CHILDREN'S HOSPITAL CORPORATION, THE
Comparative phenotypic, functional, and molecular analysis of pluripotent stem cells arguably the most significant challenge in stem cell biology today is determining whether human induced pluripotent stem cells (hiPSC) are truly equivalent to human embryonic stem cells (hESC), and thus can serve as a stable, safe, and less controversial resource for basic research and cell replacement therapies. Although the evidence to date suggests that murine ESC and iPSC are functionally interchangeable, the analysis is preliminary and incomplete, especially for human cells, and evidence is accumulating that important molecular differences distinguish the two types of pluripotent stem cells. To answer whether significant functional and molecular differences exist, we have assembled an outstanding cohort of collaborators, each with unique and complementary expertise, to perform a comprehensive phenotypic, functional, and molecular comparison of multiple ESC and iPSC lines using genomic, epigenetic, proteomic, computational, and pathologic analysis. In recent years, the Daley lab has simultaneously pursued derivation of novel hESC from discarded IVF embryos and generation of hiPSC by direct somatic cell reprogramming. Moreover, we have an extensive collection of murine pluripotent stem cells generated by direct reprogramming (miPSC) or isolated from embryos after fertilization (fESC), parthenogenesis (pESC), and somatic cell nuclear transfer (ntESC). This comprehensive set of reagents affords us a unique opportunity to test the hypothesis that iPSC are the functional equivalents of ESC in assays of pluripotency, but that molecular differences persist between the two classes of pluripotent stem cells. We will further test the hypothesis that differences between ESC and iPSC are largely due to residual transgene expression in iPSC, and will resolve once transgenes are removed. However, preliminary data suggests that even transgene-free iPSC are epigenetically distinct from ESC. Thus, an alternative hypothesis is that factor-based reprogramming leaves a residual epigenetic signature of the tissue of origin ("epigenetic memory"), and that the reprogramming process confers unique molecular features on iPSC. In addition to comparing and contrasting ESC and iPSC, our analysis will illuminate the degree of variation among independent clones of ESC and iPSC. Defining the extent of functional similarity, assessing the nature of any molecular differences, and defining biomarkers of the successfully reprogrammed state are key goals of this proposal. Insights gleaned herein will contribute to improved reprogramming methods, thereby facilitating the application of iPSCs to disease research and cell therapies. PUBLIC HEALTH RELEVANCE: Pluripotent stem cells offer tremendous promise as tools for basic biomedical research, disease modeling and drug screening, and provide a means of deriving patient-specific rejection-proof cells that might be used in cell replacement therapies for a large number of genetic, malignant, and degenerative diseases. Techniques for establishing "induced pluripotent stem" or "iPS" cells fulfill the long-sought strategy for generating customized stem cells. If proven equivalent-both functionally and molecularly-to blastocyst-derived human embryonic stem cells, iPS cells will facilitate research, quell contentious public debate, and yield a new modality for tissue repair and regeneration.
Choose a quarter and click "Go."
| AWARD OVERVIEW |
| Award Number |
1RC2HL102815-01 |
Funding Agency |
Department of Health and Human Services |
| Total Award Amount |
$3,432,177 |
Project Location - City |
Boston |
| Award Date |
09/28/2009 |
Project Location - State |
MA |
| Project Status |
Completed |
Project Location - Zip |
02115-5724
|
| Jobs Reported |
0.00 |
Congressional District |
08 |
| Project Location - Country |
US |
|
|
Recipient Information
(Grants)
| Recipient Information (Grants) |
|
Recipient Name
|
CHILDREN'S HOSPITAL CORPORATION, THE |
| Recipient DUNS Number |
076593722
|
| Recipient Address |
300 LONGWOOD AVE |
| Recipient City |
BOSTON |
| Recipient State |
Massachusetts |
| Recipient Zip |
02115-5724 |
| 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 |
Comparative phenotypic, functional, and molecular analysis of ESC and iPSC |
| Project Status |
Completed |
| Final Project Report Submitted |
Yes |
| Project Activities Description |
Hospitals |
| Quarterly Activities/Project Description |
1. Analysis of the methylome of ES and iPS cells (Feinberg, Church, and Daley)—During the grant period we published several papers relevant to this aim:
a. Doi et al, Nat Genetics 2009;
b. Kim et al Nature 2010;
c. Ji et al, Nature 2010;
d. Ooi et al., Epigenetics and Chromatin 2010;
e. Kim et al., Nature Biotech 2011.
2. iPS gene expression profiling
a) Characterization of tissue specific iPS (Daley, Collins, Park); Loh et al, Cell Stem Cell 2010.
b) Characterization of partially reprogrammed and bona fide reprogrammed iPS types (Daley, Collins, Ince); Chan et al., Nature Biotechnology 2009. Additional characterization of the role of Lin28 in converting Type II to Type III cells is underway.
c) Characterization of virally-derived and non virally-derived iPS (Daley, Collins); We collaborated on the development of non-genetic, RNA-based reprogramming (Warren et al, Cell Stem Cell 2010). A paper is under review creating transgene-free lines by Cre-mediated excision of virus.
d) Sequence comparisons of ESC and iPSC (Daley/Church in collaboration with K. Zhang, UCSD); We reported high frequency point mutations in oncogenic pathways in iPSC; Gore et al, Nature, 2011.
3. iPS dynamic gene expression modeling (Daley, Collins); A paper is under preparation and a review has recently appeared (Loh et al, Annu Rev Genomics Hum Genet. 2011).
4. Gene expression variation in human pluripotent stem cells (Daley, Church); We published on use of point mutations to track tissue-specific gene expression variants (Lee at al, PLoS Genetics, 2009).
5. Differences in Linc-RNAs between ES and iPS cells (Daley, Rinn); We published on non-coding RNAs in iPS and ES cells (Loewer et al, Nat Genetics 2010).
6. Proteomic analysis of ES and iPS cells (Marto, Daley, Collins); We have identified a regulatory loop linking the control of alternative splicing to the pluripotency machinery and a paper is currently under review (Lu et al.).
|
| Jobs Created |
0.00 |
| Description of Jobs Created |
Children’s Hospital Boston is the only hospital in Massachusetts committed entirely to the health care of children and offers a comprehensive range of health care services and pioneering knowledge and therapies in accordance with its research mission. CHB is also dedicated to being a caring and responsive community partner and leader in civic and public policy.
Children's Hospital Boston is a major employer and provider of services for the city, state and greater New England region. A recent study on the social and economic impact of CHB on the local level, indicates that the operations of CHB generated $533 million in economic activity and more than $27.7 million in revenue for the City of Boston in 2006. In 2008 CHB provided direct employment for 8,832 residents of the region. This number represents an 8% growth from 2007 in direct employee numbers and reflects the upward trend we would like to continue. Opportunities from the federal stimulus funding will assist in this goal. For this reporting period 0 jobs were created/retained. Project officially ended on 2/29/2012. |
Purchaser Information
(Grants)
| Purchaser Information |
| Contracting Office ID |
Not Reported |
| Contracting Office Name |
Not Available |
| Contracting Office Region |
Not Available |
| TAS Major Program |
75-0871 |
| Award Information |
| Award Date |
09/28/2009 |
| Award Number |
1RC2HL102815-01 |
| 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 |
$3,432,177 |
| Funds Invoiced/Received |
$3,432,138 |
| Expenditure Amount |
$3,432,138 |
| 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 |
E20 - NTEE |
| Activity Description |
Hospitals |
| Sub-Awards Information |
| Sub-awards to Organizations |
6 |
| Sub-award Amounts to Organizations |
$1,864,341 |
| 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 |
633 |
| Total Amount of payments to vendors less than $25,000/award |
$457,530 |
Sub-award 0000323057 - DANA-FARBER CANCER INSTITUTE, INC.
| Sub-Award Amount |
$365,519 |
| Sub-Award Date |
02/02/2010 |
| Sub-Awards Disbursed |
$365,519.00 |
| Project Location - City |
Boston |
| Project Location - State |
MA |
| Project Location - Zip Code |
02115-6013 |
| Project Location - Congressional District |
08 |
| Sub-Recipient DUNS Number |
076580745
|
| Sub-Recipient Address |
450 BROOKLINE AVE STE 30 |
| Sub-Recipient City |
BOSTON |
| Sub-Recipient State |
Massachusetts |
| Sub-Recipient Zip Code |
02115-6013 |
| Sub-Recipient Congressional District |
08 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 323054 - HARVARD COLLEGE, PRESIDENT & FELLOWS OF
| Sub-Award Amount |
$247,882 |
| Sub-Award Date |
11/05/2009 |
| Sub-Awards Disbursed |
$224,927.79 |
| Project Location - City |
Boston |
| Project Location - State |
MA |
| Project Location - Zip Code |
02115-5727 |
| Project Location - Congressional District |
08 |
| Sub-Recipient DUNS Number |
047006379
|
| Sub-Recipient Address |
25 SHATTUCK ST |
| Sub-Recipient City |
BOSTON |
| Sub-Recipient State |
Massachusetts |
| Sub-Recipient Zip Code |
02115-6027 |
| Sub-Recipient Congressional District |
08 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 323053 - HARVARD COLLEGE, PRESIDENT & FELLOWS OF
| Sub-Award Amount |
$261,360 |
| Sub-Award Date |
11/05/2009 |
| Sub-Awards Disbursed |
$153,690.57 |
| Project Location - City |
Boston |
| Project Location - State |
MA |
| Project Location - Zip Code |
02115-5701 |
| Project Location - Congressional District |
08 |
| Sub-Recipient DUNS Number |
082359691
|
| Sub-Recipient Address |
1350 MASS AVE STE 600 |
| Sub-Recipient City |
CAMBRIDGE |
| Sub-Recipient State |
Massachusetts |
| Sub-Recipient Zip Code |
02138-3846 |
| Sub-Recipient Congressional District |
08 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 107167 - JOHNS HOPKINS UNIVERSITY, THE
| Sub-Award Amount |
$506,124 |
| Sub-Award Date |
12/11/2009 |
| Sub-Awards Disbursed |
$505,406.16 |
| Project Location - City |
Baltimore |
| Project Location - State |
MD |
| Project Location - Zip Code |
21218-2680 |
| Project Location - Congressional District |
07 |
| Sub-Recipient DUNS Number |
001910777
|
| Sub-Recipient Address |
3400 N CHARLES ST W400 WYMAN PARK BLDG |
| Sub-Recipient City |
BALTIMORE |
| Sub-Recipient State |
Maryland |
| Sub-Recipient Zip Code |
21218-2680 |
| Sub-Recipient Congressional District |
07 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 0000323970 - TRUSTEES OF BOSTON UNIVERSITY
| Sub-Award Amount |
$295,969 |
| Sub-Award Date |
11/10/2009 |
| Sub-Awards Disbursed |
$295,965.99 |
| Project Location - City |
Boston |
| Project Location - State |
MA |
| Project Location - Zip Code |
02215-1300 |
| Project Location - Congressional District |
08 |
| Sub-Recipient DUNS Number |
049435266
|
| Sub-Recipient Address |
1 SHERBORN ST |
| Sub-Recipient City |
BOSTON |
| Sub-Recipient State |
Massachusetts |
| Sub-Recipient Zip Code |
02215-1390 |
| Sub-Recipient Congressional District |
08 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 0000366542 - UNIVERSITY OF MIAMI
| Sub-Award Amount |
$187,487 |
| Sub-Award Date |
09/30/2010 |
| Sub-Awards Disbursed |
$181,794.00 |
| Project Location - City |
Miami |
| Project Location - State |
FL |
| Project Location - Zip Code |
33136-1012 |
| Project Location - Congressional District |
18 |
| Sub-Recipient DUNS Number |
052780918
|
| Sub-Recipient Address |
1400 NW 10 AVE RM 1007P |
| Sub-Recipient City |
MIAMI |
| Sub-Recipient State |
Florida |
| Sub-Recipient Zip Code |
33136-1002 |
| Sub-Recipient Congressional District |
18 |
Required To Report Top 5
Highly Compensated Officials |
No |
| Location Information |
| Latitude, Longitude |
42º 20' 14",
-71º 6' 15" |
| Congressional District |
08 |
| Address 1 |
|
| Address 2 |
|
| City |
Boston |
| County |
Suffolk |
| State |
MA |
| Zip |
02115-5724 |
|
 |