BRIGHAM AND WOMEN'S HOSPITAL, INC., THE
Transplantation is widely recognized as the treatment of choice for end stage organ failure. While short-term allograft survival has been steadily improving, long-term survival is still not optimal. Most grafts will eventually cease to function, primarily due to chronic allograft rejection. This application is based on two primary hypotheses. The first hypothesis is that T cell recognition of alloantigen, costimulation and subsequent activation plays a critical role in orchestrating the alloimmune response responsible for initiation and progression of chronic allograft rejection. The corollary hypothesis is that inhibiting T cell activation by T cell costimulatory blockade should prevent progression of chronic organ dysfunction following transplantation. The second hypothesis is that humoral immune responses play an important role in promoting chronic rejection and subsequent graft dysfunction. Therefore, targeting B cells and inhibition of further alloantibody production in transplant recipients who develop de novo anti-HLA alloantibodies early after transplantation should prevent the progression of organ dysfunction and improve long-term outcome. The overall goal of this application is to develop novel therapies for prevention and interruption of progression of chronic allograft dysfunction. As required by the CTOT-RFA we will propose to establish a consortium between the Harvard Transplant Centers and the University of California San Francisco Transplant Program to test two different approaches: the first one is a multi-organ approach and the second is an organ-specific one. In the multi-organ protocol we will test the hypothesis that B7 costimulation blockade (with LEA29Y) will block ongoing alloimmune responses and allow withdrawal of calcineurin inhibitors in renal and cardiac transplant recipients leading to prevention of progression of chronic allograft dysfunction and improvement in renal function. In the organ-specific protocol we will test the hypothesis that B cell depletion by anti-CD20 (Rituximab) in renal allograft recipients who develop early de novo anti-HLA alloantibodies will result in inhibition of antibody production, attenuation of humoral rejection and improvement of renal transplant function and pathological changes of chronic allograft nephropathy. All three trials will be accompanied by extensive mechanistic studies involving sensitive and specific assays, including peripheral cellular/humoral assays and intragraft molecular assays for expression patterns of alloimmune activation and effector function markers. The main goal of these studies is to understand the mechanisms of action of B7 blockade and B cell depletion in vivo, and to develop a set of surrogate markers of chronic allograft rejection in organ transplant recipients.
| AWARD OVERVIEW |
| Award Number |
3U01AI063623-05S1 |
Funding Agency |
Department of Health and Human Services |
| Total Award Amount |
$2,144,799 |
Project Location - City |
Boston |
| Award Date |
08/01/2009 |
Project Location - State |
MA |
| Project Status |
Completed |
Project Location - Zip |
02115-0000
|
| Jobs Reported |
1.25 |
Congressional District |
08 |
| Project Location - Country |
US |
|
|
Recipient Information
(Grants)
| Recipient Information (Grants) |
|
Recipient Name
|
BRIGHAM AND WOMEN'S HOSPITAL, INC., THE |
| Recipient DUNS Number |
030811269
|
| Recipient Address |
75 FRANCIS ST |
| Recipient City |
BOSTON |
| Recipient State |
Massachusetts |
| Recipient Zip |
02115-6110 |
| 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 |
Novel Therapies of Chronic Allograft Dysfunction |
| Project Status |
Completed |
| Final Project Report Submitted |
Yes |
| Project Activities Description |
General Medical and Surgical Hospitals |
| Quarterly Activities/Project Description |
Supplemental to Clinical Trials in Organ Transplantation U01 AI63623
Mohamed H. Sayegh, PI
Project Narrative
Scope of the overall project and the anticipated contribution of the requested supplement
The original CTOT05 study is a non-randomized, prospective cohort, multi-center, observational clinical trial in cardiac transplant recipients in which noninvasive immune monitoring by multiple approaches is being tested to assess their usefulness for diagnosis of post transplant graft injury and provide insight into mechanisms of graft injury. The study is collaborative effort between Dr. P Heeger and Dr. MH Sayegh who co-direct the study. The proposed studies have been discussed with Dr. Heeger. The study has an overall goal of enrolling 150 subjects total. As part of the study samples of sera, cells as well as biopsies have been collected at intervals following transplantation. All specimen samples are being stored centrally. A number of mechanistic studies are described in the original CTOT05 study and are currently being carried out. These include monitoring development of HLA and non-HLA antibodies, VGEF expression, gene expression, T cell activation markers, cytokine/chemokine analysis and urinary proteomics. This application is for supplemental funding that will allow us to expand these studies which are not already included in the original proposal.
|
| Jobs Created |
1.25 |
| Description of Jobs Created |
The original CTOT05 study is a non-randomized, prospective cohort, multi-center, observational clinical trial in cardiac transplant recipients in which noninvasive immune monitoring by multiple approaches is being tested to assess their usefulness for diagnosis of post transplant graft injury and provide insight into mechanisms of graft injury. The study is collaborative effort between Dr. P Heeger and Dr. MH Sayegh who co-direct the study. The proposed studies have been discussed with Dr. Heeger. The study has an overall goal of enrolling 150 subjects total. As part of the study samples of sera, cells as well as biopsies have been collected at intervals following transplantation. All specimen samples are being stored centrally. A number of mechanistic studies are described in the original CTOT05 study and are currently being carried out. These include monitoring development of HLA and non-HLA antibodies, VGEF expression, gene expression, T cell activation markers, cytokine/chemokine analysis and urinary proteomics. This application is for supplemental funding that will allow us to expand these studies which are not already included in the original proposal. The studies detailed consist of 4 separate but inter-related projects that are designed to enhance both the parent project as well as provide novel data. Project 1: Th17 and other Cytokine responses in Cardiac Transplant Recipients. (PIs Chandraker, Najafian & Ansari) This project will examine the Th17 response in cardiac transplant patients. Th17 has been shown to be of importance in acute rejection, particularly when the Th1 response is muted by immunosuppression. Paradoxically, however, certain markers more often associated with Tregs appear to be important in the Th17 response.
Project 2: Molecular Signature for hyporesponsiveness in cardiac transplant recipients. (PI Strom) These studies will correlate clinical findings of hypoeresponsiveness and characterize gene profiles in these subjects based on genes of interest derived from tolerant liver and kidney patients.
Project 3: Correlation of Novel Graft Markers with Cardiac Allograft Vasculopathy. (PIs Smith, Stone, Alessandrini & Colvin) Markers of endothelial cell activation, such as pERK, pAurora as well as IDO will be examined and correlated with findings from the other projects outlined in this proposal.
Project 4: Infections in Transplantation. (PI Fishman) Routine monitoring of infections are not part of clinical care of transplant patients. Subclinical infection is underdiagnosed in this population and the effects on rejection are unknown. Subjects will be monitored for development of a variety of infections and the finding correlated with the clinical data as well as the mechanistic studies in the original CTOT05 study as well as in athis proposal. In additional this proposal will look at novel assays for the detection of encapsulated bacteria following transplantation.
Progress Report: Samples from all four of the individual projects have been collected and the assays have been run. For Project 1 cytokines detected from immunophenotyping by flow cytometry has been completed in the subset of samples (34 patients). The data will be compared with ELISPOT studies collected from samples samples from subjects within the study. For project 2 all samples have been collected and tested for molecular signatures of hyporesponsiveness and the dat will be correlated with clinical outcomes from patients within the study. Project 3 is still ongoing as the histology samples have all been collected but not fully analyzed or correlated. In Project 4 the dat shows that it is possible to detect subclinical infection in the samples from subjects in this study.
|
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 |
08/01/2009 |
| Award Number |
3U01AI063623-05S1 |
| 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 |
$2,144,799 |
| Funds Invoiced/Received |
$2,144,799 |
| Expenditure Amount |
$2,144,799 |
| 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 |
622110 |
| Activity Description |
General Medical and Surgical Hospitals |
| Sub-Awards Information |
| Sub-awards to Organizations |
3 |
| Sub-award Amounts to Organizations |
$1,377,661 |
| Sub-Awards to Individuals |
3 |
| Sub-Award Amounts to Individuals |
$1,377,661 |
| 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 |
495 |
| Total Amount of payments to vendors less than $25,000/award |
$239,944 |
Sub-award 104850B - BETH ISRAEL DEACONESS MEDICAL CENTER INC
| Sub-Award Amount |
$332,419 |
| Sub-Award Date |
08/01/2009 |
| Sub-Awards Disbursed |
$332,419.00 |
| Project Location - City |
Boston |
| Project Location - State |
MA |
| Project Location - Zip Code |
02215-5491 |
| Project Location - Congressional District |
08 |
| Sub-Recipient DUNS Number |
071723621
|
| Sub-Recipient Address |
330 BROOKLINE AVE |
| Sub-Recipient City |
BOSTON |
| Sub-Recipient State |
Massachusetts |
| Sub-Recipient Zip Code |
02215-5400 |
| Sub-Recipient Congressional District |
08 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 104850A - MASSACHUSETTS GENERAL HOSPITAL, THE
| Sub-Award Amount |
$727,829 |
| Sub-Award Date |
08/01/2009 |
| Sub-Awards Disbursed |
$727,829.00 |
| Project Location - City |
Boston |
| Project Location - State |
MA |
| Project Location - Zip Code |
02114-2696 |
| Project Location - Congressional District |
09 |
| Sub-Recipient DUNS Number |
073130411
|
| Sub-Recipient Address |
55 FRUIT ST |
| Sub-Recipient City |
BOSTON |
| Sub-Recipient State |
Massachusetts |
| Sub-Recipient Zip Code |
02114-2621 |
| Sub-Recipient Congressional District |
09 |
Required To Report Top 5
Highly Compensated Officials |
No |
Sub-award 104850C - NORTHWESTERN UNIVERSITY
| Sub-Award Amount |
$317,413 |
| Sub-Award Date |
08/21/2009 |
| Sub-Awards Disbursed |
$296,339.29 |
| Project Location - City |
Chicago |
| Project Location - State |
IL |
| Project Location - Zip Code |
60208-0001 |
| Project Location - Congressional District |
09 |
| Sub-Recipient DUNS Number |
005436803
|
| Sub-Recipient Address |
633 CLARK ST |
| Sub-Recipient City |
EVANSTON |
| Sub-Recipient State |
Illinois |
| Sub-Recipient Zip Code |
60208-0001 |
| Sub-Recipient Congressional District |
09 |
Required To Report Top 5
Highly Compensated Officials |
No |
| Location Information |
| Latitude, Longitude |
42º 20' 9",
-71º 6' 26" |
| Congressional District |
08 |
| Address 1 |
75 Francis Street |
| Address 2 |
|
| City |
Boston |
| County |
Suffolk |
| State |
MA |
| Zip |
02115-0000 |
|
 |