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Anti-CD47 Antibody Offers New Approaches to Cancer Therapy

Updated: 2015-09-01

Under normal physiological conditions, some types of phagocytes, such as macrophages, dendritic cells, and neutrophil granulocytes in our body play an important role in protecting our health by engulfing and digesting foreign substances, microbes, dead cells and cellular debris. They are working as brave soldiers. But every coin has two sides. These types of phagocytes are also dangerous due to the fact that they can be scavengers to engulf normal cells.

The phagocytosis of cells relies on a balance between pro-phagocytic (“eat me”) and anti-phagocytic (“don’t eat me”) signals on cell surface. Cluster of differentiation 47 (CD47), a member of the immunoglobulin superfamily, expresses on all cells. CD47 inhibits phagocytosis of cells by binding to its receptor, namely, signal regulatory protein α (SIRPα), which is expressed on phagocytes. Lacking in CD47 erythrocytes, platelets and lymphohematopoetic cells will result in a rapid clearance of these cells by macrophages. Abundant CD47 has also been observed on a variety of malignant cells, where elevated CD47 expression has predicted poor survival in individuals with cancer.

Many researchers have made great efforts on studying the therapeutic effects of anti-CD47 mAb over the years. However, the approach to cancer therapy of anti-CD47 mAb has not been demonstrated clearly. Recent studies in various preclinical xenografted models of human lymphoma revealed that the therapeutic effects of anti-human CD47 were macrophage dependent. However, these studies employed xenografted human tumors in T cell-deficient mice. Therefore, these studies cannot evaluate the role of adaptive immunity in the effectiveness of anti-CD47 mAb. It remains unclear whether anti-CD47 monoclonal antibody itself can activate the adaptive immunity response of the body.

In a new study published online by Nature Medicine on Sep 1st. 2015, entitled with“CD47 Blockade Triggers T Cell–Mediated Destruction of Immunogenic Tumors”, LIU Xiaojuan from Institute of Biophysics, CAS and Meng Xu from the University of Chicago, led by Professor. FU Yang-Xin revealed that the therapeutic effect of antibody mediated CD47 blockade in syngeneic tumor models largely depends on the activation of T cells.

In this study, it is revealed that the therapeutic effect of anti-CD47 mAb relies on a cytosolic DNA sensor, dendritic cells, type I/II interferons and CD8+ T cells and it is concluded that anti-CD47 mAb-mediated tumor rejection requires both innate and adaptive immune response. In addition, they find timely combination of conventional chemotherapeutics with immunotherapy of anti-CD47 mAb can boost the host response to control tumor growth.

“Liu et al evaluate CD47 antibody blockade in a proper model and reveal strong evidence of dentritic cells dependent adaptive T cell immunity in contrast to a large body of high impact publications suggesting CD47 blockade drives mainly a macrophage-dependent phagocytic anti-tumor mechanism.” “The findings of this manuscript are therefore potentially of high impact.”“The data are very strong and clear”, said the reviewers of international counterparts.

The study will yield important information for designing new treatment using anti-CD47 mAbs and also stress the importance using immunocompetent host harboring a syngeneic tumor for future cancer studies. With the development of antibody therapeutics in cancer, monoclonal antibodies have entered the mainstream of cancer therapy. Also with the beginning of human clinical trials of the anti-human CD47 cancer therapy in 2014, this ever more promising research result of anti-CD47 mAb will definitely give physicians indicators of how the treatment is working in patients.

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