Impaired renal function and dysbiosis of gut microbiota contribute to increased trimethylamine-N-oxide in chronic kidney disease patients

In conclusion, compared to the healthy controls, CKD patients showed worse clinical manifestations and significantly elevated TMAO concentrations. The low GFR group showed significantly higher TMAO concentrations than the high GFR group, which showed significantly higher TMAO concentrations than the control group.

The α–diversity indices are commonly used to describe the ecological diversity within microbial community samples. The phylogenetic diversity whole tree index (PD-whole tree) represents the phylogenetic diversity of the whole microbial community, whereas the Shannon index considers both the species richness and evenness. According to the Wilcoxon rank sum test analysis, both of these indices were significantly lower in the CKD group (P < 0.001) (Fig. 2c,d).

In conclusion, next-generation sequence profiling of the gut microbiota revealed obvious dysbiosis of the gut microbiota in CKD patients, including reduced bacterial α–diversity and biased community constitutions.

To identify taxonomic differences between the CKD patients and healthy controls, we used the LEfSe tool with a relatively stringent LDA value of 3 (Fig. 3b). At the phylum level, the CKD patients showed increased Proteobacteria but reduced Firmicutes and Actinobacteria. At the family level, the CKD patients showed increased Enterobacteriaceae and Corynebacteriaceae but reduced Ruminococcaceae. At the genus level, Enterococcus and Clostridium were enriched in the CKD patients, whereas Prevotella, Coprococcus, Megamonas, Sutterella, Enterobacter, Acidaminococcus, Dorea, and Roseburia were more abundant in the healthy individuals.

To deduce whether these microbial community differences were related to TMAO production, we performed a PICRUSt analysis to infer the functional profiles of the microbiome communities²⁰. We found 6910 genes in total, among which 30 genes correlated with choline, betaine, carnitine and trimethylamine metabolism. Within these genes, 8 genes differed significantly between the CKD patients and the healthy controls (Mann-Whitney U test, P < 0.05) (Fig. 3c). Genes related to choline, betaine and L-carnitine metabolism were significantly depleted in the CKD patients, including K07271 (functional annotation: LPS phosphatidyl-choline acyltransferase), K01004↗ (functional annotation: phosphatidylcholine synthase), K00499↗ (functional annotation: choline monooxygenase), K00130↗ (functional annotation: betaine aldehyde dehydrogenase), and K00540↗ (functional annotation: Cnt B). The significantly increased genes in the CKD patients were related to TMA production in the intestinal tract, including K07811 (functional annotation: trimethylamine oxidoreductase (cytochrome c) 1), K07821 (functional annotation: trimethylamine oxidoreductase (cytochrome c) 2, c-type cytochrome subtribe activity regulation transducer), and K03532↗ (functional annotation: trimethylamine oxidoreductase (cytochrome c) 1, c-type cytochrome subtribe activity regulation transducer).

In summary, CKD patients showed different dominant bacteria and altered genes expression, which involved in choline, betaine, L-carnitine and trimethylamine (TMA) metabolism, compared to the control group.

Due to the different TMAO levels between the GFR groups, we attempted to evaluate differences in their bacterial communities. No obvious difference was observed in the PCoA (ADONIS analysis, P = 0.601, R² = 0.033) (Fig. 3d). By analyzing the raw microbiome data of CKD patients (Fig. S1), we further found that the low GFR group harbored reduced Streptococcus, Streptococcaceae, and Lactobacillales, compared to the high GFR group (Fig. 3e). Furthermore, the low GFR group showed increased Adlercreutzia, which was positively correlated to the TMAO level (Spearman analysis, P = 0.002, R = 0.528), but the abundance of Adlercreutzia was relatively low (<0.00005). These results indicated that the difference of microbial composition between the low GFR group and the high GFR group was not significant.

We recruited chronic kidney disease patients in this study. All patients were consecutively recruited from the Department of Nephrology of Nanfang Hospital (a teaching hospital affiliated with Southern Medical University in southern China) during 2014. The following inclusion criteria were used: proven impaired kidney structure or renal function and a measured GFR < 60 mL/min/1.73 m² for a minimum of 3 months. Patients with acute intercurrent illnesses and infections and those who used probiotics or antibiotics within 1 month before admission were excluded. The patient group (n = 32) consisted of thirty-two stable patients (16 men and 16 women, aged 53.34 ± 14.47 years) with abnormal renal functions for a minimum of 3 months. The underlying causes of CKD in this study population included nephrosclerosis in 10 patients, diabetic nephropathy in 5 patients, glomerulonephritis in 4 patients and polycystic kidney disease in 1 patient. The controls (n = 32, 16 men and 16 women, aged 55.03 ± 10.38 years) consisted of age- and gender- matched individuals from the health examination centre of Nanfang Hospital. The only exclusion criterion for the selection of the healthy controls was abnormal renal functions.

In our study, the CKD group were mainly constitutive of CKD4 and CKD5 patients. According to the new KDIGO (Kidney Disease: Improving Global Outcomes) classification, CKD stages are determined at referral and correspond to stages 4 (GFR, 15- < 30 mL/min/1.73 m²), and 5 (GFR < 15 mL/min/1.73 m²)⁴².

In this study, the GFR of each healthy participant was beyond 90 ml/min/1.73 m². According to the Initiating Dialysis Early and Late (IDEAL) study⁴³, we further divided the CKD patients into 2 subgroups. The high GFR group was determined as those patients whose GFR was higher than or equal to 7 ml/min/1.73 m² and the low GFR group was determined lower than 7 ml/min/1.73 m². Specifically, the low GFR group contained 16 CKD5 patients, and the high GFR group contained 15 CKD5 patients and 1 CKD4 patient.

For all participants, we collected fasting EDTA-plasma samples, fresh faecal samples and associated clinical data. Plasma aliquots were collected before dialysis treatment, centrifuged, and then immediately frozen at −40 °C. The faecal sample aliquots were frozen at −40 °C immediately after collection. The Ethics Committee of Southern Medical University approved the study protocol, and informed written consent was obtained from all participants. We confirmed that all methods were performed in accordance with the relevant guidelines and regulations.

DNA was extracted from the microbial flora contained in the stool samples using the PowerSoil DNA Extraction Kit (Shenzhen Bioeasy Biotechnologies. Co., Ltd) following the manufacturer’s specifications⁴⁴.

All 64 individually processed human faecal gDNA extractions were PCR amplified. The V4F (GTGTGCCAGCMGCCGCGGTAA) and V4R (CCGGACTACHVGGGTWTCTAAT) primers were used to amplify the 16S rRNA gene V4 variable region from the bacteria. The polymerase chain reaction cycle conditions were described previously⁴⁵. Amplifications were performed using a step cycling protocol consisting of 94 °C for 2 minutes, 30 cycles of 94 °C for 30 seconds, 54 °C for 30 seconds, and 72 °C for 45 seconds. A condition of 72 °C for 5 minutes was used for the final elongation. Each 25-μL PCR reaction contained 0.5 μL of template DNA, 2.0 μL of dNTP Mix (2.5 mmol/L; TaKaRa), 2.5 μL of TaKaRa 10× Ex Taq buffer (Mg2+ free), 1.5 μL of Mg²⁺ (25 mmol/L), 0.25 μL of TaKaRa Ex Taq DNA polymerase (2.5 units), 0.5 μL of 10 μmol/L bar code primer 514 F, 0.5 μL of 10 μmol/L primer 805R, and 17.25 μL of double-distilled water.

According to the manufacturer’s protocol, all polymerase chain reaction amplicons were mixed together and sent to the Beijing Genomic Institute for sequencing using Illumina Miseq (PE 150). The raw sequences were preprocessed based on the BIPES protocol⁴⁵. The sequences were analysed using QIIME version 1.8.0⁴⁶. All samples were normalized for the subsequent analysis. The sequences were stored in the Sequence Read Archive database under accession numbers ERS725509 to ERS725741.

Sequences with a distance-based similarity of 97% or greater were grouped into operational taxonomic units (OTUs) using the Usearch algorithm⁴⁷. According to the sequence frequency, we determined the representative sequences for each OTU, which were aligned using the PyNAST algorithms⁴⁸. The phylogenetic relationships were determined based on a representative sequence alignment using Fast-Tree⁴⁹. The taxonomic assignments for each representative sequence were measured, and the above information was combined to construct a BIOM file⁵⁰ using the command pick_de_novo_otus.py –i clean.fasta –o output_dir. We performed principal coordinate analysis (PCoA) using the command beta_diversity_through_plots.py –i otu.biom –o output_dir.

To determine the significantly differential taxa between the CKD patients and the healthy individuals, we applied linear discriminant analysis effect size (LEfSe) to compare samples between these 2 groups⁵¹. The threshold of the linear discriminant was set to 3. LEfSe is an algorithm for high-dimensional biomarker discovery that also identifies genomic features that characterise differences between two or more biological conditions. LEfSe allows researchers to identify differentially abundant features that are also in accord with biologically meaningful categories by emphasizing statistical significance, biological consistency and effect relevance. For each of the differential features detected by LEfSe, we calculated a linear discriminant analysis value, which represented the differences of the feature between the tested groups.

Plasma aliquots were stored at −40 °C prior to analysis. The plasma TMAO concentrations were quantified using stable isotope dilution liquid chromatography tandem mass spectrometry (6460 Series Triple Quadrupole LC/MS; Agilent) as previously described⁵².

The molecular weight of TMAO is 75.22 g/mol. The extracted plasma aliquots were spiked with internal standards comprised of d9-TMAO in methanol. The samples were mechanically vortexed for 1 minute and centrifuged at 15,000 × g for 25 minutes at 4 °C. The analytes were separated on a phenomenex Luna Silica column (4.6 mm × 250 mm, 5 μm particle size) at room temperature. The mobile phase consisted of 80% solvent A (0.1% formic acid in water) and 20% solvent B (methanol) at a flow rate of 0.5 mL/min. The MS/MS analyses for TMAO and d9-TMAO were conducted in the positive multiple reaction monitoring mass spectrometry mode at m/z 76 → 58 and m/z 85 → 66, respectively. To calculate the TMAO concentration, various concentrations of a TMAO standard were added to control plasma to prepare calibration curves. The data were collected and analysed using the chemistry station provided by Agilent Technology.

The animal experiment protocols were reviewed and approved by the Ethical Committee of Southern Medical University (SMU, Guangzhou, China). All procedures were performed in accordance with the relevant guidelines and regulations. Male C57BL/6 mice were maintained at the Experimental Animal Research Centre at Southern Medical University. The mice were given the same autoclaved standard chow and autoclaved water ad libitum. The animal room was controlled at 23 °C and 40% humidity with a 12-h light/12-h dark cycle. The general health status of the mice, including their physical appearance, was checked every day. All mice in this study had comparable normal health statuses before the experiment.

At the start of the experiment, all mice were 4 weeks old. All 25 mice were treated with a mixture of broad spectrum, poorly absorbed antibiotics, including vancomycin (100 mg/Kg), neomycin sulfate (200 mg/Kg), metronidazole (200 mg/Kg), and ampicillin (200 mg/Kg) for 1 week, in accordance with a previous study⁵³. After this procedure, the mice were randomized into two groups with 12 and 13 mice in each group, respectively. Both groups were treated with faecal microbiota transplantation (FMT) and transplanted with the faeces of the CKD patients or the healthy controls. These two groups of mice were separately bred in different isolators to prevent normalization of the gut microbiota.

Faecal samples from randomly chosen CKD patients (n = 5, male) and healthy controls (n = 5, male) were used. Each faecal sample (0.1 g) was suspended in 1.5 mL of reduced sterile phosphate-buffered saline, and pools were made from equal volumes of the donor suspensions. Adult (5 weeks old) male antibiotic-treated C57BL/6 mice were administered pooled samples derived from either the CKD patients or the healthy controls for 1 week. After centrifugation of the suspensions at 2000 rpm for 10 minutes, the supernatants were collected, and 200 μL was administered to each mouse by gastric gavage.

On day 3 post-FMT, plasma samples were obtained from the mice and immediately stored at −40 °C. These samples were analysed by stable isotope dilution liquid chromatography tandem mass spectrometry to determine the TMAO levels in the mice. The cecum contents were collected when the mice were sacrificed and immediately stored at −40 °C.

Here, we used PICRUSt (Phylogenetic Investigation of Communities by Reconstruction of Unobserved States) to gain insights into the possible functional pathways that differed between groups⁵⁴. PICRUSt uses evolutionary modelling to predict metagenomes from 16S rDNA-derived bacterial data and a reference genome database.

Statistical analysis of the clinical data was implemented using SPSS 20.0. We used the mean (standard deviation) to express measurement data that obeyed a normal distribution, the median (interquartile range) to express measurement data that obeyed a skewed distribution, and a percentage to express enumeration data. The Normality test was used to determine the distribution of the data, and the Mann-Whitney U test was used to determine significance between different groups. The Wilcoxon rank sum test was used to determine significance in α-diversity. The results of Mann-Whitney U test was two-tailed. P < 0.05 was considered significant in the compared groups.

Supplementary Information