TERMINOLOGY
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The term BENIGN MYALGIC ENCEPHALOMYELITIS was first introduced in the
UK in 1956 by a former Chief Medical Officer (Sir Donald Acheson) and not
by Dr Melvin Ramsay as is sometimes claimed. The word
"benign" was used because it was thought at the time that the
disorder was not fatal (as poliomyelitis could be, with which it had some
similarity), but it was quickly realised by clinicians that ME was not a
"benign" condition, as it has such high morbidity (ie. such a lot
of suffering and ill-health), so by 1988 clinicians had stopped using the
word "benign" and referred to it as ME, the first to do so being
Dr Ramsay. However, the ICD still uses the term "benign" in
its classification.
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MYO relates to muscle
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MYOSITIS = inflammation of muscle
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MYALGIA = pain in muscles (pain that is called
"myalgic")
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MYOPATHY = any disease or disorder of muscle
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MYEL (or MYELO) relates to the spinal cord, the main nerve in the
body
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MYELITIS = inflammation of the spinal cord (N.B.
Not to be confused with the other meaning of myelitis, which = inflammation
of the bone marrow, as in osteomyelitis)
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MYELIN SHEATH = a layer of fatty white material that
surrounds and insulates nerve fibres
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DEMYELINATION = the loss of this protective insulation
round nerve fibres, as seen in multiple sclerosis and sometimes also in ME
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ENCEPHALON = the brain
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ENCEPHALO = relating to the brain
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"ITIS" on the end of a word = inflammation
(e.g. hepatitis = inflammation of the liver)
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SO . . .
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ENCEPHALOMYELITIS = inflammation of the brain and spinal
cord
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BENIGN MYALGIC ENCEPHALOMYELITIS therefore means a non-fatal
disorder (inflammation) of the brain and spinal cord, with pain in the
muscle
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ENCEPHALOPATHY = any non-inflammatory disorder
affecting the brain
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Despite the claims of some psychiatrists, it is not true that there is
no evidence of inflammation of the brain and spinal cord in ME; there is,
but these psychiatrists ignore or deny that evidence. For example . .
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1988. In conjunction with the University of Pittsburgh, the US
NIAID held a large research workshop called "Consideration of the
Design Studies of Chronic Fatigue Syndrome". There were
participants from the Centres for Disease Control and from the National
Institutes of Health. One of the presentations was by Dr Sandra
Daugherty, who reported that MRI scans on patients demonstrated abnormalities
consistent with demyelination and cerebral oedema in 57% of patients
studied. (It was at this conference that it was recommended that the
term "CFIDS" be used instead of the term "CFS" on the
basis of the immune dysfunction that had been observed in the disorder).
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1989. Detection of Viral-Related Sequences in CFS Patients
using Polymerase Chain Reaction; W John Martin; Nightingale Research
Foundation 1989: 1-5.
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1990. Chronic Fatigue Syndrome and the Psychiatrist; SE
Abbey & PE Garfinkel; Canadian Journal of Psychiatry 1990:35:7:625-626.
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1992. A Chronic Illness Characterised by Fatigue, Neurologic
and Immunologic Disorders, and Active Human Herpesvirus Type 6 Infection;
D Buchwald, PR Cheney, R Gallo, AL Komaroff et al; Annals of
Internal Medicine 992:116:2:103. This paper states "Magnetic
resonance scans of the brain showed punctate, subcortical areas of high
signal intensity consistent with oedema or demyelination in 78% of
patients".
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1994. Detection of Intracranial Abnormalities in Patients with
Chronic Fatigue Syndrome: Comparison of MR Imaging and SPECT; RB
Schawrtz & BM Garada; American Journal of Roentgenology
1994:162:935-941.
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1995. Pathophysiology of a Central Cause of Post-Polio Fatigue;
Richard Bruno et al; Annals of the New York Academy of Sciences
1995:753:257-275.
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1997. A 56-year old woman with chronic fatigue syndrome;
Anthony J Komaroff; JAMA 1997:278:14:1179-1184.
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It is true that there is no evidence of inflammation of the brain or
spinal cord in states of chronic fatigue or "tiredness".
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It is also true that neither the 1991 (Oxford) criteria nor the 1994
(CDC) criteria select those with ME, as they both expressly include those
with somatisation disorders and they expressly exclude those with any
physical signs of disease (as is the case in ME), so by definition,
patients with signs of neurological disease have been excluded from study.
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It is also true that Professor Simon Wessely and his colleagues use the
terms "fatigue", "chronic fatigue", "the chronic
fatigue syndrome (CFS)" and "myalgic encephalomyelitis (ME)"
as synonymous. Such obfuscation has greatly hindered research, as
pointed out in the 1994 Report of the National Task Force on Chronic Fatigue
Syndrome (CFS), Post-Viral Fatigue Syndrome (PVFS) and Myalgic
Encephalomyelitis (ME), published by Westcare, Bristol and supported by the
UK Department of Health, which stated . . .
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"
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Chronic fatigue syndromes remain poorly understood. Progress in
understanding them is hampered by -
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the use by researchers of heterogeneous study groups
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the use of study groups which have been selected using different
definitions of CFS
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the invalid comparisons of contradictory research findings stemming
from the above "
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</TD< TR>
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The Report names psychiatrists Dr Simon Wessely, Dr Peter White and Dr
Michael Sharpe and acknowledged their help, but then makes the point that
"people who gave their help are not necessarily in agreement with the
opinions expressed" (page 87). It was said to be because those
psychiatrists strongly disagreed with the findings of the 1994 Westcare
Report that in 1996 they produced their own report (the Report of the Joint
Royal Colleges on CFS (CR54), which was internationally recognised as being
biased and seriously flawed).
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CLASSIFICATION
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The WHO was founded in 1948.
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The International Classification of Diseases (ICD) comes in two
volumes. Volume I is the Tabular List and is a list of codes plus the
name of the condition which goes with that code. Volume II is the
Code Index, which alphabetically lists all the phrases and names of
conditions commonly used for a condition, together with the appropriate
code.
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The Tabular List (Volume I) does not list everything which is in the
Code Index (Volume II).
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Benign Myalgic Encephalomyelitis (ME) has been classified in the
International Classification of Diseases (ICD) as a neurological disorder
since 1969, when it was included in ICD-8 at Volume I: code 323: page 158
and in Volume II (the Code Index) on page 173. ICD-8 was approved in
1965 and published in 1969.
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