An evolutionary recent IFN/IL-6/CEBP axis is linked to monocyte expansion and tuberculosis severity in humans.
Murilo DelgoboDaniel Agb MendesEdgar KozlovaEdroaldo Lummertz RochaGabriela F Rodrigues-LuizLucas MascarinGreicy DiasDaniel O PatrícioTim DierckxMaíra A BiccaGaëlle BrettonYonne Karoline Tenório de MenezesMárick R StarickDarcita RovarisJoanita Del MoralDaniel S MansurJohan Van WeyenberghAndré BáficaPublished in: eLife (2019)
Monocyte counts are increased during human tuberculosis (TB) but it has not been determined whether Mycobacterium tuberculosis (Mtb) directly regulates myeloid commitment. We demonstrated that exposure to Mtb directs primary human CD34+ cells to differentiate into monocytes/macrophages. In vitro myeloid conversion did not require type I or type II IFN signaling. In contrast, Mtb enhanced IL-6 responses by CD34+ cell cultures and IL-6R neutralization inhibited myeloid differentiation and decreased mycobacterial growth in vitro. Integrated systems biology analysis of transcriptomic, proteomic and genomic data of large data sets of healthy controls and TB patients established the existence of a myeloid IL-6/IL6R/CEBP gene module associated with disease severity. Furthermore, genetic and functional analysis revealed the IL6/IL6R/CEBP gene module has undergone recent evolutionary selection, including Neanderthal introgression and human pathogen adaptation, connected to systemic monocyte counts. These results suggest Mtb co-opts an evolutionary recent IFN-IL6-CEBP feed-forward loop, increasing myeloid differentiation linked to severe TB in humans.
Keyphrases
- mycobacterium tuberculosis
- dendritic cells
- pulmonary tuberculosis
- endothelial cells
- genome wide
- bone marrow
- acute myeloid leukemia
- peripheral blood
- single cell
- newly diagnosed
- magnetic resonance
- mesenchymal stem cells
- cell death
- induced apoptosis
- machine learning
- cell therapy
- big data
- cell cycle arrest
- drug induced
- patient reported