Infection Clinical Trial
Official title:
Open-label, Multicentre, Randomized, Parallel Group Study to Assess the Efficacy and Safety of Oxygen-ozone Therapy Plus Oral Antibiotic Therapy in the Treatment of Infections Secondary to Implant of Orthopaedic Devices
This is an open-label, multicentre, randomized, parallel group study to evaluate the efficacy of treatment with oxygen-ozone therapy plus oral antibiotic therapy, in comparison with oral antibiotic therapy alone, in the proportion of patients with resolution/improvement of signs and symptoms of infection of the wound (e.g. ulcer, eschar, sore) in the target lesion after 14 days of treatment, in patients with infections secondary to implant of orthopaedic devices.
| Status | Recruiting |
| Enrollment | 186 |
| Est. completion date | January 2026 |
| Est. primary completion date | September 2025 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years and older |
| Eligibility | Inclusion Criteria: 1. Signed written informed consent; 2. Male or female aged = 18 years; 3. Patient having undergone surgery for implant of an orthopaedic device in the previous 8 weeks; 4. Presence of at least one (but no more than 3) post-operative wounds in the site of surgery (ulcers, eschars, sores); 5. Presence of at least one symptom (pain, burning, redness and malodour) and at least one sign (erythema, local warmth, swelling, purulent secretion) of infection of at least moderate intensity (score = 2) in the target lesion at the screening visit (Visit 1), to be confirmed again at the baseline visit (Visit 2); 6. Wound area of the target lesion = 100 cm2; 7. Patient with presence at least one pathogen identified in the swab collection in the target lesion, which is amenable to be eradicated with oral antibiotic therapy; 8. In case of multiple wounds (however not more than three), non-target lesions must not overlap with the target one (i.e. the largest one); 9. Patient able to perform the wound self-care at home or care by his/her primary caregiver; 10. Willing to refrain from all non-permitted concomitant medication from the screening visit through to the entire study duration. 11. Female subjects of childbearing potential must have a negative urinary pregnancy test at Screening and must practice a reliable method of contraception throughout the study; 12. Patient able to read and understand the study procedures, the requirements for follow-up visits, willing to provide information at the scheduled evaluations and willing, able and ensuring to comply with the study requirements for the whole study period. Exclusion Criteria: 1. Wounds without signs of localized infection; 2. Presence of more than four wounds; 3. Presence of one or more wounds with area > 100 cm2; 4. Presence of undermining wounds; 5. Patients with favism, i.e. deficiency of the glucose-6-phosphate dehydrogenase (G6PD) enzyme; 6. Patients with uncontrolled hyperthyroidism; 7. Patients with history of connective tissue disease, e.g., mixed connective tissue disease; 8. Patients with active malignant disease; 9. Patients with other clinically significant diseases, or other major diseases deemed clinically significant by the Investigator or which in the opinion of the Investigator would interfere with the study procedures or study outcome; 10. Patients candidate to any surgery during the overall study duration; 11. Treatment with topical corticosteroids in the previous 4 weeks and/or with systemic corticosteroids in the previous 7 days; 12. Treatment with any hydrating and/or moisturizing cream in the previous 24 hours. 13. Patients on treatment with chemotherapeutic agents, radiation therapy or immunosuppressive therapies; 14. Patients with contraindications to antibiotic therapy; 15. Pregnant, breastfeeding women and female child-bearing potential who are not using a highly effective method of birth control and not willing to use it during the participation to the study; 16. Participation in any clinical research study evaluating another investigational drug or device within 30 days prior to consenting to study entry; 17. Patient unable to understand informed consent or having a high probability of non-compliance with the study procedures and or non-completion of the study according to investigator's judgement. |
| Country | Name | City | State |
|---|---|---|---|
| Italy | Ospedali Riuniti Torrette | Ancona | |
| Italy | Pineta Grande Hospital | Castel Volturno | Caserta |
| Italy | Università Federico II | Napoli | |
| Italy | Azienda Ospedaliera Universitaria Policlinico Paolo Giaccone di Palermo | Palermo | |
| Italy | Fondazione IRCCS Policlinico San Matteo | Pavia | |
| Italy | Casa Di Cura Citta' Di Roma | Roma |
| Lead Sponsor | Collaborator |
|---|---|
| Società Scientifica Internazionale di Ossigeno Ozono Terapia |
Italy,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | Number of subjects experiencing treatment-emergent adverse events and serious TEAEs | 7 weeks | ||
| Other | Number of subjects experiencing local TEAEs in the site of application of the IP | 7 weeks | ||
| Other | Changes from baseline to any post-baseline time point in blood pressure | Systolic and diastolic blood pressure will be measured at each study visit in sitting position after at least 10 minutes rest | 7 weeks | |
| Other | Changes from baseline to any post-baseline time point in heart rate | Heart rate will be recorded at each study visit; it will be measured for one minute just prior to the sitting blood pressure measurement. | 7 weeks | |
| Other | Changes in haemoglobin values | Haematology will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in haematocrit values | Haematology will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in red blood cell (RBC) count | Haematology will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in platelet count | Haematology will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in creatinine values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in blood urea nitrogen (BUN) values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in glucose values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in aspartate aminotransferase (AST) values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in alanine aminotransferase (ALT) values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in gamma-glutamyl transpeptidase (gamma-GT) values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in alkaline phosphatase values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in total bilirubin values | Blood chemistry will be evaluated in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in sodium values | Electrolytes will be evaluated in blood in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in potassium values | Electrolytes will be evaluated in blood in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in magnesium values | Electrolytes will be evaluated in blood in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in chloride values | Electrolytes will be evaluated in blood in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Other | Changes in calcium values | Electrolytes will be evaluated in blood in the reference local laboratory of each investigational study site at the screening visit (Visit 1, Day -7/-3) and at Visit 4 (Day 14) and Visit 6 (Day 42). | 7 weeks | |
| Primary | Clinical success at Day 14 | Resolution/improvement of signs and symptoms of infection of the wound in the target lesion (i.e. a score = 1 for a maximum of two signs/symptoms) from baseline to Day 14. The following symptoms will be evaluated by patients on a 0-4 point Likert scale (0 = no symptom; 1 = mild symptom; 2 = moderate symptom; 3 = severe symptom; 4 = very severe symptom): pain, burning, redness and malodour.
The following signs will be evaluated by investigators on a 0-4 point Likert scale (0 = no sign; 1 = mild sign; 2 = moderate sign; 3 = severe sign; 4 = very severe sign): erythema, local warmth, swelling, purulent secretion. |
2 week | |
| Secondary | Proportion of patients with clinical success at Day 7, Day 28, and Day 42 | Clinical success is defined as resolution/improvement of signs and symptoms of infection of the wound in the target lesion | Day 7, Day 28, and Day 42 | |
| Secondary | Time to resolution of all signs and symptoms of infection | It is defined as the disappearance (score = 0) of all signs and symptoms of infection of the wound in the target lesion; | 7 weeks | |
| Secondary | Eradication of the pathogen isolated at the screening visit | Bacteriological success of the wound in the target lesion at Day 14 (V4) and Day 42 (V6).A bacteriological success is defined as eradication of the pathogen isolated at the screening visit, without superinfection or reinfection with the same pathogen; | 7 weeks | |
| Secondary | Changes from baseline to any post-baseline time-point of the size of the target lesion | 7 weeks | ||
| Secondary | Global assessment of the target lesion at Day 14 and Day 42 | Investigators will be requested to score the outcome of the target lesion on a five-grade scale: 1= worsening, 2 = no change, 3 = minimal improvement, 4 = moderate improvement and 5 = good improvement/resolution; | 7 weeks | |
| Secondary | Changes from baseline to any post-baseline time-point in body temperature | 7 weeks | ||
| Secondary | Changes in WBCs count | Changes from baseline to Day 14 (V4) and Day 42 (V6) of white blood cells count (a laboratory parameters that is indicative of infection) | 7 weeks | |
| Secondary | Changes in Erythrocyte sedimentation rate | Changes from baseline to Day 14 (V4) and Day 42 (V6) of ESR values (a laboratory parameters that is indicative of infection) | 7 weeks | |
| Secondary | Changes in High-sensitivity C-reactive protein | Changes from baseline to Day 14 (V4) and Day 42 (V6) of hs-CRP values (a laboratory parameters that is indicative of infection) | 7 weeks |
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Completed |
NCT04529421 -
Assocation Between In-person Instruction and COVID-19 Risk
|
||
| Recruiting |
NCT04081792 -
Optimal Antibiotics for Operated Diabetic Foot Infections
|
N/A | |
| Completed |
NCT04332861 -
Evaluation of Infection in Obstructing Urolithiasis
|
||
| Recruiting |
NCT04674657 -
Does Extra-Corporeal Membrane Oxygenation Alter Antiinfectives Therapy Pharmacokinetics in Critically Ill Patients
|
||
| Enrolling by invitation |
NCT05052203 -
Researching the Effects of Sepsis on Quality Of Life, Vitality, Epigenome and Gene Expression During RecoverY From Sepsis
|
||
| Recruiting |
NCT00342589 -
New Techniques for Using a Saline Wash as a Diagnostic Tool for Pneumocystis Pneumonia
|
||
| Completed |
NCT03295825 -
Heparin Binding Protein in Early Sepsis Diagnosis
|
N/A | |
| Completed |
NCT03296423 -
Bacillus Calmette-guérin Vaccination to Prevent Infections of the Elderly
|
Phase 4 | |
| Withdrawn |
NCT04217252 -
Clinical Application of High-throughput Sequencing Technology for the Diagnosis of Patients With Severe Infection
|
N/A | |
| Recruiting |
NCT02905552 -
Myelodysplasic Syndromes and Risk Factors for Infection
|
N/A | |
| Recruiting |
NCT02899143 -
Short-course Antimicrobial Therapy in Sepsis
|
Phase 2 | |
| Withdrawn |
NCT02904434 -
Gastrointestinal Implications of Voriconazole Exposure
|
||
| Active, not recruiting |
NCT02768454 -
Antimicrobials Stewardship by Pharmacist
|
N/A | |
| Completed |
NCT02219776 -
Decreasing Infection In Arthroscopic Shoulder Surgery
|
N/A | |
| Completed |
NCT02210169 -
RCT of Continuous Versus Intermittent Infusion of Vancomycin in Neonates
|
N/A | |
| Recruiting |
NCT02098226 -
Evaluation of MALDI Biotyper CA System for Detection of Gram- and Gram+ Bacteria and Yeasts
|
N/A | |
| Completed |
NCT01846832 -
A Study of TMC435 Plus Pegylated Interferon Alfa-2a and Ribavirin in Participants With Chronic HCV Infection
|
Phase 3 | |
| Terminated |
NCT01441206 -
Safety and Pharmacokinetics of Single and Multiple Dose Rifampin in Infants
|
Phase 1 | |
| Completed |
NCT01434797 -
Value of PET/CT Imaging in the Diagnosis of Permanent Central Venous Catheters Infection
|
||
| Completed |
NCT01159834 -
Human Papillomavirus (HPV) Vaccination in Barretos (Pio XII Foundation - Barretos Cancer Hospital)
|
N/A |