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Does anti-HPA-1a affect birthweight in Fetal and Neonatal Alloimmune Thrombocytopenia?
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  • Margaret MCKELVY,
  • Srishti TYAGI,
  • Emilie VANDER HAAR,
  • Madhavi LAKKARAJA,
  • Tim TOMY,
  • Stacy CORKE,
  • Thea PALMER,
  • Amihai Rottenstreich,
  • Rick Kapur,
  • Huiying ZHI,
  • Debra NEWMAN,
  • Nina Schatz-Siemers,
  • James Bussel
Margaret MCKELVY
Weill Cornell Medicine
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Srishti TYAGI
Cornell University
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Emilie VANDER HAAR
Weill Cornell Medicine
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Madhavi LAKKARAJA
University of Washington Department of Pediatrics
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Tim TOMY
Hurley Medical Center
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Stacy CORKE
Natibabiesorg
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Thea PALMER
Natibabiesorg
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Amihai Rottenstreich
The Rockefeller University
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Rick Kapur
Amsterdam Universitair Medische Centra
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Huiying ZHI
Versiti Blood Research Institute
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Debra NEWMAN
Versiti Blood Research Institute
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Nina Schatz-Siemers
Weill Cornell Medicine
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James Bussel
Weill Cornell Medicine

Corresponding Author:jbussel@med.cornell.edu

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Abstract

Objective: This study tests the clinical hypothesis that FNAIT secondary to anti-HPA-1a results in smaller newborns, and the corollary hypothesis that antenatal management of FNAIT in HPA-1a-incompatible pregnancies increases birthweight by reducing the effects of anti-HPA-1a. Design: FNAIT-affected siblings, one untreated and one treated for FNAIT, were paired for the purpose of comparing their birthweights. Birthweights of FNAIT-affected and -unaffected pups in a mouse model of HPA-1a-specific-FNAIT were also analyzed. Setting: New York Presbyterian-Weill Cornell Medical Center, New York, NY; Versiti Blood Research Institute, Milwaukee, WI. Population: 270 FNAIT-affected newborns from a randomized clinical trial; responders to a NAITbabies.org; and pups in a mouse model of HPA-1a-specific-FNAIT were evaluated. Methods: Birthweight percentiles of untreated FNAIT-affected neonates were compared to those of published controls and treated FNAIT-affected siblings using one-sample, two-tailed t-tests. Body weights of FNAIT-affected and -unaffected pups in a mouse model of HPA-1a-specific-FNAIT were analyzed similarly. Main Outcome Measures: The difference in birthweight percentile between untreated and treated FNAIT-affected siblings was analyzed. Results: Untreated siblings were not small compared to normal controls. However, treated siblings in both cohorts had significantly higher birthweight percentiles compared to their untreated, affected sibling. FNAIT-affected neonatal pups had lower body weights than FNAIT-unaffected pups. Conclusions: The effect of treatment, especially high dose IVIG believed to “block” FcRn and lower maternal anti-HPA-1a levels, to increase birthweights suggests maternal anti-HPA-1a reduces birthweights. We believe this is mediated by anti-HPA-1a binding to placental syncytiotrophoblasts, resulting in placental inflammation.