Ovid: Welcome to Ovid

Methotrexate selectively targets human proinflammatory macrophages through a thymidylate synthase/p53 axis.
Municio, Cristina; Soler Palacios, Blanca; Estrada-Capetillo, Lizbeth; Benguria, Alberto; Dopazo, Ana; Garcia-Lorenzo, Elena; Fernandez-Arroyo, Salvador; Joven, Jorge; Miranda-Carus, Maria Eugenia; Gonzalez-Alvaro, Isidoro; Puig-Kroger, Amaya
[Report] Annals of the Rheumatic Diseases. 75(12):2157-2165, December 2016.

(Format: HTML, PDF)

Objectives: Methotrexate (MTX) functions as an antiproliferative agent in cancer and an anti-inflammatory drug in rheumatoid arthritis (RA). Although macrophages critically contribute to RA pathology, their response to MTX remains unknown. As a means to identify MTX response markers, we have explored its transcriptional effect on macrophages polarised by GM-CSF (GM-MO) or M-CSF (M-MO), which resemble proinflammatory and anti-inflammatory macrophages found in RA and normal joints, respectively.

Methods: The transcriptomic profile of both human macrophage subtypes exposed to 50 nM of MTX under long-term and short-term schedules were determined using gene expression microarrays, and validated through quantitative real time PCR and ELISA. The molecular pathway involved in macrophage MTX-responsiveness was determined through pharmacological, siRNA-mediated knockdown approaches, metabolomics for polyglutamylated-MTX detection, western blot, and immunofluorescence on RA and normal joints.

Results: MTX exclusively modulated gene expression in proinflammatory GM-MO, where it influenced the expression of 757 genes and induced CCL20 and LIF at the mRNA and protein levels. Pharmacological and siRNA-mediated approaches indicated that macrophage subset-specific MTX responsiveness correlates with thymidylate synthase (TS) expression, as proinflammatory TS GM-MO are susceptible to MTX, whereas anti-inflammatory TSlow/- M-MO and monocytes are refractory to MTX. Furthermore, p53 activity was found to mediate the TS-dependent MTX-responsiveness of proinflammatory TS GM-MO. Importantly, TS and p53 were found to be expressed by CD163 /TNF[alpha] GM-CSF-polarised macrophages from RA joints but not from normal synovium.

Conclusions: Macrophage response to MTX is polarisation-dependent and determined by the TS-p53 axis. CCL20 and LIF constitute novel macrophage markers for MTX responsiveness in vitro.