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Conformational flexibility of three cytoplasmic segments of the angiotensin II AT 1 A receptor: a circular dichroism and fluorescence spectroscopy study
Author(s) -
Pertinhez Thelma A.,
Krybus Regina,
Cilli Eduardo M.,
Paiva Antonio C. M.,
Nakaie Clóvis R.,
Franzoni Lorella,
Sartor Giorgio,
Spisni Alberto,
Schreier Shirley
Publication year - 2002
Publication title -
journal of peptide science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.475
H-Index - 66
eISSN - 1099-1387
pISSN - 1075-2617
DOI - 10.1002/psc.364
Subject(s) - circular dichroism , chemistry , biophysics , angiotensin ii , crystallography , intermolecular force , receptor , folding (dsp implementation) , polarity (international relations) , stereochemistry , molecule , biochemistry , biology , organic chemistry , cell , electrical engineering , engineering
The conformation of three synthetic peptides encompassing the proximal and distal half of the third intracellular loop (Ni3 and Ci3) and a portion of the cytoplasmic tail ( f CT) of the angiotensin II AT 1 A receptor has been studied using circular dischroism and fluorescence spectroscopies. The results show that the conformation of the peptides is modulated in various ways by the environmental conditions (pH, ionic strength and dielectric constant). Indeed, Ni3 and f CT fold into helical structures that possess distinct stability and polarity due to the diverse forces involved: mainly polar interactions in the first case and a combination of polar and hydrophobic interactions in the second. The presence of these various features also produce distinct intermolecular interactions. Ci3, instead, exists as an ensemble of partially folded states in equilibrium. Since the corresponding regions of the angiotensin II AT 1 A receptor are known to play an important role in the receptor function, due to their ability to undergo conformational changes, these data provide some new clues about their different conformational plasticity. Copyright © 2002 European Peptide Society and John Wiley & Sons, Ltd.