Neuronal loss or dysfunction in patients with early Lyme neuroborreliosis: a proton magnetic resonance spectroscopy study of the brain

According to the current European Federation of Neurological Societies (EFNS) guidelines for establishing a "definite" diagnosis of LNB, three conditions should be fulfilled: neurological symptoms suggestive of LNB without other obvious reasons, which occur in less than 6 months after the initial infection; cerebrospinal fluid (CSF) pleocytosis, and intrathecal synthesis of B. burgdorferi antibodies. If only two criteria are fulfilled, LNB is "possible" [10].

The study consisted of twenty-six patients with "definite" LNB according to the EFNS guidelines, hospitalized in the Department of Infectious Diseases and Neuroinfection of the Medical University of Białystok between July 2015 and December 2017. We did not include patients with "possible" LNB, because the diagnosis of LNB is speculative in this group. We also excluded patients suffering from LNB with any focal lesions in the brain on structural MRI (e.g., with T2-hyperintense foci). All our patients had early LNB (symptoms duration < 6 months). The patients’ age ranged from 19 to 65 years (sixteen males, ten females), with a mean age of 43 ± 14.3 years. The control group consisted of twenty-six healthy subjects (aged between 24 and 62 years, mean age 39.2 ± 10.8 years, eleven males, fifteen females) with no previous history of neurological dysfunction, and medical conditions affecting the brain, and with normal findings on MRI. Healthy volunteers were not taking any medication at the time of testing.

All patients with symptoms suggestive of LNB were tested for IgM and IgG antibodies to B. burgdorferi in serum and CSF by enzyme-linked immunosorbent assay (ELISA). In all patients, positive results obtained by ELISA were verified with confirmatory tests: Western blot/immunoblot (Borrelia IgM and IgG). Immunoblot for intrathecal production of specific antibodies against highly specific B. burgdorferi antigens was carried out for all patients (Virotech, Rüsselsheim, Germany). The simultaneous analysis of antibodies (IgG and IgM) against several B. burgdorferi antigens in serum and CSF was performed. Specific bands were compared and in the case where any band was expressed more in the CSF than in the serum, intrathecal synthesis was confirmed.

MRI and ¹H-MRS examinations were performed in a single session on a 3.0-T System (Biograph mMR, Siemens, Germany) using a 16-channel head matrix coil. The examinations were performed in the Independent Department, Laboratory of Molecular Imaging of the Medical University of Białystok. All patients with LNB underwent a routine brain MRI protocol to rule out any lesion or structural abnormality. The protocol included T1-weighted images (TR = 18 ms, TE = 4.92 ms, FoV = 230 mm, Base Resolution = 256, Slice thickness = 1 mm), T2-weighted images (TR = 3500 ms, TE = 117 ms, FoV = 200 mm, Base Resolution = 512, Slice thickness = 4 mm), fluid-attenuated inversion recovery (FLAIR) (TR = 2500 ms, TE = 94 ms, TI = 2500 ms, FoV = 240 mm, Base Resolution = 256, Slice thickness = 4 mm), diffusion-weighted images (DWI) (TR = 8700 ms, TE = 82, FoV = 240 mm, Base Resolution = 132, Slice thickness = 4 mm, b value 1 = 0 s/mm², b value 2 = 500 s/mm², b value 3 = 1000 s/mm², b value 4 = 1500 s/mm²), and T1-weighted images with contrast medium at the end. ¹H-MRS was obtained before T1-weighted images with contrast medium administration. Healthy volunteers underwent the same brain MRI protocol, but without T1-weighted images with contrast medium administration. The median duration from onset of symptoms until diagnosis and initiation of treatment was 15 days. The patients received antibiotic treatment regimens consisting of ceftriaxone. All patients underwent MRI and ¹H-MRS examinations shortly before or at the beginning of antibiotic therapy. Localized ¹H-MRS examinations were performed with a point-resolved spectroscopy (PRESS) sequence. The spectral acquisition parameters were TE of 135 ms, repetition time (TR) of 2000 ms, averages of 128, and 1200 Hz bandwidth. The scan time was 4 min 24 s. The volume of interest (VOI) was located in four regions of the brain: bilaterally in the anterior and posterior parts of the right and left frontal lobes (VOI size: 15 × 15 × 15 mm). We chose frontal lobes for three main reasons: (1) patients with LNB often suffer from difficulty with concentration, mood swings and inability of spontaneous thinking; the dysfunction of frontal lobes of the brain can lead to such changes (2) apart from that, we placed four voxels (VOI) frontally, because in these areas, T2-hyperintense foci tend to occur more often, than in other parts of the brain in patients with LNB (3) additionally, one positron emission tomography (PET) study reported diffuse hypometabolism that included, e.g., frontal lobes. Importantly, in the aforementioned study, there were no metabolic changes in cerebellum [11]. Another single-photon emission computed tomography (SPECT) study demonstrated decreased perfusion in the frontal lobes in 13 patients with LNB [12]. The positioning of VOI is shown in Fig. 1. The localization of VOI was confirmed by three orthogonal MR images in axial, sagittal, and coronal planes. The voxels were localized manually by a trained and experienced neuroradiology technician under my control using T1-weighted sections: in axial, coronal and sagittal planes, reducing the inclusion of CSF. The first two voxels were located on the opposite sides of the cerebral hemispheres symmetrically in anterior part of the frontal lobes (forward and laterally in relation to the anterior horns of the lateral ventricles), and encompassed mainly the frontal white matter. The second two voxels were placed on the opposite sides of the cerebral hemispheres symmetrically exclusively in centrum semiovale of the frontal lobes (above and laterally in relation to the body of the lateral ventricles). The locations of each voxel were chosen carefully to ensure that each voxel contained mainly white matter and in the same areas. No structural pathologies in the areas of VOI on performed structural MRI were observed. Data were acquired and areas of the three peaks of NAA at 2.02 ppm, Cr at 3.02 ppm, and Cho at 3.22 ppm were measured. The metabolite ratios of NAA/Cr, and Cho/Cr were calculated for each VOI, ¹H-MRS spectra were analyzed using the Linear Combination of Model spectra (LCModel) (version 6.3), using the unsuppressed water signal as a concentration reference [13]. Only metabolites with standard deviations of less than 15% were included in the analysis (Cramer-Rao lower bounds, as determined by LCModel), this being a reliable indicator of good-quality spectra.

The analysis was conducted with Stata 15 software. The significance of metabolite ratio differences between patients with LNB and control group were estimated with the unpaired t test. Since the pool of patients with LNB and control group is limited we bootstrapped the p values for the two tailed t test with 10,000 replicates. A value of p < 0.05 was considered as statistically significant. Differences between patients with LNB and healthy controls were tested separately for each VOI and each metabolite. We confirmed the robustness of the results with the parametric (one-way ANOVA) and nonparametric methods (Kruskal–Wallis test, Dunn’s pairwise comparison test, Wilcoxon rank-sum test).

Patient characteristics are shown in Table 1. Cranial nerve palsy and meningitis were the dominant clinical symptoms of LNB. Three patients demonstrated contrast enhancement of cranial nerves, which corresponded to clinical findings. The remaining patients had normal structural MRI.

MR spectra were successfully acquired in all patients and healthy controls. There was no correlation between NAA/Cr and Cho/Cr ratios and age in patients or controls. Table 2 summarized the mean and standard deviation of the metabolite ratios in the six regions of the brain in twenty-six patients diagnosed with LNB and 26 healthy control subjects. NAA/Cr ratio was significantly lower in the anterior part of the right and left frontal lobes (p ≤ 0.001 and p = 0.001 respectively), and in the posterior part of the right and left frontal lobes (p ≤ 0.001 and 0.031 respectively). There was no statistically significant change of Cho/Cr ratio within all regions. We found differences between the MR spectra obtained in patients diagnosed with early LNB and normal conventional MRI of the healthy control subjects. Representative examples of normal and abnormal spectra are shown in Fig. 2. There is a relative reduction of the NAA peak when compared with the Cr peak.