Abstract

Cellular adhesion, migration and communication mechanisms have been recognized as crucial elements regulating the fate and function of leukocytes and their participation in immune responses. As such, the direct visalization of cell-cell and cell-pathogen interactions and the fine structural feature that influence these events is central to our understanding of how the immune system responds to antigen challenge. The Intravital Microscopy Core (Core B) has been formulated based on a stated need of PPG investigators and is designed to draw on the considerable experience of its key personnel to provide expertise and specialized equipment in the design and execution of in vivo imaging studies of immune responses to viral infections and other challenges. The Specifc Aims of the Intravital Microscopy Core are as follows: 1. To provide access and expertise in conducting specific experiments utilizing multi-photon microscopy recordings of intra- and extravascular blood cell adhesion and migration as well as cell-cell and cellpathogen interactions in as many as six dimensions (i.e. space, time, color, fluorescence intensity). 2. To offer a custom-designed environment with appropriate biosafety conditions for the generation, housing and intravital microscopy analysis of virally infected mice. 3. To execute and analyze intravital microscopy-based adhesion and migration studies in murine tissues. Currently available imaging models include: bladder;bone marrow;cremaster muscle;ear skin;knee joint;liver;popliteal and inguinal lymph node;small intestine, including mesentery, Peyer's patches and lamina propria;and spinal cord. 4. To provide assistance in the planning, execution and analysis of blood cell homing in vivo by providing standardized models of inflammation and infectious diseases and on-site fluorescent tagging of cells and viruses. 5. To provide computational resources for the storage, processing and in-depth analysis of digital and video-based imaging data. Services to be provided by Core B will allow participating investigators to investigate innate and adaptive immune cell behavior at a resolution ranging from single cell organelles to intact animals in a customdesigned environment dedicated to the study of replicating mammalian pathogens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI078897-03
Application #
8121529
Study Section
Special Emphasis Panel (ZAI1)
Project Start
Project End
Budget Start
2010-08-01
Budget End
2011-07-31
Support Year
3
Fiscal Year
2010
Total Cost
$384,438
Indirect Cost

  Institution

Name
Harvard University
Department
Type
DUNS #
047006379
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Janssen, Erin; Kumari, Sudha; Tohme, Mira et al. (2017) DOCK8 enforces immunological tolerance by promoting IL-2 signaling and immune synapse formation in Tregs. JCI Insight 2:
Deruaz, Maud; Moldt, Brian; Le, Khoa M et al. (2016) Protection of Humanized Mice From Repeated Intravaginal HIV Challenge by Passive Immunization: A Model for Studying the Efficacy of Neutralizing Antibodies In Vivo. J Infect Dis 214:612-6
Wheeler, Lee Adam; Trifonova, Radiana T; Vrbanac, Vladimir et al. (2016) TREX1 Knockdown Induces an Interferon Response to HIV that Delays Viral Infection in Humanized Mice. Cell Rep 15:1715-27
Gerlach, Carmen; Moseman, E Ashley; Loughhead, Scott M et al. (2016) The Chemokine Receptor CX3CR1 Defines Three Antigen-Experienced CD8 T Cell Subsets with Distinct Roles in Immune Surveillance and Homeostasis. Immunity 45:1270-1284
Pang, Paul; Jin, Xiaohua; Proctor, Brandon M et al. (2015) RGS4 inhibits angiotensin II signaling and macrophage localization during renal reperfusion injury independent of vasospasm. Kidney Int 87:771-83
Griesbeck, Morgane; Ziegler, Susanne; Laffont, Sophie et al. (2015) Sex Differences in Plasmacytoid Dendritic Cell Levels of IRF5 Drive Higher IFN-? Production in Women. J Immunol 195:5327-36
Sewald, Xaver; Ladinsky, Mark S; Uchil, Pradeep D et al. (2015) Retroviruses use CD169-mediated trans-infection of permissive lymphocytes to establish infection. Science 350:563-567
Stary, Georg; Olive, Andrew; Radovic-Moreno, Aleksandar F et al. (2015) VACCINES. A mucosal vaccine against Chlamydia trachomatis generates two waves of protective memory T cells. Science 348:aaa8205
Porichis, Filippos; Hart, Meghan G; Zupkosky, Jennifer et al. (2014) Differential impact of PD-1 and/or interleukin-10 blockade on HIV-1-specific CD4 T cell and antigen-presenting cell functions. J Virol 88:2508-18
Sage, Peter T; Alvarez, David; Godec, Jernej et al. (2014) Circulating T follicular regulatory and helper cells have memory-like properties. J Clin Invest 124:5191-204

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