PLoS ONE (Jan 2012)

Hypoxia enhances the proliferative response of macrophages to CSF-1 and their pro-survival response to TNF.

  • John A Hamilton,
  • Derek C Lacey,
  • Amanda Turner,
  • Bernard de Kok,
  • Jennifer Huynh,
  • Glen M Scholz

DOI
https://doi.org/10.1371/journal.pone.0045853
Journal volume & issue
Vol. 7, no. 9
p. e45853

Abstract

Read online

In chronic inflammatory lesions there are increased numbers of macrophages with a possible contribution of enhanced survival/proliferation due, for example, to cytokine action; such lesions are often hypoxic. Prior studies have found that culture in low oxygen can promote monocyte/macrophage survival. We show here, using pharmacologic inhibitors, that the hypoxia-induced pro-survival response of macrophages exhibits a dependence on PI3-kinase and mTOR activities but surprisingly is suppressed by Akt and p38 MAPK activities. It was also found that in hypoxia at CSF-1 concentrations, which under normoxic conditions are suboptimal for macrophage proliferation, macrophages can proliferate more strongly with no evidence for alteration in CSF-1 receptor degradation kinetics. TNF promoted macrophage survival in normoxic conditions with an additive effect in hypoxia. The enhanced hypoxia-dependent survival and/or proliferation of macrophages in the presence of CSF-1 or TNF may contribute to their elevated numbers at a site of chronic inflammation.