CXCL10/CXCR3-Dependent Mobilization of Herpes Simplex Virus-Specific CD8
 +
 T
 EM
 and CD8
 +
 T
 RM
 Cells within Infected Tissues Allows Efficient Protection against Recurrent Herpesvirus Infection and Disease

Srivastava, Ruchi; Khan, Arif; Chilukuri, Sravya; Syed, Sabrina A.; Tran, Tien T.; Furness, Julie N.; Bahraoui, Elmostafa; BenMohamed, Lbachir

doi:10.1128/jvi.00278-17

Cited by 40 publications

(35 citation statements)

References 84 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…64 In addition to cytokines, chemokines are also important in the trafficking and localization of T RM cells. For example, the chemokine receptors CXCR6 and CCR10 are required for optimal formation of a T RM population in the skin; lack of either CXCL10 or CXCR3 compromises the mobilization of T RM cells within latently infected trigeminal ganglia and results in the absence of signals required for differentiation 15,65,66 ; CXCR3 is also critical for T cell accumulation in uninfected salivary glands, 67 and CXCL17 is required for the mobilization of T RM cells in the vaginal mucosa (VM). 68 Differentiation of recirculating T EM cells depends on prolonged cognate antigen stimulation.…”

Section: Differentiation and Maintenance Of Cd8 + T Rm Cellsmentioning

confidence: 99%

“…68 Significant increases in both the number and function of HSV-specific CXCR3 + T RM cells have been detected in the trigeminal ganglia of mice following UV-B-induced HSV-1 reactivation, which protects the host from recurrent HSV infection, and a lack of T RM is again associated with recurrent ocular HSV infection. 65 In addition, accumulation of T RM cells in the skin provides enhanced control against viral infection with HSV-1. 11,62,82 T RM cells generated by the "prime and pull" protocol may reduce the spread of infectious HSV-2 into the sensory neurons and prevent development of clinical disease.…”

Section: Cd8 + T Rm Cells In Anti-viral Immunitymentioning

confidence: 99%

See 1 more Smart Citation

Tissue-resident lymphocytes: from adaptive to innate immunity

et al. 2019

View full text Add to dashboard Cite

Efficient immune responses against invading pathogens often involve coordination between cells from both the innate and adaptive immune systems. For multiple decades, it has been believed that CD8 + memory T cells and natural killer (NK) cells constantly and uniformly recirculate. Only recently was the existence of noncirculating memory T and NK cells that remain resident in the peripheral tissues, termed tissue-resident memory T (T RM) cells and tissue-resident NK (trNK) cells, observed in various organs owing to improved techniques. T RM cells populate a wide range of peripheral organs, including the skin, sensory ganglia, gut, lungs, brain, salivary glands, female reproductive tract, and others. Recent findings have demonstrated the existence of T RM in the secondary lymphoid organs (SLOs) as well, leading to revision of the classic theory that they exist only in peripheral organs. trNK cells have been identified in the uterus, skin, kidney, adipose tissue, and salivary glands. These tissue-resident lymphocytes do not recirculate in the blood or lymphatic system and often adopt a unique phenotype that is distinct from those of circulating immune cells. In this review, we will discuss the recent findings on the tissue residency of both innate and adaptive lymphocytes, with a particular focus on CD8 + memory T cells, and describe some advances regarding unconventional T cells (invariant NKT cells, mucosal-associated invariant T cells (MAIT), and γδ T cells) and the emerging family of trNK cells. Specifically, we will focus on the phenotypes and functions of these subsets and discuss their implications in anti-viral and anti-tumor immunity.

show abstract

Section: Differentiation and Maintenance Of Cd8 + T Rm Cellsmentioning

confidence: 99%

Section: Cd8 + T Rm Cells In Anti-viral Immunitymentioning

confidence: 99%

Tissue-resident lymphocytes: from adaptive to innate immunity

et al. 2019

View full text Add to dashboard Cite

show abstract

“…Of these, the CD4 + and CD8 + T cells have been shown to be important for resolution of the acute infection [44] and CD8 + T cells directed against an epitope on glycoprotein B are hypothesized to maintain the latent state [76] and there is evidence that this is dependent on MHC class I expression [77]. Further, CXCR3 + CD8 + T cells have been shown to increase in the TG and the epithelial surface following a reactivation stimulus and this correlated with a decrease in viral shedding at the surface, noting that outcomes in the TG were not examined [78]. It has also been proposed that regulatory T cells function to suppress CD8 + T cells and facilitate HSV reactivation [79].…”

Section: Discussionmentioning

confidence: 99%

Resolution of herpes simplex virus reactivation in vivo results in neuronal destruction

et al. 2020

View full text Add to dashboard Cite

A fundamental question in herpes simplex virus (HSV) pathogenesis is the consequence of viral reactivation to the neuron. Evidence supporting both post-reactivation survival and demise is published. The exceedingly rare nature of this event at the neuronal level in the sensory ganglion has limited direct examination of this important question. In this study, an in-depth in vivo analysis of the resolution of reactivation was undertaken. Latently infected C57BL/6 mice were induced to reactivate in vivo by hyperthermic stress. Infectious virus was detected in a high percentage (60-80%) of the trigeminal ganglia from these mice at 20 hours post-reactivation stimulus, but declined by 48 hours post-stimulus (0-13%). With increasing time post-reactivation stimulus, the percentage of reactivating neurons surrounded by a cellular cuff increased, which correlated with a decrease in detectable infectious virus and number of viral protein positive neurons. Importantly, in addition to intact viral protein positive neurons, fragmented viral protein positive neurons morphologically consistent with apoptotic bodies and containing cleaved caspase-3 were detected. The frequency of this phenotype increased through time post-reactivation. These fragmented neurons were surrounded by Iba1 + cells, consistent with phagocytic removal of dead neurons. Evidence of neuronal destruction post-reactivation prompted re-examination of the previously reported non-cytolytic role of T cells in controlling reactivation. Latently infected mice were treated with anti-CD4/CD8 antibodies prior to induced reactivation. Neither infectious virus titers nor neuronal fragmentation were altered. In contrast, when viral DNA replication was blocked during reactivation, fragmentation was not observed even though viral proteins were expressed. Our data demonstrate that at least a portion of reactivating neurons are destroyed. Although no evidence for direct T cell mediated antigen recognition in this process was apparent, inhibition of viral DNA replication blocked neuronal fragmentation. These unexpected findings raise new questions about the resolution of HSV reactivation in the host nervous system. Herpes simplex virus (HSV)is an endemic human pathogen that establishes latency in neurons and can periodically reactivate over the lifetime of the host. Whether or not neurons survive post-reactivation is controversial and has significant implications for longterm infection. HSV reactivation events can be characterized in mice, which maintain the complexity of host-pathogen interactions, with the goal to provide insight into how the virus behaves in the nervous system. In this report, it is shown that the elimination of infectious virus following reactivation in vivo corresponded with a highly focused cellular response and destruction of the neuron containing HSV proteins. The role of T cells in this response was investigated. Previous work identified T cells as major regulators of HSV reactivation. However, neuronal destruction was still observed when T cell anti...

show abstract

“…Prime-and-pull was developed to establish local tissue Trm cells at target sites by parenterally vaccinating to elicit systemic T cell responses (prime) and then to recruit activated T cells to specific tissues with a topical chemokine (66) or with nonspecific inflammation (67) (pull), where such T cells could become Trm cells and mediate protection. Methods have been reported for the liver (19), urogenital tract (66,68,69), and lungs (70,71). The recent malaria prime-and-trap report showed that TCR transgenic cells adoptively transferred into naive recipient mice could be primed with peptide-pulsed DCs and then trapped with a liver-specific, Ag-expressing recombinant adeno-associated virus (19).…”

Section: Discussionmentioning

confidence: 99%

Prime-and-Trap Malaria Vaccination To Generate Protective CD8+ Liver-Resident Memory T Cells

Olsen

Stone

Chuenchob

et al. 2018

The Journal of Immunology

View full text Add to dashboard Cite

Tissue-resident memory CD8 T (Trm) cells in the liver are critical for long-term protection against pre-erythrocytic infection. Such protection can usually be induced with three to five doses of i.v. administered radiation-attenuated sporozoites (RAS). To simplify and accelerate vaccination, we tested a DNA vaccine designed to induce potent T cell responses against the SYVPSAEQI epitope of circumsporozoite protein. In a heterologous "prime-and-trap" regimen, priming using gene gun-administered DNA and boosting with one dose of RAS attracted expanding Ag-specific CD8 T cell populations to the liver, where they became Trm cells. Vaccinated in this manner, BALB/c mice were completely protected against challenge, an outcome not reliably achieved following one dose of RAS or following DNA-only vaccination. This study demonstrates that the combination of CD8 T cell priming by DNA and boosting with liver-homing RAS enhances formation of a completely protective liver Trm cell response and suggests novel approaches for enhancing T cell-based pre-erythrocytic malaria vaccines.

show abstract

CXCL10/CXCR3-Dependent Mobilization of Herpes Simplex Virus-Specific CD8 ⁺ T _EM and CD8 ⁺ T _RM Cells within Infected Tissues Allows Efficient Protection against Recurrent Herpesvirus Infection and Disease

Cited by 40 publications

References 84 publications

Tissue-resident lymphocytes: from adaptive to innate immunity

Tissue-resident lymphocytes: from adaptive to innate immunity

Resolution of herpes simplex virus reactivation in vivo results in neuronal destruction

Prime-and-Trap Malaria Vaccination To Generate Protective CD8+ Liver-Resident Memory T Cells

Contact Info

Product

Resources

About

CXCL10/CXCR3-Dependent Mobilization of Herpes Simplex Virus-Specific CD8 + T EM and CD8 + T RM Cells within Infected Tissues Allows Efficient Protection against Recurrent Herpesvirus Infection and Disease

Cited by 40 publications

References 84 publications

Tissue-resident lymphocytes: from adaptive to innate immunity

Tissue-resident lymphocytes: from adaptive to innate immunity

Resolution of herpes simplex virus reactivation in vivo results in neuronal destruction

Prime-and-Trap Malaria Vaccination To Generate Protective CD8+ Liver-Resident Memory T Cells

Contact Info

Product

Resources

About

CXCL10/CXCR3-Dependent Mobilization of Herpes Simplex Virus-Specific CD8 ⁺ T _EM and CD8 ⁺ T _RM Cells within Infected Tissues Allows Efficient Protection against Recurrent Herpesvirus Infection and Disease