Optimization and structure-activity relationships of phosphinic pseudotripeptide inhibitors of aminopeptidases that generate antigenic peptides
Optimization and structure-activity relationships of phosphinic pseudotripeptide inhibitors of aminopeptidases that generate antigenic peptides
The oxytocinase subfamily of M1 aminopeptidases, consisting of ER aminopeptidase 1 (ERAP1), ER aminopeptidase 2 (ERAP2), and insulin-regulated aminopeptidase (IRAP), plays critical roles in the generation of antigenic peptides and indirectly regulates human adaptive immune responses. We have previously demonstrated that phosphinic pseudotripeptides can constitute potent inhibitors of this group of enzymes. In this study, we used synthetic methodologies able to furnish a series of stereochemically defined phosphinic pseudotripeptides and demonstrate that side chains at P1′ and P2′ positions are critical determinants in driving potency and selectivity. We identified low nanomolar inhibitors of ERAP2 and IRAP that display selectivity of more than 2 and 3 orders of magnitude, respectively. Cellular analysis demonstrated that one of the compounds that is a selective IRAP inhibitor can reduce IRAP-dependent but not ERAP1-dependent cross-presentation by dendritic cells with nanomolar efficacy. Our results encourage further preclinical development of phosphinic pseudotripeptides as regulators of adaptive immune responses.
9107-9123
Kokkala, Paraskevi
d9dba396-95d5-42b6-b26b-dd28a80c10d5
Mpakali, Anastasia
7e75e4c1-4bfc-4f7e-ba2c-2602f02d517b
Mauvais, Francois Xavier
2378542b-7332-4d04-958a-659d7c7b56f0
Papakyriakou, Athanasios
939bc8c9-1693-4530-9099-c55772b22f1d
Daskalaki, Ira
cc74790f-5efa-43e8-8590-c7fd54cc183a
Petropoulou, Ioanna
de8a1408-039d-4011-877e-febda28ddf02
Kavvalou, Sofia
60f926bf-2145-4796-95d0-aee4e29d684a
Papathanasopoulou, Mirto
d6d224e4-7b3a-49ae-9b76-a10b177b33a7
Agrotis, Stefanos
29d215c5-a2e7-4388-89f3-dfff61cbe33f
Fonsou, Theodora Markisia
7578eb5f-ab36-44ac-a5ac-143557bda239
Van Endert, Peter
17d8b50b-53a0-4064-b054-bd42f425acf4
Stratikos, Efstratios
85f4a2e4-422a-4dab-a067-f50ea7238c00
Georgiadis, Dimitris
a8c4d24c-cb85-4722-b021-796f5411e797
29 September 2016
Kokkala, Paraskevi
d9dba396-95d5-42b6-b26b-dd28a80c10d5
Mpakali, Anastasia
7e75e4c1-4bfc-4f7e-ba2c-2602f02d517b
Mauvais, Francois Xavier
2378542b-7332-4d04-958a-659d7c7b56f0
Papakyriakou, Athanasios
939bc8c9-1693-4530-9099-c55772b22f1d
Daskalaki, Ira
cc74790f-5efa-43e8-8590-c7fd54cc183a
Petropoulou, Ioanna
de8a1408-039d-4011-877e-febda28ddf02
Kavvalou, Sofia
60f926bf-2145-4796-95d0-aee4e29d684a
Papathanasopoulou, Mirto
d6d224e4-7b3a-49ae-9b76-a10b177b33a7
Agrotis, Stefanos
29d215c5-a2e7-4388-89f3-dfff61cbe33f
Fonsou, Theodora Markisia
7578eb5f-ab36-44ac-a5ac-143557bda239
Van Endert, Peter
17d8b50b-53a0-4064-b054-bd42f425acf4
Stratikos, Efstratios
85f4a2e4-422a-4dab-a067-f50ea7238c00
Georgiadis, Dimitris
a8c4d24c-cb85-4722-b021-796f5411e797
Kokkala, Paraskevi, Mpakali, Anastasia, Mauvais, Francois Xavier, Papakyriakou, Athanasios, Daskalaki, Ira, Petropoulou, Ioanna, Kavvalou, Sofia, Papathanasopoulou, Mirto, Agrotis, Stefanos, Fonsou, Theodora Markisia, Van Endert, Peter, Stratikos, Efstratios and Georgiadis, Dimitris
(2016)
Optimization and structure-activity relationships of phosphinic pseudotripeptide inhibitors of aminopeptidases that generate antigenic peptides.
Journal of Medicinal Chemistry, 59 (19), .
(doi:10.1021/acs.jmedchem.6b01031).
Abstract
The oxytocinase subfamily of M1 aminopeptidases, consisting of ER aminopeptidase 1 (ERAP1), ER aminopeptidase 2 (ERAP2), and insulin-regulated aminopeptidase (IRAP), plays critical roles in the generation of antigenic peptides and indirectly regulates human adaptive immune responses. We have previously demonstrated that phosphinic pseudotripeptides can constitute potent inhibitors of this group of enzymes. In this study, we used synthetic methodologies able to furnish a series of stereochemically defined phosphinic pseudotripeptides and demonstrate that side chains at P1′ and P2′ positions are critical determinants in driving potency and selectivity. We identified low nanomolar inhibitors of ERAP2 and IRAP that display selectivity of more than 2 and 3 orders of magnitude, respectively. Cellular analysis demonstrated that one of the compounds that is a selective IRAP inhibitor can reduce IRAP-dependent but not ERAP1-dependent cross-presentation by dendritic cells with nanomolar efficacy. Our results encourage further preclinical development of phosphinic pseudotripeptides as regulators of adaptive immune responses.
This record has no associated files available for download.
More information
Submitted date: 12 July 2016
Accepted/In Press date: 8 September 2016
e-pub ahead of print date: 8 September 2016
Published date: 29 September 2016
Identifiers
Local EPrints ID: 414119
URI: http://eprints.soton.ac.uk/id/eprint/414119
ISSN: 0022-2623
PURE UUID: 21ed74c4-8940-4e15-80e8-6d80c3d1d549
Catalogue record
Date deposited: 14 Sep 2017 16:32
Last modified: 16 Mar 2024 04:28
Export record
Altmetrics
Contributors
Author:
Paraskevi Kokkala
Author:
Anastasia Mpakali
Author:
Francois Xavier Mauvais
Author:
Athanasios Papakyriakou
Author:
Ira Daskalaki
Author:
Ioanna Petropoulou
Author:
Sofia Kavvalou
Author:
Mirto Papathanasopoulou
Author:
Stefanos Agrotis
Author:
Theodora Markisia Fonsou
Author:
Peter Van Endert
Author:
Efstratios Stratikos
Author:
Dimitris Georgiadis
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics