Comparative Molecular Docking Studies of Selected Phytoconstituents on Adenosine A2A Receptor (PDB ID: 3UZA) as Potential Anti-Parkinson’s Agents

Kumari, Namrata; Chandra, Priyanka; Ghosh, Manik

doi:10.3390/ecsoc-27-16119

Open AccessProceeding Paper

Comparative Molecular Docking Studies of Selected Phytoconstituents on Adenosine A2A Receptor (PDB ID: 3UZA) as Potential Anti-Parkinson’s Agents^†

by

Namrata Kumari

,

Priyanka Chandra

and

Manik Ghosh

^*

Department of Pharmaceutical Sciences and Technology, Birla Institute of Technology, Ranchi 835215, Jharkhand, India

^*

Author to whom correspondence should be addressed.

^†

Presented at the 27th International Electronic Conference on Synthetic Organic Chemistry (ECSOC-27), 15–30 November 2023; Available online: https://ecsoc-27.sciforum.net/.

Chem. Proc. 2023, 14(1), 84; https://doi.org/10.3390/ecsoc-27-16119

Published: 15 November 2023

(This article belongs to the Proceedings of 27th International Electronic Conference on Synthetic Organic Chemistry)

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Abstract

:

Parkinson’s disease is a neurodegenerative disease which involves the malfunction and death of vital nerve cells in the brain, called neurons, which produce dopamine. Dopamine is a neurotransmitter that communicates with the area of the brain responsible for movement and coordination. As Parkinson’s disease progresses, the amount of dopamine production in the brain declines, leaving a person unable to control movement. Typically, natural compounds such as flavanoids have been cited in the literature for having the ability to penetrate the blood–brain barrier and halt the progression of such disorders. In this study, ten phytoconstituents were screened using molecular docking against adenosine A2A to identify potential inhibitors. Target protein of interest, Adenosine A2A receptor (PDB ID: 3UZA) was extracted from PDB database. Test drugs as well as standard drug were extracted in their 3D conformation from the PubChem in .SDF format, and docking was done using FlexX software. The docking scores of the selected photochemical were compared with levodopa as a positive control. Docking studies revealed that Baicaline has best molecular docking result (−21.6 kcal/mol) for Adenosine A2A receptor, with low toxicity as per pro Tox-II online server which indicates that the Baicalein is a potential lead to be drug candidate for Parkinson’s disease.

Keywords:

Parkinson’s disease; dopamine; molecular docking; adenosine; baicalein

1. Introduction

Parkinson’s disease (PD) is the second most common neurodegenerative disorder globally, which leads to severe behavioral and cognitive dysfunction [1], with a prevalence of about 0.5–1% among people 65 to 69 years old and rising to 1–3% among people 80 and older [2]. It was initially described in 1817 by James Parkinson, and it was further defined by Jean-Martin Charcot [3].

The etiology of Parkinson’s disease remains a topic of intense investigation, with both genetic and environmental factors implicated in its development. The main risk factor for PD is age, with a median onset age of 60 years old [4]. The hallmark pathological feature of Parkinson’s is the progressive loss of dopamine-producing neurons in the substantia nigra, a region of the brain critical for motor control [5]. This depletion of dopamine leads to the characteristic motor symptoms of tremors, bradykinesia, rigidity, and postural instability, which significantly hamper patients’ daily lives [6].

Deep brain stimulation and dopaminergic medications are currently accessible to enhance daily activities and quality of life while lessening the motor impairment in the patient with Parkinson’s disease [7]. In order to encourage neuroprotective intervention prior to the commencement of clinical manifestation, new investigations are being done to identify suitable therapy approaches [8].

Recently, natural medicines, mostly molecules derived from plants, have gained wide acceptance to treat Parkinson’s disease, since they are known to have fewer negative side effects than synthetic ones [9].

From the literature, ten phytoconstituents were selected for their neuroprotective action (Table 1) are caffeine (1), lenoleic acid (2), oleic acid (3), vasicine (4), vasicinol (5), vasicol (6), baicalein (7), amentoflavone (8), ginkgolide-B (9) and alpha cubebene (10) (Figure 1).

Using molecular docking analysis, phytoconstituents were investigated and were compared with the standard drug Levodopa. FlexX is a quick and flexible docking tool that docks ligands into the active site of proteins. It possesses excellent ligand flexibility by changing the conformations in the active site although protein is rigid [10]. Using the FlexX docking software, screening of ten natural compounds with the Adenosine A2A receptor (3UZA) was done on the basis of their binding energy and conformation.

Table 1. Neuroprotective action of phytoconstituents.

Phytoconstituents	Mechanism of Neuroprotective Action
Caffeine	Caffeine has capacity to antagonize adenosine receptors, particularly A2A receptors present in striatopallidal neurons and improves PD motor functioning [11].
Lenoleic acid	Antidepressant and anti-inflammatory properties, as well as increases in neuronal plasticity [12].
Oleic acid	Oleic acid serves as a neurotrophic factor that promotes synapse formation, axonal and dendritic growth, neuronal migration and aggregation, and the production of myelin phospholipids during brain development [13].
Vasicine	Effectively inhibited cholinesterases and Aβ aggregates, as well as neuroprotection activity [14].
Vasicinol
Vasicol
Baicalein	Baicalein has a protective effect against oxidative stress-related damage. It also suppressed cell viability loss, intracellular ROS production, and prevented the buildup of ROS [15].
Amentoflavone	Protects dopaminergic neurons from neurotoxicity by activating the PI3K/Akt and ERK signalling pathways, and reducing neuroinflammation in dopaminergic neurons [16].
Ginkgolide-B	Anti-inflammatory effects and scavenging of oxygen free radicals [17].
Alpha cubebene	Reduces the amyloid-induced neuroinflammatory response of microglia [18].

2. Material and Methods

2.1. Preparation of Ligands

From the literature, we selected the set of ten phytoconstituents structure, known for their brain stimulant action and can be used for Parkinson’s disease.

The phytoconstituent were extracted in their 3D conformation from the PubChem and were in .SDF format. Levodopa was used as the reference standard, as the first line of treatment for Parkinson’s disease is levodopa.

2.2. Retrieval of Protein Structure and Preparation

The X-ray-co-crystallized structures of the protein molecules (PDB ID: 3UZA) used in the study were retrieved from the Research Collaboratory for Structural Bioinformatics (RCSB). The receptor file was saved in “Mol2” format.

2.3. Molecular Docking Studies

The FlexX v 2.1.3 program was used to load the potential binding sites between the various ligands and the target protein. Prediction of protein–ligand interactions is performed using FlexX v 2.1.3 docking software. The results of docking were then compared with the docked result of reference ligand obtained from the corresponding PDB ID. The docking scores, 2D and 3D pose views, as well as the binding affinities of the selected natural compounds, were generated for further investigation.

The best docked phytoconstituent for neuroprotective action was identified on the basis of binding energy and interaction with amino acid residues.

2.4. Toxiciy Study

Toxicity of each phytoconstituents were determined with the help of pro Tox-II online server. ProTox-II is a virtual toxicity lab that enables the prediction of multiple toxicological endpoints related with a chemical structure.

3. Results and Discussion

It has been discovered that natural substances operate preferentially as brain stimulants. The objective of the current study was to investigate the effects of natural substances as brain stimulants. Among the ten ligands, Baicalein showed a superior docking score of −21.60 kcal/mol. Baicalein (5,6,7-trihydroxy-2-phenylchromen-4-one) is a naturally occurring substance mainly found in stachys annua, stellera chamaejasme and other organisms. It belongs to the trihydroxyflavone class of group with the hydroxy groups at positions C-5, -6 and -7. Binding configuration of the reference ligand and best dock ligand is depicted in Figure 2 and Figure 3 and Table 2 and Table 3.

Predictive Toxicity Studies

Toxicity of baicalein was determined with the help of pro Tox-II online server, and it was found that the predicted LD50 value of baicalein was 3919 mg/kg and the predictive toxicity class of baicalein is 5.

4. Conclusions

Docking studies were performed on the ten selected phytoconstituents. The docking result of plant compound compared to levodopa, standard drug shows that baicalein, caffeine, vasicol, vasicinol, vasicine, and amentoflavone have negative docking energy, which corresponds to good binding. Baicalein has a more negative value (−21.6080), which corresponds to very high binding and is closest to levodopa binding energy. Lineolic acid and oleic acid has positive score, which corresponds to non-existing binding (Table 4).

Author Contributions

Conceptualization, M.G.; methodology, M.G. and P.C.; software, M.G. and P.C.; writing, N.K.; supervision, M.G. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

Data are contained within the article.

Acknowledgments

The authors would like to acknowledge the Department of Pharmaceutical Sciences and Technology, Birla Institute of Technology, Mesra, Ranchi.

Conflicts of Interest

The authors declare no conflicts of interest.

References

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Figure 1. Structure of compound.

Figure 2. Binding configuration of levodopa with 3UZA (a) high dock, (b) low dock, (c) high match, (d) low match.

Figure 3. Binding configuration of Baicalein with 3UZA (a) high dock, (b) low dock, (c) high match, (d) low match.

Table 2. Docking result of levodopa in 3UZA.

Docking Result	High Dock	Low Dock	High Match	Low Match
Rank	1	323	2	259
Score	−23.118	−2.4571	−14.6326	−12.4526
Match	12	3	13	2

Table 3. Docking result of baicalein in 3UZA.

Docking Result	High Dock	Low Dock	High Match	Low Match
Rank	1	177	36	174
Score	−21.6080	0.2300	−13.9364	−0.3296
Match	17	11	22	5

Table 4. Docking score of phytoconstituents in the active site of Adenosine A2A receptor (PDB ID:3UZA).

Protein	Ligands	Binding Affinity (Kcal/mol)
3UZA	Levodopa	−23.118
	Baicalein	−21.6080
	Caffiene	−17.9397
	Vasicol	−14.5378
	Vasicinol	−9.3958
	Vasicine	−8.5219
	Amentoflavone	−4.5378
	Linoleic acid	4.2474
	Oleic acid	5.1262
	Alpha cubebene	Not docked
	Ginkgolide B	Not docked

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Kumari, N.; Chandra, P.; Ghosh, M. Comparative Molecular Docking Studies of Selected Phytoconstituents on Adenosine A2A Receptor (PDB ID: 3UZA) as Potential Anti-Parkinson’s Agents. Chem. Proc. 2023, 14, 84. https://doi.org/10.3390/ecsoc-27-16119

AMA Style

Kumari N, Chandra P, Ghosh M. Comparative Molecular Docking Studies of Selected Phytoconstituents on Adenosine A2A Receptor (PDB ID: 3UZA) as Potential Anti-Parkinson’s Agents. Chemistry Proceedings. 2023; 14(1):84. https://doi.org/10.3390/ecsoc-27-16119

Chicago/Turabian Style

Kumari, Namrata, Priyanka Chandra, and Manik Ghosh. 2023. "Comparative Molecular Docking Studies of Selected Phytoconstituents on Adenosine A2A Receptor (PDB ID: 3UZA) as Potential Anti-Parkinson’s Agents" Chemistry Proceedings 14, no. 1: 84. https://doi.org/10.3390/ecsoc-27-16119

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Comparative Molecular Docking Studies of Selected Phytoconstituents on Adenosine A2A Receptor (PDB ID: 3UZA) as Potential Anti-Parkinson’s Agents^†

Abstract

1. Introduction