Clinical Study of OncoSorb® in Patients With Advanced Cancer Entities (BP-005)

BioPheresis

Status and phase

Terminated

Phase 2

Phase 1

Conditions

Advanced Cancer Entities

Treatments

Procedure: Apheresis using the OncoSorb column

Study type

Interventional

Funder types

Industry

Other

Identifiers

NCT01013168

BP-005

Details and patient eligibility

About

The purpose of this study is to collect further data for safety and feasibility for the use of the medical device OncoSorb® in clinical routine for the treatment of patients with solid metastatic cancer entities who have failed standard therapies. OncoSorb® device is intended to specifically adsorb three soluble receptors (sTNF-R1, sTNF-R2 and sIL-2R α), which are known to inhibit the natural immune response of cancer patients mediated via tumor necrosis factor α (TNF- α).

Full description

STUDY PURPOSE: The purpose of this study is to collect further data for safety and feasibility for the use of the medical device OncoSorb® in clinical routine for the treatment of patients with solid metastatic cancer entities who have failed standard therapies.

MEDICAL DEVICE: The medical device used in this clinical study is the OncoSorb® column. It is used with a specially modified Fresenius ART apheresis machine, associated tubing sets and an Albuflow plasma filter, also from Fresenius. These components comprise the extracorporeal immune apheresis system. The OncoSorb® column was CE certified in April 2008. The OncoSorb® device is intended to specifically adsorb three soluble receptors (sTNF-R1, sTNF-R2 and sIL-2R α), which are known to inhibit the natural immune response of cancer patients mediated via tumor necrosis factor α (TNF- α).

OBJECTIVES: Primary objective:

The primary objective is to evaluate the use of OncoSorb® therapy in clinical practice in terms of both safety and feasibility. This involves the evaluation of system-immanent issues (particularly occurrence of possible catheter infections and suitability of citrate/heparin anticoagulation) during the course of the clinical study prior the initiation of a phase II study.

Primary variables:

Occurrence of

Possible catheter infection
Suitability of citrate/heparin anticoagulation (with clogging of the extracorporeal circuit or bleeding as potential consequences)
Adverse events/serious adverse events in general including changes of clinically relevant laboratory parameters, changes of vital signs, ECG changes)

Secondary objectives Evaluation of clinical efficacy as defined as objective response to treatment (according to RECIST), progression free survival (PFS), time to progression (TTP), clinical benefit, quality of life (QoL) and kinetics of soluble receptors.

Secondary variables:

Objective response rate (ORR) to OncoSorb® therapy, defined as the proportion of patients with a confirmed CR or PR according to RECIST at efficacy evaluations I, II and III (after monthly Cycles 2, 4 and 6 and continuation until disease progression)
Progression free survival (PFS)
Time to progression (TTP)
Clinical benefit of OncoSorb® therapy (defined as the proportion of patients with confirmed CR, PR and stable disease [SD]) in the evaluable patient population
QoL (as assessed by EORTC QLQ-C30 rev. 3.0)
Kinetics of sTNF-R1, sTNF-R2 and sIL-2R α (concentration levels pre-/post-apheresis as well as determination of receptor levels during treatments). Soluble receptor levels will be measured in the first 3 recruited patients at day 4 to 5 (hourly for the first 3 hours, every 2 hours for the following 6 hours and every 3 hours until treatment start on day 5).

STUDY POPULATION: A total of 5 evaluable patients will be recruited, aged 18 or older. Eligible patients will be identified at the NCT, Department of Medical Oncology or Department of Dermatology (Prof. Enk). Patient 5 will be a patient with cutaneous metastatic melanoma. One tumor lesion will be biopsied (tumor excision) in order to evaluate the induction of apoptosis triggered by TNF-α. The staging examination according to RECIST criteria will be conducted at the radiological department of the University of Heidelberg. Patients will receive a central venous catheter for the extracorporeal treatment at the site of Prof. Quentmeyer (St. Josefskrankenhaus, Heidelberg). The OncoSorb® treatment of the patients with OncoSorb® as extracorporeal immune apheresis device will be conducted either at the site of Prof. Rohmeiss (ze:ro dialysis center Schwetzingen) or at the site of Prof. Zeier (Nierenzentrum Heidelberg). For security reasons the recruitment of patients will be in consecutive order for patients 1 and 2: Patient 2 can be recruited only in the case that patient 1 has finalized OncoSorb treatments until the end of cycle 2. For the recruitment of subsequent patients (patients 3 to 5), no consecutive recruitment is planned. Patient 5 will optionally receive another biopsy (tumor excision) on day 5 of week 3 of the second treatment cycle to evaluate the biological effect of the OncoSorb treatment with respect to induction of apoptosis in response to TNF-α.

STUDY TREATMENTS: The study will start with a screening visit (day -21 to day 0) after obtaining informed consent of the patient. Patients screened for recruitment of patient 5 must give their consent for a baseline biopsy (tumor excision) and optional for a follow-up biopsy (after end of week 3 of cycle 2; tumor excision). Patients, who qualify for participation and are willing to participate, will receive in this period a central venous catheter for the conduction of the extracorporeal OncoSorb® therapy. During the treatment period all patients will receive OncoSorb® treatments consisting of daily immune adsorption treatment procedures 5 days per week for 3 weeks, followed by a resting period of one week. Due to safety reasons all patients will be hospitalized at the NCT during the first week of OncoSorb® treatment. Since currently no information exists about the counterregulation kinetics of sTNF-R1, sTNF-R2 and sIL-2Rα upon OnsoSorb® treatment, the collection of pharmacokinetic (PK) data is planned for the first 3 recruited patients. Blood samples for PK measurements of these patients will be taken between day 4 and 5 of the first treatment cycle under hospitalized conditions. PK data will be essential for designing an optimized treatment schedule (potential reduction of both frequency and apheresis time) of subsequent patients on trial. The schedule of the first 3 patients constitutes a one monthly treatment cycle. For the 2 remaining patients of this study the treatment plan will be re-designed according to the PK data obtained from the first 3 patients on treatment. The efficacy evaluation will be carried out 8 weeks after beginning of treatment. Patients with progression of disease may be withdrawn from OncoSorb® treatment. Patients with complete response (CR), partial response (PR) or stable disease (SD) will be offered to continue OncoSorb® treatments until disease progression. In this case efficacy evaluation (CT scans) will be performed every 8 weeks.

Enrollment

4 patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Patients with metastatic solid cancer who have documented progressive disease and who have failed standard therapy
Measurable disease (RECIST criteria)
Expected survival of at least 4 months
Performance status ECOG 0 and 1
Vital laboratory parameters within normal range, or protocol specified ranges
Able to give written informed consent
The patient's sTNF-R1, sTNF-R2 levels in citrate plasma are > 500 pg/ml and > 1000 pg/ml respectively
The patient has adequate renal function as evidenced by glomerular filtration rate > 80 ml/min
Patient 5 with metastatic melanoma must have skin lesion(s)
Patient 5 with metastatic melanoma should have slow tumor progression
Patient 5 with metastatic melanoma must have an intact TNF-receptor signaling cascade, resulting in measurable induction of cancer cell apoptosis following the exposition to TNF-α in vitro. This will be evidenced by destruction of primary autologous cancer cells obtained by biopsy.

Exclusion criteria

Other serious or significant illnesses
Other malignancy within the last 3 years, except for target oncological indication (does not exclude metastatic sites)
Known immunodeficiency
Known HIV or hepatitis positivity
Using systemic immunosuppressive drugs. (Exceptions: Specific COX-2 inhibitors; low dose aspirin for cardiovascular event prevention; topical/inhaled steroids)
Chemotherapy, immunotherapy or radiotherapy within two weeks prior to start of OncoSorb® treatments provided that all prior therapy related toxicities are resolved
Participation in a prior clinical trial involving an investigational agent within the last 2 weeks
Not available for clinical follow-up assessments
Pregnancy or breastfeeding
Refusal or inability to use effective means of contraception for women of childbearing potential
Mental impairment that may compromise ability to give informed consent and to comply with study requirements
History of a myocardial infarction within 6 months prior to the start of study, uncontrolled congestive heart failure, or any current Grade 3 or 4 cardiovascular disorder despite treatment
Coagulation disorders and / or a history of thromboembolic complications
Any significant disease that, in the Investigator's opinion, should exclude the patient from the study
Known hypersensitivity or allergy to rabbit proteins
Known hypersensitivity to heparin or citrate
The patient receives Angiotensin-Converting Enzyme (ACE) inhibitors or Coumadin (Marcumar®) as concomitant medication
Patient 5 with metastatic melanoma with brain metastases (MRT scan)
Patient 5 with metastatic melanoma is severely immunocompromised (patient must have average or low TREG counts, no dysfunctional T cells like e.g. CD28-)