论文信息 - Molecular analysis of cerebrospinal fluid: potential for the study of HIV-1 infection of the central nervous system.

Molecular analysis of cerebrospinal fluid: potential for the study of HIV-1 infection of the central nervous system.

The molecular analysis of cerebrospinal fluid (CSF) provides an inestimable tool for the study of HIV infection of the central nervous system (CNS). Current nucleic acid amplification techniques enable the measurement of CSF HIV-1 RNA levels which can be predictive of HIV-associated neurological damage. CSF HIV-1 RNA levels do not necessarily correlate with the corresponding plasma levels, thus supporting the possibility of an intrathecal virus production, i.e., from brain macrophages. However, in early stages of HIV infection, as well as during some opportunistic CNS diseases, CNS or CSF infiltrating lymphocytes might be the main source of CSF virus. A drastic decrease in CSF viral load is usually observed along with a decrease in plasma levels in patients receiving highly active antiretroviral therapy (HAART), with durable suppression of CSF viral load over months. However, during the first weeks of therapy, the dynamics of response may differ in the CSF as compared to plasma, again suggesting that virus replication may be compartmentalised in the CSF. A number of mechanisms are likely to be involved in the response to therapy in CSF, including among the others the trafficking of cell populations supporting viral replication between blood, CNS and CSF, and the role of the anatomical brain barriers in limiting the access of antiretroviral drugs into the CSF. A potential risk associated with compartmentalisation of HIV infection is of an incomplete suppression of virus replication in the CSF, thus creating the ground for local development of anti-HIV drug resistance. In order to assess this occurrence, long-term studies of viral load and genotypic analyses on paired CSF and plasma will be necessary and these will also help elucidate the complex interrelationship between viral replication in these compartments.

P. Cinque | S. Presi | A. Bestetti | P. Morelli

[1] C. Mims. 5 – The Spread of Microbes through the Body , 2001 .

[2] P. Narciso,et al. Positive and sustained effects of highly active antiretroviral therapy on HIV-1-associated neurocognitive impairment. , 1999, AIDS.

[3] B. Clotet,et al. Cerebrospinal fluid HIV-1 RNA levels in asymptomatic patients with early stage chronic HIV-1 infection: support for the hypothesis of local virus replication. , 1999, AIDS.

[4] M. Lederman,et al. Presence of mutation conferring resistance to lamivudine in plasma and cerebrospinal fluid of HIV-1-infected patients. , 1999, Journal of acquired immune deficiency syndromes.

[5] D. Glidden,et al. Time course of cerebrospinal fluid responses to antiretroviral therapy: evidence for variable compartmentalization of infection. , 1999, AIDS.

[6] O. Selnes,et al. Combination antiretroviral therapy improves psychomotor speed performance in HIV-seropositive homosexual men , 1999, Neurology.

[7] J. van Lunzen,et al. HIV infection of the central nervous system is characterized by rapid turnover of viral RNA in cerebrospinal fluid. , 1999, Journal of acquired immune deficiency syndromes and human retrovirology : official publication of the International Retrovirology Association.

[8] M A Fischl,et al. A randomized, controlled, double-blind study comparing the survival benefit of four different reverse transcriptase inhibitor therapies (three-drug, two-drug, and alternating drug) for the treatment of advanced AIDS. AIDS Clinical Trial Group 193A Study Team. , 1998, Journal of acquired immune deficiency syndromes and human retrovirology : official publication of the International Retrovirology Association.

[9] W. Kelder,et al. β‐Chemokines MCP‐1 and RANTES are selectively increased in cerebrospinal fluid of patients with human immunodeficiency virus–associated dementia , 1998 .

[10] H. Gendelman,et al. Suppression of inflammatory neurotoxins by highly active antiretroviral therapy in human immunodeficiency virus-associated dementia. , 1998, The Journal of infectious diseases.

[11] D. Fuchs,et al. Neurological efficacy of stavudine, zidovudine, and lamivudine , 1998, The Lancet.

[12] B. Brew. Neurological efficacy of stavudine, zidovudine, and lamivudine , 1998, The Lancet.

[13] V. Torri,et al. Elevated cerebrospinal fluid levels of monocyte chemotactic protein‐1 correlate with HIV‐1 encephalitis and local viral replication , 1998, AIDS.

[14] B Clotet,et al. Antiretroviral drug resistance testing in adults with HIV infection: implications for clinical management. International AIDS Society--USA Panel. , 1998, JAMA.

[15] I. Keet,et al. Cerebrospinal-fluid HIV-1 RNA and drug concentrations after treatment with lamivudine plus zidovudine or stavudine , 1998, The Lancet.

[16] A. Berger,et al. Randomized, controlled phase II trial of subcutaneous interleukin‐2 in combination with highly active antiretroviral therapy (HAART) in HIV patients , 1998, AIDS.

[17] J. R. Fiore,et al. Neurological disorders during HIV‐1 infection correlate with viral load in cerebrospinal fluid but not with virus phenotype , 1998, AIDS.

[18] V. Calvez,et al. The level of human immunodeficiency virus (HIV) type 1 RNA in cerebrospinal fluid as a marker of HIV encephalitis. , 1998, Clinical infectious diseases : an official publication of the Infectious Diseases Society of America.

[19] C. Rouzioux,et al. Longitudinal comparison of HIV-1 RNA burden in plasma and cerebrospinal fluid in two patients starting triple combination antiretroviral therapy. , 1998, AIDS.

[20] A. Lazzarin,et al. Cerebrospinal fluid HIV‐1 RNA levels: correlation with HIV encephalitis , 1998, AIDS.

[21] P. Pehrsson,et al. Cerebrospinal fluid mononuclear cell counts influence CSF HIV-1 RNA levels. , 1998, Journal of acquired immune deficiency syndromes and human retrovirology : official publication of the International Retrovirology Association.

[22] P. Sonnenberg,et al. High human immunodeficiency virus type 1 RNA load in the cerebrospinal fluid from patients with lymphocytic meningitis. , 1998, The Journal of infectious diseases.

[23] M. Maschke,et al. HIV-1 RNA levels in cerebrospinal fluid and plasma correlate with AIDS dementia. , 1998, AIDS.

[24] G. Norkrans,et al. HIV-1 RNA detectable with ultrasensitive quantitative polymerase chain reaction in plasma but not in cerebrospinal fluid during combination treatment with zidovudine, lamivudine and indinavir. , 1998, AIDS.

[25] C. Hall,et al. CSF, plasma viral load and HIV associated dementia. , 1998, Journal of neurovirology.

[26] R Brookmeyer,et al. Identification of a reservoir for HIV-1 in patients on highly active antiretroviral therapy. , 1997, Science.

[27] I. Grant,et al. Cerebrospinal fluid human immunodeficiency virus type 1 RNA levels are elevated in neurocognitively impaired individuals with acquired immunodeficiency syndrome , 1997, Annals of neurology.

[28] J. McArthur,et al. Relationship between human immunodeficiency virus—associated dementia and viral load in cerebrospinal fluid and brain , 1997, Annals of neurology.

[29] S. Staprans,et al. Measuring the “viral load” in cerebrospinal fluid in human immunodeficiency virus infection: Window into brain infection? , 1997, Annals of neurology.

[30] F. Clavel,et al. Central nervous system as a sanctuary for HIV-1 infection despite treatment with zidovudine, lamivudine and indinavir. , 1997, AIDS.

[31] Alan S. Perelson,et al. Decay characteristics of HIV-1-infected compartments during combination therapy , 1997, Nature.

[32] B. Brew,et al. Levels of human immunodeficiency virus type 1 RNA in cerebrospinal fluid correlate with AIDS dementia stage. , 1997, The Journal of infectious diseases.

[33] D. Richman,et al. In vivo compartmentalization of human immunodeficiency virus: evidence from the examination of pol sequences from autopsy tissues , 1997, Journal of virology.