Druglikeness: Difference between revisions

• Druglikeness is a fundamental concept in drug discovery and development that refers to the likelihood of a chemical compound to possess the necessary properties to become a safe and effective medication.
• It involves the assessment of a compound's structural and physicochemical properties to determine its potential as a drug candidate.
• The concept of druglikeness helps researchers and pharmaceutical companies prioritize compounds for further development and increase the probability of successfully bringing new medications to the market.

Key Principles of Druglikeness

Several key principles govern druglikeness assessments:

• Molecular Size and Complexity: Drug candidates should have a molecular size and complexity that allows them to be easily synthesized and modified, while still having sufficient specificity for the drug target.
• Physicochemical Properties: Drug candidates should exhibit desirable physicochemical properties, including lipophilicity, solubility, and permeability, to facilitate their absorption, distribution, metabolism, and excretion (ADME) in the body.
• Bioavailability: Drug candidates should have adequate bioavailability, meaning they can reach the target site in sufficient concentrations to exert a therapeutic effect.
• Toxicity and Safety: Drug candidates should have a favorable safety profile, with low toxicity and minimal adverse effects.
• Target Specificity: Drug candidates should selectively interact with the intended drug target, minimizing interactions with off-target proteins to reduce the risk of side effects.

Evaluation of Druglikeness

Assessing druglikeness involves various computational and experimental methods:

• Lipinski's Rule of Five: Lipinski's Rule of Five is a widely used guideline that predicts druglikeness based on four criteria: molecular weight, lipophilicity (logP), hydrogen bond donors, and hydrogen bond acceptors. Compounds that violate more than one of these criteria are considered less likely to be orally bioavailable.
• Molecular Descriptors: Computational methods use various molecular descriptors, such as molecular weight, logP, polar surface area (PSA), and hydrogen bond donors/acceptors, to assess druglikeness.
• ADME Properties: Predictive models evaluate a compound's ADME properties, such as solubility, permeability, metabolic stability, and potential for drug-drug interactions.
• Toxicity Prediction: In silico models and in vitro assays help predict a compound's potential toxicity and safety profile.

Significance in Drug Development

Druglikeness is a crucial concept in drug development for several reasons:

• Lead Optimization: Assessing druglikeness guides medicinal chemists in modifying chemical structures to enhance a compound's drug-like properties while retaining its activity against the target.
• Candidate Prioritization: Druglikeness assessments allow researchers to prioritize compounds with the highest potential for success in preclinical and clinical development.
• Resource Allocation: Focusing resources on drug candidates with favorable druglikeness properties increases the efficiency of the drug development process and reduces the risk of costly failures.
• Regulatory Approval: Considering druglikeness early in drug development helps identify compounds that are more likely to meet regulatory requirements for safety and efficacy.
• Ethical Considerations: Prioritizing drug candidates with better druglikeness properties may reduce the use of animals in preclinical studies and human subjects in clinical trials.

Conclusion

• Druglikeness is a fundamental concept that plays a crucial role in drug discovery and development.
• By assessing the structural and physicochemical properties of chemical compounds, researchers can prioritize drug candidates with the highest likelihood of success and increase the efficiency of the drug development process.
• Ultimately, druglikeness assessments contribute to the identification of safe and effective medications that can improve patient outcomes and address unmet medical needs.

See also

• Lipinski's rule of five (RO5)
• Fragment-based lead discovery (FBLD)

References

• Lipinski CA, Lombardo F, Dominy BW, Feeney PJ. Experimental and computational approaches to estimate solubility and permeability in drug discovery and development settings. Adv Drug Deliv Rev. 1997;23(1-3):3-25. doi:10.1016/s0169-409x(96)00423-1.
• Singh J, Petter RC, Baillie TA, Whitty A. The resurgence of covalent drugs. Nat Rev Drug Discov. 2011;10(4):307-317. doi:10.1038/nrd3410.
• Doak BC, Zheng J, Dobritzsch D, Kihlberg J. How beyond rule of 5 drugs and clinical candidates bind to their targets. J Med Chem. 2015;58(21):8313-8324. doi:10.1021/acs.jmedchem.5b00954.