| CTRI Number |
CTRI/2021/04/033214 [Registered on: 28/04/2021] Trial Registered Prospectively |
| Last Modified On: |
03/11/2023 |
| Post Graduate Thesis |
No |
| Type of Trial |
Interventional |
|
Type of Study
|
Drug |
| Study Design |
Single Arm Study |
|
Public Title of Study
|
Leflunomide for musculoskeletal GVHD after allogeneic stem cell transplant |
|
Scientific Title of Study
|
Pilot study of leflunomide as first line therapy for musculoskeletal GVHD |
| Trial Acronym |
|
|
Secondary IDs if Any
|
| Secondary ID |
Identifier |
| NIL |
NIL |
|
|
Details of Principal Investigator or overall Trial Coordinator (multi-center study)
|
| Name |
Sachin Punatar |
| Designation |
Associate Professor |
| Affiliation |
Tata Memorial Centre |
| Address |
Room 211, Stem cell transplant unit OPD,
Department of Medical Oncology
Paymaster Shodhika,
ACTREC, Tata Memorial Centre,
Kharghar, Navi Mumbai
Raigarh
MAHARASHTRA
410210
India |
| Phone |
|
| Fax |
|
| Email |
drsachin_punatar@yahoo.in |
|
Details of Contact Person
Scientific Query
|
| Name |
Sachin Punatar |
| Designation |
Associate Professor |
| Affiliation |
Tata Memorial Centre |
| Address |
Room 211, Stem cell transplant unit OPD,
Department of Medical Oncology
Paymaster Shodhika,
ACTREC, Tata Memorial Centre,
Kharghar, Navi Mumbai
Raigarh
MAHARASHTRA
410210
India |
| Phone |
|
| Fax |
|
| Email |
drsachin_punatar@yahoo.in |
|
Details of Contact Person
Public Query
|
| Name |
Sachin Punatar |
| Designation |
Associate Professor |
| Affiliation |
Tata Memorial Centre |
| Address |
Room 211, Stem cell transplant unit OPD,
Department of Medical Oncology
Paymaster Shodhika,
ACTREC, Tata Memorial Centre,
Kharghar, Navi Mumbai
Raigarh
MAHARASHTRA
410210
India |
| Phone |
|
| Fax |
|
| Email |
drsachin_punatar@yahoo.in |
|
|
Source of Monetary or Material Support
|
| Tata Memorial Centre
ACTREC, Kharghar, Navi Mumbai 410210 |
|
|
Primary Sponsor
|
| Name |
Dr Sachin Punatar |
| Address |
ACTREC,
Tata Memorial Centre, Kharghar,
Navi Mumbai 410210 |
| Type of Sponsor |
Other [] |
|
|
Details of Secondary Sponsor
|
|
|
Countries of Recruitment
|
India |
|
Sites of Study
|
| No of Sites = 1 |
| Name of Principal
Investigator |
Name of Site |
Site Address |
Phone/Fax/Email |
| Dr Sachin Punatar |
Tata Memorial Centre |
Room 211, Stem cell transplant unit OPD, Department of Medical Oncology, ACTREC, Tata Memorial Centre, Kharghar, Navi Mumbai
Raigarh
MAHARASHTRA |
02227405096
drsachin_punatar@yahoo.in |
|
|
Details of Ethics Committee
|
| No of Ethics Committees= 1 |
| Name of Committee |
Approval Status |
| TMC IEC - III |
Approved |
|
|
Regulatory Clearance Status from DCGI
|
|
|
Health Condition / Problems Studied
|
| Health Type |
Condition |
| Patients |
(1) ICD-10 Condition: M95-M95||Other disorders of the musculoskeletal system and connective tissue, |
|
|
Intervention / Comparator Agent
|
| Type |
Name |
Details |
| Intervention |
Leflunomide |
Leflunomide will be given at standard dose (100 mg OD x 3 days followed by 20 mg OD) in adults and weight based dose in children |
| Comparator Agent |
Not applicable |
Not applicable |
|
|
Inclusion Criteria
|
| Age From |
0.00 Year(s) |
| Age To |
65.00 Year(s) |
| Gender |
Both |
| Details |
1. Willing to give written informed consent
2. Patients diagnosed with musculoskeletal mGvHD based on 2014 NIH consensus criteria (with diagnosis confirmed by biopsy only if clinically required).
3. Willing and able to comply with all study requirements, including treatment, and periodic assessments.
|
|
| ExclusionCriteria |
| Details |
1. Patients with known hypersensitivity to leflunomide especially previous Steven Johnson syndrome, toxic epidermal necrolysis after leflunomide.
2. Pregnant females
3. Patients with musculoskeletal manifestations explained by other potential causes (drugs, trauma, etc).
4. Patients with calculated GFR <30ml/min at the time of screening.
|
|
|
Method of Generating Random Sequence
|
Not Applicable |
|
Method of Concealment
|
Not Applicable |
|
Blinding/Masking
|
Not Applicable |
|
Primary Outcome
|
| Outcome |
TimePoints |
| Overall objective response rate |
At any time following start of intervention |
|
|
Secondary Outcome
|
| Outcome |
TimePoints |
| Time to response |
Time from start of leflunomide to attainment of any response |
| Time to best response |
Time from start of leflunomide to the best response |
| Duration of response |
Time from first response to relapse or progression of musculoskeletal GVHD |
| Relapse rate |
Proportion of patients relapsing after attaining a response |
|
|
Target Sample Size
|
Total Sample Size="10"
Sample Size from India="10"
Final Enrollment numbers achieved (Total)= "Applicable only for Completed/Terminated trials"
Final Enrollment numbers achieved (India)="Applicable only for Completed/Terminated trials" |
|
Phase of Trial
|
Phase 2 |
|
Date of First Enrollment (India)
|
03/05/2021 |
| Date of Study Completion (India) |
Applicable only for Completed/Terminated trials |
| Date of First Enrollment (Global) |
Date Missing |
| Date of Study Completion (Global) |
Applicable only for Completed/Terminated trials |
|
Estimated Duration of Trial
|
Years="2"
Months="0"
Days="0" |
Recruitment Status of Trial (Global)
Modification(s)
|
Not Applicable |
| Recruitment Status of Trial (India) |
Open to Recruitment |
|
Publication Details
|
Nil |
|
Individual Participant Data (IPD) Sharing Statement
|
Will individual participant data (IPD) be shared publicly (including data dictionaries)?
Response - NO
|
|
Brief Summary
|
The curative potential of allogeneic hematopoietic stem cell transplantation (allo-HCT) is hampered by acute and chronic graft-versus-host disease (GVHD). Although chronic GVHD (cGVHD) can affect any organ / system in the body, commonly affected are skin, oral cavity, eyes, liver, joints and fascia, and lungs. Involvement of these can occur alone or concurrently, and these lead to a significant negative impact on the patient’s quality of life. Musculoskeletal involvement in chronic GVHD (mGVHD) can have varied presentations like fasciitis, myositis, arthritis, etc. The basic pathogenesis of mGvHD closely mimics autoimmune disorders like rheumatoid arthritis, systemic sclerosis, systemic lupus, etc.
The treatment goals of mGvHD include improvement or stabilisation of manifestations, limitation of long-term treatment related toxicities, improvement in functional capacity and quality of life. Corticosteroids, the standard frontline treatment, are typically administered for a median of 2 to 3years, leading to substantial morbidity. An effort to decrease corticosteroid doses has led to their use in combination with other drugs, such as cyclosporine, tacrolimus, sirolimus, mycophenolate mofetil, rituximab, etanarcept, ruxulotinib, imatinib, ibrutinib, ECP (extra corporeal photopheresis), methotrexate etc, in frontline or second-line settings. All these drugs have been used with far and few responses but with significant treatment related toxicity and costs. As far as musculoskeletal GVHD is concerned, the British guidelines recommend corticosteroids as first line treatment and rituximab as second line option. However, the morbidity associated with long term steroid use warrants a quest for use of non-steroid therapies to be used in 1st line setting for chronic GVHD. Leflunomide has been used in rheumatoid arthritis. At our centre, we have previously used leflunomide for patients with musculoskeletal GVHD and found it to be effective and safe. Leflunomide is relatively cheap and potentially more effective compared to other more expensive alternatives. If proven to be effective in a larger cohort of patients, this drug could become the standard first line agent in this setting.
With this, we have planned to carry out this study to assess the efficacy of leflunomide in musculoskeletal GVHD post allogeneic stem cell transplant. |