Cynthia Schall
University of Michigan
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Publication
Featured researches published by Cynthia Schall.
Journal of Heart and Lung Transplantation | 2009
Jeremy Yang; Cynthia Schall; Doug Smith; Lisa Kreuser; Mary Zamberlan; Karen King; Robert J. Gajarski
BACKGROUND HLA sensitization rates in children on extracorporeal membrane oxygenation (ECMO) or ventricular assist devices (VADs) are unknown. In addition, panel-reactive antibody (PRA) assessment is increasingly being performed by Luminex, whose role in comparison to other conventional methods is unclear. We investigated HLA sensitization of mechanically supported children using established PRA methods and then retested stored serum using Luminex to assess its impact on initial PRA results and post-heart transplant (post-HTx) outcomes. METHODS Data on 22 pre-HTx ECMO or VAD patients (0 to 18 years of age) included: age; duration of mechanical support; use of homograft; red cell transfusion volume; PRAs; and outcome. Comparative data were collected from 10 non-supported, age-matched controls. RESULTS Median age of the 13 ECMO and 9 VAD patients was 1.4 and 192 months (p < 0.001), respectively. Six (27%) device patients and 4 (40%) controls had baseline PRAs >10% (p = 0.7). No ECMO but 6 VAD patients were sensitized after 50 +/- 51 days of support (p = 0.02). Compared with ECMO, VAD patients had higher Class I PRAs according to enzyme-linked immunoassay (p = 0.03). VAD patients had higher final vs initial PRAs for Class I (p = 0.05) and II (p = 0.04) antigens. HLA sensitization was independent of transfusion volume. Only complement-dependent cytotoxicity (CDC) Class I PRAs were different from their respective Luminex values (p = 0.03). Four HTx patients with initially low PRAs but elevated post hoc Luminex assays had no rejection at 3.8 +/- 1.6 years post-HTx. CONCLUSIONS Infants supported with ECMO are at low risk for HLA sensitization. Because it provides full antibody specificity disclosure, Luminex complements more conventional PRA assays by quantitatively identifying potential donor-specific antibodies, which should facilitate the virtual crossmatch process, thereby minimizing post-HTx humoral rejection risk.
Human Immunology | 2005
Cynthia Schall; L. Klingman; Daniel J. Cook; Riccardo Valdez
Human Immunology | 2017
Gregory Simmons; Timothy Williams; Maria E. Ramirez; Debra Schauss; Cynthia Schall; Omar Moussa
F1000Research | 2014
Mia Kost; Paraskevi Vogiatzi; Timothy Williams; Bradley Christensen; Nell Field; Judith Knakiewicz; Toan Ngo; Andrea Parkinson; Gregory Simmons; Thomas Franks; Debra Schauss; Judy Wysocki; Cynthia Schall; Daniel S. Ramon
Human Immunology | 2012
Timothy Williams; Cynthia Schall; Nell Field; Andrea Parkinson; Debra Schauss; Judy Knakiewicz; Judy Wysocki; Thomas Franks; Daniel S. Ramon
Human Immunology | 2011
Robert Bresler; Judith C. Knakewicz; Judith M. Wysocki; Gregory S. Stempfle; Kamal Abuarquob; Cynthia Schall; Daniel S. Ramon
Human Immunology | 2010
Debra Dudeck; Cynthia Schall; Millie Samaniego; Randy Sung; Jeff Punch; Jerry C. Rosenberg; A. Bradley Eisenbrey; Malek Kamoun
Human Immunology | 2009
Cynthia Schall; Malek Kamoun; Debra Schauss; Judith Knakiewicz; M. Zamberlan; Robert J. Gajarski
Journal of Heart and Lung Transplantation | 2008
James J. Yang; Cynthia Schall; Doug Smith; L. Kreuser; M. Zamberlan; Karen King; Robert J. Gajarski
Human Immunology | 2006
Cynthia Schall; Debra Dudeck; James R. Baker; L. Klingman; Daniel J. Cook; Riccardo Valdez