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The Biological Significance of Targeting Acetylation-Mediated Gene Regulation for Designing New Mechanistic Tools and Potential Therapeutics

期刊

BIOMOLECULES
卷 11, 期 3, 页码 -

出版社

MDPI
DOI: 10.3390/biom11030455

关键词

epigenetic modifications; acetylation; lysine acetyltransferases; gene regulation; molecular interactions and biological outcomes

资金

  1. NIH/NCI [R01CA143662]
  2. City University of New York Advanced Scientific Research Center Award
  3. PSC CUNY
  4. CUNY/DASNY [GRTI19, GRTI20]

向作者/读者索取更多资源

Epigenetic modifications like acetylation play a crucial role in regulating gene transcription and cellular responses, particularly in maintaining cell homeostasis and stress signaling. Acetylation influences various biological processes such as the cell cycle, DNA repair, and metabolism, and understanding KAT functions can aid in developing new disease treatments.
The molecular interplay between nucleosomal packaging and the chromatin landscape regulates the transcriptional programming and biological outcomes of downstream genes. An array of epigenetic modifications plays a pivotal role in shaping the chromatin architecture, which controls DNA access to the transcriptional machinery. Acetylation of the amino acid lysine is a widespread epigenetic modification that serves as a marker for gene activation, which intertwines the maintenance of cellular homeostasis and the regulation of signaling during stress. The biochemical horizon of acetylation ranges from orchestrating the stability and cellular localization of proteins that engage in the cell cycle to DNA repair and metabolism. Furthermore, lysine acetyltransferases (KATs) modulate the functions of transcription factors that govern cellular response to microbial infections, genotoxic stress, and inflammation. Due to their central role in many biological processes, mutations in KATs cause developmental and intellectual challenges and metabolic disorders. Despite the availability of tools for detecting acetylation, the mechanistic knowledge of acetylation-mediated cellular processes remains limited. This review aims to integrate molecular and structural bases of KAT functions, which would help design highly selective tools for understanding the biology of KATs toward developing new disease treatments.

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