Your search keyword '"Feng Yuqing"' showing total 5 results

1. Peptide Degrader-Based Targeting of METTL3/14 Improves Immunotherapy Response in Cutaneous Melanoma.

Author

Han H, Li Z, Feng Y, Song H, Fang Z, Zhang D, Yuan D, and Shi J

Subjects

Humans, Cell Proliferation drug effects, Animals, Mice, Antineoplastic Agents pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents therapeutic use, Cell Line, Tumor, Melanoma, Cutaneous Malignant, Apoptosis drug effects, Methyltransferases metabolism, Methyltransferases antagonists & inhibitors, Melanoma drug therapy, Melanoma pathology, Melanoma metabolism, Immunotherapy, Peptides chemistry, Peptides pharmacology, Skin Neoplasms drug therapy, Skin Neoplasms pathology, Skin Neoplasms immunology, Skin Neoplasms metabolism

Abstract

METTL3 has emerged as a promising therapeutic target in cancer treatment, although its oncogenic functions in melanoma development and potential for therapeutic targeting drug have not been fully explored. In this study, we define the oncogenic role of METTL3 in melanoma development and progression. Building on this insight, we examine our recently designed peptide inhibitor RM3, which targets the binding interface of METTL3/14 complex for disruption and subsequent ubiquitin-mediated proteasomal degradation via the E3 ligase STUB1. RM3 treatment reduces proliferation, migration, and invasion, and induces apoptosis in melanoma cells in vitro and in vivo. Subsequent transcriptomic analysis identified changes in immuno-related genes following RM3-mediated suppression of METTL3/14 N 6 -methyladenosine (m 6 A) methyltransferase activity, suggesting a potential for interaction with immunotherapy. A combination treatment of RM3 with anti-PD-1 antibody results in significantly higher beneficial tumor response in vivo, with a good safety profile. Collectively, these findings not only delineate the oncogenic role of METTL3 in melanoma but also showcase RM3, acting as a peptide degrader, as a novel and promising strategy for melanoma treatment., (© 2024 Wiley-VCH GmbH.)

Published

2024

2. Stabilization of RRBP1 mRNA via an m 6 A-dependent manner in prostate cancer constitutes a therapeutic vulnerability amenable to small-peptide inhibition of METTL3.

Author

Feng Y, Li Z, Zhu J, Zou C, Tian Y, Xiong J, He Q, Li W, Xu H, Liu L, Xu B, Shi J, and Zhang D

Subjects

Humans, Male, Animals, Mice, Cell Line, Tumor, Cell Proliferation genetics, Gene Expression Regulation, Neoplastic, Adenosine analogs & derivatives, Adenosine metabolism, RNA Stability genetics, Peptides metabolism, RNA-Binding Proteins metabolism, RNA-Binding Proteins genetics, Prostatic Neoplasms pathology, Prostatic Neoplasms metabolism, Prostatic Neoplasms genetics, Prostatic Neoplasms drug therapy, Methyltransferases metabolism, Methyltransferases genetics, Methyltransferases antagonists & inhibitors, RNA, Messenger genetics, RNA, Messenger metabolism

Abstract

Mounting evidence has implicated the RNA m 6 A methylation catalyzed by METTL3 in a wide range of physiological and pathological processes, including tumorigenesis. The detailed m 6 A landscape and molecular mechanism of METTL3 in prostate cancer (PCa) remains ill-defined. We find that METTL3 is overexpressed in PCa and correlates with worse patient survival. Functional studies establish METTL3 as an oncoprotein dependent on its m 6 A enzymatic activity in both AR + and AR - PCa cells. To dissect the regulatory network of m 6 A pathway in PCa, we map the m 6 A landscape in clinical tumor samples using m 6 A-seq and identify genome-wide METTL3-binding transcripts via RIP-seq. Mechanistically, we discover RRBP1 as a direct METTL3 target in which METTL3 stabilizes RRBP1 mRNA in an m 6 A-dependent manner. RRBP1 positively correlates with METTL3 expression in PCa cohorts and exerts an oncogenic role in aggressive PCa cells. Leveraging the 3D structural protein-protein interaction between METTL3 and METTL14, we successfully develop two potential METTL3 peptide inhibitors (RM3 and RSM3) that effectively suppress cancer cell proliferation in vitro and tumor growth in vivo. Collectively, our study reveals a novel METTL3/m 6 A/RRBP1 axis in enhancing aggressive traits of PCa, which can be therapeutically targeted by small-peptide METTL3 antagonists., (© 2024. The Author(s).)

Published

2024

3. A Stapled Peptide Inhibitor Targeting the Binding Interface of N6-Adenosine-Methyltransferase Subunits METTL3 and METTL14 for Cancer Therapy.

Author

Li Z, Feng Y, Han H, Jiang X, Chen W, Ma X, Mei Y, Yuan D, Zhang D, and Shi J

Subjects

Humans, Adenosine analogs & derivatives, Adenosine chemistry, Adenosine metabolism, Adenosine pharmacology, Animals, Cell Proliferation drug effects, Mice, Neoplasms drug therapy, Neoplasms metabolism, Neoplasms pathology, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Cell Line, Tumor, Apoptosis drug effects, Methyltransferases metabolism, Methyltransferases antagonists & inhibitors, Peptides chemistry, Peptides pharmacology, Peptides metabolism, Antineoplastic Agents pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents metabolism

Abstract

METTL3, a primary methyltransferase catalyzing the RNA N6-methyladenosine (m6A) modification, has been identified as an oncogene in several cancer types and thus nominated as a potentially effective target for therapeutic inhibition. However, current options using this strategy are limited. In this study, we targeted protein-protein interactions at the METTL3-METTL14 binding interface to inhibit complex formation and subsequent catalysis of the RNA m6A modification. Among candidate peptides, RM3 exhibited the highest anti-cancer potency, inhibiting METTL3 activity while also facilitating its proteasomal degradation. We then designed a stapled peptide inhibitor (RSM3) with enhanced peptide stability and formation of the α-helical secondary structure required for METTL3 interaction. Functional and transcriptomic analysis in vivo indicated that RSM3 induced upregulation of programmed cell death-related genes while inhibiting cancer-promoting signals. Furthermore, tumor growth was significantly suppressed while apoptosis was enhanced upon RSM3 treatment, accompanied by increased METTL3 degradation, and reduced global RNA methylation levels in two in vivo tumor models. This peptide inhibitor thus exploits a mechanism distinct from other small-molecule competitive inhibitors to inhibit oncogenic METTL3 activity. Our findings collectively highlight the potential of targeting METTL3 in cancer therapies through peptide-based inhibition of complex formation and proteolytic degradation., (© 2024 Wiley-VCH GmbH.)

Published

2024

4. Peptide Degrader‐Based Targeting of METTL3/14 Improves Immunotherapy Response in Cutaneous Melanoma.

Author

Han, Hong, Li, Zenghui, Feng, Yuqing, Song, He, Fang, Zhixiong, Zhang, Dingxiao, Yuan, Dan, and Shi, Junfeng

Subjects

UBIQUITIN ligases, PEPTIDES, MELANOMA, CANCER treatment, METHYLTRANSFERASES

Abstract

METTL3 has emerged as a promising therapeutic target in cancer treatment, although its oncogenic functions in melanoma development and potential for therapeutic targeting drug have not been fully explored. In this study, we define the oncogenic role of METTL3 in melanoma development and progression. Building on this insight, we examine our recently designed peptide inhibitor RM3, which targets the binding interface of METTL3/14 complex for disruption and subsequent ubiquitin‐mediated proteasomal degradation via the E3 ligase STUB1. RM3 treatment reduces proliferation, migration, and invasion, and induces apoptosis in melanoma cells in vitro and in vivo. Subsequent transcriptomic analysis identified changes in immuno‐related genes following RM3‐mediated suppression of METTL3/14 N6‐methyladenosine (m6A) methyltransferase activity, suggesting a potential for interaction with immunotherapy. A combination treatment of RM3 with anti‐PD‐1 antibody results in significantly higher beneficial tumor response in vivo, with a good safety profile. Collectively, these findings not only delineate the oncogenic role of METTL3 in melanoma but also showcase RM3, acting as a peptide degrader, as a novel and promising strategy for melanoma treatment. [ABSTRACT FROM AUTHOR]

Published

2024

5. A Stapled Peptide Inhibitor Targeting the Binding Interface of N6‐Adenosine‐Methyltransferase Subunits METTL3 and METTL14 for Cancer Therapy.

Author

Li, Zenghui, Feng, Yuqing, Han, Hong, Jiang, Xingyue, Chen, Weiyu, Ma, Xuezhen, Mei, Yang, Yuan, Dan, Zhang, Dingxiao, and Shi, Junfeng

Subjects

PEPTIDES, CANCER treatment, RNA modification & restriction, PROTEOLYSIS, RNA methylation, METHYLTRANSFERASES

Abstract

METTL3, a primary methyltransferase catalyzing the RNA N6‐methyladenosine (m6A) modification, has been identified as an oncogene in several cancer types and thus nominated as a potentially effective target for therapeutic inhibition. However, current options using this strategy are limited. In this study, we targeted protein–protein interactions at the METTL3–METTL14 binding interface to inhibit complex formation and subsequent catalysis of the RNA m6A modification. Among candidate peptides, RM3 exhibited the highest anti‐cancer potency, inhibiting METTL3 activity while also facilitating its proteasomal degradation. We then designed a stapled peptide inhibitor (RSM3) with enhanced peptide stability and formation of the α‐helical secondary structure required for METTL3 interaction. Functional and transcriptomic analysis in vivo indicated that RSM3 induced upregulation of programmed cell death‐related genes while inhibiting cancer‐promoting signals. Furthermore, tumor growth was significantly suppressed while apoptosis was enhanced upon RSM3 treatment, accompanied by increased METTL3 degradation, and reduced global RNA methylation levels in two in vivo tumor models. This peptide inhibitor thus exploits a mechanism distinct from other small‐molecule competitive inhibitors to inhibit oncogenic METTL3 activity. Our findings collectively highlight the potential of targeting METTL3 in cancer therapies through peptide‐based inhibition of complex formation and proteolytic degradation. [ABSTRACT FROM AUTHOR]

Published

2024