Mucosal immune effector mechanisms-secretory antibodies and mucosal
cellular responses-could enhanced immune protection against HIV by
intercepting virus at mucosal surfaces and reducing this effective
"challenge dose" at mucosal portals of entry. The purpose of this project
is to develop immunization protocols using a live, highly-attenuated SIV
vaccine candidate, that could enhance local mucosal immune responses and
shorten the time required for development of immune protection against
mucosal challenge.
Aim 1 is to define effective mucosal immunization protocols. First,
SIVmac239delta4 will be inoculated via rectum or vagina with or without a
mucosal adjuvant; local immune responses will be compared to those in
systemically-inoculated monkeys. Then, systemic prime/mucosal boost
strategies will be tested, including live SIVmac239delta4 given IV,
followed by live or inactivated SIVmac239delta4 or oligomeric envelope
protein (with adjuvant) administered nasally, rectally and/or vaginally.
Anti-SIV IgA, IgM and IgG antibodies in serum and secretions, and anti-SIV
T cells in blood will be monitored over time. Aim II is to compare levels
of SIVmac239delta4 in the mucosal after mucosal versus systemic
inoculation of SIVmac239delta4, and to evaluate possible effects of
attenuated SIV infection on mucosal immune function. Viral genome and
antigens will be localized in rectal biopsies and correlated with the
immune responses observed in Aim I. Antigen-presenting cells, IgA, IgM and
IgG producing cells and T cell subsets in mucosal lymphoid follicles and
lamina propria will be quantitated, and mucosal responses to test antigens
evaluated. Aim III is to test the capacity of SIVmac239delta4 to protect
against mucosal challenge with virulent SIV. Monkeys immunized using the
optimal SIVmac239delta4 prime/boost protocol identified in Aim I will be
challenged at 2 time points (in parallel with systemically-inoculated
monkeys in Project III) to compare the time required for development of
immune protection against mucosal challenge with that seen after systemic
inoculation alone. These studies will guide future investigations of the
utility of live, attenuated SIV/HIV vaccines for mucosal immune
protection.
Public Health Relevance Statement
Data not available.
NIH Spending Category
No NIH Spending Category available.
Project Terms
AIDS vaccinesMacaca mulattaactive immunizationattenuated microorganismbiopsycytotoxic T lymphocytedrug administration routesgenomehuman immunodeficiency virus 1immunocytochemistryimmunoglobulin Aimmunoglobulin Gimmunoglobulin Mimmunomodulatorslive vaccinemonoclonal antibodymucosamucosal immunityvaccine developmentvirulencevirus genetics
National Institute of Allergy and Infectious Diseases
CFDA Code
DUNS Number
047006379
UEI
JDLVAVGYJQ21
Project Start Date
01-May-2000
Project End Date
30-April-2001
Budget Start Date
01-October-1998
Budget End Date
30-September-1999
Project Funding Information for 2000
Total Funding
$448,605
Direct Costs
$448,605
Indirect Costs
Year
Funding IC
FY Total Cost by IC
2000
National Institute of Allergy and Infectious Diseases
$448,605
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5P01AI035365-07 0006
Publications
Publications are associated with projects, but cannot be identified with any particular year of the project or fiscal year of funding. This is due to the continuous and cumulative nature of knowledge generation across the life of a project and the sometimes long and variable publishing timeline. Similarly, for multi-component projects, publications are associated with the parent core project and not with individual sub-projects.
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Clinical Studies
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