Chronic Myeloid Leukemia Clinical Trial
Official title:
Autologous Cytokine Induced Killer Cells as Adjuvant Adoptive Immunotherapy in Patients With Chronic Myeloid Leukemia on Standard Drug Therapy
This is an extension of our ongoing clinical trial using ex vivo expanded autologous
Cytokine-induced killer (CIK) cells as an adoptive cellular immunotherapy for haematological
malignancies. The pre-existing clinical trial targets patient with acute myeloid leukemia or
MDS, and relapsed disease post allogeneic transplant.
Chronic myeloid leukemia (CML) is a disease with good response to kinase inhibitors. There
are however patients in transformed phase of the disease who do not respond to these
treatment. A small proportion of patients with response to Imatinib may develop mutations
resulting in drug resistance. In addition, the vast majority of patients with a good
response to the kinase inhibitors still have persistent CML cells detectable at a molecular
level. It is known that the CML progenitors are not sensitive to the kinase inhibitors. On
the other hand, immune mediated mechanism is known to be able to eradicate CML as shown by
efficacy of donor lymphocyte infusion in the allogeneic transplant setting. Early clinical
trials have shown clearance of bcr-abl using peptide vaccination. There is also convincing
mouse data showing eradication of CML at molecular level by autologous CIK cells, but no
clinical trial has been done using CIK cells for CML.
We therefore plan to expand our current CIK trial to include CML as a disease, for CML
patients with various degree of response to the kinase inhibitors which have already offered
its maximal effect. We aim to study whether autologous CIK cells may further improve disease
response, either in the eradiation of minimal residual disease, or in conjunction with
chemotherapy for control of high tumour load disease.
Patients with CML falls into various groups based on their disease stage and response to
kinase inhibitors. In the context of currently available kinase inhibitors, allogeneic
transplant and the various available new drug trials, there are still some patients who will
not achieve a satisfactory or sustainable response. For such patients, we aim to employ CIK
cell as an immunotherapeutic modality concurrent with their original CML-specific therapy.
This will enable us to explore any additional activity of CIK cells against CML without any
compromise to their ongoing, established treatment.
The following groups of patients are potential candidates:
1. Blast crisis / accelerated phase patients who have failed to response to the kinase
inhibitors but are fit to undergo induction chemotherapy as for the acute leukemia.
Repeated cycles of CIK will be given in phase with the planned chemotherapy cycles, to
observe for achievement of any remission and its durability.
2. Blast crisis / accelerated phase patients who have achieved a haematological or
cytogenetic response to the kinase inhibitors, but do not have further definitive
curative options eg allogeneic transplant. In the absence of long term data with
Dasatinib or Nilotinib , it is justifiable to study the efficacy of addition of CIK
therapy to their baseline best response achievable with drug therapy.
3. Patients with resistance to the currently available kinase inhibitors due to T315I
mutation or other undefined mutations, with progressive relapse either at molecular,
cytogenetic or haematological level, and do not have transplant as a curative option.
In this group of patients additional of CIK to current treatment will show any activity
of CIK against the drug-resistant mutant CML cells.
4. Patients who have achieved a stable but residual molecular evidence of CML, who are
willing to explore additional means with a hope to eradication of MRD. Since the role
of immunotherapy is most relevant in MRD, CIK infusion will provide the proof of
principal observation of whether imatinib-resistant CML Philadelphia stem cells can be
eradicated by these ex vivo activated and expanded cytotoxic T cells.
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