Micro-RNA in ME/CFS

Hutan

Hutan

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Prompted by a recent paper claiming to have identified a micro-RNA signature for endometriosis in saliva:
Jonathan Edwards said:
I have been sceptical about the power of miRNA analysis to help with ME/CFS. I mentioned this to my pain genetics colleagues who have an interest in long non-coding RNAs and they agreed. But I wonder if we should discuss miRNAs in a bit more detail on a thread.

I can see that endometriosis cells and nearby peritoneal cells might chuck out miRNAs of a particular pattern just through random leakage, in the way that prostate specific antigen leaks out of prostate cancer cells.

What I find odd is that they should need to study 109 miRNAs to show the pattern. For most diseases where biomarkers make use of combinations of molecules it is 2, 3 or maybe 4. Presumably the 109 just reflects throwing in anything that adds a little bit more discrimination but it remains puzzling.

My main puzzlement about miRNAs is that I find it hard to see how they could be much use as deliberate biological signals, perhaps passed from one cell to another in extracellular vesicles, as is claimed. If a cell threw out vesicles then why should they reach any other particular cell rather than just got gobbled up by spleen. On the other hand if these are non-specific danger signals or possibly specific signals for lack of something specific like insulin or blood flow then maybe that would not be a worry, if specific vesicle-grabbing cells in immune organs, liver or even brainstem got the message. But then maybe you wouldn't expect any very fancy pattern of miRNAs?

In ME/CFS we do not so far have any indication that any very unusual cells, like endometrial cells, are signalling. Which makes me still sceptical that they would ever be an miRNA signature. On the other hand maybe miRNA analysis might at least tell us about immune cell populations that at present we cannot track by blood tests but which are behaving badly in a way that is reflected in miRNA output. My memory is that there have been studies from Canada but I haven't heard more about that recently.
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There have been some studies of micro-RNA in the blood of people with ME/CFS. It's worth having another look at the papers to see where we have got to.
 
John Mac

Thread 'MicroRNAs as biomarkers of pain intensity in patients with chronic fatigue syndrome. Al-Rawaf (2019)'

Abstract
BACKGROUND:
Numerous experimental models have shown that microRNAs play an important role in regulating pain-processing in clinical pain disorders.
In this study, we evaluated a set of micro-RNAs as diagnostic biomarkers of pain intensity in adolescents with chronic fatigue syndrome (CFS).
We then correlated the expression of these microRNAs with the levels of inflammatory markers and pain-related comorbidities in adolescents with CSF and healthy controls (HCs).

METHODS:
A total of 150 adolescents, aged 12-18 years, participated in this study between April 2016 and April...
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  • John Mac
  • al-rawaf biomarker me/cfs micro-rna mir-124 mir-143 mir-146a mir-150 mir-558 pain
  • Replies: 11
  • Forum: ME/CFS research
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Differential expression of miR-558, miR-146a, miR-150, miR-124, and miR-143 was significantly down regulated and notably interfered with pain intensity and frequency in patients with CFS.
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We weren't too impressed with this paper.
 
Nor this one that had 9 participants and aimed to identify changes in microRNA after sessions of yoga. There were no healthy controls.

Sly Saint

Thread 'Changes in circulating microRNA after recumbent isometric yoga practice by patients with ME/CFS: pilot study, 2019, Takakura,Oka,Sudo'

Abstract
Background
Yoga is a representative mind-body therapy. Our previous studies have demonstrated that isometric yoga (i.e. yoga programs that we developed so individuals can practice yoga poses with a self-adjustable isometric load) reduces the fatigue of patients with myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS); however, the underlying mechanisms remain unclear. Several studies have suggested that the micro-ribonucleic acid (miRNA) expression of ME/CFS patients is different from that of healthy subjects. However, it has not to date been...
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This one is from Maureen Hanson's lab - microRNA in PBMCs and EVs. I'm not sure if we have heard more from them?


John Mac

Thread 'Assessing diagnostic value of microRNAs from peripheral blood mononuclear cells and extracellular vesicles in ME/CFS, Almenar-Perez et al. 2020'

Full Title:
Assessing diagnostic value of microRNAs from peripheral blood mononuclear cells and extracellular vesicles in Myalgic Encephalomyelitis/Chronic Fatigue Syndrome

Abstract
Myalgic Encephalomyelitis/Chronic Fatigue Syndrome (ME/CFS) is a debilitating multisystemic disease of unknown etiology, affecting thousands of individuals worldwide. Its diagnosis still relies on ruling out medical problems leading to unexplained fatigue due to a complete lack of disease-specific biomarkers.

Our group and others have explored the potential value of microRNA profiles...
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  • John Mac
  • 2020 almenar-perez creatine kinase extracellular vesicles me/cfs micro-rna paper severe uk me/cfs biobank
  • Replies: 6
  • Forum: ME/CFS research
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SNT Gatchaman said:
PBMCs
Over-expressed (p<0.05)
  • miR-374a-5p
  • miRNA-4516
  • miR-340–5p
  • miR-140-5p
  • miR-18a-5p
  • miR-146a-5p
  • miR-106a-5p
  • miR-17-5p
  • miR-106b
p<0.1
  • miR-21-5p
Under-expressed (p<0.05)
  • miR-644a
  • miR-451a
  • miR-4454
  • miR-7975
  • miR-549a
  • miR361-3p
  • miR-1253
  • miR-590-5p
EVs
Over-expressed (p<0.05)
  • miR-4454
  • miR-7975
  • miR-150-5p
  • miR-15a-5p
  • let-7d-5p
  • miR-423-5p
  • miR-374a-5p
  • miR-130a-3p
p<0.1
  • miR-21-5p
  • miR-320e
  • miR-185-5p
  • let-7g-5p
  • miR-126-3p
  • miR-223-3p
  • miR-93-5p
Under-expressed (p<0.05)
  • miR-183-3p
  • miR-33a-5p
p<0.1
  • miR-203a-5p
  • miR-607
  • miR-369-3p
Bold are miRs that are differentially expressed in both the PBMCs and EVs. Note that miR-4454 and miR-7975 are over-expressed in EVs but under-expressed in PBMCs. The paper says "At present, the significance of these differences is not understood." (I don't know if one possibility would be that PBMCs are off-loading those particular miRs via EVs.)
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There was this thesis.
Dolphin

Thesis Thread 'Circulating miRNAs in myalgic encephalomyelitis : chronic fatigue syndrome, 2023, Nepotchatykh (advisor: Moreau)'

https://papyrus.bib.umontreal.ca/xmlui/handle/1866/32791

Circulating miRNAs in myalgic encephalomyelitis : chronic fatigue syndrome
Thesis or Dissertation


Author(s)
Nepotchatykh, Evguenia
Advisor(s)
Moreau, Alain
Level
Doctoral
Discipline
Biologie moléculaire

Myalgic encephalomyelitis (ME) is a complex chronic heterogeneous illness whose etiology and pathophysiology remain poorly understood. This disease has a multitude of symptoms, and it is characterised by unexplained constant fatigue unrelieved by rest and...
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This one was from Klimas' lab. The results were underwhelming, just a couple of microRNAs were different from healthy controls only in males:
miRNA-423-5p and miRNA-4443

Andy

Thread 'Unravelling .. (ME/CFS): Gender‐specific changes in the microRNA expression profiling in ME/CFS, 2020, Cheema, Klimas et al'

Myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS) is a multisystem illness characterized by medically unexplained debilitating fatigue with suggested altered immunological state.

Our study aimed to explore peripheral blood mononuclear cells (PBMCs) for microRNAs (miRNAs) expression in ME/CFS subjects under an exercise challenge. The findings highlight the immune response and inflammation links to differential miRNA expression in ME/CFS. The present study is particularly important in being the first to uncover the differences that exist in miRNA expression patterns in males...
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  • Andy
  • 2020 cheema exercise gender klimas leptin me/cfs micro-rna transcriptomics
  • Replies: 2
  • Forum: ME/CFS research
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This one was from the Moreau lab. It looked at microRNA before and after the application of an inflatable cuff stressor (like a blood pressure cuff). to people with severe ME/CFS.

We don't seem to have discussed the microRNA findings much. Nepotchatykh is the primary author of the study (her thesis is in post #6 of this thread.

S

Thread 'Profile of circulating microRNAs in Myalgic Encephalomyelitis......(2020), Nepotchatykh, Moreau et al'

Google translated:

The Canadian Press
MONTREAL - A new test developed by Montreal researchers is expected to improve the diagnosis and treatment of patients with myalgic encephalomyelitis (ME), a condition better known as chronic fatigue syndrome.


L'EM is currently diagnosed primarily by elimination, as doctors put aside other possible causes of the patient's symptoms.

Researchers from the University of Montreal and the CHU Sainte-Justine led by Professor Alain Moreau have now put their finger on a blood biomarker that can identify patients with ME....
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"In the present study, we performed extensive profiling of circulating miRNAs on plasma samples of patients with severe ME/CFS (housebound), both at baseline and in response to the application of a post-exertional stress challenge. This unique experimental design led us to determine distinct molecular footprints of ME/CFS by comparing the differential expression plasma miRNA levels before and after 90 min of stimulation, which induced PEM, compared to age- and sex-matched controls. With implementa-tion of a machine learning algorithm (i.e., Random Forest), we validated eleven microRNAs (
hsa-miR-28-5p,
hsa-miR-29a-3p,
hsa-miR-127-3p,
hsa-miR-140-5p,
hsa-miR-150-5p,
hsa-miR-181b-5p,
hsa-miR-374b-5p,
hsa-miR-486-5p,
hsa-miR-3620-3p,
hsa-miR-4433a-5p, and
hsa-miR-6819-3p),
the first diagnostic panel of its kind.

Differential expression of these eleven circulating miRNAs led to the identification of four ME/CFS clusters with distinct miRNA profiles and specific symptom severities"
 
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This one is another from the Moreau team, from 2023, working with plasma samples. We had some questions about whether there might have been some technical problems with the fibromyalgia samples, but the ME/CFS results might be worth checking out.

It was noted by the people doing the endometriosis study that saliva samples are a lot easier to work with than blood samples.


Andy

Thread 'Circulating microRNA expression signatures accurately discriminate [ME] from fibromyalgia and comorbid conditions 2023 Moreau et al'

Abstract

Myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS), and fibromyalgia (FM) are two chronic complex diseases with overlapping symptoms affecting multiple systems and organs over time. Due to the absence of validated biomarkers and similarity in symptoms, both disorders are misdiagnosed, and the comorbidity of the two is often unrecognized. Our study aimed to investigate the expression profiles of 11 circulating miRNAs previously associated with ME/CFS pathogenesis in FM patients and individuals with a comorbid diagnosis of FM associated with ME/CFS...
  • Andy
  • fibromyalgia me/cfs micro-rna mir-124 mir-127 mir-140 mir-374 moreau
  • Replies: 11
  • Forum: ME/CFS research
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These are the three miRNA that were different between the ME/CFS samples and the healthy controls (all of which made the short list in the 2020 study). I think the levels were higher in ME/CFS but need to check that.

hsa-miR-127-3p
hsa-miR-374b-5p
hsa-miR-140-5p
 
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So possibly Moreau's lab identified miR-374b-5p as having a higher expression in ME/CFS compared to controls , and Hanson's lab identified miR-374a-5p as being over-expressed (in PBMCs and in EVs). I'm not sure how consequential the 'a' and 'b' difference is.

If you click on those links in my last post (copied from @SNT Gatchaman), it takes you to a database where you can click through to see the known targets of the specific miRNA. There are number of X chromosome targets for miR374b-5p.

I think I need to read the discussion section of the Hanson and Moreau papers. It would be interesting to have a good look at the targets of the miR374.
 
Super interesting.

Hutan said:
Differential expression of these eleven circulating miRNAs led to the identification of four ME/CFS clusters with distinct miRNA profiles and specific symptom severities"
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I need to read this study but this was exactly what I was wondering: could a large study potentially find subtypes (if they exist) in an unbiased way.

I’m going to try and read up on just the basics of miRNA. I’m curious how far along they’ve gone as a biomarker in other diseases (looks like a lot of the interest has been in various cancers?). Im also wondering how consistent salivary miRNA is. Do people have similar profiles day to day?

Kitty said:
AI summaries from https://mirbase.org (hard to know how accurate these are):
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Ooo this AI summary at least provides references, which helps a lot.
 
ScoutB said:
I’m going to try and read up on just the basics of miRNA. I’m curious how far along they’ve gone as a biomarker in other diseases (looks like a lot of the interest has been in various cancers?). Im also wondering how consistent salivary miRNA is. Do people have similar profiles day to day?
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A lot of miRNA screens have been done in almost every context, especially cancer, largely because the technology for it is pretty cheap these days. It’s similar to differential gene expression where nearly every comparison will show some differences, but those findings often won’t replicate between cohorts or it’s very hard to draw conclusions on what those differences really mean. And compared to genomic studies, we tend to have even less information about what the miRNAs in question actually do.

There are a couple instances I know of where miRNAs were experimentally confirmed to be actually central to the disease process—Hep C infection is the example that comes to mind.
 
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