Date Published:
2014 Jan 02

Publication Type:
Journal Article

Authors:

S.M. Dever
B.N. Costin
R. Xu
N. El-Hage
J. Balinang
A. Samoshkin
M.A. O'Brien
M. McRae
L. Diatchenko
P.E. Knapp
K.F. Hauser

Secondary:
AIDS

Volume:
28

Pagination:
19-30

Issue:
1

PMID:
24413261

URL:
https://pubmed.ncbi.nlm.nih.gov/24413261

DOI:
10.1097/QAD.0000000000000113

Keywords:
AIDS Dementia Complex;External;HIV Infections;Humans;Protein Isoforms;Real-Time Polymerase Chain Reaction;Receptors, Opioid, mu;RNA Splicing

Abstract:
<p>OBJECTIVE: We previously examined the expression of specific C-terminal μ-opioid receptor (MOR) splice variants in human central nervous system cell types and HIV-infected brain tissue from individuals with neurocognitive impairment ± HIV encephalitis (HIVE). In the present study, we examined the N-terminal splice variant MOR-1K, which mediates excitatory cellular signaling.METHODS AND RESULTS: We found segregation of expression ranging from undetectable to seemingly exclusive across nervous system cell types compared to the pool of C-terminal MOR splice variants using the real-time polymerase chain reaction (RT-PCR). Expression of MOR-1K mRNA was also increased in HIV-infected individuals with combined neurocognitive impairment and HIVE compared with the other groups. MOR-1K expression correlated with the level of patient neurocognitive impairment, whereas the pool of C-terminal MOR splice variants did not. HIVE was also associated with increased expression of the inflammatory mediators MCP-1, MCP-2, and RANTES, but not the host HIV coreceptors CXCR4 and CCR5 or the CD4 receptor using qRT-PCR. Network analysis of microarray data from these same patients revealed filamin A (FLNA) as a possible interaction partner with MOR-1K, and FLNA gene expression was also found to be upregulated in HIVE using qRT-PCR. Overexpression of FLNA in HEK293 cells redistributed MOR-1K from intracellular compartments to the cell surface.CONCLUSION: These results suggest that HIVE, and neurocognitive impairment depending on its severity, are associated with enhanced MOR-1K signaling through both increased expression and trafficking to the cell surface, which may alter the contribution of MOR receptor isoforms and exacerbate the effects of MOR activation in neuroAIDS.</p>