棕榈酰化
内吞作用
生物化学
化学
细胞生物学
生物
半胱氨酸
受体
酶
作者
Niall M. Fraser,Jacqueline Howie,Krzysztof J. Wypijewski,William Fuller
出处
期刊:Biochemical Society Transactions
[Portland Press]
日期:2020-02-28
卷期号:48 (1): 281-290
被引量:14
摘要
The post-translational modification protein S-acylation (commonly known as palmitoylation) plays a critical role in regulating a wide range of biological processes including cell growth, cardiac contractility, synaptic plasticity, endocytosis, vesicle trafficking, membrane transport and biased-receptor signalling. As a consequence, zDHHC-protein acyl transferases (zDHHC-PATs), enzymes that catalyse the addition of fatty acid groups to specific cysteine residues on target proteins, and acyl proteins thioesterases, proteins that hydrolyse thioester linkages, are important pharmaceutical targets. At present, no therapeutic drugs have been developed that act by changing the palmitoylation status of specific target proteins. Here, we consider the role that palmitoylation plays in the development of diseases such as cancer and detail possible strategies for selectively manipulating the palmitoylation status of specific target proteins, a necessary first step towards developing clinically useful molecules for the treatment of disease.
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