Design, Synthesis, and Pharmacological Evaluation of Novel Isoform-specific Histone Deacetylase (HDAC) Inhibitors as Potential Anticancer Therapeutics, via A Fluorous-tag Assisted High-throughput Synthetic Platform
Implementing Organization
Indian Institute of Technology (IIT)
Principal Investigator
Dr. Sushabhan Sadhukhan
Indian Institute of Technology (IIT)
About
Histone deacetylases (HDACs) are a family of zinc-dependent hydrolases that regulate gene expression and enzymatic activity. They have been extensively studied due to their role in cancer pathogenesis and the potential of small-molecule HDAC inhibitors (HDACi). HDACs can be divided into three classes, Class I, II, and IV, consisting of eleven mammalian HDACs. These HDACs have been identified as potential therapeutic targets to reverse aberrant epigenetic modification associated with cancer. However, the design of isoform-specific inhibitors remains a challenge. Most reported HDACs are either class-selective or not selective, causing adverse side effects by inhibiting undesired HDACs or non-HDAC targets. Therefore, there is a pressing need for the development of isoform-specific HDACi. The proposed research aims to develop isoform-specific lysine-based HDACi using a novel high-throughput strategy built on a fluorous platform. The zinc-binding group (ZBG) of HDACi will also be explored to achieve isoform-specificity. Hydroxamates, commonly used as ZBG in HDACs, will be explored for their strong chelation property but suffer from poor pharmacokinetics and non-selective binding to other zinc-dependent enzymes. The promising HDACi will be tested in different cancer cell lines, using a multidisciplinary approach from high-throughput synthesis to mammalian cell culture. Results from these studies will help better understand the function of individual isoforms and provide therapeutic agents with potentially fewer adverse effects by minimizing off-targets.
Source
Source
Anusandhan National Research Foundation/Science and Engineering Research Board (SERB), DST 2023-24
Science and Engineering Research Board (SERB), New Delhi
Anusandhan National Research Foundation (ANRF)
Quick Information
Area of Research
Chemical Sciences
Start Year
2024
End Year
2027
Sanction Amount
₹ 45.21 L
Status
Ongoing
Contact
sushabhan@iitpkd.ac.in
Output
No. of Research Paper
00
Technologies (If Any)
00
No. of PhD Produced
00
No. of Patents
Filed :00
Grant :00
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