Abstract
CCR5, a chemokine receptor central for orchestrating lymphocyte/cell migration to the sites of inflammation and to the immunosurveillance, is involved in the pathogenesis of a wide spectrum of health conditions, including inflammatory diseases, viral infections, cancers and autoimmune diseases. CCR5 is also the primary coreceptor for the human immunodeficiency viruses (HIVs), supporting its entry into CD4+ T lymphocytes upon transmission and in the early stages of infection in humans. A natural loss-of-function mutation CCR5-Δ32, preventing the mutated protein expression on the cell surface, renders homozygous carriers of the null allele resistant to HIV-1 infection. This phenomenon was leveraged in the development of therapies and cure strategies for AIDS. Meanwhile, over 40 African nonhuman primate species are long-term hosts of simian immunodeficiency virus (SIV), an ancestral family of viruses that give rise to the pandemic CCR5 (R5)-tropic HIV-1. Many natural hosts typically do not progress to immunodeficiency upon the SIV infection. They have developed various strategies to minimize the SIV-related pathogenesis and disease progression, including an array of mechanisms employing modulation of the CCR5 receptor activity: (i) deletion mutations abrogating the CCR5 surface expression and conferring resistance to infection in null homozygotes; (ii) downregulation of CCR5 expression on CD4+ T cells, particularly memory cells and cells at the mucosal sites, preventing SIV from infecting and killing cells important for the maintenance of immune homeostasis, (iii) delayed onset of CCR5 expression on the CD4+ T cells during ontogenetic development that protects the offspring from vertical transmission of the virus. These host adaptations, aimed at lowering the availability of target CCR5+ CD4+ T cells through CCR5 downregulation, were countered by SIV, which evolved to alter the entry coreceptor usage toward infecting different CD4+ T-cell subpopulations that support viral replication yet without disruption of host immune homeostasis. These natural strategies against SIV/HIV-1 infection, involving control of CCR5 function, inspired therapeutic approaches against HIV-1 disease, employing CCR5 coreceptor blocking as well as gene editing and silencing of CCR5. Given the pleiotropic role of CCR5 in health beyond immune disease, the precision as well as costs and benefits of such interventions needs to be carefully considered.
Highlights
CCR5, a chemokine receptor central for orchestrating lymphocyte/cell migration to the sites of inflammation and to the immunosurveillance, is involved in the pathogenesis of a wide spectrum of health conditions, including inflammatory diseases, viral infections, cancers and autoimmune diseases
CCR5 is the primary coreceptor for the human immunodeficiency viruses (HIVs), supporting its entry into CD4+ T lymphocytes upon transmission and in the early stages of infection in humans
Many natural hosts typically do not progress to immunodeficiency upon the simian immunodeficiency virus (SIV) infection. They have developed various strategies to minimize the SIV-related pathogenesis and disease progression, including an array of mechanisms employing modulation of the CCR5 receptor activity: (i) deletion mutations abrogating the CCR5 surface expression and conferring resistance to infection in null homozygotes; (ii) downregulation of CCR5 expression on CD4+ T cells, memory cells and cells at the mucosal sites, preventing SIV from infecting and killing cells important for the maintenance of immune homeostasis, (iii) delayed onset of CCR5 expression on the CD4+ T cells during ontogenetic development that protects the offspring from vertical transmission of the virus
Summary
CCR5, a C-C chemokine receptor 5 (formerly known as CCCKR-5 or CKR5), is primarily involved in immune surveillance, inflammatory response, tumor formation and metastasis [1,2,3], pathogenesis of inflammatory diseases [4,5,6], asthma [7, 8], and cancer [2, 3]. CCR5-D2 Mutation in SM In addition to the CCR5-D24 allele (that they carry at a frequency of 3%), SMs are frequently (26%) carrying a 2-bp deletion in the CCR5 gene (CCR5-D2), which, like the CCR5-D24 allele, encodes a truncated molecule that is not expressed at the cell surface [59] The presence of these common deletion alleles of CCR5 in different primate species (CCR5-D32 in humans, CCR5-D24 in RCMs and SM, and CCR5-D2 in SM) suggests that the emergence and high frequencies of these alleles may represent a convergent evolution, yet it remains unclear what pathogens were driving these adaptations, most likely different for humans and African NHPs. To infect CD4+ T cells in humans, HIV-1 utilizes CCR5 (mediating entry of R5 viruses) or CXCR4 (mediating entry of X4 viruses), or both entry coreceptors [67]. In vitro studies suggested a dual role of CCR5 in determining HIV-1 production: as an entry coreceptor, it acts as a critical factor for infection, yet exerts only a moderate influence on the magnitude of viral loads, while as a postentry regulator of the HIV-1 life cycle, at reverse transcription stage, it accounts for the logarithmic relation between the viremia and CCR5 density [75]
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