Does GM-CSF Restore Neutrophil Phagocytosis in Critical Illness?

Phase 1

Completed

• Conditions: Immuno-suppression; Critical Illness; Sepsis
• Interventions: Drug: Normal Saline; Drug: Leukine

• Registration Number: NCT01653665
• Lead Sponsor: Newcastle-upon-Tyne Hospitals NHS Trust

Brief Summary

Despite the introduction of multiple preventative measures rates of hospital acquired infection in the intensive care unit remain high. New approaches to tackling this problem are required. The neutrophil (a type of white blood cell) is the key cell fighting bacterial and fungal infection in the body. This research group has already shown that the majority of patients on intensive care have neutrophils which don't ingest germs effectively and are therefore less able to fight infection. These patients, whose white blood cells don't work properly, are much more likely to develop a second infection whilst in hospital (hospital acquired infection).

Previous work done by this group has shown that by adding a drug called granulocyte macrophagecolony stimulating

factor (GM-CSF) to a sample of blood from these patients in the lab, it is possible to restore the ability of the white blood cells to ingest bacteria and fight infection.

This study will test whether it is possible to restore the capacity of patients' white blood cells to eat germs by giving them GM-CSF as an injection while they are on intensive care.

The study will involve identifying adult patients on intensive care whose white blood cells don't work properly in this way. Patients taking part in the study will receive an injection, under the skin, of either the drug, GM-CSF, or a solution which will have no effect (placebo). The investigators will compare whether those patients who have received the GM-CSF injection have an improvement in the function of the white blood cells compared to those who don't.

As well as looking at the function of the white blood cells the investigators will also study whether there is a difference in the rates of infection picked up in hospital between the two groups.

This study is funded by the Medical Research Council.

Detailed Description

Not available

Study Timeline

• Study First Submitted: 2012-07-16
• Study First Submitted QC: 2012-07-30
• Study First Posted: 2012-07-31
• Study Start: 2012-08
• Primary Completion: 2015-01
• Study Completion: 2015-02
• Status Verified: 2018-02
• Last Update Submitted: 2018-02-12
• Last Update Posted: 2018-02-13

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 64

Inclusion Criteria

• Fulfil criteria for systemic inflammatory response syndrome on admission to ICU (see appendix 1)
• Has required support of one or more organ systems (invasive ventilation, inotropes or haemofiltration) during current ICU stay
• Survival over next 48 hours deemed most likely outcome by responsible ICU clinician
• Admitted to ICU within last 72 hours
• Neutrophil phagocytic capacity <50%

Exclusion Criteria

• Absence/refusal of informed consent
• Current prescription of a colony stimulating factor
• Any history of allergy/adverse reaction to GM-CSF
• Total white cell count >30x109/litre at time of screening
• Haemoglobin < 7.5g/dl at the time of screening
• Age < 18 years
• Pregnancy or lactation
• Known in-born errors of neutrophil metabolism
• Known haematological malignancy and/or known to have >10% peripheral blood blast cells
• Known aplastic anaemia or pancytopaenia
• Platelet count <50x109/litre
• Chemotherapy or radiotherapy within the last 24 hours
• Solid organ or bone marrow transplantation
• Use of maintenance immunosuppressive drugs other than maintenance corticosteroids (allowed up to 10mg prednisolone/day or equivalent)
• Known HIV infection
• Active connective tissue disease (e.g. rheumatoid disease, systemic lupus erythematosus) requiring active pharmacological treatment.
• ST-segment elevation myocardial infarction, acute pericarditis (by ECG criteria) or pulmonary embolism (radiographically confirmed) in previous week
• Involvement in any study involving an investigational medicinal product in the previous 30 days

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Placebo (normal saline)	Normal Saline	Participants in the randomised controlled trial may be randomised to receive a daily subcutaneous injection of normal saline (placebo) for 4 or 7 days as decided following the results of the dose finding study
Leukine (Sargramostim, GM-CSF)	Leukine	Participants in dose finding study will receive either 3 or 6 micrograms per kilo per day as a daily subcutaneous injection for either 4 or 7 days. Within the Randomised controlled trial, participants will receive the dose as chosen following the dose finding study.

Primary Outcome Measures

Name	Time	Method
Neutrophil phagocytosis	2 days after GMCSF/placebo administration	neutrophil phagocytic capacity will be measured as the percentage of neutrophils ingesting 2 or more zymosan particles ex vivo

Secondary Outcome Measures

Name	Time	Method
neutrophil phagocytic capacity on alternate study days	0 - 9 days	Measured on alternate days and also as 'area under the curve' over the study period
Monocyte HLA-DR expression	0-9 days	Alternate days by flow-cytometry
Serum measures of inflammatory response	0-9 days	May include but not limited to: cytokine levels
Other measures of neutrophil function	0-9 days	May include but not limited to: ROS generation, migration capacity and apoptotic rate
Length of ICU stay	Up to end of participation in study, a maximum of 30 days
Incidence of ICUAIs (Intensive care unit acquired infection)	Up to end of study participation, a maximum of 30 days for each patients	As defined by hospitals in europe link for infection control surveillance (HELICS)
All cause mortality	30 days post randomisation
Number of days of mechanical ventilation	Up to end of study participation, a maximum of 30 days
Sequential organ failure assessment (SOFA)	up to end of study participation, a maximum of 30 days for each participant
Blood sample analysis	0-9 days	To measure safety of study medication from blood samples, which will include measures of Full blood count, white cell count (including differential), U\&Es and LFTs, development of neutralising antibodies to GMCSF

Trial Locations

Locations (4)

Sunderland Royal Hospital; 🇬🇧 Sunderland, United Kingdom

Freeman Hospital; 🇬🇧 Newcastle upon Tyne, Tyne And Wear, United Kingdom

Queen Elizabeth Hospital; 🇬🇧 Gateshead, Tyne And Wear, United Kingdom

Royal Victoria Infirmary; 🇬🇧 Newcastle upon Tyne, Tyne And Wear, United Kingdom