Abstract
BackgroundThe inhibition of dopamine transporter is known to play a significant role in the treatment of schizophrenia-related and other mental disorders. In a continuing from our previous study, computational drug design approach, molecular docking simulation, and pharmacokinetics study were explored for the identification of novel inhibitors dopamine transporter as potential Antischizophrenic agents. Consequently, thirteen (13) new inhibitors of dopamine transporter were designed by selecting the molecule with serial number 39 from our previous study as the template molecule because it exhibits good pharmacological attributes.ResultsMolecular docking simulation results revealed excellent molecular interactions between the protein target (PDB: 4m48) and the ligands (designed inhibitors) with major interactions that involved hydrogen bonding and hydrophobic interactions. Also, some of the designed inhibitors displayed a superior binding affinity range from − 10.0 to − 10.7 kcal/mol compared to the referenced drug (Lumateperone) with a binding affinity of − 9.7 kcal/mol. Computed physicochemical parameters showed that none of the designed inhibitors including the referenced drug violate Lipinski’s rule of five indicating that all the designed inhibitors would be orally bioavailable as potential drug candidates. Similarly, the ADMET/pharmacokinetics evaluations of some designed inhibitors revealed that they possessed good absorption, distribution, metabolism and excretion properties and none of the inhibitors is neither carcinogens nor toxic toward human ether-a-go-go related gene (hERG I) inhibitor or skin sensitization. Likewise, the BOILED-Egg graphics unveils that all the designed inhibitors demonstrate a high probability to be absorbed by the human gastrointestinal tract and could permeate into the brain. Besides, the predicted bioactive parameters suggested that all the selected inhibitors would be active as drug candidates. Furthermore, the synthetic accessibility scores for all the selected inhibitors and referenced drug lied within the easy zone (i.e., between 1–4) with their computed values range from 2.55 to 3.92, this implies that all the selected inhibitors would be very easy to synthesize in the laboratory.ConclusionsHence, all the designed inhibitors having shown excellent pharmacokinetics properties and good bioavailabilities attributes with remarkable biochemical interactions could be developed and optimized as novel Antischizophrenic agents after the conclusion of other experimental investigations.
Highlights
The inhibition of dopamine transporter is known to play a significant role in the treatment of schizophrenia-related and other mental disorders
Mental disorders associated with immoderate neurotransmission of dopamine levels by implicating dopamine transporter (DAT) as well as dysfunction of dopamine (DA) neurotransmission are important contributing factors in the pathophysiology of neuropsychiatric disorders such as depression, bipolar disorder, Parkinson’s disease, and attention deficit hyperactivity disorder (ADHD) [3]
The inhibition of DAT blocks the reuptake of dopamine from extracellular space into the synapse thereby raising the quantity of dopamine availability which in turns improves the possibility of dopamine receptor activation; the inhibition by most of the DAT inhibitors is limited with associated adverse side effects [4, 5]
Summary
The inhibition of dopamine transporter is known to play a significant role in the treatment of schizophrenia-related and other mental disorders. Drugs targeting the dopamine transporter (DAT) are majorly used to improve cognitive abilities as therapeutic agents for schizophrenia-related cognitive impairments and other neuropsychiatric disorders [6]. Many antipsychotics known as neuroleptics medications such as Lumateperone, Modafinil, Chloropromazine Cariprazine, Risperidon are available as a class of compounds with a strong affinity for various subtypes of dopamine receptors for the treatment of schizophrenic patients to decrease excess levels of dopamine thereby lessen the positive symptoms of the disorder but none of the beneficial effects for any of the medication strategies were considered to be of clinically significant [2, 7]. The need to design new inhibitors of DAT having more therapeutic potential with lower or no side effects as antischizophrenic agents is calling for global attention
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