2012
DOI: 10.1097/qad.0b013e328355e6b2
|View full text |Cite
|
Sign up to set email alerts
|

Cerebrospinal fluid HIV escape associated with progressive neurologic dysfunction in patients on antiretroviral therapy with well controlled plasma viral load

Abstract: Objective To characterize HIV-infected patients with neuro-symptomatic CSF ‘escape,’ defined as detectable CSF HIV RNA in the setting of treatment-suppressed plasma levels or CSF RNA >1 log higher than plasma RNA. Design Retrospective case series. Setting 4 urban medical centers in the United States and Europe. Subjects Virologically controlled HIV-infected patients on antiretroviral therapy (ART) with progressive neurologic abnormalities who were determined to have CSF ‘escape.’ Intervention Optimizat… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
2
1
1
1

Citation Types

12
220
2
4

Year Published

2014
2014
2022
2022

Publication Types

Select...
8
1

Relationship

1
8

Authors

Journals

citations
Cited by 226 publications
(238 citation statements)
references
References 31 publications
12
220
2
4
Order By: Relevance
“…[22,23,[139][140][141][142] In most of the subjects differential viral evolution (with resistance-associated mutation selected in the CSF compartment) was shown and it was explained by asymmetrical penetration of ARVs (with some cerebrospinal fluid concentrations below the limit of detection) but not confirmed by other reports. [143] In a large longitudinal study the factors associated with CSF escape were the presence of CSF pleocytosis, the use of a PI-containing HAART and ultrasensitive plasma HIV RNA level: [144] the poor CSF to plasma ratios observed with protease inhibitors (0 to 1.4% with currently used PIs) may possibly explain these results as well as persistent intrathecal immune activation and plasma residual viremia.…”
Section: Csf Escapementioning
confidence: 70%
“…[22,23,[139][140][141][142] In most of the subjects differential viral evolution (with resistance-associated mutation selected in the CSF compartment) was shown and it was explained by asymmetrical penetration of ARVs (with some cerebrospinal fluid concentrations below the limit of detection) but not confirmed by other reports. [143] In a large longitudinal study the factors associated with CSF escape were the presence of CSF pleocytosis, the use of a PI-containing HAART and ultrasensitive plasma HIV RNA level: [144] the poor CSF to plasma ratios observed with protease inhibitors (0 to 1.4% with currently used PIs) may possibly explain these results as well as persistent intrathecal immune activation and plasma residual viremia.…”
Section: Csf Escapementioning
confidence: 70%
“…The patient was a 46-year-old man, who was admitted with behavioral and cognitive changes while on treatment with lamivudine, abacavir, and saquinavir. Blood and CSF examinations at admission showed plasma HIV RNA <40 c/mL, CSF HIV RNA 274 c/mL, CSF HIV genotyping M184V reverse transcriptase mutation, CSF white blood cells 68/μL, and CD4+ 545/μL Values refer to refs [57,58] a Ref [57] only; ref. [58]: median 31, range achieved in the CNS is inadequate to suppress the local, compartmentalized infection.…”
Section: Symptomatic Escape: Isolated Cns Treatment Failurementioning
confidence: 99%
“…Blood and CSF examinations at admission showed plasma HIV RNA <40 c/mL, CSF HIV RNA 274 c/mL, CSF HIV genotyping M184V reverse transcriptase mutation, CSF white blood cells 68/μL, and CD4+ 545/μL Values refer to refs [57,58] a Ref [57] only; ref. [58]: median 31, range achieved in the CNS is inadequate to suppress the local, compartmentalized infection. Biologically, the relative preservation of the systemic immune system with restored CD4 and high CD8 T cells characteristic of treated patients may be important in determining the phenotype of the disease with its CSF pleocytosis and frequent CD8 encephalitis.…”
Section: Symptomatic Escape: Isolated Cns Treatment Failurementioning
confidence: 99%
“…Ongoing cognitive impairment, occasional episodes of viral replication developing in the brain (termed CSF viral escape), and evidence of ongoing inflammatory responses in the brain compartment reflected in CSF continue to support trials targeting CNS HIV complications [24][25][26]. The target of curing HIV must include the brain reservoir of virus, which is likely to be one of the most challenging targets for this agenda, because of the unique environment of the brain.…”
Section: Hiv-associated Neurocognitive Disordermentioning
confidence: 99%