Tetrahedral DNA Nanostructure with Interferon Stimulatory DNA Delivers Highly Potent Toxins and Activates the cGAS‐STING Pathway for Robust Chemotherapy and Immunotherapy

Zhang, Lingpu; Wang, Yuqi; Karges, Johannes; Tang, Dongsheng; Zhang, Hanchen; Zou, Kexuan; Song, Jie; Xiao, Haihua

doi:10.1002/adma.202210267

Cited by 41 publications

(33 citation statements)

References 45 publications

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“…To further investigate the effect of NP2+L on the release of DMAPs and DC maturation, BMDCs were extracted from mice, which were then co‐incubated with pretreated C4‐2 cells according to the previous report. [ 26 ] Subsequently, the DCs were examined and analyzed using flow cytometry. The results shown in Figure 5F,G demonstrated the highest percentage of DC maturation (CD80 + CD86 + ) was up to 40.5% caused by coincubation of BMDC with NP2+L‐pretreated tumor cells, which was 1.38 times higher than that caused by coincubation with NP2‐ pretreated tumor cells.…”

Section: Resultsmentioning

confidence: 99%

Polyphotosensitizer‐Based Nanoparticles with Michael Addition Acceptors Inhibiting GST Activity and Cisplatin Deactivation for Enhanced Chemotherapy and Photodynamic Immunotherapy

et al. 2023

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Glutathione S‐transferase (GST), which is a key enzyme in the conjugation reaction of glutathione (GSH), is overexpressed in cancer cells, leading to cisplatin deactivation and ultimately drug resistance. In addition, many tumors are immune “cold tumors,” limiting the application of immune checkpoint inhibitors. Herein, a reactive oxygen species (ROS)‐responsive polyphotosensitizer‐based nanoparticle (NP2) with Michael addition acceptors inhibiting GST activity and cisplatin deactivation is designed. Under the 808 nm light irradiation, on the one hand, the Michael addition acceptor in NP2 can react with GST and inhibit its activity, thereby decreasing the GSH conjugation and reducing the GSH‐mediated deactivation of cisplatin and improving its chemotherapeutic effect. On the other hand, NP2+L induces more ROS production in prostate tumor cells, which can further induce type II immunogenic cell death (ICD) and stimulate a stronger antitumor immune response. It is found that NP2 under the 808 nm light irradiation (NP2+L) can increase PD‐L1 expression on the surface of prostate cancer cells. Subsequently, NP2+L combined with PD‐L1 treatment is found to simultaneously enhance the efficacies of chemotherapy and photodynamic immunotherapy in prostate tumors, providing a new paradigm for the clinical multimodal treatment of tumors.

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Section: Resultsmentioning

confidence: 99%

Polyphotosensitizer‐Based Nanoparticles with Michael Addition Acceptors Inhibiting GST Activity and Cisplatin Deactivation for Enhanced Chemotherapy and Photodynamic Immunotherapy

et al. 2023

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“…In addition, this tetrahedron loaded with anticancer drug 56MESS was constructed to improve the efficacy of cancer treatment (Figure 3c). 100 Although cGAS-STING-mediated DNA sensing played an important role in mediating antitumor immunity, its working mechanism in T cells remained unclear. Based on this, Li et al studied the mechanism of how the cGAS-STING pathway maintained the stemness of CD8 + T cells and explored its potential in antitumor T cell therapy.…”

Section: Fna-based Regulation Of Antigen Capture and Presentation By ...mentioning

confidence: 99%

Functional Nucleic Acid-Based Immunomodulation for T Cell-Mediated Cancer Therapy

Wu,

Lin,

Ling

et al. 2023

ACS Nano

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T cell-mediated immunity plays a pivotal role in cancer immunotherapy. The anticancer actions of T cells are coordinated by a sequence of biological processes, including the capture and presentation of antigens by antigen-presenting cells (APCs), the activation of T cells by APCs, and the subsequent killing of cancer cells by activated T cells. However, cancer cells have various means to evade immune responses. Meanwhile, these vulnerabilities provide potential targets for cancer treatments. Functional nucleic acids (FNAs) make up a class of synthetic nucleic acids with specific biological functions. With their diverse functionality, good biocompatibility, and high programmability, FNAs have attracted widespread interest in cancer immunotherapy. This Review focuses on recent research progress in employing FNAs as molecular tools for T cell-mediated cancer immunotherapy, including corresponding challenges and prospects.

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“…Platinum anticancer drugs, such as cisplatin, oxaliplatin, and carboplatin, are the first-line anticancer alkylating agents in clinic practice [ 20 , 21 ]. These drugs can cause DNA damage and induce cell apoptosis by cross-linking with DNAs in cancer cells [ 22 , 23 ]. Unfortunately, the DNA repair machinary is powerful in cancer cells, resulting in resistance to platinum drugs [ 24 , 25 ].…”

Section: Introductionmentioning

confidence: 99%

Disulfide-containing polymer delivery of C527 and a Platinum(IV) prodrug selectively inhibited protein ubiquitination and tumor growth on cisplatin resistant and patient-derived liver cancer models

Shang

Zhang

et al. 2023

Materials Today Bio

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Tetrahedral DNA Nanostructure with Interferon Stimulatory DNA Delivers Highly Potent Toxins and Activates the cGAS‐STING Pathway for Robust Chemotherapy and Immunotherapy

Cited by 41 publications

References 45 publications

Polyphotosensitizer‐Based Nanoparticles with Michael Addition Acceptors Inhibiting GST Activity and Cisplatin Deactivation for Enhanced Chemotherapy and Photodynamic Immunotherapy

Polyphotosensitizer‐Based Nanoparticles with Michael Addition Acceptors Inhibiting GST Activity and Cisplatin Deactivation for Enhanced Chemotherapy and Photodynamic Immunotherapy

Functional Nucleic Acid-Based Immunomodulation for T Cell-Mediated Cancer Therapy

Disulfide-containing polymer delivery of C527 and a Platinum(IV) prodrug selectively inhibited protein ubiquitination and tumor growth on cisplatin resistant and patient-derived liver cancer models

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