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Selective use of primate CD4 receptors by HIV-1
- Source :
- PLOS Biology, PLoS Biology, PLoS Biology, Vol 17, Iss 6, p e3000304 (2019)
- Publication Year :
- 2019
- Publisher :
- Public Library of Science (PLoS), 2019.
-
Abstract
- Individuals chronically infected with HIV-1 harbor complex viral populations within their bloodstreams. Recently, it has come to light that when these people infect others, the new infection is typically established by only one or a small number of virions from within this complex viral swarm. An important goal is to characterize the biological properties of HIV-1 virions that seed and exist early in new human infections because these are potentially the only viruses against which a prophylactic HIV-1 vaccine would need to elicit protection. This includes understanding how the Envelope (Env) protein of these virions interacts with the T-cell receptor CD4, which supports attachment and entry of HIV-1 into target cells. We examined early HIV-1 isolates for their ability to infect cells via the CD4 receptor of 15 different primate species. Primates were the original source of HIV-1 and now serve as valuable animal models for studying HIV-1. We find that most primary isolates of HIV-1 from the blood, including early isolates, are highly selective and enter cells through some primate CD4 receptor orthologs but not others. This phenotype is remarkably consistent, regardless of route of transmission, viral subtype, or time of isolation post infection. We show that the weak CD4 binding affinity of blood-derived HIV-1 isolates is what makes them sensitive to the small sequence differences in CD4 from one primate species to the next. To substantiate this, we engineered an early HIV-1 Env to have high, medium, or low binding affinity to CD4, and we show that it loses the ability to enter cells via the CD4 receptor of many primate species as the binding affinity gets weaker. Based on the phenotype of selective use of primate CD4, we find that weak CD4 binding appears to be a nearly universal property of HIV-1 circulating in the bloodstream. Therefore, weak binding to CD4 must be a selected and important property in the biology of HIV-1 in the body. We identify six primate species that encode CD4 receptors that fully support the entry of early HIV-1 isolates despite their low binding affinity for CD4. These findings will help inform long-standing efforts to model HIV-1 transmission and early disease in primates.<br />The current animal model for HIV, the macaque, encodes a CD4 receptor that is non-permissive for HIV entry. This paper reveals that six primate species encode CD4 receptors compatible with HIV infection, potentially making them powerful tools for the study of HIV biology. Furthermore, weak CD4 binding is a nearly constant, and apparently selected, property of HIV circulating in the human bloodstream.
- Subjects :
- RNA viruses
0301 basic medicine
Physiology
Human immunodeficiency virus (HIV)
HIV Infections
Signal transduction
Monkeys
HIV Envelope Protein gp120
Pathology and Laboratory Medicine
medicine.disease_cause
Biochemistry
Macaque
Green fluorescent protein
0302 clinical medicine
Immunodeficiency Viruses
HIV Seropositivity
Medicine and Health Sciences
Primate
Biology (General)
Receptor
Mammals
biology
Transmission (medicine)
General Neuroscience
env Gene Products, Human Immunodeficiency Virus
Eukaryota
Animal Models
Cd4 receptors
Phenotype
Body Fluids
3. Good health
Blood
Experimental Organism Systems
Medical Microbiology
Viral Pathogens
Viruses
Vertebrates
CD4 Antigens
Aotidae
Pathogens
Anatomy
General Agricultural and Biological Sciences
Coreceptors
Research Article
Primates
Cell biology
QH301-705.5
Research and Analysis Methods
Microbiology
Green Fluorescent Protein
General Biochemistry, Genetics and Molecular Biology
Cell Line
03 medical and health sciences
biology.animal
Retroviruses
Old World monkeys
medicine
Animals
Humans
CCR5 coreceptor
Microbial Pathogens
Rhesus Monkeys
General Immunology and Microbiology
Lentivirus
Organisms
Biology and Life Sciences
HIV
Proteins
CD coreceptors
Macaca mulatta
Virology
Luminescent Proteins
Disease Models, Animal
HEK293 Cells
030104 developmental biology
Amniotes
HIV-1
Animal Studies
030217 neurology & neurosurgery
Subjects
Details
- ISSN :
- 15457885
- Volume :
- 17
- Database :
- OpenAIRE
- Journal :
- PLOS Biology
- Accession number :
- edsair.doi.dedup.....b476555bfbae0e6f3a435bd16f10188a
- Full Text :
- https://doi.org/10.1371/journal.pbio.3000304