Browse the corpus

Human immunodeficiency virus-associated neurocognitive disorders (HAND) encompass a spectrum of neurological and cognitive impairments in patients with human immunodeficiency virus (HIV), ranging from asymptomatic neurocognitive impairment to HIV-associated dementia. These disorders were formerly termed acquired immunodeficiency syndrome dementia complex. HAND affects 4% to 15% of patients with HIV and results from HIV-mediated damage to the central nervous system. In 2007, the National Institutes of Health categorized HAND into 3 classifications to assist with clinical evaluation and management. Early recognition and intervention are crucial to managing symptoms and preventing progression to severe impairment. Participants gain insight into the pathophysiology, clinical presentation, and classifications of HAND, along with effective evaluation and management strategies. The course emphasizes the importance of routine neurocognitive monitoring in patients with HIV and explores evidence-based approaches to treatment. Collaboration with an interprofessional team, including infectious disease specialists, neurologists, nurses, and mental health professionals, enhances patient outcomes through comprehensive care and tailored interventions. Objectives: Identify the classifications of human immunodeficiency virus-associated neurocognitive disorders and their distinguishing features. Differentiate between human immunodeficiency virus-associated neurocognitive disorders and other causes of neurocognitive impairment in patients with human immunodeficiency virus. Implement evidence-based guidelines for assessing and managing human immunodeficiency virus-associated neurocognitive disorders in clinical practice. Communicate interprofessional team strategies to improve care coordination and communication, advancing the prevention, diagnosis, and management of human immunodeficiency virus-associated neurocognitive disorders and improving patient outcomes. Access free multiple choice questions on this topic.

Neurocognitive deficits are the presenting complaint in 4% to 15% of patients diagnosed with human immunodeficiency virus (HIV). Patients may present with nonspecific complaints such as deficits in memory, concentration, attention, and motor skills. These symptoms are common in many disorders, and accurate diagnosis is critical for appropriate treatment. The acquired immunodeficiency syndrome (AIDS) dementia complex (ADC) was first defined in 1986. This was a frequent feature of HIV disease before antiretroviral therapy (ART) and highly active antiretroviral therapy came into common use in the mid-1990s. In addition to medical comorbidities, patients also frequently have various mental or psychosocial issues that can affect cognitive function, including mood disorders, post-traumatic stress disorder, and substance abuse or dependence. Increased risk of opportunistic infections, tumors, and side effects of ART drugs may also contribute to neurologic effects. Patients can experience delirium as part of the acute HIV syndrome or develop dementia during the later stages of their disease.[1][2] The spectrum of progressively more severe neurologic and cognitive symptoms (previously known as ADC) are now referred to as HIV-associated neurocognitive disorders (HAND) and were categorized in 2007 by the United States National Institutes of Health to include 3 classifications. These range in severity from asymptomatic neurocognitive impairment to minor neurocognitive disorder and HIV-associated dementia (HAD). The distinction between these levels is made by the use of neuropsychological testing in addition to observation of symptomatic functional impairment. Any other condition, including infection, cerebrovascular disease, or toxic encephalopathy, must not explain the observed impairment. In practice, distinguishing between the less severe categories of disease in the acute care setting is difficult due to the necessity of neuropsychological testing. Due to the profound symptomology and functional deficits associated with HAD, this diagnosis may be presumed, especially in patients with untreated or advanced stages of AIDS disease.[3]

The relationship between HIV infection and observed neurocognitive deficits is not clearly understood but is thought to be due to several factors. Proteins expressed from viral genes in infected cells can directly damage neurons. Cytokines that activate the immune response in surrounding healthy glial cells may also contribute to neuronal damage. Additionally, autoimmune antibodies against brain tissue have been isolated in patients infected with HIV and HAD, which appear to be present less frequently in those who do not develop dementia. Autoantibodies continue to be present in patients' cerebrospinal fluid following treatment and may explain the progression of symptoms in patients with low viral counts.[4][5][6]

Neuropsychological testing may reveal subtle cognitive deficits in as many as 40% of HIV-infected individuals treated with antiretrovirals. A nationwide Danish study estimated that 1 of 1000 patients not treated with highly active ART and with a low cluster of differentiation (CD)4 counts would progress to HAD. Data from the European CASCADE study suggest an incidence of HAD of 0.66 per 1000 person-years, a decrease of almost tenfold from the pre-ART era. In the United States, the CHARTER study estimated an incidence of HAD of 10.5 cases per 1000 patient-years; this is down from 21 cases per 1000 patient years before the advent of ART therapy. The prevalence of HAND among White and non White individuals, as well as between men and women, appears to mimic that of HIV infection and increases with age.[7]

Initial pathological changes include reduced cortical gray matter and brain atrophy. Autopsy examination of affected patients' brain tissue may show perivascular macrophage and lymphocyte infiltration, multinucleated giant cells, myelin loss, and white matter astrogliosis. The basal ganglia are most commonly affected.

Microscopic analysis is also likely to show evidence of encephalitis due to common complications of HIV, including progressive multifocal leukoencephalopathy, non-Hodgkin lymphoma, or infection such as from cytomegalovirus, toxoplasmosis, varicella-zoster, herpes simplex, or Human polyomavirus virus 1.

A complete history and physical examination should be obtained to identify risk factors for HAND/HAD as well as to rule out other causes of dementia. Risk factors identified by the CASCADE study include low CD4 count, advanced age at seroconversion, duration of HIV infection, and prior AIDS-defining diagnosis. Particular attention should be given to adherence to the medication regimen and medical follow-up, as well as the timing of HIV diagnosis, stage of disease, and current treatment. The time course of symptoms and degree of functional impairment should be elicited. Other conditions potentially contributing to cognitive impairment should be identified, including any history of head trauma, substance abuse, or psychiatric disorders. The onset of complaints is generally indolent. Patients and their families or caregivers may report mood changes, memory impairment, insomnia, weight loss, or apathy.[8] Patients experiencing mild neurocognitive deficits are unlikely to have specific complaints. As a result, neuropsychological testing should be administered routinely with HAD risk factors or low CD4 counts. Patients may exhibit flattened affect and lack of emotional lability, which may distinguish them from those with a major depressive disorder. Verbal fluency, decision-making, executive functioning, and memory deficits are common. Higher cortical dysfunctions such as aphasia, agnosia, and apraxia are generally absent but may develop in the later stages of progression. Patients with advanced disease may develop frontal release signs, hyperreflexia, and difficulty with rapid alternating movements. A neurologic exam should assess the level of alertness (HAD generally does not cause an alteration in the level of consciousness) and findings suggestive of an alternative neurologic disorder such as Parkinson disease, stroke, tumor, or progressive multifocal leukoencephalopathy.

Diagnostic studies should focus on excluding other conditions that produce cognitive impairment in the patient. This may include infectious, neurological, or psychiatric disorders in addition to toxic encephalopathies. Liver function, blood glucose, vitamin B12, thyroid hormone, syphilis, and hepatitis serologies may be useful depending on the patient's presentation. The stage of HIV infection may be assessed with CD4 count and viral load.[9][10] Neuroimaging, such as magnetic resonance imaging, should be ordered to evaluate for neurologic disorders or cerebrovascular disease. Diffuse cerebral atrophy is usually present and can affect the basal ganglia, white matter, and cortical regions. In advanced disease, an electroencephalogram shows generalized slowing. Cerebral spinal fluid (CSF) studies may show elevated viral load, lymphocytic pleocytosis, and increased total protein levels; however, these findings are nonspecific. If drawn, CSF serologies should include toxoplasmosis, cryptococcal antigen, syphilis, and viral polymerase chain reaction studies, including John Cunningham virus, Epstein-Barr virus, and cytomegalovirus.

The mainstay of prevention and treatment of HAND spectrum disorders is adherence to ART. Appropriate treatment of HIV infection shows improvement in cognitive function in patients diagnosed with severe deficits. The incidence of HAD has also decreased over time with the widespread use of ART in observational studies. ART should be initiated for any untreated patient with HIV infection who is beginning to experience cognitive decline. Selecting a specific ART regimen should follow standard protocols based on viral ribonucleic acid load, genotype, drug interactions, and comorbidities. The effectiveness of ART in preventing the milder forms of minor neurocognitive disorder and asymptomatic neurocognitive impairment is less clear as these conditions are subtle and likely underdiagnosed. Whether specific ART regimens are more effective at preventing the progression of cognitive decline remains unclear. The antiretroviral efavirenz should be avoided in patients undergoing evaluation for HAD due to its adverse effect profile that may interfere with neuropsychological testing. In patients on appropriate therapy with low viral counts and high CD4 levels, progressive neurocognitive deficits are more likely to be due to another etiology. Appropriate evaluation should be done to rule out these conditions. Psychiatric comorbidities may be present, and treatment should be initiated following a psychiatric evaluation.

The differential diagnoses for HIV-1 encephalopathy and AIDS dementia complex include the following: CNS infection, especially in those with a low CD4 count who are not on antibiotic prophylaxis Consider herpes simplex, varicella-zoster, cytomegalovirus, Epstein-Barr virus, John Cunningham virus, toxoplasmosis, syphilis, and Cryptococcus. Malignancy, including CNS lymphoma and metastatic disease (usually identified on neuroimaging) Dementia, including Parkinson, Alzheimer, Lewy Body, and frontal and temporal lobe dementias Be aware of the increased risk of dementia syndromes due to the increase in the long-term survival of the HIV-infected population in general. Endocrine disorders such as adrenal insufficiency or hypothyroidism Substance use or acute intoxication Delirium Nutritional deficiencies, particularly cognitive impairment secondary to B12 deficiency, may be associated with paresthesia and sensory problems. Acute intoxication Drug effects

Mean survival in HAD without ART is 3 to 6 months. This increased to 38.5 months with the initiation of ART therapy in the 1990s, and it is thought that with adherence to highly active ART, mean survival should approach that of the general HIV-affected population. A worse prognosis is associated with the following factors: lower educational level, increasing age, lower CD4 count, higher viral load, decreasing hemoglobin, decreasing platelets, lower body mass index, hepatitis C coinfection, intravenous drug use, and poor medication adherence. In addition, the presence of HAD is an independent predictor of risk of death in patients with HIV.[11][12]

Consultation with an infectious disease specialist or clinician experienced in caring for patients with HIV is recommended for managing the highly active ART regimen. Psychiatric consultation may also be indicated as patients with HIV and HAD commonly have comorbidities, including generalized anxiety disorder, major depressive disorder, and agitation, and may present with psychosis. A neurologic evaluation may be necessary to complete the full workup for alternative causes of cognitive deficits.

Key facts to keep in mind about HIV-1 encephalopathy and aids dementia complex are as follows: Alteration in mental status is common in patients with HIV, and etiology may be unclear. The common use of highly active ART in developed countries has dramatically decreased the risk of developing HAND; however, disorders on this spectrum are common in patients from developing countries or in patients whose advanced diseases have gone untreated. Cognitive deficits associated with HAD include impaired executive function, decision-making, and language; their onset is generally slow and progressive. Patients with nonspecific cognitive symptoms, low CD4 count, or risk factors for HAD should be screened using neuropsychologic testing. Workup should focus on excluding other causes of cognitive impairment in immunocompromised individuals. Treatment for patients with HIV with neurocognitive impairment is the initiation of or adherence to HAART therapy. Rapid neurologic or cognitive decline, especially in an appropriately treated patient with a high CD4 count and low viral load, should prompt investigation into alternative causes, including CNS infection, tumor, neurodegenerative diseases, or toxic encephalopathy.

To improve outcomes in patients with HIV, the key is to encourage compliance with highly active ART. Appropriate treatment of HIV infection shows improvement in cognitive function in patients diagnosed with severe deficits. The incidence of HAD has also decreased over time with the widespread use of ART in observational studies. ART should be initiated for any untreated patient with HIV infection who is beginning to experience cognitive decline. Selecting a specific ART regimen should follow standard protocols based on viral ribonucleic acid load, genotype, drug interactions, and the presence of comorbidities. Continually monitoring of neurophysiological function is recommended to ensure the patient is not deteriorating. Interprofessional healthcare team dynamics drive optimal outcomes for these patients.