Philippa C. May scite author profile

Background In this study, we aimed to evaluate the effects of tocilizumab in adult patients admitted to hospital with COVID-19 with both hypoxia and systemic inflammation. Methods This randomised, controlled, open-label, platform trial (Randomised Evaluation of COVID-19 Therapy [RECOVERY]), is assessing several possible treatments in patients hospitalised with COVID-19 in the UK. Those trial participants with hypoxia (oxygen saturation <92% on air or requiring oxygen therapy) and evidence of systemic inflammation (C-reactive protein ≥75 mg/L) were eligible for random assignment in a 1:1 ratio to usual standard of care alone versus usual standard of care plus tocilizumab at a dose of 400 mg–800 mg (depending on weight) given intravenously. A second dose could be given 12–24 h later if the patient's condition had not improved. The primary outcome was 28-day mortality, assessed in the intention-to-treat population. The trial is registered with ISRCTN (50189673) and ClinicalTrials.gov ( NCT04381936 ). Findings Between April 23, 2020, and Jan 24, 2021, 4116 adults of 21 550 patients enrolled into the RECOVERY trial were included in the assessment of tocilizumab, including 3385 (82%) patients receiving systemic corticosteroids. Overall, 621 (31%) of the 2022 patients allocated tocilizumab and 729 (35%) of the 2094 patients allocated to usual care died within 28 days (rate ratio 0·85; 95% CI 0·76–0·94; p=0·0028). Consistent results were seen in all prespecified subgroups of patients, including those receiving systemic corticosteroids. Patients allocated to tocilizumab were more likely to be discharged from hospital within 28 days (57% vs 50%; rate ratio 1·22; 1·12–1·33; p<0·0001). Among those not receiving invasive mechanical ventilation at baseline, patients allocated tocilizumab were less likely to reach the composite endpoint of invasive mechanical ventilation or death (35% vs 42%; risk ratio 0·84; 95% CI 0·77–0·92; p<0·0001). Interpretation In hospitalised COVID-19 patients with hypoxia and systemic inflammation, tocilizumab improved survival and other clinical outcomes. These benefits were seen regardless of the amount of respiratory support and were additional to the benefits of systemic corticosteroids. Funding UK Research and Innovation (Medical Research Council) and National Institute of Health Research.

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PP2A-activating drugs selectively eradicate TKI-resistant chronic myeloid leukemic stem cells

Neviani

et al. 2013

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Clinical drug resistance linked to interconvertible phenotypic and functional states of tumor-propagating cells in multiple myeloma

et al. 2013

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IntroductionMultiple myeloma (MM) is an incurable plasma cell (PC) malignancy of the bone marrow (BM). Although acquired genetic events and the tumor microenvironment are well-established regulators of myeloma cell survival and proliferation pathways, the identity and functional properties of the myeloma-propagating cells have been a matter of controversy. 1,2 The terminal differentiation of normal mature B lymphocytes to immunoglobulin (Ig)-secreting PCs entails conversion of antigennaive to antigen-experienced B cells in the germinal center of secondary lymphoid organs and their subsequent differentiation to either memory B cells or PCs. 3,4 Each stage of B-cell differentiation can be defined by surface markers with naive and memory B cells expressing CD19 and terminally differentiated normal and malignant PCs, but not B cells, expressing CD138 (Syndecan-1). 5,6 Given this linear B-cell lineage developmental process, it was suggested that myeloma cell growth is sustained by a minority of cells more immature than the PC. This hypothesis is supported by the presence of CD19 ϩ CD138 Ϫ clonotypic B cells (ie, cells sharing the same Ig heavy chain [IgH] complementarity region 3 [CDR3] sequence with the myeloma PCs) in peripheral blood (PB) and BM of patients with MM. 7-10 Indeed, because CD138 Ϫ but not CD138 ϩ PCs were found to lead to myeloma engraftment in NOD/SCID mice, it was proposed that CD138 Ϫ cells were the principal myeloma-propagating or "myeloma stem" cells [11][12][13][14] Earlier studies, For personal use only. on May 9, 2018. by guest www.bloodjournal.org From though, using a huSCID mouse model, had concluded that mature PCs (defined as CD38 hi CD45 Ϫ ), and not the CD19 ϩ B-cell fraction, contained the entire myeloma-propagating activity, 15 whereas more recently, CD19 Ϫ CD138 Ϫ as well as CD138 ϩ cells engrafted SCID-rab mice with myeloma. 16 Furthermore, whereas earlier studies reported that the myeloma side population is enriched in clonogenic activity and identifies with CD138 Ϫ but not CD138 ϩ myeloma cells, 13 recent evidence shows that both CD138 ϩ and CD138 Ϫ cells are included in the highly clonogenic myeloma side population. 17 Whether these discrepancies result from different animal models and phenotypic definitions of PC is not clear. Here, through a detailed phenotypic and genetic analysis of primary human myeloma cells and a prospective, dynamic ex vivo and in vivo study of the constituents of the myeloma cellular architecture, we show that a phenotypic and functional interconvertible state between CD138 ϩ and CD138 Ϫ cells underpins myelomapropagating activity and clinical drug resistance. Methods Patient and normal donor BM and PB samplesPatient BM and PB samples were obtained after written informed consent and appropriate institutional ethics committee approval. Patient characteristics are shown in supplemental Table 1 (available on the Blood Web site; see the Supplemental Materials link at the top of the online article). Diagnosis, remission, and relapse of MM were defined accordi...

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Philippa C. May

Tocilizumab in patients admitted to hospital with COVID-19 (RECOVERY): a randomised, controlled, open-label, platform trial

PP2A-activating drugs selectively eradicate TKI-resistant chronic myeloid leukemic stem cells

Clinical drug resistance linked to interconvertible phenotypic and functional states of tumor-propagating cells in multiple myeloma

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