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1qvo

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STRUCTURES OF HLA-A*1101 IN COMPLEX WITH IMMUNODOMINANT NONAMER AND DECAMER HIV-1 EPITOPES CLEARLY REVEAL THE PRESENCE OF A MIDDLE ANCHOR RESIDUE

1 Overview
2 Disease
3 About this Structure
4 Reference

Overview

HLA-A*1101 is one of the most common human class I alleles worldwide. An increased frequency of HLA-A*1101 has been observed in cohorts of female sex workers from Northern Thailand who are highly exposed to HIV-1 and yet have remained persistently seronegative. In view of this apparent association of HLA-A*1101 with resistance to acquisition of HIV-1 infection, and given the importance of eliciting strong CTL responses to control and eliminate HIV-1, we have determined the crystal structure of HLA-A*1101 complexed with two immunodominant HIV-1 CTL epitopes: the nonamer reverse transcriptase(313-321) (AIFQSSMTK) and decamer Nef(73-82) (QVPLRPMTYK) peptides. The structures confirm the presence of primary anchor residues P2-Ile/-Val and P9-/P10-Lys, and also clearly reveal the presence of secondary anchor residues P6-Ser for reverse transcriptase and P7-Met for Nef. The overall backbone conformation of both peptides is defined as two bulges that are separated by a more buried middle residue. In this study, we discuss how this topology may offer functional advantages in the selection and presentation of HIV-1 CTL epitopes by HLA-A*1101. Overall, this structural analysis permits a more accurate definition of the peptide-binding motif of HLA-A*1101, the characterization of its antigenic surface, and the correlation of molecular determinants with resistance to HIV-1 infection. These studies are relevant for the rational design of HLA-A*1101-restricted CTL epitopes with improved binding and immunological properties for the development of HIV-1 vaccines.

Disease

Known diseases associated with this structure: Abacavir hypersensitivity, susceptibility to OMIM:[142800], Ankylosing spondylitis, susceptibility to, 1 OMIM:[142800], Hypoproteinemia, hypercatabolic OMIM:[109700], Stevens-Johnson syndrome, susceptibility to OMIM:[142800]

About this Structure

1QVO is a Protein complex structure of sequences from Homo sapiens. Full crystallographic information is available from OCA.

Reference

Structures of HLA-A*1101 complexed with immunodominant nonamer and decamer HIV-1 epitopes clearly reveal the presence of a middle, secondary anchor residue., Li L, Bouvier M, J Immunol. 2004 May 15;172(10):6175-84. PMID:15128805

Page seeded by OCA on Thu Feb 21 14:44:18 2008

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OCA

Retrieved from "http://52.214.119.220/wiki/index.php/1qvo"

@@ Line 1: / Line 1: @@
-[[Image:1qvo.gif|left|200px]]<br />
+[[Image:1qvo.gif|left|200px]]<br /><applet load="1qvo" size="350" color="white" frame="true" align="right" spinBox="true"
-<applet load="1qvo" size="450" color="white" frame="true" align="right" spinBox="true"
 caption="1qvo, resolution 2.22&Aring;" />
 '''STRUCTURES OF HLA-A*1101 IN COMPLEX WITH IMMUNODOMINANT NONAMER AND DECAMER HIV-1 EPITOPES CLEARLY REVEAL THE PRESENCE OF A MIDDLE ANCHOR RESIDUE'''<br />
 ==Overview==
-HLA-A*1101 is one of the most common human class I alleles worldwide. An, increased frequency of HLA-A*1101 has been observed in cohorts of female, sex workers from Northern Thailand who are highly exposed to HIV-1 and yet, have remained persistently seronegative. In view of this apparent, association of HLA-A*1101 with resistance to acquisition of HIV-1, infection, and given the importance of eliciting strong CTL responses to, control and eliminate HIV-1, we have determined the crystal structure of, HLA-A*1101 complexed with two immunodominant HIV-1 CTL epitopes: the, nonamer reverse transcriptase(313-321) (AIFQSSMTK) and decamer Nef(73-82), (QVPLRPMTYK) peptides. The structures confirm the presence of primary, anchor residues P2-Ile/-Val and P9-/P10-Lys, and also clearly reveal the, presence of secondary anchor residues P6-Ser for reverse transcriptase and, P7-Met for Nef. The overall backbone conformation of both peptides is, defined as two bulges that are separated by a more buried middle residue., In this study, we discuss how this topology may offer functional, advantages in the selection and presentation of HIV-1 CTL epitopes by, HLA-A*1101. Overall, this structural analysis permits a more accurate, definition of the peptide-binding motif of HLA-A*1101, the, characterization of its antigenic surface, and the correlation of, molecular determinants with resistance to HIV-1 infection. These studies, are relevant for the rational design of HLA-A*1101-restricted CTL epitopes, with improved binding and immunological properties for the development of, HIV-1 vaccines.
+HLA-A*1101 is one of the most common human class I alleles worldwide. An increased frequency of HLA-A*1101 has been observed in cohorts of female sex workers from Northern Thailand who are highly exposed to HIV-1 and yet have remained persistently seronegative. In view of this apparent association of HLA-A*1101 with resistance to acquisition of HIV-1 infection, and given the importance of eliciting strong CTL responses to control and eliminate HIV-1, we have determined the crystal structure of HLA-A*1101 complexed with two immunodominant HIV-1 CTL epitopes: the nonamer reverse transcriptase(313-321) (AIFQSSMTK) and decamer Nef(73-82) (QVPLRPMTYK) peptides. The structures confirm the presence of primary anchor residues P2-Ile/-Val and P9-/P10-Lys, and also clearly reveal the presence of secondary anchor residues P6-Ser for reverse transcriptase and P7-Met for Nef. The overall backbone conformation of both peptides is defined as two bulges that are separated by a more buried middle residue. In this study, we discuss how this topology may offer functional advantages in the selection and presentation of HIV-1 CTL epitopes by HLA-A*1101. Overall, this structural analysis permits a more accurate definition of the peptide-binding motif of HLA-A*1101, the characterization of its antigenic surface, and the correlation of molecular determinants with resistance to HIV-1 infection. These studies are relevant for the rational design of HLA-A*1101-restricted CTL epitopes with improved binding and immunological properties for the development of HIV-1 vaccines.
 ==Disease==
@@ Line 11: / Line 10: @@
 ==About this Structure==
-QVO is a [http://en.wikipedia.org/wiki/Protein_complex Protein complex] structure of sequences from [http://en.wikipedia.org/wiki/Homo_sapiens Homo sapiens]. Full crystallographic information is available from [http://ispc.weizmann.ac.il/oca-bin/ocashort?id=1QVO OCA].
+QVO is a [http://en.wikipedia.org/wiki/Protein_complex Protein complex] structure of sequences from [http://en.wikipedia.org/wiki/Homo_sapiens Homo sapiens]. Full crystallographic information is available from [http://oca.weizmann.ac.il/oca-bin/ocashort?id=1QVO OCA].
 ==Reference==
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 [[Category: Bouvier, M.]]
 [[Category: Li, L.]]
-[[Category: McNicholl, J.M.]]
+[[Category: McNicholl, J M.]]
 [[Category: immune system]]
-''Page seeded by [http://ispc.weizmann.ac.il/oca OCA ] on Mon Nov 12 18:57:00 2007''
+''Page seeded by [http://oca.weizmann.ac.il/oca OCA ] on Thu Feb 21 14:44:18 2008''

1qvo

From Proteopedia

Revision as of 12:44, 21 February 2008

Contents

Overview

Disease

About this Structure

Reference

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