HLA-B*35-Px–mediated acceleration of HIV-1 infection by increased inhibitory immunoregulatory impulses

Huang, Jinghe; Goedert, James J.; Sundberg, Eric J.; Cung, Thai; Burke, Patrick S.; Martin, Maureen P.; Preiss, Liliana; Lifson, Jeffrey D.; Lichterfeld, Mathias; Carrington, Mary; Yu, Xu G.

doi:10.1084/jem.20091386

Cited by 72 publications

(95 citation statements)

References 24 publications

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“…The protective effect of HLA-B*57 was also confirmed in this population, while B35 and B53 alleles were associated with poor outcome. These results are inconsistent with the previously described PX/PY theory (Huang et al, 2009) (section 7.1). Lazaryan et al (2011) found that both B*5301 (PX) and B*3501 (PY), the most frequent alleles in their groups, were equally disadvantageous.…”

Section: Susceptibility Conferred By Hla-b35 Allelescontrasting

confidence: 99%

“…Differences in innate immunity could be the underlying cause: the B*35-PY molecule B*3501 and the B*35-Px molecule B*3503 differ by only one amino acid and present identical HIV-1 epitopes, yet the B*35-Px molecule binds with greater affinity to immunoglobulin-like transcript 4 (ILT4), an inhibitory MHC class I receptor expressed on DCs. This binding to ILT4 is associated with significantly stronger DC dysfunction during in vitro functional assays (Huang et al, 2009). That study concludes that differential interactions between HLA class I allele subtypes and immune regulatory MHC class I receptors on DCs is an important determinant of the immune response to the HIV virus.…”

Section: Susceptibility Conferred By Hla-b35 Allelesmentioning

confidence: 59%

“…CTL responses associated with lack of HIV control. DC dysfunction Klein et al, 1994;Carrington et al, 1999;Kawana et al, 1999;Jin et al, 2002;FloresVillanueva et al, 2003;Liu et al, 2003;Arnaiz-Villena et al, 2009;Huang et al, 2009 ;Pereyra et al, 2010 Kaslow et al, 1996;den Uyl et al, 2004;Fellay et al, 2007;Pereyra et al, 2010 ;Salgado et al, 2011b …”

Section: B35mentioning

confidence: 99%

See 2 more Smart Citations

Genetic Factors that Influence HIV Infection: The Role of the Major Histocompatibility Complex System

Pérez-Núñez¹,

Martı́nez-Quiles²

2011

HIV-Host Interactions

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Section: Susceptibility Conferred By Hla-b35 Allelescontrasting

confidence: 99%

Section: Susceptibility Conferred By Hla-b35 Allelesmentioning

confidence: 59%

Section: B35mentioning

confidence: 99%

See 1 more Smart Citation

Genetic Factors that Influence HIV Infection: The Role of the Major Histocompatibility Complex System

Pérez-Núñez¹,

Martı́nez-Quiles²

2011

HIV-Host Interactions

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“…One polymorphic residue between Eqca-N*00602 and Eqca-N*00601 was able to lead to a distinct conformation of GW12, indicating this diverse peptide presentation manner, as the peptide conformation can be changed so easily. Martin and colleagues found drastically different interactions between a self-peptide pVIPR with two HLA subtypes HLA-B*2705 and HLA-B*2709, which only differ with respect to residue 116 (Asp versus His) within the peptidebinding groove (21). The recently determined HLA-A*0301 complexed with an HIV-derived peptide RT313 also reflects the important role of residue 152 in the minor tuning of peptide side chains presented by HLA-A*0301 (Glu 152 ) and HLA-A*1101 (Ala 152 ) (59).…”

Section: Discussionmentioning

confidence: 99%

“…Immunogenic epitope peptides recognized by virus-specific CTLs are presented by MHC (equine leukocyte Ag [ELA] in the horse and HLA in humans) molecules. The subtle changes in the peptide-binding region of MHC molecules that leads to amino acid differences have a significant impact on the immune responses to a similar peptide (21,22). It has been reported that a single amino acid polymorphism within the a2 domain of ELA can alter or even abolish recognition of Env-RW12 and another EIAV-derived CTL epitope peptide, Rev-QW11 (QAEVLQERLEW) (20).…”

mentioning

confidence: 99%

Structural Illumination of Equine MHC Class I Molecules Highlights Unconventional Epitope Presentation Manner That Is Evolved in Equine Leukocyte Antigen Alleles

Yao

et al. 2016

The Journal of Immunology

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MHC class I (MHC I)–restricted virus-specific CTLs are implicated as critical components in the control of this naturally occurring lentivirus and in the protective immune response to the successfully applied attenuated equine infectious anemia virus vaccine in the horse. Nevertheless, the structural basis for how the equine MHC I presents epitope peptides remains unknown. In this study, we investigated the binding of several equine infectious anemia virus–derived epitope peptides by the ability to refold recombinant molecules and by thermal stability, and then by determining the x-ray structure of five peptide–MHC I complexes: equine MHC class I allele (Eqca)-N*00602/Env-RW12, Eqca-N*00602/Gag-GW12, Eqca-N*00602/Rev-QW11, Eqca-N*00602/Gag-CF9, and Eqca-N*00601/Gag-GW12. Although Eqca-N*00601 and Eqca-N*00602 differ by a single amino acid, Eqca-N*00601 exhibited a drastically different peptide presentation when binding a similar CTL epitope, Gag-GW12; the result makes the previously reported function clear to be non–cross-recognition between these two alleles. The structures plus Eqca-N*00602 complexed with a 9-mer peptide are particularly noteworthy in that we illuminated differences in apparent flexibility in the center of the epitope peptides for the complexes with Gag-GW12 as compared with Env-RW12, and a strict selection of epitope peptides with normal length. The featured preferences and unconventional presentations of long peptides by equine MHC I molecules provide structural bases to explain the exceptional anti-lentivirus immunity in the horse. We think that the beneficial reference points could serve as an initial platform for other human or animal lentiviruses.

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CDK4/6 inhibitors induce breast cancer senescence with enhanced anti‐tumor immunogenic properties compared with DNA‐damaging agents

Lee,

Imran,

Choi

et al. 2023

Molecular Oncology

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Since therapy‐induced senescence (TIS) can either support or inhibit cancer progression, identifying which types of chemotherapeutic agents can produce the strongest anti‐tumor TIS is an important issue. Here, cyclin‐dependent kinase4/6 inhibitors (CDK4/6i)‐induced senescence was compared to the TIS induced by conventional DNA‐damaging agents. Despite both types of agents eliciting a similar degree of senescence, we observed increased expression of the senescence‐associated secretory phenotype (SASP) and ligands related to pro‐tumor immunity (IL6, CXCL8, TGFβ, CD274, CEACAM1) and angiogenesis (VEGFA) mainly in TIS induced by DNA‐damaging agents rather than by CDK4/6i. Additionally, although all agents increased the expression of anti‐tumor immunomodulatory proteins related to antigen presentation (MHC‐I, B2M) and T cell chemokines (CXCL9, 10, 11), CDK4/6i‐induced senescent cells still maintained this expression at a similar or even higher intensity than cells treated with DNA‐damaging agents, despite the absence of nuclear factor‐kappa‐B (NF‐κB) and p53 activation. These data suggest that in contrast with DNA‐damaging agents, which augment the pro‐tumorigenic microenvironment via pro‐inflammatory SASP, CDK4/6i can generate TIS only with antitumor immunomodulatory proteins.

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HLA-B*35-Px–mediated acceleration of HIV-1 infection by increased inhibitory immunoregulatory impulses

Cited by 72 publications

References 24 publications

Genetic Factors that Influence HIV Infection: The Role of the Major Histocompatibility Complex System

Genetic Factors that Influence HIV Infection: The Role of the Major Histocompatibility Complex System

Structural Illumination of Equine MHC Class I Molecules Highlights Unconventional Epitope Presentation Manner That Is Evolved in Equine Leukocyte Antigen Alleles

CDK4/6 inhibitors induce breast cancer senescence with enhanced anti‐tumor immunogenic properties compared with DNA‐damaging agents

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