4.5 Article

CD163L1 and CLEC5A discriminate subsets of human resident and inflammatory macrophages in vivo

Journal

JOURNAL OF LEUKOCYTE BIOLOGY
Volume 98, Issue 4, Pages 453-466

Publisher

FEDERATION AMER SOC EXP BIOL
DOI: 10.1189/jlb.3HI1114-531R

Keywords

myeloid subsets; polarization; inflammation; cancer

Funding

  1. SEP-CONACYT (Mexico) [179388]
  2. Ministerio de Economia y Competitividad (Spain) [SAF2011-23801]
  3. Instituto de Salud Carlos III [PI13/01454]
  4. CONACYT predoctoral scholarship [302832, 322167]

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Macrophages (M phi) can be differentiated and polarized in vitro from human CD14(+) monocytes under the influence of GM-CSF (GM-M phi) and M-CSF (M-M phi). GM-M phi s are proinflammatory and M-M phi s have an anti-inflammatory phenotype. We found selective expression of the lectin C-type lectin domain family 5 member A (CLEC5A) transcripts in GM-M phi s and the scavenger receptor CD163 molecule-like 1 (CD163L1) in M-M phi s bymicroarray assay. In vitro, CD163L1 expression was induced by IL-10 and M-CSF and CLEC5A by inflammatory cytokines and cell adherence. In secondary lymphoid organs, their respective expression was restricted to CD68(+)/CD163(+) M phi s that preferentially produced either TNF (CLEC5A(+)) or IL-10 (CD163L1(+)). Mfs from healthy liver and colon tissue were mostly CD163L1(+), and CLEC5A(+) cells were scarce. In contrast, CLEC5A(+) M phi s were abundant in the intestinal lamina propria from patients with inflammatory bowel disease (IBD), with higher numbers of CLEC5A(+)CD163L1(+) found compared with those in secondary lymphoid organs. CLEC5A(+) cells were CD14(+)CD209(-)CD11b(+)CD11c(+)TNF(+)IL-10(+), and single positive CD163L1(+) cells were CD14(-)CD209(+)CD11b(-)CD11c(-)TNF(-)IL-10(+) in healthy donors and had lost the ability to produce IL-10 and to express CD209 in those with IBD. In melanomas, CLEC5A(+) tumor-associated M phi s (TAMs) were not detected in 42% of the cases evaluated, but CD163L1(+) TAMs were found in 100%. Similar to IBD, CD163L1(+) TAMs expressed high levels of CD209 and produced significant amounts of IL-10, and CLEC5A(+) TAMs were CD14(hi) and produced enhanced levels of TNF in metastases. Overall, these results suggest that CD163L1 expression is associated with tissue-resident M phi s with an anti-inflammatory or anergic phenotype and that CLEC5A(+) M phi s exhibit TNF-producing ability and might display a proinflammatory effect.

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