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Query: UMLS:C0015674 (
chronic fatigue syndrome
)
2,978
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
This study investigated the cell surface expression of
CD11b
(Mo 1, Mac-1, CR 3) by neutrophils (PMNs) from human crevicular fluid (CF-PMNs).
CD11b
expression on CF-PMNs was compared, using flow cytometry, to that on peripheral blood PMNs (PB-PMNs) isolated simultaneously from the same subjects.
CD11b
expression by CF-PMNs was also compared to that on PB-PMNs stimulated with formylmethionylleucylphenylalanine (fMLP) or crevicular fluid supernatant (cell-free portion of CF diluted with buffer) (
CFS
). Crevicular PMNs consistently expressed more
CD11b
than unstimulated PB-PMNs (p less than 0.001). The level of
CD11b
expressed on these CF-PMNs was significantly greater than that expressed by PB-PMNs stimulated with 10(-8) M fMLP (p less than 0.05). The level of
CD11b
surface expression on CF-PMNs was not statistically different from that expressed on PB-PMNs stimulated with
CFS
or 10(-6) M fMLP. However,
CFS
significantly stimulated upregulation of surface
CD11b
expression on PB-PMNs relative to that achieved with 10(-8) M fMLP (0.01 less than p less than or equal to 0.025). Thus it is concluded that CF-PMNs express a high level of
CD11b
and
CFS
can upregulate
CD11b
expression on PB-PMNs to a level that is at least as great as that achieved with 10(-8) M fMLP.
...
PMID:CD11b expression on neutrophils in human crevicular fluid collected from clinically healthy gingivae. 167 90
Between January 1991 and January 1993, 265 patients who fulfilled the CDC criteria of the working case definition of
Chronic Fatigue Syndrome
(
CFS
) have been observed at our Institution and submitted for clinical and laboratory evaluation. One hundred and sixty-three patients were females and 102 males, the median age was 35 years (range 4-55 years); all patients reported profound and prolonged fatigue, lasting for a median of 3 years (range 6 months-10 years), preceded or accompanied at appearance by fever in 185 cases, and neuropsychologic problems including inability to concentrate, difficulty in thinking, confusion, irritability, forgetfulness, and depression. The fatigue was so severe that it required 102 patients to stop their working activities for a period of time ranging from 3 months to 2 years (range 7 months). In 40 consecutive patients a comprehensive immunologic testing by single and two-colour flow cytometry was performed and results compared with a group of 35 healthy, age- and sex-matched controls. Whilst no significant differences were found in the absolute numbers of circulating total T cells (CD3+) and of total helper/inducer (CD4+) or suppressor/cytotoxic (CD8+) T cells, an evident reduction in CD3-/CD16+ and CD57+/CD56+ NK lymphocytes along with an expansion of the CD8+/CD56+ and CD16-/CD56+ NK subsets, were found in the
CFS
group. In addition, CD56+ NK cells from
CFS
subjects were found to express an increased amount of cell adhesion molecules (
CD11b
, CD11c, CD54) and activation antigens (CD38). Both the percentage and absolute numbers of CD4+ T cells bearing the CD45RA antigen appeared significantly reduced in
CFS
patients, and CD4+ T lymphocytes from
CFS
subjects displayed an increased expression of the intercellular adhesion molecule-1 (ICAM-1/CD54). Finally, the total numbers of circulating (CD19+) B lymphocytes, were significantly higher in
CFS
cases than in controls, and in 11 out of 30
CFS
patients the increase in circulating B cells was sustained by the expansion of the CD5+/CD19+ subset of B lymphocytes. We conclude that
CFS
is a syndrome not previously described in Italy, with already known clinical characteristics and appears to be associated with several immunologic abnormalities, including those reported previously in cohort of patients from different countries. We also show for the first time that CD56- NK cell subsets from
CFS
patients display an abnormally increased expression of cell adhesion molecules and activation markers.
...
PMID:Immunological abnormalities in patients with chronic fatigue syndrome. 799 49
Several aspects of cellular immunity in patients with clinically defined
chronic fatigue syndrome
(
CFS
) were evaluated and compared with those in healthy individuals. Flow cytometric analyses revealed normal expression of total T (CD3+), B (CD19+), and NK (natural killer) (CD16+, CD56+) markers on the surface of peripheral blood mononuclear cells (PMC) from patients with
CFS
. However, compared with those of healthy individuals, patients' CD8+ T cells expressed reduced levels of
CD11b
and expressed the activation markers CD38 and HLA-DR at elevated levels. In many of the individuals in whom expression of
CD11b
was reduced the expression of CD28 was increased. These findings indicate expansion of a population of activated CD8+ cytotoxic T lymphocytes. A marked decrease in NK cell activity was found in almost all patients with
CFS
, as compared with that in healthy individuals. No substantial abnormalities in monocyte activity or T cell proliferation were observed. The results of this study suggest that immune cell phenotype changes and NK cell dysfunction are common manifestations of
CFS
.
...
PMID:Immunologic abnormalities associated with chronic fatigue syndrome. 814 41
Whether immunologic abnormalities correlate with fatigue severity and functional impairment in
chronic fatigue syndrome
(
CFS
) was investigated. Blood mononuclear cells were immunophenotyped and circulating ex vivo-produced cytokines were measured in 76
CFS
patients and 69 healthy matched controls. Expression of
CD11b
on CD8 cells was significantly decreased in
CFS
patients. However, the previously reported increased expression of CD38 and HLA-DR was not confirmed. There was no obvious difference in apoptosis in leukocyte cultures, circulating cytokines, and ex vivo production of interleukin (IL)-1 alpha and IL-1 receptor antagonist. Endotoxin-stimulated ex vivo production of tumor necrosis factor-alpha and IL-beta was significantly lower in
CFS
. The immunologic test results did not correlate with fatigue severity or psychologic well-being was measured by Checklist Individual Strength, Beck Depression Inventory, and Sickness Impact Profile. Thus, these immunologic tests cannot be used as diagnostic tools in individual
CFS
patients.
...
PMID:Lymphocyte subsets, apoptosis, and cytokines in patients with chronic fatigue syndrome. 856 12
The purpose of this study was to evaluate the immune dysfunction hypothesis of
chronic fatigue syndrome
(
CFS
) by comparing immunologic data from patients with
CFS
with data from patients with other fatiguing illnesses--major depression and multiple sclerosis (MS)--and with data from healthy sedentary controls. The subjects were 65 healthy sedentary controls, 71
CFS
patients (41 with no axis-I diagnosis), 23 patients with mild MS, and 21 patients with major depression. Blood was sampled and assayed for the following: (1) immunologic serologic variables--circulating immune complexes (i.e., Raji cell and C1q binding), immunoglobulins A, E, G, and M, and IgG subclasses; (2) cell surface activation markers--the proportion of CD4+ cells expressing CD45RA+ and CD45RO+ and the proportion of CD8+ cells expressing CD38+,
CD11b
-, HLA-DR+ and CD28+; and (3) natural killer (NK) total cell count as well as the proportion of lymphocytes expressing NK cell surface markers (i.e., CD3-/CD16+ and CD56+. Of the 18 variables studied, differences between
CFS
patients and controls were found only for IgG1 and IgG3. When
CFS
patients were stratified by the presence or absence of concurrent axis-I disease, it was the group with axis-I disorder that had the lowest IgG1 values-contrary to expectation. When data from patients with MS and major depression were also evaluated, the subclass deficiency was no longer significant. The one group to show evidence for immune activation (i.e., an elevated proportion of CD4+ cells expressing the CD45RA+ activation marker) was the group with mild MS. These data support neither immune dysfunction nor immune activation in
CFS
or in major depression, for the variables studied. The reductions in IgG subclasses may be an epiphenomenon of patient or control subject composition. In contrast, MS, even in the mild and early stages, as in the patients studied here, is associated with immune activation.
...
PMID:Immunologic parameters in chronic fatigue syndrome, major depression, and multiple sclerosis. 979 Apr 81
Chronic fatigue syndrome
(
CFS
) is a specific clinical condition that characterises unexplained disabling fatigue and a combination of non-specific accompanying symptoms for at least 6 months, in the absence of a medical diagnosis that would otherwise explain the clinical presentation. Other common symptoms include headaches, myalgia, arthralgia, and post-exertional malaise; cognitive difficulties, with impaired memory and concentration; unrefreshing sleep; and mood changes. Similar disorders have been described for at least two centuries and have been differently named neurasthenia, post-viral fatigue,
myalgic encephalomyelitis
and chronic mononucleosis. Recent longitudinal studies suggest that some people affected by
chronic fatigue syndrome
improve with time but that most remain functionally impaired for several years. The estimated worldwide prevalence of
CFS
is 0.4-1% and it affects over 800,000 people in the United States and approximately 240,000 patients in the UK. No physical examination signs are specific to
CFS
and no diagnostic tests identify this syndrome. The pathophysiological mechanism of
CFS
is unclear. The main hypotheses include altered central nervous system functioning resulting from an abnormal immune response against a common antigen; a neuroendocrine disturbance; cognitive impairment caused by response to infection or other stimuli in sentient people. The current concept is that
CFS
pathogenesis is a multifactorial condition. Various studies have sought evidence for a disturbance in immunity in people with
CFS
. An alteration in cytokine profile, a decreased function of natural killer (NK) cells, a presence of autoantibodies and a reduced responses of T cells to mitogens and other specific antigens have been reported. The observed high level of pro-inflammatory cytokines may explain some of the manifestations such as fatigue and flu-like symptoms and influence NK activity. Abnormal activation of the T lymphocyte subsets and a decrease in antibody-dependent cell-mediated cytotoxicity have been described. An increased number of CD8+ cytotoxic T lymphocytes and CD38 and HLA-DR activation markers have been reported, and a decrease in
CD11b
expression associated with an increased expression of CD28+ T subsets has been observed. This review discusses the immunological aspects of
CFS
and offers an immunological hypothesis for the disease processes.
...
PMID:Immunological aspects of chronic fatigue syndrome. 1880 65
