HARVARD COLLEGE, PRESIDENT & FELLOWS OF
Relapse after therapy remains a critical problem for most types of cancer in humans, even when cancer-specific therapy is initially effective. Understanding the basis for cancer resistance and recurrence is a critical pre-requisite for developing more effective treatments. Recent data indicate that in some cancers, including leukemia, colon cancer, and certain brain tumors, a minority of cells in the initial tumor possesses unique properties reminiscent of normal tissue stem cells: a capacity for extensive self-renewal and differentiation potential. Relative drug resistance in these cells may be especially relevant for cancer recurrence. Thus, it is important to understand the precise relationship between these tumor-initiating cells and stem cells found in normal tissue, as key differences might be exploited for therapeutic benefit. In this project we outline an approach to identify critical similarities and differences in the genetic material of normal and cancer stem cells isolated from normal intestine/colorectal cancer, neural stem cells/glioblastoma multiforme (GBM) and hematopoietic stem cells/acute myelogenous leukemia (AML). We will isolate cancer stem-cells from human tumors and mouse models of cancer, and we will compare them with normal tissue stem cells. The analysis will provide an unprecedented and comprehensive picture of normal and cancer stem cells, highlighting key differences that may be exploited therapeutically. The dataset and concomitant analysis will be made available as a resource to the stem cell and cancer research communities. To complement these efforts, we will also develop sophisticated mouse models of four signaling pathways that play seminal roles in cancer stem cell biology. In sum, the studies proposed in this highly collaborative project will provide vital information to aid in developing therapies that might target cancer stem cells while sparing their normal counterparts.
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| AWARD OVERVIEW |
| Award Number |
1RC2CA148222-01 |
Funding Agency |
Department of Health and Human Services |
| Total Award Amount |
$3,425,234 |
Project Location - City |
Boston |
| Award Date |
09/30/2009 |
Project Location - State |
MA |
| Project Status |
Completed |
Project Location - Zip |
02115-6013
|
| Jobs Reported |
0.00 |
Congressional District |
08 |
| Project Location - Country |
US |
|
|
Recipient Information
(Grants)
| Recipient Information (Grants) |
|
Recipient Name
|
HARVARD COLLEGE, PRESIDENT & FELLOWS OF |
| Recipient DUNS Number |
082359691
|
| Recipient Address |
1350 MASS AVE STE 600 |
| Recipient City |
CAMBRIDGE |
| Recipient State |
Massachusetts |
| Recipient Zip |
02138-3846 |
| Recipient Congressional District |
08 |
| Recipient Country |
USA |
Required to Report Top 5
Highly Compensated Officials |
No |
Projects and Jobs Information
| Projects and Jobs Information |
| Project Title |
Comprehensive Phenotypic Comparison of Normal and Cancer Stem Cells |
| Project Status |
Completed |
| Final Project Report Submitted |
Yes |
| Project Activities Description |
Colleges, Universities, and Professional Schools |
| Quarterly Activities/Project Description |
P1: Histone methylation profiles of stem/progenitor cells have been published, and we are assessing changes in various model systems. We have demonstrated that leukemia stem cell population is specifically dependent upon sustained high-level expression of DMRT1, and the mechanism behind this dependence is due to reactivation of repressed genes that are associated with H3K27me3 and H3K4me3. This will be submitted shortly. P2: We have mapped genome-wide epigenetic histone modifications, H3K4Me2 and H3K27Ac, in relation to gene expression in mouse intestinal crypts and a human colon cancer cell line, hence identifying functional intestinal epithelial gene enhancers. This was recently published. We studied the roles and mechanisms of interaction between epigenetic alterations and transcription factors in cell lines and in vivo. Efforts to integrate the resulting insights with those from hematopoietic and neural stem and progenitor cells are in progress. P3: We have completed genomic and epi-genomic datasets in pre-malignant and malignant neural stem cells, including profiles for all protein-coding genes & miRNA genes, & global histone modification patterns. Integrated genomic analyses continue and functional validation of these candidates & their roles in gliomagenesis are in progress. P4: We have completed development and have launched an online cancer stem cell molecular data integration tool. The online platform (available at http://discovery.hsci.harvard.edu/) allows interrogation and comparison of cancer stem cell molecular profiles at the level of the gene using shared gene expression, and shared, discrete functions at the pathway level. We are currently working to incorporate epigenetic data into this platform. P5: Our most recent progress has come with the Hedgehog Reporter; Gli1-Luc/TdTomato Knock-in: The Gil1 targeting vector has been completed and 4 correctly targeted ES clones have been identified and are ready to be confirmed via sequencing and karyotyped. |
| Jobs Created |
0.00 |
| Description of Jobs Created |
There are no jobs to report this quarter. |
Purchaser Information
(Grants)
| Purchaser Information |
| Contracting Office ID |
Not Reported |
| Contracting Office Name |
Not Available |
| Contracting Office Region |
Not Available |
| TAS Major Program |
75-0850 |
| Award Information |
| Award Date |
09/30/2009 |
| Award Number |
1RC2CA148222-01 |
| 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 |
$3,425,234 |
| Funds Invoiced/Received |
$3,380,626 |
| Expenditure Amount |
$3,380,626 |
| 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 |
611310 |
| Activity Description |
Colleges, Universities, and Professional Schools |
| 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 |
0 |
| Total Amount of payments to vendors greater than $25,000/award |
$0 |
| Number of payments to vendors less than $25,000/award |
94 |
| Total Amount of payments to vendors less than $25,000/award |
$5,190 |
| Location Information |
| Latitude, Longitude |
42º 20' 16",
-71º 6' 23" |
| Congressional District |
08 |
| Address 1 |
|
| Address 2 |
|
| City |
Boston |
| County |
Suffolk |
| State |
MA |
| Zip |
02115-6013 |
|
 |