Objective  To describe a 31-year-old patient infected with HIV who presented with 2 recurrent, acute episodes of neurologic impairment in a 5-month period.

Design  Comparison of clinical and histologic data between the present case and previously published cases.

Setting  Community hospital.

Patient  A 31-year-old, HIV-infected patient with recurrent strokes and chronic lymphocytic meningitis.

Intervention  After ruling out cardiac embolisms and coagulation disorders, the presence of central nervous system vasculitis, probably secondary to an infectious process, was suspected based on the clinical examination and cerebrospinal fluid abnormalities.

Results  Necropsy findings suggest the diagnosis of primary angiitis of the central nervous system, and the only infectious agent that could be found was HIV.

Conclusions  Histologic studies were compatible with a diagnosis of primary angiitis of the central nervous system, but the pathogenic role of HIV in the genesis of the vasculitic process cannot be elucidated.

REPORT OF A CASE

Computed tomography (CT) of the brain showed no abnormalities. Lumbar puncture revealed clear cerebrospinal fluid (CSF) with the following values: white blood cell count, 130/µL (90% lymphocytes); glucose, 38 mg/dL (2.11 mmol/L); protein, 0.27 g/dL; and adenosine deaminase, 12 U/L. The HIV-CSF viral load was not measurable at that moment. Magnetic resonance imaging (MRI) of the brain and brainstem showed areas of low intensity on T1-weighted signal and of high intensity on T2-weighted signal with no contrast enhancement within the pons, left semioval center, and left subcortical frontoparietal area. The MRI suggested rhomboencephalitis, and vascular damage or ischemic lesions could not be ruled out (Figure 1). The results of the following CSF analyses were negative: cytologic testing; VDRL test; bacterial, mycobacterial, fungal and viral cultures; Cryptococcus latex agglutination; and polymerase chain reaction (PCR) for herpes simplex virus (HSV) types 1 and 2, cytomegalovirus (CMV), and varicella-zoster virus (VZV). In blood analysis, the results were also negative for viral cultures, CMV antigen, and Cryptococcus latex detection, as well as for serologic tests for Treponema pallidum, Brucella, Legionella, Mycoplasma, and Borrelia burgdorferi.

View larger version (34K): [in this window] [in a new window] Figure 1. T2-weighted magnetic resonance images, dating from October 1996, showing abnormal signal in the frontoparietal area (A) and pons (B).

The patient achieved slow clinical improvement during a 3-month period until only a slight unsteady gait persisted. He was empirically treated with tuberculostatic drugs for 9 months. A follow-up MRI obtained 1 month after starting treatment was identical to the earlier one and the abnormalities of the CSF persisted. In February 1997, the patient experienced loss of muscle strength of his left side in less than 24 hours. Neurologic examination on admission revealed reduced alertness and cognition. He had horizontal nystagmus on looking to the right and flaccid left-sided hemiparesis (manual muscle test score: arm, 1/5; leg, 4/5). A CT scan of the brain showed multiple residual focal cystic-necrotic lesions within the pons, midbrain, and the region of the right basal ganglia. A third MRI revealed a retractile dilation of the right frontal horn of the lateral ventricle and progression of lesions with new areas of low signal intensity on T1-weighted images and high signal intensity on T2-weighted images within the right caudate, putamen, and globus pallidus and bilaterally in the pons and right midbrain (Figure 2). Magnetic resonance angiography showed abnormalities that suggested segmental stenosis of the supraclinoid segments of both internal carotid arteries and the distal segment of the basilar artery (Figure 3). Conventional angiography and CNS biopsy were not performed. Despite new empirical treatment with acyclovir and prednisone (60 mg/d orally) for 2 months, the patient's neurologic status gradually deteriorated. The study findings from CSF, repeated during the next few months, remained unchanged with characteristic findings of aseptic meningitis. A CT scan of the brain in April 1997 revealed multifocal low-density areas within the midbrain and the right capsuloganglionar region and obvious asymmetry on the lateral ventricle, all compatible with cerebral ischemia. The patient died in July 1997, in an impaired immunologic situation with a CD4 cell count of 105/µL, 10 months after the onset of symptoms.

View larger version (30K): [in this window] [in a new window] Figure 2. T2-weighted magnetic resonance images obtained in February 1997 showing new lesions in the right caudate, putamen, and globus pallidus.

View larger version (31K): [in this window] [in a new window] Figure 3. Magnetic resonance angiogram showing segmental narrowing of intracranial arteries.

A CNS-limited necropsy was performed. Macroscopically, there were multiple areas of softening and cysts of 1.5 cm in diameter within the putamen, caudate, right thalamus, and brainstem (Figure 4). The meninges were thickened at the base of the brain and cerebellum. There was segmental thickening of vessels in the Willis circle with luminal narrowing. Microscopically, the areas with softening and cysts corresponded to focuses of necrosis with abundant macrophages and adjacent reactive gliosis. Lymphocytic vasculitis was observed in the meningeal and parenchymal vessels, mainly in nuclei at the base and brainstem. The vessels in the Willis circle showed evidence of fibrous vasculitis with focal destruction of the muscular structure, fibrosis of the intima, giant multinucleated cells, lymphoplasmocyte infiltrate, and focal fibrinoid degeneration (Figure 5). No microorganisms or cytopathic changes were observed on the usual stains. Brain bacterial and viral cultures (enteroviruses, HSV types 1 and 2, CMV, and VZV) were all negative. Immunohistochemical studies of the lymphocyte cells (pan T, pan B) did not show any monoclonality. Brain infection by CMV, HSV types 1 and 2, and VZV was also excluded by immunohistochemical studies. The necropsy findings suggested the diagnosis of PACNS, but the etiologic role of HIV could not be ruled out. Afterward, the nuclei from the base (globus pallidus and putamen) were analyzed for HIV. Using the PCR qualitative technique (Amplicor HIV; Roche, Branchburg, NJ), it was possible to demonstrate the presence of HIV-integrated DNA in the tissues studied.

View larger version (50K): [in this window] [in a new window] Figure 4. Macroscopic examination of cerebrum showing cysts in the putamen and caudate.

View larger version (68K): [in this window] [in a new window] Figure 5. Microscopic examination of the vessels in the Willis circle, showing fibrous vasculitis with plasmocyte infiltrate (A; hematoxylin-eosin, original magnification x20) and the presence of giant multinucleated cells (B; hematoxylin-eosin, original magnification x200).

COMMENT

Central nervous system vascular involvement is relatively frequent in HIV infection,³ usually as a result of infections (bacterial, viral, fungal, or parasitic), neoplastic disease, or toxic drug abuse. Moreover, HIV frequently is associated with coexisting infections such as Epstein-Barr virus, CMV, hepatitis B, and others, all of which have been linked to various vasculitic syndromes. Up to 25% of HIV-infected patients have cerebral infarcts in some autopsy series.⁴ Ruling out secondary infarcts, thickening of the small vessels, dilation of perivascular spaces, mineralization of the walls, and inflammatory infiltrates, all of these cerebral infarcts have been HIV related. The pathogenic role of HIV in cerebral vasculitis is supported by evidence of the infection of brain cells by HIV. In 1985, Ho et al⁵ conducted human T-cell lymphotropic virus type III isolation from CSF and neural tissues of patients with neurologic syndromes related to acquired immunodeficiency syndrome, mainly chronic meningitis and dementia. Afterward, it was shown that the perivascular or transluminal inflammation was composed of CD3⁺ T cells or CD68⁺ monocytes-macrophages reactive to the p24 protein of HIV,⁶ producing vasculitis and leptomeningitis.⁷ The PCR in situ hybridization technique shows HIV in the CNS in a productive form in mononuclear cells and in a proviral and integrated HIV-DNA or HIV-RNA form in microglia, macrophage and perivascular, giant multinucleated, and endothelial cells. The same technique shows HIV–reverse transcriptase in the same cells.⁸

Rarely, PACNS is accepted in HIV-infected patients. In a review of the literature, we found only 22 cases of histologically accepted CNS vasculitis.^9-18 The clinical, radiologic, and histologic features of the described patients are given in Table 1. Patients described as individual cases showed neurologic events, whereas those described in series had their conditions diagnosed at necropsy. In 1986, Yankner et al¹⁰ described an HIV-infected patient with a progressive decline of mental status, confusion, and headache. A mild dysmetria of the left arm and leg was observed. The CSF study disclosed lymphocytic meningitis with negative findings on routine cultures. Angiography revealed diffuse segmental narrowing of multiple large and medium vessels in all the cerebral arteries. Results of an initial brain biopsy were negative, but at the postmortem examination there were multiple subacute and partially cavitated infarcts in both cerebral hemispheres involving the basal ganglia, internal capsule, subcortical white matter, cortices, and pontine tegmentum. Microscopic examination revealed multiple segments with fibrous intimal scarring and marked luminal narrowing. There were multinucleated cell infiltrates with multinucleated giant cells. All layers of the vessel walls were infiltrated by inflammatory cells and were focally necrotic. They could not find evidence of systemic vasculitis in any other organ. Cultures of the CSF sample and brain biopsy were positive for HIV-1, but 3 serum samples were negative for HIV by different techniques. Probably the patient had an acute HIV infection. This case is extremely similar to ours except in the moment when the vasculitis appeared.

View this table: [in this window] [in a new window] Cerebral Vasculitis in HIV-Infected Patients Not Associated With Infections or Tumoral Processes*

Vasculitis restricted to the CNS frequently has been observed in the setting of immunosuppressive or infectious illnesses. It is well described following herpes zoster ophthalmicus. In several reported cases, the clinical and histologic features of classic PACNS have been observed as an antecedent to herpes zoster infection. Thus, it should be not surprising to find that numerous case reports of PACNS associated with HIV infection could exist.¹⁹

The pathogenesis of the accepted cases of PACNS in HIV-infected patients described in the literature is largely speculative and may result from many different mechanisms, including infection of endothelial cells by HIV or other organisms, immune complex deposition, and impaired regulation of cytokines and adhesion molecules.³ Whether the retrovirus itself, some associated viral structure, or some unusual endothelial reaction to the virus and its products, the etiopathology of vasculitis has yet to be determined.

The method for diagnosing cerebral vasculitis in an HIV-infected patient should be to identify infective or neoplastic causes; however, if none are found, PACNS should be considered, just as it is in immunocompetent patients. The disease should be suspected if a patient has acute or subacute recurrent focal deficits sometimes in the presence of diffuse neurologic dysfunction, especially when abnormalities in the CSF are found and always after ruling out other causes. The combination of CSF analysis and MRI has a strong predictive value for a diagnosis that is later confirmed by angiography and brain biopsy specimens. Although magnetic resonance angiography has not been viewed until now as equivalent to conventional angiography for the detection of CNS vasculitis, the finding of vascular abnormalities in medium-sized vessels by magnetic resonance angiography, as occurred in our patient, may suggest the diagnosis and therefore could be useful whenever conventional angiography is not accessible.

The presence of HIV in the brain of the HIV-infected patients is currently evident, but clinically symptomatic cerebral primary vasculitis in these patients remains extremely rare. In primary HIV infection, it is not unusual to find evidence of neurologic manifestations, including acute meningitis. It seems that in these cases neurologic symptoms can have a strong correlation with HIV viral load in the CSF.²⁰ The CSF viral load in our patient could not be measured because this technique was not available in our setting when the patient was examined. Nevertheless, before the use of highly active antiretroviral therapy (HAART), patients used to have very high plasma and probably CSF viral loads, and most HIV carriers remained neurologically symptom free throughout their lives; therefore, the natural history of CNS changes in HIV infection still remains poorly understood.

Our patient died in 1997 before the widespread use of HAART. Because the mortality of HIV-infected patients has considerably decreased since the introduction of this therapy, an aggressive diagnostic approach to cerebral vasculitis in these patients must be undertaken. Ulterior therapeutic decisions should be individualized in each case. If HIV had a pathogenetic role in cerebral vasculitis in these patients, the good blood-brain barrier penetration of new antiretroviral therapies could be a good therapeutic approach for this process, because it occurs in HIV-associated dementia.

Author contributions: Study concept and design (Drs Nogueras, Sala, and Cervantes); acquisition of data (Drs Nogueras, Sala, Sasal, Garcia, and Bella); analysis and interpretation of data (Drs Nogueras, Sala, Sasal, Viñas, Garcia, and Bella); drafting of the manuscript (Drs Nogueras, Sasal, Garcia, and Bella); critical revision of the manuscript for important intellectual content (Drs Sala, Viñas, Cervantes, and Segura); administrative, technical, and material support (Drs Nogueras, Garcia, and Bella); study supervision (Drs Sala, Sasal, Viñas, Bella, and Cervantes).

We thank Isidre Ferrer, MD, from the Department of Neuropathology, Hospital de Bellvitge, Barcelona, Spain, for his expert opinion and Jose Luis Perez, PhD, from the Laboratory of Microbiology, Hospital de Bellvitge, Barcelona, Spain, for the PCR analysis of HIV in the brain tissues.

Corresponding author: Montserrat Sala, MD, Department of Internal Medicine, Corporació Sanitària Parc Taulí, Parc Taulí s/n, Sabadell, 08208 Barcelona, Spain (e-mail: msala{at}cspt.es).