Study setting {9}
The study will be conducted in the emergency department and intensive care unit (ICU) department of Peking Union Medical College Hospital (PUMCH), a Grade III Level A hospital in China.
Eligibility criteria {10}
The detailed inclusion and exclusion criteria are outlined in Table 1. Briefly, patients with newly onset of acute alcoholic or hyperlipidemia AP and evidence of organ failure will be included. Patients that have contraindication to neostigmine methylsulfate injection or other severe diseases will be excluded.
Table 1. Eligibility criteria
Inclusion criteria
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Exclusion criteria
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- Ageing between 18 and 75
- Diagnosed with alcoholic or hyperlipidemia acute pancreatitis
- Evidence of organ failure (according to Marshall scoring system)
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- Allergic to neostigmine methylsulfate injection
- Contradiction to neostigmine methylsulfate injection
- Epilepsy
- Angina, arrhythmia, Ventricular tachycardia, Sinus bradycardia,
- Mechanical intestinal obstruction, urethra tract obstruction, asthma
- Uncontrolled hypotension, elevated vagus nerve tone.
- Pregnancy
- Uncontrolled hypertension and severe cardiocerebrovascular disease
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Who will take informed consent? {26a}
Informed consent will be obtained by a member of study team.
For any AP patients who visit the emergency department of PUMCH and meets the inclusion and exclusion criteria, he will be approached to participate in the study by one of the investigators from the study team. The investigator will be responsible for providing each patient with an informed consent form (ICF) about the study’s purpose and procedures, foreseeable benefits and potential risks of participation, compensation for any potential harms, data protection procedures and option to withdraw from the study at any time and without any given reason, which should be read by the patient. The investigator will answer any questions the patient may have, and both the patient and investigator will sign the ICF to indicate the patient’s full understanding of the protocol. Written informed consent must be obtained for all participants prior to any intervention.
Additional consent provisions for collection and use of participant data and biological specimens {26b}
Not applicable
Interventions
Explanation for the choice of comparators {6b}
The dose of neostigmine used in this trial (0.5mg twice a day) has been chosen based on the guidance from FDA. 1ml of saline will be used as placebo, which will be taken identically.
Intervention description {11a}
Participants will be randomized in a 1:1 ratio via envelope randomization. The study will be blinded to participants. Neostigmine Methylsulfate Injection and the saline are identical visually.
For experiment group, 0.5mg/1ml of Neostigmine Methylsulfate Injection will be injected intramuscularly at deltoideus triangularis twice a day right after the enrollment. For control group, 1ml of 0.9% NS will be injected intramuscularly at deltoideus triangularis twice a day.
Apart from intervention, other treatment of AP will be performed according to American Gastroenterological Association Institute Guideline31.
Criteria for discontinuing or modifying allocated interventions {11b}
Adverse events determined by clinical doctors will be reported to the study team and IRB. The study team will determine whether the event is likely to be due to intervention and whether to discontinue the study medication. The IRB will review the event routinely and determine whether it is safe to continue the study.
Strategies to improve adherence to interventions {11c}
All participants will be informed of the study procedures, as well as potential benefits and risks to make them fully understand the significance of their involvement in the study. The study team will check the nursing document of each participant routinely to determine that the participants are taking intervention properly.
Relevant concomitant care permitted or prohibited during the trial {11d}
There will be no restrictions regarding concomitant care during the trial.
Provisions for post-trial care {30}
Not applicable. Study participants will exit the study after discharging from hospital. There will be no further follow-up.
Outcomes {12}
Primary outcome
The effect of neostigmine on gastrointestinal motility will be assessed using time span from onset of disease to the first time of spontaneous defection (defined as at least 1 hour apart from enema). The defection times will be documented by clinical doctors and reported to study team for documentation.
Secondary endpoint
- the proportion of adverse events and serious adverse events identified in both groups
- Intra-abdominal pressure, measured indirect using bladder pressure32 every day after enrollment.
- Borborygmus, measured every day by member of study team.
- Occurrence of abdominal infection, based on the diagnosis when discharging.
- Length of ICU stay, documented based on hospital information system.
- Length of hospital stay, documented based on hospital information system.
- Total cost in hospital, documented based on hospital information system.
Participant timeline {13}
The participant timeline is presented in table 2.
Sample size {14}
This is a randomized controlled trial. The bilateral significance level is 5% with an assurance of 90%. We estimate the standard deviation is 36 hours and the mean difference is 36 hours. In the case of 1:1 ratio between intervention group and control group, a total of 44 patients will be needed (22 patients in each group). Considering a 20% drop-out rate, 56 patients will be recruited.
Recruitment {15}
A total of 56 patients will be recruited and participate in the study. Prior to recruitment, investigators will carefully study the medical history, laboratory test and imaging test of each patient. If the patient meets the inclusion and exclusion criteria, researchers will fully consider the compliance of the patients and informed consent forms (ICFs) will be obtained before collecting any data or performing any intervention. after initial assessment and randomization, patients will receive intervention and 48 hours after onset. if the patient still has evidence of organ failure, he will be diagnosed with SAP and will be formally enrolled in the study. The follow-up will be ended when patients leave hospital.
Assignment of interventions: allocation
Sequence generation {16a}
All participants will be randomly divided into intervention group or control group in a 1:1 ratio. Randomization will be performed using opaque envelopes. 56 envelopes will be labeled ‘intervention group’ or ‘control group’ in a 1:1 ratio.
Concealment mechanism {16b}
The envelopes will then be sealed, shuffled by a third party not related to the study. Each new participant entering the study a random envelope will be opened. The envelopes will be not accessible to individuals directly involved in the study.
Implementation {16c}
A third party, not involved in the assignment or care of the trial participants, will randomly open the sealed envelopes, and assign participants to intervention or control group. Study investigators will lead participant recruitment, informing participants of all the trial procedures and obtaining their ICF before the initial inclusion in the study. Study investigators will confirm the eligibility of the participant prior to any study procedures being undertaken.
Assignment of interventions: Blinding
Who will be blinded {17a}
The participant will remain blinded to the intervention.
Procedure for unblinding if needed {17b}
There should not be any need to unblind the participants. The investigation is not blinded to clinical doctors. Nevertheless, if required, unblinding can be carried out by the study team.
Data collection and management
Plans for assessment and collection of outcomes {18a}
Socio-demographic characteristics and required clinical information will be obtained from the hospital information system of PUMCH. IAP and borborygmus of participants will be measured every day by the researcher. A third person with adequate clinical acumen independent to the project will assess the data collected. If inappropriate data is discovered, study team will be notified to remedy the error.
Plans to promote participant retention and complete follow-up {18b}
During study period, participants will stay in hospital. No follow-up after discharge is arranged. If there is a significant protocol violation, data will not be included in the analysis.
Data management {19}
The data will be collected in a Microsoft Excel database for assessment; data will be kept securely within the organization’s network. All data will be stored with the principal investigator in a password-protected computer for a period of 5 years. All soft copies of the data will be permanently deleted from the computer once the data storage time is over or at the conclusion of the study.
Confidentiality {27}
The collected information will remain anonymous; participants will be allocated a participant number for de-identification purposes. The data will be stored in a password-protected computer and will only be accessed by study team.
Plans for collection, laboratory evaluation and storage of biological specimens for genetic or molecular analysis in this trial/future use {33}
Not applicable. No specimens will be collected.
Statistical methods
Statistical methods for primary and secondary outcomes {20a}
- Intention-to-treat (ITT): No one was excluded from the main analysis set after randomization
- Per-protocol set (PPS): Good compliance case data that meets the main inclusion and exclusion criteria and reach the primary endpoint.
The number of participants selected and complete the study will be listed and the two analysis data sets (ITT and PPS) as specified above will be identified. Cases of protocol violation will also be listed with reasons documented. In terms of outcome indicator analysis, continuous variable indicators will count the number of cases (n), mean (x), standard deviation (SMD), median (M), minimum (min), and maximum (max). The difference between groups will be analyzed using Student’s t-test. Counting and grading data will be used to calculate the frequency and composition ratio. The χ2 test/chi-square test will be used for differences between groups. Unless otherwise stated, all statistical tests will be conducted in a bilateral manner. All data will be entered in Microsoft Excel, and all statistical analyses will be performed using the SPSS version 25 statistical package.
Interim analyses {21b}
No planned interim analyses will be arranged because of relatively small sample size of this study.
Methods for additional analyses {20b}
Currently, there is no planned additional subgroup or adjusted analyses.
Methods in analysis to handle protocol non-adherence and any statistical methods to handle missing data {20c}
An ITT data set will be used for protocol non-adherence and no imputation of missing data will be performed for statistical analysis.
Plans to give access to the full protocol, participant level-data and statistical code {31c}
Any data required to support the protocol can be supplied on reasonable request. Only de-identified datasets will be supplied.
Oversight and monitoring
Composition of the coordinating center and trial steering committee {5d}
This is a single-center trial. The study team will coordinate and manage the entire study process. A regular meeting will be arranged to discuss study questions of any type. An IRB consisting of three experts not involved in this study will be formed to monitor the trial.
Composition of the data monitoring committee, its role and reporting structure {21a}
This is a single-center trial with relatively small sample-size, data monitoring will therefore be conducted by study team. No data monitoring committee is required.
Adverse event reporting and harms {22}
All participants will be monitored with respect to any possible adverse events related to the administration of interventions. All adverse events (AEs) observed or reported by the participants or clinical doctors are collected and evaluated for relatedness to trial intervention, seriousness, severity, expectedness, and outcome by study team. All adverse events will be documented and reported to IRB.
Frequency and plans for auditing trial conduct {23}
For the quality assurance, 20% randomly selected data from the collected information will be re-interviewed. Any discrepancies will be corrected accordingly. In addition, the IRB will audit the data every month.
Plans for communicating important protocol amendments to relevant parties {25}
The principal investigator will be responsible for any protocol modification and any modification will be submitted to the Research Ethics committee of PUMCH for approval. The principal investigator will disseminate the changes of the protocol and all team members will be trained.
Dissemination plans {31a}
The study findings will be presented in national or international conferences. A full scientific article will be developed and published in peer-reviewed journal/s. The results of the study will be released to the participating patients.