Severe posterior hypometabolism but normal perfusion in a patient with CFS/ME

Abstract:

Chronic fatigue syndrome/myalgic encephalitis (CFS/ME) is a complex clinical condition defined by prolonged severe fatigue without medical or psychiatric causes, and by a subset of symptoms that mostly includes arthromyalgias, cognitive impairment, sleeping troubles, and unusual headaches [1]. Previous FDG-PET studies showed unspecific patterns of hypometabolism in the frontal and cingulate cortex in half of CFS patients compared to healthy controls [2].

We present 18F-FDG PET/MRI findings in a 21-year-old woman who fulfilled the criteria of CFS with a Fukuda score of 4. PET images (a) show severe and extensive hypometabolism in the posterior cortical regions (precuneus, parietal, temporal, and occipital), amygdalo-hippocampal complexes, and cerebellum. No structural abnormalities were found on T1 MPRAGE (b) or T2 FLAIR (c) MRI sequences. Interestingly, cerebral blood flow evaluated with Gadolinium first-pass method (d) was not decreased in these regions.

This peculiar pattern of hypometabolism was recently described in a large series of patients with aluminium-induced macrophagic myofasciitis (MMF) followed in our reference center [3]. However, the present patient had negative muscular biopsies for MMF. Neuropsychological testing showed severe impairment of short-term memory (immediate and working memory) in visual modality, and weakness of visual selective attention and executive functions, which are concordant with the pattern of hypometabolism. Finally, perfusion-metabolism uncoupling suggests that posterior hypometabolism may not be related to neuronal loss such as in degenerative diseases [4], but rather to an inflammatory or immunological process [5]. Further studies are warranted to investigate metabolism and perfusion using simultaneous PET/MRI in larger groups of patients with CFS/ME.

Source: S. Sahbai & P. Kauv & M. Abrivard & P. Blanc-Durand & M. Aoun-Sebati & B. Emsen & A. Luciani & J. Hodel & F-J. Authier & E. Itti. Severe posterior hypometabolism but normal perfusion in a patient with chronic fatigue syndrome/myalgic encephalomyelitis revealed by PET/MRI. Eur J Nucl Med Mol Imaging. 2018 Dec 14. doi: 10.1007/s00259-018-4229-3. [Epub ahead of print] https://forums.phoenixrising.me/index.php?threads/severe-posterior-hypometabolism-but-normal-perfusion-in-a-patient-with-cfs-me.62543/

Neurocognitive functioning in chronic fatigue syndrome

Abstract:

Although substantial research has been conducted on chronic fatigue syndrome (CFS) over the past decade, the syndrome remains poorly understood. The most recent case definition describes CFS as being characterized both by disabling fatigue and by subjective reports of difficulty with concentration and “short-term” memory. However, research into the neurocognitive and psychological functioning of individuals with CFS has provided mixed objective results. The current paper reviews studies that have examined the neurocognitive and/or psychological functioning of individuals with CFS. Changes in research design and instruments employed to study individuals with CFS are suggested.

 

Source: DiPino RK, Kane RL. Neurocognitive functioning in chronic fatigue syndrome. Neuropsychol Rev. 1996 Mar;6(1):47-60. http://www.ncbi.nlm.nih.gov/pubmed/9144668

 

Attention and short-term memory in chronic fatigue syndrome patients: an event-related potential analysis

Abstract:

We recorded event-related brain potentials (ERPs) from 13 patients with chronic fatigue syndrome (CFS) and 13 matched normal controls. To assess attentional and memory deficits in CFS patients, we used a short-term memory task in which events occurred in different spatial locations and the patients made a rapid-response (RT) when a letter in a relevant location matched a letter in the prememorized set (Attention paradigm).

Time-on-task effects on the ERP and behavioral measures were assessed over the 2 1/4-hour duration of this task. Both groups also performed a visual Oddball paradigm, with an RT, before and after the Attention paradigm. The patients’ RTs were much more variable and, in nine of 13 cases, slower than the mean RT of the controls in both paradigms.

The patients’ memory performance was not significantly different from that of the controls and there were no group differences in the overall amplitude, latency, or scalp distribution of the N1, P2, N2, or P300 components of the ERP in either paradigm. The ERP and performance data from both paradigms suggest that perceptual, attentional, and short-term memory processes were unaffected in CFS patients and that the differences were limited to response-related processes.

 

Source: Scheffers MK, Johnson R Jr, Grafman J, Dale JK, Straus SE. Attention and short-term memory in chronic fatigue syndrome patients: an event-related potential analysis. Neurology. 1992 Sep;42(9):1667-75. http://www.ncbi.nlm.nih.gov/pubmed/1513453

 

Neuropsychological and psychiatric abnormalities in myalgic encephalomyelitis: a preliminary report

Abstract:

Ten patients attending one general medical hospital clinic who fulfilled operational criteria for the diagnosis of myalgic encephalomyelitis (ME) and with a history longer than three months, underwent a series of standardized neuropsychological and psychiatric tests. Nine were able to complete the tests and were individually matched with a normal control group for age, sex, educational background and premorbid intelligence. The ME subjects showed inferior performance to the controls on two tests of verbal memory. Their personality scores displayed less extraversion and less psychoticism. This is the first report of objective neuropsychological abnormalities in patients with ME, suggesting a discrete deterioration of short-term memory. The findings may also suggest a concurrent psychiatric component of the condition, but the direction of causality remains to be clarified.

 

Source: Riccio M, Thompson C, Wilson B, Morgan DJ, Lant AF. Neuropsychological and psychiatric abnormalities in myalgic encephalomyelitis: a preliminary report. Br J Clin Psychol. 1992 Feb;31 ( Pt 1):111-20. http://www.ncbi.nlm.nih.gov/pubmed/1559114