Chronic Rhinosinusitis (Diagnosis) Clinical Trial
Official title:
Phase-II Randomized Control Trial of Nasal Microbiota Transplant Therapy in Chronic Rhinosinusitis Without Nasal Polyps (CRSsNP)
Chronic Rhinosinusitis (CRS) is a chronic inflammatory condition of the nasal passage and paranasal sinuses that places significant burden on affected patients and global healthcare systems. Current treatments for CRS such as long-term antibiotics, anti-inflammatory drugs, and surgery often reduce symptoms and signs of disease temporarily, however long-term results are much less satisfactory. Recently, the theory of a damaged microbiome (dysbiosis) as a cause or promoting factor behind CRS has gained increasing evidence from the scientific community. A condition of the gut with microbial dysbiosis (c.difficile) has previously employed microbiota transplant treatment with great success in long-term health outcomes. Such treatments are shown to repopulate bacterial microenvironment and restore protective commensal bacterial load. A pilot study conducted by this study team trialed a novel intervention of a Nasal Microbiota Transplant in a small group of participants. Preliminary results suggested significantly improved CRS symptoms after treatment with a healthy donor microbiota transplant, compared to the pre-transplant baseline. The addition of a randomized-control trial with inclusion of a placebo group is the next step. In this study, investigators aim to perform a two-arm, double-blinded, phase II randomized controlled clinical trial in order to assess the efficacy of a Nasal Microbiota Transplant against a placebo in a cohort of CRS patients without Nasal Polyps (CRSsNP).
| Status | Recruiting |
| Enrollment | 60 |
| Est. completion date | December 2025 |
| Est. primary completion date | December 2024 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | All |
| Age group | 18 Years to 80 Years |
| Eligibility | Inclusion criteria (patient): - Diagnosis of Chronic Rhinosinusitis as defined by the presence of 2 or more major sinonasal symptoms (nasal blockage, nasal discharge, loss of smell, and facial pain/ fullness) for a minimum of 12 weeks - Endoscopic confirmation of middle meatus inflammation or presence of mucopurulence, and /or CT confirmation of paranasal sinus inflammation. - Previous nasal surgery with patent ostia to the diseased ethmoids and maxillary sinuses - Signed written informed consent Inclusion criteria (donor): - No history of sinonasal or lower airway disease for the last 2 years other than the common cold. - No clinical findings of sinonasal disease at the inclusion visit. - Accepted as a donor by the patient. - Signed informed consent to participate in the study. Exclusion Criteria: Exclusion criteria (patient): - Aged <18 or >80 years - Allergy to amoxicillin or clavulanate potassium and Clarithromycin. - Excessive Nasal polyposis - Antibiotic treatment in the last 4 weeks - Patients with a history supporting a diagnosis of immune deficiency will be tested (Immunoglobulin A (IgA), Immunoglobulin M (IgM), Immunoglobulin G (IgG) and IgG subclasses, MBL) and /or are immunocompromised due to disease and / or medication ( e.g., insulin dependent diabetes mellitis, systemic corticosteroids) - Patients who live with someone who is severly immunocompromised. - Patients with cystic fibrosis or ciliary dyskinesia - Patients who have been on an active investigational therapy within 2 months of screening - Patients who have clinically significant laboratory abnormalities - Patients who are pregnant, breast feeding or planning to become pregnant during the study - Patients who are not willing to use a double barrier method of contraception during the study that is:- 1. females must use contraceptive pill or Intra-uterine device (IUD) or similar and condoms 2. males must use condoms and spermicidal gel - Patients currently on any medication that may affect the results in an unpredictable manner - The patient does not agree to comply with or is unable to meet all study requirements for the duration of the study period - Patients deemed by the investigator to be unsuitable for participation in the study - Patients who have had Coronavirus-19 (COVID-19) within the last month. Exclusion criteria (donor): - Findings in the prestudy pathogen scan that makes the donor unsuitable. Prestudy pathogen scan: Prior to first donation, the donors will be tested for HIV, Human T-lymphotropic virus 1 and 2, Hepatitis B and C, Syphilis, Tuberculosis, Herpes Simplex (HSV 1 and 2), Varicella Zoster (VZV), Cytomegalovirus (CMV), Epstein-Barr virus (EBV), Methicillin-resistant Staphylococcus aureus (MRSA) and a standard panel for sinonasal pathogens (Pneumococci, H. Influenza, Beta-streptococci and M. Catarrhalis). - Donors who have had COVID-19 within the last 2 months. - If the donor is positive for Herpes Simplex, CMV or EBV they will be considered unsuitable as a donor for a patient negative for the same pathogen. If the donor is positive for any other pathogen they will be considered unsuitable as a donor entirely. |
| Country | Name | City | State |
|---|---|---|---|
| Australia | Royal Brisbane and Women's Hospital | Brisbane | Queensland |
| Australia | University of Queensland | Brisbane | Queensland |
| Australia | Monash Health | Melbourne |
| Lead Sponsor | Collaborator |
|---|---|
| The University of Queensland | Monash Health, Queensland University of Technology, Royal Brisbane and Women's Hospital |
Australia,
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Cho DY, Hunter RC, Ramakrishnan VR. The Microbiome and Chronic Rhinosinusitis. Immunol Allergy Clin North Am. 2020 May;40(2):251-263. doi: 10.1016/j.iac.2019.12.009. Epub 2020 Jan 16. — View Citation
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Mahdavinia M, Keshavarzian A, Tobin MC, Landay AL, Schleimer RP. A comprehensive review of the nasal microbiome in chronic rhinosinusitis (CRS). Clin Exp Allergy. 2016 Jan;46(1):21-41. doi: 10.1111/cea.12666. — View Citation
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Psaltis AJ, Wormald PJ. Therapy of Sinonasal Microbiome in CRS: A Critical Approach. Curr Allergy Asthma Rep. 2017 Sep;17(9):59. doi: 10.1007/s11882-017-0726-x. — View Citation
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| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Sino-Nasal Outcome Test (SNOT-22) - 22 Item Questionnaire | Change of burden of disease as measured by the SNOT-22 (22 item sinonasal outcome test) questionnaire in patients. Each item graded 0-5. Minimum score 0, Maximum 105 Interpretation: Higher score indicates poorer disease control. |
Week 1 (Day 1) to Week 20 | |
| Secondary | Lund-Kennedy endoscopic assessment score | Change of grading of disease severity using the Lund-Kennedy endoscopy score based on clinical assessment of the middle meatus. 4-item criteria, with score of 0-2 Minimum score: 0, Maximum 8 Interpretation: Higher score indicates a higher degree of disease severity based on clinical assessment. | Week 1 (Day 1) to Week 20 | |
| Secondary | Characterisation of nasal microbiome in study participants | Change in nasal microbiome associated with clinical outcomes such as decrease in presence, absence or abundance of bacterial pathogens. | Week 1 (Day 1) to Week 20 | |
| Secondary | Characterisation of microbiome within effective donors as compared to ineffective donors | Analysis of microbes (bacterial strains, viruses and fungi), and human cell types within donor specimens. | Week 1 (Day 1) - Week 2 (Day 9) | |
| Secondary | Adverse events of Participating Patients | Any adverse event | From the day participating patients give signed consent (2-4 weeks before baseline) until the day of their End of study visit (Up to 33 weeks). | |
| Secondary | Cytokine level - Interleukin 5 or (IL-5) | Change of lL-5 in nasal secretion/swab markers across duration of study. Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). | Week 1 (Day 1) to Week 20 | |
| Secondary | Cytokine level - Interleukin 13 (IL-13) | Change of lL-13 in nasal secretion/swab markers across duration of study. Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). |
Week 1 (Day 1) to Week 20 | |
| Secondary | Cytokine level - Interleukin 2 (IL-2) | Change of lL-2 in nasal secretion/swab markers across duration of study. Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). |
Week 1 (Day 1) to Week 20 | |
| Secondary | Cytokine level - Interleukin 6 (IL-6) | Change of lL-6 in nasal secretion/swab markers across duration of study.Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). |
Week 1 (Day 1) to Week 20 | |
| Secondary | Cytokine level - Interleukin 10 (IL-10) | Change of lL-10 in nasal secretion/swab markers across duration of study.Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). |
Week 1 (Day 1) to Week 20 | |
| Secondary | Cytokine level - Interferon gamma (IFN-?) | Change of IFN-Y in nasal secretion/swab markers across duration of study.Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). |
Week 1 (Day 1) to Week 20 | |
| Secondary | Cytokine level - Interleukin 4 (IL-4) | Change of IL-4 in nasal secretion/swab markers across duration of study.Each cytokine will be quantified using a highly sensitive immunoassay which will use biotinylated antibodies specific to each cytokine to bind the cytokine molecules in the sample. Interactions measured on a flow cytometer and compared against its relevant standard. this will result in a measure of the total concentration of the cytokine in the sample (pg/ml). |
Week 1 (Day 1) to Week 20 |
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