| Literature DB >> 27437102 |
Brendon J Coventry1, Carrie A Lilly1, Peter Hersey2, Antonio Michele3, Richard J Bright1.
Abstract
BACKGROUND: Repetitive long-term Vaccinia Melanoma Cell Lysate (VMCL) vaccination schedules have proved clinically effective in producing Complete Responses and strong durable survivals for up to 6.1 years in a previous study of patients with advanced Stage IV and Stage IIIc melanoma. These studies were expanded to include 54 patients for further evaluation of these findings.Entities:
Keywords: Complete response; Immuno-Chemotherapy; Immunotherapy; Metastatic melanoma; Repetitive vaccinations; Survival; VMCL; Vaccine
Year: 2014 PMID: 27437102 PMCID: PMC4950896 DOI: 10.1186/2051-1426-2-9
Source DB: PubMed Journal: J Immunother Cancer ISSN: 2051-1426 Impact factor: 13.751
Characteristics for the 54 patients entered into the study
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|---|---|---|
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| Mean | 61.6 | |
| Median | 66 | |
|
| 35-97 | |
| <55 | 18 | |
| 55- < 65 | 14 | |
| 65+ | 22 | |
|
| ||
| Male | 32 | |
| Female | 22 | |
|
| ||
|
|
| |
| 0 = 51 | 0 = 51 | |
| 1 = 2 | 1 = 2 | |
| 2 = 1 | 2 = 1 | |
|
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| IIIb | 1 (2%) | |
| IIIc | 5 (9%) | |
| M1a | 6 (11%) | |
| M1b | 14 (26%) | |
| M1c | 28 (52%) | |
Figure 1Kaplan-Meier survival curve for VMCL Treated Patients (n = 54).
Figure 2Individual patient survival and treatment data to December 2010 (n = 54) [Korn line is survival data from Korn et al.,[28]]; time is to follow-up or death; vaccine is VMCL; Chemotherapy is systemic chemotherapy].
Clinical outcome details for 16 patients surviving ≥ 23 months including survival times (to follow-up at end 2010 or death) in months, disease sites at commencement of vaccination, treatments prior to commencement of vaccination and current status
| Survival (Months) | ID | Disease sites | Prior Tx | Status |
|---|---|---|---|---|
| 121 | 015 | s/c, LN | S, R | Alive, fully functional |
| 117 | 002 | S/C, lung, LN | S, B | Alive, fully functional |
| 93 | 010 | s/c | S, ILI | Alive, fully functional |
| 76 | 021 | s/c | S, ILI | Alive, fully functional |
| 61 | 031 | s/c, lung, LN | S, R | Alive, fully functional |
| 44 | 008 | s/c | S | Died |
| 35 | 049 | s/c, lung | S | AWD, fully functional |
| 34 | 050 | s/c, LN, brain, spleen | R, S | Alive, fully functional |
| 34 | 046 | s/c, lung | S | Died |
| 33 | 053 | s/c, lung | S | Alive, fully functional |
| 29 | 023 | S/C, GB, lung | S | Died |
| 27 | 052 | s/c, umbilical | S | Off trial/died |
| 26 | 045 | s/c | S | Died |
| 24 | 006 | s/c | S | Died |
| 24 | 017 | s/c, LN, lung, liver, spleen | S | Died |
| 23 | 009 | S/C, Bone, lung | S, R | Died |
Abbreviations: s/csub-cutaneous, LN lymph nodes, GB gall bladder, S surgery, B biological therapy, ILI isolated limb infusion (of chemotherapy), R radiotherapy, AWD alive with disease.
Figure 3Effects of VMCL vaccine alone on a patient treated from August 2005 (before therapy; a) to December 2005 (during therapy; b) using repetitive dosing. She was able to walk after the therapy and the tumour size, pain, and odour decreased, with substantial improvement in self-care and walking ability. (reproduced with permission Journal of Cancer Therapy©[15]).