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NCT00131196 Clinical Trial

Functional Genomic Influences on Disease Progression and Outcome in Sepsis

Pneumonia Clinical Trial

GAinS

Official title:
Functional Genomic Influences on Disease Progression and Outcome in Sepsis Due to Pneumonia or Peritonitis

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT00131196
Other study ID # N8518
Secondary ID
Status Recruiting
Phase N/A
First received August 15, 2005
Last updated May 13, 2016
Start date September 2005
Est. completion date December 2017

Study information
Verified date May 2016
Source University of Oxford
Contact Charles J Hinds, MD
Phone +44 20346 57294
Email c.j.hinds@qmul.ac.uk
Is FDA regulated No
Health authority United Kingdom: National Health Service
Study type Observational

Clinical Trial Summary

The proposal is aimed at identifying genetic factors that determine the incidence and severity of, and the outcome from life−threatening infections (severe sepsis/septic shock) in patients admitted to High Dependency Units (HDUs) or Intensive Care Units (ICUs) with pneumonia which developed outside the hospital (community acquired pneumonia − CAP) or contamination of the abdominal cavity with faeces due to a leak in the bowel (faecal peritonitis). This will require the acquisition of a large, high quality resource of genetic material (DNA), plasma, urine, white blood cells and clinical information from well characterized groups of similar patients with, or at risk for, severe sepsis/septic shock. The principal objective is to perform studies which are sufficiently large to establish beyond doubt the influence of a series of selected "candidate" genes on the development, progress and outcome of sepsis.

Description:

The investigators plan to recruit 2,000 cases of community acquired pneumonia (CAP) and 2,000 cases of faecal peritonitis (FP) from 30 UK ICUs and HDUs (members of the UK Critical Care Genomics group − UKCCG). The large number of patients is required to satisfy the power calculations based upon the predicted allele frequencies of candidate genes and the level of functional expression of the gene polymorphisms.

If a patient is eligible, written, informed consent will be obtained either from the patient or, if the patient is incompetent via the patient's legal representative. Patients will be characterized clinically in terms of admission diagnosis, severity of illness (APACHE II), organ failures (SOFA) and final outcome (ICU and hospital mortality, death or survival 6 months following ICU admission. Date of death will be recorded when appropriate). Clinical status will be assessed daily for days 1, 2, 3, 5 and 7 of ICU admission using the Sepsis criteria, SOFA score, microbiological culture results and antibiotic therapy.

Selected ICUs will, following consent, also undertake blood and urine sampling on days 1, 3 and 5 for genomic, proteomic and metabolomic studies. Information will be recorded on a bar−coded paper clinical report form (CRF) at the bedside. The CRFs will be securely stored locally and copied to the research coordinator, where they will be archived. The data will be entered independently by the research coordinator and one of the investigators into a secure, central web−based electronic database for storage of clinical data and the calculation of derived values. The patient codes for genetic analysis will be derived directly from the clinical database. Those undertaking genotyping will be blinded to the clinical details and these two databases will be brought together at the time of analysis only under the direct supervision of one of the principal investigators.

Recruitment information / eligibility
Status Recruiting
Enrollment 4000
Est. completion date December 2017
Est. primary completion date December 2017
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Patient, or legal representative, is able to give informed consent

- Male or female of 18 years or more

- Patient admitted to ICU/HDU with faecal peritonitis or community acquired pneumonia

Exclusion Criteria:

- Patient or legal representative is unwilling to consent

- Patient is under the age of 18 years

- Patient is already enrolled in an interventional study

- Patient is immunocompromised

- Patient is pregnant

- There is an advance directive to withhold or withdraw life-sustaining treatment or patient is admitted for palliative care only.

Study Design

Observational Model: Cohort, Time Perspective: Prospective

Related Conditions & MeSH terms

Locations
Country Name City State
United Kingdom Aberdeen Royal Infirmary Aberdeen
United Kingdom Antrim Hospital Antrim County Antrim
United Kingdom Queen Elizabeth Hospital Birmingham West Midlands
United Kingdom Royal Blackburn Hospital Blackburn Lancashire
United Kingdom Blackpool Victoria Hospital Blackpool Lancashire
United Kingdom Royal Sussex County Hospital Brighton Sussex
United Kingdom Bristol Royal Infirmary Bristol Gloucestershire
United Kingdom Frenchay Hospital Bristol South Gloucestershire
United Kingdom Southmead Hospital Bristol Avon
United Kingdom Addenbrooke's Hospital Cambridge Cambridgeshire
United Kingdom University Hospital of Wales Cardiff South Glamorgan
United Kingdom Broomfield Hospital Chelmsford Essex
United Kingdom Cheltenham General Hospital Cheltenham Gloucestershire
United Kingdom Colchester General Hospital Colchester Essex
United Kingdom Castle Hill Hospital Cottingham East Riding of Yorkshire
United Kingdom University Hospital Coventry Warwickshire
United Kingdom Frimley Park Hospital Frimley Surrey
United Kingdom Calderdale Royal Hospital Halifax West Yorkshire
United Kingdom Huddersfield Royal Infirmary Huddersfield West Yorkshire
United Kingdom Hull Royal Infirmary Hull Yorkshire
United Kingdom The Ipswich Hospital Ipswich Suffolk
United Kingdom Kettering General Hospital Kettering Northants
United Kingdom Queen Elizabeth Hospital King's Lynn Norfolk
United Kingdom St James's University Hospital Leeds West Yorkshire
United Kingdom Glenfield Hospital Leicester
United Kingdom Leicester General Hospital Leicester
United Kingdom Leicester Royal Infirmary Leicester Leicestershire
United Kingdom University Hospital Lewisham Lewisham London
United Kingdom Charing Cross Hospital London
United Kingdom Chelsea and Westminster Hospital London
United Kingdom Hammersmith Hospital London
United Kingdom Homerton Hospital London
United Kingdom North Middlesex University Hospital London
United Kingdom St Bartholomew's Hospital London
United Kingdom St Mary's Hospital London
United Kingdom UCLH Middlesex Hospital London
United Kingdom Hope Hospital Manchester Greater Manchester
United Kingdom Withington Hospital Manchester Greater Manchester
United Kingdom Wythenshawe Hospital Manchester Greater Manchester
United Kingdom James Cook University Hospital Middlesborough Cleveland
United Kingdom Royal Victoria Infirmary Newcastle-Upon-Tyne Tyne and Wear
United Kingdom Norfolk and Norwich University Hospitals Norwich Norfolk
United Kingdom John Radcliffe Hospital Oxford Oxon
United Kingdom Royal Preston Hospital Preston Lancashire
United Kingdom Royal Berkshire Hospital Reading Berkshire
United Kingdom Royal Halamshire Hospital Sheffield
United Kingdom Southend General Hospital Southend Essex
United Kingdom The Great Western Hospital Swindon
United Kingdom Walsall Manor Hospital Walsall West Midlands
United Kingdom Worthing and Southlands Hospitals NHS Trust Worthing West Sussex

Sponsors (5)
Lead Sponsor Collaborator
University of Oxford Barts and the London School of Medicine and Dentistry, Queen Mary University of London, Sainsbury Family Charitable Trusts, Wellcome Trust Centre for Human Genetics, Oxford

Country where clinical trial is conducted

United Kingdom, 

References & Publications (8)

Brun-Buisson C, Doyon F, Carlet J, Dellamonica P, Gouin F, Lepoutre A, Mercier JC, Offenstadt G, Régnier B. Incidence, risk factors, and outcome of severe sepsis and septic shock in adults. A multicenter prospective study in intensive care units. French ICU Group for Severe Sepsis. JAMA. 1995 Sep 27;274(12):968-74. — View Citation

File TM. Community-acquired pneumonia. Lancet. 2003 Dec 13;362(9400):1991-2001. Review. — View Citation

Gordon AC, Lagan AL, Aganna E, Cheung L, Peters CJ, McDermott MF, Millo JL, Welsh KI, Holloway P, Hitman GA, Piper RD, Garrard CS, Hinds CJ. TNF and TNFR polymorphisms in severe sepsis and septic shock: a prospective multicentre study. Genes Immun. 2004 Dec;5(8):631-40. — View Citation

Mira JP, Cariou A, Grall F, Delclaux C, Losser MR, Heshmati F, Cheval C, Monchi M, Teboul JL, Riché F, Leleu G, Arbibe L, Mignon A, Delpech M, Dhainaut JF. Association of TNF2, a TNF-alpha promoter polymorphism, with septic shock susceptibility and mortality: a multicenter study. JAMA. 1999 Aug 11;282(6):561-8. — View Citation

Roy S, Knox K, Segal S, Griffiths D, Moore CE, Welsh KI, Smarason A, Day NP, McPheat WL, Crook DW, Hill AV; Oxford Pneumoccocal Surveillance Group. MBL genotype and risk of invasive pneumococcal disease: a case-control study. Lancet. 2002 May 4;359(9317):1569-73. — View Citation

Sands KE, Bates DW, Lanken PN, Graman PS, Hibberd PL, Kahn KL, Parsonnet J, Panzer R, Orav EJ, Snydman DR, Black E, Schwartz JS, Moore R, Johnson BL Jr, Platt R; Academic Medical Center Consortium Sepsis Project Working Group. Epidemiology of sepsis syndrome in 8 academic medical centers. JAMA. 1997 Jul 16;278(3):234-40. — View Citation

Sørensen TI, Nielsen GG, Andersen PK, Teasdale TW. Genetic and environmental influences on premature death in adult adoptees. N Engl J Med. 1988 Mar 24;318(12):727-32. — View Citation

Vincent JL, Angus D, Annane D, Bernard G, Faist E, Giroir B, Reinhart K. Clinical expert round table discussion (session 5) at the Margaux Conference on Critical Illness: outcomes of clinical trials in sepsis: lessons learned. Crit Care Med. 2001 Jul;29(7 Suppl):S136-7. — View Citation

Outcome
Type Measure Description Time frame Safety issue
Primary ICU and hospital Mortality ICU discharge, hospital discharge and 6 month. The date of death will be recorded, as appropriate, for each patient. No
Secondary Severity of illness, duration of organ support, shock reversal, duration of ICU and hospital stay From ICU admission to discharge No
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