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Pharmacokinetic and Biological Properties Evaluation of Drug Candidates

Grant number: 24/12642-1
Support Opportunities:Scholarships in Brazil - Post-Doctoral
Effective date (Start): September 01, 2024
Effective date (End): June 30, 2025
Field of knowledge:Biological Sciences - Biophysics - Molecular Biophysics
Principal Investigator:Adriano Defini Andricopulo
Grantee:Analu Rocha Costa
Host Institution: Instituto de Física de São Carlos (IFSC). Universidade de São Paulo (USP). São Carlos , SP, Brazil
Associated research grant:13/07600-3 - CIBFar - Center for Innovation in Biodiversity and Drug Discovery, AP.CEPID

Abstract

Pharmacokinetics (PK) is the study of the time course of drug absorption, distribution, metabolism and excretion (ADME), and how these ADME processes are related to the intensity and time course of the pharmacological (therapeutic and toxic) effects of drugs. Orally delivered pharmacologically active compounds must have favorable absorption and clearance properties and satisfactory metabolic stability to provide adequate systemic exposure to elicit a pharmacodynamic response. If the compounds possess reasonable physicochemical properties, have low to intermediate clearance and reasonable absorption, adequate oral bioavailability may be achieved. Because conducting an in vivo experiment is time-consuming and material-consuming, early discovery efforts have focused on assessing in vitro absorption potential and in vitro metabolic stability. Such experiments are intended to screen compounds and identify candidates that are most likely to have adequate PK properties for further pharmacological evaluation. Modifications of the in vitro and in situ approaches to assess the potential of absorption and metabolism have enabled a higher throughput and an ability to correlate better with in vivo pharmacokinetics of compounds. We have established a strong joint initiative with Drug for Neglected Diseases Initiative (DNDi) and AbbVie. In this partnership, we will evaluate both pharmacokinetic and biological properties of drug candidates. The methods employ will follow the DNDi and AbbVie pipeline for new drugs against parasitic diseases.

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