A Totipotent “All‐In‐One” Peptide Sequentially Blocks Immune Checkpoint and Reverses the Immunosuppressive Tumor Microenvironment

Zhang, Limin; Jiang, Zhenqi; Yang, Xi; Qian, Yixia; Wang, Minxuan; Wu, Shang Yin; Li, Lingyun; Jia, Fu; Wang, Zihua; Hu, Zhiyuan; Zhao, Minzhi; Tang, Xiaoying; Li, Gang; Shang, Haitao; Chen, Xiaoyuan; Wang, Weizhi

doi:10.1002/adma.202207330

Cited by 16 publications

(15 citation statements)

References 66 publications

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“…On the other hand, dual-signal detection provides complementary information to avoid false positive signals and environmental interference. 42,43 As shown in Figure 4A,B,D, after treatment with various concentrations of trypsin, the color and absorption/fluorescence spectra of the BSA-mediated AgNT biosensors were consistent with the above-mentioned thiolated-mediated change in AgNTs. However, the response in color change, the LSPR peak shift, and fluorescence intensity in the samples with pepsin treatment were completely opposite to the experiments within trypsin (Figure S4).…”

Section: Roles Of Thiolated Biomolecules As Etching Agents In the Etc...supporting

confidence: 77%

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Dual-Functional Capping Agent-Mediated Transformation of Silver Nanotriangles to Silver Nanoclusters for Dual-Mode Biosensing

et al. 2023

Anal. Chem.

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The localized surface plasmon resonance (LSPR) property, depending on the structure (morphology and assembly) of nanoparticles, is very sensitive to the environmental fluctuation. Retaining the colorimetric effect derived from the LSPR property while introducing new optical properties (such as fluorescence) that provide supplementary information is an effective means to improve the controllability in structures and reproducibility in optical properties. DNA as a green and low-cost etching agent has been demonstrated to effectively control the morphology and optical properties (the blue shift of the LSPR peak) of the plasmonic nanoparticles. Herein, taking silver nanotriangles (AgNTs) as a proof of concept, we report a novel strategy to induce precisely tunable LSPR and fluorescence-composited dual-mode signals by using mono-DNA first as an etching agent for etching the morphology of AgNTs and later as a template for synthesizing fluorescent silver nanoclusters (AgNCs). In addition, common templates for synthesizing AgNCs, such as L-glutathione and bovine serum albumin, were demonstrated to have the capability to serve as etching agents. More importantly, these biomolecules as dualfunctional capping agents (etching agents and templates) follow the size-dependent rule: as the size of the thiolated biomolecule increases, the blue shift of the LSPR peak increases; at the same time, the fluorescence intensity increases. The enzyme that can change the molecular weight (size) of the biomolecular substrates (DNA, peptides, and proteins) through an enzymatic cleavage reaction was explored to regulate the LSPR and fluorescent properties of the resulting nanoparticles (by etching of AgNTs and synthesis of AgNCs), achieving excellent performance in detection of cancer-related proteases. This study can be expanded to other biopolymers to impact both fundamental nanoscience and applications and provide powerful new tools for bioanalytical biosensors and nanomedicine.

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Section: Roles Of Thiolated Biomolecules As Etching Agents In the Etc...supporting

confidence: 77%

“…On the one hand, the robust response signal from the BSA-mediated sensing strategy could be read by the naked eye under ambient conditions. On the other hand, dual-signal detection provides complementary information to avoid false positive signals and environmental interference. , …”

Section: Resultsmentioning

confidence: 99%

Dual-Functional Capping Agent-Mediated Transformation of Silver Nanotriangles to Silver Nanoclusters for Dual-Mode Biosensing

et al. 2023

Anal. Chem.

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“…Researchers created TPA, a combined targeted peptide that inhibited the PD-1/PD-L1 axis, activated p53, and showed tumor killing and immunotherapeutic sensitization effects on a humanized PBMCengrafted PDX model. There is now a potential pathway for the development of self-assembled peptide drugs for cancer therapy (105). For tumor targeting, the researchers synthesized size-tunable nanostructures with a spherical morphology by combining partially reductive HSA with hydrophobic Fluvastatin, known as According to the study, these nanodrugs effectively enhanced the potency of Anti-PD1 antibodies against colon cancer in a humanized CRC-PDX mouse model while maintaining acceptable levels of safety (100).…”

Section: Oncolytic Virusesmentioning

confidence: 99%

Patient-derived xenografts or organoids in the discovery of traditional and self-assembled drug for tumor immunotherapy

Zhang

Zheng

2023

Front. Oncol.

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In addition to the rapid development of immune checkpoint inhibitors, there has also been a surge in the development of self-assembly immunotherapy drugs. Based on the immune target, traditional tumor immunotherapy drugs are classified into five categories, namely immune checkpoint inhibitors, direct immune modulators, adoptive cell therapy, oncolytic viruses, and cancer vaccines. Additionally, the emergence of self-assembled drugs with improved precision and environmental sensitivity offers a promising innovation approach to tumor immunotherapy. Despite rapid advances in tumor immunotherapy drug development, all candidate drugs require preclinical evaluation for safety and efficacy, and conventional evaluations are primarily conducted using two-dimensional cell lines and animal models, an approach that may be unsuitable for immunotherapy drugs. The patient-derived xenograft and organoids models, however, maintain the heterogeneity and immunity of the pathological tumor heterogeneity.

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Section: Targeting Peptide Design and Screeningmentioning

confidence: 99%

“…In the TME, TAP can transform into α-helical structures and assemble into dense nanofibers under the recruitment of PD-L1, thus blocking the PD-1/PD-L1 axis. After entering the tumor cells, it blocks the formation of the Rbm38-eIF4E complex, thus upregulating p53 (Figure c) . It should be noted that the α-helical entropy value is low and the hydrogen-bonding network is blocked inside the peptide, leading to its poor stability.…”

Section: Targeting Peptide Design and Screeningmentioning

confidence: 99%

Construction of Targeting-Peptide-Based Imaging Reagents and Their Application in Bioimaging

Zhang,

Wang,

Zhao

et al. 2023

Chemical & Biomedical Imaging

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Molecular imaging was developed from basic molecular recognition. It can visualize not only the expression levels of specific molecules in a living system but also specific biological processes, thus providing guidance for early detection and treatment of diseases. As a noninvasive method, imaging agents are one of the foundations of high spatial resolution imaging, and their sensitivity and specificity can be improved by coupling targeting ligands to imaging probes. Among the various targeting ligands (antibodies, aptamers, etc.), targeting peptides are widely used in various modalities of molecular imaging due to their high affinities toward the molecular target and their excellent physicochemical properties. In this review, we summarize the design concepts and methods of targeting peptides in molecular imaging, introduce the combination of targeting peptides and imaging probes in different imaging modalities (e.g., fluorescence imaging, radionuclide imaging), and provide examples of their applications in bioimaging. Finally, the challenges and strategies for clinical translation and practical application of targeting peptide-based imaging reagents are briefly discussed.

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A Totipotent “All‐In‐One” Peptide Sequentially Blocks Immune Checkpoint and Reverses the Immunosuppressive Tumor Microenvironment

Cited by 16 publications

References 66 publications

Dual-Functional Capping Agent-Mediated Transformation of Silver Nanotriangles to Silver Nanoclusters for Dual-Mode Biosensing

Dual-Functional Capping Agent-Mediated Transformation of Silver Nanotriangles to Silver Nanoclusters for Dual-Mode Biosensing

Patient-derived xenografts or organoids in the discovery of traditional and self-assembled drug for tumor immunotherapy

Construction of Targeting-Peptide-Based Imaging Reagents and Their Application in Bioimaging

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