Comparison of T-cell Receptor Diversity of people with Myalgic Encephalomyelitis versus controls

Joshua Dibble; Ben Ferneyhough; Matthew Roddis; Sam  millington; Michael D Fischer; Nick J Parkinson; Chris P Ponting

Comparison of T-cell Receptor Diversity of people with Myalgic Encephalomyelitis versus controls

Joshua Dibble, Ben Ferneyhough, Matthew Roddis, Sam millington, Michael D Fischer^*, Nick J Parkinson^*, Chris P Ponting^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

Abstract

Objective: Myalgic Encephalomyelitis (ME; sometimes referred to as Chronic Fatigue Syndrome) is a chronic disease without laboratory test, detailed aetiological understanding or effective therapy. Its symptoms are diverse, but it is distinguished from other fatiguing illnesses by the experience of post-exertional malaise, the worsening of symptoms even after minor physical or mental exertion. Its frequent onset after infection suggests autoimmune involvement or that it arises from abnormal T-cell activation.

Results: To test this hypothesis, we sequenced the genomic loci of and T-cell receptors (TCR) from 40 human blood samples from each of four groups: severely affected people with ME; mildly or moderately affected people with ME; people diagnosed with Multiple Sclerosis, as disease controls; and, healthy controls. Seeking to automatically classify these individuals’ samples by their TCR repertoires, we applied P-SVM, a machine learning method. However, despite working well on a simulated data set, this approach did not allow statistically significant partitioning of samples into the four subgroups. Our findings do not support the hypothesis that blood samples from people with ME frequently contain altered T-cell receptor diversity.

Original language	English
Journal	BMC Research Notes
Publication status	Published - 4 Jan 2024

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s13104-023-06616-4Final published version, 1.79 MBLicence: Creative Commons: Attribution (CC-BY)
2023-11-03 MECFS TCR repertoires Dibble et al FINAL2

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@article{83092905d80048358d8424038ab609b6,

title = "Comparison of T-cell Receptor Diversity of people with Myalgic Encephalomyelitis versus controls",

abstract = "Objective: Myalgic Encephalomyelitis (ME; sometimes referred to as Chronic Fatigue Syndrome) is a chronic disease without laboratory test, detailed aetiological understanding or effective therapy. Its symptoms are diverse, but it is distinguished from other fatiguing illnesses by the experience of post-exertional malaise, the worsening of symptoms even after minor physical or mental exertion. Its frequent onset after infection suggests autoimmune involvement or that it arises from abnormal T-cell activation. Results: To test this hypothesis, we sequenced the genomic loci of and T-cell receptors (TCR) from 40 human blood samples from each of four groups: severely affected people with ME; mildly or moderately affected people with ME; people diagnosed with Multiple Sclerosis, as disease controls; and, healthy controls. Seeking to automatically classify these individuals{\textquoteright} samples by their TCR repertoires, we applied P-SVM, a machine learning method. However, despite working well on a simulated data set, this approach did not allow statistically significant partitioning of samples into the four subgroups. Our findings do not support the hypothesis that blood samples from people with ME frequently contain altered T-cell receptor diversity. ",

author = "Joshua Dibble and Ben Ferneyhough and Matthew Roddis and Sam millington and Fischer, \{Michael D\} and Parkinson, \{Nick J\} and Ponting, \{Chris P\}",

note = "Funding Information: JJD was funded by Action for M.E. and the Chief Scientist Office, Scotland [AME/CSO/18/01]. BF, MF, MR, NP and SM were funded by the Fischer Family Foundation. CPP was supported by the Medical Research Council University Unit award to the MRC Human Genetics Unit, University of Edinburgh, grant number MC\_UU\_00007/15. Funding Information: This study was carried out using samples from the UK ME/CFS Biobank, which were processed and stored at the UCL-RFH Biobank. We thank Prof Georg Holl{\"a}nder and Simon J McGrath for valuable discussions during the planning of this project, and {\O}yvind Almelid for help solving coding problems. We also thank Mark M. Davis (Stanford University School of Medicine) whose unpublished TCR studies initially inspired this work. Publisher Copyright: {\textcopyright} 2024, The Author(s).",

year = "2024",

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language = "English",

journal = "BMC Research Notes",

issn = "1756-0500",

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T1 - Comparison of T-cell Receptor Diversity of people with Myalgic Encephalomyelitis versus controls

AU - Dibble, Joshua

AU - Ferneyhough, Ben

AU - Roddis, Matthew

AU - millington, Sam

AU - Fischer, Michael D

AU - Parkinson, Nick J

AU - Ponting, Chris P

N1 - Funding Information: JJD was funded by Action for M.E. and the Chief Scientist Office, Scotland [AME/CSO/18/01]. BF, MF, MR, NP and SM were funded by the Fischer Family Foundation. CPP was supported by the Medical Research Council University Unit award to the MRC Human Genetics Unit, University of Edinburgh, grant number MC_UU_00007/15. Funding Information: This study was carried out using samples from the UK ME/CFS Biobank, which were processed and stored at the UCL-RFH Biobank. We thank Prof Georg Holländer and Simon J McGrath for valuable discussions during the planning of this project, and Øyvind Almelid for help solving coding problems. We also thank Mark M. Davis (Stanford University School of Medicine) whose unpublished TCR studies initially inspired this work. Publisher Copyright: © 2024, The Author(s).

PY - 2024/1/4

Y1 - 2024/1/4

N2 - Objective: Myalgic Encephalomyelitis (ME; sometimes referred to as Chronic Fatigue Syndrome) is a chronic disease without laboratory test, detailed aetiological understanding or effective therapy. Its symptoms are diverse, but it is distinguished from other fatiguing illnesses by the experience of post-exertional malaise, the worsening of symptoms even after minor physical or mental exertion. Its frequent onset after infection suggests autoimmune involvement or that it arises from abnormal T-cell activation. Results: To test this hypothesis, we sequenced the genomic loci of and T-cell receptors (TCR) from 40 human blood samples from each of four groups: severely affected people with ME; mildly or moderately affected people with ME; people diagnosed with Multiple Sclerosis, as disease controls; and, healthy controls. Seeking to automatically classify these individuals’ samples by their TCR repertoires, we applied P-SVM, a machine learning method. However, despite working well on a simulated data set, this approach did not allow statistically significant partitioning of samples into the four subgroups. Our findings do not support the hypothesis that blood samples from people with ME frequently contain altered T-cell receptor diversity.

AB - Objective: Myalgic Encephalomyelitis (ME; sometimes referred to as Chronic Fatigue Syndrome) is a chronic disease without laboratory test, detailed aetiological understanding or effective therapy. Its symptoms are diverse, but it is distinguished from other fatiguing illnesses by the experience of post-exertional malaise, the worsening of symptoms even after minor physical or mental exertion. Its frequent onset after infection suggests autoimmune involvement or that it arises from abnormal T-cell activation. Results: To test this hypothesis, we sequenced the genomic loci of and T-cell receptors (TCR) from 40 human blood samples from each of four groups: severely affected people with ME; mildly or moderately affected people with ME; people diagnosed with Multiple Sclerosis, as disease controls; and, healthy controls. Seeking to automatically classify these individuals’ samples by their TCR repertoires, we applied P-SVM, a machine learning method. However, despite working well on a simulated data set, this approach did not allow statistically significant partitioning of samples into the four subgroups. Our findings do not support the hypothesis that blood samples from people with ME frequently contain altered T-cell receptor diversity.

UR - https://www.scopus.com/pages/publications/85181476171

M3 - Article

SN - 1756-0500

JO - BMC Research Notes

JF - BMC Research Notes

ER -

Comparison of T-cell Receptor Diversity of people with Myalgic Encephalomyelitis versus controls

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Comparison of T-cell Receptor Diversity of people with Myalgic Encephalomyelitis versus controls

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