Biotypes of HIV-associated neurocognitive disorders based on viral and immune pathogenesis

Johnson, Tory P.; Nath, Avindra

doi:10.1097/qco.0000000000000825

Cited by 20 publications

(16 citation statements)

References 86 publications

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“…Human immunodeficiency virus (HIV) penetrates the CNS early during acute infection and infects microglia, macrophages, and to a lesser extent astrocytes, which can result in a macrophage-mediated encephalitis [ 18 , 19 ]. Clinically this is associated with a rapidly progressing subacute subcortical dementia [ 20 ] which is treatable with antiretroviral therapies (ART). However, even with adequate ART and suppression of virus both in the periphery and the CNS, HIV can cause CNS disease years after initial infection, collectively known as HIV-associated neurocognitive disorders (HAND).…”

Section: Infections Associated With Late Central Nervous System Diseasementioning

confidence: 99%

“…This may be due to the relationship between lower CD4+ T-cell nadirs and a larger viral reservoir and more residual viral activity [ 21 ]. This larger and more active viral presence can lead to CSF viral escape and T-cell mediated encephalitis, which presents clinically with headache, tremors, cognitive impairment, confusion, focal neurologic deficits, and seizures [ 20 ]. However, even in the absence of viral replication, expression of viral proteins can lead to CNS disease.…”

Section: Infections Associated With Late Central Nervous System Diseasementioning

confidence: 99%

“…These proteins are toxic and alter neuronal and glial cell functioning (reviewed in [25][26][27]). Patients present with varying degrees of cognitive and psychomotor impairments that slowly progress over time, a spectrum disorder collectively known as HIV-protein associated encephalopathy [20]. As ART does not impact the production of viral proteins from integrated virus, the development of new therapies to inhibit viral transcription and translation are needed.…”

Section: Human Immunodeficiency Virusmentioning

confidence: 99%

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Chronic and delayed neurological manifestations of persistent infections

Pandya

Johnson

2023

Current Opinion in Neurology

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Purpose of the review Persistent infections capable of causing central nervous system (CNS) complications months or years after the initial infection represent a major public health concern. This concern is particularly relevant considering the ongoing coronavirus disease 2019 pandemic, where the long-term neurological effects are still being recognized. Recent findings Viral infections are a risk factor for the development of neurodegenerative diseases. In this paper, we provide an in-depth exploration of the prevalent known and suspected persistent pathogens and their epidemiological and mechanistic links to later development of CNS disease. We examine the pathogenic mechanisms involved, including direct viral damage and indirect immune dysregulation, while also addressing the challenges associated with detecting persistent pathogens. Summary Viral encephalitis has been closely associated with the later development of neurodegenerative diseases and persistent viral infections of the CNS can result in severe and debilitating symptoms. Further, persistent infections may result in the development of autoreactive lymphocytes and autoimmune mediated tissue damage. Diagnosis of persistent viral infections of the CNS remains challenging and treatment options are limited. The development of additional testing modalities as well as novel antiviral agents and vaccines against these persistent infections remains a crucial research goal.

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Section: Infections Associated With Late Central Nervous System Diseasementioning

confidence: 99%

Section: Infections Associated With Late Central Nervous System Diseasementioning

confidence: 99%

Section: Human Immunodeficiency Virusmentioning

confidence: 99%

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Chronic and delayed neurological manifestations of persistent infections

Pandya

Johnson

2023

Current Opinion in Neurology

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“…A new look at how PLWH develop NCDs, whether or not they are on ART, emphasises how patients with similar clinical phenotypes may have very different underlying disease processes, thus requiring different treatments. The proposition of different ‘biotypes’ of HAND is built on the older neuropathology but its case definitions mainly eschew diagnostic tissue pathology and rely on CSF and blood profiles of immunity, virology, and neuroimaging [ 21 ]. There are four biotypes proposed: Macrophage-mediated HIV encephalitis: essentially the original classic HIVE in ART-untreated patients; CNS viral escape, in ART-treated patients, with a lymphocytic encephalitis, elevated HIV viral load in CSF (viral escape), white matter hyperintensities on neuroimaging, and related to poor CNS ART penetration and ART drug resistance; T-cell mediated encephalitis: associated with immune reconstitution reaction (IRIS) on ART, the target being HIV or opportunistic infection; pathologically there are CD4 + or CD8 + T-cell infiltrates in brain parenchyma (i.e.…”

Section: Biotypes Of Hand: a Summation Approachmentioning

confidence: 99%

Historical and current issues in HIV encephalitis, and the role of neuropathology in HIV disease: a pathological perspective

Lucas

2022

J Neurol

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In the 1980s, after the HIV pandemic was recognised, neuropathology identified cerebral white matter lesions that were found in the brains of infected persons with a severe irreversible dementia syndrome, this became known as ‘HIV encephalitis’. Subsequent work in Europe and north America found subtle morphological abnormalities in cerebral neurones and their connections. With the advent of effective anti-retroviral therapies after 1996, the incidence of severe HIV-related dementia declined, as did investigative tissue pathology into this HIV brain disease. Currently, the intense interest over HIV neurocognitive impairment focuses on neuroimaging, comparative blood and cerebrospinal fluid analysis, viral subtype analysis, and the search for biomarkers that correlate with brain function. Tissue neuropathology in HIV is more restricted to the diagnosis of acute disease such as opportunistic infections and tumours, and confirmation of the acute CD8 + T-cell encephalitis syndrome. But correlative tissue pathology will still be needed as newer therapeutic measures are developed to prevent and manage chronic HIV brain impairment.

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“…Other causes of neuroinflammation in persons with well-controlled HIV include macrophage-mediated HIV encephalitis and CD8 encephalitis ( 3 )—a hallmark of both of which is CNS HIV escape, in which HIV RNA can be detected in the CSF ( 4 ). Persons living with HIV are also at an increased risk for immune dysregulation ( 5 , 6 ) and autoimmune disorders of the nervous system including acute and chronic inflammatory demyelinating polyneuropathy ( 7 ) (AIDP and CIDP, respectively).…”

Section: Introductionmentioning

confidence: 99%

Dual ankyrinG and subpial autoantibodies in a man with well-controlled HIV infection with steroid-responsive meningoencephalitis: A case report

et al. 2023

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Neuroinvasive infection is the most common cause of meningoencephalitis in people living with human immunodeficiency virus (HIV), but autoimmune etiologies have been reported. We present the case of a 51-year-old man living with HIV infection with steroid-responsive meningoencephalitis whose comprehensive pathogen testing was non-diagnostic. Subsequent tissue-based immunofluorescence with acute-phase cerebrospinal fluid revealed anti-neural antibodies localizing to the axon initial segment (AIS), the node of Ranvier (NoR), and the subpial space. Phage display immunoprecipitation sequencing identified ankyrinG (AnkG) as the leading candidate autoantigen. A synthetic blocking peptide encoding the PhIP-Seq-identified AnkG epitope neutralized CSF IgG binding to the AIS and NoR, thereby confirming a monoepitopic AnkG antibody response. However, subpial immunostaining persisted, indicating the presence of additional autoantibodies. Review of archival tissue-based staining identified candidate AnkG autoantibodies in a 60-year-old woman with metastatic ovarian cancer and seizures that were subsequently validated by cell-based assay. AnkG antibodies were not detected by tissue-based assay and/or PhIP-Seq in control CSF (N = 39), HIV CSF (N = 79), or other suspected and confirmed neuroinflammatory CSF cases (N = 1,236). Therefore, AnkG autoantibodies in CSF are rare but extend the catalog of AIS and NoR autoantibodies associated with neurological autoimmunity.

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Biotypes of HIV-associated neurocognitive disorders based on viral and immune pathogenesis

Cited by 20 publications

References 86 publications

Chronic and delayed neurological manifestations of persistent infections

Chronic and delayed neurological manifestations of persistent infections

Historical and current issues in HIV encephalitis, and the role of neuropathology in HIV disease: a pathological perspective

Dual ankyrinG and subpial autoantibodies in a man with well-controlled HIV infection with steroid-responsive meningoencephalitis: A case report

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