UCDCC#269: A Pilot Study of Interlesional IL-2 and RT in Patients With NSCLC.
| Status: | Recruiting |
|---|---|
| Conditions: | Lung Cancer, Lung Cancer, Cancer |
| Therapuetic Areas: | Oncology |
| Healthy: | No |
| Age Range: | 18 - Any |
| Updated: | 3/27/2019 |
| Start Date: | August 11, 2017 |
| End Date: | July 30, 2020 |
| Contact: | Kristy Lundahl, MS |
| Email: | krlundahl@ucdavis.edu |
| Phone: | 720-270-9458 |
UCDCC#269: A Pilot Study of Interlesional IL-2 and Hypofractionated Radiotherapy in Patients With Metastatic Non-small Cell Lung Cancer Who Are Refractory to PD 1 / PD L1 Blockade.
The advent of checkpoint blockade immunotherapy has revolutionized the management of
metastatic non-small cell lung cancer (NSCLC). Despite the promising evidence for deep and
durable responses with these agents the majority of patients fail to respond. The
investigators hypothesize that a novel strategy combining radiotherapy and intralesional
interleukin-2 (IL-2), a signaling molecule and member of the cytokine family involved in the
activation of leukocytes and lymphocytes, may overcome resistance to checkpoint blockade
therapy and offer significant clinical benefit to patients who fail to respond to checkpoint
blockade alone. The investigators propose a microtrial testing the feasibility of a bold
combinatorial immunotherapy strategy consisting of radiotherapy (RT), intralesional IL-2, and
check-point blockade for metastatic non-small cell lung cancer patients who have progressed
after checkpoint inhibition. IL-2 can upregulate PD-1 expression and activate T-cells.
metastatic non-small cell lung cancer (NSCLC). Despite the promising evidence for deep and
durable responses with these agents the majority of patients fail to respond. The
investigators hypothesize that a novel strategy combining radiotherapy and intralesional
interleukin-2 (IL-2), a signaling molecule and member of the cytokine family involved in the
activation of leukocytes and lymphocytes, may overcome resistance to checkpoint blockade
therapy and offer significant clinical benefit to patients who fail to respond to checkpoint
blockade alone. The investigators propose a microtrial testing the feasibility of a bold
combinatorial immunotherapy strategy consisting of radiotherapy (RT), intralesional IL-2, and
check-point blockade for metastatic non-small cell lung cancer patients who have progressed
after checkpoint inhibition. IL-2 can upregulate PD-1 expression and activate T-cells.
The advent of checkpoint blockade immunotherapy has revolutionized the management of
metastatic non-small cell lung cancer (NSCLC). Despite the promising evidence for deep and
durable responses with these agents the majority of patients fail to respond. The
investigators hypothesize that a novel strategy combining radiotherapy and intralesional
interleukin-2 (IL-2), a signaling molecule and member of the cytokine family involved in the
activation of leukocytes and lymphocytes, may overcome resistance to checkpoint blockade
therapy and offer significant clinical benefit to patients who fail to respond to checkpoint
blockade alone. The investigators propose a microtrial testing the feasibility of a bold
combinatorial immunotherapy strategy consisting of radiotherapy (RT), intralesional IL-2, and
check-point blockade for metastatic non-small cell lung cancer patients who have progressed
after checkpoint inhibition. IL-2 can upregulate PD-1 expression and activate T-cells. There
is data supporting combination therapies with IL-2 and checkpoint blockade, IL-2 and
radiotherapy, and checkpoint blockade and radiotherapy but clinical data is limited and the
triple combination has never been tested. IL-2 + checkpoint blockade was recently tested in a
small clinical trial and showed promising results but RT was not included in this trial. As
outlined above RT has been demonstrated to increase the efficacy of both IL-2 and checkpoint
blockade. The investigators believe that the triple combination of radiotherapy + IL-2 +
checkpoint inhibition will be highly effective as RT + IL-2 can serve highly activate the
immune system and checkpoint blockade can reverse the immune suppressive pathways induced by
tumor and therapy. The investigators hypothesize that the combination of intralesional IL-2
with radiotherapy will act as an "in-situ" vaccine inducing an anti-tumor immune response.
The investigators further hypothesize that this vaccine effect will convert patients with
primary or secondary resistance to checkpoint blockade into responders since one mechanism of
resistance to checkpoint blockade appears to be lack of a pre-existing anti-tumor immune
response. The primary endpoint is tolerability, safety and toxicity. Exploratory endpoints
include abscopal response rate, objective response rate, disease control rate, progression
free survival, and correlative studies. This trial will incorporate robust correlative assays
to provide insights into mechanisms of resistance to checkpoint blockade and how this therapy
may overcome that resistance. This trial, although small, has the potential to drastically
advance both our understanding and treatment of metastatic lung cancer.
This is a pilot phase I study that will evaluate the safety and toxicity of this
combinatorial approach. Eligible patients with NSCLC who fail to respond to PD1/PDL1
checkpoint blockade will be enrolled. Patients will continue on checkpoint blockade and
receive intralesional IL-2 in combination with hypofractionated radiotherapy. Radiotherapy
will be delivered to the treatment lesion during the first week of therapy using an 8 Gy x 3
fractions palliative regimen. Fractions may be delivered on consecutive or every other day
but must be completed during week 1 and will not be repeated in future cycles. Immune
checkpoint blockade will be started on week 1 day 1, concurrent with radiotherapy and
continue with cycles every 2 (nivolumab) or 3 (pembrolizumab) weeks. A total of four
Interleukin-2 treatments will be delivered into the treatment lesion by intralesional
injections twice weekly starting 24-72 hours after the completion of radiotherapy and to be
completed no later than study Day 21. Intralesional injections will be performed by palpation
of the lesion or under ultrasound or CT guidance as indicated. Intralesional IL-2 injections
will follow guidelines, which we have previously published. Briefly, each patient will
receive an initial test dose of 3 x 106 IU of IL-2, which will be escalated to 7 x 106 for
the second treatment and then 15 x 106 IU for the final two treatments as tolerated. If a
dose level is not tolerated the treatment will be de-escalated to previous dose levels for
subsequent treatments. If 3 million IU IL-2 is not tolerated the dose can be de-escalated to
1 million IU IL-2. If 1 million IU IL-2 is not tolerated the treatment will be deemed
intolerable and patient removed from study.
metastatic non-small cell lung cancer (NSCLC). Despite the promising evidence for deep and
durable responses with these agents the majority of patients fail to respond. The
investigators hypothesize that a novel strategy combining radiotherapy and intralesional
interleukin-2 (IL-2), a signaling molecule and member of the cytokine family involved in the
activation of leukocytes and lymphocytes, may overcome resistance to checkpoint blockade
therapy and offer significant clinical benefit to patients who fail to respond to checkpoint
blockade alone. The investigators propose a microtrial testing the feasibility of a bold
combinatorial immunotherapy strategy consisting of radiotherapy (RT), intralesional IL-2, and
check-point blockade for metastatic non-small cell lung cancer patients who have progressed
after checkpoint inhibition. IL-2 can upregulate PD-1 expression and activate T-cells. There
is data supporting combination therapies with IL-2 and checkpoint blockade, IL-2 and
radiotherapy, and checkpoint blockade and radiotherapy but clinical data is limited and the
triple combination has never been tested. IL-2 + checkpoint blockade was recently tested in a
small clinical trial and showed promising results but RT was not included in this trial. As
outlined above RT has been demonstrated to increase the efficacy of both IL-2 and checkpoint
blockade. The investigators believe that the triple combination of radiotherapy + IL-2 +
checkpoint inhibition will be highly effective as RT + IL-2 can serve highly activate the
immune system and checkpoint blockade can reverse the immune suppressive pathways induced by
tumor and therapy. The investigators hypothesize that the combination of intralesional IL-2
with radiotherapy will act as an "in-situ" vaccine inducing an anti-tumor immune response.
The investigators further hypothesize that this vaccine effect will convert patients with
primary or secondary resistance to checkpoint blockade into responders since one mechanism of
resistance to checkpoint blockade appears to be lack of a pre-existing anti-tumor immune
response. The primary endpoint is tolerability, safety and toxicity. Exploratory endpoints
include abscopal response rate, objective response rate, disease control rate, progression
free survival, and correlative studies. This trial will incorporate robust correlative assays
to provide insights into mechanisms of resistance to checkpoint blockade and how this therapy
may overcome that resistance. This trial, although small, has the potential to drastically
advance both our understanding and treatment of metastatic lung cancer.
This is a pilot phase I study that will evaluate the safety and toxicity of this
combinatorial approach. Eligible patients with NSCLC who fail to respond to PD1/PDL1
checkpoint blockade will be enrolled. Patients will continue on checkpoint blockade and
receive intralesional IL-2 in combination with hypofractionated radiotherapy. Radiotherapy
will be delivered to the treatment lesion during the first week of therapy using an 8 Gy x 3
fractions palliative regimen. Fractions may be delivered on consecutive or every other day
but must be completed during week 1 and will not be repeated in future cycles. Immune
checkpoint blockade will be started on week 1 day 1, concurrent with radiotherapy and
continue with cycles every 2 (nivolumab) or 3 (pembrolizumab) weeks. A total of four
Interleukin-2 treatments will be delivered into the treatment lesion by intralesional
injections twice weekly starting 24-72 hours after the completion of radiotherapy and to be
completed no later than study Day 21. Intralesional injections will be performed by palpation
of the lesion or under ultrasound or CT guidance as indicated. Intralesional IL-2 injections
will follow guidelines, which we have previously published. Briefly, each patient will
receive an initial test dose of 3 x 106 IU of IL-2, which will be escalated to 7 x 106 for
the second treatment and then 15 x 106 IU for the final two treatments as tolerated. If a
dose level is not tolerated the treatment will be de-escalated to previous dose levels for
subsequent treatments. If 3 million IU IL-2 is not tolerated the dose can be de-escalated to
1 million IU IL-2. If 1 million IU IL-2 is not tolerated the treatment will be deemed
intolerable and patient removed from study.
Inclusion Criteria:
1. Adults ≥18 years of age with histologically proven NSCLC.
2. Failure to respond to standard of care checkpoint blockade therapy or previously
responding patients who progress on checkpoint blockade therapy.
3. ECOG (Eastern Cooperative Oncology Group) performance status score of 0 - 2 (Appendix
1)
4. Presence of a candidate treatment lesion (subcutaneous or nodal lesions are preferable
but visceral lesions will be considered) accessible and safe for radiotherapy and
serial intralesional injections.
5. Presence of at least one target lesion (distinct from treatment lesion and outside of
treatment lesion radiation field) evaluable for response by RECIST 1.1
6. Life expectancy ≥ 6 months
7. The following laboratory results obtained within 14 days of the first study treatment:
- ANC > 1500 cells/ul
- WBC count > 2500/uL
- Lymphocyte count >500/uL
- Platelet count > 100,000/uL
- Hemoglobin > 9 g/dL
8. Liver function tests meeting one of the following criteria:
- AST and ALT < 2.5 x ULN with alkaline phosphatase < 2.5 x ULN OR
- AST and ALT < 1.5 x ULN, with alkaline phosphatase > 2.5 x ULN
9. Serum bilirubin ≤ 1.0 x ULN.
10. INR and aPTT ≤ 1.5 x ULN.
11. Creatinine clearance > 30 mL/min by Cockcroft-Gault formula.
12. No other active malignancy.
13. For female patients of childbearing potential and male patients with partners of
childbearing potential agreement (by patient and/or partner) to use highly effective
form(s) of contraception (i.e., one that results in a low failure rate [<1% per year]
when used consistently and correctly) and to continue its use for 6 months after trial
completion.
14. Signed informed consent.
15. Ability to comply with the protocol.
16. Systolic ≥80.
Exclusion Criteria:
1. Uncontrolled concomitant disease.
2. History of severe autoimmune disease.
3. Treatment with systemic immunostimulatory agents within 4 weeks or five half-lives of
the drug, whichever is shorter, prior to enrollment (with the exception of checkpoint
blockade therapy).
4. Treatment with systemic corticosteroids or other systemic immunosuppressive
medications within past 4 weeks or 5 half-lives whichever is shorter.
5. Pregnant and/or lactating women.
6. Patients unable to tolerate checkpoint inhibitor therapy.
7. Grade 3 or 4 non-hematological, treatment-related AEs.
We found this trial at
1
site
Sacramento, California 95814
Principal Investigator: Arta Monjazeb, MD
Phone: 916-734-8252
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