AI Article Synopsis
- Many factors influence how fast HIV disease progresses, with the IL-7 receptor (IL-7R) being a crucial regulator of T cell balance.
- Research found that IL-7R expression is significantly lower in all T cell subsets of HIV-positive individuals compared to HIV-negative individuals, particularly in those with advanced disease.
- A decrease in IL-7R expression is linked to higher immune activation and lower CD4 counts, suggesting that the immune system's response in HIV may disrupt IL-7R expression, which is vital for T cell maintenance and memory.
Article Abstract
Many factors can influence the rate of HIV disease progression, including those that maintain T cell homeostasis. One key homeostatic regulator is the IL-7 receptor (IL-7R). Previous studies have shown IL-7R expression levels decrease in HIV infection, but effects on memory subtypes, CD4(+) T cells, and cell function have not been explored. The present study examined the expression of the IL-7Ralpha chain on naïve and memory T lymphocyte subsets of both HIV-positive and HIV-negative individuals from Nairobi, Kenya to assess the role of IL-7Ralpha in HIV disease. Expression of IL-7Ralpha was significantly reduced in all CD4(+) and CD8(+) T cell subsets in HIV-positive individuals. This reduction was further enhanced in those with advanced HIV progression. Expression of IL-7Ralpha was inversely correlated to immune activation, and apoptosis, and was positively correlated with CD4 count in both bivariate and multivariate analysis. Expression of IL-7Ralpha did not correlate with HIV viral loads, indicating the elevated immune activation seen in HIV-infected individuals may be impacting expression of IL-7Ralpha, independent of viral loads. Signaling via the IL-7R is essential for T cell homeostasis and maintenance of T cell memory. Reduction of this receptor may contribute to the homeostatic disruption seen in HIV.
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| http://dx.doi.org/10.1002/eji.200535111 | DOI Listing |
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