2015
DOI: 10.1073/pnas.1424907112
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Macrophages eat cancer cells using their own calreticulin as a guide: Roles of TLR and Btk

Abstract: Macrophage-mediated programmed cell removal (PrCR) is an important mechanism of eliminating diseased and damaged cells before programmed cell death. The induction of PrCR by eat-me signals on tumor cells is countered by don’t-eat-me signals such as CD47, which binds macrophage signal-regulatory protein α to inhibit phagocytosis. Blockade of CD47 on tumor cells leads to phagocytosis by macrophages. Here we demonstrate that the activation of Toll-like receptor (TLR) signaling pathways in macrophages synergizes w… Show more

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Cited by 227 publications
(216 citation statements)
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“…All MDS that transition to AML upregulate CD47, so we conceivably have a roadmap for the development of MDS and its progression to AML. We and others have recently addressed the biochemical pathway for secreted calreticulin, in our studies in macrophages that can deposit calrecticulin on the surface of cancer cells lacking a calreticulin message (234). In these macrophages, stimulation of TLR3, 4, or 7 leads to phosphorylation and activation of BTK, which in turn leads to the phosphorylation of endoplasmic reticulum (ER)-resident calreticulin (234).…”
Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning
confidence: 98%
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“…All MDS that transition to AML upregulate CD47, so we conceivably have a roadmap for the development of MDS and its progression to AML. We and others have recently addressed the biochemical pathway for secreted calreticulin, in our studies in macrophages that can deposit calrecticulin on the surface of cancer cells lacking a calreticulin message (234). In these macrophages, stimulation of TLR3, 4, or 7 leads to phosphorylation and activation of BTK, which in turn leads to the phosphorylation of endoplasmic reticulum (ER)-resident calreticulin (234).…”
Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning
confidence: 98%
“…Anti-CD47 antibodies that block CD47-Sirpα interactions cause the tumor cells to be phagocytosed, and killed intracellularly (232). Antibody-blocked CD47 + Jurkat lymphoma cells are phagocytosed, whereas most normal blood and tissue cells that are CD47 + are not, presumably because most normal cells lack programmed cell removal via "eat me" signals (233,234).…”
Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning
confidence: 99%
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