Abstract

Because of its expression in a large percentage of melanoma lesions and its restricted distribution in normal tissues, the human high molecular weight-melanoma associated antigen (HMW-MAA) has been used for immunotherapy in patients with melanoma. The proposed studies stem from our previous findings that i) unresponsiveness to HMW-MAA, which is a self-antigen, can be overcome by immunizing patients with melanoma with the mouse anti-idiotypic (anti-id) mAbMK2-23, which mimics the determinant, defined by anti-HMW-MAA mAb 763.74; ii) anti-HMW-MAA antibodies elicited by mAb MK2-23 appear to have a beneficial effect on the clinical course of the disease, although they have a low titer and iii) the apparent beneficial effect of anti-HMW-MAA antibodies on the disease does not appear to be mediated by complement- and/or cell-dependent lysis of melanoma cells, but is likely to reflect an effect of the antibodies on the biology of melanoma cells. It is our working hypothesis that enhancement of the humoral anti-HMW-MAA immunity may increase its beneficial effect on the clinical course of melanoma. Since the low titer of anti-HMW-MAA antibodies elicited by anti-id mAb MK2-23 does not reflect its low immunogenicity, but its low mimicry of HMW-MAA, we plan to test the hypothesis that improvement of the HMW-MAA mimicry may enhance the humoral anti-HMW-MAA immune response. To test our hypothesis we will utilize the 12 amino acid long peptide P763.74 which has been isolated from the LX-8 phage display peptide library with anti-HMW-MAA mAb 763.74. Like the anti-id mAb MK2-23, the peptide P763.74 has been found to be able to break unresponsiveness to HMW-MAA in rabbits with a constitutive expression of a human HMW-MAA homologue and to induce low titer HMW-MAA specific antibodies. To improve the mimicry of HMW-MAA amino acid substitutions will be introduced in the peptide mimic P763.74 on the basis of the characterization at the atomic level of its interactions with mAb 763.74. The modified peptides will be tested in their in vitro reactivity with mAb 763.74 and for their ability to induce HMW-MAA specific antibodies in hosts with a constitutive HMW-MAA expression. Since anti-HMW-MAA antibodies are poor in mediating complement -and cell- dependent lysis of melanoma cells, we plan to investigate the mechanisms underlying the direct effect of anti-HMW-MAA antibodies on the biology of melanoma.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA105500-03
Application #
7116296
Study Section
Experimental Immunology Study Section (EI)
Program Officer
Howcroft, Thomas K
Project Start
2004-09-20
Project End
2007-08-31
Budget Start
2006-07-01
Budget End
2007-08-31
Support Year
3
Fiscal Year
2006
Total Cost
$342,612
Indirect Cost

  Institution

Name
Roswell Park Cancer Institute Corp
Department
Type
DUNS #
824771034
City
Buffalo
State
NY
Country
United States
Zip Code
14263

  Publications

Rivera, Zeyana; Ferrone, Soldano; Wang, Xinhui et al. (2012) CSPG4 as a target of antibody-based immunotherapy for malignant mesothelioma. Clin Cancer Res 18:5352-63
Kirkwood, John M; Butterfield, Lisa H; Tarhini, Ahmad A et al. (2012) Immunotherapy of cancer in 2012. CA Cancer J Clin 62:309-35
Mayayo, Saray Lorda; Prestigio, Simone; Maniscalco, Lorella et al. (2011) Chondroitin sulfate proteoglycan-4: a biomarker and a potential immunotherapeutic target for canine malignant melanoma. Vet J 190:e26-30
Wang, Xinhui; Katayama, Akihiro; Wang, Yangyang et al. (2011) Functional characterization of an scFv-Fc antibody that immunotherapeutically targets the common cancer cell surface proteoglycan CSPG4. Cancer Res 71:7410-22
Campoli, Michael; Ferris, Robert; Ferrone, Soldano et al. (2010) Immunotherapy of malignant disease with tumor antigen-specific monoclonal antibodies. Clin Cancer Res 16:11-20
Wang, X; Wang, Y; Yu, L et al. (2010) CSPG4 in cancer: multiple roles. Curr Mol Med 10:419-29
Wang, Xinhui; Osada, Takuya; Wang, Yangyang et al. (2010) CSPG4 protein as a new target for the antibody-based immunotherapy of triple-negative breast cancer. J Natl Cancer Inst 102:1496-512
Campoli, Michael; Ferrone, Soldano; Wang, Xinhui (2010) Functional and clinical relevance of chondroitin sulfate proteoglycan 4. Adv Cancer Res 109:73-121
Drake, Allison S; Brady, Michael T; Wang, Xin Hui et al. (2009) Targeting 11q23 positive acute leukemia cells with high molecular weight-melanoma associated antigen-specific monoclonal antibodies. Cancer Immunol Immunother 58:415-27
Kitago, Minoru; Koyanagi, Kazuo; Nakamura, Takeshi et al. (2009) mRNA expression and BRAF mutation in circulating melanoma cells isolated from peripheral blood with high molecular weight melanoma-associated antigen-specific monoclonal antibody beads. Clin Chem 55:757-64

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