4.5 Article

Interactive Effects of HIV Infection and Cannabis Use on Insula Subregion Functional Connectivity

Journal

JOURNAL OF NEUROIMMUNE PHARMACOLOGY
Volume 17, Issue 1-2, Pages 289-304

Publisher

SPRINGER
DOI: 10.1007/s11481-021-10005-8

Keywords

HIV; Cannabis; Insula; Functional connectivity; TNF- alpha; Inflammation

Funding

  1. National Institutes of Health (NIH) [K01DA037819, R01DA033156]
  2. Florida International University (FIU) Graduate School Dissertation Year Fellowship
  3. NIH [U54MD012393, R01DA041353]
  4. National Science Foundation (NSF) [1631325]
  5. Div Of Information & Intelligent Systems
  6. Direct For Computer & Info Scie & Enginr [1631325] Funding Source: National Science Foundation

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Chronic inflammation in the central nervous system is a mechanism by which HIV can lead to cognitive decline. The study examined the effects of HIV and cannabis on insular circuitry, cognition, and immune function, finding that cannabis may help normalize insula functioning among people living with HIV.
Chronic inflammation in the central nervous system is one mechanism through which human immunodeficiency virus (HIV) may lead to progressive cognitive decline. Given cannabis's (CB's) anti-inflammatory properties, use prevalence among people living with HIV (PLWH), and evidence implicating the insula in both, we examined independent and interactive effects of HIV and CB on insular circuitry, cognition, and immune function. We assessed resting-state functional connectivity (rsFC) of three insula subregions among 106 participants across four groups (co-occurring: HIV+/CB+; HIV-only: HIV+/CB-; CB-only: HIV-/CB+; controls: HIV-/CB-). Participants completed a neurocognitive battery assessing functioning across multiple domains and self-reported somatic complaints. Blood samples quantified immune function (T-cell counts) and inflammation (tumor necrosis factor alpha [TNF-alpha]). We observed interactive HIV x CB effects on rsFC strength between two anterior insula (aI) subregions and sensorimotor cortices such that, CB appeared to normalize altered rsFC among non-using PLWH. Specifically, compared to controls, HIV-only and CB-only groups displayed decreased dorsal anterior insula (DI) - postcentral gyrus rsFC and increased ventral anterior insula (VI) - supplementary motor area rsFC, whereas the co-occurring group displayed DI and VI rsFC more akin to that of controls. Altered DI - postcentral rsFC correlated with decreased processing speed and somatic complaints, but did not significantly correlate with inflammation (TNF-alpha). These outcomes implicate insula - sensorimotor neurocircuitries in HIV and CB and are consistent with prior work suggesting that CB use may normalize insula functioning among PLWH.

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