Cognitive Decline in HIV/AIDS Linked to Lipid Disorder

In the current study, published September 11 in Neurology, Haughey and colleagues enrolled 291 HIV-positive and 30 HIV-negative individuals to assess the correlation between CSF lipid content and ARV therapies with HAND progression. The longitudinal study was performed at seven U.S. sites, including ones in Hawaii and Puerto Rico, to ensure that the study population was diverse.

CSF was collected from each participant and evaluated for cholesterol and sphingomyelin concentrations. Cognitive impairment was measured by the Memorial Sloan-Kettering (MSK) Dementia Severity Scale. Participants were measured on all parameters at baseline and during a one-year follow-up.

ARV drug classes prescribed to treat HIV infection included protease inhibitors, nucleoside reverse transcriptase inhibitors (NRTIs), nonnucleoside reverse transcriptase inhibitors (NNRTIs), and integrase inhibitors.

At baseline, HIV-positive individuals could be distinguished from controls by elevated levels of CSF cholesterol, which was further increased by an average of 50 percent by ARV therapy—in particular, NRTIs and NNRTIs. There was no difference in overall MSK scale scores among subjects from baseline to follow-up.

At follow-up, elevation of a single sphingomyelin and reduction of cholesterol esters, a less water-soluble form of cholesterol, were predictive indicators for the onset of HAND in the HIV-infected cohort.

“This suggests that this dyslipidemia that occurs in the periphery may also occur in the central nervous system and seems to be related to a particular class of drugs,” said Haughey. He noted that NRTIs and NNRTIs are generally the first line of therapy for HIV viral suppression.

“Prior to ARV therapy, neurocognitive impairment occurred at a quicker rate and was very progressive. After ARV [therapies], there was still a forward progression, but it was milder,” he explained. “People are living longer, and impairment onset is variable.”

When asked about the clinical implications of his research, Haughey said, “It’s good to remember that rates of cognitive impairment [in HIV-infected individuals] are quite high. The rates of comorbid depression and other psychiatric disorders are also quite high, and sometimes it’s difficult to tease these conditions out. From our studies we hope to have a biomarker that can be identified very early in HIV [positive] subjects who seem perfectly normal by any cognitive test but whose lipid profiles indicate that they are at risk for cognitive impairment.”

“Neuroprotective therapy works best prior to neurocognitive damage….Several trials have failed trying to reverse it,” he concluded.

The study was funded by the National Institutes of Health. ■