Your search keyword '"Meola, Gregory"' showing total 10 results

1. Comparing the cardiorespiratory safety of parenteral olanzapine and benzodiazepines to parenteral haloperidol/droperidol and benzodiazepines in emergency department patients.

Author

Bradley, Katherine, Feldman, Elizabeth A., Schrader, Joshua, Meola, Gregory, Miller, Christopher D., Darko, William, and Seabury, Robert

Abstract

This study sought to assess the cardiorespiratory safety of parenteral olanzapine and benzodiazepine combination treatment compared to parenteral droperidol or haloperidol and benzodiazepine combination treatment. This was a retrospective chart review conducted in adult emergency department patients who received intramuscular (IM) or intravenous (IV) droperidol, haloperidol, or olanzapine within one hour of IM or IV benzodiazepine. Patients were stratified into groups based on whether they received either olanzapine in combination with a benzodiazepine (n = 48) or droperidol or haloperidol in combination with a benzodiazepine (n = 48). Patients in each group had a decrease in their systolic blood pressure (SBP) after IM/IV olanzapine and IM/IV droperidol or haloperidol when used in combination with an IM/IV benzodiazepine ((Olanzapine + benzodiazepine (mmHg), median (IQR): Pre-SBP: 132 (117–151) vs. Post-SBP: 117 (99–131), p < 0.01) (Droperidol or haloperidol + benzodiazepine (mmHg), median (IQR): Pre-SBP: 138 (122–149) vs. Post-SBP: 106 (98–127), p < 0.01)). Both groups had similar percent SBP decreases post-combination treatment (Olanzapine + benzodiazepine (15.6 %) vs. Droperidol or haloperidol + benzodiazepine (15.2 %); p = 0.55). We did not observe any statistically significant between group differences for hypotension (Olanzapine + benzodiazepine: 1/48, 2.1 % vs. Droperidol or haloperidol + benzodiazepine: 3/48, 6.3 %; p = 0.62)), escalation in oxygen requirements (Olanzapine + benzodiazepine: 7/48, 14.6 %) vs. Droperidol or haloperidol + benzodiazepine: 5/48, 10.4 %; p = 0.76)), or intubation due to cardiorespiratory depression (Olanzapine + benzodiazepine: 0/0, 0 % vs. Droperidol or haloperidol + benzodiazepine: 0/0, 0 %; p = 1.00)). This study found decreases in SBP after administering parenteral olanzapine and parenteral droperidol or haloperidol in combination with a parenteral benzodiazepine. The percent change in SBP and the frequency of hypotensive episodes post-combination treatment were not different between groups. There were also no differences between groups in need of increased oxygen requirements post-combination treatment or need for intubation due to cardiorespiratory depression. This study suggests parenteral olanzapine in combination with a parenteral benzodiazepine may have comparable cardiorespiratory safety versus parenteral droperidol or haloperidol in combination with a parenteral benzodiazepine when treating agitation in the adult ED. [ABSTRACT FROM AUTHOR]

Published

2025

2. Preparation/administration of push-dose versus continuous infusion epinephrine and phenylephrine: A simulation

Author

Morley, Hannah, primary, Seabury, Robert, additional, Parsels, Katie, additional, Miller, Christopher, additional, Darko, William, additional, Schrader, Joshua, additional, and Meola, Gregory, additional

Published

2023

3. Effect of etomidate on systolic blood pressure in emergency department patients undergoing rapid sequence intubation with high and low shock index.

Author

Amedeo, Valerie, Seabury, Robert, Meola, Gregory, Barbay, Erica, and Feldman, Elizabeth

Published

2024

4. Retrospective Assessment of Desmopressin Effectiveness and Safety in Patients With Antiplatelet-Associated Intracranial Hemorrhage*

Author

Feldman, Elizabeth A., Meola, Gregory, Zyck, Stephanie, Miller, Christopher D., Krishnamurthy, Satish, Cwikla, Gregory M., Darko, William, Jennings, Shane, Sullivan, Ross, and Seabury, Robert

Published

2019

5. Low-Dose Alteplase May Be a Potential Treatment in Some But Not All Submassive Pulmonary Embolism: The Importance of an Abstract Conclusion

Author

Meola, Gregory, primary, Seabury, Robert, additional, and Paolo, William, additional

Published

2020

6. Retrospective assessment of succinylcholine use in acute stroke care: What are the risks?

Author

Fancher, Jenna, primary, Meola, Gregory, additional, Paolo, William, additional, and Seabury, Robert, additional

Published

2018

7. Impact of a Combination Antibiotic Bag on Compliance With Surviving Sepsis Campaign Goals in Emergency Department Patients With Severe Sepsis and Septic Shock

Author

Lorenzo, Michael P., primary, MacConaghy, Lindsay, additional, Miller, Christopher D., additional, Meola, Gregory, additional, Probst, Luke A., additional, Pratt, Brian, additional, Steele, Jeff, additional, and Seabury, Robert W., additional

Published

2017

8. Impact of premix antimicrobial preparation and time to administration in septic patients

Author

Kufel, Wesley D., primary, Seabury, Robert W., additional, Meola, Gregory M., additional, Darko, William, additional, Probst, Luke A., additional, and Miller, Christopher D., additional

Published

2017

9. Impact of a Combination Antibiotic Bag on Compliance With Surviving Sepsis Campaign Goals in Emergency Department Patients With Severe Sepsis and Septic Shock.

Author

Lorenzo, Michael P., MacConaghy, Lindsay, Miller, Christopher D., Meola, Gregory, Probst, Luke A., Pratt, Brian, Steele, Jeff, and Seabury, Robert W.

Published

2018

10. Impact of premix antimicrobial preparation and time to administration in septic patients

Author

Kufel, Wesley D., Seabury, Robert W., Meola, Gregory M., Darko, William, Probst, Luke A., and Miller, Christopher D.

Abstract

ABSTRACTObjectiveStrategies that reduce the time to antimicrobial administration, such as the availability of premix antimicrobials (PMAs) in the emergency department (ED), may better align with the goals of the Surviving Sepsis Campaign and improve outcomes in septic patients. The objective of this study was to evaluate the impact of antimicrobial preparation on time to administration in septic patients located in the emergency department (ED).MethodsThis was a retrospective, single-center, cohort study and adult patients with a diagnosis of sepsis who received at least one initial intravenous (IV) antimicrobial in the ED were included. Time to complete an empiric antimicrobial therapy was defined as the time between prescriber order entry and the infusion initiation time of the final antimicrobial agent of a patient’s antimicrobial regimen. Appropriate, empiric antimicrobial therapy was based on treatment recommendations by nationally accepted guidelines for the specific indication.ResultsThe first antimicrobial was initiated earlier when available as a PMA preparation (median (IQR): premix 25 minutes (16.5-42.3) vs. non-premix 46 minutes (20-102), p=0.027). When comparing complete, empiric antimicrobial regimen administration, there was no difference in time to administration between regimens containing one or more non-premix antimicrobials and regimens containing all PMAs (median (IQR): premix 69 minutes (21-115) vs. non-premix 65 minutes (38.5-133.8); p=0.455).ConclusionsPMA preparations significantly reduced time to administration of the first antimicrobial agent for septic patients treated in the ED, but time to administration of subsequent antimicrobials were not improved.

Published

2018