A function-blocking CD47 antibody modulates extracellular vesicle-mediated intercellular signaling between breast carcinoma cells and endothelial cells

Kaur, Sukhbir; Elkahloun, Abdel G.; Singh, Satya P.; Arakelyan, Anush; Roberts, D. A.

doi:10.1007/s12079-017-0428-0

Cited by 28 publications

(29 citation statements)

References 80 publications

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“…All RNA samples were subjected to treatment with DNAse-1 prior to first strand cDNA synthesis according to the manufacturer's instructions (Thermo Fisher Scientific). Real-time PCR was performed using SYBR Green detection on a Bio-Rad CFX instrument as described previously (36).…”

Section: Methodsmentioning

confidence: 99%

Identification of Schlafen-11 as a Target of CD47 Signaling That Regulates Sensitivity to Ionizing Radiation and Topoisomerase Inhibitors

et al. 2019

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Knockdown or gene disruption of the ubiquitously expressed cell surface receptor CD47 protects non-malignant cells from genotoxic stress caused by ionizing radiation or cytotoxic chemotherapy but sensitizes tumors in an immune competent host to genotoxic stress. The selective radioprotection of non-malignant cells is mediated in part by enhanced autophagy and protection of anabolic metabolism pathways, but differential H2AX activation kinetics suggested that the DNA damage response is also CD47-dependent. A high throughput screen of drug sensitivities indicated that CD47 expression selectively sensitizes Jurkat T cells to inhibitors of topoisomerases, which are known targets of Schlafen-11 (SLFN11). CD47 mRNA expression positively correlated with schlafen-11 mRNA expression in a subset of human cancers but not the corresponding non-malignant tissues. CD47 mRNA expression was also negatively correlated with SLFN11 promoter methylation in some cancers. CD47 knockdown, gene disruption, or treatment with a CD47 function-blocking antibody decreased SLFN11 expression in Jurkat cells. The CD47 signaling ligand thrombospondin-1 also suppressed schlafen-11 expression in wild type but not CD47-deficient T cells. Re-expressing SLFN11 restored radiosensitivity to a CD47-deficient Jurkat cells. Disruption of CD47 in PC3 prostate cancer cells similarly decreased schlafen-11 expression and was associated with a CD47-dependent decrease in acetylation and increased methylation of histone H3 in the SLFN11 promoter region. The ability of histone deacetylase or topoisomerase inhibitors to induce SLFN11 expression in PC3 cells was lost when CD47 was targeted in these cells. Disrupting CD47 in PC3 cells increased resistance to etoposide but, in contrast to Jurkat cells, not to ionizing radiation. These data identify CD47 as a context-dependent regulator of SLFN11 expression and suggest an approach to improve radiotherapy and chemotherapy responses by combining with CD47-targeted therapeutics.

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Section: Methodsmentioning

confidence: 99%

Identification of Schlafen-11 as a Target of CD47 Signaling That Regulates Sensitivity to Ionizing Radiation and Topoisomerase Inhibitors

et al. 2019

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“…SIRP α binds to VEGF and immunoprecipitates with VEGFR2. CD47 antibody B6H12 downregulates VEGFR2 and SHP-2 phosphorylation [ 46 ] and CD47 binds SIRP α and TSP-1 to regulate the expression of VEGF and VEGFR2, thereby affecting the progression of atherosclerosis. Recent studies have shown that CD47 plays a role in atherosclerosis not through “cell aggregation” but through the dysregulation and activation of NK cells.…”

Section: The Influence Of Cd47 Signaling Pathway On the Formationmentioning

confidence: 99%

Recent Advancements in CD47 Signal Transduction Pathways Involved in Vascular Diseases

Dou

Chen

et al. 2020

BioMed Research International

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Cardiovascular and cerebrovascular diseases caused by atherosclerosis have a high disability rate and reduce the quality of life of the population. Therefore, understanding the mechanism of atherosclerosis and its control may interfere with the progression of atherosclerosis and thus control the occurrence of diseases closely related to atherosclerosis. TSP-1 is a factor that has been found to have an antiangiogenic effect, and CD47, as the receptor of TSP-1, can participate in the regulation of antiangiogenesis of atherosclerosis. VEGF is an important regulator of angiogenesis, and TSP-1/CD47 can cause VEGF and its downstream expression. Therefore, the TSP-1/CD47/VEGF/VEGFR2 signal may have an important influence on atherosclerosis. In addition, some inflammatory factors, such as IL-1 and NLRP3, can also affect atherosclerosis. This review will be expounded focusing on the pathogenesis and influencing factors of atherosclerosis.

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“…Other exosomal surface proteins such as CD47 may modulate the uptake process. For example, CD47, a thrombospondin 1 receptor, is present on the surface of EVs derived from Jurkat T cells and can alter gene expression and functional signaling in endothelial cells . Whether other microenvironmental factors modulate exosome uptake is largely unknown.…”

Section: Exosome Uptakementioning

confidence: 99%

Examining the Paracrine Effects of Exosomes in Cardiovascular Disease and Repair

Gartz

Strande

2018

JAHA

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A function-blocking CD47 antibody modulates extracellular vesicle-mediated intercellular signaling between breast carcinoma cells and endothelial cells

Cited by 28 publications

References 80 publications

Identification of Schlafen-11 as a Target of CD47 Signaling That Regulates Sensitivity to Ionizing Radiation and Topoisomerase Inhibitors

Identification of Schlafen-11 as a Target of CD47 Signaling That Regulates Sensitivity to Ionizing Radiation and Topoisomerase Inhibitors

Recent Advancements in CD47 Signal Transduction Pathways Involved in Vascular Diseases

Examining the Paracrine Effects of Exosomes in Cardiovascular Disease and Repair

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