NQO-1 Enzyme-Activated NIR Theranostic Agent for Pancreatic Cancer

Peng, Bo; Chen, Gang; Li, Yahui; Zhang, Hao; Shen, Jianliang; Hou, Ji-Ting; Li, Zhipeng

doi:10.1021/acs.analchem.2c01189

Cited by 14 publications

(7 citation statements)

References 42 publications

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“…Consistent with the results of in vitro experiments (Figure S22b), the ENBS plus irradiation group (20.3%) possessed the highest induction of DCs’ maturation compared to all other treatments (Figure a and Figure S31), which was 2.46- and 2.80-fold higher than that observed in the presence of the ENBS group (8.24%) and PBS group (7.26%), respectively. As is well-known, CD8 + cytotoxic T lymphocytes (CTLs) (CD8 + T cells) can kill cancer cells by releasing cytotoxins, which play essential roles in the antitumor immune response. − Moreover, helper T cells (CD4 + T cells) are critical in regulating adaptive immunity. , Therefore, the helper T cells (CD4 + ) and cytotoxic T cells (CD8 + ) in the spleen after different treatments were analyzed by flow cytometry (Figures S32–S33). As shown in Figure b-c, the ENBS-mediated treatment group significantly improved the proportion of CD4 + and CD8 + T cells.…”

Section: Resultsmentioning

confidence: 99%

“…69−72 Moreover, helper T cells (CD4 + T cells) are critical in regulating adaptive immunity. 38,39 Therefore, the helper T cells (CD4 + ) and cytotoxic T cells (CD8 + ) in the spleen after different treatments were analyzed by flow cytometry (Figures S32−S33). As shown in Figure 5b-c, the ENBS-mediated treatment group significantly improved the proportion of CD4 + and CD8 + T cells.…”

Section: ■ Results and Discussionmentioning

confidence: 99%

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Lysosome-Anchoring Activation Design of Type I Photosensitizer Evokes Pyroptosis and Antitumor Immunity

Li,

Gu,

Yang

et al. 2024

ACS Materials Lett.

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Pyroptosis, an inflammatory form of programmed cell death, has attracted growing attention as a promising pathway for cancer immunotherapy. However, few molecular design strategies with near-infrared (NIR) photoactivated pyroptosis inducers have been developed. Herein, a lysosome-targeted NIR type I photoinduced superoxide radical (O 2 −• ) generator (ENBS) that can evoke pyroptosis and antitumor immunity was presented here for the first time. In this work, ENBS not only selectively accumulates in lysosomes and disrupts the integrity of lysosomes but also induces gasdermin D (GSDMD) mediated pyroptosis. As a result, it finally promotes the maturation of dendritic cells (DCs), achieving T-cell-mediated immune activation in vivo. To the best of our knowledge, this is the first example of an NIR photoactivated superoxide radical pyroptosis generator-based immunotherapy system through the caspase-1/GSDMD pathway, anticipated to provide valuable guidelines for pyroptosismediated cancer immunotherapy.

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Section: Resultsmentioning

confidence: 99%

Section: ■ Results and Discussionmentioning

confidence: 99%

Lysosome-Anchoring Activation Design of Type I Photosensitizer Evokes Pyroptosis and Antitumor Immunity

Li,

Gu,

Yang

et al. 2024

ACS Materials Lett.

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“…In studies related to PAAD, Cui et al that MST1 inhibits pancreatic cancer progression via ROS-induced pyroptosis (56). Peng et al showed that ICy OH produced by ICy Q could damage mitochondrial membranes, induce intracellular inflammatory responses, and selectively induce pancreatic cancer cell death via the cell pyroptosis pathway (a series of enzymatic reactions leading to the production of fragments of pyroptosis protein GSDMD-N) (57).…”

Section: Discussionmentioning

confidence: 99%

Construction and comprehensive analysis of a novel prognostic signature associated with pyroptosis molecular subtypes in patients with pancreatic adenocarcinoma

Huang

Peng

et al. 2023

Front. Immunol.

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BackgroundTreatment of cancer with pyroptosis is an emerging strategy. Molecular subtypes based on pyroptosis-related genes(PRGs) seem to be considered more conducive to individualized therapy. It is meaningful to construct a pyroptosis molecular subtypes-related prognostic signature (PMSRPS) to predict the overall survival (OS) of patients with pancreatic adenocarcinoma(PAAD) and guide treatment.MethodsBased on the transcriptome data of 23 PRGs, consensus clustering was applied to divide the TCGA and GSE102238 combined cohort into three PRGclusters. Prognosis-related differentially expressed genes(DEGs) among PRGclusters were subjected to LASSO Cox regression analysis to determine a PMSRPS. External cohort and in vitro experiments were conducted to verify this PMSRPS. The CIBERSORT algorithm, the ESTIMATE algorithm and the Immunophenoscore (IPS) were used to analyze the infiltrating abundance of immune cells, the tumor microenvironment (TME), and the response to immunotherapy, respectively. Wilcoxon analysis was used to compare tumor mutational burden (TMB) and RNA stemness scores (RNAss) between groups. RT-qPCR and in vitro functional experiments were used for evaluating the expression and function of SFTA2.ResultsBased on three PRGclusters, 828 DEGs were obtained and a PMSRPS was subsequently constructed. In internal and external validation, patients in the high-risk group had significantly lower OS than those in the low-risk group and PMSRPS was confirmed to be an independent prognostic risk factor for patients with PAAD with good predictive performance. Immune cell infiltration abundance and TME scores indicate patients in the high-risk group have typical immunosuppressive microenvironment characteristics. Analysis of IPS suggests patients in the high-risk group responded better to novel immune checkpoint inhibitors (ICIs) than PD1/CTLA4. The high-risk group had higher TMB and RNAss. In addition, 10 potential small-molecule compounds were screened out. Finally, we found that the mRNA expression of SFTA2 gene with the highest risk coefficient in PMSRPS was significantly higher in PAAD than in paracancerous tissues, and knockdown of it significantly delayed the progression of PAAD.ConclusionsPMSRPS can well predict the prognosis, TME and immunotherapy response of patients with PAAD, identify potential drugs, and provide treatment guidance based on individual needs.

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“…This advanced imaging modality can efficiently detect ONOO À in situ in vivo, while simultaneously offering benefits such as high sensitivity, non-invasiveness, ease of operation, excellent selectivity, and high efficiency. [26][27][28][29][30] In light of these advantages, we intend to design and synthesize a stable fluorescence sensor that can precisely and exclusively identify ONOO À in living cells, tissues, or organisms.…”

Section: Introductionmentioning

confidence: 99%

Shedding light on ONOO⁻ detection: the emergence of a fast-response fluorescent probe for biological systems

Wu,

Li,

Huang

et al. 2024

J. Mater. Chem. B

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NQO-1 Enzyme-Activated NIR Theranostic Agent for Pancreatic Cancer

Cited by 14 publications

References 42 publications

Lysosome-Anchoring Activation Design of Type I Photosensitizer Evokes Pyroptosis and Antitumor Immunity

Lysosome-Anchoring Activation Design of Type I Photosensitizer Evokes Pyroptosis and Antitumor Immunity

Construction and comprehensive analysis of a novel prognostic signature associated with pyroptosis molecular subtypes in patients with pancreatic adenocarcinoma

Shedding light on ONOO⁻ detection: the emergence of a fast-response fluorescent probe for biological systems

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NQO-1 Enzyme-Activated NIR Theranostic Agent for Pancreatic Cancer

Cited by 14 publications

References 42 publications

Lysosome-Anchoring Activation Design of Type I Photosensitizer Evokes Pyroptosis and Antitumor Immunity

Lysosome-Anchoring Activation Design of Type I Photosensitizer Evokes Pyroptosis and Antitumor Immunity

Construction and comprehensive analysis of a novel prognostic signature associated with pyroptosis molecular subtypes in patients with pancreatic adenocarcinoma

Shedding light on ONOO− detection: the emergence of a fast-response fluorescent probe for biological systems

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Shedding light on ONOO⁻ detection: the emergence of a fast-response fluorescent probe for biological systems