Crystal Structure and Structural Mechanism of a Novel Anti-Human Immunodeficiency Virus and d -Amino Acid-Containing Chemokine-Reference-Cited by-同舟云学术

Crystal Structure and Structural Mechanism of a Novel Anti-Human Immunodeficiency Virus and d -Amino Acid-Containing Chemokine

Published:2007-10-15 Issue:20 Volume:81 Page:11489-11498
ISSN:0022-538X
Container-title:Journal of Virology
language:en
Short-container-title:J Virol

Author:

Liu Dongxiang¹,Madani Navid²,Li Ying³,Cao Rong³,Choi Won-Tak¹,Kawatkar Sameer P.⁴,Lim Mi Youn⁴,Kumar Santosh¹,Dong Chang-Zhi¹,Wang Jun¹,Russell Julie D.⁵,Lefebure Caroline R.⁵,An Jing¹⁴,Wilson Scott⁶,Gao Yi-Gui⁶,Pallansch Luke A.⁵,Sodroski Joseph G.²,Huang Ziwei¹⁶³

Affiliation:

1. Departments of Biochemistry

2. Department of Cancer Immunology and AIDS, Harvard Medical School, Boston, Massachusetts 02115

3. Center of Biophysics and Computational Biology, University of Illinois at Urbana-Champaign, Urbana, Illinois 61801

4. Raylight Corporation, Chemokine Pharmaceutical Incorporated, La Jolla, California 92037

5. Infectious Disease Research Department, Southern Research Institute, Frederick, Maryland 21701

6. Chemistry

Abstract

ABSTRACT Chemokines and their receptors play important roles in normal physiological functions and the pathogeneses of a wide range of human diseases, including the entry of human immunodeficiency virus type 1 (HIV-1). However, the use of natural chemokines to probe receptor biology or to develop therapeutic drugs is limited by their lack of selectivity and the poor understanding of mechanisms in ligand-receptor recognition. We addressed these issues by combining chemical and structural biology in research into molecular recognition and inhibitor design. Specifically, the concepts of chemical biology were used to develop synthetically and modularly modified (SMM) chemokines that are unnatural and yet have properties improved over those of natural chemokines in terms of receptor selectivity, affinity, and the ability to explore receptor functions. This was followed by using structural biology to determine the structural basis for synthetically perturbed ligand-receptor selectivity. As a proof-of-principle for this combined chemical and structural-biology approach, we report a novel d -amino acid-containing SMM-chemokine designed based on the natural chemokine called viral macrophage inflammatory protein II (vMIP-II). The incorporation of unnatural d -amino acids enhanced the affinity of this molecule for CXCR4 but significantly diminished that for CCR5 or CCR2, thus yielding much more selective recognition of CXCR4 than wild-type vMIP-II. This d -amino acid-containing chemokine also showed more potent and specific inhibitory activity against HIV-1 entry via CXCR4 than natural chemokines. Furthermore, the high-resolution crystal structure of this d -amino acid-containing chemokine and a molecular-modeling study of its complex with CXCR4 provided the structure-based mechanism for the selective interaction between the ligand and chemokine receptors and the potent anti-HIV activity of d -amino acid-containing chemokines.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

Link

https://journals.asm.org/doi/pdf/10.1128/JVI.02845-06

Reference50 articles.

1. Alkhatib, G., C. Combadiere, C. C. Broder, Y. Feng, P. E. Kennedy, and P. M. Murphy. 1996. CC CKR5: a RANTES, MIP-1α, MIP-1β receptor as a fusion cofactor for macrophage-tropic HIV-1. Science272:1955-1958.

2. Amara, A., S. L. Gall, O. Schwartz, J. Salamero, M. Montes, P. Loetscher, M. Baggiolini, J.-L. Virelizier, and F. Arenzana-Seisdedos. 1997. HIV coreceptor downregulation as antiviral principle: SDF-1α-dependent internalization of the chemokine receptor CXCR4 contributes to inhibition of HIV replication. J. Exp. Med.186:139-146.

3. Baggiolini, M., B. Dewald, and B. Moser. 1997. Human chemokines: an update. Annu. Rev. Immunol.15:675-705.

4. CHEMOKINE RECEPTORS AS HIV-1 CORECEPTORS: Roles in Viral Entry, Tropism, and Disease

5. Bleul, C. C., M. Farzan, H. Choe, C. Parolin, I. Clark-Lewis, and J. Sodroski. 1996. The lymphocyte chemoattractant SDF-1 is a ligand for LESTR/fusin and blocks HIV-1 entry. Nature382:829-833.

Cited by 16 articles. 订阅此论文施引文献订阅此论文施引文献，注册后可以免费订阅5篇论文的施引文献，订阅后可以查看论文全部施引文献

1. Biological and mutational analyses of CXCR4–antagonist interactions and design of new antagonistic analogs;Bioscience Reports;2023-12

2. Pathogen-derived peptides in drug targeting and its therapeutic approach;Journal of Controlled Release;2022-10

3. A fragment integrational approach to GPCR inhibition: Identification of a high affinity small molecule CXCR4 antagonist;European Journal of Medicinal Chemistry;2022-03

4. Chemical mutagenesis of a GPCR ligand: Detoxifying “inflammo-attraction” to direct therapeutic stem cell migration;Proceedings of the National Academy of Sciences;2020-11-20

5. Discoveries and developments of CXCR4-targeted HIV-1 entry inhibitors;Experimental Biology and Medicine;2020-02-04