloid beta (Aβ), a peptide implicated in the dementia disorder Alzheimer's disease (AD). If IAPP becomes modified, it loses its biological activity and starts to aggregate. Such aggregations have been found in the AD brain and decreased plasma levels of the unmodified IAPP (uIAPP) have been shown in the same patients. In the current study, we analyze levels of uIAPP and total IAPP (unmodified and modified) in cerebrospinal fluid (CSF) to investigate its potential as a biomarker for AD. We found no differences in neither CSF nor plasma levels of uIAPP or total IAPP in AD patients compared to cognitive healthy individuals (NC). The levels of uIAPP in CSF of NC were positively correlated with uIAPP in plasma, Q-albumin and albumin levels in CSF, but negatively correlated with CSF levels of t-tau and p-tau. These findings were not seen in AD patients. Levels of total CSF IAPP correlated positively with total Q-albumin and albumin levels in CSF in both AD and NC. In addition, total plasma IAPP correlated positively with CSF t-tau and p-tau in NC and negatively with CSF Aβ42 in AD patients. To conclude, our studies did not find evidence supporting the use of CSF IAPP as an AD biomarker. However, our findings, indicating a compromised translocation of uIAPP in and out of the brain in AD patients as well as the correlations between total plasma IAPP and AD biomarkers, encourage further research on the role for IAPP in AD.Entities:
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Year: 2019 PMID: 31206565 PMCID: PMC6576764 DOI: 10.1371/journal.pone.0218561
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Fig 1Correlations between CSF unmodified IAPP and Q-albumin, CSF albumin and AD biomarkers.
Scatter plots demonstrating significant correlations between logarithmic transformed values of unmodified CSF IAPP and logarithmic transformed values of unmodified plasma IAPP (A), logarithmic transformed values of Q-Alb (B), logarithmic transformed values of CSF albumin levels (C), logarithmic transformed values of CSF t-tau levels (D) and logarithmic transformed values of CSF p-tau levels in cognitively healthy individuals (NCs)(E). Data was analyzed with Pearson correlation test. * Significant correlation at p<0.05 level.
Data on individuals included in the study.
| Variables | NC (n = 44) | AD (n = 30) | T2D + AD (n = 7) |
|---|---|---|---|
| Age (years) | 73.41 ± 6.16 | 73.57 ± 6.56 | 75.57 ± 11.24 |
| Gender (M/F) | 13/31 | 9/21 | 1/6 |
| APOEε4 carrier (no) | 17 | 21 | 4 |
| MMSE | 29.18 ± 0.81 | 19.50 ± 4.26 | 20.57 ± 5.13 |
| Q-albumin | 6.68 ± 3.73 | 6.80 ± 2.54 | 8.39 ± 6.23 |
| CSF albumin (mg/l) | 267.20 ± 164.03 | 268.967 ± 108.28 | 311.14 ± 221.27 |
| CSF Aβ42 (pg/ml) | 790.76 ± 291.04 | 386.70 ± 110.29 | 522.51 ± 112.73 |
| CSF t-tau (pg/ml) | 344.34 ± 105.12 | 621.81 ± 207.42 | 683.78 ± 213.30 |
| CSF p-tau (pg/ml) | 46.11 ± 18.21 | 120.40 ± 41.23 | 119.14 ± 57.43 |
| CSF uIAPP (pM) | 2.74 ± 1.38 | 2.81 ± 0.88 | 3.20 ± 1.72 |
| Plasma uIAPP (pM) | 262.81 ± 162.86 | 316.82 ± 159.52 | 428.78 ± 162.41 |
| CSF IAPP WB (abs) | 289447.81± 89972.04 | 262526.62 ± 72777.26 | 246513.14 ± 80454.55 |
| CSF total IAPP (abs) | 1.36 ± 0.18 | 1.37 ± 0.16 | 1.36 ± 0.10 |
| Plasma total IAPP (abs) | 1.31 ± 0.17 | 1.31 ± 0.18 | 1.21 ± 0.23 |
NC = cognitive healthy individuals controls, AD = Alzheimer’s disease patients, AD+T2D = patients with Alzheimer’s disease and type 2 diabetes.
a = data is missing on NC n = 1.
b = data is missing on AD n = 1. Data is analyzed using ANOVA followed by Dunnett post-hoc test and values are presented as mean value ± SD.
* Significant correlation at p<0.05 level.
** Significant correlation at p<0.01 level.
*** Significant correlation at p<0.001 level.
Fig 2Western blot analysis of islet amyloid polypeptide (IAPP) preparations and cerebrospinal fluid (CSF) and correlations between total IAPP, Q-albumin, CSF albumin and AD biomarkers.
Immunoblotting with T4149, T4157 recognized low molecular weight (A133,) IAPP in wells loaded with monomeric preparations of IAPP (mIAPP), whereas A133 only recognized the LMW after membrane boiling (A). All three antibodies also recognized several bands with various molecular weights (ranging from 10 kDa to over 300kDa) in the pre-aggregated preparation of IAPP (aIAPP) and a 120 kDa in CSF (A). The A133 detected additional bands in CSF both before and after membrane boiling (A). Scatter plots in (B-D) demonstrate correlations between total CSF IAPP and logarithmic transformed values of Q-albumin in NC (B), AD patients (C) and patients with both AD and T2D (D). Scatter plots in (E-G) demonstrate correlations between total CSF IAPP and logarithmic transformed values of CSF albumin in NC (E), AD patients (F) and patients with AD and T2D (G). Data was analyzed with Pearson correlation test. * Significant correlation at p< 0.05. ** Significant correlation at p<0.001. *** Significant correlation at p< 0.0001.
Fig 3Correlations between total plasma IAPP and AD biomarkers.
Scatter plots demonstrate correlation between levels of total plasma IAPP and logarithmic transformed values of CSF t-tau in NCs (A) and a trend towards a correlation in patients with AD+T2D (B). Scatters plots also demonstrate a positive correlation between levels of total plasma IAPP and logarithmic transformed values of CSF p-tau in NCs (C) as well as a negative correlation between levels of total plasma IAPP and logarithmic transformed values of CSF Aβ42 in AD patients (D). Data was analyzed using Pearson correlation test. * Significant correlation at p<0.05.