Your search keyword '"Zheng, Qinghui"' showing total 2 results

1. A Review of Gut Microbiota‐Derived Metabolites in Tumor Progression and Cancer Therapy.

Author

Yang, Qiqing, Wang, Bin, Zheng, Qinghui, Li, Heyu, Meng, Xuli, Zhou, Fangfang, and Zhang, Long

Subjects

CANCER invasiveness, MICROBIAL metabolites, CANCER treatment, METABOLITES, FECAL microbiota transplantation, NANOMEDICINE, SYNTHETIC biology

Abstract

Gut microbiota‐derived metabolites are key hubs connecting the gut microbiome and cancer progression, primarily by remodeling the tumor microenvironment and regulating key signaling pathways in cancer cells and multiple immune cells. The use of microbial metabolites in radiotherapy and chemotherapy mitigates the severe side effects from treatment and improves the efficacy of treatment. Immunotherapy combined with microbial metabolites effectively activates the immune system to kill tumors and overcomes drug resistance. Consequently, various novel strategies have been developed to modulate microbial metabolites. Manipulation of genes involved in microbial metabolism using synthetic biology approaches directly affects levels of microbial metabolites, while fecal microbial transplantation and phage strategies affect levels of microbial metabolites by altering the composition of the microbiome. However, some microbial metabolites harbor paradoxical functions depending on the context (e.g., type of cancer). Furthermore, the metabolic effects of microorganisms on certain anticancer drugs such as irinotecan and gemcitabine, render the drugs ineffective or exacerbate their adverse effects. Therefore, a personalized and comprehensive consideration of the patient's condition is required when employing microbial metabolites to treat cancer. The purpose of this review is to summarize the correlation between gut microbiota‐derived metabolites and cancer, and to provide fresh ideas for future scientific research. [ABSTRACT FROM AUTHOR]

Published

2023

2. Radiation Changes the Metabolic Profiling of Melanoma Cell Line B16.

Author

Wu, Lige, Hu, Zixi, Huang, Yingying, Yu, Yating, Liang, Wei, Zheng, Qinghui, Huang, Xianing, Huang, Yong, Lu, Xiaoling, and Zhao, Yongxiang

Subjects

METABOLIC profile tests, CELL lines, CANCER treatment, RADIOTHERAPY, RADIATION tolerance

Abstract

Radiation therapy can be an effective way to kill cancer cells using ionizing radiation, but some tumors are resistant to radiation therapy and the underlying mechanism still remains elusive. It is therefore necessary to establish an appropriate working model to study and monitor radiation-mediated cancer therapy. In response to cellular stress, the metabolome is the integrated profiling of changes in all metabolites in cells, which can be used to investigate radiation tolerance mechanisms and identify targets for cancer radiation sensibilization. In this study, using 1H nuclear magnetic resonance for untargeted metabolic profiling in radiation-tolerant mouse melanoma cell line B16, we comprehensively investigated changes in metabolites and metabolic network in B16 cells in response to radiation. Principal component analysis and partial least squares discriminant analysis indicated the difference in cellular metabolites between the untreated cells and X-ray radiated cells. In radiated cells, the content of alanine, glutamate, glycine and choline was increased, while the content of leucine, lactate, creatine and creatine phosphate was decreased. Enrichment analysis of metabolic pathway showed that the changes in metabolites were related to multiple metabolic pathways including the metabolism of glycine, arginine, taurine, glycolysis, and gluconeogenesis. Taken together, with cellular metabolome study followed by bioinformatic analysis to profile specific metabolic pathways in response to radiation, we deepened our understanding of radiation-resistant mechanisms and radiation sensibilization in cancer, which may further provide a theoretical and practical basis for personalized cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2016