Cellular zinc metabolism and zinc signaling: from biological functions to diseases and therapeutic targets

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作者
Bonan Chen
Peiyao Yu
Wai Nok Chan
Fuda Xie
Yigan Zhang
Li Liang
Kam Tong Leung
Kwok Wai Lo
Jun Yu
Gary M. K. Tse
Wei Kang
Ka Fai To
机构
[1] Prince of Wales Hospital,Department of Anatomical and Cellular Pathology, State Key Laboratory of Translational Oncology
[2] The Chinese University of Hong Kong,State Key Laboratory of Digestive Disease, Institute of Digestive Disease
[3] The Chinese University of Hong Kong,CUHK
[4] The Chinese University of Hong Kong,Shenzhen Research Institute
[5] Southern Medical University,Department of Pathology, Nanfang Hospital and Basic Medical College
[6] Guangdong Province Key Laboratory of Molecular Tumor Pathology,Institute of Biomedical Research
[7] Taihe Hospital,Department of Pediatrics
[8] Hubei University of Medicine,Department of Medicine and Therapeutics
[9] The Chinese University of Hong Kong,undefined
[10] The Chinese University of Hong Kong,undefined
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摘要
Zinc metabolism at the cellular level is critical for many biological processes in the body. A key observation is the disruption of cellular homeostasis, often coinciding with disease progression. As an essential factor in maintaining cellular equilibrium, cellular zinc has been increasingly spotlighted in the context of disease development. Extensive research suggests zinc’s involvement in promoting malignancy and invasion in cancer cells, despite its low tissue concentration. This has led to a growing body of literature investigating zinc’s cellular metabolism, particularly the functions of zinc transporters and storage mechanisms during cancer progression. Zinc transportation is under the control of two major transporter families: SLC30 (ZnT) for the excretion of zinc and SLC39 (ZIP) for the zinc intake. Additionally, the storage of this essential element is predominantly mediated by metallothioneins (MTs). This review consolidates knowledge on the critical functions of cellular zinc signaling and underscores potential molecular pathways linking zinc metabolism to disease progression, with a special focus on cancer. We also compile a summary of clinical trials involving zinc ions. Given the main localization of zinc transporters at the cell membrane, the potential for targeted therapies, including small molecules and monoclonal antibodies, offers promising avenues for future exploration.
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