Abstract

Maternal RBC alloimmunization, induced by prior pregnancy/delivery or prior transfusion, puts the developing fetus/neonate at risk for anemia and hemolytic disease of the fetus and newborn (HDFN). 1 in 600 infants is at risk for HDFN, with no targeted therapies available to offer alloimmunized pregnant women, and no prophylactic therapies available for non-D antigens. This paucity of targeted therapies is due in part to an understandable reluctance to test innovative therapies on pregnant women or their fetuses. To circumvent this issue, we have developed what we believe is the first animal model of HDFN in which pregnancy/delivery is capable of stimulating maternal alloimmunization and in which these maternal antibodies result in HDFN. The fact that this model involves RBC specific expression of a human antigen highly implicated in HDFN (KEL) adds further to its innovation. As an extension of our R21 to develop and characterize this model, we now propose to utilize this model to protect developing fetuses from existing maternal alloantibodies in a damage control manner, and to prevent primary anti-KEL formation in a prophylactic manner. Central Hypothesis: The dangers of existing or developing maternal anti-RBC alloantibodies to fetuses and newborns can be prevented through active or passive maternal immunomodulatory therapies.
Specific Aim 1 : Investigate strategies to minimize the dangers of existing maternal anti-KEL alloantibodies to developing fetuses and newborns.
Specific Aim 2 : Investigate strategies to prevent primary anti-KEL RBC alloimmunization during pregnancy/delivery.
Specific Aim 3 : Investigate the impact of other (non-KEL) RBC alloantibodies on developing fetuses and newborn. Public Health Significance/Long Term Goals: The development of targeted therapies to minimize the dangers of existing RBC alloantibodies or to prevent primary alloimmunization in women carrying fetuses expressing the cognate RBC antigen would have significant public health significance, through a decrease in fetal and neonatal HDFN morbidity and mortality. Long term goals of this project include translating successful murine innovative therapies to humans, initially in a transfusion setting and ultimately in a pregnancy setting, usin a bench to bedside and back approach.

Public Health Relevance

Maternal RBC alloantibodies may be dangerous to developing fetuses/neonates, affecting 1 in 600 births and leading to short and long term morbidity/mortality due to suppression of erythropoiesis and/or hemolysis. Currently, very few treatment options exist to minimize the dangers of maternal alloantibodies to fetuses, and not a single prophylactic therapy exists to prevent maternal alloimmunization to any RBC antigen besides D. Using what we believe is the first animal model of hemolytic disease of the newborn (HDFN) involving a clinically significant human RBC antigen (KEL), we propose reductionist studies to better understand maternal antibody development and prevention thereof; long term goals of these studies include developing translational therapies to minimize the fetal/neonatal morbidity and mortality currently associated with maternal alloimmunization and HDFN.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL126076-03
Application #
9069975
Study Section
Pregnancy and Neonatology Study Section (PN)
Program Officer
Welniak, Lisbeth A
Project Start
2014-07-15
Project End
2019-06-30
Budget Start
2016-07-01
Budget End
2017-06-30
Support Year
3
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Pathology
Type
Schools of Medicine
DUNS #
043207562
City
New Haven
State
CT
Country
United States
Zip Code

  Publications

Mener, Amanda; Arthur, Connie M; Patel, Seema R et al. (2018) Complement Component 3 Negatively Regulates Antibody Response by Modulation of Red Blood Cell Antigen. Front Immunol 9:676
Gibb, David R; Liu, Jingchun; Santhanakrishnan, Manjula et al. (2017) B cells require Type 1 interferon to produce alloantibodies to transfused KEL-expressing red blood cells in mice. Transfusion 57:2595-2608
Natarajan, Prabitha; Liu, Dong; Patel, Seema R et al. (2017) CD4 Depletion or CD40L Blockade Results in Antigen-Specific Tolerance in a Red Blood Cell Alloimmunization Model. Front Immunol 8:907
Natarajan, P; Santhanakrishnan, M; Tormey, C A et al. (2017) The impact of vaccination on RBC alloimmunization in a murine model. Vox Sang 112:598-600
Gibb, David R; Liu, Jingchun; Natarajan, Prabitha et al. (2017) Type I IFN Is Necessary and Sufficient for Inflammation-Induced Red Blood Cell Alloimmunization in Mice. J Immunol 199:1041-1050
Natarajan, Prabitha; Liu, Jingchun; Santhanakrishnan, Manjula et al. (2017) Bortezomib decreases the magnitude of a primary humoral immune response to transfused red blood cells in a murine model. Transfusion 57:82-92
Santhanakrishnan, M; Tormey, C A; Natarajan, P et al. (2016) Clinically significant anti-KEL RBC alloantibodies are transferred by breast milk in a murine model. Vox Sang 111:79-87
Liu, Jingchun; Santhanakrishnan, Manjula; Natarajan, Prabitha et al. (2016) Antigen modulation as a potential mechanism of anti-KEL immunoprophylaxis in mice. Blood 128:3159-3168
Stowell, Sean R; Arthur, C Maridith; Girard-Pierce, Kathryn R et al. (2015) Anti-KEL sera prevents alloimmunization to transfused KEL RBCs in a murine model. Haematologica 100:e394-7