Near-Death Cells Cause Chemotherapy-Induced Metastasis via ATF4-Mediated NF-κB Signaling Activation.
Chenchen ZhuPei LiuChuan-Yuan LiYuli ZhangJiang YinLinlin HouGuopei ZhengXinjian LiuPublished in: Advanced science (Weinheim, Baden-Wurttemberg, Germany) (2023)
Cytotoxic chemotherapy is a primary treatment modality for many patients with advanced cancer. Increasing preclinical and clinical observations indicate that chemotherapy can exacerbate tumor metastasis. However, the underlying mechanism remains unclear. Here, it is attempted to identify the mechanisms underlying chemotherapy-induced cancer recurrence and metastasis. It is revealed that a small subpopulation of "near-death cells" (NDCs) with compromised plasma membranes can reverse the death process to enhance survival and repopulation after exposure to lethal doses of cytotoxins. Moreover, these NDCs acquire enhanced tumorigenic and metastatic capabilities, but maintain chemosensitivity in multiple models. Mechanistically, cytotoxin exposure induces activating transcription factor 4 (ATF4)-dependent nonclassical NF-κB signaling activation; ultimately, this results in nuclear translocation of p52 and RelB in NDCs. Deletion of ATF4 in parental cancer cells significantly reduces colony formation and metastasis of NDCs, whereas overexpression of ATF4 activates the nonclassical NF-κB signaling pathway to promote chemotherapy-induced metastasis of NDCs. Overall, these results provide novel mechanistic insights into the chemotherapy-induced metastasis and indicate the pivotal role of NDCs in mediating tumor relapse after cytotoxic therapy. This study also suggests that targeting ATF4 may be an effective approach in improving the efficacy of chemotherapy.
Keyphrases
- chemotherapy induced
- transcription factor
- signaling pathway
- induced apoptosis
- endoplasmic reticulum stress
- pi k akt
- advanced cancer
- squamous cell carcinoma
- oxidative stress
- palliative care
- dna binding
- nuclear factor
- cell proliferation
- free survival
- epithelial mesenchymal transition
- immune response
- stem cells
- toll like receptor
- single cell
- papillary thyroid
- young adults
- replacement therapy
- smoking cessation
- genome wide identification