Hemostatic efficacy of pathogen-inactivated vs untreated platelets: a randomized controlled trial

Meer, Pieter F. van der; Ypma, Paula F.; Geloven, Nan van; Hilten, J. A. van; Wordragen-Vlaswinkel, Rinie J. van; Eissen, Okke; Zwaginga, Jaap Jan; Trus, Michael; Beckers, Erik A.M.; Boekhorst, Peter te; Tinmouth, Alan; Lin, Yulia; Hsia, Cyrus C.; Lee, David; Norris, Philip J.; Goodrich, Raymond P.; Brand, Anneke; Hervig, Tor; Heddle, Nancy M.; Bom, Johanna G. van der; Kerkhoffs, Jean-Louis

doi:10.1182/blood-2018-02-831289

Cited by 62 publications

(58 citation statements)

References 27 publications

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“…This, however, may be explained by the fact that these only use fresh platelets ( 55 , 56 ), while pathogen reduction did not affect platelet internalization directly after treatment, but rather enhanced the storage-mediated internalization. Interestingly, two clinical trials were recently published that may confirm this hypothesis ( 57 , 58 ). Namely, one of these studies stored platelets on average for 1 day and showed a protective effect of pathogen inactivation ( 58 , 59 ), whereas the other trial stored platelets on average for 4 days and did not show any protective effect of pathogen inactivation ( 57 ).…”

Section: Discussionmentioning

confidence: 92%

“…Interestingly, two clinical trials were recently published that may confirm this hypothesis ( 57 , 58 ). Namely, one of these studies stored platelets on average for 1 day and showed a protective effect of pathogen inactivation ( 58 , 59 ), whereas the other trial stored platelets on average for 4 days and did not show any protective effect of pathogen inactivation ( 57 ).…”

Section: Discussionmentioning

confidence: 92%

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Storage-Induced Platelet Apoptosis Is a Potential Risk Factor for Alloimmunization Upon Platelet Transfusion

et al. 2018

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Platelet transfusion can elicit alloimmune responses leading to alloantibody formation against donor-specific polymorphic residues, ultimately resulting in platelet transfusion refractoriness. Universal leukoreduction significantly reduced the frequency of alloimmunization after platelet transfusion, thereby showing the importance of white blood cells (WBCs) in inducing this alloresponse. It is, however, unknown if the residual risk for alloimmunization is caused by WBCs remaining after leukoreduction or if alloimmunization can be induced by platelets themselves. This study investigated the capacity of platelets to induce alloimmunization and identified potential product-related risk factors for alloimmunization. First, internalization of allogeneic platelets by dendritic cells (DCs) was demonstrated by confocal microscopy. Second, after internalization, presentation of platelet-derived peptides was shown by mass spectrometry analysis of human leukocytes antigen (HLA)-DR eluted peptides. Third, platelet-loaded DCs induced platelet-specific CD4 T cell responses. Altogether, this indicates a platelet-specific ability to induce alloimmunization. Therefore, factors enhancing platelet internalization may be identified as risk factor for alloimmunization by platelet concentrates. To investigate if storage of platelets is such a risk factor, internalization of stored platelets was compared with fresh platelets and showed enhanced internalization of stored platelets. Storage-induced apoptosis and accompanied phosphatidylserine exposure seemed to be instrumental for this. Indeed, DCs pre-incubated with apoptotic platelets induced the strongest IFN-γ production by CD4 T cells compared with pre-incubation with untreated or activated platelets. In conclusion, this study shows the capacity of platelets to induce platelet-specific alloimmune responses. Furthermore, storage-induced apoptosis of platelets is identified as potential risk factor for alloimmunization after platelet transfusions.

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Section: Discussionmentioning

confidence: 92%

Section: Discussionmentioning

confidence: 92%

Storage-Induced Platelet Apoptosis Is a Potential Risk Factor for Alloimmunization Upon Platelet Transfusion

et al. 2018

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“…12 Concerns expressed regarding the use of PRPs include the potential need for maintaining a dual inventory of platelets due to supply limitations, decreased platelet count increments (PCIs), 13 risk of human leukocyte antigen (HLA) alloimmunization, 14 and the effect of psoralen on neonatal, pediatric, and obstetric patients. [15][16][17] Even with noninferior hemostatic function in hematology oncology patients, 18,19 decreased PCIs may result in increased platelet utilization and reduced platelet inventory. Increased HLA alloimmunization 14 may make finding suitable platelet products more difficult, an additional challenge for TSPs and clinicians.…”

Section: Pathogen Reduction (Pr)mentioning

confidence: 99%

How do you… decide which platelet bacterial risk mitigation strategy to select for your hospital‐based transfusion service?

Delaney

Flegel

et al. 2020

Transfusion

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The United States Food and Drug Administration Final Guidance for Industry titled, “Bacterial Risk Control Strategies for Blood Collection Establishments and Transfusion Services to Enhance the Safety and Availability of Platelets for Transfusion” provides nine strategies for platelet bacterial risk mitigation. Even if it is assumed all strategies are comparable in terms of safety and efficacy, the decision of which to implement remains challenging. Some additional factors that warrant evaluation before selecting a strategy include the financial impact, process for implementation, logistics upon implementation, institutional acceptance by blood bank staff, administration and clinicians, and effect on platelet availability. To assist with this difficult choice, a panel of transfusion service physicians who have expertise on the topic and have already selected strategies for their transfusion services were recruited to provide varied perspectives. In addition, the use of a decision‐making tool that objectively evaluates defined criteria for assessment of the nine strategies is described.

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“…The CCI at one and 24 h after transfusion is decreased in patients receiving PRT treated products, compared to patients receiving control products. In two recent clinical trials Grade 2 or higher bleeding was the primary endpoint [55,66].…”

Section: Clinical Performancementioning

confidence: 99%

Vitamin B2 and Innovations in Improving Blood Safety

Goodrich¹,

Cardoso²,

Marschner³

2018

B Group Vitamins - Current Uses and Perspectives

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Although transfusion of blood components is becoming increasingly safe, the risk of transmission of known and unknown pathogens persists. The application of vitamin B2 (riboflavin) and UV light to pathogen inactivation has several appealing factors. Riboflavin is a naturally occurring vitamin with a well-known and well-characterized safety profile. This photochemical-based method is effective against clinically relevant pathogens and inactivates leukocytes without significantly compromising the content and the efficacy of whole blood or blood component. This chapter gives an overview of the innovative technology for pathogen inactivation, the Mirasol ® pathogen reduction technology (PRT) System, based on riboflavin and UV light, summarizing the mechanism of action, toxicology profile, pathogen reduction performance and clinical efficacy of the process.

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Hemostatic efficacy of pathogen-inactivated vs untreated platelets: a randomized controlled trial

Cited by 62 publications

References 27 publications

Storage-Induced Platelet Apoptosis Is a Potential Risk Factor for Alloimmunization Upon Platelet Transfusion

Storage-Induced Platelet Apoptosis Is a Potential Risk Factor for Alloimmunization Upon Platelet Transfusion

How do you… decide which platelet bacterial risk mitigation strategy to select for your hospital‐based transfusion service?

Vitamin B2 and Innovations in Improving Blood Safety

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