LELAND STANFORD JUNIOR UNIVERSITY, THE
The immune system is profoundly affected by aging. Older individuals are at higher risk of death and disability from infections and cancer. The reason for such disproportionate susceptibility appears to be age-attributed impairment or suboptimal performance of immune system. Such age-attributed immune dysfunction might have a hidden role in other disease states such as chronic inflammatory diseases (COPD or rheumatoid arthritis) and degenerative diseases such as atherosclerosis and osteoarthritis. Yet, systematic efforts to understand the role of aging on immunological mechanisms are lacking. There are two reasons for this. The first is absence of well-defined set of immunological measures that are easy to perform but comprehensive in scope. A well-defined battery of such tests, similar to those for renal or hepatic function, would allow one to characterize the functional status of immunity (innate, adaptive or even aberrant) in varied settings including old age, health and disease. The second reason is the absence of understanding of what constitutes 'normal' immunobiology of aging in the general population Our proposal would have one overriding aim: To develop and make available to other investigators a control healthy subject registry and immune profile database and bio-specimen repository developed from a cohort of at least 1100 normal healthy individuals. The dataset will comprise a cross-sectional analysis of the local San Francisco Peninsula general population between the ages of 20 and 90 (representing equal gender and representative ethnic population, and equal distribution by decade of life). The registry will contain demographic data, race/ethnicity, prescribed medications, over the counter medications, vitamins, alternative therapies, physical function questionnaire, alternative contact person, and HIPPA release. Fasting blood will be obtained for immune phenotyping as described in Specific Aim 3 the immune profile will contain the results of both conventional and novel immune profiling assays to develop the normative immune profile of aging (using PBMC subset analysis, cytokines, and activation induced signaling of PBMCs for phosphoepitope and gene expression analyses). Data from these analyses will be useful in identifying biomarkers of the normal immune profile associated with aging as well as correlation with phenotypic aspects of aging such as sarcopenia and disability The immune profile (as well as normal blood chemistries and demographic data) of these subjects will be made available to serve as the basis for future longitudinal study of change in the immune profile over time in association with the development of co-morbidities associated with aging. The primary deliverable for this proposal will be a unique open access electronic data repository that has phenotypic information in multiple scales (epidemiological, and clinical, and, at the cell and molecular level, of immune phenotype) and genetic and proteomic information (gene and protein expression of resting and activated PBCs) on 1100 healthy individuals at different ages from 20 to 90 years. This resource will enable a systems-based approach to the immunology of aging. PUBLIC HEALTH RELEVANCE: Our proposal is an initiative of the new Stanford Institute of Immunity, Transplantation and Infection (ITI) to develop an immune profile of normal healthy subjects throughout 7 decades of life consisting of a cross sectional analysis of 1100 normal individuals representing equal distribution of gender and from age 20 to 90. Demographic data and normal lab chemistries will be obtained from each individual as well as their immune profile using instrumentation and technology available in the Stanford Human Immune Monitoring Center. We will develop an open-access data repository that will enable free sharing of high throughput analyte data and appropriately de-identified phenotypic data on a web-based platform using high quality open source and statistical tools.
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| AWARD OVERVIEW |
| Award Number |
1RC4AG039014-01 |
Funding Agency |
Department of Health and Human Services |
| Total Award Amount |
$3,495,470 |
Project Location - City |
Palo Alto |
| Award Date |
09/30/2010 |
Project Location - State |
CA |
| Project Status |
More than 50% Completed |
Project Location - Zip |
94304-1212
|
| Jobs Reported |
4.41 |
Congressional District |
18 |
| Project Location - Country |
US |
|
|
Recipient Information
(Grants)
| Recipient Information (Grants) |
|
Recipient Name
|
LELAND STANFORD JUNIOR UNIVERSITY, THE |
| Recipient DUNS Number |
009214214
|
| Recipient Address |
450 SERRA MALL |
| Recipient City |
STANFORD |
| Recipient State |
California |
| Recipient Zip |
94305-2004 |
| Recipient Congressional District |
18 |
| Recipient Country |
USA |
Required to Report Top 5
Highly Compensated Officials |
No |
Projects and Jobs Information
| Projects and Jobs Information |
| Project Title |
IMMUNOBIOLOGY OF AGING |
| Project Status |
More than 50% Completed |
| Final Project Report Submitted |
No |
| Project Activities Description |
Research & Public Policy Analysis |
| Quarterly Activities/Project Description |
As of March 12, 2013, we have enrolled 744 participants. Of these, 5 were enrolled since our prior report in December 2012. The age distribution of participants is: 40-50 = 102; 51-60 = 204; 61-70 = 162; 71-80 =180; 81+= 95. Of these, 64% were women; 75% were Caucasian, 2% African American, 15% Asian and 4% Hispanic, decline to state or other (multi-racial) 4%. We have collected data on physical function, depression inventory, measures of frailty, medication and comorbidities, as well as clinical laboratory testing that includes a complete blood count, comprehensive metabolic profile, lipid panel and C-reactive protein. Data verification and dataset cleanup have been completed on 625 participants. We expect to enroll the 750th person in the next few weeks.
Immune assays have been completed on approximately 100 individuals, with an additional cohort of 40, chosen from the oldest (80+ years) and youngest age groups (41-50 years) based on initial results showing the greatest difference between these two age groups. We are performing serum Luminex, whole blood gene expression, Luminex on stimulated supernatants, gene expression on stimulated PBMC, CyTOF immunophenotyping, and phospho-flow on PBMC. Initial analysis of CyTOF data on the first 40 individuals revealed some age-specific trends. In particular, there is an age-specific increase in the total percentage of CD8+ T cells and B cells with a minor trend towards an increase in percentage of monocytes. While no change in phosphorylated Stat(pStat1) was observed in response in IFN¿, an age-specific decrease in pStat3 in response to IL-6 and IFN¿ was observed in CD4+, CD8+ and monocytes. We are currently integrating all the immune data that are already generated for computational analyses and will add data for the additional 40 cohort into the final analysis pool. By the end of this funding period, we plan to complete data generation and analysis for 200 individuals.
|
| Jobs Created |
4.41 |
| Description of Jobs Created |
Associate Researcher, Research Assistant, Research Associate, Research Technician, Senior Researcher
|
Purchaser Information
(Grants)
| Purchaser Information |
| Contracting Office ID |
Not Reported |
| Contracting Office Name |
Not Available |
| Contracting Office Region |
Not Available |
| TAS Major Program |
75-0842 |
| Award Information |
| Award Date |
09/30/2010 |
| Award Number |
1RC4AG039014-01 |
| 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 |
$3,495,470 |
| Funds Invoiced/Received |
$1,936,946 |
| Expenditure Amount |
$1,936,946 |
| Infrastructure Expenditure Amount |
$0 |
| Infrastructure Purpose and Rationale |
Not Reported |
| Infrastructure Point of Contact Name |
Not Reported |
| Infrastructure Point of Contact Email |
Not Reported |
| Infrastructure Point of Contact Phone |
Not Reported |
| Infrastructure Point of Contact Address |
Not Reported |
| Infrastructure Point of Contact City |
Not Reported |
| Infrastructure Point of Contact State |
Not Reported |
| Infrastructure Point of Contact Zip |
Not Reported |
Product or Service Information
(Grants)
| Product or Service Information |
| Primary Activity Code |
**K |
| Activity Description |
Research & Public Policy Analysis |
| Sub-Awards Information |
| Sub-awards to Organizations |
0 |
| Sub-award Amounts to Organizations |
$0 |
| 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 |
1 |
| Total Amount of payments to vendors greater than $25,000/award |
$29,227 |
| Number of payments to vendors less than $25,000/award |
712 |
| Total Amount of payments to vendors less than $25,000/award |
$303,055 |
- Award Number 1RC4AG039014-01 -
| Award Number |
1RC4AG039014-01 |
| Sub-Award Number |
N/A |
| Vendor DUNS Number |
831905125 |
| Vendor HQ Zip Code + 4 |
|
| Vendor Name |
|
| Product and Service Description |
Laboratory Supplies |
| Payment Amount |
$29,227 |
| Location Information |
| Latitude, Longitude |
37º 24' 30",
-122º 9' 4" |
| Congressional District |
18 |
| Address 1 |
3160 Porter Drive |
| Address 2 |
|
| City |
Palo Alto |
| County |
Santa Clara |
| State |
CA |
| Zip |
94304-1212 |
|
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