Solid organ transplantation is currently the treatment of choice for children with a variety of end-stage organ diseases. The success of clinical transplantation is dependent on the use of potent immunosuppressive drugs to prevent rejection of the allograft. However, chronic immunosuppression is linked to a number of serious side effects in children including an increased risk of infection and de novo malignancies. Post-transplant lymphoproliferative disorder (PTLD) is the most common malignancy in this population, occurring in 10% of pediatric heart, 1-3% of kidney, 1-3% of liver, and 10-30% of small bowel transplant recipients. PTLD describes a spectrum of abnormal B cell lymphoproliferations associated with Epstein-Barr Virus (EBV) infection, the most serious of which manifest as frank lymphoma. As the risk of developing PTLD is greater in patients who are EBV seronegative at the time of transplant, infants and children are at particular risk. Currently, there is no EBV vaccine available;reduction in immunosuppression and antiviral therapy are used as the first line of treatment. However, there are major gaps in our understanding of the immune response to EBV infection in the immunosuppressed patient and no clear evidence that current therapies are effective. Advances in this field are limited by the absence of proven biomarkers to reliably diagnose EBV-associated cancers and to follow those who are at highest risk. We hypothesize that unique molecular and functional changes in the EBV genome, the infected B cells, and the responsive T cells occur in transplant recipient children with EBV disease and that these changes can be utilized as novel biomarkers associated with detection and prognosis of EBV-positive PTLD. We have developed compelling preliminary data suggesting that the attainment of such biomarkers may be within reach. In this observational study, coupled with a strong mechanistic component, we bring together 5 leading pediatric programs in heart, liver and small intestinal transplantation to identify biomarkers of EBV disease and its progression to PTLD. To test this hypothesis we propose the following specific aims:
Aim 1 : Assess gain of function mutations in the EBV protein LMP1 as a biomarker for PTLD risk.
Aim 2 : Assess the emergence of pathogenic B cell clonotypes using high-throughput V(D)J sequencing as a biomarker for emergence of pre-clinical PTLD. Our goal is the development of a biomarker that would identify patients at risk for PTLD or those in the very early stages of the disease, which will represent a major advance in pediatric solid organ transplantation.

Public Health Relevance

Solid organ transplantation is an important therapeutic option for children with a variety of end stage diseases. However, the same immunosuppressive medications that are required to prevent the child's immune system from attacking and rejecting the transplanted organ, can predispose children to developing a very serious cancer that is linked to the Epstein Barr virus (EBV). Diagnosis and effective treatment of the EBV-associated cancer is hampered by our inability to determine which children are at risk of developing these cancers and to detect the cancer at an early stage. In this proposal we plan to test new biomarkers in the blood of children that will tell us very early on if the child is at risk of developing the EBV-associated cancer or if the cancer is present. These studies provide new opportunities for detection, diagnosis, and treatment of children with EBV- associated post-transplant cancer.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project--Cooperative Agreements (U01)
Project #
1U01AI104342-01
Application #
8466656
Study Section
Special Emphasis Panel (ZAI1-JTS-I (J1))
Program Officer
Odim, Jonah
Project Start
2013-02-01
Project End
2018-01-31
Budget Start
2013-02-01
Budget End
2014-01-31
Support Year
1
Fiscal Year
2013
Total Cost
$1,363,549
Indirect Cost
$459,373
Name
Stanford University
Department
Surgery
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305
Kaul, Vandana; Weinberg, Kenneth I; Boyd, Scott D et al. (2017) Dynamics of Viral and Host Immune Cell MicroRNA Expression during Acute Infectious Mononucleosis. Front Microbiol 8:2666
Martinez, Olivia M; Krams, Sheri M (2017) The Immune Response to Epstein Barr Virus and Implications for Posttransplant Lymphoproliferative Disorder. Transplantation 101:2009-2016
Krams, S M; Schaffert, S; Lau, A H et al. (2017) Applying Mass Cytometry to the Analysis of Lymphoid Populations in Transplantation. Am J Transplant 17:1992-1999
Sang, Adam X; Harris-Arnold, Aleishia; Kambham, Neeraja et al. (2016) Epstein-Barr virus-associated lymphoepithelial carcinoma after pediatric liver transplant. Liver Transpl 22:849-53
Lau, Audrey H; Vitalone, Matthew J; Haas, Kelly et al. (2016) Mass cytometry reveals a distinct immunoprofile of operational tolerance in pediatric liver transplantation. Pediatr Transplant 20:1072-1080
Boyd, Scott D; Crowe Jr, James E (2016) Deep sequencing and human antibody repertoire analysis. Curr Opin Immunol 40:103-9
Ellebedy, Ali H; Jackson, Katherine J L; Kissick, Haydn T et al. (2016) Defining antigen-specific plasmablast and memory B cell subsets in human blood after viral infection or vaccination. Nat Immunol 17:1226-34
Yang, Christine H; Gombar, Saurabh; Twist, Clare J et al. (2016) Plasmacytic posttransplant lymphoproliferative disorder with hyperviscosity syndrome in a child after liver transplant. Hepatology 64:2250-2252