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Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia

Transfusion‐dependent thalassaemia (TDT) requires red blood cell concentrates (RBCC) to prevent complications of anaemia, but carries risk of infection. Pathogen reduction of RBCC offers potential to reduce infectious risk. We evaluated the efficacy and safety of pathogen‐reduced (PR) Amustaline‐Glu...

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Autores principales: Aydinok, Yesim, Piga, Antonio, Origa, Raffaella, Mufti, Nina, Erickson, Anna, North, Anne, Waldhaus, Katie, Ernst, Christine, Lin, Jin‐Sying, Huang, Norman, Benjamin, Richard J., Corash, Laurence
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6771954/
https://www.ncbi.nlm.nih.gov/pubmed/31148155
http://dx.doi.org/10.1111/bjh.15963
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author Aydinok, Yesim
Piga, Antonio
Origa, Raffaella
Mufti, Nina
Erickson, Anna
North, Anne
Waldhaus, Katie
Ernst, Christine
Lin, Jin‐Sying
Huang, Norman
Benjamin, Richard J.
Corash, Laurence
author_facet Aydinok, Yesim
Piga, Antonio
Origa, Raffaella
Mufti, Nina
Erickson, Anna
North, Anne
Waldhaus, Katie
Ernst, Christine
Lin, Jin‐Sying
Huang, Norman
Benjamin, Richard J.
Corash, Laurence
author_sort Aydinok, Yesim
collection PubMed
description Transfusion‐dependent thalassaemia (TDT) requires red blood cell concentrates (RBCC) to prevent complications of anaemia, but carries risk of infection. Pathogen reduction of RBCC offers potential to reduce infectious risk. We evaluated the efficacy and safety of pathogen‐reduced (PR) Amustaline‐Glutathione (A‐GSH) RBCC for TDT. Patients were randomized to a blinded 2‐period crossover treatment sequence for six transfusions over 8–10 months with Control and A‐GSH‐RBCC. The efficacy outcome utilized non‐inferiority analysis with 90% power to detect a 15% difference in transfused haemoglobin (Hb), and the safety outcome was the incidence of antibodies to A‐GSH‐PR‐RBCC. By intent to treat (80 patients), 12·5 ± 1·9 RBCC were transfused in each period. Storage durations of A‐GSH and C‐RBCC were similar (8·9 days). Mean A‐GSH‐RBCC transfused Hb (g/kg/day) was not inferior to Control (0·113 ± 0·04 vs. 0·111 ± 0·04, P = 0·373, paired t‐test). The upper bound of the one‐sided 95% confidence interval for the treatment difference from the mixed effects model was 0·005 g/kg/day, within a non‐inferiority margin of 0·017 g/kg/day. A‐GSH‐RBCC mean pre‐transfusion Hb levels declined by 6·0 g/l. No antibodies to A‐GSH‐RBCC were detected, and there were no differences in adverse events. A‐GSH‐RBCCs offer potential to reduce infectious risk in TDT with a tolerable safety profile.
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spelling pubmed-67719542019-10-07 Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia Aydinok, Yesim Piga, Antonio Origa, Raffaella Mufti, Nina Erickson, Anna North, Anne Waldhaus, Katie Ernst, Christine Lin, Jin‐Sying Huang, Norman Benjamin, Richard J. Corash, Laurence Br J Haematol Transfusion Transfusion‐dependent thalassaemia (TDT) requires red blood cell concentrates (RBCC) to prevent complications of anaemia, but carries risk of infection. Pathogen reduction of RBCC offers potential to reduce infectious risk. We evaluated the efficacy and safety of pathogen‐reduced (PR) Amustaline‐Glutathione (A‐GSH) RBCC for TDT. Patients were randomized to a blinded 2‐period crossover treatment sequence for six transfusions over 8–10 months with Control and A‐GSH‐RBCC. The efficacy outcome utilized non‐inferiority analysis with 90% power to detect a 15% difference in transfused haemoglobin (Hb), and the safety outcome was the incidence of antibodies to A‐GSH‐PR‐RBCC. By intent to treat (80 patients), 12·5 ± 1·9 RBCC were transfused in each period. Storage durations of A‐GSH and C‐RBCC were similar (8·9 days). Mean A‐GSH‐RBCC transfused Hb (g/kg/day) was not inferior to Control (0·113 ± 0·04 vs. 0·111 ± 0·04, P = 0·373, paired t‐test). The upper bound of the one‐sided 95% confidence interval for the treatment difference from the mixed effects model was 0·005 g/kg/day, within a non‐inferiority margin of 0·017 g/kg/day. A‐GSH‐RBCC mean pre‐transfusion Hb levels declined by 6·0 g/l. No antibodies to A‐GSH‐RBCC were detected, and there were no differences in adverse events. A‐GSH‐RBCCs offer potential to reduce infectious risk in TDT with a tolerable safety profile. John Wiley and Sons Inc. 2019-05-30 2019-08 /pmc/articles/PMC6771954/ /pubmed/31148155 http://dx.doi.org/10.1111/bjh.15963 Text en © 2019 The Authors. British Journal of Haematology published by British Society for Haematology and John Wiley & Sons Ltd This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Transfusion
Aydinok, Yesim
Piga, Antonio
Origa, Raffaella
Mufti, Nina
Erickson, Anna
North, Anne
Waldhaus, Katie
Ernst, Christine
Lin, Jin‐Sying
Huang, Norman
Benjamin, Richard J.
Corash, Laurence
Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
title Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
title_full Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
title_fullStr Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
title_full_unstemmed Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
title_short Amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
title_sort amustaline‐glutathione pathogen‐reduced red blood cell concentrates for transfusion‐dependent thalassaemia
topic Transfusion
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6771954/
https://www.ncbi.nlm.nih.gov/pubmed/31148155
http://dx.doi.org/10.1111/bjh.15963
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