Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)

Background: Targeting the CD47/SIRPα signaling pathway represents a novel approach to enhance anti-tumor immunity. However, the crystal structure of the CD47/SIRPα has not been fully studied. This study aims to analyze the structure interface of the complex of CD47 and IMM01, a novel recombinant SIR...

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Autores principales: Yu, Jifeng, Li, Song, Chen, Dianze, Liu, Dandan, Guo, Huiqin, Yang, Chunmei, Zhang, Wei, Zhang, Li, Zhao, Gui, Tu, Xiaoping, Peng, Liang, Liu, Sijin, Bai, Xing, Song, Yongping, Jiang, Zhongxing, Zhang, Ruliang, Tian, Wenzhi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9457805/
https://www.ncbi.nlm.nih.gov/pubmed/36080360
http://dx.doi.org/10.3390/molecules27175574
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author Yu, Jifeng
Li, Song
Chen, Dianze
Liu, Dandan
Guo, Huiqin
Yang, Chunmei
Zhang, Wei
Zhang, Li
Zhao, Gui
Tu, Xiaoping
Peng, Liang
Liu, Sijin
Bai, Xing
Song, Yongping
Jiang, Zhongxing
Zhang, Ruliang
Tian, Wenzhi
author_facet Yu, Jifeng
Li, Song
Chen, Dianze
Liu, Dandan
Guo, Huiqin
Yang, Chunmei
Zhang, Wei
Zhang, Li
Zhao, Gui
Tu, Xiaoping
Peng, Liang
Liu, Sijin
Bai, Xing
Song, Yongping
Jiang, Zhongxing
Zhang, Ruliang
Tian, Wenzhi
author_sort Yu, Jifeng
collection PubMed
description Background: Targeting the CD47/SIRPα signaling pathway represents a novel approach to enhance anti-tumor immunity. However, the crystal structure of the CD47/SIRPα has not been fully studied. This study aims to analyze the structure interface of the complex of CD47 and IMM01, a novel recombinant SIRPα-Fc fusion protein. Methods: IMM01-Fab/CD47 complex was crystalized, and diffraction images were collected. The complex structure was determined by molecular replacement using the program PHASER with the CD47-SIRPαv2 structure (PDB code 2JJT) as a search model. The model was manually built using the COOT program and refined using TLS parameters in REFMAC from the CCP4 program suite. Results: Crystallization and structure determination analysis of the interface of IMM01/CD47 structure demonstrated CD47 surface buried by IMM01. Comparison with the literature structure (PDB ID 2JJT) showed that the interactions of IMM01/CD47 structure are the same. All the hydrogen bonds that appear in the literature structure are also present in the IMM01/CD47 structure. These common hydrogen bonds are stable under different crystal packing styles, suggesting that these hydrogen bonds are important for protein binding. In the structure of human CD47 in complex with human SIRPα, except SER66, the amino acids that form hydrogen bonds are all conserved. Furthermore, comparing with the structure of PDB ID 2JJT, the salt bridge interaction from IMM01/CD47 structure are very similar, except the salt bridge bond between LYS53 in IMM01 and GLU106 in CD47, which only occurs between the B and D chains. However, as the side chain conformation of LYS53 in chain A is slightly different, the salt bridge bond is absent between the A and C chains. At this site between chain A and chain C, there are a salt bridge bond between LYS53 (A) and GLU104 (C) and a salt bridge bond between HIS56 (A) and GLU106 (C) instead. According to the sequence alignment results of SIRPα, SIRPβ and SIRPγ in the literature of PDB ID 2JJT, except ASP100, the amino acids that form common salt bridge bonds are all conserved. Conclusion: Our data demonstrated crystal structure of the IMM01/CD47 complex and provides a structural basis for the structural binding interface and future clinical applications.
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spelling pubmed-94578052022-09-09 Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A) Yu, Jifeng Li, Song Chen, Dianze Liu, Dandan Guo, Huiqin Yang, Chunmei Zhang, Wei Zhang, Li Zhao, Gui Tu, Xiaoping Peng, Liang Liu, Sijin Bai, Xing Song, Yongping Jiang, Zhongxing Zhang, Ruliang Tian, Wenzhi Molecules Article Background: Targeting the CD47/SIRPα signaling pathway represents a novel approach to enhance anti-tumor immunity. However, the crystal structure of the CD47/SIRPα has not been fully studied. This study aims to analyze the structure interface of the complex of CD47 and IMM01, a novel recombinant SIRPα-Fc fusion protein. Methods: IMM01-Fab/CD47 complex was crystalized, and diffraction images were collected. The complex structure was determined by molecular replacement using the program PHASER with the CD47-SIRPαv2 structure (PDB code 2JJT) as a search model. The model was manually built using the COOT program and refined using TLS parameters in REFMAC from the CCP4 program suite. Results: Crystallization and structure determination analysis of the interface of IMM01/CD47 structure demonstrated CD47 surface buried by IMM01. Comparison with the literature structure (PDB ID 2JJT) showed that the interactions of IMM01/CD47 structure are the same. All the hydrogen bonds that appear in the literature structure are also present in the IMM01/CD47 structure. These common hydrogen bonds are stable under different crystal packing styles, suggesting that these hydrogen bonds are important for protein binding. In the structure of human CD47 in complex with human SIRPα, except SER66, the amino acids that form hydrogen bonds are all conserved. Furthermore, comparing with the structure of PDB ID 2JJT, the salt bridge interaction from IMM01/CD47 structure are very similar, except the salt bridge bond between LYS53 in IMM01 and GLU106 in CD47, which only occurs between the B and D chains. However, as the side chain conformation of LYS53 in chain A is slightly different, the salt bridge bond is absent between the A and C chains. At this site between chain A and chain C, there are a salt bridge bond between LYS53 (A) and GLU104 (C) and a salt bridge bond between HIS56 (A) and GLU106 (C) instead. According to the sequence alignment results of SIRPα, SIRPβ and SIRPγ in the literature of PDB ID 2JJT, except ASP100, the amino acids that form common salt bridge bonds are all conserved. Conclusion: Our data demonstrated crystal structure of the IMM01/CD47 complex and provides a structural basis for the structural binding interface and future clinical applications. MDPI 2022-08-30 /pmc/articles/PMC9457805/ /pubmed/36080360 http://dx.doi.org/10.3390/molecules27175574 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Yu, Jifeng
Li, Song
Chen, Dianze
Liu, Dandan
Guo, Huiqin
Yang, Chunmei
Zhang, Wei
Zhang, Li
Zhao, Gui
Tu, Xiaoping
Peng, Liang
Liu, Sijin
Bai, Xing
Song, Yongping
Jiang, Zhongxing
Zhang, Ruliang
Tian, Wenzhi
Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)
title Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)
title_full Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)
title_fullStr Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)
title_full_unstemmed Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)
title_short Crystal Structure of Human CD47 in Complex with Engineered SIRPα.D1(N80A)
title_sort crystal structure of human cd47 in complex with engineered sirpα.d1(n80a)
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9457805/
https://www.ncbi.nlm.nih.gov/pubmed/36080360
http://dx.doi.org/10.3390/molecules27175574
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