2021
DOI: 10.1186/s13613-021-00947-w
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Insights from patients screened but not randomised in the HYPERION trial

Abstract: Background Few data are available about outcomes of patients screened for, but not enrolled in, randomised clinical trials. Methods We retrospectively reviewed patients who had non-inclusion criteria for the HYPERION trial comparing 33 °C to 37 °C in patients comatose after cardiac arrest in non-shockable rhythm, due to any cause. A good neurological outcome was defined as a day-90 Cerebral Performance Category score of 1 or 2. … Show more

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Cited by 5 publications
(3 citation statements)
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“…One limitation of our study is that the findings apply only to patients with mild-to-moderate PRS, since major hemodynamic instability defined as a continuous epinephrine or norepinephrine infusion > 1 μg/kg/min was an exclusion criterion: only patients with mild-to-moderate shock were included in our analysis [ 35 ]. Surprisingly, the global prognosis for patients without PRS (9.1%) or with moderate PRS (7.1%) was poorer than for patients with severe PRS (defined as receiving norepinephrine > 1 µg/kg/min, 13.3%)).…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…One limitation of our study is that the findings apply only to patients with mild-to-moderate PRS, since major hemodynamic instability defined as a continuous epinephrine or norepinephrine infusion > 1 μg/kg/min was an exclusion criterion: only patients with mild-to-moderate shock were included in our analysis [ 35 ]. Surprisingly, the global prognosis for patients without PRS (9.1%) or with moderate PRS (7.1%) was poorer than for patients with severe PRS (defined as receiving norepinephrine > 1 µg/kg/min, 13.3%)).…”
Section: Discussionmentioning
confidence: 99%
“…In addition, several origins for shock state can coexist (septic shock related to inhalation pneumonia, cardiogenic shock related to acute coronary occlusion, PRS itself) and complicate interpretation of physiopathology. The prognosis of patients with severe PRS is difficult to assess at ICU admission [ 35 ]. Patients were not randomized according to the presence or absence of PRS.…”
Section: Discussionmentioning
confidence: 99%
“…Although this trial design is well suited for assessing novel therapeutics, the time (often years) and effort required to enroll and monitor patients makes it impractical to conduct trials large enough to identify small but clinically relevant effects that would likely be expected for many therapies targeting AKI. Further, restrictive inclusion and exclusion criteria often result in trial populations that do not represent the broader population of patients who experience AKI, or fail to include groups of patients who might have benefited from the proposed intervention 10 .…”
Section: Overcoming Barriers To Clinical Trials In Akimentioning
confidence: 99%