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Volume 17 Issue 8, August 2020

In this issue, read about alternative splicing in cancer, the biology of allogeneic HSCT, treatment-free remission in patients with CML, and treatment of immune-related adverse events.

Image of a primary human invasive ductal carcinoma tissue section stained for immune cells supplied by Ms Sayali Onkar, University of Pittsburgh School of Medicine, and Dr. Marion Joy, National Surgical Adjuvant Breast and Bowel Project.

Research Highlights

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News & Views

  • Bacteria within tumours affect progression and response to therapy; in addition, bacterial DNA can be detected in cell-free plasma. Herein, we discuss evidence showing that intratumoural bacteria are characteristic for each tumour type, and that detection of cell-free bacterial DNA in blood could provide an accurate and non-invasive test for cancer diagnosis.

    • Amiran Dzutsev
    • Giorgio Trinchieri
    News & Views
  • Mature results of the PROfound study demonstrate that the poly(ADP-ribose) polymerase (PARP) inhibitor olaparib prolongs progression-free survival compared with second-generation hormonal therapies in men with metastatic castration-resistant prostate cancer harbouring BRCA1, BRCA2 or ATM mutations. However, a closer look at the efficacy of olaparib on a gene-by-gene basis suggests that its activity is most pronounced in BRCA2-mutant prostate cancers and might not be equally active in all homologous recombination repair-deficient cancers.

    • Emmanuel S. Antonarakis
    News & Views
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Reviews

  • Alternative splicing enables the regulated generation of multiple mRNA and protein products from a single gene. This Review outlines the splicing process and its alterations in cancer before highlighting related opportunities for the development of innovative therapeutic approaches.

    • Sophie C. Bonnal
    • Irene López-Oreja
    • Juan Valcárcel
    Review Article
  • Haematopoietic stem cell transplantation (HSCT) is a potentially curative treatment for several haematological malignancies. Improvements in HSCT methodologies have considerably reduced treatment-related morbidity and mortality, thus broadening eligibility and placing increased emphasis on the prevention of disease relapse. In this Review, the authors discuss approaches to dissecting the biology of HSCT and exploiting the biological insights to enhance the graft-versus-tumour response, in particular with adoptive cell therapies and other immune-directed therapies, whilst minimizing graft-versus-host disease.

    • Bruce R. Blazar
    • Geoffrey R. Hill
    • William J. Murphy
    Review Article
  • International treatment guidelines for chronic myeloid leukaemia incorporate recommendations for attempting discontinuation of treatment with tyrosine-kinase inhibitors (TKIs) with the aim of a treatment-free remission (TFR). The authors of this Review discuss how results of clinical studies of TFR can guide routine practice, address the development of predictors of outcome after TKI discontinuation and present strategies that warrant further consideration to enable more patients to enter TFR.

    • David M. Ross
    • Timothy P. Hughes
    Review Article
  • The treatment of immune-related adverse events (irAEs) in patients receiving immune checkpoint inhibitors has mostly been based on adapting therapeutic approaches used in the management of primary autoimmune diseases. The authors of this Review provide an overview of the different cellular and soluble immune factors involved in the pathogenesis of irAEs in order to help clinicians deliver personalized immunopathologically guided treatment to manage these adverse events.

    • Khashayar Esfahani
    • Arielle Elkrief
    • Leonard Calabrese
    Review Article
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Correspondence

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