The tumour microenvironment creates a niche for the self-renewal of tumour-promoting macrophages in colon adenoma

نویسندگان

  • Irene Soncin
  • Jianpeng Sheng
  • Qi Chen
  • Shihui Foo
  • Kaibo Duan
  • Josephine Lum
  • Michael Poidinger
  • Francesca Zolezzi
  • Klaus Karjalainen
  • Christiane Ruedl
چکیده

Circulating CCR2+ monocytes are crucial for maintaining the adult tissue-resident F4/80hiMHCIIhi macrophage pool in the intestinal lamina propria. Here we show that a subpopulation of CCR2-independent F4/80hiMHCIIlow macrophages, which are the most abundant F4/80hi cells in neonates, gradually decline in number in adulthood; these macrophages likely represent the fetal contribution to F4/80hi cells. In colon adenomas of ApcMin/+ mice, F4/80hiMHCIIlow macrophages are not only preserved, but become the dominant subpopulation among tumour-resident macrophages during tumour progression. Furthermore, these pro-tumoural F4/80hiMHCIIlow and F4/80hiMHCIIhi macrophages can self-renew in the tumour and maintain their numbers mostly independent from bone marrow contribution. Analyses of colon adenomas indicate that CSF1 may be a key facilitator of macrophage self-renewal. In summary, the tumour microenvironment creates an isolated niche for tissue-resident macrophages that favours macrophage survival and self-renewal.

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عنوان ژورنال:

دوره 9  شماره 

صفحات  -

تاریخ انتشار 2018