Banca de QUALIFICAÇÃO: JOHN LENON DE SOUZA SANTOS
Uma banca de QUALIFICAÇÃO de MESTRADO foi cadastrada pelo programa.STUDENT : JOHN LENON DE SOUZA SANTOS
DATE: 31/01/2020
TIME: 10:00
LOCAL: sala da física na biofísica
TITLE:
STUDY OF INTERACTIONS ENERGY BETWEEN THE NOCICEPTIN / ORPHANIN FQ RECEPTOR AND TWO COMPOUNDS WITH ANTIDEPRESSIVE ACTION
KEY WORDS:
Depression, NOP, DFT, MFCC, SB-612111, C-35, Antagonists, Energy analysis
PAGES: 70
BIG AREA: Ciências Biológicas
AREA: Biofísica
SUBÁREA: Biofísica Molecular
SUMMARY:
Depression is a serious disorder common throughout the world and its recurrence is closely linked to harm in the lives of the individuals who carry it. Its main characteristics, such as depressed mood, anhedonia, irritability, concentration difficulties, fatigue, increased or decreased appetite, insomnia or hypersomnia, and cognitive and locomotor losses, justify its gravity. Therefore, there is a great challenge for the development of new drugs for the treatment of depression. In the last two decades, several studies have shown that the NOP receptor can be a valuable therapeutic target in the field of pharmacological therapy. Some pharmacological tools addressing to NOP have been developed, such as the antagonists SB-612111 and compound 35 (C-35). In this sense, the present work aims to evaluate, by means of computer simulation techniques, using the Functional Density Theory (DFT) and the Molecular Fractionation Method with Conjugate Covers (MFCC), the energetic particularities present in the interaction between the NOP receptor and the SB-612111 ligand, as well as between it and the C-35 ligand, which are antagonists. From obtaining the crystalline structures in the PDB and using the tools inherent to the field of computational simulation, it was possible to analyze the energetic contributions present in each complex formed by these binders and the receptor in question. In total 102 (101) amino acid fragments for SB (C-35) were observed, with most of the most energetically relevant residues being part of the hydrophobic bonding pocket and the fragments with the most attractive energy are located at a distance of up to 3 Å, in both complexes: NOP-SB (ASP130 > GLN107 > TYR309 > TYR131); NOP-C-35 (ASP130 > GLN107 > ASP110 > ILE127 > TYR131 > GLN280 > TYR309). The results presented and discussed here are of substantial relevance, given that in recent decades, especially in recent years, there has been intense research and investment in the search for the development of more effective antidepressants. Therefore, analyses as described here can help in the advancement of the pharmacological scenario directed to antidepressants, targeting the NOP receptor.
BANKING MEMBERS:
Presidente - 1352009 - UMBERTO LAINO FULCO
Interno - 2985070 - JONAS IVAN NOBRE OLIVEIRA
Externa ao Programa - 1645202 - ELAINE CRISTINA GAVIOLI