Spatial Network Mapping of Pulmonary Multidrug-Resistant Tuberculosis Cavities Using RNA Sequencing.
Keertan DhedaLaura LendersShashikant SrivastavaGesham MagombedzeHelen WainwrightPrithvi RajStephen J BushGabriele PollaraRachelle SteynMalika DavidsAnil PooranTimothy PennelAnthony LinegarRuth McNerneyLoven MoodleyJotam G PasipanodyaCarolin T TurnerMahdad NoursadeghiRobin M WarrenEdward WakelandTawanda GumboPublished in: American journal of respiratory and critical care medicine (2020)
Rationale: There is poor understanding about protective immunity and the pathogenesis of cavitation in patients with tuberculosis.Objectives: To map pathophysiological pathways at anatomically distinct positions within the human tuberculosis cavity.Methods: Biopsies were obtained from eight predetermined locations within lung cavities of patients with multidrug-resistant tuberculosis undergoing therapeutic surgical resection (n = 14) and healthy lung tissue from control subjects without tuberculosis (n = 10). RNA sequencing, immunohistochemistry, and bacterial load determination were performed at each cavity position. Differentially expressed genes were normalized to control subjects without tuberculosis, and ontologically mapped to identify a spatially compartmentalized pathophysiological map of the cavity. In silico perturbation using a novel distance-dependent dynamical sink model was used to investigate interactions between immune networks and bacterial burden, and to integrate these identified pathways.Measurements and Main Results: The median (range) lung cavity volume on positron emission tomography/computed tomography scans was 50 cm3 (15-389 cm3). RNA sequence reads (31% splice variants) mapped to 19,049 annotated human genes. Multiple proinflammatory pathways were upregulated in the cavity wall, whereas a downregulation "sink" in the central caseum-fluid interface characterized 53% of pathways including neuroendocrine signaling, calcium signaling, triggering receptor expressed on myeloid cells-1, reactive oxygen and nitrogen species production, retinoic acid-mediated apoptosis, and RIG-I-like receptor signaling. The mathematical model demonstrated that neuroendocrine, protein kinase C-θ, and triggering receptor expressed on myeloid cells-1 pathways, and macrophage and neutrophil numbers, had the highest correlation with bacterial burden (r > 0.6), whereas T-helper effector systems did not.Conclusions: These data provide novel insights into host immunity to Mycobacterium tuberculosis-related cavitation. The pathways defined may serve as useful targets for the design of host-directed therapies, and transmission prevention interventions.
Keyphrases
- mycobacterium tuberculosis
- computed tomography
- positron emission tomography
- multidrug resistant
- pulmonary tuberculosis
- hiv aids
- induced apoptosis
- endothelial cells
- dendritic cells
- single cell
- protein kinase
- drug resistant
- cell cycle arrest
- physical activity
- acute myeloid leukemia
- immune response
- cell proliferation
- genome wide
- regulatory t cells
- magnetic resonance
- machine learning
- high density
- high resolution
- escherichia coli
- gene expression
- gram negative
- oxidative stress
- pulmonary hypertension
- hiv infected
- emergency department
- contrast enhanced
- molecular docking
- endoplasmic reticulum stress
- solid phase extraction
- molecularly imprinted
- dna methylation
- genome wide analysis
- antiretroviral therapy
- deep learning
- pluripotent stem cells