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NCT06115044 Clinical Trial

The DINE-Normal Proof-of-concept Study

Critical Illness Clinical Trial

Official title:
Does Intermittent Nutrition Enterally Normalise Hormonal and Metabolic Responses to Feeding in Critically Ill Adults: The DINE-Normal Proof-of-concept Study

Clinical Trial Details — Status: Active, not recruiting

Administrative data
NCT number NCT06115044
Other study ID # R&D 5454
Secondary ID IRAS 328469
Status Active, not recruiting
Phase N/A
First received
Last updated
Start date December 27, 2023
Est. completion date October 2024

Study information
Verified date April 2024
Source North Bristol NHS Trust
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Overarching hypothesis In critically ill adults enteral feeding in a diurnal intermittent pattern improves patient centred outcomes. Research questions for this study Are the same derangements in metabolic and hormonal function observed in healthy volunteers when fed continuously via a nasogastric tube observed in critically ill patients and can those derangements be mitigated by intermittent diurnal feeding? Aim of this study Assess the effect of an enteral nutrition regimen mimicking the usual diurnal meal pattern on hormonal profile and metabolism in critically ill adults. This will generate novel and important proof of concept data and support progression to a clinical trial integrating investigation of physiological responses and patient centred outcomes. Objectives of this study Laboratory: Characterise patterns of hormone, lipid and metabolite response to intermittent diurnal feeding in critically ill adults. Clinical: assess feasibility, tolerability (vomiting and gastric residual volume) and efficacy (calorie delivery) of intermittent diurnal feeding in critically ill adults.

Description:

Setting Single adult general intensive care unit in Bristol with 48 beds and ~2500 admissions annually Design Parallel group randomised, open-label trial Population We will recruit from a representative critically ill population and exclude patients with conditions that pose undue risk and/or introduce bias. See eligibility criteria. Screening and recruitment Usual care team will screen daily. Eligibility will be confirmed by health care professional on the delegation log and recorded in the ICU clinical information system. This may be done remotely. A screening log will be kept. Randomisation Via sealed opaque envelopes prepared in advance, allocation 1:1 to intervention or control, stratified by sex. Consent Enteral nutrition is a necessary intervention. Early nutrition (within hours) is the current standard of care. Prolonged continuous feeding prior to enrolment may bias results. An emergency waiver will be used and deferred consent sought from participants. Where participants lack capacity, this will be from a personal or professional consultee as appropriate. Intervention Participants will receive their estimated nutritional requirement in 3 equal "meals" each over 30-60 minutes at 0800, 1300, and 1800 with first meal given after an overnight fast from 1900 on the day of enrolment. Controls Participants will receive their estimated nutritional requirement as continuous feed starting at 0800 after an overnight fast from 1900 on the day of enrolment. The daily nutritional requirement will be estimated by dietetic staff in the Intensive Care Unit as per usual practice. All other care for both groups will follow usual unit practice as directed by treating intensivist. Once blood sampling for the primary outcome is complete the study intervention period ends and feeding will continue according to usual unit practice. Blood sampling Primary outcome assessment requires six one-hourly samples will be hourly around the fourth bolus feed with equivalent timing in control group. Outcomes See outcomes section Adverse events The natural history of critical illness includes many events that might be considered adverse events or serious adverse events including death, organ failure or nosocomial infection. Such expected events do not need to be reported. Events that are not recorded as study outcomes and are considered possibly related to the study will be reported. The reporting period runs for 72 hours from the start of the overnight fast. Follow up Routinely collected clinical audit data will be used for ICU and hospital length of stay and mortality. Sample size Overall sample size is 30. Based on the data from healthy subjects this study is powered to detect smaller (but substantial) effect sizes (d=1.26) with 15 per group while allowing for some drop out. Analysis Analysis will be undertaken blinded to group allocation. Normality will be tested and appropriate parametric / non-parametric tests used for the primary outcome. Additional analysis of the insulin response (e.g. area under the curve) will be undertaken. Repeated measures ANOVA will be used for physiological secondary outcomes. P < 0.05 will be taken as significant.

Recruitment information / eligibility
Status Active, not recruiting
Enrollment 30
Est. completion date October 2024
Est. primary completion date April 24, 2024
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Adults (=18) on intensive care - Planned for gastric enteral nutrition (anticipated duration >48 hours) Exclusion Criteria: - >24 hours after commencement of enteral nutrition - Gastrointestinal surgery or pathology - Diabetic emergencies - Pregnancy - Parenteral or jejunal nutrition - Trophic feed only - Prone positioning - High risk of refeeding syndrome

Study Design

Related Conditions & MeSH terms

Intervention

Procedure:
Intermittent diurnal nutrition
Calculated daily nutritional requirement given as three equal bolus feeds in daytime with prolonged overnight fast
Continuous
Calculated daily nutritional requirement given over 24 hours

Locations
Country Name City State
United Kingdom Southmead Hospital Bristol

Sponsors (4)
Lead Sponsor Collaborator
North Bristol NHS Trust University of Bath, University of Bristol, University of the West of England

Country where clinical trial is conducted

United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary Insulin Plasma insulin and C-Peptide Peak within 3 hours of bolus feed (comparable time point in comparator)
Secondary Endocrine and metabolic Urea Peak within 3 hours of bolus feed (comparable time point in comparator)
Secondary Endocrine and metabolic Glucagon-like peptide 1 (GLP-1) Peak within 3 hours of bolus feed (comparable time point in comparator)
Secondary Calories delivered Calories delivered (absolute and % of target) Study day 1 and study day 2
Secondary Incidence of gastrointestinal upset (GI upset) Number of events of delayed gastric emptying, vomiting, diarrhoea, ileus Study day 1 and study day 2
Secondary Mortality All cause crude mortality ICU and acute hospital
Secondary Length of stay Length of stay (days) ICU and acute hospital
Secondary Delta-SOFA Difference between baseline and end of intervention sequential organ failure assessment Day 0 and day 2
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