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Query: UMLS:C0019693 (
HIV
)
170,526
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Microglia, brain macrophages, are thought to be the primary target of
HIV
-1 infection in the brain, because they exclusively express the CD4 antigen which is effectively used for viral entry. The expression of CD4 mRNA in cultured microglia could be detected by the reverse-PCR method. Using this and immunohistochemical staining, we found that the immunosuppressants cyclosporin A and FK506 decreased CD4 expression in cultured murine microglia without causing any significant decrease in cell viability. FK506 was more potent than cyclosporin A. Lipopolysaccharide also decreased CD4 mRNA expression in microglia. The effects of immunosuppressants and lipopolysaccharide seemed to be specific for microglia since these chemicals did not alter the CD4 expression in lymphocytes or peritoneal macrophages. These agents, if modified to pass through the blood-brain barrier, may prevent viral spread of
HIV
-1 infection in the central nervous system and the
AIDS-dementia complex
.
...
PMID:Down regulation of CD4 expression in cultured microglia by immunosuppressants and lipopolysaccharide. 128
We detected the cytokines interleukin-6 (IL-6) and granulocyte macrophage-CSF (GM-CSF) by ELISA in the CSF and serum of 30
HIV
-infected patients classified as
AIDS dementia complex
(
ADC
), and 20 subjects with other neurological diseases (OND). We have found a high incidence of detectable IL-6 and GM-CSF in the CSF of
ADC
patients compared with OND patients. No statistical differences were observed between both groups for serum IL-6 and GM-CSF levels. These results suggest an intrathecal synthesis of these cytokines and a possible involvement in the pathogenesis of
ADC
.
...
PMID:Interleukin-6 and granulocyte macrophage-CSF in the cerebrospinal fluid from HIV infected subjects with involvement of the central nervous system. 130 87
A retrospective study of the neurological problems arising in
HIV
-I seropositive patients in a single defined geographical area was undertaken. Ninety patients were referred for a neurological opinion from a total known
HIV
-I seropositive population of 436. Minor problems were frequently encountered early in the course of disease (20 at CDC stage II, 12 at CDC stage III), including seizures related to drug abuse in six. The most frequent neurological problem in those patients in CDC group IV (58 patients) were the
AIDS dementia complex
(14 patients), an axonal sensorimotor neuropathy (12), toxoplasmosis (nine) and cryptococcal meningitis (three). All patients with a structural lesion had appropriate focal signs on examination. The value and role of CT cranial scanning in the diagnosis of toxoplasmosis is discussed and the importance of recognizing potentially treatable causes of both intellectual impairment and cytomegalovirus-related neuropathies is stressed. This is the first report of an unselected series of patients at all stages of
HIV
-I related neurological disease from a single UK centre.
...
PMID:The neurological features of HIV-positive patients in Glasgow--a retrospective study of 90 cases. 132 56
Retroviruses of the nervous system cause HTLV-1-associated myelopathy and
HIV
-associated diseases. The treatment of HTLV-1 disease is essentially conservative; there is no effective drug treatment and therefore patients should be simply supported and reassured. If appropriate, other members of the family should be tested for HTLV-1 disease and counselled. The effects of
HIV
on the nervous system are much more complex. Therapy must take account of the diverse complications of
HIV disease
. Patients are probably best managed in specialized clinics which can cope with the different manifestations of the disease. Zidovudine (AZT) is the only effective anti-
HIV
drug that is licensed. It is indicated in complicated seroconversion disease and for any manifestation of
HIV
progression including
AIDS dementia complex
. Management of severe neurological disease depends critically on the ability to diagnose and treat CNS-specific opportunistic infections. Whether zidovudine is indicated for early asymptomatic disease when CD4 counts are below 500 microliters-1 is controversial. The main problems of zidovudine are reversible anaemia which results in about 30% of patients not tolerating long-term use, and the development of drug resistance which may be associated with clinical failure of the drug. Other, new and experimental drug treatments are discussed but none of them has as yet shown any convincing evidence of efficacy. Future improvements in treatment appear to depend on the development of effective multiple drug regimens (concurrently or sequentially) which will overcome the challenge of drug resistance.
...
PMID:Therapeutic aspects of retroviral disease. 134 52
AIDS dementia complex
is a common neurologic disorder in later stages of
HIV
-1 infection. Because virus-specific CTL have been shown to contribute to neurologic disease in certain viral illnesses, we examined the cerebrospinal fluid of
HIV
-1-infected persons with various stages of
AIDS dementia complex
for the presence of
HIV
-1-specific CTL. In five of six subjects studied,
HIV
-1-specific CTL were identified in the cerebrospinal fluid. These CTL were directed at epitopes within the gag, reverse transcriptase, envelope, and nef proteins and restricted by HLA class I Ag. In four of these subjects, virus-specific CTL were detected in higher numbers in the cerebrospinal fluid compared to the peripheral blood, suggesting a specific recruitment to or local induction within the nervous system. These studies demonstrate the presence of a vigorous and broadly directed CTL response to
HIV
-1 in the central nervous system of infected persons with
AIDS dementia complex
, and provide immunologic evidence of localized intrathecal infection. Although
HIV
-1-specific CTL may serve to inhibit viral replication in the central nervous system, the presence of a persistent CTL response in the central nervous system may also contribute to the neurologic disorders characteristic of
HIV
-1 infection.
...
PMID:Detection of a vigorous HIV-1-specific cytotoxic T lymphocyte response in cerebrospinal fluid from infected persons with AIDS dementia complex. 138 38
To examine the neuropsychiatric effects of infection with
HIV
, 220 drug users (27
HIV
negative, 193
HIV
positive) completed tests evaluating premorbid intelligence, memory, non-verbal performance, information processing speed, and mood. When these measures were compared cross-sectionally by the severity of
HIV
illness, symptomatic patients (in CDC stage IV) were impaired on Trails B, two-choice decision time, delayed recall of the Wechsler Logical Memory Test and most components of the Auditory Verbal Learning Test. These findings imply reduced capacity for concentration, speed of thought and memory. When 101 patients were retested a mean of 16 months after their initial assessment, performance on Trails A and B, Block Design and delayed recall of the Wechsler Logical Memory Test deteriorated more for patients at, or progressing within, CDC stage IV, than performance of patients at stage III. The results broadly correspond to the cross-sectional findings. However, there was a decline in all tests of memory function for the sample independent of clinical staging. This may be evidence of brain involvement before the appearance of other symptoms. Self-rated measures of mood did not change cross-sectionally, progressively, or interactively with time and stage of
HIV
illness, and cannot account for the changes in cognitive function observed. Change in drug use, similarly, does not account for the cognitive findings. Four (5%) of the retested subjects developed
AIDS dementia complex
, but most of the performance and memory impairments seen were subclinical despite the destructive neuropathology presumed to underlie intellectual decline in patients with
HIV infection
.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:The Edinburgh cohort of HIV-positive drug users: pattern of cognitive impairment in relation to progression of disease. 139 40
We evaluated cerebrospinal fluid (CSF) and serum concentrations of interleukin-1-alpha (IL-1-alpha), interleukin-6 (IL-6) and tumour necrosis factor-alpha (TNF-alpha) in 30 patients with
AIDS dementia complex
(
ADC
), and in 20
HIV
-seronegative subjects with other neurological diseases (OND). CSF TNF-alpha, IL-1-alpha and IL-6 were more frequently detectable in
ADC
patients than in OND subjects. These cytokines were also detectable in CSF of
ADC
patients with minimal symptoms. In contrast, the majority of both
ADC
and OND patients did not contain detectable serum levels of cytokines. Our data support the notion of intrathecal synthesis of cytokines in
ADC
patients and raise the possibility that activated macrophages may play a significant role in the pathogenesis of
ADC
.
...
PMID:Cerebrospinal fluid cytokines in AIDS dementia complex. 140 21
A spectrum of neurocognitive defects, termed human immunodeficiency virus type 1 (HIV-1)-associated cognitive/motor complex, has been described in patients with acquired immunodeficiency syndrome (AIDS).
AIDS dementia complex
(
ADC
) is a severe form of this disease seen in 20 to 30% of terminally ill patients. The etiology of this complex is distinct from commonly observed opportunistic infections seen in brains of patients with AIDS and has been attributed to
HIV infection
within the brain. At autopsy, the brains of patients with
ADC
contain numerous
HIV
-infected macrophages/microglia with prominent subcortical damage, together termed HIV encephalitis. We retrospectively analyzed all 107 brains from a three-year period (1988-1990) of AIDS autopsies using immunocytochemistry to detect
HIV
. Rather than breaking into distinct groups of HIV encephalitis versus non-HIV encephalitis, the specimens revealed a spectrum of severity of
HIV infection
. Although only 16% of the brains showed the histological hallmarks of HIV encephalitis, more than 50% of the autopsies showed moderate to severe
HIV infection
. In a subset of 23 AIDS autopsies during which short postmortem times and absence of significant opportunistic infection permitted quantitative analysis of dendritic and synaptic complexities, we identified a strong correlation between neocortical dendritic and presynaptic damage and abundance of
HIV
envelope protein in the neocortical gray and deep white matter. This correlation suggests that the presence of
HIV
-1 in the neocortex may be responsible by direct or indirect mechanisms for dendritic and synaptic damage.
...
PMID:Spectrum of human immunodeficiency virus-associated neocortical damage. 141 2
Neurological disease frequently complicates
HIV
-1 infection. In addition to opportunistic infections, a syndrome of combined cognitive and motor impairment, referred to as the
AIDS dementia complex
, has been recognized. While presumed to relate to
HIV
-1 itself, the pathogenesis of this syndrome remains uncertain. Because of the limited extent of productive brain
HIV
-1 infection in many cases, and because such infection involves macrophages and microglia rather than cells of neuroectodermal origin, current speculation centers on indirect mechanisms of brain injury including virus- or cell-coded neurotoxins. We review clinical and laboratory studies and also describe models of the interaction of
HIV
-1 and immune responses that might account for brain injury.
...
PMID:Human immunodeficiency virus and the central nervous system. 144 70
Infection of the central nervous system by
HIV
-1, the agent of AIDS, is characterized by the presence of infected and giant microglial cells as well as astrocytosis, demyelination, and neuronal loss. To determine whether cells of neuroectoderm origin can be infected by
HIV
-1, we have inoculated primary cultures derived from adult human brain with a lymphotropic virus (LAV) or a neurotropic virus (Jr-FL) isolated from a patient with
AIDS dementia
. While Jr-FL invariably causes productive infection of cultured brain microglia, neither astrocytes nor oligodendrocytes became productively infected by these viral strains. Moreover, the cultured oligodendrocytes develop a normal network of processes and express differentiation antigens in the presence of an ongoing lytic infection of microglial cells. No
HIV
-1 proviral DNA was detected in primary astrocyte cultures devoid of microglial after inoculation of either
HIV
-1 strain. Similarly, the neuronal cell line HCN-1 in its differentiated state did not allow the virus to go through cycles of reverse transcription and replication. LAV, however, was able to replicate in undifferentiated HCN-1 cells. Thus, tropism of
HIV
-1 appears tightly restricted to only one type of differentiated cell in the CNS, the microglia.
...
PMID:The restricted nature of HIV-1 tropism for cultured neural cells. 144 25
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