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Pharmaceutical Biology Volume 55, 2017 - Issue 1
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Research Article

Inhibition of IKKβ by celastrol and its analogues – an in silico and in vitro approach

Karpagam VeerappanDepartment of Biochemistry, VRR Institute of Biomedical Science (Affiliated to University of Madras), Chennai, Tamilnadu, India;
,
Sathishkumar NatarajanDepartment of Horticulture, Sunchon National University, Suncheon, Republic of Korea;
,
Purushoth EthirajDepartment of Medical Research, SRM Medical College Hospital and Research Centre, SRM University, Kattankulathur, Tamilnadu, India;
,
Umashankar VetrivelCenter for Bioinformatics, Vision Research Foundation, Sankara Nethralaya, Chennai, Tamilnadu, India
&
Shila SamuelDepartment of Biochemistry, VRR Institute of Biomedical Science (Affiliated to University of Madras), Chennai, Tamilnadu, India; Correspondence[email protected]
Pages 368-373 | Received 29 Jan 2016, Accepted 23 Sep 2016, Published online: 08 Dec 2016
 
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Abstract

Context: Alzheimer’s disease (AD) is the most common form of dementia affecting the aged population and neuroinflammation is one of the most observed AD pathologies. NF-κB is the central regulator of inflammation and inhibitor κB kinase (IKK) is the converging point in NF-κB activation. Celastrol is a natural triterpene used as a treatment for inflammatory conditions.

Objective: This study determines the neuroprotective and inhibitory effect of celastrol on amyloid beta1-42 (Aβ1-42) induced cytotoxicity and IKKβ activity, respectively.

Materials and methods: Retinoic acid differentiated IMR-32 cells were treated with celastrol (1 μM) before treatment with Aβ1-42 (IC30 10 μM) for 24 h. The cytotoxicity and IKK phosphorylation were measured by MTT and western blotting analysis, respectively. We screened 36 celastrol analogues for the IKKβ inhibition by molecular docking and evaluated their drug like properties to delineate the neuroprotective effects.

Results: Celastrol (1 μM) inhibited Aβ1-42 (10 μM) induced IκBα phosphorylation and protected IMR-32 cells from cell death. Celastrol and 25 analogues showed strong binding affinity with IKKβ as evidenced by strong hydrogen-bonding interactions with critical active site residues. All the 25 analogues displayed strong anti-inflammatory properties but only 11 analogues showed drug-likeness. Collectively, molecule 15 has highest binding affinity, CNS activity and more drug likeness than parent compound celastrol.

Discussion and conclusion: The decreased expression of pIκBα in celastrol pretreated cells affirms the functional representation of inhibited IKKβ activity in these cells. The neuroprotective potentials of celastrol and its analogues may be related to IKK inhibition.

Disclosure statement

The authors declare that there are no conflicts of interest.

Funding

This research was supported by Department of Biotechnology – Neurosciences, India [BT/PR14058/MED/30/353/2010]. KV is thankful to CSIR for sanction of senior research fellowship to carry out this work [09/1122(0001)/2014].

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