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Assessing the Efficacy of Anti-staphylococcal Phages in the Management of Infected Foot Ulcers in Diabetes (PDFI)

Primary Purpose

Diabetes, Diabetic Foot, Diabetic Foot Infection

Status
Withdrawn
Phase
Phase 1
Locations
United Kingdom
Study Type
Interventional
Intervention
Phage
Sponsored by
University Hospitals of Derby and Burton NHS Foundation Trust
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Diabetes focused on measuring Diabetes, Diabetic Foot Disease, Diabetic Foot Ulcer

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  1. Diabetes Mellitus according to WHO criteria
  2. are aged 18 years or over
  3. Additionally, patients must meet one of the following criteria to participate in the described Work Package:

    • Patients are only eligible for WP1 if they also have one or more DFUs (area 25mm2) below the malleoli without infection according to IDSA criteria that have been present for at least 4 weeks
    • Patients are only eligible for WP2 if they also have one or more DFUs (area 25mm2) below the malleoli with mild or moderate infection according to IDSA criteria that have been present for at least 4 weeks
    • Patients are only eligible for WP3 if they also have one or more DFUs (area 25mm2) below the malleoli with mild infection according to IDSA criteria that have been present for at least 4 weeks

Exclusion Criteria:

We will exclude patients who meet ANY of the following criteria:

  1. with mental incapacity to give informed consent,
  2. who have other major co-morbidities, which in the opinion of the investigator would mean that the patient would not be able to complete the study
  3. with significant peripheral arterial disease (PAD): ABPI (ankle brachial pressure index) <0.7,
  4. Who have osteomyelitis defined by agreed clinical criteria
  5. who are receiving treatment with systemic glucocorticoids or other immunosuppressants,
  6. who have received systemic or topical antibiotics in the preceding 14 days,
  7. who are judged to require parenteral administration of antibiotics,
  8. Who have been previously recruited to an earlier part of the project
  9. who are women of childbearing age who are at risk of conception
  10. History of antibiotic hypersensitivity

Sites / Locations

  • University Hospitals Derby and Burton NHS Foundation Trust

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Placebo Comparator

Arm Label

Phage

Placebo

Arm Description

Outcomes

Primary Outcome Measures

Work Package 1: To assess the safety of the use of anti-staphylococcal phages therapy on the wound bacterial microbiome of uninfected DFU's.
- Safety : Clinically significant change in safety bloods, vital signs, Full Blood Count (FBC), renal function, C-Reactive protein (CRP), Liver function Tests (LFT)s, Adverse events
Work Package 2
To compare the effect on the microbiome of empirical systemic antibiotic therapy alone (ESAT) versus ESAT plus phage therapy in ulcers complicated by mild or moderate infection as assessed by IDSA criteria
Work Package 3
To compare the use of empirical systemic antibiotic therapy versus phage therapy in ulcers complicated by mild infection on the eradication of the infection as assessed by IDSA criteria.

Secondary Outcome Measures

Work Package 1: Safety of phage gel and overt toxic effect of phage gel.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Incidence of new infection Number of days of antibiotic usage Change in surface microbiome Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Vital signs (Resting pulse and blood pressure (BP))
Work Package 1: • Impact on the bacterial microbiome of anti-staphylococcal phage gel and systemically chosen antibiotics.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Incidence of new infection Number of days of antibiotic usage Change in surface microbiome Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Vital signs (Resting pulse and blood pressure (BP))
Work Package 2: Safety of phage gel and overt toxic effect of phage gel.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Work Package 2: Clinical benefit and patient well-being associated with adding phage gel to systemically chosen antibiotics compared to placebo in the management of mild or moderate infection.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Work Package 2: Impact on the bacterial microbiome of systemically chosen antibiotics and of anti-staphylococcal phage gel.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Work Package 3: Safety of phage gel and overt toxic effect of phage gel.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Work Package 3: Clinical benefit and patient well-being associated with phage gel therapy compared to systemically chosen antibiotics in the management of mild infection.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Work Package 3: Impact on the bacterial microbiome of systemically chosen antibiotics and of anti-staphylococcal phage gel.
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)

Full Information

First Posted
September 3, 2018
Last Updated
February 26, 2020
Sponsor
University Hospitals of Derby and Burton NHS Foundation Trust
Collaborators
Wellcome Trust, BioPhage Theraputics Limited, Nottingham University Hospitals NHS Trust
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1. Study Identification

Unique Protocol Identification Number
NCT04289948
Brief Title
Assessing the Efficacy of Anti-staphylococcal Phages in the Management of Infected Foot Ulcers in Diabetes
Acronym
PDFI
Official Title
Assessing the Efficacy of Anti-staphylococcal Phages in the Management of Infected Foot Ulcers in Diabetes
Study Type
Interventional

2. Study Status

Record Verification Date
February 2020
Overall Recruitment Status
Withdrawn
Why Stopped
Funding issues meant that development of the study was halted.
Study Start Date
March 1, 2019 (Anticipated)
Primary Completion Date
June 1, 2022 (Anticipated)
Study Completion Date
September 1, 2022 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
University Hospitals of Derby and Burton NHS Foundation Trust
Collaborators
Wellcome Trust, BioPhage Theraputics Limited, Nottingham University Hospitals NHS Trust

4. Oversight

Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
Work Package 1: Observational cohort pilot safety study Work Package 2: Randomised, double-blind, placebo controlled pilot study Work Package 3: Observer-blind pilot RCT
Detailed Description
Work Package 1 WP1 is a safety cohort pilot study targeting patients with DFU which are non-infected as determined by the IDSA criteria. 20 participants will be recruited from Diabetic Foot Clinic at the Royal Derby Hospital. Phage gel will be applied to the index ulcer after the first and second sets of measures at baseline, weeks 1, 2 and 3. Samples will be taken at baseline and weekly up to 4 weeks by surface swab and deep tissue sample for determination of bacterial colonisation using both conventional and genotypic (molecular) microbiological methods, prior to any IMP application. Work Package 2 WP2 is a pilot double blind, placebo-controlled, randomised study targeting patients with mild or moderate infection of DFUs and comparing systemic antibiotic therapy plus phage gel against systemic antibiotics therapy plus placebo gel. A total of 50 participants from two centres (foot clinics at Royal Derby Hospital and City Campus, Nottingham University Hospitals NHS Trust) will be recruited. Phage gel or placebo will be applied to the index ulcer after the first and second sets of measures at baseline, weeks 1, 2 and 3. Samples will be taken at baseline and weekly up to 4 weeks by surface swab and deep tissue sample for determination of bacterial colonisation using both conventional and genotypic (molecular) microbiological methods Work Package 3 WP3 is an observer-blind RCT targeting patients with mild diabetic foot infection by IDSA criteria and comparing phage gel with systemic antibiotics. A total of 50 participants from two centres (foot clinics at Royal Derby Hospital and City Campus, Nottingham University Hospitals NHS Trust) will be recruited. Those with moderately severe infections will be withheld from this work package because of the clinical and ethical issues associated with withholding antibiotics in those with a moderately severe infection.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Diabetes, Diabetic Foot, Diabetic Foot Infection
Keywords
Diabetes, Diabetic Foot Disease, Diabetic Foot Ulcer

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 1, Phase 2
Interventional Study Model
Parallel Assignment
Masking
ParticipantCare ProviderInvestigator
Masking Description
Work Package 1: Observational cohort pilot safety study Work Package 2: Randomised, double-blind, placebo controlled pilot study Work Package 3: Observer-blind pilot RCT
Allocation
Randomized
Enrollment
0 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Phage
Arm Type
Experimental
Arm Title
Placebo
Arm Type
Placebo Comparator
Intervention Type
Drug
Intervention Name(s)
Phage
Intervention Description
The studies will be undertaken using a cocktail of at least 2-3 anti-staphylococcal phages produced by Intralytix Inc, Baltimore, Maryland, USA. The phages will be included in a gel designed for application directly to the wound surface and packaged in 5 ml single use tubes.
Primary Outcome Measure Information:
Title
Work Package 1: To assess the safety of the use of anti-staphylococcal phages therapy on the wound bacterial microbiome of uninfected DFU's.
Description
- Safety : Clinically significant change in safety bloods, vital signs, Full Blood Count (FBC), renal function, C-Reactive protein (CRP), Liver function Tests (LFT)s, Adverse events
Time Frame
7 months
Title
Work Package 2
Description
To compare the effect on the microbiome of empirical systemic antibiotic therapy alone (ESAT) versus ESAT plus phage therapy in ulcers complicated by mild or moderate infection as assessed by IDSA criteria
Time Frame
16 months
Title
Work Package 3
Description
To compare the use of empirical systemic antibiotic therapy versus phage therapy in ulcers complicated by mild infection on the eradication of the infection as assessed by IDSA criteria.
Time Frame
16 months
Secondary Outcome Measure Information:
Title
Work Package 1: Safety of phage gel and overt toxic effect of phage gel.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Incidence of new infection Number of days of antibiotic usage Change in surface microbiome Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Vital signs (Resting pulse and blood pressure (BP))
Time Frame
7 months
Title
Work Package 1: • Impact on the bacterial microbiome of anti-staphylococcal phage gel and systemically chosen antibiotics.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Incidence of new infection Number of days of antibiotic usage Change in surface microbiome Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Vital signs (Resting pulse and blood pressure (BP))
Time Frame
7 months
Title
Work Package 2: Safety of phage gel and overt toxic effect of phage gel.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Time Frame
7 months
Title
Work Package 2: Clinical benefit and patient well-being associated with adding phage gel to systemically chosen antibiotics compared to placebo in the management of mild or moderate infection.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Time Frame
16 months
Title
Work Package 2: Impact on the bacterial microbiome of systemically chosen antibiotics and of anti-staphylococcal phage gel.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, vital signs, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Time Frame
16 months
Title
Work Package 3: Safety of phage gel and overt toxic effect of phage gel.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Time Frame
16 months
Title
Work Package 3: Clinical benefit and patient well-being associated with phage gel therapy compared to systemically chosen antibiotics in the management of mild infection.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Time Frame
16 months
Title
Work Package 3: Impact on the bacterial microbiome of systemically chosen antibiotics and of anti-staphylococcal phage gel.
Description
The following outcomes will be recorded at weekly intervals for 4 weeks from baseline: Change in surface microbiome Number of antibiotic-free days Adverse events Change in safety bloods, FBC, renal function, CRP, LFTs Wound status (clinical infection, area, depth, extent of surface slough, pain by VAS, peri ulcer appearance) Patient well-being using a Visual Analogue Scale, 0-100mm. Eradication of clinical evidence of the infection in the index ulcer at weeks 1, 2 and 3, and time to eradication Healing of all ulcers and time to healing Resting pulse and blood pressure (BP)
Time Frame
16 months

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Diabetes Mellitus according to WHO criteria are aged 18 years or over Additionally, patients must meet one of the following criteria to participate in the described Work Package: Patients are only eligible for WP1 if they also have one or more DFUs (area 25mm2) below the malleoli without infection according to IDSA criteria that have been present for at least 4 weeks Patients are only eligible for WP2 if they also have one or more DFUs (area 25mm2) below the malleoli with mild or moderate infection according to IDSA criteria that have been present for at least 4 weeks Patients are only eligible for WP3 if they also have one or more DFUs (area 25mm2) below the malleoli with mild infection according to IDSA criteria that have been present for at least 4 weeks Exclusion Criteria: We will exclude patients who meet ANY of the following criteria: with mental incapacity to give informed consent, who have other major co-morbidities, which in the opinion of the investigator would mean that the patient would not be able to complete the study with significant peripheral arterial disease (PAD): ABPI (ankle brachial pressure index) <0.7, Who have osteomyelitis defined by agreed clinical criteria who are receiving treatment with systemic glucocorticoids or other immunosuppressants, who have received systemic or topical antibiotics in the preceding 14 days, who are judged to require parenteral administration of antibiotics, Who have been previously recruited to an earlier part of the project who are women of childbearing age who are at risk of conception History of antibiotic hypersensitivity
Facility Information:
Facility Name
University Hospitals Derby and Burton NHS Foundation Trust
City
Derby
State/Province
Derbyshire
ZIP/Postal Code
DE22 3DT
Country
United Kingdom

12. IPD Sharing Statement

Plan to Share IPD
Undecided

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Assessing the Efficacy of Anti-staphylococcal Phages in the Management of Infected Foot Ulcers in Diabetes

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