Identification of positions in the human neuropeptide Y/peptide YY receptor Y2 that contribute to pharmacological differences between receptor subtypes

Abstract The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and pancreatic polypeptide (PP) which interact with distinct preference for the four receptors showing very low sequence identity, i.e. Y1, Y2, Y...

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Published in:	Neuropeptides (Edinburgh) Vol. 45; no. 4; pp. 293 - 300
Main Authors:	Fällmar, Helena, Åkerberg, Helena, Gutiérrez-de-Terán, Hugo, Lundell, Ingrid, Mohell, Nina, Larhammar, Dan
Format:	Journal Article
Language:	English
Published:	Kidlington Elsevier Ltd 01-08-2011 Elsevier
Subjects:	Advanced Basic Science Amino Acid Sequence Animals Appetite regulation BIIE0246 Binding experiment Biological and medical sciences Endocrinology & Metabolism Fundamental and applied biological sciences. Psychology HEK293 Cells Humans Ligands Models, Molecular Molecular Sequence Data Mutagenesis, Site-Directed Neuropeptide Y Neuropeptide Y - metabolism Peptide YY Peptide YY - metabolism Protein Binding Protein Conformation Protein Isoforms - chemistry Protein Isoforms - genetics Protein Isoforms - metabolism Receptors, Gastrointestinal Hormone - chemistry Receptors, Gastrointestinal Hormone - genetics Receptors, Gastrointestinal Hormone - metabolism Receptors, Neuropeptide Y - chemistry Receptors, Neuropeptide Y - genetics Receptors, Neuropeptide Y - metabolism Sequence Alignment Vertebrates: endocrinology Y1 receptor Y2 receptor PP neuropeptide Y Y1 receptor dissociation constant phosphate-buffered saline K d BIIE0246 GFP human embryonic kidney K i NPY peptide YY pancreatic polypeptide wt human polymerase chain reaction G protein-coupled receptor PBS Appetite regulation maximal binding capacity inhibition constant h porcine green fluorescent protein HEK p PYY Binding experiment B max Y2 receptor GPCR wild type PCR Neuropeptide Y Peptide YY Appetite Human Peptide hormone YY peptide Subtype Biological receptor
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Abstract	Abstract The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and pancreatic polypeptide (PP) which interact with distinct preference for the four receptors showing very low sequence identity, i.e. Y1, Y2, Y4 and Y5. The binding of similar peptides to these divergent receptors makes them highly interesting for mutagenesis studies. We present here a site-directed mutagenesis study of four amino acid positions in the human Y2 receptor. T3.40 was selected based on sequence alignments both between subtypes and between species and G2.68 , L4.60 and Q6.55 also on previous binding studies of the corresponding positions in the Y1 receptor. The mutated receptors were characterized pharmacologically with the peptide agonists NPY, PYY, PYY(3–36), NPY(13–36) and the non-peptide antagonist BIIE0246. Interestingly, the affinity of NPY and PYY(3–36) increased for the mutants T3.40 I and Q6.55 A. Increased affinity was also observed for PYY to Q6.55 A. PYY(3–36) displayed decreased affinity for G2.68 N and L4.60 A whereas binding of NPY(13–36) was unaffected by all mutations. The antagonist BIIE0246 showed decreased affinity for T3.40 I, L4.60 A and Q6.55 A. Although all positions investigated were found important for interaction with at least one of the tested ligands the corresponding positions in hY1 seem to be of greater importance for ligand binding. Furthermore these data indicate that binding of the agonists and the antagonist differs in their points of interaction. The increase in the binding affinity observed may reflect an indirect effect caused by a conformational change of the receptor. These findings will help to improve the structural models of the human NPY receptors.
AbstractList	The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and pancreatic polypeptide (PP) which interact with distinct preference for the four receptors showing very low sequence identity, i.e. Y1, Y2, Y4 and Y5. The binding of similar peptides to these divergent receptors makes them highly interesting for mutagenesis studies. We present here a site-directed mutagenesis study of four amino acid positions in the human Y2 receptor. T super(3.40 was selected based on sequence alignments both between subtypes and between species and G) super(2).68, L super(4.60 and Q) super(6).55 also on previous binding studies of the corresponding positions in the Y1 receptor. The mutated receptors were characterized pharmacologically with the peptide agonists NPY, PYY, PYY(3-36), NPY(13-36) and the non-peptide antagonist BIIE0246. Interestingly, the affinity of NPY and PYY(3-36) increased for the mutants T super(3.40I and Q) super(6).55A. Increased affinity was also observed for PYY to Q super(6.55A. PYY(3-36) displayed decreased affinity for G) super(2).68N and L super(4.60A whereas binding of NPY(13-36) was unaffected by all mutations. The antagonist BIIE0246 showed decreased affinity for T) super(3).40I, L super(4.60A and Q) super(6).55A. Although all positions investigated were found important for interaction with at least one of the tested ligands the corresponding positions in hY1 seem to be of greater importance for ligand binding. Furthermore these data indicate that binding of the agonists and the antagonist differs in their points of interaction. The increase in the binding affinity observed may reflect an indirect effect caused by a conformational change of the receptor. These findings will help to improve the structural models of the human NPY receptors. The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and pancreatic polypeptide (PP) which interact with distinct preference for the four receptors showing very low sequence identity, i.e. Y1, Y2, Y4 and Y5. The binding of similar peptides to these divergent receptors makes them highly interesting for mutagenesis studies. We present here a site-directed mutagenesis study of four amino acid positions in the human Y2 receptor. T(3.40) was selected based on sequence alignments both between subtypes and between species and G(2.68), L(4.60) and Q(6.55) also on previous binding studies of the corresponding positions in the Y1 receptor. The mutated receptors were characterized pharmacologically with the peptide agonists NPY, PYY, PYY(3-36), NPY(13-36) and the non-peptide antagonist BIIE0246. Interestingly, the affinity of NPY and PYY(3-36) increased for the mutants T(3.40)I and Q(6.55)A. Increased affinity was also observed for PYY to Q(6.55)A. PYY(3-36) displayed decreased affinity for G(2.68)N and L(4.60)A whereas binding of NPY(13-36) was unaffected by all mutations. The antagonist BIIE0246 showed decreased affinity for T(3.40)I, L(4.60)A and Q(6.55)A. Although all positions investigated were found important for interaction with at least one of the tested ligands the corresponding positions in hY1 seem to be of greater importance for ligand binding. Furthermore these data indicate that binding of the agonists and the antagonist differs in their points of interaction. The increase in the binding affinity observed may reflect an indirect effect caused by a conformational change of the receptor. These findings will help to improve the structural models of the human NPY receptors. The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and pancreatic polypeptide (PP) which interact with distinct preference for the four receptors showing very low sequence identity, i.e. Y1, Y2, Y4 and Y5. The binding of similar peptides to these divergent receptors makes them highly interesting for mutagenesis studies. We present here a site-directed mutagenesis study of four amino acid positions in the human Y2 receptor. T 3.40 was selected based on sequence alignments both between subtypes and between species and G 2.68, L 4.60 and Q 6.55 also on previous binding studies of the corresponding positions in the Y1 receptor. The mutated receptors were characterized pharmacologically with the peptide agonists NPY, PYY, PYY(3–36), NPY(13–36) and the non-peptide antagonist BIIE0246. Interestingly, the affinity of NPY and PYY(3–36) increased for the mutants T 3.40I and Q 6.55A. Increased affinity was also observed for PYY to Q 6.55A. PYY(3–36) displayed decreased affinity for G 2.68N and L 4.60A whereas binding of NPY(13–36) was unaffected by all mutations. The antagonist BIIE0246 showed decreased affinity for T 3.40I, L 4.60A and Q 6.55A. Although all positions investigated were found important for interaction with at least one of the tested ligands the corresponding positions in hY1 seem to be of greater importance for ligand binding. Furthermore these data indicate that binding of the agonists and the antagonist differs in their points of interaction. The increase in the binding affinity observed may reflect an indirect effect caused by a conformational change of the receptor. These findings will help to improve the structural models of the human NPY receptors. Abstract The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and pancreatic polypeptide (PP) which interact with distinct preference for the four receptors showing very low sequence identity, i.e. Y1, Y2, Y4 and Y5. The binding of similar peptides to these divergent receptors makes them highly interesting for mutagenesis studies. We present here a site-directed mutagenesis study of four amino acid positions in the human Y2 receptor. T3.40 was selected based on sequence alignments both between subtypes and between species and G2.68 , L4.60 and Q6.55 also on previous binding studies of the corresponding positions in the Y1 receptor. The mutated receptors were characterized pharmacologically with the peptide agonists NPY, PYY, PYY(3–36), NPY(13–36) and the non-peptide antagonist BIIE0246. Interestingly, the affinity of NPY and PYY(3–36) increased for the mutants T3.40 I and Q6.55 A. Increased affinity was also observed for PYY to Q6.55 A. PYY(3–36) displayed decreased affinity for G2.68 N and L4.60 A whereas binding of NPY(13–36) was unaffected by all mutations. The antagonist BIIE0246 showed decreased affinity for T3.40 I, L4.60 A and Q6.55 A. Although all positions investigated were found important for interaction with at least one of the tested ligands the corresponding positions in hY1 seem to be of greater importance for ligand binding. Furthermore these data indicate that binding of the agonists and the antagonist differs in their points of interaction. The increase in the binding affinity observed may reflect an indirect effect caused by a conformational change of the receptor. These findings will help to improve the structural models of the human NPY receptors.
Author	Åkerberg, Helena Gutiérrez-de-Terán, Hugo Mohell, Nina Fällmar, Helena Lundell, Ingrid Larhammar, Dan
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Keywords	PP neuropeptide Y Y1 receptor dissociation constant phosphate-buffered saline K d BIIE0246 GFP human embryonic kidney K i NPY peptide YY pancreatic polypeptide wt human polymerase chain reaction G protein-coupled receptor PBS Appetite regulation maximal binding capacity inhibition constant h porcine green fluorescent protein HEK p PYY Binding experiment B max Y2 receptor GPCR wild type PCR Neuropeptide Y Peptide YY Appetite Human Peptide hormone YY peptide Subtype Biological receptor
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Snippet	Abstract The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and... The members of the neuropeptide Y (NPY) family are key players in food-intake regulation. In humans this family consists of NPY, peptide YY (PYY) and...
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SubjectTerms	Advanced Basic Science Amino Acid Sequence Animals Appetite regulation BIIE0246 Binding experiment Biological and medical sciences Endocrinology & Metabolism Fundamental and applied biological sciences. Psychology HEK293 Cells Humans Ligands Models, Molecular Molecular Sequence Data Mutagenesis, Site-Directed Neuropeptide Y Neuropeptide Y - metabolism Peptide YY Peptide YY - metabolism Protein Binding Protein Conformation Protein Isoforms - chemistry Protein Isoforms - genetics Protein Isoforms - metabolism Receptors, Gastrointestinal Hormone - chemistry Receptors, Gastrointestinal Hormone - genetics Receptors, Gastrointestinal Hormone - metabolism Receptors, Neuropeptide Y - chemistry Receptors, Neuropeptide Y - genetics Receptors, Neuropeptide Y - metabolism Sequence Alignment Vertebrates: endocrinology Y1 receptor Y2 receptor
Title	Identification of positions in the human neuropeptide Y/peptide YY receptor Y2 that contribute to pharmacological differences between receptor subtypes
URI	https://www.clinicalkey.es/playcontent/1-s2.0-S014341791100045X https://dx.doi.org/10.1016/j.npep.2011.05.006 https://www.ncbi.nlm.nih.gov/pubmed/21696823 https://search.proquest.com/docview/888117800 https://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-156633
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