Neuroprotective Effects of Sodium Butyrate by Restoring Gut Microbiota and Inhibiting TLR4 Signaling in Mice with MPTP-Induced Parkinson’s Disease

Male C57BL/6 mice that were 7 weeks old were obtained from Changzhou Cavens Experimental Animal Co., Ltd. (Jiangsu, China) and housed for 7 days to acclimate to the standard habitat before being used in the experiment. Mice were kept in standard settings, including a 12 h dark/light cycle, 55 ± 10% humidity, and 25 ± 1 °C temperatures. Food and water were available to the mice without restriction. The Chongqing Medical University Ethics Committee granted its approval for all of the animal experiments.

Mice were randomly classified (n = 12 per group) into the three following groups: control; MPTP; and MPTP + NaB groups. To create the MPTP mouse model, we applied a technique that was previously reported [25,26]. Specifically, 30 mg/kg MPTP (Sigma Co., Ltd., St. Louis, MO, USA) was administered intraperitoneally to mice in the MPTP and MPTP + NaB groups for 7 consecutive days. In the mice belonging to the control group, an injection of an equivalent volume of normal saline solution was administered. NaB (Sigma Co., Ltd., USA) or saline solution was intragastrically administered, lasting for 14 days after 2 h of MPTP injection for 21 days. The experimental timeline is displayed in Figure 1A.

A total of 7 mice in each group were randomly selected to collect feces. Each mouse was placed individually in an autoclaved cage in the morning following the last treatment. Fecal samples from mice were collected in sterile EP tubes on ice and stored at −80 °C.

All mice were anaesthetized with isoflurane. Whole blood was drawn from the heart. Following incubation at ambient temperature for 0.5 h, whole blood was centrifuged at 3000× g for 15 min at 4 °C. The collected supernatant was stored at −80 °C until subsequent use. A total of 7 mice in each group were randomly selected and in order to collect their fresh striatal and colonic tissues, they were perfused with sterile PBS. The tissue was collected on ice and stored at −80 °C for the determination of neurotransmitters and proteins.

The remaining 5 mice were used for staining experiments after whole brain tissue and colon tissue were collected. After perfusion with PBS and 4% paraformaldehyde (PFA), the colonic tissue was placed in 4% PFA for preservation. Whole brain tissue was fixed overnight in 4% PFA, followed by 24 h incubation in 20% sucrose solution and another 24 h incubation in 30% sucrose solution before embedding in OCT compound (SAURA, Shiogama, Japan). Whole brain tissue was stored at −80 °C for backup.

The levels of striatal DA and serotonin (5-HT), as well as their corresponding metabolites, dihydroxyphenylacetic acid (DOPAC) and 5-hydroxyindoleacetic acid (5-HIAA), respectively, were measured using HPLC on a fluorescence detector (LC-20A, SHIMADZU, Kyoto, Japan). The Wonda Sil C18 Superb chromatographic column (4.6 mm × 150 mm, 5 μm, SHIMADZU, Japan) was used. In addition, methanol–citrate buffer (adjust pH to 5 with hydrochloric acid) served as the mobile phase. After the homogenization of the striatum in 0.1 m perchloric acid (1 mg, 10 μL), it was centrifugated at a rate of 12,000× g for 10 mins at 4 °C. Next, after collecting the supernatant, a filter with a pore size of 0.22 μm was employed for filtration, and then 10 μL of each sample was utilized for the detection procedure. The standard samples were dissolved in methanol. Standard curves were plotted using measurements from a range of dilutions of the mixed standard samples.

A cryostat microtome was used to slice the brain tissues of mice into 5 μm-thick sections (CM1950, Leica, Wetzlar, Germany). Sections containing the nigrostriatal fraction were collected. A total of 10 representative sections containing the major part of the substantia nigra from bregma 2.92 mm to 3.52 mm were selected for TH staining from the sections collected for each mouse. Briefly, following the repair of the slides with sodium citrate buffer (pH value, 6.0), brain slices were subjected to incubation in PBS with 0.2% v/v TritonX 100 for 10 min, followed by incubation in 5% v/v goat serum at 37 °C for 1 h. The samples were subjected to overnight incubation with the rabbit anti-TH (1:200, EP1532Y, Abcam, Cambridge, UK) primary antibody at 4 °C. After rewarming for 0.5 h, the primary antibody was detected with appropriate goat anti-rabbit antibody (1:500, A-11008, Thermo Fisher, Waltham, MA, USA) labeled with FITC. Nuclei were detected with DAPI solution (Solarbio, Beijing, China). The representative images were recorded with the aid of a fluorescence microscope (DFC7000T, Leica, Germany). Each group contained 5 animals. The TH-positive cells in substantia nigra from each group were counted with the ImageJ (NIH, Bethesda, MD, USA, version 1.53) software.

The microbiota DNA was extracted using the TianGen TIANamp Bacteria DNA Kit. Barcoded primer sequences, 806R: GGACTACNNGGGTATCTAAT and 341F: CCTAYGGGRBGCASCAG, were utilized for the amplification of the V3-V4 hypervariable region of 16S rRNA, and the PCR-amplified products were purified following electrophoresis using 2% agarose gel. A library was constructed with The TruSeqDNA PCR-Free Sample Preparation Kit, after which it was quantitated using qPCR and Qubit. This was followed by library sequencing on the NovaSeq6000 (Illumina, San Diego, CA, USA) platform. The off-machine data were filtered; chimerism was eliminated, and other steps were undertaken to obtain effective tags. Based on the Uparse algorithm, effective tags were clustered into OTUs with an overall similarity of 97%. The SSUrRNA database of SILVA138 and the Mothur method were used for species annotation. The α-diversity and β-diversity indexes were computed utilizing QIIME (version 1.9.1), and the Wilcoxon test was conducted using R (version 2.15.3). An analytical tool, linear discriminant analysis (LDA) effect size (LEfSe), was utilized for identifying and interpreting high-dimensional biomarkers for detecting bacterial differences. For< 0.05, the value of LDA > 4 indicated a significant enrichment. ® p

The colon of each mouse was paraffin-embedded and sliced into 5 μm-thick sections, which were subjected to the HE staining protocol and scored pathologically according to previously described criteria [27]. The degree of inflammation was defined as follows: 3, severe; 2, moderate; 1, mild; and 0, no inflammation. The extent of damage was defined as follows: 0, no damage; 1, damage to the mucosal layer; 2, damage to the submucosal layer; and 3, damage to the whole layer. Crypt disruption was scored as follows: 0, no disruption; 1, disruption to 1/3 of basal layer; 2, disruption to 2/3 of basal layer with an intact surface epithelium only; and 3, all epithelial basal layers were disrupted. Each of the above scores was multiplied by the proportion of colon involved (0–25% times 1, 26–50% times 2, 51–75% times 3, and 76–100% times 4) and finally, each score was summed to obtain the final pathology score.

The Interleukin-6 (IL-6) and tumor necrosis factor-α (TNF-α) levels in the sera of mice were measured with the aid of the corresponding kits (Solarbio Technology Co., Ltd., Beijing, China) following kit protocols. A standard protein curve was used to determine the target protein concentration. IL-6 and TNF-α concentrations were expressed in pg/L protein.

To extract protein from the striatum and colon, we added the RIPA lysis buffer with 1% phenylmethylsulphonyl fluoride (Beyotime, Shanghai, China) to the ground tissue. Subsequently, we homogenized the samples and centrifugated them at a rate of 12,000× g for 15 min at 4 °C. Thereafter, the BCA Protein Assay Kit (Beyotime, Shanghai, China) was employed to measure the supernatant’s protein concentration after centrifugation. SDS-PAGE (sodium dodecyl sulfate-polyacrylamide gel electrophoresis) was employed to extract the denatured protein sample before it was transferred onto a polyvinylidene fluoride (PVDF) membrane (Millipore, Burlington, MA, USA). Next, the membranes were blocked following protein transfer with 5% skim milk before being treated for an entire night with the specific primary antibodies at 4 °C. Specifically, the primary antibodies below were utilized in the experiments: rabbit anti-TH antibody (1:1000, 25859-1-AP, Proteintech, Rosemont, IL, USA), rabbit anti-GFAP antibody (1:1000, K106966P, Solarbio), rabbit anti-Iba-1 antibody (1:1000, 10904-1-AP, Proteintech), rabbit anti-occludin antibody (1:1000, 27260-1-AP, Proteintech), rabbit anti-ZO-1 (1:1000, 21773-1-AP, Proteintech), rabbit anti-TLR4 antibody (1:1000, 19811-1-AP, Proteintech), rabbit anti-MyD88 antibody (1:1000, ab40676, Abcam), rabbit anti-IL-6 antibody (1:1000, K009385P, Solarbio), rabbit anti-TNF-α antibody (1:1000, 17590-1-AP, Proteintech), rabbit anti-NF-κB antibody (1:1000, #8242, Cell Signaling Technology, Danvers, MA, USA), rabbit anti-β-actin antibody (1:1000, 20536-1-AP, Proteintech), and rabbit anti-GAPDH antibody (1:1000, 10494-1-AP, Proteintech). The primary antibody was recognized using an HRP-conjugated anti-rabbit antibody (1:5000, BA1054, Boster, San Mateo, CA, USA). The chemiluminescence solution (Millipore, Billerica, MA, USA) was dripped on the PVDF membrane and exposed to an automatic gel imaging analyzer (Bio-Rad, Hercules, CA, USA). Lastly, ImageJ was applied to measure the protein band density.

The GraphPad software (version 8.0.2), was employed for the analyses of statistical data. A one-way analysis of variance (ANOVA) followed by Tukey’s post-hoc test was conducted for detecting differences. The Kruskal–Wallis test, followed by Dunn’s multiple comparison test (α < 0.05) or the Wilcoxon rank sum test, was conducted to make a comparison among three groups of specific taxa of microbiota. All data were presented as mean ± standard error of the mean (SEM). A value of p < 0.05 indicated the significance criterion.

We tested the effects of NaB on the motor function in mice with PD using poles and rotarods. In comparison to the control mice, the MPTP-induced mice exhibited severe locomotor impairment, as shown by a considerably longer pole test time and a considerably shorter rotarod test time (p < 0.001). In contrast, the MPTP + NaB mice exhibited significantly better performance in the pole test (p < 0.001) and rotarod test (p < 0.001) relative to the MPTP mice (Figure 1B,C). Subsequently, we assessed the effect of NaB on locomotor abilities and exploratory behaviors based on the OFT by measuring the paths traversed by the mice (Figure 1D). A lesser total distance (p < 0.001), a smaller central distance (p < 0.001), and fewer crossings in the central zone (p < 0.001) were found in MPTP mice relative to the control mice. The performance in terms of the total distance (p < 0.001), central distance (p < 0.001), and the total number of crossings in the central zone (Figure 1E–G) (p < 0.001) was better for the MPTP + NaB mice relative to the MPTP mice. These results demonstrated that NaB could improve locomotor functions and exploratory behaviors in the PD mice.

To ascertain whether or not NaB had a neuroprotective function, we used fluorescence detection after HPLC to measure the levels of striatal neurotransmitters, as well as their metabolites. A 31.5% decrease in DA levels in the striatum of MPTP mice (p < 0.01) was observed. In contrast, DA levels in the striatum increased remarkably by 49.2% in the MPTP + NaB mice (p < 0.01) relative to the MPTP mice (Figure 2A). Additionally, 5-HT levels decreased by 34.6% in the MPTP mice (p < 0.01), whereas these increased by 49.2% in the MPTP + NaB mice (p < 0.01) (Figure 2B). The MPTP mice tended to have lower DOPAC and 5-HIAA levels than the normal mice but these differences were statistically insignificant. The striatal levels of DOPAC and 5-HIAA were elevated remarkably in the MPTP + NaB group by 38.7% and 32.0%, respectively, compared to the MPTP group (p < 0.05 for both) (Figure 2C,D).

We conducted an IF analysis on the PD mice to determine if NaB protected the TH+ dopaminergic neurons. Striatal TH protein expression was examined using Western blotting. As shown using IF analysis, a remarkable decrease in TH+ dopaminergic neurons of 51.2% was seen in the PD mice (p < 0.01) compared to the control mice but NaB exposure inhibited the decline by 83.0% compared to the MPTP group (p < 0.05) (Figure 3A,B). Consistently, the Western blotting demonstrated that the TH levels in the MPTP mice decreased remarkably by 47.5% (p < 0.01) compared to the control mice, while the NaB treatment increased the TH expression significantly (p < 0.01) by 93.0% compared to MPTP alone (Figure 3C,D). The above results suggested that NaB performed a neuroprotective function in the PD mice by increasing striatal TH expression and restoring dopaminergic neuron loss.

Neuroinflammation in neurodegenerative diseases, including PD, may be associated with astrocyte and microglial activation [28]. To assess whether microglia and astrocytes were activated, Western blotting was conducted for the detection of protein markers, Iba-1 and GFAP, in microglia and astrocytes, respectively. Additionally, in the striatum of the PD mice, Iba-1 levels were substantially higher by 102.2% (p < 0.001), while the NaB treatment in the mice with MPTP-induced PD decreased its expression by 45.4% compared to the MPTP-treated mice (p < 0.001) (Figure 4A). As well, the MPTP mice displayed a 53.6% decrease in GFAP expression compared to the control mice in the striatum (p < 0.001). The treatment with NaB decreased GFAP expression (p < 0.01) by 26.2% in the MPTP mice (Figure 4B,C). Thus, the NaB treatment inhibited glial cell activation, leading to reduced neuroinflammation.

To assess the ameliorative impact of NaB exposure on gut microbiome dysbiosis in PD mice, a 16S rRNA seq-analysis of fecal gut microbiota was conducted in each mouse group. First, an α-diversity analysis was performed to assess bacterial diversity and richness. The MPTP group exhibited significantly higher Shannon and Simpson indexes relative to the controls. The NaB mice showed a downward trend relative to the MPTP group but this was statistically insignificant (Figure 5A,B). Furthermore, β-diversity was assessed based on weighted UniFrac distances and Bray–Curtis distances to determine the similarity in microbiota composition across these three groups (Figure 5C,D). A significant difference in the gut microbiota was observed, indicating substantial variations in the overall structure of the gut microbiota across the control, MPTP, and MPTP + NaB mice. Moreover, the results demonstrated that the control and MPTP mice were separated, with the NaB treatment group located in between the two groups, suggesting that the NaB treatment shifted the overall MPTP-damaged gut microbiota composition towards that of the control group. To further clarify the key bacteria causing the occurrence of PD, the relative abundances of different taxa of microorganisms were compared (Figure 5E,F). A dramatic change in microbiota composition was observed. In terms of the phylum level, Verrucomicrobiota and Proteobacteria were elevated in the PD mice (p < 0.001, p < 0.05, respectively) but the NaB treatment significantly decreased their abundances (p > 0.05, p > 0.05, respectively). In terms of the family level, the MPTP mice recorded an increased abundance of Bacteroidaceae (p < 0.001), along with a reduction in Erysipelotrichaceae abundance (p < 0.05). However, the abundance of Bacteroidaceae was lowered in the NaB group (p < 0.05), whereas that of Erysipelotrichaceae was elevated considerably (p > 0.05). In terms of the bacterial genera, the MPTP mice had higher relative abundances of Bacteroides, Parabacteroides, Akkermansia, and Lactobacillus (p < 0.01, p < 0.01, p < 0.01, p < 0.05, respectively), while those of Dubosiella and Odoribacter in the MPTP group were lowered (p < 0.05, p < 0.01, respectively). However, the relative abundance of Parabacteroides, Bacteroides, Akkermansia, and Lactobacillus decreased after NaB administration (p > 0.05, p < 0.05, p > 0.05, p < 0.05, correspondingly), whereas that of Dubosiella and Odoribacter was elevated substantially (p > 0.05, p < 0.05, respectively) (Figure 5G). To assess the specific bacterial taxa associated with PD, we determined the mice gut microbiota composition across the three groups using LEfSe based on relative abundances, along with the significant changes (Figure 5H,I). The data suggested that the MPTP-induced mice had gut microbial dysbiosis, and that the NaB treatment improved gut dysbiosis in these animals by modulating microbiota composition.

To verify the impact of NaB on colonic pathology, HE staining on mouse colonic sections was performed to observe inflammation. The MPTP group showed more severe colonic inflammation relative to the control group. The NaB group exhibited lower colonic inflammation than the MPTP group (Figure 6A). Moreover, the MPTP mice showed significantly higher HE histological scores (p < 0.01), whereas the NaB-treated mice showed significantly lower scores (p < 0.05) (Figure 6B). Western blotting was conducted to measure the expression profiles of ZO-1 and occludin to assess the influence of NaB administration on the colonic barrier (Figure 6C). The expression levels of ZO-1 and occludin were reduced remarkably by 32.1% and 55.8%, respectively, in the colon of the MPTP mice (p < 0.05 and p < 0.01, respectively), whereas in the MPTP + NaB mice, the occludin and ZO-1 levels increased by 100.5% and 49.2% (p < 0.01 and p < 0.05, respectively) (Figure 6D,E). Taken together, NaB could restore colonic barrier damage in the MPTP mice.

The gut microbiota in the PD mice was found to contain an abundance of pro-inflammatory bacteria based on the 16S rRNA sequencing analysis. The intestinal permeability in the PD mice was also increased. Therefore, we first detected inflammatory factor levels in the colon, serum, and striatum of the mice, followed by the TLR4/MyD88/NF-κB pathway expression in the colon and striatum. The ELISA findings illustrated that the IL-6 and TNF-α levels in the serum were higher by 193.6% and 150.5%, respectively, in MPTP mice (p < 0.001 for both), whereas these levels decreased correspondingly by 64.2% and 50.0% in the MPTP + NaB mice (p < 0.001 for both) (Figure 7A,B). The Western blotting illustrated a substantial decline in the levels of TNF-α and IL-6 of 78.7% and 55.1%, respectively, in the striatum of the MPTP mice (p < 0.01, p < 0.05), while the NaB treatment considerably lowered the corresponding expression levels by 41.0% and 37.9% (p < 0.01, p < 0.05, respectively) (Figure 7C–E). The colonic TNF-α and IL-6 levels increased remarkably by 88.2% and 83.6% in the MPTP mice (p < 0.001, p < 0.05, respectively), whereas these levels correspondingly decreased by 45.0% and 42.0% in the MPTP + NaB mice (p < 0.001, p < 0.05, respectively) (Figure 7F–H).

The Western blot results for the signaling pathway proteins indicated that the TLR4, MyD88, and NF-κB levels increased significantly in the striatum by 78.4%, 75.8%, and 91.6%, respectively, in the PD mice (p < 0.05, p < 0.001, p < 0.01, respectively), whereas these levels declined significantly by 45.4%, 44.1%, and 45.9% in the MPTP + NaB mice (p < 0.05, p < 0.001, p < 0.01, respectively) (Figure 7I–L). Similarly, TLR4, MyD88, and NF-B protein expression decreased nearly 70%, 94.7%, and 94.2% in the colons of the PD group mice, respectively (p < 0.01, p < 0.05, p < 0.05, respectively). In contrast, NaB exposure substantially decreased these protein expression levels by 41.2%, 67.0%, and 48.0% (p < 0.01, p < 0.01, p < 0.05, respectively) (Figure 7M–P). Thus, NaB reduced intestinal inflammation and neuroinflammation by suppressing the activities of the TLR4/MyD88/NF-κB signaling pathway.