BAYLOR RESEARCH INSTITUTE, THE
Vaccination represents one of the major successes of medicine as it has spared countless people from polio, tetanus and other acute infections. Yet, improved immunization strategies are needed to make vaccines for microbes that cause considerable morbidity . To identify novel strategies for protective vaccination we will study dendritic cells (DCs) which specialized to capture and process antigens in vivo, presenting the MHC molecules to T cells. DCs also present antigens to B cells. Maturation and subsets allow DCs to control diverse immune responses. Our long-term goal is to develop novel human vaccines based on in vivo DC-targeting. Our hypothesis is that Human Dendritic cells subsets express distinct uptake and signaling receptors that need to be mobilized in concert to provide durable immune responses leading to increased resistance to microbes at the mucosal port of entry. To this end, we have made high affinity monoclonal antibodies against several DC surface molecules and conjugated them to several influenza virus proteins. We have shown that antigens delivered to a single type of human DCs through different surface lectins induce distinct types of antigen-specific CD4+ T cell responses. The current focus is on mucosal immunity because mucosa is a major site of invasion as well as replication of pathogens, including influenza virus. Thus, the induction/activation of two major effectors, B cells and CD8+ T cells, with mucosal homing capacity is expected to limit viral replication, resulting in reduced disease burden. Furthermore, induction of CD4+ T cells with helper functions for B cells or CTLs will enhance the longevity of memory cells and the magnitude and the quality of mucosal homing effectors. We view the candidate vaccine as a bispecific antibody a) binding to two different cell surface antigens, such as specific lectin for antigen delivery and CD40 for activation, or to two different DC subsets, to harness their capacity to induce different type of immune effectors, and in addition b)TLR agonists as DC activators. We propose four projects and two technical development components which will be supported by six cores.
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| AWARD OVERVIEW |
| Award Number |
3U19AI057234-06S3 |
Funding Agency |
Department of Health and Human Services |
| Total Award Amount |
$1,600,000 |
Project Location - City |
Dallas |
| Award Date |
09/16/2009 |
Project Location - State |
TX |
| Project Status |
Completed |
Project Location - Zip |
75204-6409
|
| Jobs Reported |
3.66 |
Congressional District |
30 |
| Project Location - Country |
US |
|
|
Recipient Information
(Grants)
| Recipient Information (Grants) |
|
Recipient Name
|
BAYLOR RESEARCH INSTITUTE, THE |
| Recipient DUNS Number |
145745022
|
| Recipient Address |
3310 LIVE OAK STE 501 |
| Recipient City |
DALLAS |
| Recipient State |
Texas |
| Recipient Zip |
75204-6134 |
| Recipient Congressional District |
30 |
| Recipient Country |
USA |
Required to Report Top 5
Highly Compensated Officials |
No |
Projects and Jobs Information
| Projects and Jobs Information |
| Project Title |
Harnessing Human DC Subsets for Improved Muscosal Vaccines |
| Project Status |
Completed |
| Final Project Report Submitted |
Yes |
| Project Activities Description |
Allergy & Immunological Diseases |
| Quarterly Activities/Project Description |
Report: conclusion was clear ? there was no or minimal efficacy evident from IN administration without adjuvant of the tested DC-targeting vaccines ? more robust responses were observed via the ID route, but even these needed adjuvant for protective immunity. Nasal administration with adjuvant was not tested.Vaccines tested were: anti-LOX-1-HA1, anti-Dectin-1-HA1, anti-MARCO-HA1, control IgG4-HA1, and FluMist.Also one groups previously infected with virus two given a single dose(ID) with anti-Dectin-1-NP with and without Poly ICLC to test boosting of memory T and B cell responses. This dataset is almost complete and a significant boost in humoral immunity was observed without adjuvant, while the adjuvant group gave strong boosts in both B and T cell immunity.This study was aimed to determine and compare the effectiveness of the best vaccine candidates with Poly ICLC as a vaccine adjuvant with the commercially available Flu kit vaccine. Poly ICLC group (G8) was used as control. Antibiotics added to the ELISPOT tests rescued some, but not all of this data. Also, it became clear that one group (anti-CD40-NP vaccine) was mistakenly administered with a HA targeting vaccine during one of the 3 vaccinations, scientifically devaluing this particular group. TECH DEV 2 Aim: To test single antigen-specific B cells elicited by the DC-targeting vaccines in the Supplement Project 1 (Aim 1 and 2) NHP trials.Progress: Based on our annual review meeting, this area is currently on hold as all remaining resources are focused on the NHP studies looking at protective immunity as described above. When the most efficacious vaccines are established, then these single cell studies can be revived in a very meaningful setting ? to better understand the mechanism of protection. |
| Jobs Created |
3.66 |
| Description of Jobs Created |
New jobs: Post doctoral fellow 1 FTE and 66% FTE.
Jobs preserved 50% of a PhD Research Associate and 1.5 FTE Research assistants at BRI/BIIR
Veterinarian and 84% FTE of a Medical Research Technician.
|
Purchaser Information
(Grants)
| Purchaser Information |
| Contracting Office ID |
Not Reported |
| Contracting Office Name |
Not Available |
| Contracting Office Region |
Not Available |
| TAS Major Program |
75-0900 |
| Award Information |
| Award Date |
09/16/2009 |
| Award Number |
3U19AI057234-06S3 |
| Order Number |
|
| Award Type |
Grants |
| Funding Agency ID |
75 |
| Funding Agency Name |
Department of Health and Human Services |
| Funding Office Name |
Not Available |
| Awarding Agency ID |
75 |
| Awarding Agency Name |
Department of Health and Human Services |
| Amount of Award |
$1,600,000 |
| Funds Invoiced/Received |
$1,600,000 |
| Expenditure Amount |
$1,600,000 |
| Infrastructure Expenditure Amount |
$0 |
| Infrastructure Purpose and Rationale |
Not Reported |
| Infrastructure Point of Contact Name |
Deborah Price |
| Infrastructure Point of Contact Email |
deborapr@baylorhealth.edu |
| Infrastructure Point of Contact Phone |
(214) 820-9990 |
| Infrastructure Point of Contact Address |
3310 Live Oak |
| Infrastructure Point of Contact City |
Dallas |
| Infrastructure Point of Contact State |
TX |
| Infrastructure Point of Contact Zip |
75204-6409 |
Product or Service Information
(Grants)
| Product or Service Information |
| Primary Activity Code |
G02.02 |
| Activity Description |
Allergy & Immunological Diseases |
| Sub-Awards Information |
| Sub-awards to Organizations |
1 |
| Sub-award Amounts to Organizations |
$1,361,239 |
| Sub-Awards to Individuals |
0 |
| Sub-Award Amounts to Individuals |
$0 |
| Number of Sub-awards less than $25,000/award |
0 |
| Amount of Sub-awards less than $25,000/award |
$0 |
| Number of payments to vendors greater than $25,000 |
0 |
| Total Amount of payments to vendors greater than $25,000/award |
$0 |
| Number of payments to vendors less than $25,000/award |
0 |
| Total Amount of payments to vendors less than $25,000/award |
$0 |
Sub-award 01 - ADMINISTRATORS OF THE TULANE EDUCATIONAL FUND, THE
| Sub-Award Amount |
$1,361,239 |
| Sub-Award Date |
09/28/2009 |
| Sub-Awards Disbursed |
$1,346,418.49 |
| Project Location - City |
New Orleans |
| Project Location - State |
LA |
| Project Location - Zip Code |
70112-2699 |
| Project Location - Congressional District |
02 |
| Sub-Recipient DUNS Number |
053785812
|
| Sub-Recipient Address |
6823 SAINT CHARLES AVE |
| Sub-Recipient City |
NEW ORLEANS |
| Sub-Recipient State |
Louisiana |
| Sub-Recipient Zip Code |
70118-5665 |
| Sub-Recipient Congressional District |
02 |
Required To Report Top 5
Highly Compensated Officials |
No |
| Location Information |
| Latitude, Longitude |
32º 47' 35",
-96º 47' 1" |
| Congressional District |
30 |
| Address 1 |
3434 Live Oak |
| Address 2 |
|
| City |
Dallas |
| County |
Dallas |
| State |
TX |
| Zip |
75204-6409 |
|
 |