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Cancer immune checkpoint blockade therapy and its associated autoimmune cardiotoxicity
by
Wei-dong, Chen
, Jean Bustamante Alvarez
, Jia, Kelly
, Jiu-cheng Zhang
, He, Kai
, Shi, Lei
, Wang, Qiang
, Zhu, Hua
, Zou, Ning
in
Antitumor agents
/ Blocking antibodies
/ Cancer
/ Cardiotoxicity
/ Clinical trials
/ CTLA-4 protein
/ Cytotoxicity
/ Immune checkpoint
/ Immune checkpoint inhibitors
/ Immune response (cell-mediated)
/ Lymphocytes T
/ PD-1 protein
2018
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Cancer immune checkpoint blockade therapy and its associated autoimmune cardiotoxicity
by
Wei-dong, Chen
, Jean Bustamante Alvarez
, Jia, Kelly
, Jiu-cheng Zhang
, He, Kai
, Shi, Lei
, Wang, Qiang
, Zhu, Hua
, Zou, Ning
in
Antitumor agents
/ Blocking antibodies
/ Cancer
/ Cardiotoxicity
/ Clinical trials
/ CTLA-4 protein
/ Cytotoxicity
/ Immune checkpoint
/ Immune checkpoint inhibitors
/ Immune response (cell-mediated)
/ Lymphocytes T
/ PD-1 protein
2018
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Cancer immune checkpoint blockade therapy and its associated autoimmune cardiotoxicity
by
Wei-dong, Chen
, Jean Bustamante Alvarez
, Jia, Kelly
, Jiu-cheng Zhang
, He, Kai
, Shi, Lei
, Wang, Qiang
, Zhu, Hua
, Zou, Ning
in
Antitumor agents
/ Blocking antibodies
/ Cancer
/ Cardiotoxicity
/ Clinical trials
/ CTLA-4 protein
/ Cytotoxicity
/ Immune checkpoint
/ Immune checkpoint inhibitors
/ Immune response (cell-mediated)
/ Lymphocytes T
/ PD-1 protein
2018
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Cancer immune checkpoint blockade therapy and its associated autoimmune cardiotoxicity
Journal Article
Cancer immune checkpoint blockade therapy and its associated autoimmune cardiotoxicity
2018
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Overview
The immune checkpoint molecules are emerged in the evolution to protect the host from self-attacks by activated T cells. However, cancer cells, as a strategy to survive and expand, can hijack these molecules and mechanisms to suppress T cell-mediated immune responses. Therefore, an idea of blocking the checkpoint molecules to enhance the anti-tumor activities of the host immune system has been developed and applied to the cancer therapy after discovery of the inhibitory T cell co-receptor, cytotoxic T-lymphocyte associated protein 4 (CTLA-4), and further enhanced on the identification of PD-1 and its ligands. Since 2010, several checkpoint inhibitors have been approved by FDA and many more are in clinical trials. In the treatment of advanced cancers, these inhibitors significantly increased response rates and survival benefits. However, accompanied with the striking results, immune-related adverse events (irAEs) that broadly occurred in many organs were observed and reported, some of which were fatal. Herein, we first review the recent progressions in the research of the immune checkpoint molecules and the application of their blocking antibodies in cancer treatment, and then discuss the cardiac toxicity induced by the therapy and the strategy to monitor, manage this adverse event when it occurs.
Publisher
Nature Publishing Group
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