Elevated Basal Pre-infection CXCL10 in Plasma and in the Small Intestine after Infection Are Associated with More Rapid HIV/SIV Disease Onset.
Mickaël J PloquinYoann MadecArmanda CasrougeNicolas HuotCaroline PassaesCamille LécurouxAsma EssatFaroudy BoufassaBéatrice JacquelinSimon P JochemsGaël PetitjeanMathieu AnginKathleen GärtnerThalía Garcia-TellezNicolas NoelThijs BooimanBrigitte D Boeser-NunninkPierre RoquesAsier Saez-CirionBruno VaslinNathalie Dereudre-BosquetFrançoise Barré-SinoussiMathilde GhislainChristine RouziouxOlivier LambotteMatthew L AlbertCécile GoujardNeeltje KootstraLaurence MeyerMichaela C Müller-TrutwinPublished in: PLoS pathogens (2016)
Elevated blood CXCL10/IP-10 levels during primary HIV-1 infection (PHI) were described as an independent marker of rapid disease onset, more robust than peak viremia or CD4 cell nadir. IP-10 enhances the recruitment of CXCR3+ cells, which include major HIV-target cells, raising the question if it promotes the establishment of viral reservoirs. We analyzed data from four cohorts of HIV+ patients, allowing us to study IP-10 levels before infection (Amsterdam cohort), as well as during controlled and uncontrolled viremia (ANRS cohorts). We also addressed IP-10 expression levels with regards to lymphoid tissues (LT) and blood viral reservoirs in patients and non-human primates. Pre-existing elevated IP-10 levels but not sCD63 associated with rapid CD4 T-cell loss upon HIV-1 infection. During PHI, IP-10 levels and to a lesser level IL-18 correlated with cell-associated HIV DNA, while 26 other inflammatory soluble markers did not. IP-10 levels tended to differ between HIV controllers with detectable and undetectable viremia. IP-10 was increased in SIV-exposed aviremic macaques with detectable SIV DNA in tissues. IP-10 mRNA was produced at higher levels in the small intestine than in colon or rectum. Jejunal IP-10+ cells corresponded to numerous small and round CD68neg cells as well as to macrophages. Blood IP-10 response negatively correlated with RORC (Th17 marker) gene expression in the small intestine. CXCR3 expression was higher on memory CD4+ T cells than any other immune cells. CD4 T cells from chronically infected animals expressed extremely high levels of intra-cellular CXCR3 suggesting internalization after ligand recognition. Elevated systemic IP-10 levels before infection associated with rapid disease progression. Systemic IP-10 during PHI correlated with HIV DNA. IP-10 production was regionalized in the intestine during early SIV infection and CD68+ and CD68neg haematopoietic cells in the small intestine appeared to be the major source of IP-10.
Keyphrases
- antiretroviral therapy
- induced apoptosis
- hiv positive
- hiv infected
- gene expression
- human immunodeficiency virus
- hepatitis c virus
- hiv testing
- hiv aids
- end stage renal disease
- oxidative stress
- newly diagnosed
- poor prognosis
- ejection fraction
- single cell
- stem cells
- chronic kidney disease
- mesenchymal stem cells
- cell therapy
- cell death
- signaling pathway
- artificial intelligence
- working memory
- cell free
- nk cells
- cell migration
- induced pluripotent stem cells