Genetic risk score in multiple sclerosis is associated with unique gut microbiome

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作者
Noha S. Elsayed
Robert K. Valenzuela
Terrie Kitchner
Thao Le
John Mayer
Zheng-Zheng Tang
Vishnu R. Bayanagari
Qiongshi Lu
Paula Aston
Karthik Anantharaman
Sanjay K. Shukla
机构
[1] Marshfield Clinic Research Institute,Center for Precision Medicine Research
[2] Albert Einstein Medical College,Department of Pediatrics
[3] Marshfield Clinic Research Institute,Integrated Research Development Laboratory
[4] Marshfield Clinic Health System,Office of Research Computing and Analytics
[5] Marshfield Clinic Research Institute,Department of Biostatistics and Medical Informatics
[6] Marshfield Clinic Health System,Roger Williams Medical Center
[7] University of Wisconsin,Department of Neurology
[8] Boston University School of Medicine,Department of Bacteriology
[9] Marshfield Clinic Health System,Computational and Informatics in Biology and Medicine Program
[10] University of Wisconsin-Madison,undefined
[11] University of Wisconsin-Madison,undefined
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摘要
Multiple sclerosis (MS) is a complex autoimmune disease in which both the roles of genetic susceptibility and environmental/microbial factors have been investigated. More than 200 genetic susceptibility variants have been identified along with the dysbiosis of gut microbiota, both independently have been shown to be associated with MS. We hypothesize that MS patients harboring genetic susceptibility variants along with gut microbiome dysbiosis are at a greater risk of exhibiting the disease. We investigated the genetic risk score for MS in conjunction with gut microbiota in the same cohort of 117 relapsing remitting MS (RRMS) and 26 healthy controls. DNA samples were genotyped using Illumina’s Infinium Immuno array-24 v2 chip followed by calculating genetic risk score and the microbiota was determined by sequencing the V4 hypervariable region of the 16S rRNA gene. We identified two clusters of MS patients, Cluster A and B, both having a higher genetic risk score than the control group. However, the MS cases in cluster B not only had a higher genetic risk score but also showed a distinct gut microbiome than that of cluster A. Interestingly, cluster A which included both healthy control and MS cases had similar gut microbiome composition. This could be due to (i) the non-active state of the disease in that group of MS patients at the time of fecal sample collection and/or (ii) the restoration of the gut microbiome post disease modifying therapy to treat the MS. Our study showed that there seems to be an association between genetic risk score and gut microbiome dysbiosis in triggering the disease in a small cohort of MS patients. The MS Cluster A who have a higher genetic risk score but microbiome profile similar to that of healthy controls could be due to the remitting phase of the disease or due to the effect of disease modifying therapies.
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