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https://doi.org/10.3390/ijms22041626
Title: | Hiltonol Cocktail Kills Lung Cancer Cells by Activating Cancer-Suppressors, PKR/OAS, and Restraining the Tumor Microenvironment | Authors: | Chang, Shu-Chun Zhang, Bo-Xiang Su, Emily Chia-Yu Wu, Wei-Ciao Hsieh, Tsung-Han Salazar, Andres M Lin, Yen-Kuang Ding, Jeak Ling |
Keywords: | Science & Technology Life Sciences & Biomedicine Physical Sciences Biochemistry & Molecular Biology Chemistry, Multidisciplinary Chemistry NSCLC (non-small cell lung cancer) combinatorial treatment with Hiltonol(+++) cocktail [Hiltonol+anti-IL6+stattic+AG490] tumorigenic microenvironment anti and pro-tumorigenic cytokine production tumor-suppressors PKR (protein kinase R) and OAS (2′ 5′ oligoadenylate synthetase) |
Issue Date: | 1-Feb-2021 | Publisher: | MDPI | Citation: | Chang, Shu-Chun, Zhang, Bo-Xiang, Su, Emily Chia-Yu, Wu, Wei-Ciao, Hsieh, Tsung-Han, Salazar, Andres M, Lin, Yen-Kuang, Ding, Jeak Ling (2021-02-01). Hiltonol Cocktail Kills Lung Cancer Cells by Activating Cancer-Suppressors, PKR/OAS, and Restraining the Tumor Microenvironment. INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES 22 (4). ScholarBank@NUS Repository. https://doi.org/10.3390/ijms22041626 | Abstract: | NSCLC (non-small cell lung cancer) is a leading cause of cancer-related deaths worldwide. Clinical trials showed that Hiltonol, a stable dsRNA representing an advanced form of polyI:C (polyinosinic-polycytidilic acid), is an adjuvant cancer-immunomodulator. However, its mechanisms of action and effect on lung cancer have not been explored pre-clinically. Here, we examined, for the first time, how a novel Hiltonol cocktail kills NSCLC cells. By retrospective analysis of NSCLC patient tissues obtained from the tumor biobank; pre-clinical studies with Hiltonol alone or Hiltonol+++ cocktail [Hiltonol+anti-IL6+AG490 (JAK2 inhibitor)+Stattic (STAT3 inhibitor)]; cytokine analysis; gene knockdown and gain/loss-of-function studies, we uncovered the mechanisms of action of Hiltonol+++. We demonstrated that Hiltonol+++ kills the cancer cells and suppresses the meta-static potential of NSCLC through: (i) upregulation of pro-apoptotic Caspase-9 and Caspase-3, (ii) induction of cytosolic cytochrome c, (iii) modulation of pro-inflammatory cytokines (GRO, MCP-1, IL-8, and IL-6) and anticancer IL-24 in NSCLC subtypes, and (iv) upregulation of tumor suppres-sors, PKR (protein kinase R) and OAS (2′5′ oligoadenylate synthetase). In silico analysis showed that Lys296 of PKR and Lys66 of OAS interact with Hiltonol. These Lys residues are purportedly involved in the catalytic/signaling activity of the tumor suppressors. Furthermore, knockdown of PKR/OAS abrogated the anticancer action of Hiltonol, provoking survival of cancer cells. Ex vivo analysis of NSCLC patient tissues corroborated that loss of PKR and OAS is associated with cancer advancement. Altogether, our findings unraveled the significance of studying tumor biobank tis-sues, which suggests PKR and OAS as precision oncological suppressor candidates to be targeted by this novel Hiltonol+++ cocktail which represents a prospective drug for development into a potent and tailored therapy for NSCLC subtypes. | Source Title: | INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES | URI: | https://scholarbank.nus.edu.sg/handle/10635/193720 | ISSN: | 16616596 14220067 |
DOI: | 10.3390/ijms22041626 |
Appears in Collections: | Elements Staff Publications |
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