Table 1.
Molecular factors cancer-specifically driving self-renewal of macrophages.
| Molecular Factor | Mechanism to Drive Macrophages Self-Renewal | References |
|---|---|---|
| CSF-1 | • ERK1/2 activation, inducing the activation of Ets transcription factors, thus increasing of cyclin-D expression. | [12,78]. |
| • ERK5 activation, downregulation of p21 expression and increased expression of Ets2 and Cyclin-D | [63] | |
| • KLF2 and KLF4 upregulation. | [13] | |
| • c-myc upregulation. | [13] | |
| IL-34 | • Partially affects TAMs proliferation through its ability to interact with CSF1R. | [99] |
| GM-CSF | • Activation of JAK2/STAT5 pathway. | [12,13,14] |
| • Activation of Bhlhe40/Bhlhe41 which inhibits c-Maf and Mafb transcription factors, thereby directly promoting expression of transcripts encoding cell cycle-related proteins. | [107,108] | |
| ADO-1 | • Working synergically with GM-CSF causes the upregulaion of PI3K/Akt and MEK/ERK signaling downstream of A2A activation. | [106] |
| • Promotes macrophage proliferation, in part, through the transcriptional regulation of A2A. | [106] | |
| IL-4 | • Induce the transcription of STAT6 and activates PI3K/AKT signaling. | [12] |
| • May stimulate macrophage proliferation in an Akt- and ACLY-dependent manner. | [109] |