4.6 Article

Cordycepin Sensitizes Cholangiocarcinoma Cells to Be Killed by Natural Killer-92 (NK-92) Cells

期刊

MOLECULES
卷 26, 期 19, 页码 -

出版社

MDPI
DOI: 10.3390/molecules26195973

关键词

cordycepin; sensitization; immunomodulation; NK cell-based immunotherapy; cholangiocarcinoma; cancer treatment

资金

  1. Center of Excellence on Medical Biotechnology (CEMB) [CB-61-006-03]
  2. The S&T Postgraduate Education and Research Development Office (PERDO), The Commission on Higher Education (CHE), Thailand
  3. Research Center in Bioresources for Agriculture, Industry and Medicine, Chiang Mai University

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Immunotherapy utilizing immune functions is a promising strategy for cancer treatment, and the bioactive compound cordycepin has been shown to enhance the susceptibility of cancer cells to NK cell cytotoxicity, possibly through the TRAIL signaling pathway. This study provides evidence that cordycepin can sensitize cancer cells to NK cell cytotoxicity, supporting its potential as an alternative immunomodulating agent.
Immunotherapy harnessing immune functions is a promising strategy for cancer treatment. Tumor sensitization is one approach to enhance tumor cell susceptibility to immune cell cytotoxicity that can be used in combination with immunotherapy to achieve therapeutic efficiency. Cordycepin, a bioactive compound that can be extracted from some Cordyceps spp. has been reported to effectively inhibit tumor growth, however, the mechanism of its tumor sensitization activity that enhances immune cell cytotoxicity is unknown. In the present study, we investigated the potency of cordycepin to sensitize a lethal cancer, cholangiocarcinoma (CCA), to natural killer (NK) cells. Treatment with cordycepin prior to and during co-culturing with NK-92 cells significantly increased cell death of KKU-213A as compared to solitary cordycepin or NK treatment. Moreover, sensitization activity was also observed in the combination of NK-92 cells and Cordyceps militaris extract that contained cordycepin as a major component. The cordycepin treatment remarkably caused an increase in TRAIL receptor (DR4 and DR5) expression in KKU-213A, suggesting the possible involvement of TRAIL signaling in KKU-213A sensitization to NK-92 cells. In conclusion, this is the first report on the sensitization activity of cordycepin on CCA cells to NK cytotoxicity, which supports that cordycepin can be further developed as an alternate immunomodulating agent.

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