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Recently, the microbiome-derived trimethylamine-N-oxide (TMAO) was shown to be present in human cerebrospinal fluid (CSF). However, data on the potential of TMAO crossing the blood-CSF barrier are still lacking. This retrospective study aimed at investigating possible associations between the CSF/serum albumin (QALB) and TMAO (QTMAO) quotient and evaluating QTMAO values in individuals with and without blood-CSF barrier dysfunction. A total of 290 patients, who underwent diagnostic lumbar puncture with QALB and QTMAO determination, were evaluated. Serum and CSF TMAO measurements were performed on a tandem mass spectrometry SCIEX QTRAP 4500 (Applied Biosystems, Framingham, MA, USA) coupled with an Agilent 1260 Infinity HPLC system (Agilent Technologies Santa Clara, CA, USA). Serum and CSF albumin were measured on the Atellica® NEPH 630 system (Siemens Healthineers, Erlangen, Germany). CSF TMAO levels were positively correlated with serum TMAO levels (ρ = 0.709, p < 0.001). The QALB was significantly associated with the QTMAO (ß-coefficient = 0.312; p < 0.001). A total of 117 patients with blood-CSF barrier dysfunction had significantly higher median (Q1 - Q3) QTMAO values (4.7 (2.8 - 7.5) vs. 3.8 (2.5 - 5.7) x 10-1, p = 0.002) compared to 173 individuals with normal blood-CSF barrier function. CSF and serum TMAO concentrations were significantly associated in 290 CSF/serum pairs from lumbar punctures of clinical routine. QALB showed a relevant influence on QTMAO. Present results indicate that TMAO may cross the blood-CSF barrier.
The small organic molecule trimethylamine-N-oxide (TMAO) is generated in a gut microbiota-dependent way. The gut microbiome metabolizes L-carnitine and phosphatidylcholine containing nutrients (i.e., eggs, cheese, sea salt fish, red meat) to trimethylamine (TMA), which is absorbed into the bloodstream and oxidized by the hepatic flavin mono-oxygenases (FMOs) (Tang et al., 2013[
Several works suggested that TMAO is closely related to neurological disorders (Zhai et al., 2019[
It is well known that the CSF analysis is an essential diagnostic tool for neurological diseases. However, the role of TMAO in the brain has not been fully explored yet. The blood-CSF barrier, which is formed by apical tight junctions between the choroid plexus epithelial cells, regulates the permeability of agents from the bloodstream to the CSF (Engelhardt and Sorokin, 2009[
The aim of this retrospective study was to evaluate the albumin and TMAO concentrations in 290 consecutive CSF/serum pairs of lumbar punctures. We assessed possible associations between the CSF/serum albumin (QALB) and the CSF/serum TMAO (QTMAO) quotient and investigated the QTMAO in individuals sub-grouped by the presence or absence of blood-CSF barrier dysfunction.
In total, the medical records of 290 consecutive patients, who received diagnostic lumbar puncture with QALB and QTMAO assessment at the Institute of Clinical Chemistry and Laboratory Medicine of the General Hospital Hochsteiermark (Leoben, Austria) in a one year period (2019), were retrospectively examined. Patients < 18 years of age were excluded. Informed consent was obtained from all patients. The ethical approval of this study was provided by the Ethical Committee of the Medical University Graz (Graz, Austria) and carried out with the current version of the declaration of Helsinki.
CSF and venous blood were taken simultaneously and collected in sterile 2 mL VACUETTE® Z No Additive and 5 mL VACUETTE® Z Serum Clot activator tubes (Greiner Bio-one International GmbH, Kremsmünster, Austria). Samples were kept at 4 °C and batch analyzed within one week. The serum (reference range: 3.5 - 5.2 g/dL) and CSF (reference range: ≤ 0.35 g/L) concentrations of albumin were determined by nephelometric method on the Atellica® NEPH 630 system (Siemens Healthineers, Erlangen, Germany). The intra- and inter-day coefficients of variation (CVs) ranged between 2.7 - 3.1 and 1.7 - 3.5 %. The QALB was calculated to assess the blood-CSF barrier function (Sindic et al., 2001[
Serum and CSF TMAO were measured using a stable-isotope-dilution assay and high-performance liquid chromatography (HPLC) with electrospray ionization tandem mass spectrometry on a SCIEX QTRAP 4500 triple quadrupole instrument (Applied Biosystems, Framingham, MA, USA) equipped with an Agilent 1260 Infinity HPLC system (Agilent Technologies Santa Clara, CA, USA). The intra- and inter-day CVs ranged between 2.2 - 5.5 and 7.6 - 9.9 %. The serum TMAO reference range (0.98 - 15.5 µmol/L) was calculated according to the literature (Wang et al., 2014[
The Kolmogorov-Smirnov test was performed to calculate data distribution. As all analyzed continuous variables were not normally distributed, they were expressed as medians (Q1 - Q3). To assess potential correlation between two continuous variables the Spearman's rank correlation coefficient (not normally distributed data) was used. Linear regression models were performed to assess the association between variables. The exact Mann-Whitney U test was used for subgroup comparisons. A p-value < 0.05 was considered statistically significant. For statistical analysis, the Analyse-it® software version 4.92 (Analyse-it Software, Ltd., Leeds, United Kingdom) was used.
The baseline characteristics of the study population are shown in Table 1
The median (Q1 - Q3) QALB was 6.8 (5.0 - 9.9) x 10-3. All in all, 117 and 173 individuals were identified with and without blood-CSF barrier dysfunction. The median TMAO CSF and serum concentrations (Q1 - Q3) were 0.9 (0.5 - 1.4) and 2.1 (1.3 - 3.4) µmol/L.
CSF TMAO levels were positively correlated with serum TMAO levels (ρ = 0.709, p < 0.001). The univariate regression model for CSF TMAO is presented in Figure 1
The univariate regression model between the QTMAO and the QALB is illustrated in Figure 3
In the present study, possible CSF and serum TMAO associations were assessed at the blood-CSF barrier in 290 liquor/serum pairs obtained from clinical routine. It was hypothesized that TMAO could cross the blood-CSF barrier. This aspect has never been demonstrated
In comparison, Del Rio et al. measured for the first-time CSF TMAO in 58 subjects with diagnostic lumbar punctures (Del Rio et al., 2017[
The transport of molecules across the blood-CSF barrier is regulated by passive diffusion (e.g. albumin, immunglobulins) or facilitated by active transporters (e.g. glucose, drugs) (Tumani et al., 2017[
The function and dysfunction of the blood-CSF barrier are best characterized by the QALB (Brettschneider et al., 2005[
Herein, 117 patients with blood-CSF barrier dysfunction were found with significantly higher QTMAO values compared to 173 individuals with normal blood-CSF barrier function (p = 0.002). Many neurological diseases have been shown to be accompanied by an altered blood-CSF barrier permeability (Reiber, 1994[
The major advance of the present study is the high number of diagnostic lumbar punctures obtained from neurological patients. Nevertheless, the major limitation of this retrospective analysis is that it is not possible to draw conclusions about possible links between CSF TMAO concentrations and different neurological conditions. Conducting prospective studies may contribute to this gap of knowledge in the future.
Significant association of CSF and serum TMAO concentrations was observed in 290 diagnostic CSF/serum pairs of clinical routine. QALB showed a relevant influence on QTMAO. Patients with blood-CSF barrier dysfunction had significantly higher CSF TMAO concentrations compared to individuals with normal blood-CSF function.
The authors declare that there is no conflict of interest.