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Volume 16 Issue 1
May 2026
UK Charity Invest in ME Research
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From the Chair
Our Conference Week Partners
Fellowship Update: Ian Gibson & LunaNova
Light ME Up: Red Light Therapy for ME
LunaNova Fellowship: Ancient Viruses, Modern Disease
COMPASS-ME
SEE ME
RESTORE-ME Clinical Trial
The Centre of Excellence for ME – A Case for Investment
Dutch Research Award
Summer Student Bursaries 2026
Young EMERG: Supporting Young Researchers
Mike's European Marathons
How to Support the Charity
Germany Takes Action
The BRMEC Colloquia - Fifteen Years of Building ME Research
BRMEC15 Day 1 Programme
BRMEC15 Day 2 Programme
BRMEC15 Day 3 / IIMEC18 Conference
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5
6
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DISCLAIMER
The views expressed in this Journal by contributors and others do not necessarily represent those of
Invest in ME Research. No medical recommendations are given or implied. Patients with any illness
are recommended to consult their personal physician at all times.
Published by Invest in ME Research, May 2026
Invest in ME Research
Registered Charity No. 1153730 PO Box 561 Eastleigh SO50 0GQ Hampshire, UK
investinme.org
© Invest in ME Research 2026. All rights reserved. No part of this publication may be reproduced
without the prior permission of the publisher.
׉	 7cassandra://vldogoD6Ay5R4iglDEwiNlkwNSmHEBm-rZUEPd8VfWUZ`̷ j#\^D^E׉E/JOURNAL OF IIMER
May 2026
CHAIRMAN’S MESSAGE
Dear Friends and Supporters,
Welcome to International ME Conference Week
2026 - a milestone year in every sense as we mark
twenty years of Invest in ME Research and reflect
on what two decades of dedication, collaboration,
and principled advocacy have made possible.
Over twenty years, this charity has remained
focused on one unwavering objective: meaningful
progress in the understanding and treatment of
ME.
Our efforts have ranged from direct advocacy and raising educational standards through influential
international conferences, to establishing research fellowships, funding the UK's only clinical trial for ME,
and initiating and sustaining European networks of researchers, clinicians, and patient groups. These
efforts have made a difference - and we have achieved them thanks to the extraordinary support of our
supporters and the collaboration of this community of researchers, clinicians, patients, carers, and
supporters.
This year's conference week spans five days - uniquely the only such 5-day event for ME in the world - and
brings together a wonderful combination of events: the seventh early-career workshop led by Young
EMERG; the European ME Research Group Annual Meeting, which this year discusses an EMERG-led panEuropean
research project for ME; our fifteenth Biomedical Research into ME Colloquium; the eighteenth
International ME Conference, now integrated into the final day of the colloquium, bringing researchers,
clinicians, and patients together in a shared forum; and a planning meeting organised for a future critical
clinical platform project. The theme of the events this year - "20 Years of Investing in ME Research to
Discover ME" - reflects both where we have come from and where we now proceed.
Our research colloquium focuses on systems biology, immunology, metabolism, neurology, microbiome
research, AI and bioinformatics, and future pathways for treatment - representing the breadth and depth
of international scientific engagement that our annual gatherings have helped to foster. We are delighted
to welcome Professor Sarah Teichmann as keynote speaker at BRMEC15, and to host delegates and
speakers from institutions across more than twenty countries - including the NIH, Karolinska Institutet,
Columbia University, Imperial College London, the Quadram Institute, Cornell University, the University of
Cambridge, Med. University of Vienna, Catholic University of Valencia and many more.
This is, quietly but significantly, a landmark year. Though formal announcements must wait a little longer,
two major developments - one representing the first substantial pan-European research initiative of its
kind for ME, the other a meaningful advance in clinical research capacity - are the direct result of work
built patiently over two decades by this charity, its collaborators, and its supporters. Both are landmarks
for European ME research. Both are the direct consequence of sustained network-building, collaboration,
and long-term investment in research infrastructure. The groundwork laid through EMERG, through our
annual colloquia, through investment in early-career researchers, and through European partnership is
bearing fruit in ways that will become clear in due course. We look forward to sharing the full story when
the time is right.
Invest in ME Research
Page 2 of 35
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JOURNAL OF IIMER
May 2026
It is worth reflecting on how progress of this kind is made. The networks, research relationships, and
institutional infrastructure that now exist were built here - collaboratively, persistently, and without
public support - over twenty years. That is not a complaint; it is context.
Public funding, when it has materialised, has too often been directed towards familiar recipients and
familiar approaches, at times reconstructing what already existed rather than building upon it. The effect
has been to introduce delay where there was opportunity for acceleration, and to consume resource that
might otherwise have gone directly to research. This may not be unique to ME; it is a pattern well
recognised across many fields. But for a condition where patients have waited long enough, the cost is felt
particularly keenly. Influence over the research agenda is not the same as advancing it. Administrative
overhead is not the same as doing the work. And the structures this community has spent twenty years
building do not need to be replicated elsewhere - they need to be resourced.
Control is not progress.
Administration is not research.
The wheel does not need reinventing - it needs funding and support.
The Centre at Norwich Research Park stands as one of the clearest expressions of what vision,
commitment, and genuine collaboration can produce. The scientific and institutional infrastructure is in
place. The missing ingredient has been consistent, adequate funding from those with both the means and
the mandate to provide it.
Twenty years have shown that persistence, integrity, and collaboration yield results. Yet, as a small,
entirely volunteer-run charity - no salaries, every donation directed to biomedical research - we continue
to swim against the tide with continuing missed opportunities at the policy level demonstrating that, in
the UK at least, rapid progress will come primarily through the efforts of the biomedical research
community that has been built here, not through the goodwill of institutions that have repeatedly shown
their preference for a status quo or strategic indecision.
Our great thanks to conference sponsors the Irish ME Trust, Quadram Institute Bioscience, Terra
Biological LLC, PrecisionLife, and Vazyme, and to The Hendrie Foundation and LunaNova for their
immense and valued commitment to our research.
As we open this conference week, we invite all delegates - researchers, clinicians, patients, early-career
scientists, and supporters - to engage fully with the presentations, participate in the discussions, and build
the connections that will carry ME research forward into its next chapter.
Welcome to International ME Conference Week 2026.
Kathleen McCall
Chairman, Invest in ME Research
Invest in ME Research
Page 3 of 35
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May 2026
Our 2026 Conference Week Partners
This May, Invest in ME Research marks twenty years of funding and facilitating biomedical research into
Myalgic Encephalomyelitis - and does so by bringing the global ME research community together for the
International ME Conference Week 2026.
Five days. Five events.
Researchers, clinicians, early-career scientists and patients from more than twenty countries.
To our knowledge, the only five-day international conference week dedicated entirely to ME anywhere in
the world.
That this week exists at all is a reflection of twenty years of determination. That it continues to grow is, in
no small part, due to the partners we are proud to acknowledge here.
The Irish ME Trust has supported every single conference since 2006 - a partnership spanning the full
twenty years of this charity's history. That kind of sustained, unconditional commitment to ME research is
rare, and its value cannot be overstated.
We extend our sincere thanks also to Quadram Institute Bioscience, Terra Biological LLC, PrecisionLife
and Vazyme.
Together, these organisations represent something important - not simply financial support, but
confidence in the science, in the researchers, and in the work this community is doing.
That confidence is what allows this conference week to exist, to grow, and to matter. We are grateful for
every part of it.
Invest in ME Research
Page 5 of 35
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JOURNAL OF IIMER
May 2026
Advancing ME Research
The Fellowships at Norwich Research Park
Invest in ME Research, in partnership with the Quadram Institute, has established two postdoctoral
fellowships at Norwich Research Park - the Ian Gibson Fellowship and the LunaNova Fellowship - both
dedicated to advancing biomedical research into myalgic encephalomyelitis.
The Ian Gibson Fellowship, launched in 2022 and named in honour of the late Dr Ian Gibson - scientist,
politician and tireless advocate for people with ME - was the first
postdoctoral fellowship in the UK dedicated solely to ME research.
Held by Dr Katharine Seton, it continues her career in ME research at
the Quadram Institute, building on her PhD funded by Invest in ME
Research and the University of East Anglia.
Dr Seton's research focuses on determining the contribution of the
intestinal microbiome to oxidative stress in ME patients, and whether
this drives alterations in immune function that accelerate premature
immune ageing. She is also investigating the impact of microbiota
replacement therapy on intestinal and systemic oxidative stress in ME
patients - the first study to directly assess this relationship - with the
aim of identifying whether targeting the gut microbiome can restore immune function and alleviate
symptoms.
The LunaNova Fellowship, funded by technology company LunaNova and introduced in 2023, is held by
Dr Krishani Perera, who joined Professor Simon Carding's laboratory at the Quadram Institute of
Bioscience in July 2024. Her two-year fellowship centres on the gut-immune-brain axis and the search for
biomarkers, with strong links to the European ME Research Group and international partners.
Dr Perera's research investigates whether the
reactivation of human endogenous retroviruses - genes
embedded within our genome that are ordinarily kept
inactive - may drive accelerated ageing of immune cells
in ME patients. Her work seeks to establish whether
HERV reactivation plays a causal role in immune dysfunction. She is also contributing to the RESTORE-ME
clinical trial, a phase IIb placebo-controlled study investigating microbiota replacement therapy, and to
the COMPASS ME Study, which analyses microbial communities - viruses, bacteria, and fungi - in the
mucus of people with ME.
Both fellowships sit at the heart of the strategy to develop the UK Centre of Excellence for ME at Norwich
Research Park, supporting ongoing clinical trials and PhD studentships, and building the sustained
research capacity that this seriously under-resourced condition demands.
With revised estimates now placing the number of people with ME in the UK at over 400,000 - a figure
that continues to grow in the wake of the Covid pandemic - the urgency of this work has never been
clearer.
Invest in ME Research
Page 6 of 35
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JOURNAL OF IIMER
May 2026
Invest in ME Research has always maintained a clear focus: directing funding towards rigorous biomedical
research with real potential, building a sustainable research base, and driving meaningful progress.
The fellowships at Norwich Research Park are a direct expression of that commitment.
Further information on Dr Seton: https://quadram.ac.uk/people/katherine-seton/
Further information on Dr Perera: https://tinyurl.com/Quadram-Krishani
Light ME Up – Exploring Red Light Therapy for ME
In April 2024, Dr Katharine Seton, PhD – the Ian Gibson Fellow funded by
Invest in ME Research – began a pilot study looking at whether red light
therapy could be helpful for people with ME.
Red light therapy is already an approved treatment (by the FDA) for
conditions such as chronic pain, wound healing, and hair regrowth.
However, it has not previously been formally tested in people with ME/CFS.
Early research in other conditions suggests it may help improve energy
levels, reduce pain, and support blood circulation. These are all areas that
can be challenging for people with ME, so it made sense to explore whether
this therapy might offer some benefit.
Red light is absorbed by the mitochondria – often described as the
“batteries” inside our cells – where it may help increase energy production.
Research also suggests that timing matters, as the therapy appears to work best in the morning, in line
with the body’s internal (circadian) clock, particularly between 9am and 11am.
Importantly, the device used in this study was a targeted single-wavelength red light specifically designed
for research purposes. This is difference from many commercially available products, which usually emit a
broad spectrum of light. We would strongly advise patients not to purchase or use red light devices based
on this early-stage research.
How the study worked
Over a 12-month period, 26 people with ME from across the UK took part in this 9-week study.
Importantly, the study was carried out entirely from home, so participants could take part in a way that
suited their needs. This approach also made it possible for people who are more severely affected by ME
to be involved in research.
Before starting the therapy, participants completed a set of assessments to understand their symptoms
and daily functioning.
These included:
• A questionnaire about their ability to carry out everyday activities (FUNCAP27)
• Online cognitive (thinking and memory) tests
• Wearing a wrist activity monitor for seven days
• Keeping a sleep diary for seven days
Once these were completed, participants were sent a red light lamp to use at home.
Invest in ME Research
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May 2026
They were asked to use the lamp for 2 minutes each morning, between 9am and 11am, for two weeks.
After this two-week period, the same assessments were repeated to see whether there were any changes
in symptoms. Participants were also asked to share feedback about their experience of taking part.
What did participants tell us?
Of the 26 people who started the study, 20 completed all aspects of it.
The early findings show that most participants found the red light therapy easy to use:
• 86% were able to set up and use the lamp on their own
• All participants said they would be willing to use the lamp again
• Around 14% said they would prefer a different time schedule
More than half of participants found it
difficult to use the lamp between 9am and
11am. Despite this, participants showed
remarkable commitment, with everyone
using the lamp for at least 12 out of the 14
recommended days.
The therapy also appeared to be safe. Only
one participant reported a mild reaction to
the light.
Feedback on study assessments
Most people (86%) were able to wear the
activity monitor for the full seven days.
However, eight participants reported discomfort from the wrist strap, and some experienced worsening
of eczema. As a result, the research team is now exploring more comfortable strap options for future
studies.
Participants were also asked to complete up to six cognitive tests in one sitting. Nearly everyone
completed all the tests, but about one-third reported a temporary worsening of symptoms afterwards.
This feedback is important and will help shape how assessments are designed in future research.
What happens next?
The research team is now carrying out the next stage of analysis. This includes working with a statistical
expert to combine information from multiple sources, such as questionnaires, activity monitoring, sleep
diaries, and cognitive tests, to explore whether red light therapy may provide any measurable benefits for
people with ME.
The team hope to have results ready by the autumn and they look forward to sharing further updates
with you then.
Sharing the research
We are also pleased to share that Katharine presented the preliminary findings from this study at the
Young EMERG Workshop in Vienna in November 2025.
Her work was very well received, and she was awarded first place in the poster presentation competition
– a fantastic achievement and recognition of the importance of this research.
Invest in ME Research
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May 2026
LUNANOVA FELLOWSHIP - RESEARCH IN FOCUS
Ancient Viruses, Modern Disease - The Role of Human Endogenous
Retroviruses in ME
A review published in the International Journal of Molecular Sciences argues that
human endogenous retroviruses - ancient viral sequences embedded in our
genome - may be active drivers of the biological processes underlying ME.
Written by Perera, Oltra and Carding of the Quadram Institute Bioscience and
Norwich Research Park, it represents a significant step towards understanding
ME as a mechanism-driven, biologically distinct condition.
What Are Human Endogenous Retroviruses?
Human endogenous retroviruses (HERVs) are the remnants of ancient viral
infections that integrated into human DNA millions of years ago. They now make up approximately 8% of
the human genome. Under normal conditions they are kept inactive. When that suppression breaks down
- through infection, stress, or immune dysfunction - HERVs can reactivate and begin producing viral
proteins and RNA. This can amplify immune responses, drive chronic inflammation, and disrupt normal
gene regulation. Reactivated HERVs have already been implicated in autoimmune diseases including
multiple sclerosis, lupus, and juvenile rheumatoid arthritis.
The Link to ME
The review proposes that reactivated HERVs are plausible contributors to the hallmark features of ME -
persistent post-infectious immune dysfunction, chronic inflammation, and the neurological and cognitive
symptoms that characterise the disease.
Three principal mechanisms are identified. First, HERV proteins trigger sustained immune responses that
may perpetuate the immune activation seen after acute viral infection. Second, HERV elements can act as
alternative gene switches, upregulating inflammatory networks in ways consistent with the immune
patterns observed in ME. Third, HERV reactivation disrupts the very mechanisms that would normally
suppress it, creating a self-reinforcing cycle.
The paper draws on evidence from multiple sclerosis research, where a specific endogenous retrovirus
has been the most thoroughly studied. The authors argue that the immune and inflammatory changes
associated with HERV reactivation closely mirror those documented in ME - including altered natural killer
cell function, T-cell exhaustion, and elevated pro-inflammatory cytokines. Viral infections known to trigger
ME onset - including SARS-CoV-2, Epstein-Barr virus, and enteroviruses - are also known to reactivate
HERVs, providing a coherent molecular link between post-infectious onset and the chronic immune
dysregulation that follows.
Biomarkers and Treatment Implications
ME currently has no validated biological diagnostic test. The review identifies HERV expression patterns as
a promising approach for distinguishing ME from healthy controls and from overlapping conditions such
as fibromyalgia, long COVID, and depression. If validated, HERV signatures could also provide a
quantitative measure of disease severity and a means of monitoring treatment response.
On the therapeutic side, the paper identifies several candidate strategies: HERV-targeted antibodies,
antiviral agents that suppress HERV activity, immune modulators targeting downstream inflammation,
and epigenetic interventions aimed at restoring HERV suppression at source. The authors are careful to
present these as directions requiring clinical validation, not established treatments. They specifically call
for clinical trials enrolling patients selected on the basis of defined HERV expression profiles as the
necessary next step.
Invest in ME Research
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May 2026
The authors’ explicit goal is to transform ME from a symptom-based syndrome into a mechanism-driven,
treatable condition. This review is a substantive step in that direction.
Original Paper
Perera KD, Oltra E, Carding SR. Human Endogenous Retroviruses in Myalgic Encephalomyelitis/Chronic
Fatigue Syndrome: Emerging Roles in Pathogenesis, Immunity, Biomarkers and Therapeutics. Int. J. Mol.
Sci. 2026, 27(10), 4309.
DOI: 10.3390/ijms27104309 - Published: 12 May 2026 - Open Access (CC BY)
COMPASS-ME
The COMPASS-ME Study - Investigating the Microbial Landscape of ME
One of the questions that has persistently complicated ME research is
deceptively simple: what role, if any, do microbes play in triggering or
sustaining the disease? Many patients report a viral infection preceding the
onset of their symptoms, and the overlap with long COVID has reinforced the
view that post-infectious mechanisms are central to understanding ME. Yet
despite decades of investigation, no single pathogen has been definitively
linked to the condition, and the broader microbial picture - encompassing not
only viruses but bacteria and fungi - has remained poorly characterised.
The COMPASS-ME study, funded by Invest in ME Research and based at the Quadram Institute Bioscience
on Norwich Research Park, is designed to address precisely this gap. Led by LunaNova fellow Dr Krishani
Perera, working within Professor Simon Carding's research group, the study will analyse the mucosal
microbial communities - including viruses, bacteria, and fungi - of individuals with and without ME, using
mucosal swab samples taken from sites where microbial infections commonly begin. The approach is both
scientifically rigorous and practically considered: given the significant mobility difficulties experienced by
many people with ME, sampling methods have been chosen specifically to minimise the burden on
participants and ensure the study is as inclusive as possible.
Dr Perera brings to this work a background in molecular virology developed across Kansas State University
and postdoctoral research in France, where she studied viruses that persist in immune-privileged sites in
the body and contribute to long-term health consequences. That expertise in viral persistence and
immune evasion is directly relevant to ME, where the mechanism by which an initial infection might give
rise to chronic, systemic illness remains one of the field's central unanswered questions.
The longer-term ambition of the COMPASS-ME study is to contribute to the development of reliable
diagnostic tools for a disease that currently has none, and to identify the biological mechanisms that
might, in time, be amenable to targeted treatment. It is work that is painstaking, methodologically careful,
and - given the complexity of ME and the number of intersecting biological systems involved - necessarily
cautious in its conclusions. That caution is a strength, not a limitation. The field has suffered from
premature certainty in the past.
What is needed now is precisely the kind of systematic, well-grounded investigation that this study
represents.
Further information: quadram.ac.uk
Invest in ME Research
Page 10 of 35
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May 2026
SEE ME
A clinical innovation fund which benefits patients through research by bringing together Quadram
Institute (QI) scientists and doctors at the Norfolk and Norwich University Hospital (NNUH) has selected
five new projects for funding.
The Quadram Institute Clinical Seedcorn Fund was first established in 2021/2022 to help clinicians
develop research ideas with scientists at the Quadram Institute. The fund supports secondments of NHS
staff to Quadram Institute laboratories and associated research costs.
Quadram Institute Bioscience (QIB) in partnership with the Norfolk & Norwich Hospitals Charity have
provided £100,000 each to jointly fund £200,000 of new collaborative clinical research projects.
Included in this is a project entitled SEE-ME - Retinal Biomarkers of Visual Disturbances in Myalgic
Encephalomyelitis/Chronic Fatigue Syndrome – and this will be run by ‘Ian Gibson fellow’ Dr Katharine
Seton (QI) and NNUH consultant ophthalmologist Mr Colin Jones (NNUH).
This is a very novel research pathway and another spin-off from the ME research being carried out at the
centre.
Further information: quadram.ac.uk
RESTORE-ME Clinical Trial
The RESTORE-ME trial - a phase IIb, randomised, placebocontrolled
study of microbiota replacement therapy at
the Quadram Institute - remains the UK’s only clinical trial
of its kind for ME, and one of the first to use objective
outcome measures.
Progress has taken longer than originally anticipated. Microbiota replacement therapy is regulated by the
MHRA as an investigational medicinal product, and obtaining the necessary manufacturing licence and
regulatory approvals has proved a complex and time-consuming process.
The pandemic added further delay to building and infrastructure work required at the Quadram Institute.
The research team continues to work on related studies that will optimise the trial protocols alongside the
regulatory preparations.
A further update will be shared as soon as there is more to report.
Meanwhile the associated PPI group that has been formed for the trial continues to meet, with the next
meeting scheduled for July.
Further information: quadram.ac.uk
Invest in ME Research
Page 11 of 35
׉	 7cassandra://vuFjTcteJup4Ydo_fQf9gafyFAHiuUK9as95jBscTrg`̷ j#\^D^O׉E*JOURNAL OF IIMER
May 2026
The Centre of Excellence for ME - A Case for Investment
The research infrastructure at Norwich Research Park was constructed over more than a decade through
the sustained commitment of a volunteer-run charity and its supporters, and the dedication of a handful
of researchers - without government funding, without research council backing, and without the
institutional infrastructure that better-resourced disease areas take as given. Five PhD studentships. The
first dedicated fellowships for ME research in the UK. The RESTORE-ME trial - a phase IIb, randomised,
placebo-controlled study of microbiota replacement therapy, using objective outcome measures, funded
entirely by Invest in ME Research. A programme of basic science, immunology, virology, and microbiome
research embedded within one of Europe's leading gut biology
institutes in one of Europe's most advanced research parks.
The Quadram Institute at Norwich Research Park houses one of
Europe's largest endoscopy units, a clinical research facility, and
world-class expertise in mucosal immunology and gut biology. It
sits within a park of over 3,000 scientists spanning genomics,
immunology, food science, and clinical medicine - one of the
largest single-site concentrations of health research in Europe.
Alongside RESTORE-ME, the COMPASS-ME study is investigating
the mucosal microbes of people with ME, and Dr Krishani Perera's
Luna Nova fellowship is examining the role of human endogenous
retroviruses in immune ageing. The platform for translational
biomedical ME research - the kind that moves between laboratory
and clinic, generating findings that directly inform patient care -
already exists. It was not created by a government initiative.
What sustained public investment in that platform could deliver is not difficult to imagine. Even a
relatively small amount of funding - say, £4-5 million - could fund the expansion of the centre with
multiple fellowships, PhD studentships, and early-career researcher positions needed to grow and sustain
the programme over the long term. It could establish and expand the biobank and clinical database
infrastructure that translational research requires. It could accelerate the work already underway on viral,
fungal, and microbial contributions to ME. It could catalyse the European collaboration building on
already established links and partnerships. It could, in short, transform a functioning research foundation -
driven and funded over twenty years without government or research council support - into the properly
resourced centre of excellence that patients need and the science is ready to deliver.
The context for that case is sobering. Between 2015 and 2020, UK public research funding for ME totalled
just £6 million - compared to £53 million for Parkinson's disease and £22 million for multiple sclerosis,
despite ME affecting comparable or greater numbers of people. The economic cost of ME to the UK was
estimated at £3.3 billion annually by the 2020health Counting the Cost report - a figure based on 2014-15
data and a conservative prevalence estimate of 0.2% of the population, which the report itself
acknowledged could be as high as 0.7%. That estimate is now a decade old, and with prevalence
substantially revised upward and post-COVID case numbers having increased the affected population
considerably, the economic burden will have risen in proportion. The case for directing serious, sustained
investment towards research infrastructure that already exists, is already producing results, and was built
without the support it deserved is not complex. It is simply overdue.
The Centre at Norwich Research Park is not a proposal awaiting validation. It is a functioning reality that
requires only the investment the establishment has thus far chosen to direct elsewhere.
Invest in ME Research
Page 12 of 35
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May 2026
Dutch Research Award
Virus infection and reactivation and the gastrointestinal microbiome in
myalgic encephalomyelitis
Rik Haagmans, one of the PhDs funded by Invest in ME Research, recently completed his project and, with
the Quadram Institute, applied to the Dutch ZonMW agency for a recent round of awards for research as
part of the ongoing Dutch strategy in their 10 year plan for research into ME.
We are glad to report that Rik was successful in this application and so continues with research into ME
and has established now a collaboration with the Dutch programme.
Here below Rik has written a brief description of the new project.
Viral infections have long been associated with ME/CFS, and may trigger or contribute to maintaining
ME/CFS.
In addition, gut microbiome as well as immune system abnormalities have been found in ME/CFS patients
and gastrointestinal disturbances are a frequent occurrence in ME/CFS.
Gut microbiota play an important role in regulating the immune system and microbiome abnormalities
may affect the immune reaction against viral infections, and chronic viral infections may contribute to
immune system abnormalities themselves.
How the gut microbiome and viral infections interact and contribute to ME/CFS is still unclear, however.
Our project is funded by the Dutch funding organisation ZonMw through their ME/CFS research
programme.
We will be investigating the activity of several viruses commonly associated with ME/CFS, as well as the
composition of the gut microbiome and virome and markers of gut barrier integrity.
This will be done in the Dutch ME/CFS Biobank and Cohort (NMCB) and ME/CFS Lines cohort, as well as in
a group of patients participating in the RESTORE-ME study which will take place at the Quadram Institute
in the UK.
Invest in ME Research
Page 13 of 35
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JOURNAL OF IIMER
May 2026
This way we hope to get a better understanding of the mechanisms underlying ME/CFS, as well as gain
more insight into potential biomarkers and treatments.
More information about the project can be found at the QR code link on the right.
This project investigates the relationship between viruses and the gut microbiome in ME/CFS patients.
This may assist in developing new diagnostic biomarkers for ME/CFS and identifying patients who may
benefit from antiviral or microbiome-targeted treatments, such as faecal microbiota transplantation
(FMT). In a faecal microbiota transplantation, stool containing healthy bacteria from a healthy donor is
transferred to the intestines of a patient to restore the balance of bacteria.
Summer Student Bursaries for 2026
In 2026, Invest in ME Research again partners with the Quadram Institute to encourage knowledge and
awareness of ME amongst undergraduate students via the Invest in ME Research Summer Student
Bursaries.
Quadram Institute will offer up to three awards. The
successful applicants will begin in June.
Invest in ME Research, in collaboration with the Quadram
Institute at Norwich Research Park, is pleased to
announce that we will again partner to establish new
Summer Student Bursaries for 2026. These bursaries are
designed to support undergraduate students in gaining
practical experience in biomedical research, with a focus
on Myalgic Encephalomyelitis.
This initiative aligns with the charity’s objective of raising
education and fostering the next generation of doctors
and researchers. The discovery of new treatments relies
heavily on research into the causes of the disease. The
Summer Student Bursaries provide a unique opportunity for students to contribute to this vital research
while developing their skills and knowledge in biomedical science - raising awareness of ME and
influencing the next generation of researchers in the process.
Three eight-week bursaries are being offered, with involvement in various research projects at the
Quadram Institute. Summer students will join an active research group working on microbiological and
immunological aspects of ME. Projects will be aligned with ongoing research activities and may involve a
combination of laboratory-based and computational approaches.
More details: https://quadram.ac.uk/vacancies/invest-in-me-research-summer-student-bursaries-2/
We are grateful to the Quadram Institute and Carding Lab for making this opportunity possible, further
building on the excellent Centre of Excellence for ME foundations that already exist in Norwich Research
Park.
Thanks to our supporters for making this, and the other forthcoming projects which we have initiated and
in which we are involved, possible.
Invest in ME Research
Page 14 of 35
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May 2026
Last Year’s Bursary Students
From over 50 applications, three students were selected for the 2025 bursaries: Mya Pearce (University of
York, Biology), Paige Cameron (University of Southampton, Biomedical Sciences) and Tayyibah Sarwar
(University of Westminster, Biomedical Sciences). Following their six-week placement at the Quadram
Institute, they shared their reflections.
Their motivations were personal as well as academic. Paige’s sister has ME, making the research feel
urgent and meaningful. Mya was drawn to under-researched, idiopathic conditions. Tay discovered the
bursary almost by chance through LinkedIn - and applied immediately.
All three arrived expecting a step beyond the teaching lab. What they found exceeded that. Mya
investigated antibody reactivity to fungal antigens, learning flow cytometry alongside DNA extraction and
PCR. Paige and Tay both worked on the virome in mucosal cavities of ME patients, developing qPCR, cDNA
synthesis, and bioinformatic analysis skills - much of it entirely new to them.
The Quadram team made a strong impression. The students describe a welcoming, collaborative
environment where questions were encouraged and expertise was freely shared. Tay noted that everyone
- from scientists to canteen staff - was approachable.
All three leave with deepened ambitions: Mya is heading towards a masters in immunology, Paige
towards biomedical research in disease mechanisms, and Tay towards drug development - with ME
treatments in her sights.
As Tay put it: “It was incredibly rewarding to know that the work I was contributing to could one day help
improve understanding and treatment of ME.”
Further information: Invest in ME Research
Young EMERG Workshop Series
The idea behind the formation of the Young EMERG network was to build awareness and provide
opportunities for emerging researchers in Europe and create a support network that could encourage
interest in research into ME, thereby increasing capacity. Last year Young EMERG held their workshop in
Vienna last November.
Invest in ME Research
Page 15 of 35
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May 2026
Supporting Young Researchers at Young EMERG Vienna Workshop
In addition to supporting Young EMERG committee members, Invest
in ME Research offered a number of grants for young European
researchers to attend the Young EMERG International ME
Workshop in Vienna, enabling full engagement in the workshop at
the Medical University of Vienna.
The charity's ongoing efforts to promote and develop ME research
capacity are part of almost two decades of commitment to
collaborative research.
Awardees shared their experiences for our supporters, highlighting the importance of advancing ME
research.
Feedback from Young EMERG Vienna Workshop 2025
"The Young EMERG workshop in Vienna was
exceptionally well organised, with engaging and
relevant content throughout. It was inspiring to see
young researchers exploring diverse approaches to
ME/CFS. The programme was enriched by activities and
the chance to connect with fellow researchers. My
expectations were high, yet the workshop exceeded
them.
I am deeply grateful to the UK charity Invest in ME Research for supporting my participation."
Aline Zamoro Martinez
MSc Nutrition and Health
Wageningen University & Research
"Participating in the Young EMERG Workshop in Vienna
was an absolutely exceptional and deeply inspiring
experience for me. From the very beginning, I felt that
the workshops were prepared with great attention to
every detail, both in terms of academic content and
organization. Everything was executed at the highest
level, which allowed me to fully focus on learning,
exchanging experiences, and personal development.
The atmosphere throughout the workshop was incredibly supportive, open, and motivating. I truly felt
part of an engaged, ambitious, and kind community of young people who share a passion for learning and
continuous self-improvement. The energy was very uplifting and gave me a great deal of motivation to
move forward and keep developing.
The lecturers made a particularly strong impression on me. Their expertise, experience, openness, and
genuine commitment to working with participants were truly inspiring. The way they delivered the
content was engaging, accessible, and thought-provoking. I often found myself reflecting deeply on the
Invest in ME Research
Page 16 of 35
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May 2026
topics discussed, as they challenged my perspective and encouraged me to ask important questions about
my future development, both professionally and personally.
The Young EMERG Workshop Vienna was much more than just a series of workshops for me. It was a true
impulse for growth, reflection, and further action. I am extremely grateful for the opportunity to
participate in this event, and I can confidently say that it was one of the most valuable educational
experiences I have ever had."
Hanna Tabisz
Nicolaus Copernicus University in Torun Collegium Medicum in Bydgoszcz
Poland
"I recently received a travel grant from Invest in ME
Research to attend the Young EMERG workshop in
Vienna, where I presented our upcoming project aimed
at better characterising the mechanisms underlying
post-exertional malaise (PEM). This project will use
non-invasive metabolic imaging techniques to
investigate muscle metabolic alterations during PEM.
Attending the Young EMERG workshop provided an
excellent opportunity to gain a comprehensive
overview of current research directions and priorities within the ME/CFS field. As with fatigue symptoms
in other chronic conditions, the aetiology of ME/CFS is complex and multifactorial, requiring
multidisciplinary approaches to identify underlying mechanisms and inform the development and testing
of treatment targets.
The workshop showcased a broad range of ongoing research, with presentations spanning health
economics, immunology, metabolism, and other relevant disciplines. I found it particularly valuable to
learn about current initiatives aimed at strengthening collaboration within the field, including funding
opportunities for visiting fellowships designed to support cross-institutional partnerships. Such
collaborations will be essential for accelerating progress in ME/CFS research.
As a result of this experience, we have identified potential external research collaborators and aim to
continue developing and applying metabolic imaging approaches to better characterise the mechanisms
contributing to fatigue in ME/CFS. Ultimately, we plan to integrate these novel techniques into future
study protocols to enhance mechanistic understanding and to provide objective measures of organ
function and metabolism when assessing responses to management strategies and pharmacological
interventions."
Jordan McGing
Oxford Centre for Clinical Magnetic Resonance Research
University of Oxford
Invest in ME Research
Page 17 of 35
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May 2026
Mike’s European Marathons Spring 2026 update
I’ve just returned from running my 39th marathon for Invest In ME
Research in European country 35 in Sarajevo, Bosnia.
Now entering my 12th year running for the charity, I’ve managed to
raise £53K through my European marathon running project,
interviewing people with ME in 30 countries that I’ve visited.
Sarajevo Marathon is only in it’s 7th year and I lined up with only
around 250 runners in warm temperatures (c20c) to run a single lap
of the centre and out towards the West of the city with it’s villages
and mountainous backdrop. There was a 5 hour cut-off which I
needed to be aware of but I got around the course fairly steadily and
well within the limit. There were plenty of parts to the race where I
didn’t see anyone else on the course and had to ask the police for
directions! Sarajevo itself was a wonderful mix of Ottoman and
Orthodox architecture with beautiful mosques and churches, historic
bridges and lush green hills all around.
Full race report and trip pictures:
https://www.mikeseumarathons.eu/sarajevo-bosnia.html
Next up for me is Reykjavik Marathon on August 22nd where I’m hoping to meet and liaise with ME Felag,
the country’s ME Association to help raise money and awareness. I’ve been to Iceland 10 years ago with
my wife and enjoyed doing the ‘Gold Circle’ and exploring Reykjavik. I never thought I’d be back to run a
marathon there! I’ve heard positive things about the race and the cool temperatures will be a welcome
gift given all the hot races I’ve been through in Southern Europe. From what I understand, the course is
relatively flat with often windy conditions and hopefully some stunning scenery to keep my brain
occupied.
Although Iceland has a small population, my understanding is that there are quite a few people struggling
with ME and that the Icelandic ME Association has been doing some excellent work in supporting them. I
think they have had runners in the marathon fundraising before and I’m aware that they have some
representatives coming to the Invest In ME Conference which I look forward to attending for the first time
in 8 years.
I’m working on plans for next year, it’s proving tricky as there aren’t
many countries left in Europe to go but I do still have Albania,
Moldova, Turkey, Kosovo, Vatican, Faeroe Islands, Wales, Scotland
and England(!) left to go. After that, I have a few more on my
‘bucket-list’ with a mix of big and small races -one of which includes a
race that runs through Switzerland, Austria and Germany around
Lake Constance which looks awesome.
I may also run a few more local half-marathons to me and see if I can
raise the profile of ME in local media which I’ve done before a few
times.
If you’d like to sponsor me and help fund biomedical research then please visit:
https://www.justgiving.com/fundraising/mikeseumarathons
Invest in ME Research
Page 18 of 35
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May 2026
Germany Takes Action:
A Decade of Funding for Post-Infectious
International collaboration has always been central to this charity's strategy - and European partnership in
particular. The formation of EMEA, EMERG, EMECC, and Young EMERG reflects a long-held conviction that
progress in ME research would be built across borders before it was built within them. Experience
suggested that meaningful change in the UK would depend, in part, on what was demonstrated and
achieved elsewhere first.
That conviction shaped the programme for IIMEC18. Rather than look to UK ministers or research
agencies to open the conference - an avenue pursued many times over the years without result - we
looked to where genuine political will for post-infectious disease research had actually materialised.
The announcement of a decade of dedicated federal funding for post-infectious disease research in
Germany represented exactly the kind of sustained, strategic commitment that patients with ME have
long needed to see.
So we invited Federal Minister of Research, Technology and Space Dorothee Bär to open IIMEC18.
Minister Bär was unable to attend in person, but she kindly contributed the following to our journal.
Journal of IiMER
Invest in ME Research
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May 2026
Bundesministerium für Forschung, Technologie und Raumfahrt,
Berlin
Dorothee Bär MdB
Federal Minister of Research, Technology and Space
Berlin, arch 2026
Invitation to deliver the opening address at the 18th Invest in ME Research Conference
Dear Invest in ME Research,
Thank you for invitation to deliver the opening address at the 18th Invest in ME Research
Conference on 29 May 2026 in Hinxton Hall, UK.
I appreciate your kind words about the leading role of the German National Decade Against PostInfectious
Diseases.
I can assure you that research and development of effective therapies against post-infectious
diseases are of great importance to me and the Federal Ministry of Research, Technology and Space
(BMFTR). I know from many conversations with patients that everyday life is difficult or even
impossible to manage independently for people suffering from ME.
This disease is an enormous bürden for those affected, for their relatives as well as for our entire
society. That is why organisations like yours and the commitment to funding biomedical ME
research and enabling network events through Conferences and colloquia are important in
countering this disease.
As you mention, the BMFTR will intensify research in this area over the next ten years as part of the
National Decade Against Post-Infectious Diseases. Funds totalling 500 million euros have been
earmarked for this purpose and for the duration of the Decade.
In accordance with the latest scientific findings, the focus within the National Decade will be on
research into biomedical causes of these diseases and, building on this, improved diagnostic and
therapeutic procedures.
I want to assure all those affected by post-infectious diseases that we are taking the necessary steps
into the right direction.
We are committed to further creating the ideal research basis for realising treatment options that
can provide a eure or significantly alleviate their suffering.
With the Decade, we are making significant leaps towards achieving these goals together.
Thank you once again for your kind Invitation and the honour of delivering the opening
address at IIMEC18.
Unfortunately, I am unable to take part due to other commitments.
Yours sincerely,
Dorothee Bär
Invest in ME Research
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The BRMEC Colloquia - Fifteen Years of Building ME
The Biomedical Research into ME Colloquium series began in 2011 with what the charity described at the
time as a "Corridor Conference" - an informal gathering of clinicians and researchers during the IIMEC6
conference weekend, discussing ways to collaborate and progress knowledge. Fifteen years on, that idea
has grown into one of the most distinctive annual events in international ME research.
The colloquia are unique symposia designed specifically for biomedical researchers working on ME, or
able to bring relevant expertise into the field. Unlike larger open conferences, they are focused, invitationbased
gatherings - CPD-accredited, and attended by delegates from more than 20 countries. They bring
together scientists, clinicians and early-career researchers in an environment that prioritises exchange
and collaboration over presentation.
That emphasis on collaboration has had tangible results. The colloquia have been directly instrumental in
forming new ME research partnerships across continents, and have spawned lasting international
structures including the European ME Research Group (EMERG) and its associated early-career researcher
network, Young EMERG.
Across fifteen colloquia the themes have shifted as the field has evolved - from early work on aetiology
and autoimmunity, through metabolomics and systems biology, to the emergence of long COVID as both a
parallel and a lens. BRMEC15 in 2026 addresses mechanisms and treatment strategies across nine
sessions spanning systems biology, post-genomics, chronic infection, neuroinflammation, metabolism,
immunology, biomarker discovery and therapeutics.
The ethos has remained constant throughout: volunteer-run, invitation-based, and focused solely on
advancing the science that patients with ME need.
The colloquia have been chaired since 2019 by Professor Simon Carding
of the Quadram Institute Bioscience, Norwich Research Park. Professor
Carding brings exceptional breadth to the role.
His research career has spanned postdoctoral work at New York University
School of Medicine and Yale University, where he worked on the
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May 2026
molecular genetics of gamma-delta T cells - a field of direct relevance to immune dysfunction in ME - and
faculty positions at the University of Pennsylvania, the University of Leeds, and the University of East
Anglia.
At the Quadram Institute he leads the Gut Microbes and Health research programme, one of the foremost
centres for gut biology and mucosal immunology in Europe. He is co-chair of EMERG, and has been a
central figure in building the international research infrastructure around ME.
https://www.investinme.org/brmec15-news-the-colloquia.shtml
This year’s sessions are as follows -
Session 1: A Systems Biology Approach to ME
Moderated by Tamas Korcsmaros, Imperial College Londo, a systems biologist at Imperial
College London whose work focuses on signalling networks, multi-omics data integration
and the application of network medicine to complex disease.
Systems biology offers ME research something it has long needed - a way of looking at
the whole picture. Rather than examining individual genes, proteins or pathways in
isolation, it integrates data from across biological systems, combining computational
modelling with experimental findings to reveal how the parts interact. For a disease as
complex and variable as ME, this kind of joined-up approach may prove essential.
Dezső Modos, also of Imperial College London, applies network biology to
understand how genetic variants - particularly those in non-coding regions of the
genome - drive disease at the cellular level. His iSNP platform maps how these
variants affect regulatory networks, building patient-specific models of disease
pathogenesis that are directly relevant to the challenge of translating ME genomic
data into meaningful biological insights.
Marek Ostaszewski of the Luxembourg Centre for Systems
Biomedicine brings a different but complementary perspective.
As a lead contributor to the COVID-19 Disease Map and a core member of the Disease
Maps Project, his work focuses on building structured, reusable computational
repositories of molecular interaction data - the kind of infrastructure that allows
findings from across the ME research community to be integrated and interrogated
systematically.
Veronika Kedlian, a postdoctoral fellow in the Saez-Rodriguez group at EMBL-EBI,
will present work on a Human Thymus Ageing Cell Atlas that defines a spatially
resolved model of thymic involution. The thymus plays a central role in adaptive
immune development, and its decline with age has direct implications for immune
function. Kedlian will also address current known links between thymic involution,
immune ageing and ME - bringing single-cell and spatial transcriptomics
approaches to bear on questions that matter directly to this audience.
Together, the three presentations reflect a field beginning to harness the full power of computational and
systems-level science in the pursuit of ME's mechanisms.
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Session 2: A Post-Genomics Approach to ME
The sequencing of the human genome was a beginning, not an end. Post-genomics
research takes what that sequencing revealed and asks the harder questions - how
are genes expressed, how is expression regulated, and how do molecular processes
go wrong in disease? For ME, a condition whose biological mechanisms remain
incompletely understood, these tools are proving increasingly powerful.
The session is moderated by Dr Elisa Oltra, professor of Cell and Molecular Biology
at the Universidad Católica de Valencia and a member of the EMERG. Dr Oltra has investigated the
molecular basis of ME, identifying irregularities in RNAseL expression and miRNA profile changes in
patients - work that places her at the intersection of molecular biology and ME research.
Andrew Grimson, Professor of Molecular Biology and Genetics at Cornell University
and Associate Director of the Cornell NIH ME Research Center, will present on T cell
dysregulation in ME. His laboratory has used single-cell RNA sequencing to examine
circulating immune cells in ME patients, finding evidence of T cell exhaustion - a
state in which immune cells become progressively less effective, associated with
chronic immune stimulation or long-term pathogen exposure. Published in the
Proceedings of the National Academy of Sciences, the findings also identified
changes in platelet gene expression during post-exertional malaise. The same
pattern of T cell exhaustion has been observed in long COVID.
Dr Vilma Lammi of the Institute for Molecular Medicine Finland (FIMM), University
of Helsinki, coordinates the international Long COVID Host Genetics Initiative. Her
work spans the genetics of both long COVID and ME, including a genome-wide
association study of long COVID published in Nature Genetics in 2025. At BRMEC15
she will present findings on common genetic variants across long COVID and ME
from large-scale international cohorts - evidence that the two conditions may share
underlying biological architecture.
Dr Elizabeth Worthey, Director of the Center for Computational Genomics and Data Science at the
University of Alabama at Birmingham, brings a precision medicine perspective. A
pioneer in clinical genomics, she was part of the team that in 2009 performed the
first successful use of genomic sequencing to change a patient's treatment. At
BRMEC15 she will present on actionable molecular stratification of ME using an N-of1
precision medicine approach - work with direct implications for how patients might
one day be diagnosed and treated according to their individual molecular profiles.
The three presentations reflect a field moving from description towards mechanism - and from
mechanism towards the prospect of targeted intervention.
Session 3: Chronic Infection Aetiology
The role of chronic or persistent infection in ME has been debated for decades, but the tools to
investigate it rigorously are now available. Viral persistence in tissue reservoirs, myeloid reprogramming,
intracellular pathogens and the long-term consequences of immune activation following infection are all
areas where ME research is now making meaningful progress. The parallels with long COVID - where spike
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May 2026
protein persistence and sustained immune dysregulation have been documented - have added new
impetus to this work and new frameworks through which to interpret it.
The session is moderated by Dr Friðbjörn Sigurðsson, Akureyri Hospital, Iceland /
EMERG and a leading figure in ME clinical services in Iceland. He was instrumental in
founding the Akureyri Clinic - a nationally designated specialist service for ME and long
COVID patients opened in 2024 - and has long championed awareness of the 1948-49
Akureyri Disease epidemic, one of the earliest and best-documented outbreaks of
what would later be recognised as ME.
Fernando Real of the Institut Pasteur de Lille will present on viral persistence in tissue
reservoirs and myeloid reprogramming. His work examines how macrophages and
other myeloid cells can act as long-term hosts for persistent intracellular pathogens,
and what this means for understanding chronic infection in ME.
Professor Greg Towers of Queen Mary University of London brings a molecular
virology perspective. His research on host-virus interactions - including innate
immune responses to HIV and SARS-CoV-2 - informs his BRMEC15 presentation
on inflammatory responses to viral infection and how they might drive post-viral
syndromes.
Professor Maureen Hanson of Cornell University has been one of the most
productive ME researchers of the past two decades, with work spanning the
microbiome, immune cell gene expression and exercise challenge studies. At
BRMEC15 she will present on the search for chronic infection in ME.
Professor Nancy Klimas of Nova Southeastern University is one of the world's foremost
clinician-researchers in ME and long COVID. Her landmark immunological work includes
establishing natural killer cell dysfunction as a feature of ME. At BRMEC15 she will
present on spike protein antigen persistence and long COVID from a monoclonal
antibody perspective - work that speaks directly to the question of what sustains illness
following acute infection.
Professor Branislav Milovanović of the Institute for Cardiovascular Diseases Dedinje,
Belgrade, and a member of EMERG, will present findings on intracellular infection with
coxiella burnetii and bartonella in ME patients, and the relationship between these
infections and dysautonomia - connecting the chronic infection hypothesis directly to
one of ME's most consistent c linical features
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May 2026
Session 4: Nervous System and Neuroinflammation
Moderated by Dr Jon Brooks, University of Liverpool, UK
Neurological symptoms are among the most disabling features of ME - cognitive
impairment, unrefreshing sleep, sensory sensitivity and autonomic dysfunction are
reported consistently across patient populations worldwide. Yet the biological
mechanisms underlying these symptoms remain poorly understood. Neuroimaging,
neuro-PET and postmortem brain research are now beginning to reveal structural and
inflammatory changes in the central nervous system in ME and related post-viral
conditions, offering the prospect of both biological explanation and, in time, therapeutic targets.
The session is moderated by Dr Jon Brooks, Senior Lecturer at the University of Liverpool, whose research
uses MRI-based neuroimaging techniques to study changes in the central nervous system in chronic pain
and related conditions, including ME.
Associate Professor Gwenaëlle Douaud of the Wellcome Centre for Integrative Neuroimaging at the
University of Oxford brings one of the most powerful datasets in neuroscience to
bear on post-viral illness. As a core member of the UK Biobank imaging team, she has
contributed to the analysis of brain scans from 100,000 participants. She led the
landmark 2022 Nature study demonstrating that SARS-CoV-2 infection is associated
with measurable changes in brain structure - including greater reduction in grey
matter thickness in the orbitofrontal cortex and parahippocampal gyrus - findings
with direct relevance to understanding the neurological basis of ME and long COVID.
Her BRMEC15 presentation title is to be confirmed.
Dr Denise Visser of Amsterdam UMC will present Neuro-PET data from postCOVID
patients. Her imaging work has demonstrated significant
neuroinflammation throughout the brain in patients with long-term post-COVID
symptoms - providing some of the first direct in vivo evidence of widespread
brain inflammation in living patients following COVID-19 infection. The parallels
with ME are clear and the implications significant.
Felipe Correa da Silva of the Netherlands Institute for
Neuroscience works in postmortem brain research and neuroimmunology. At
BRMEC15 he will present on microglial profiling in ME - examining the brain's resident
immune cells directly in postmortem tissue from ME patients. This work offers a level
of resolution into neuroinflammation in ME that has rarely been achieved before, and
may help explain the cognitive and neurological symptoms that define the disease for
so many patients.
Session 5: Immune System - Primary and Secondary
Immune dysfunction is one of the most consistently reported biological features of ME. Abnormalities
have been identified across both innate and adaptive immune compartments - from natural killer cell
dysfunction and T cell exhaustion to ion channel dysregulation and aberrant cytokine signalling. Whether
these represent primary drivers of the disease or secondary consequences of another underlying process
remains a central question in the field. This session brings together researchers working at the forefront
of ME and post-viral immunology to examine the evidence from multiple angles.
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The session is moderated by Associate Professor Eva Untersmayr-Elsenhuber, a
specialist in immunology and head of the Gastrointestinal Immunology research
group at the Medical University of Vienna. A member of EMERG, her extensive
research background in food allergy, gastrointestinal immunology and
pathophysiology brings a broad immunological perspective to the session.
Professor Leo Joosten of Radboud University Medical Centre in Nijmegen
focuses on host defence mechanisms and the chronic inflammation
that can follow pathogen exposure. His work on innate immune
receptors, the inflammasome and Lyme disease pathogenesis is
directly relevant to the question of how an initial infection can set in
motion a sustained immune response. At BRMEC15 he will present
on innate immunity and post-infectious immune dysregulation, and
the insights this offers for ME research.
Professor Sonya Marshall-Gradisnik, Director of the National Centre for
Neuroimmunology and Emerging Diseases (NCNED) at Griffith University,
Australia, is one of the world's leading ME researchers. Her laboratory has
pioneered work on natural killer cell dysfunction and calcium ion channel
dysregulation in ME, and has demonstrated significant overlaps between ME and
long COVID in immune cell dysfunction and symptom presentation. At BRMEC15
she will present on ion channels, calcium signalling and inner cell function - work
that sits at the intersection of immunology and cell biology.
Marcus Buggert, Associate Professor Marcus Buggert, Center for Infectious
Medicine, Karolinska Institutet studies human adaptive immunity to viral
infections across blood and tissue compartments. His research on antigen-specific
T cells and tissue-based immunology has informed understanding of how immune
responses persist and become dysfunctional following infection.
At BRMEC15 he will present on tissue-specific immune dysregulation in long
COVID - findings with clear implications for ME.
Session 6: Metabolism
Metabolic dysfunction is increasingly recognised as a central feature of ME. Studies have identified
abnormalities in energy metabolism, mitochondrial function, fatty acid oxidation and cellular oxygen
utilisation in ME patients. These findings point towards a disease in which the body's ability to generate
and use energy at the cellular level is fundamentally compromised - a hypothesis that may explain the
post-exertional malaise that is the hallmark symptom of ME, and which distinguishes it from other
conditions characterised by fatigue.
Moderated by Associate Professor Rikke Katrine Jentoft Olsen, Aarhus University, Denmark / EMERG
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Rikke Katrine Jentoft Olsen’group has a longstanding focus on inborn errors of
mitochondrial metabolism and fatty acid oxidation disorders. In recent years she
has extended this work to examine the role mitochondria may play in ME -
bringing deep expertise in mitochondrial biology to a question that is now central
to the field.
Professor Edmund Kunji of the MRC Mitochondrial Biology
Unit, University of Cambridge, studies mitochondrial carrier proteins and their role in
transporting metabolites, cofactors and ions across the inner mitochondrial
membrane. His work on how these carriers regulate the flow of energy substrates is
directly relevant to whether impaired mitochondrial transport underlies the energy
metabolism failures observed in ME. At BRMEC15 he will present on the role of
transport in mitochondrial energy metabolism.
Dr Robert Phair of Integrative Bioinformatics Inc, USA, is a
systems biologist with over 35 years of experience in kinetic modelling of complex
biological systems. He has developed the Itaconate Shunt Hypothesis for ME
pathogenesis - proposing that a metabolic switch involving the itaconate shunt,
normally part of the innate immune response, is inappropriately activated in ME,
diverting energy metabolism away from normal mitochondrial function. At
BRMEC15 he will present model predictions and experimental tests of this
hypothesis.
Anouk Slaghekke of Vrije Universiteit Amsterdam is a PhD candidate whose research focuses on skeletal
muscle adaptations in ME - peripheral muscle oxygenation, muscle structure and
function, and post-exertional malaise. Her work on microvascular dysfunction
and basal membrane thickening in skeletal muscle connects the metabolic
abnormalities of ME directly to structural changes in tissue, offering a
mechanistic account of why physical exertion produces such severe and
prolonged consequences for ME patients. At BRMEC15 she will present on
failures in the peripheral oxygen transport cascade - microvascular and
mitochondrial dysregulation in long COVID and ME.
Session 7: Keynote
Professor Sarah Teichmann of the University of Cambridge is one of the
world's leading computational biologists and a pioneer of single-cell
genomics. As a founder of the Human Cell Atlas - the landmark
international project to map every cell type in the human body - her work
has transformed the way biology understands cellular diversity, tissue
organisation and immune function. At BRMEC15 she will present on
mapping the human body one cell at a time, bringing to the colloquium a
perspective that spans the full breadth of modern biological science. Her
presence as keynote speaker reflects the ambition of BRMEC15 to situate
ME research within the wider frontier of biomedical discovery.
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Session 8: Biomarker Discovery and Emerging Research Approaches
One of the most pressing needs in ME research is the development of objective,
validated biomarkers - measurable biological indicators that can confirm diagnosis,
stratify patients and track response to treatment. Progress in this area is now
accelerating. But this session goes beyond biomarkers in the conventional sense,
encompassing emerging research directions and novel therapeutic hypotheses
that may shape the field in the years ahead.
The session is moderated by Professor Jonas Bergquist, Full Chair in Analytical Chemistry and
Neurochemistry at Uppsala University in Sweden, with a background spanning clinical neuroscience,
analytical chemistry and ME research across more than two decades.
Dr Jesper Mehlsen, co-chair of EMERG and a specialist in autonomic nervous
system dysfunction with over 35 years of clinical and research experience, will
present on objective tools for diagnosing autonomic dysfunction in ME - the
tilt-test, Valsalva Manoeuvre, Heart Rate Variability and the COMPASS-31
questionnaire. These approaches offer a means of characterising the
autonomic abnormalities consistently reported in ME patients and may
contribute to validated diagnostic criteria.
Professor Ronald W. Davis, Director of the Stanford Genome Technology
Center and a world-recognised figure in the development of genomic and
biotechnological methodologies, has in recent years dedicated substantial
effort to ME research. His team have developed novel nanotechnology-based
diagnostic tools, including a nanoelectronics assay that has attracted
considerable international attention as a potential objective test for the
disease. His presentation addresses oxidative stress in ME/CFS and Long
COVID - a domain of growing significance as researchers seek to characterise
the metabolic and mitochondrial disturbances that may underlie the illness -
and reflects the session's ambition to pursue biomarker discovery through the
most advanced technological means available.
Dr Alexandre Akoulitchev of Oxford BioDynamics and Professor Dmitry Pshezhetskiy of the University of
East Anglia will present on a potentially transformative
development: the application of EpiSwitch 3D genomic profiling to
ME. Their collaborative work, published in the Journal of
Translational Medicine in 2025, identified a unique and
reproducible pattern of three-dimensional chromatin architecture
in ME patients absent in healthy controls, achieving diagnostic
accuracy of 96% in an initial cohort - offering the prospect of the
first reliable blood-based diagnostic test for the disease.
The Carding Group at the Quadram Institute will present on bacterial extracellular vesicle research and
the pathways and mediators of the gut-microbiome-brain axis - exploring how signals from gut microbes
transmitted via extracellular vesicles may influence brain function and immune responses in ME.
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@JOURNAL OF IIMER
May 2026
Dr Wenzhong Xiao of Harvard Medical School will present on a mouse model for
reversing post-exertional malaise. If translatable to humans, this work could open a
direct path towards therapeutic intervention for one of ME's most debilitating and
defining features.
Dr Steve Gardner, CEO of PrecisionLife, will address the question of GLP-1 receptor
agonists for ME and long COVID - drugs that have transformed treatment of obesity
and type 2 diabetes - examining the evidence, the hope and the potential risks of
applying them to post-viral conditions.
IIMEC18 International ME Conference Day – Colloquium Day 3
The day opens with an address from Dr Hans Kluge, WHO Regional Director for Europe.
As members of the European ME Alliance we have been working with our European
partners on several campaigns relating to WHO Europe initiatives.
This will be the second time that WHO has contributed a message to the events.
BRMEC15 Session 9: Therapeutics
The Therapeutics session marks a pivotal point in the three-day programme - moving from the science of
mechanisms towards the science of intervention. After two days of presentations on the biological
underpinnings of ME, this session addresses what can now be done: clinical trial infrastructure, cognitive
rehabilitation, mitochondrial intervention, and the use of digital and wearable technology to capture the
complexity of ME in research and trials.
Moderated by Professor Andrew Wilson, University of East Anglia, UK
The final day of BRMEC15 merges with the 18th International ME Conference
(IIMEC18), bringing researchers, clinicians and patients together for the first time in
the programme.
Professor Wilson also presents in his own right, on the development of a platform for
clinical trials in ME - infrastructure that is essential if the growing body of mechanistic
findings in ME research is to be translated into tested and validated treatments.
Dr Vicky Whittemore is a Programme Director in the Division of Neuroscience at the
National Institutes of Health, where she has played a central role in coordinating and
advancing the NIH's investment in ME research. With a background spanning
epilepsy, neurological disorders and translational neuroscience, she has served on
key advisory and working groups shaping the direction of ME research at a national
and international level, including the NIH P2P CFS Committee and the National
Academy of Medicine's ME/CFS case definition working group. Her contribution to
this session reflects the importance of sustained institutional commitment to the
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9JOURNAL OF IIMER
May 2026
field, and the role of collaborative international frameworks in moving ME research forward.
Professor Gitendra Uswatte of the University of Alabama at Birmingham will
present preliminary findings from cognitive rehabilitation trials in adults with postviral
syndromes. Brain fog is one of the most common and disabling symptoms
reported by ME patients, yet it has received comparatively little attention as a
target for intervention. His work explores whether targeted rehabilitation
approaches can produce measurable improvements in cognitive function in this
population.
Associate Professor Rikke Katrine Jentoft Olsen of Aarhus University, who also
moderates the Metabolism session at BRMEC15, will present on a randomised
controlled trial examining hypoxia-induced mitochondrial stress-signalling in ME.
This represents one of the most direct attempts yet to test and potentially intervene in
the metabolic dysfunction that may lie at the heart of ME pathogenesis.
Dr Caroline Dalton of Sheffield Hallam University will present on harnessing
wearable data in ME research and trials - addressing both the potential of digital
tools to capture the complexity of ME in ways that conventional clinical
assessments cannot, and their role in supporting more rigorous and sensitive
outcome measurement in clinical trials.
The remainder of the IIMEC18 conference day will have the following presentations -
Eva Untersmayr-Elsenhuber - Associate Professor of Pathophysiology and Allergy
Research at the Medical University of Vienna, and a member of EMERG, presents
on emerging research for the discovery of ME mechanisms, with a focus on the
DISCOVER-ME project. Her background spans immunology, gastrointestinal
immunology, and allergy research, and she leads the Department of
Pathophysiology and Allergy's gastrointestinal immunology group. As a lead and
co-investigator in the DISCOVER-ME consortium, she brings expertise in immune
mechanisms to the pan-European effort to identify biological markers and disease
subtypes in ME.
Douglas D. Fraser - Professor and Clinician Scientist in Paediatric Critical Care at
Western University in London, Ontario, presents on a global platform trial of
repurposed drugs for long COVID. Director of the Translational Research Centre
- a human tissue biobank with over fifteen years of operation - Professor Fraser
leads two international multicentred long COVID research programmes
examining sub-phenotypes and outcomes, and has extensive experience in
profiling post-COVID patients for immune and proteomic changes.
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May 2026
Rowan Gardner, co-founder of PrecisionLife, a UK-based precision medicine company,
brings over thirty years of experience applying computational methods to life science
and patient data. Her work at PrecisionLife focuses on identifying novel disease
mechanisms and therapeutic targets through advanced combinatorial analytics applied
to complex disease datasets, including ME. In this session she examines new mechanistic
insights into ME from large-scale genomic analysis, and considers what emerging
findings may offer for future research directions.
Ana Palacio - University of Miami, presents follow-up findings from the Covid-UPP trial,
examining outcomes in post-COVID patients and contributing to the growing evidence
base on cardiovascular and systemic effects of long COVID and related post-viral
conditions.
Leo Tamariz - University of Miami, presents a comparison of
cardiovascular symptoms across ME, long COVID, and Gulf War Syndrome (GWS)
cohorts. This cross-condition analysis contributes to understanding the shared and
distinct physiological features of post-viral and post-toxic multi-symptom illnesses, with
implications for diagnosis and clinical management.
Mari Gamme Sollie and Trine Alm Holterbakken - Røysumtunet,
Norway, present on specialised care for seriously and very seriously ill
people with ME. Røysumtunet is a Norwegian facility with particular
expertise in managing severely affected ME patients, and this
presentation addresses one of the most underserved areas in ME
clinical practice - the provision of appropriate, safe, and informed care
for those who are housebound or bedbound.
Friðbjörn Sigurðsson - Akureyri Hospital, Iceland, and EMERG member, presents on
clinical approaches to treatment in ME. Drawing on clinical experience from Iceland's
national hospital in Akureyri, this presentation addresses the practical management
of ME patients and contributes to EMERG's work on developing harmonised
European clinical protocols.
Per Julin - Karolinska Universitetssjukhuset, Sweden, and
EMERG member, presents on the Karolinska Policlinic for Post-infectious Diseases,
covering both its clinical work and associated research programme. The Karolinska
clinic represents one of Europe's dedicated post-infectious disease centres, and this
presentation describes its approach to the assessment and management of ME and
related conditions alongside the research it generates.
Invest in ME Research
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