Your search keyword '"Espinosa, Vanessa"' showing total 7 results

1. Critical role of interferons in gastrointestinal injury repair.

Author

McElrath, Constance, Espinosa, Vanessa, Lin, Jian-Da, Peng, Jianya, Sridhar, Raghavendra, Dutta, Orchi, Tseng, Hsiang-Chi, Smirnov, Sergey V., Risman, Heidi, Sandoval, Marvin J., Davra, Viralkumar, Chang, Yun-Juan, Pollack, Brian P., Birge, Raymond B., Galan, Mark, Rivera, Amariliz, Durbin, Joan E., and Kotenko, Sergei V.

Subjects

GASTROINTESTINAL system injuries, INTERFERON receptors, TYPE I interferons, INTERFERONS, ULCERATIVE colitis, DEXTRAN sulfate

Abstract

The etiology of ulcerative colitis is poorly understood and is likely to involve perturbation of the complex interactions between the mucosal immune system and the commensal bacteria of the gut, with cytokines acting as important cross-regulators. Here we use IFN receptor-deficient mice in a dextran sulfate sodium (DSS) model of acute intestinal injury to study the contributions of type I and III interferons (IFN) to the initiation, progression and resolution of acute colitis. We find that mice lacking both types of IFN receptors exhibit enhanced barrier destruction, extensive loss of goblet cells and diminished proliferation of epithelial cells in the colon following DSS-induced damage. Impaired mucosal healing in double IFN receptor-deficient mice is driven by decreased amphiregulin expression, which IFN signaling can up-regulate in either the epithelial or hematopoietic compartment. Together, these data underscore the pleiotropic functions of IFNs and demonstrate that these critical antiviral cytokines also support epithelial regeneration following acute colonic injury. Despite being prevalent yet well studied, ulcerative colitis still has poorly characterized pathophysiology. Here the authors use mouse colitis models to find that type I and III interferon (IFN) both contribute to ameliorating the disease, with IFN signaling in either the epithelial or hematopoietic compartment sufficient for this protective effect. [ABSTRACT FROM AUTHOR]

Published

2021

2. Type III interferon is a critical regulator of innate antifungal immunity.

Author

Espinosa, Vanessa, Dutta, Orchi, McElrath, Constance, Peicheng Du, Yun-Juan Chang, Cicciarelli, Bryan, Pitler, Amy, Whitehead, Ian, Obar, Joshua J., Durbin, Joan E., Kotenko, Sergei V., and Rivera, Amariliz

Subjects

INTERFERONS, ANTIFUNGAL agents, CYTOKINES, ASPERGILLUS fumigatus, NEUTROPHILS

Abstract

Type III interferons (IFN-λs) are the most recently found members of the IFN cytokine family and engage IFNLR1 and IL10R2 receptor subunits to activate innate responses against viruses. We have identified IFN-λs as critical instructors of antifungal neutrophil responses. Using Aspergillus fumigatus (Af) as a model to study antifungal immune responses, we found that depletion of CCR2+ monocytes compromised the ability of neutrophils to control invasive fungal growth. Using an unbiased approach, we identified type I and III IFNs as critical regulators of the interplay between monocytes and neutrophils responding to Af. We found that CCR2+ monocytes are an important early source of type I IFNs that prime optimal expression of IFN-λ. Type III IFNs act directly on neutrophils to activate their antifungal response, and mice with neutrophil-specific deletion of IFNLR1 succumb to invasive aspergillosis. Dysfunctional neutrophil responses in CCR2-depleted mice were rescued by adoptive transfer of pulmonary CCR2+ monocytes or by exogenous administration of IFN-α and IFN-λ. Thus, CCR2+ monocytes promote optimal activation of antifungal neutrophils by initiating a coordinated IFN response. We have identified type III IFNs as critical regulators of neutrophil activation and type I IFNs as early stimulators of IFN-λ expression. [ABSTRACT FROM AUTHOR]

Published

2017

3. Trajectory tracking for quadcopter's formation with two control strategies.

Author

Moya, Viviana, Espinosa, Vanessa, Chavez, Danilo, Leica, Paulo, and Camacho, Oscar

Published

2016

4. First Line of Defense: Innate Cell-Mediated Control of Pulmonary Aspergillosis.

Author

Espinosa, Vanessa and Rivera, Amariliz

Subjects

ASPERGILLUS fumigatus, NATURAL immunity, PULMONARY aspergillosis

Abstract

Mycotic infections and their effect on the human condition have been widely overlooked and poorly surveilled by many health organizations even though mortality rates have increased in recent years. The increased usage of immunosuppressive and myeloablative therapies for the treatment of malignant as well as non-malignant diseases has contributed significantly to the increased incidence of fungal infections. Invasive fungal infections have been found to be responsible for at least 1.5 million deaths worldwide. About 90% of these deaths can be attributed to Cryptococcus, Candida, Aspergillus, and Pneumocystis. A better understanding of how the host immune system contains fungal infection is likely to facilitate the development of much needed novel antifungal therapies. Innate cells are responsible for the rapid recognition and containment of fungal infections and have been found to play essential roles in defense against multiple fungal pathogens. In this review we summarize our current understanding of host-fungi interactions with a focus on mechanisms of innate cell-mediated recognition and control of pulmonary aspergillosis. [ABSTRACT FROM AUTHOR]

Published

2016

5. IL-1α Signaling Is Critical for Leukocyte Recruitment after Pulmonary Aspergillus fumigatus Challenge.

Author

Caffrey, Alayna K., Lehmann, Margaret M., Zickovich, Julianne M., Espinosa, Vanessa, Shepardson, Kelly M., Watschke, Christopher P., Hilmer, Kimberly M., Thammahong, Arsa, Barker, Bridget M., Rivera, Amariliz, Cramer, Robert A., and Obar, Joshua J.

Subjects

INTERLEUKIN-1, LEUCOCYTES, ASPERGILLUS fumigatus, LUNG infections, MACROPHAGES

Abstract

Aspergillus fumigatus is a mold that causes severe pulmonary infections. Our knowledge of how A. fumigatus growth is controlled in the respiratory tract is developing, but still limited. Alveolar macrophages, lung resident macrophages, and airway epithelial cells constitute the first lines of defense against inhaled A. fumigatus conidia. Subsequently, neutrophils and inflammatory CCR2+ monocytes are recruited to the respiratory tract to prevent fungal growth. However, the mechanism of neutrophil and macrophage recruitment to the respiratory tract after A. fumigatus exposure remains an area of ongoing investigation. Here we show that A. fumigatus pulmonary challenge induces expression of the inflammasome-dependent cytokines IL-1β and IL-18 within the first 12 hours, while IL-1α expression continually increases over at least the first 48 hours. Strikingly, Il1r1-deficient mice are highly susceptible to pulmonary A. fumigatus challenge exemplified by robust fungal proliferation in the lung parenchyma. Enhanced susceptibility of Il1r1-deficient mice correlated with defects in leukocyte recruitment and anti-fungal activity. Importantly, IL-1α rather than IL-1β was crucial for optimal leukocyte recruitment. IL-1α signaling enhanced the production of CXCL1. Moreover, CCR2+ monocytes are required for optimal early IL-1α and CXCL1 expression in the lungs, as selective depletion of these cells resulted in their diminished expression, which in turn regulated the early accumulation of neutrophils in the lung after A. fumigatus challenge. Enhancement of pulmonary neutrophil recruitment and anti-fungal activity by CXCL1 treatment could limit fungal growth in the absence of IL-1α signaling. In contrast to the role of IL-1α in neutrophil recruitment, the inflammasome and IL-1β were only essential for optimal activation of anti-fungal activity of macrophages. As such, Pycard-deficient mice are mildly susceptible to A. fumigatus infection. Taken together, our data reveal central, non-redundant roles for IL-1α and IL-1β in controlling A. fumigatus infection in the murine lung. [ABSTRACT FROM AUTHOR]

Published

2015

6. Inflammatory Monocytes Orchestrate Innate Antifungal Immunity in the Lung.

Author

Espinosa, Vanessa, Jhingran, Anupam, Dutta, Orchi, Kasahara, Shinji, Donnelly, Robert, Du, Peicheng, Rosenfeld, Jeffrey, Leiner, Ingrid, Chen, Chiann-Chyi, Ron, Yacov, Hohl, Tobias M., and Rivera, Amariliz

Subjects

MONOCYTES, ANTIFUNGAL agents, ASPERGILLUS fumigatus, IMMUNOCOMPROMISED patients, CHEMOKINE receptors, DENDRITIC cells, LUNG diseases

Abstract

Aspergillus fumigatus is an environmental fungus that causes invasive aspergillosis (IA) in immunocompromised patients. Although -CC-chemokine receptor-2 (CCR2) and Ly6C-expressing inflammatory monocytes (CCR2+Mo) and their derivatives initiate adaptive pulmonary immune responses, their role in coordinating innate immune responses in the lung remain poorly defined. Using conditional and antibody-mediated cell ablation strategies, we found that CCR2+Mo and monocyte-derived dendritic cells (Mo-DCs) are essential for innate defense against inhaled conidia. By harnessing fluorescent Aspergillus reporter (FLARE) conidia that report fungal cell association and viability in vivo, we identify two mechanisms by which CCR2+Mo and Mo-DCs exert innate antifungal activity. First, CCR2+Mo and Mo-DCs condition the lung inflammatory milieu to augment neutrophil conidiacidal activity. Second, conidial uptake by CCR2+Mo temporally coincided with their differentiation into Mo-DCs, a process that resulted in direct conidial killing. Our findings illustrate both indirect and direct functions for CCR2+Mo and their derivatives in innate antifungal immunity in the lung. [ABSTRACT FROM AUTHOR]

Published

2014

7. Helminth resistance is mediated by differential activation of recruited monocyte-derived alveolar macrophages and arginine depletion.

Author

Chen, Fei, El-Naccache, Darine W., Ponessa, John J., Lemenze, Alexander, Espinosa, Vanessa, Wu, Wenhui, Lothstein, Katherine, Jin, Linhua, Antao, Olivia, Weinstein, Jason S., Damani-Yokota, Payal, Khanna, Kamal, Murray, Peter J., Rivera, Amariliz, Siracusa, Mark C., and Gause, William C.

Abstract

Macrophages are known to mediate anti-helminth responses, but it remains uncertain which subsets are involved or how macrophages actually kill helminths. Here, we show rapid monocyte recruitment to the lung after infection with the nematode parasite Nippostrongylus brasiliensis. In this inflamed tissue microenvironment, these monocytes differentiate into an alveolar macrophage (AM)-like phenotype, expressing both SiglecF and CD11c, surround invading parasitic larvae, and preferentially kill parasites in vitro. Monocyte-derived AMs (Mo-AMs) express type 2-associated markers and show a distinct remodeling of the chromatin landscape relative to tissue-derived AMs (TD-AMs). In particular, they express high amounts of arginase-1 (Arg1), which we demonstrate mediates helminth killing through L-arginine depletion. These studies indicate that recruited monocytes are selectively programmed in the pulmonary environment to express AM markers and an anti-helminth phenotype. [Display omitted] • Helminth infection promotes a restructuring of myeloid cells in the lung • Highly activated monocyte-derived macrophages populate the lung post-infection • These macrophages express alveolar macrophage markers and elevated levels of Arg1 • Arg1 mediates helminth killing through localized depletion of arginine Chen et al. show that, during helminth infection, monocytes recruited to the lung can assume an alveolar-like macrophage phenotype and differentially express markers associated with tissue remodeling and allergic inflammation, including arginase-1 (Arg1). Arg1 mediates helminth killing through depletion of arginine, indicating nutrient deprivation as a host resistance mechanism. [ABSTRACT FROM AUTHOR]

Published

2022