The oral microbiome of early stage Parkinson's disease and its relationship with functional measures of motor and non-motor function.

Dragos Mihaila,Christopher Neville,Qian Du,Richard Uhlig,Jordan Donegan,Danny Zheng,Daria Larocca,Sarah Barns,Frank A Middleton,Michael Vidal,Brenda A Wilson

doi:10.1371/journal.pone.0218252

Abstract

Changes in the function and microbiome of the upper and lower gastrointestinal tract have been documented in Parkinson’s disease (PD), although most studies have examined merely fecal microbiome profiles and patients with advanced disease states. In the present study we sought to identify sensitive and specific biomarkers of changes in the oral microbiome of early stage PD through shotgun metatranscriptomic profiling. We recruited 48 PD subjects and 36 age- and gender-matched healthy controls. Subjects completed detailed assessments of motor, cognitive, balance, autonomic and chemosensory (smell and taste) functions to determine their disease stage. We also obtained a saliva sample for profiling of microbial RNA and host mRNA using next generation sequencing. We found no differences in overall alpha and beta diversity between subject groups. However, changes in specific microbial taxa were observed, including primarily bacteria, but also yeast and phage. Nearly half of our findings were consistent with prior studies in the field obtained through profiling of fecal samples, with others representing highly novel candidates for detection of early stage PD. Testing of the diagnostic utility of the microbiome data revealed potentially robust performance with as few as 11 taxonomic features achieving a cross-validated area under the ROC curve of 0.90 and overall accuracy of 84.5%. Bioinformatic analysis of 167 different metabolic pathways supported shifts in a small set of distinct pathways involved in amino acid and energy metabolism among the organisms comprising the oral microbiome. In parallel with the microbial analysis, we also examined the evidence for changes in human salivary mRNAs in the same subjects. This revealed significant changes in a set of 9 host mRNAs, several of which mapped to various brain functions and showed correlations with some of the significantly changed microbial taxa. Unexpectedly, we also observed robust correlations between many of the microbiota and functional measures, including those reflecting cognition, balance, and disease duration. These results suggest that the oral microbiome may represent a highly-accessible and informative microenvironment that offers new insights in the pathophysiology of early stage PD.

Highlights

The etiology of Parkinson’s Disease (PD) is complex
Among the Parkinson’s disease (PD) subjects, the average duration of a diagnosis was 3.4 years (SE ± 0.56 years), with an average Hoehn & Yahr Stage of 1.92, and average scores for subscales of the MDS-UPDRS, Non-Motor Symptom Questionnaire (NMS), SCOPA-AUT, PDQUALIF, and Beck Depression Inventory (BDI) all falling in established ‘mild’ ranges for those instruments according to published criteria (UPDRS-I 10.0, UPDRS-II 8.6, UPDRS-III 23.9) Most PD subjects (69%) were observed to have resting tremor and 87% were on PD medication (Table 2)
The early stage PD subjects showed significant increases in completion times for the Trailmaking A and B tasks, and corresponding significant decreases in Trailmaking A and B completion scores (Table 3). These deficits were present in the absence of a significant change in Simple Reaction Time Score, a trend for slower reaction times was apparent. Complementing these findings, the Procedural Reaction Time (PRT) Score was significantly decreased in the DANA Brain Vitals set of measures (SRT, Procedural Reaction Time test (PRT), Go/No-Go test (GNG)) (Table 3)

Summary

Introduction

The etiology of Parkinson’s Disease (PD) is complex. According to Braak and colleagues [5, 7] the submandibular salivary gland and lower esophagus appear to have a high frequency of alpha-synuclein associated Lewy Body (LB) pathology, followed by the stomach, small intestine and colon. Submandibular biopsy specimens from living PD subjects have been recently reported to contain LBs [8, 9]. The appearance of LBs in these sites is thought to coincide with symptoms of GI dysfunction before the onset of motor symptoms in a large proportion of PD subjects, a feature that has been seen in mouse and non-human primate models of PD [10]

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