Thomsen-Friedenreich (TF) antigen as a target for prostate cancer vaccine: Clinical trial results with TF cluster (c)-KLH plus QS21 conjugate vaccine in patients with biochemically relapsed prostate cancer Journal Article


Authors: Slovin, S. F.; Ragupathi, G.; Musselli, C.; Fernandez, C.; Diani, M.; Verbel, D.; Danishefsky, S.; Livingston, P.; Scher, H. I.
Article Title: Thomsen-Friedenreich (TF) antigen as a target for prostate cancer vaccine: Clinical trial results with TF cluster (c)-KLH plus QS21 conjugate vaccine in patients with biochemically relapsed prostate cancer
Abstract: The differential overexpression of self-antigens on tumor cells is a prime feature of malignant transformation. Thomsen-Friedenreich (TF), a core disaccharide of O-glycosylated complex glycoproteins, is one of many "self" antigens expressed on malignantly transformed cells that has served as a target for immune recognition and attack. Previously, we conducted clinical trials with a series of synthetic glycolipid, peptide and carbohydrate antigens conjugated to the immunological carrier keyhole limpet hemocyanin (KLH) mixed with the immunological saponin adjuvant, QS21. These trials resulted in the generation of high-titer IgM and IgG antibody responses specific for the individual antigens, and, in several cases, the capacity of those antibodies to mediate complement lysis. Four groups of five patients who had evidence of a biochemical relapse defined as rising prostate-specific antigens (PSAs) following primary therapy for prostate cancer with either prostatectomy or radiation were treated with escalating doses of 1, 3, 10 and 30 μg of synthetic TF in a clustered formation (c) which was conjugated to KLH and given with 100 μg of QS21. Patients received a total of five subcutaneous vaccines over 6 months and were monitored expectantly with scans every 3-4 months. Serum samples were obtained at weeks 1, 2, 3, 7, 9, 13, 19, 26, 50 and every 3 months. Antibody titers were monitored by ELISA and antibody binding to the cell surface of prostate cell lines was performed by flow cytometry. Complement-dependent cytotoxicity was performed on selected patients. Twenty evaluable patients were accrued to the study, of whom only one did not receive all six vaccinations. All patients developed maximum IgM and IgG antibody titers by week 9. The median IgM antibody titer by week 7 was 1/1,280 at 10 μg, 1/320 at 30 μg, 1/1,280 at 3 μg and 1/1,280 at 1 μg dose groups. The IgM titers from all groups remained greater than 1/320 by week 32 and beyond through week 50. We report here the results of a dose-escalating trial of a TF(c)-KLH conjugate vaccine in patients in the clinical state of a rising PSA in the absence of radiographic disease. For the first time, a synthetically made TF trimer or cluster (c) was made with three TF disaccharides attached to three sequential threonines on a peptide backbone. TF(c) doses of 1, 3, 10 and 30 μg were conjugated to KLH and administered with QS21. All doses induced high-titer IgM and IgG antibodies against TF. Unlike our findings in previous dose-escalating phase I trials, there did not appear to be increased antibody production with increasing doses of vaccine; higher titers of IgM and IgG antibodies developed at the lowest dose level (1 μg). An anti-tumor effect in the form of a change in post-treatment versus pretreatment logPSA slopes was also observed. The results justify the inclusion of TF(c) at a dose of 1 μg as a relevant antigenic target in a multivalent phase II vaccine trial in patients in the high-risk minimal disease state. © Springer-Verlag 2005.
Keywords: adult; clinical article; controlled study; aged; middle aged; unclassified drug; clinical trial; dose response; drug efficacy; drug safety; cancer radiotherapy; antigen expression; prostate specific antigen; edema; controlled clinical trial; pain; neoplasm recurrence, local; myalgia; antineoplastic activity; drug effect; arthralgia; fever; injection site reaction; prostate cancer; pruritus; prostate-specific antigen; prostatic neoplasms; antigen; antigens, neoplasm; cancer vaccine; cancer vaccines; prostatectomy; vaccination; psa; recurrent disease; immunological adjuvant; flu like syndrome; adjuvants, immunologic; immunoglobulin g antibody; drug conjugation; vaccine; antigens, tumor-associated, carbohydrate; antibody production; antibody titer; immunoglobulin m antibody; hemocyanin; saponins; vaccines, conjugate; cluster; klh; thomsen friedenreich antigen; tf; qs21 adjuvant; thomsen friedenreich cluster keyhole limpet hemocyanin vaccine
Journal Title: Cancer Immunology, Immunotherapy
Volume: 54
Issue: 7
ISSN: 0340-7004
Publisher: Springer  
Date Published: 2005-07-01
Start Page: 694
End Page: 702
Language: English
DOI: 10.1007/s00262-004-0598-5
PUBMED: 15726361
PROVIDER: scopus
DOI/URL:
Notes: --- - "Cited By (since 1996): 52" - "Export Date: 24 October 2012" - "CODEN: CIIMD" - "Source: Scopus"
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MSK Authors
  1. Susan Slovin
    186 Slovin
  2. David A Verbel
    20 Verbel
  3. Govindaswami Ragupathi
    133 Ragupathi
  4. Howard Scher
    835 Scher
  5. Meghan Diani
    5 Diani