Evaluation of Fomesafen for Broadleaf Weed Control, In Soybeans (Glycine Max)

Jimenez, Ricardo A.

01 November 1988

The lack of effective broadleaf weed control represents one of the major factors having detrimental effects on growth and yield of soybeans. Broadleaf weeds are a serious threat to soybean growers in the southeastern United States. A broad range of herbicides is being used in an effort to control broadleaf weeds in soybeans, and research is still being conducted to find new herbicides that can best work for this purpose. This study involved the use of one these herbicides. It was fomesafen, 5-[2-chloro-4-trifluromethyl) phenoxy]-N-(methyl-sulfonyl)-2-nitrobenzamide, which controls a broad spectrum of broadleaf weeds in soybeans. The experiment was conducted in the summers of 1987 and 1988. Broadleaf weed control treatments with fomesafen at rates at 0.07, 0.14, 0.28, and 0.35 kg ai/ha in single early postemergence and late postemergence applications were evaluated using the herbicide with a nonionic surfactant at 0.25% and 0.50% of the solution. All treatments were compared with a check which did not receive herbicide application. Among the most common broadleaf weeds found in the area under study during the summer of 1987 were morningglories (Ipomoea spp), redroot pigweed (Amaranthus retroflexus L.), jimsonweed (Datura stramonium L.), common lambsquarters (Chenopodium album L.), carpetweed (Moliugo verticillata L.), and prickly sida (Sida spinose L.), For the summer of 1988 the most prevalent broadleaf weeds were morningglories, horsenettle (Solanum carolinense L.), horseweed [Conyza canadensis (L.), Cronq.], and prickly sida. The results of the experiment showed no significant differences between early postemergence and late postemergence treatments. There were no significant differences in broadleaf weed control in treatments which received 0.14, 0.28 and 0.35 kg ai/ha of fomesafen for either 1987 or 1988. Poor broadleaf weed control resulted with the application of fomesafen at its lowest rate (0.07 kg ai/ha). No significant differences were found in broadleaf weed control between concentration of 0.25% and 0.50% of the nonionic surfactant added to fomesafen. Statistically significant yield variation did occur among treatments in 1987. No significant differences in yields were found between any of the herbicide treatments in 1988. Soybean yields were significantly higher in 1988 than in 1987.

Western Kentucky University

Herbicides

Weed Killer

Agricultural Science

Agriculture

Agronomy and Crop Sciences

Botany

Plant Sciences

Weed Science

Modulation of innate immune responses by hepatitis C virus

Huston, Leila

January 2012

Hepatitis C virus (HCV) establishes a chronic infection in about 70% of infected individuals that is associated with the development of liver cirrhosis and hepatocellular carcinoma. The mechanisms by which HCV avoids clearance by the host immune response are not fully understood. The first aim of this project was to determine whether immune cell subsets could become infected by HCV in vitro. None of the haematopoietic subsets analysed expressed all of the required entry factors, CD81, SR-BI, claudin-1 and occludin. Also, PBMCs were not susceptible to infection with HCVpp and HCVcc expressing glycoproteins of hepatotropic strains. Infection by a supposedly lymphotropic strain (SB) was found to be inefficient. The second aim was to identify in vitro immunomodulatory effects of HCV on innate immune cells that may impact on the immune response activated in acute infection. Crosslinking of CD81 on NK cells by antibody was found to have a minor inhibitory effect on their activation via CD16, but CD81 crosslinking by viral particles had no detectable effect. In contrast to other viruses, HCVcc elicited very little interferon-α production by pDC. HCVcc also did not affect pDC or mDC responses to TLR ligation. Systemic cytokine and chemokine responses were analysed in subjects with primary acute HCV infection and in HCV-infected patients undergoing liver transplantation (LT). Interestingly, induction of systemic type I and type III interferon was not observed in either group. Marked perturbations in systemic cytokine and chemokine levels were detected in uninfected LT patients, precluding use of HCV-infected LT patients to study the innate immune response activated in response to acute viral replication. Together, these results suggest that HCV may principally evade innate immune cell responses by avoidance rather than impairment strategies.

616.3623

Déprédation par les orques (Orcinus Orca) et les cachalots (Physeter Macrocephalus) sur les palangriers à la legine australe dans la ZEE de l' archipel de Crozet

Tixier, Paul

10 July 2012

C'est dans le contexte délicat du milieu marin, marqué par l'écroulement des stockshalieutiques et la conservation urgente des espèces de prédateurs marins, que s'inscrit cette étude sur la déprédation (i.e. prélèvement des poissons capturés) par les orques et les cachalots sur la pêche à lapalangre dans la ZEE de l'Archipel de Crozet.Le premier objectif a été d'évaluer les conséquences socio-économiques du phénomène. Entre 2003 et2010 les orques ont interagi avec un total de 43,3% des palangres relevées et les cachalots avec 57,5%,les deux espèces étant présentes simultanément sur 27.8% des palangres (n=5438). Les orques, seulesou associées aux cachalots ont été estimées prélever 926 ± 76 tonnes de légines sur l'ensemble de lapériode, représentant un taux de déprédation de 17,7%.Trois facteurs opérationnels ont été identifiés comme faisant varier la déprédation par les orques : i)utilisation de palangres courtes (<5000m) en absence d'orques, ii) déplacement du navire sur desdistances supérieures à 40nq pour quitter une zone confrontée à la déprédation et changer de zone, iii)utilisation de vitesse de remontée des hameçons à bord supérieures à 50 H.min-1.Le deuxième objectif de cette étude a été d'évaluer les conséquences démographiques de ladéprédation sur la population d'orques de Crozet. Le suivi à long terme des individus a permis demettre en évidence des réponses différentielles des unités sociales en fonction de leur degréd'interaction avec les pêcheries. / Over the last 50 years, fisheries have undergone a major decline worldwide. With an increasedcompetition for resource, depredation (i.e. removal of catches on fishing gear) has recently become amajor case of conflict between humans and marine predators. In this study I focused on thedepredation on Patagonian toothfish fisheries by killer and sperm whales in the Crozet EEZ. The firstpart of the study aimed at assessing the socio-economic consequences of this issue. Killer and spermwhales have interacted with 43.3% and 57.5% of longlines (n=6751) respectively from 2003 to 2010.Killer whales, alone or co-occurring with sperm whales were responsible for an estimated loss of 926± 76 tons of toothfish over that period, which represents 17.7% of the total catch.Three operational factors were identified as influencing significantly depredation levels: i) the use ofshort longlines (<5000m) in absence of killer whales, ii) the displacement of vessels on distances>40nq to leave the whales behind and iii) the use of longline hauling speed > 50 H.min-1.The second aim of the study was to investigate the consequences of depredation on the Crozet killerwhale population. The long term monitoring of individuals showed divergent demographic trajectoriesrelated to the depredation level of matrilines. During the 1990s, matrilines interacting with fisherieshave undergone a high mortality due to lethal interactions with illegal fishing vessels using explosivesto repel the whales.

Déprédation

Orque

Mitigation

Organisation sociale

Démographie

Écologie alimentaire

Conservation

Depredation

Killer whale

Mitigation

Social organization

Demography

Feeding ecology

Conservation

Implication des cellules NK au cours des maladies auto-immunes / Implication of NK cells in auto-immune diseases

Hervier, Baptiste

02 July 2014

Les maladies auto-immunes (MAI) correspondent à un large ensemble de pathologies cliniquement hétérogènes, affectant le plus souvent des adultes jeunes, de façon volontiers chronique. Du point de vue physiopathologique, ces maladies correspondent à la survenue d’une rupture de tolérance au soi, dont les mécanismes sont complexes et font appel à l’ensemble des acteurs du système immunitaire. Si l’implication des cellules de l’immunité adaptative est largement documentée dans ce contexte, celle des cellules appartenant à l’immunité innée, comme les cellules Natural Killer (NK) est peu étudié. A travers deux exemples de MAI systémiques, le Lupus Systémique (LS) et le Syndrome des Antisynthétases (SAS), l’objet de ce travail est de montrer l’implication des cellules NK au cours des MAI et d’étudier les mécanismes en cause.L’étude phénotypique et fonctionnelle des cellules NK chez des patients présentant une MAI révèle de nombreuses anomalies comparativement aux sujets contrôles. Ces dernières sont plus marquées chez les patients en phase active plutôt qu’en rémission. De plus, l’infiltration des tissus cibles au cours du SAS par les cellules NK d’une part, et l’activation in vitro de ces cellules par les auto-antigènes au cours du LS d’autre part, confirme l’implication des cellules NK au cours de ces deux MAI. Par ailleurs, des interactions des cellules NK avec plusieurs types cellulaires impliqués dans l’immunopathologie de ces maladies semblent conditionner les anomalies observées. Ces dernières sont différentes selon la maladie étudiée : le profil des cellules NK des patients atteints de LS étant plutôt immature et tourné vers la production de cytokines, tandis que celui des patients atteints de SAS correspond à un stade de différentiation terminal mais hypofonctionnel.L’ensemble des résultats suggère que les cellules NK participent à l’immunopathologie des MAI. Leur implication est conditionnée par l’effet de certains stimuli et certaines interactions cellulaires, qui sont de nature différente d’une MAI à l’autre. / Auto-immune diseases (AID) form a broad spectrum of heterogeneous and chronic pathologies, most commonly affecting young adults. The etiopathogenesis of AID corresponds to a breakdown of the immunological tolerance: the result of complex mechanisms, implicating every component of the immune system. While adaptive immune cells has been extensively studied in this context, the role of innate immune cells, including Natural Killer (NK) cells, is much less understood. Using Systemic Lupus Erythematosus (SLE) and Antisynthetase Syndrome (ASS) as model pathologies, the main objective of this work is to demonstrate the involvement of NK cells in AID and to study the relevant mechanisms. Patients with AID showed numerous anomalies in the phenotypical and functional analysis of their NK cells, as compared to healthy controls. These differences are more pronounced in active rather than inactive patients. Moreover, the infiltration of target tissues by NK cells in ASS as well as the activation of these cells by SLE specific auto-antigens confirm the involvement of NK cells in AID. Additionally, interactions of NK cells with different immune cells, known to be involved in AID pathogenesis, seem to be the cause of the observed anomalies. These anomalies differ among both AID: NK cells from patients with SLE are immature and devoted to cytokine production, whereas those from patients with ASS have reached a highly differentiated but hypofunctional stage. Taken as a whole, these data suggest that NK cells are involved in the immuno-pathogenesis of AID. This involvement seems conditioned by the effect of different stimuli and different cellular interactions, which are distinct from one form of AID to another.

Maladies auto-immunes

Immunité innée

Cellules NK

Lupus systémique

Myosites

Syndrome des antisynthétases

Auto-immune diseases

Natural Killer cells

570

Rôle de l’activation des cellules « Natural Killer » par le « missing self » dans la génération de lésions de rejet vasculaire chronique après transplantation d’organe / Missing self triggers NK cell-mediated chronic vascular rejection of solid organ transplants

Koenig, Alice

21 September 2018

La transplantation d'organe est le meilleur traitement en cas de défaillance terminale d'un organe vital. Cependant, la survie sur le long terme est limitée par la perte inexorable de la fonction des greffons. Cette dernière est attribuée à l'inflammation microvasculaire (1MV) causée par la réponse anticorps contre les alloantigènes (rejet humoral chronique (RHC)). En analysant une cohorte de 129 transplantés rénaux présentant de l'1MV sur une biopsie de greffon, nous avons trouvé que, dans la moitié des cas, les lésions n'étaient pas médiées par les anticorps. Chez ces patients, des études génétiques ont révélé une prévalence plus élevée de « mismatches » entre les molécules HLA de classe 1 (HLA-1) du donneur et les « Killer-cell immunoglobulin-receptors » (K1R) inhibiteurs des NK du receveur. Nous avons émis l'hypothèse que la nature allogénique de l'endothélium du greffon pouvait créer un « pseudo-missing-self ». De ce fait, les NK du receveur, exposés à des stimuli inflammatoires, ne reçoivent plus les signaux inhibiteurs transmis par le HLA-1 de la part des cellules endothéliales du donneur. Dans un modèle de co-culture de cellules endothéliales et de NK humains, nous avons démontré que l'absence d'un ligand HLA-1 du soi sur la cellule endothéliale peut activer les NK. Cette activation dépend de la voie mTOR dans les NK, qui peut être bloquée par la rapamycine, un inhibiteur de mTORC1 disponible en clinique. Enfin, nous avons confirmé l'existence de rejets NK induit par le « missing-self » et leur sensibilité à la rapamycine dans un modèle murin de transplantation cardiaque. Notre travail identifie un nouveau type de rejet chronique, exclusivement médié par l'immunité innée, les NK, ayant le même impact délétère sur la survie des greffons que le RHC. Cependant, alors qu'il n'y a pas de traitement disponible pour le RHC, les inhibiteurs de mTOR préviennent efficacement le développement de lésions dans un modèle murin de rejet vasculaire chronique induit par le « missing self » / Organ transplantation is the best treatment for terminal organ failure. However, long-term outcome of organ transplantation remains limited by inexorable loss of graft function, which the prevalent dogma links to the microvascular inflammation (MVI) triggered by the recipient's antibody response against alloantigens (antibody-mediated chronic rejection, AMR). Analysing a cohort of 129 renal transplant patients with MVI on graft biopsy, we found that, in half of the cases, histological lesions were not mediated by antibodies. In these patients, genetic studies revealed a higher prevalence of mismatches between donor HLA-I and inhibitory Killer-cell immunoglobulin-receptors (KIR) of recipient's NK cells. We hypothesized that the allogeneic nature of graft endothelium could create a "pseudo-missing self" situation, thereby the recipient's NK cells exposed to inflammatory stimuli would not receive HLA I-mediated inhibitory signals from donor endothelial cells. In co-culture experiments with human NK cells and endothelial cells, we demonstrated that the lack of self HLA-I on endothelial cells can activate NK. This activation triggers mTOR pathway in NK, which can be blocked by rapamycin, a commercially available inhibitor of mTORC1. Finally, we confirmed the existence of missing self-induced rejection and its sensitivity to mTOR inhibition in a murine heart transplantation model. Our work identifies a new type of chronic rejection, exclusively mediated by innate NK cells, with the same detrimental impact on graft survival as AMR. However, while no therapy is available for AMR, mTOR inhibitors efficiently prevent the development of lesions in murine models of NK cell-mediated chronic vascular rejection

Cellule Natural Killer

Rejet chronique

Missing-self

Transplantation

Inhibiteurs de mTOR

NK cell

Chronic rejection

Missing-self

Transplantation

MTOR inhibitors

570

Exploring Narrator-Reader Relationships with Jim Thompson’s Victims of Circumstance: Lou Ford, Dolly Dillon, William “Kid” Collins, and Charles Bigger

Unknown Date

By examining Jim Thompson’s novels, published between 1952-1955–The Killer Inside Me, A Hell of a Woman, After Dark, My Sweet, and Savage Night–this essay interrogates the relationship created between the narrator and the reader, how the narrator–and Thompson in turn–highlights certain societal flaws, emphasizing how ethical consequence is born out of the attempt to attain freedom from one’s cultural circumstance–both in terms of economic restraint and mental health status. Through this, Thompson implies that the reader is trapped in similar economic and ethical predispositions. The reader is often left questioning what they might have done, or been able to do, in similar circumstances. This creates a larger frame by which Thompson implies that the reader is trapped in similar economic and ethical pre-dispositions as his narrators. He highlights societal flaws, demonstrating how the pursuit of freedom of one’s cultural circumstance bears ethical consequence. / Includes bibliography. / Thesis (M.A.)--Florida Atlantic University, 2018. / FAU Electronic Theses and Dissertations Collection

Thompson, Jim, 1906-1977--Fiction

Role of the inhibitory receptor LAIR-1 on NK cells in chronic hepatitis B

Hansi, Navjyot Kaur

January 2018

There are multiple immune mechanisms identified for persistence of hepatitis B virus (HBV) infection. This thesis considers the vital role that inhibitory receptors play in contributing to impairment of the adaptive immune system in chronic hepatitis B (CHB), and the potential role they play in the innate immune system, focusing on the inhibitory receptor leucocyte-associated immunoglobulin-like receptor (LAIR)-1. The unique aspect of this work is that for the first time LAIR-1 expression has been investigated on natural killer (NK) cells in CHB. Our striking findings of increased LAIR-1 expression on peripheral NK cells in CHB and an inverse correlation between expression and effector function suggest this inhibitory receptor could have a potential role in exhaustion of NK cells in CHB. We therefore additionally explored the expression of LAIR-1 on circulating NK cells from patients with hepatocellular carcinoma (HCC) and non-alcoholic fatty liver disease (NAFLD). The particular relevance of LAIR-1 to liver disease is that one of its major ligands is collagen. We demonstrated a downregulation of LAIR-1 expression on intrahepatic NK cells, which we postulate might occur following repetitive engagement with abundant collagen within the liver. In line with this, intrahepatic NK cells with a liver-resident (CXCR6+) phenotype had even lower LAIR-1 expression than liver infiltrating (non-resident, CXCR6-) NK cells. Furthermore, preliminary experiments display attenuation of the cytotoxic degranulation capacity (CD107a) by circulating NK cells from CHB patients upon exposure to plate-bound collagen. We demonstrate differential expression of LAIR-1 on NK cells in viral hepatitis, HCC and NAFLD and between peripheral and intrahepatic NK cells. Preliminary experiments demonstrate a role in inhibiting NK cell function suggesting this as a novel therapeutic target to harness the capacity of NK cells to control chronic infection and cancer.

Estudos sobre o isolamento e expansão de células Natural Killer (NK) do sangue de cordão umbilical e placentário na presença de células mesenquimais

Furlan, Juliana Monteiro

January 2016

Introdução: A célula NK possui uma importante função no sistema imune inato de defesa primária contra vírus e patógenos e também realiza a imunovigilâcia tumoral. Muitos estudos clínicos tem avaliado o uso dessas células na imunoterapia adotiva. A expansão e a ativação da célula NK requer sinais e estímulos para manter a sua sobrevivência. Atualmente existem muitos protocolos para a expansão e ativação da célula NK, porém não existe uma definição do melhor método para uso clínico. Objetivo: O estudo tem como objetivo avaliar a melhor forma para expansão das células NK isoladas de células mononucleares do sangue de cordão umbilical e placentário.Método: Foram avaliadas cinco diferentes condições para expansão de células NK de mononucleares isoladas do sangue do cordão umbilical e placentário. Foram testados protocolos utilizando as interleucinas (IL), IL-2, IL-3, IL-15; com ou sem a presença do co-cultivo com células-tronco mesenquimais do cordão umbilical (CTM-CU) e, também o co-cultivo com células apresentadoras de antígeno artificiais ligadas a IL-21 à membrana (mbIL21 APC). Resultados: Os protocolos utilizando co-cultivo com APC mbIL21 foram superiores aos demais quanto à capacidade de expansão de células NK (CD3-, CD56+, CD16+). O protocolo de co-cultura de APC, CTM-CU e estímulo com IL-2 apresentaram um aumento significativo de NK (CD3-, CD56+, CD16+) quando comparado ao protocolo de APC/IL-2 sem CTM-CU (p<0,05). Conclusão: A expansão ex vivo de células NK na presença das APC e CTM-CU apresentaram uma proporção estatisticamente superior de célula NK CD16+ quando comparada com condições de cultivo com apenas a APC, tendo essas células NK potencial para utilização na imunoterapia adotiva associada com anticorpos monoclonais ou anticorpos bi-específicos. / Background: Natural killer (NK) cells play a major role in innate immunity, especially against viral pathogens, and are also a part of the immune surveillance of tumors. Several clinical trials have evaluated the use of these cells for adoptive cell immunotherapy. Ex vivo expansion of NK cells, however, is a complex process which requires multiple cell signals to ensure cell survival, proliferation, and activation. There are many protocols used for NK cell expansion and activation, however, there is a lack of evidence regarding which method is the most effective for clinical grade NK cells expansion. Objective: The main purpose of this study is to evaluate an optimal protocol for the ex vivo expansion of NK cells isolated from umbilical cord blood mononuclear cells (CB-MNC). Methods: Five different conditions for the expansion of umbilical cord-derived NK cells were evaluated. Each protocol was a different combination of interleukins (IL-2, IL-3, and IL-15) with or without the presence of feeder cells or artificial antigen presenting cells (aAPCs). Feeder cells utilized were umbilical cord-derived mesenchymal stem cells (UC-MSC), and aAPCs were membrane-bound IL-21 artificial APCs (mbIL21 aAPCs). Results: Protocols employing mbIL21 aAPCs demonstrated greater expansion of natural killer cells (CD3- CD56+) than the other protocols. The protocol employing aAPCs, IL-2 and UC-MSC feeder cells had a statistically significant higher proportion of CD16+ NK cells when compared to the protocol without the MSC feeder cells, but there was no significant difference in the expansion of total natural killer cells concerning these two protocols. Conclusion: Ex vivo expansion of NK cells in the presence of aAPCs and UC-MSC feeder cells yielded a significant higher proportion of CD16+ NK when compared to the aAPCs only culture condition, and could be a better product for NK adoptive immunotherapy in conjunction with monoclonal or bi-specific antibodies.

Células matadoras naturais

Sangue fetal

Células-tronco mesenquimais

Imunoterapia

Natural killer cell

Umbilical cord blood

Mesenchymal stem cells

Immunotherapy

Otimização da produção e purificação de compostos antimicrobianos de leveduras para desenvolvimento de um novo agente antifúngico / Optimization of production and purification of antimicrobial compounds from yeast for the development of a new antifungal agent

Senter, Luciana

January 2010

Infecções fúngicas em humanos vem aumentando nos últimos anos e acometem principalmente pacientes imunocomprometidos, portadores do vírus HIV, transplantados ou com câncer. Os antifúngicos empregados no tratamento pertencem a poucos grupos de fármacos e o aparecimento de resistência antifúngica em muitos patógenos leva à necessidade de desenvolvimento de novos agentes antifúngicos. As cepas Trichosporon japonicum QU139 e Candida catenulata LV102 apresentam atividade killer sobre diversas leveduras patogênicas, apresentando bom potencial para desenvolvimento de novos agentes antimicrobianos. O objetivo do trabalho foi a otimização das condições para produção e detecção dos compostos antimicrobianos, para seu futuro uso terapêutico, e sua purificação. O efeito killer da cepa T. japonicum QU139 foi avaliado pelo método dos poços contra células sensíveis de Cryptococcus gattii C20 nos meios GYP, YM e Queijo em diferentes pH e temperaturas. A máxima atividade killer foi encontrada no meio GYP, pH 4,5 à 25°C após 24 horas de incubação para T.japonicum QU139 e C. catenulata LV102. Não foi possível isolar o composto antimicrobiano produzido pela levedura T.japonicum QU139 pelos métodos de isolamento de proteína/glicoproteína, corroborando a hipótese de que a toxina seja um glicolipídeo. / Human fungal infections have increased in the last years and affect mainly immunocompromised patients, carriers of HIV vírus, transplanted or with cancer. The antifungal agents used in treatment belong to a few groups of drugs and the increase of antifungal resistance in many pathogens leads to the necessity of developing new antifungal agents. Strains Trichosporon japonicum QU139 and Candida catenulata LV102 showed killer activity against several pathogenic yeasts, having a good potential for the development of new antimicrobial agents. The objective of the work was the optimization of conditions for production and detection of the antimicrobial compounds, aiming their future terapeutic use, and their purification. The killer effect of T. japonicum QU139 strain was evaluated by the well method against sensitive cells of Cryptococcus gattii C20 in media GYP, YM and Cheese in different pH and temperatures. The maximum killer activity was found in media GYP, pH 4.5, 25°C after 24 hours of incubation for T.japonicum QU139 and C. catenulata LV102. The isolation of the antimicrobial compound produced by the yeast T.japonicum QU139 was not possible by the methods for isolation of proteins/glicoproteins, corroborating the hypothesis that the toxin is a glycolipid.

Leveduras

Antifúngicos

Antimicrobianos

Candida

Cryptococcus gattii

Trichosporon

Trichosporon japonicum

Candida catenulata

Cryptococcus neoformans

Killer yeasts

Biotechnological potential

The Multifaceted Contribution of Natural Killer Cells During Herpes Simplex Type-1 Viral Infection.

Woolard, Stacie N

08 May 2010

Natural killer (NK) cells are non-specific killer cells of the innate immune system that eliminate target cells based on discrimination between self and non-self. Activation is carefully regulated through integration of signals received through both activating and inhibitory receptors. During the course of a herpes simplex virus type-1 (HSV-1) infection, NK cells can influence host susceptibility to infection with severe infections occurring in individuals with genetic defects in the NK cell response. In response to HSV infection, NK cells are recruited to the inflammatory tissue where ensuing reciprocal interactions with accessory cells and proinflammatory cytokines induce NK cell activation, cytolytic activity, and cytokine production, contributing to innate immune response and ultimately influencing the adaptive immune response. The objective of this study was to elucidate the multiple roles of NK cells during the numerous steps in anti-HSV immune induction. Accordingly, we have demonstrated that NK cells are novel helpers that assist and influence an anti-HSV immune response via the secretion of cytokines that enhance HSV-specific CD8+ T cell effector function and cytokine production. Taken together, data from this study presented the critical importance of NK cells in mounting an essential and efficient anti-HSV immunity. The key findings of our study were: 1. In the absence of NK cells, dendritic cells have decreased capacity to prime HSV-specific T cells. 2. HSV infected NK cells can be directly activated via toll-like receptor (TLR) in a MyD88-dependent mechanism; however, interaction with HSV infected dendritic cells yields optimal NK cell activation and function (CD69 and IFNγ). 3. TRAIL-expressing NK cells eliminate antigen-bearing immature dermal DCs (CD11c+CD8α-DR5+), that migrate to draining lymphoid organs, to facilitate antigen transfer to lymphoid resident CD8α+ DC for T cell cross priming. 4. 'Helpless' CD8+ T cell function, generated in the absence of CD4+ T cells, can be partially restored to wild-type levels by NK cell supplementation. 5. Treatment of NK cells with anti-CD69 antibody results in a heightened NK activated state and augments the adaptive immune response, without increasing NK cell numbers. These findings may contribute to the potential revelation of avenues to manipulate NK cells for anti-viral therapies.

CD8+ T cells

Dendritic cells

Natural Killer cells

Herpes Simplex Virus-1

Medical Immunology

Medical Sciences

Medicine and Health Sciences