Tuberculosis Clinical Trial
Official title:
Efficacy and Safety of Cyclophosphamide in the Treatment of Refractory Proliferative Arachnoiditis in Central Nervous System Tuberculosis- A Randomized Double Blinded Placebo Controlled Trial
Tubercular meningitis occurs in around 10% of those with extrapulmonary tuberculosis and is a major cause of mortality and morbidity. Inspite of effective Anti-tubercular drugs, still around 30% of patients develop complications due to arachnoiditis such as spinal tubercular radiculomyelitis, optico-chiasmatic arachnoiditis, development of new tuberculomas after starting therapy etc. which are probably immune mediated inflammatory responses due to paradoxical reaction to ATT. The management of arachnoiditis is far from satisfactory. High dose methylprednisolone, intrathecal hyaluronic acid, thalidomide have been tried in small case series and case reports. However, the results have not been satisfactory. There are two published reports of cyclophosphamide usage in TBM related vasculitis and stroke The investigators tried cyclophosphamide in four patients after consent, and found remarkable improvement in all of them. (Under peer review) In order to test this hypothesis, a randomized controlled trial is needed.
Status | Not yet recruiting |
Enrollment | 40 |
Est. completion date | December 31, 2024 |
Est. primary completion date | December 31, 2023 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 14 Years to 60 Years |
Eligibility | Inclusion Criteria: - Patients attending Neurology/Pulmonary Medicine/Medicine/Geriatric Medicine OPD/admitted in respective wards with proliferative tubercular arachnoiditis refractory to corticosteroids and standard Anti-tubercular drugs for CNS tuberculosis - Atleast 14 years of age of all sexes - Not more than 60 years of age at time of enrolment - Patient was started on ATT for tubercular meningitis and had clearcut clinical improvement with resolution of fever/constitutional symptoms AND improvement in headache, vomiting and sensorium for atleast 10 days following which there is deterioration again due to arachnoiditis - Developed paraparesis/quadriparesis/sphincter dysfunction due to spinal radiculomyelitis or vision loss due to due to optico-chiasmatic arachnoiditis with imaging evidence of arachnoiditis - Has received standard ATT for atleast 3 months with adequate dose and compliance - Received corticosteroids for treatment of arachnoiditis and deemed to be refractory to corticosteroids by the primary physician treating the patient - MRI brain and spine are suggestive of Arachnoiditis - CSF GeneXpert/Line Probe assay/cultures are not suggestive of drug resistant tuberculosis - Reasonable clinical certainty OR allied investigations such as CECT chest/abdomen/PET CT ruling out drug resistant tuberculosis - Other relevant investigations like CSF analysis not suggestive of alternative diagnosis such as cysticercal/ cryptococcal/other fungal infections/other causes of chronic meningitis such as brucella/ nocardia/ syphilis/recurrent viral meningitis/ carcinomatous/ lymphomatous meningitis or non infective causes such as sarcoidoisis/sub-arachnoid hemorrhage etc. - Willing to undergo periodic assessment clinically and with MRI. - Ready to provide consent for cyclophosphamide therapy - Willing to adhere to protocol and comply with follow up visits Exclusion Criteria: - Not willing to provide consent - Not willing to adhere to protocol - Developed significant drug induced liver dysfunction so that patient is not being given Rifampicin, INH or pyrazinamide and is on modified ATT including quinolones, ethambutol and aminoglycosides or second line drugs only in the absence of Rifampicin and INH - Drug resistant tubeculosis - Men and Women of childbearing potential who are not using adequate contraception or women who are pregnant and lactating - Patients who are on immunosuppressants such as cyclophosphamide/ azathioprine/ methotrexate/MMF/ calcineurin inhibitors for autoimmune conditions/post transplantation or chemotherapy for any systemic malignancy - HBsAg, HIV serology and anti HCV positive - Having life threatening infections such as pneumonia/urosepsis - Patients who have developed large artery strokes with significant brain parenchymal damage - Patients with expected life expectancy less than 1 year due to primary disease or comorbidity based on clinical prediction scores for specific disease - Patients with systemic malignancy within the last 5 years - Known allergy to cyclophosphamide or its preservatives/excipients - Receiving cyclophosphamide for any indication in the last 12 weeks - Gross hematuria prior to enrolment to the study/USG features of hemorrhagic cystitis - Cytopenias Hct <25%, TLC<4000/mm3 or Platelet count <1,20,000/mm3 at the time of enrolment - Alanine amino transferase (ALT) > 3 upper limit of normal at time of enrolment |
Country | Name | City | State |
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n/a |
Lead Sponsor | Collaborator |
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All India Institute of Medical Sciences, New Delhi |
Celotti A, Vianello F, Sattin A, Malipiero G, Faggin R, Cattelan A. Cyclophosphamide immunomodulation of TB-associated cerebral vasculitis. Infect Dis (Lond). 2018 Oct;50(10):779-782. doi: 10.1080/23744235.2018.1467038. Epub 2018 Apr 28. — View Citation
Gonzalez-Duarte A, Higuera-Calleja J, Flores F, Davila-Maldonado L, Cantú-Brito C. Cyclophosphamide treatment for unrelenting CNS vasculitis secondary to tuberculous meningitis. Neurology. 2012 Apr 17;78(16):1277-8. doi: 10.1212/WNL.0b013e318250d84a. Epub 2012 Apr 4. — View Citation
Goyal V, Elavarasi A, Abhishek, Shukla G, Behari M. Practice Trends in Treating Central Nervous System Tuberculosis and Outcomes at a Tertiary Care Hospital: A Cohort Study of 244 Cases. Ann Indian Acad Neurol. 2019 Jan-Mar;22(1):37-46. doi: 10.4103/aian.AIAN_70_18. — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Functional independece at 6 months | To compare the proportion of patients who attain functional independence (mRS-modified Rankin scale 0-2) 6 months after cyclophosphamide therapy for proliferative arachnoiditis refractory to corticosteroids and standard Anti-tubercular therapy in CNS tuberculosis to those who receive placebo. | 6 months | |
Secondary | Independent ambulation | To compare the proportion of patients who attain independent ambulation 6 months after cyclophosphamide therapy for proliferative arachnoiditis refractory to corticosteroids and standard Anti-tubercular therapy in CNS tuberculosis to those who receive placebo. | 6 months | |
Secondary | Improvement in modified Rankin scale | To compare the proportion of patients improving from mRS =3 to mRS =2 six months post cyclophosphamide therapy | 6 months | |
Secondary | Improvement in visual acuity (1) | To compare the proportion of patients who attain atleast 2 points improvement on Snellen's chart in visual acuity 6 months after cyclophosphamide therapy for proliferative arachnoiditis refractory to corticosteroids and standard Anti-tubercular therapy in CNS tuberculosis to those who receive placebo. | 6 months | |
Secondary | Improvement in visual acuity (2) | To compare proportion of patients who attain atleast two point improvement on a semiquantitative visual acuity measurement in those who have visual acuity less than 1/60 on snellen's chart (finger counting at 1 m, hand movements at 1 m, perception of light, no perception of light considered as discrete points below 1/60 vision on standard Snellen's chart) 6 months after cyclophosphamide therapy | 6 months | |
Secondary | Improvement in visual acuity (3) | To compare proportion of patients improving from visual acuity of <3/60 in the better eye to 3/60 or more 6 months post cyclophosphamide therapy | 6 months | |
Secondary | Improvement in sphincter function | To compare the proportion of patients who attain improvement in bladder/bowel function 6 months after cyclophosphamide therapy for proliferative arachnoiditis refractory to corticosteroids and standard Anti-tubercular therapy in CNS tuberculosis to those who receive placebo.. | 6 months | |
Secondary | Change in mRS | Shift analysis pre-and 6 months post therapy in terms of change in mRS | 6 months | |
Secondary | Patient well being | Comparing Global patient well being as assessed by SF-36 pre and 6 months post cyclophosphamide therapy | 6 months | |
Secondary | Life threatening infections | Occurrence of life threatening infections necessitating cessation of therapy upto 3 months post cyclophosphamide therapy | 3 months | |
Secondary | Infections needing hospitalization | Occurrence of infections needing hospitalization or intravenous antibiotic/antiviral/anti-fungal therapy upto 3 months post cyclophosphamide therapy | 3 months | |
Secondary | Flare up of TB | Flare up of underlying tuberculosis upto 3 months post cyclophosphamide therapy | 3 months | |
Secondary | Cytopenias | Occurrence of Grade III cytopenias defined as per common terminology criteria for adverse events v 5.0 upto 6 weeks post cyclophosphamide therapy | 6 weeks | |
Secondary | Transaminitis | Grade III transaminitis as per CTCAE v 5.0 upto 6 weeks post cyclophosphamide therapy | 6 weeks | |
Secondary | Hemorrhagic cystitis | Occurrence of hemorrhagic cystitis upto 2 weeks post cyclophosphamide therapy | 2 weeks | |
Secondary | Adverse effects | Any other significant adverse effect | 3 months |
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