| CTRI Number |
CTRI/2024/12/078211 [Registered on: 17/12/2024] Trial Registered Prospectively |
| Last Modified On: |
|
| Post Graduate Thesis |
No |
| Type of Trial |
Interventional |
|
Type of Study
|
Drug |
| Study Design |
Single Arm Study |
|
Public Title of Study
|
Study to evaluate the Safety and Effectiveness of Withaferin A as a treatment to Prevent GvHD in Transplant Patients
|
|
Scientific Title of Study
|
A Phase I/II trial to assess Safety and Activity of Standardized Withaferin A as GvHD prophylaxis in patients undergoing Matched related donor Hematopoietic stem cell transplant |
| Trial Acronym |
NIL |
|
Secondary IDs if Any
|
| Secondary ID |
Identifier |
| NIL |
NIL |
|
|
Details of Principal Investigator or overall Trial Coordinator (multi-center study)
|
| Name |
Dr Akanksha Chichra |
| Designation |
Associate Professor |
| Affiliation |
Advanced Centre for Treatment, Research and Education in Cancer Tata Memorial Centre |
| Address |
Dept Medical Oncology AHL and BMT Room No.305 ,306 and 307 Shanti sadan OPD building ACTREC Tata Memorial Centre Sector 22, Utsav Chowk CISF Rd Owe Camp, Kharghar
Raigarh
MAHARASHTRA
410210
India |
| Phone |
09004920555 |
| Fax |
|
| Email |
akanksha7@hotmail.com |
|
Details of Contact Person
Scientific Query
|
| Name |
Dr Akanksha Chichra |
| Designation |
Associate Professor |
| Affiliation |
Advanced Centre for Treatment, Research and Education in Cancer Tata Memorial Centre |
| Address |
Dept Medical Oncology AHL and BMT Room No.305 ,306 and 307 Shanti sadan OPD building ACTREC Tata Memorial Centre Sector 22, Utsav Chowk CISF Rd Owe Camp, Kharghar
Raigarh
MAHARASHTRA
410210
India |
| Phone |
09004920555 |
| Fax |
|
| Email |
akanksha7@hotmail.com |
|
Details of Contact Person
Public Query
|
| Name |
Dr Akanksha Chichra |
| Designation |
Associate Professor |
| Affiliation |
Advanced Centre for Treatment, Research and Education in Cancer Tata Memorial Centre |
| Address |
Dept Medical Oncology AHL and BMT Room No.305 ,306 and 307 Shanti sadan OPD building ACTREC Tata Memorial Centre Sector 22, Utsav Chowk CISF Rd Owe Camp, Kharghar
Raigarh
MAHARASHTRA
410210
India |
| Phone |
09004920555 |
| Fax |
|
| Email |
akanksha7@hotmail.com |
|
|
Source of Monetary or Material Support
|
| Indian Council of Medical ResearchV. Ramalingaswami Bhawan, P.O. Box No. 4911
Ansari Nagar, New Delhi 110029 India |
|
|
Primary Sponsor
|
| Name |
ACTREC, Tata Memorial Centre |
| Address |
Advanced Centre for Treatment, Research and Education in Cancer Tata Memorial Centre Sector 22, Utsav Chowk - CISF Rd, Owe Camp, Kharghar, Navi Mumbai, Maharashtra 410210 |
| Type of Sponsor |
Research institution and hospital |
|
|
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 Akanksha Chichra |
ACTREC-Tata Memorial Centre |
Dept Medical Oncology AHL and BMT Room No.305 ,306 and 307 Shanti sadan OPD building Sector 22, Utsav Chowk CISF Rd Owe Camp, Kharghar
Raigarh
MAHARASHTRA |
9004920555
akanksha7@hotmail.com |
|
|
Details of Ethics Committee
|
| No of Ethics Committees= 1 |
| Name of Committee |
Approval Status |
| Tata Memorial Centre Advanced Centre for Treatment, Research and Education in Cancer Institutional Ethics Committee (TMC-IEC III) |
Approved |
|
|
Regulatory Clearance Status from DCGI
|
|
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Health Condition / Problems Studied
|
| Health Type |
Condition |
| Patients |
(1) ICD-10 Condition: C969||Malignant neoplasm of lymphoid, hematopoietic and related tissue, unspecified, |
|
|
Intervention / Comparator Agent
|
| Type |
Name |
Details |
| Comparator Agent |
NA |
NA |
| Intervention |
Standardized Withaferin-A |
SWA will be started from Day +1 to Day +90 in addition to the standard GvHD prophylaxis backbone of calcineurin inhibitor and methotrexate. Following standard dose escalation design, patients will be enrolled at 4 dose levels (500 mg OD, 1000 mg OD, 1500 mg OD and 1500 mg BD). |
|
|
Inclusion Criteria
|
| Age From |
18.00 Year(s) |
| Age To |
80.00 Year(s) |
| Gender |
Both |
| Details |
1.ECOG performance score of 0 or 1
2.Adequate liver function (Total serum bilirubin less than twice upper normal limit or Alanine aminotransferase (ALT) or aspartate aminotransferase (AST) less than 3 fold higher than laboratory upper normal limits)
3.Adequate renal function (creatinine clearance more than 50 ml per min)
4.Adequate cardiac function (LVEF more than 40 percent)
5.Women of childbearing potential must have a negative pregnancy test done within 7 days prior to registration.
6.Signed, written informed consent
|
|
| ExclusionCriteria |
| Details |
1.Known hypersensitivity or contraindications against Withaferin A.
2.Presence of an active uncontrolled infection defined as hemodynamic instability attributable to sepsis or new symptoms, worsening physical signs, or radiographic findings attributable to infection.
3.Any medical or psychiatric illness which precludes the participant from giving informed consent
4.Pregnancy, lactation, or inadequate contraception
|
|
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Method of Generating Random Sequence
|
Not Applicable |
|
Method of Concealment
|
Not Applicable |
|
Blinding/Masking
|
Open Label |
|
Primary Outcome
|
| Outcome |
TimePoints |
Phase 1
1.Safety and tolerability of oral SWA in patients undergoing hematopoietic stem cell transplant (by assessment of more than 3toxicity by CTCAE version 5 and PRO-CTCAE version 1.
2.To study the clinical pharmacokinetics of standardized Withaferin-A and establish recommended Phase II dose (RP2D).
Phase 2
1.To determine the activity of WA in GvHD prophylaxis. (by assessing the cumulative incidence of clinically significant (Grade 2 to 4) aGvHD at Day 100)
|
Phase 1 90 days
Phase 2 100 days
|
|
|
Secondary Outcome
|
| Outcome |
TimePoints |
1.To evaluate the cumulative incidence of severe aGvHD (grade 3-4) at Day 100 and Day 180.
2.To evaluate the GvHD free- and relapse free- survival (GRFS) rate at 1 year post transplant.
3.To study the incidence of chronic GvHD at 1 year post transplant.
4.To study engraftment kinetics.
5.To study the non-relapse mortality at 1 year post transplant.
6.To study the overall survival (OS) at 1 year post transplant.
|
at Day 100 and Day 180, 1 year |
|
|
Target Sample Size
|
Total Sample Size="54"
Sample Size from India="54"
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 1/ Phase 2 |
|
Date of First Enrollment (India)
|
30/12/2024 |
| 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="5"
Months="0"
Days="0" |
|
Recruitment Status of Trial (Global)
|
Not Applicable |
| Recruitment Status of Trial (India) |
Not Yet Recruiting |
|
Publication Details
|
N/A |
|
Individual Participant Data (IPD) Sharing Statement
|
Will individual participant data (IPD) be shared publicly (including data dictionaries)?
Response - NO
|
|
Brief Summary
|
What
is acute Graft versus host disease (aGvHD)? GvHD is a complication that can
occur after an allogeneic stem cell transplant resulting in damage to some
organs. The death rate of GvHD patients is 15-40%. In GvHD, the donated
peripheral blood stem cells or bone marrow view the recipient’s body as
foreign, and the donated cells/bone marrow harm the body. aGvHD usually
develops in skin, liver or gastrointestinal tract, and symptoms might appear
within few weeks after transplant. Symptoms of acute GvHD are observed as skin
rash or reddened areas on the skin, yellow discoloration of the skin and/or
eyes, and abnormal blood test results, nausea, vomiting, diarrhea, or abdominal
cramping.
What
is the current prevention used for GvHD?
To prevent development of GvHD many standard drugs like cyclosporine
(CSA), tacrolimus (TAC), methotrexate (MTX), mycophenolate mofetil (MMF),
rapamycin and cyclophosphamide are given.
What is standardized
Withaferin-A (SWA)? Withaferin-A (WA) is the
main active component of Withania
somnifera (Ashwagandha). It has been shown in many studies to have
properties of healing and immune-modulation (improving the immune system).
Studies have been done in our Clinical Pharmacology Laboratory that have shown
a significant beneficial effect of this drug, when added to the standard drugs
used for prophylaxis of GvHD, on reducing the risk of acute GvHD. The drug has
also been tested and proven to be very safe in humans.
What
is the rationale of this trial? As has been described earlier, GvHD is a difficult
complication of allogeneic stem cell transplant which can lead to increased
hospital stay and deaths post-transplant. The standard drugs for prevention of
GvHD are cyclosporine (CSA), tacrolimus (TAC), methotrexate (MTX),
mycophenolate mofetil (MMF), rapamycin and cyclophosphamide. These drugs also
have some side effects during the course of transplant. This points out the
need for new preventive drugs that are safe and effective.
SWA
is an oral formulation of WA which seems to be beneficial in the early studies
done in the Clinical Pharmacology Laboratory, ACTREC. SWA has also been found
to be safe at very high doses.
SWA
will be given along with the standard drugs given to prevent GvHD. Despite of
consuming these drugs, about 40 – 60% patients still develop GvHD. We aim to
add SWA to these standard drugs during transplant to reduce significant aGvHD.
How
will SWA be given? Patients
who agree to participate in this trial and are found to be eligible will be
given SWA as a capsule at a dose of 500 mg/day (2 capsules of 250 mg) to 3000
mg/day (6 capsules of 250 mg) as per the dose level allotted to the patient.
The drug will be given for a total duration 90 days starting from Day +1 of
transplant. All other standard treatments which are part of a transplant
procedure will be carried out without any change.
Participants will be
monitored clinically for any adverse events and followed up as per standard
protocols post-transplant.
What
additional tests will be carried out? Additional blood
sampling to study the levels of the drug WA blood samples will be collected at
0, 1, 2, 4, 8 hours on the day of start of SWA (Day +1) and Day +7. Checking immune
cell profile and cytokines (which are markers of - immunity levels) will be
done at Day+30, Day +90, Day+180, Day+365 from the start of SWA which is also
the part of routine care. Blood sample of 5 ml will also be
taken at Day 0, Day +14, Day +30, Day +60 and Day +90 after start of drug to
see level of some special protein called JAK2 STAT3 protein.
What
are the risks involved in participation? According to available literature
and information, SWA is a safe and well tolerated drug. In a phase 1 study,
Standardized Withaferin-A was administered to patients with advanced stage
osteosarcoma. The drug was well tolerated by patients up to a dose of 4800 mg.
No severe side effects were observed. Increase in liver enzymes and skin rash were the
most common side effects. Other side effects included fatigue, fever, swelling,
and diarrhea.
What is the
possible impact of this trial? If indeed SWA works and prevents GvHD
effectively then this could be a breakthrough in treatment. It would help many
patients to prevent GvHD post allogeneic stem cell transplant and would be a
safe, easily available, inexpensive and oral drug for the same. This possibly
could benefit and help future patients who undergo bone marrow transplant (BMT)
to have better chances of survival and reduce their financial burden.
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