CD47 Is Upregulated on Circulating Hematopoietic Stem Cells and Leukemia Cells to Avoid Phagocytosis

Jaiswal, Siddhartha; Jamieson, Catriona; Pang, Wendy W.; Park, Christopher Y.; Chao, Mark; Majeti, Ravindra; Traver, David; Rooijen, Nico van; Weissman, Irving L.

doi:10.1016/j.cell.2009.05.046

Cited by 1,287 publications

(1,185 citation statements)

References 40 publications

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“…However, when bone marrow HSCs were mobilized out of bone marrow, they upregulated CD47. 11 Ide et al 30 demonstrated that the overexpression of CD47 on donor cells or treatment of recipient mice with soluble CD47 enhanced the engraftment of xenogenic donor cells. This suggests that the overexpression of CD47 may be correlated with higher resistance to phagocytosis by macrophages.…”

Section: Discussionmentioning

confidence: 99%

“…Anti-CD47 monoclonal antibodies inhibiting the interaction of CD47 and SIRPa promote the phagocytosis of tumor cells by macrophages, and also by monocytes and neutrophils. [9][10][11] Cancer cells including acute myelogenous leukemias, 11,12 lymphomas, 13,14 and various solid cancers [15][16][17] express CD47 at a high level, and can be phagocytosed by macrophages in the presence of blocking antibodies to CD47. [11][12][13][14][15][16][17] In those cases where the tumor-initiating cells (or cancer stem cells) are known, for example, from acute myelogenous leukemias and bladder cancers, the tumor-initiating cells also upregulate CD47 expression, possibly to avoid phagocytosis.…”

Section: Introductionmentioning

confidence: 99%

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Anti-CD47 antibodies promote phagocytosis and inhibit the growth of human myeloma cells

et al. 2012

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Multiple myeloma is a plasma cell neoplasm residing in bone marrow. Despite advances in myeloma therapies, novel therapies are required to improve patient outcomes. CD47 is highly expressed on myeloma cells and a potential therapeutic candidate for myeloma therapies. Flow cytometric analysis of patient bone marrow cells revealed that myeloma cells overexpress CD47 when compared with non-myeloma cells in 73% of patients (27/37). CD47 expression protects cells from phagocytosis by transmitting an inhibitory signal to macrophages. Here we show that blocking CD47 with an anti-CD47 monoclonal antibody increased phagocytosis of myeloma cells in vitro. In xenotransplantation models, anti-CD47 antibodies inhibited the growth of RPMI 8226 myeloma cells and led to tumor regression (42/57 mice), implicating the eradication of myeloma-initiating cells. Moreover, anti-CD47 antibodies retarded the growth of patient myeloma cells and alleviated bone resorption in human bone-bearing mice. Irradiation of mice before myeloma cell xenotransplantation abolished the therapeutic efficacy of anti-CD47 antibodies delivered 2 weeks after radiation, and coincided with a reduction of myelomonocytic cells in spleen, bone marrow and liver. These results are consistent with the hypothesis that anti-CD47 blocking antibodies inhibit myeloma growth, in part, by increasing phagocytosis of myeloma cells.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Anti-CD47 antibodies promote phagocytosis and inhibit the growth of human myeloma cells

et al. 2012

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“…We realized that our AML LSC gene encoded a protein that is a "don't eat me" signal (226). We rapidly showed that CD47-negative HSCs cannot engraft in wild-type irradiated hosts (224). We found that normal HSCs mobilized by Cytoxan and G-CSF upregulated CD47 transiently, then extravasated into the bloodstream (224), whereupon they homed rapidly to the vascular sinusoids of bone marrow, spleen, and liver (224), presumably using integrin α 4 β 1 to bind luminal VCAM1, then followed their cell surface chemokine receptor CXCR4 and transmigrated across fields of perivascular sinusoidal macrophages to reach CXCL12-secreting niches (227)(228)(229)(230)(231).…”

Section: Cancer Stem Cells and The Therapeutics That Come From Themmentioning

confidence: 98%

“…We found that normal HSCs mobilized by Cytoxan and G-CSF upregulated CD47 transiently, then extravasated into the bloodstream (224), whereupon they homed rapidly to the vascular sinusoids of bone marrow, spleen, and liver (224), presumably using integrin α 4 β 1 to bind luminal VCAM1, then followed their cell surface chemokine receptor CXCR4 and transmigrated across fields of perivascular sinusoidal macrophages to reach CXCL12-secreting niches (227)(228)(229)(230)(231). Knockdown of leukemia cell CD47 led to their elimination by macrophages in vitro, and upon intravenous injection in vivo, they were removed by sinusoidal tissue macrophages (224). CD47-negative cell lines placed in vitro with macrophages usually are phagocytosed, whereas the same cells transfected with and expressing CD47 were not (224).…”

Section: Cancer Stem Cells and The Therapeutics That Come From Themmentioning

confidence: 99%

How One Thing Led to Another

Weissman

2016

Annu. Rev. Immunol.

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I started research in high school, experimenting on immunological tolerance to transplantation antigens. This led to studies of the thymus as the site of maturation of T cells, which led to the discovery, isolation, and clinical transplantation of purified hematopoietic stem cells (HSCs). The induction of immune tolerance with HSCs has led to isolation of other tissue-specific stem cells for regenerative medicine. Our studies of circulating competing germline stem cells in colonial protochordates led us to document competing HSCs. In human acute myelogenous leukemia we showed that all preleukemic mutations occur in HSCs, and determined their order; the final mutations occur in a multipotent progenitor derived from the preleukemic HSC clone. With these, we discovered that CD47 is an upregulated gene in all human cancers and is a “don't eat me” signal; blocking it with antibodies leads to cancer cell phagocytosis. CD47 is the first known gene common to all cancers and is a target for cancer immunotherapy.

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“…Tumor cells were shown to constitutively up-regulate CD47 expression in multiple tumor entities and animal models. Furthermore, over-expression of CD47 was a poor prognostic factor and correlated with increased pathogenicity [106][107][108][109][110]. Treatment of solid or hematopoietic tumors with either CD47-specific blocking antibodies or SIRPα-fusion proteins resulted in an increase in macrophage-dependent phagocytosis of tumor cells and a corresponding decrease in tumor size and number of metastases [107][108][109][110][111].…”

Section: Therapeutic Reprogramming Of Tumor-associated Macrophagesmentioning

confidence: 99%

Monocytes and Macrophages in Cancer: Development and Functions

Richards

Hettinger

Feuerer

2012

Cancer Microenvironment

163

121

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Monocytes and tumor-associated macrophages are part of the myeloid family, a group of hematopoietic derived cells. Monocytes are direct precursors of hematopoietic stem cell-derived macrophages. After their recruitment into the tumor tissue, they can differentiate into tumor-associated macrophages, a very heterogeneous cell population in terms of phenotype and pro-tumor function, supporting tumor initiation, local progression and distant metastasis. Therefore, targeting monocytes and macrophages is a promising immunotherapeutic approach. This review will focus on the development of monocytes as macrophage precursors, the functions of tumorassociated macrophages and the possibility of interfering with tumor development and progression by targeting these myeloid cells.

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CD47 Is Upregulated on Circulating Hematopoietic Stem Cells and Leukemia Cells to Avoid Phagocytosis

Cited by 1,287 publications

References 40 publications

Anti-CD47 antibodies promote phagocytosis and inhibit the growth of human myeloma cells

Anti-CD47 antibodies promote phagocytosis and inhibit the growth of human myeloma cells

How One Thing Led to Another

Monocytes and Macrophages in Cancer: Development and Functions

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