Literature DB >> 31468506

A journey through infectious risk associated with ruxolitinib.

Emanuela Sant'Antonio1, Massimiliano Bonifacio2, Massimo Breccia3, Elisa Rumi4.   

Abstract

Ruxolitinib has proved to be effective for the treatment of patients with myelofibrosis (either primary or secondary) and polycythaemia vera, and its approval led to a significant change in the current treatment algorithm. Despite its efficacy and beyond its well described haematological toxicity, a peculiar immunosuppressive effect emerged as our clinical experience grew, both within and outside of a clinical trial setting. Definite and negative interactions with multiple pathways of the immune system of patients have been reported so far, involving both adaptive and innate immune responses. These pathophysiological mechanisms may contribute to the increased risk of reactivation of silent infections (e.g., tuberculosis, hepatitis B virus and varicella zoster virus) that have been associated with the drug. Even though such infectious events may be fatal or may lead to significant impairment of organ function, compromising the eligibility of patients for an allotransplant procedure, there are no dedicated guidelines that may help us in assessing and managing the risk of developing serious infections. On this basis, our aim for the present work was to review the current knowledge on the pathophysiological mechanisms through which ruxolitinib may exert its immunosuppressive effect, and to illustrate our personal approach to the management of three peculiar clinical scenarios, for which a risk-based algorithm is suggested.
© 2019 British Society for Haematology and John Wiley & Sons Ltd.

Entities:  

Keywords:  infection; management; myelofibrosis; polycythaemia vera; ruxolitinib

Year:  2019        PMID: 31468506     DOI: 10.1111/bjh.16174

Source DB:  PubMed          Journal:  Br J Haematol        ISSN: 0007-1048            Impact factor:   6.998


  8 in total

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Review 3.  Immune Dysregulation and Infectious Complications in MPN Patients Treated With JAK Inhibitors.

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Review 4.  Impact of JAK Inhibitors in Pediatric Patients with STAT1 Gain of Function (GOF) Mutations-10 Children and Review of the Literature.

Authors:  Olaf Neth; Peter Olbrich; Angela Deyà-Martínez; Jaques G Rivière; Pérsio Roxo-Junior; Jan Ramakers; Markéta Bloomfield; Paloma Guisado Hernandez; Pilar Blanco Lobo; Soraya Regina Abu Jamra; Ana Esteve-Sole; Veronika Kanderova; Ana García-García; Mireia Lopez-Corbeto; Natalia Martinez Pomar; Andrea Martín-Nalda; Laia Alsina
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5.  COVID-19: Considerations about immune suppression and biologicals at the time of SARS-CoV-2 pandemic.

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6.  JAK/STAT pathway inhibition sensitizes CD8 T cells to dexamethasone-induced apoptosis in hyperinflammation.

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7.  Severe COVID-19 in a patient with chronic graft-versus-host disease after hematopoietic stem cell transplant successfully treated with ruxolitinib.

Authors:  Francesco Saraceni; Ilaria Scortechini; Giorgia Mancini; Marianna Mariani; Irene Federici; Mariana Gaetani; Paolo Barbatelli; Maria Luisa Minnucci; Patrizia Bagnarelli; Attilio Olivieri
Journal:  Transpl Infect Dis       Date:  2020-07-14

8.  Tracing the decision-making process for myelofibrosis: diagnosis, stratification, and management of ruxolitinib therapy in real-word practice.

Authors:  Massimo Breccia; Claudia Baratè; Giulia Benevolo; Massimiliano Bonifacio; Elena Maria Elli; Paola Guglielmelli; Margherita Maffioli; Alessandra Malato; Francesco Mendicino; Giuseppe Alberto Palumbo; Novella Pugliese; Elena Rossi; Elisa Rumi; Emanuela Sant'Antonio; Alessandra Ricco; Mario Tiribelli; Francesca Palandri
Journal:  Ann Hematol       Date:  2019-12-12       Impact factor: 3.673

  8 in total

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