c0rfv16p

Property	Value
?:abstract	BACKGROUND: High levels of serum interleukin-6 (IL-6) correlate with disease severity in COVID-19. We hypothesized that tocilizumab (a recombinant humanized anti-IL-6 receptor) could improve outcomes in selected patients with severe worsening COVID-19 pneumonia and high inflammatory parameters. METHODS: The TOCICOVID study included a prospective cohort of patients aged 16–80 years with severe (requiring > 6 L/min of oxygen therapy to obtain Sp02 > 94%) rapidly deteriorating (increase by ≥ 3 L/min of oxygen flow within the previous 12 h) COVID-19 pneumonia with ≥ 5 days of symptoms and C-reactive protein levels > 40 mg/L. They entered a compassionate use program of treatment with intravenous tocilizumab (8 mg/kg with a maximum of 800 mg per infusion; and if needed a second infusion 24 to 72 h later). A control group was retrospectively selected with the same inclusion criteria. Outcomes were assessed at D28 using inverse probability of treatment weighted (IPTW) methodology. RESULTS: Among the 96 patients included (81% male, mean (SD) age: 60 (12.5) years), underlying conditions, baseline disease severity, and concomitant medications were broadly similar between the tocilizumab (n = 49) and the control (n = 47) groups. In the IPTW analysis, treatment with tocilizumab was associated with a reduced need for overall ventilatory support (49 vs. 89%, wHR: 0.39 [0.25–0.56]; p < 0.001). Albeit lacking statistical significance, there was a substantial trend towards a reduction of mechanical ventilation (31% vs. 45%; wHR: 0.58 [0.36–0.94]; p = 0.026). However, tocilizumab did not improve overall survival (wHR = 0.68 [0.31–1.748], p = 0.338). Among the 85 (89%) patients still alive at D28, patients treated with tocilizumab had a higher rate of oxygen withdrawal (82% vs. 73.5%, wHR = 1.66 [1.17–2.37], p = 0.005), with a shorter delay before being weaned of oxygen therapy (mean 11 vs. 16 days; p < 0.001). At D28, the rate of patients discharged from hospital was higher in the tocilizumab group (70% vs. 40%, wHR = 1.82 [1.22–2.75]; p = 0.003). The levels of CRP and fibrinogen post therapy (p < 0.001 for both variables) were significantly lower in the tocilizumab group (interaction test, mixed model). Rates of neutropenia (35% vs. 0%; p < 0.001) were higher in the tocilizumab group, yet rates of infections (22% vs. 38%, p = 0.089) including ventilator-acquired pneumonia (8% vs. 26%, p = 0.022) were higher in the control group. CONCLUSION: These data could be helpful for the design of future trials aiming to counter COVID-19-induced inflammation, especially before patients require admission to the intensive care unit. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s10875-020-00911-6.
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?:creator	<https://research.tib.eu/covid-19/entity/Roumier%2C_Mathilde%3B_Paule%2C_Romain%3B_Vall%C3%A9e%2C_Alexandre%3B_Rohmer%2C_Julien%3B_Ballester%2C_Marie%3B_Brun%2C_Anne-Laure%3B_Cerf%2C_Charles%3B_Chabi%2C_Marie-Laure%3B_Chinet%2C_Thierry%3B_Colombier%2C_Marie-Alice%3B_Farfour%2C_Eric%3B_Fourn%2C_Erwan%3B_G%C3%A9ri%2C_Guillaume%3B_Khau%2C_David%3B_Marroun%2C_Ibrahim%3B_Ponsoye%2C_Matthieu%3B_Roux%2C_Antoine%3B_Salvator%2C_H%C3%A9l%C3%A8ne%3B_Schoindre%2C_Yoland%3B_Si_Larbi%2C_Anne-Ga%C3%ABlle%3B_Tch%C3%A9rakian%2C_Colas%3B_Vasse%2C_Marc%3B_Verrat%2C_Anne%3B_Zuber%2C_Benjamin%3B_Couderc%2C_Louis-Jean%3B_Kahn%2C_Jean-Emmanuel%3B_Groh%2C_Matthieu%3B_Ackermann%2C_F%C3%A9lix>
?:doi	<https://research.tib.eu/covid-19/entity/10.1007/s10875-020-00911-6>
?:doi	10.1007/s10875-020-00911-6
?:journal	J_Clin_Immunol
?:license	no-cc
?:pdf_json_files	document_parses/pdf_json/9473656895991edc552fe9eb336884e3a489c84e.json
?:pmc_json_files	document_parses/pmc_json/PMC7666405.xml.json
?:pmcid	<https://research.tib.eu/covid-19/entity/PMC7666405>
?:pmid	<https://research.tib.eu/covid-19/entity/33188624.0>
?:pmid	33188624.0
?:publication_isRelatedTo_Disease	<https://research.tib.eu/covid-19/entity/COVID-19>
is ?:relation_isRelatedTo_publication of	<https://research.tib.eu/covid-19/entity/c0rfv16p_HAS_C0021760_ASSOCIATED_WITH_C5203670> <https://research.tib.eu/covid-19/entity/c0rfv16p_HAS_C1609165_TREATS_C5244027> <https://research.tib.eu/covid-19/entity/c0rfv16p_HAS_C5203670_CAUSES_C0021368>
?:sha_id	<https://research.tib.eu/covid-19/entity/9473656895991edc552fe9eb336884e3a489c84e>
?:source	Medline; PMC
?:title	Tocilizumab for Severe Worsening COVID-19 Pneumonia: a Propensity Score Analysis
?:type	<https://research.tib.eu/covid-19/vocab/Publication>
?:year	2020-11-14

Property

Value

?:abstract

BACKGROUND: High levels of serum interleukin-6 (IL-6) correlate with disease severity in COVID-19. We hypothesized that tocilizumab (a recombinant humanized anti-IL-6 receptor) could improve outcomes in selected patients with severe worsening COVID-19 pneumonia and high inflammatory parameters. METHODS: The TOCICOVID study included a prospective cohort of patients aged 16–80 years with severe (requiring > 6 L/min of oxygen therapy to obtain Sp02 > 94%) rapidly deteriorating (increase by ≥ 3 L/min of oxygen flow within the previous 12 h) COVID-19 pneumonia with ≥ 5 days of symptoms and C-reactive protein levels > 40 mg/L. They entered a compassionate use program of treatment with intravenous tocilizumab (8 mg/kg with a maximum of 800 mg per infusion; and if needed a second infusion 24 to 72 h later). A control group was retrospectively selected with the same inclusion criteria. Outcomes were assessed at D28 using inverse probability of treatment weighted (IPTW) methodology. RESULTS: Among the 96 patients included (81% male, mean (SD) age: 60 (12.5) years), underlying conditions, baseline disease severity, and concomitant medications were broadly similar between the tocilizumab (n = 49) and the control (n = 47) groups. In the IPTW analysis, treatment with tocilizumab was associated with a reduced need for overall ventilatory support (49 vs. 89%, wHR: 0.39 [0.25–0.56]; p < 0.001). Albeit lacking statistical significance, there was a substantial trend towards a reduction of mechanical ventilation (31% vs. 45%; wHR: 0.58 [0.36–0.94]; p = 0.026). However, tocilizumab did not improve overall survival (wHR = 0.68 [0.31–1.748], p = 0.338). Among the 85 (89%) patients still alive at D28, patients treated with tocilizumab had a higher rate of oxygen withdrawal (82% vs. 73.5%, wHR = 1.66 [1.17–2.37], p = 0.005), with a shorter delay before being weaned of oxygen therapy (mean 11 vs. 16 days; p < 0.001). At D28, the rate of patients discharged from hospital was higher in the tocilizumab group (70% vs. 40%, wHR = 1.82 [1.22–2.75]; p = 0.003). The levels of CRP and fibrinogen post therapy (p < 0.001 for both variables) were significantly lower in the tocilizumab group (interaction test, mixed model). Rates of neutropenia (35% vs. 0%; p < 0.001) were higher in the tocilizumab group, yet rates of infections (22% vs. 38%, p = 0.089) including ventilator-acquired pneumonia (8% vs. 26%, p = 0.022) were higher in the control group. CONCLUSION: These data could be helpful for the design of future trials aiming to counter COVID-19-induced inflammation, especially before patients require admission to the intensive care unit. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s10875-020-00911-6.

is ?:annotates of