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Inhibition of DNA methylation promotes breast tumor sensitivity to netrin-1 interference. | LitMetric

AI Article Synopsis

  • NTN1 upregulation in some human cancers prevents programmed cell death (apoptosis) through its dependence receptors DCC and UNC5H, aiding tumor growth.
  • In many breast tumors, DNA methylation leads to decreased expression of NTN1 and DAPK1, which are critical for apoptosis, suggesting a link between methylation and tumor survival.
  • Combining DNA methylation-inhibiting drugs like decitabine with strategies that silence NTN1 or neutralize netrin-1 enhances cancer cell death and could be a promising approach for cancer treatment.

Article Abstract

In a number of human cancers, NTN1 upregulation inhibits apoptosis induced by its so-called dependence receptors DCC and UNC5H, thus promoting tumor progression. In other cancers however, the selective inhibition of this dependence receptor death pathway relies on the silencing of pro-apoptotic effector proteins. We show here that a substantial fraction of human breast tumors exhibits simultaneous DNA methylation-dependent loss of expression of NTN1 and of DAPK1, a serine threonine kinase known to transduce the netrin-1 dependence receptor pro-apoptotic pathway. The inhibition of DNA methylation by drugs such as decitabine restores the expression of both NTN1 and DAPK1 in netrin-1-low cancer cells. Furthermore, a combination of decitabine with NTN1 silencing strategies or with an anti-netrin-1 neutralizing antibody potentiates tumor cell death and efficiently blocks tumor growth in different animal models. Thus, combining DNA methylation inhibitors with netrin-1 neutralizing agents may be a valuable strategy for combating cancer.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4967941PMC
http://dx.doi.org/10.15252/emmm.201505945DOI Listing

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