Abstract

The overall goal of the present application is to develop more specific and sensitive immunoassays for circulating breast epithelial antigens (CBE-Ags), using recent information we have obtained on the antigenicity and catabolism of CBE-Ags and employing newer immunoassay systems that we have created. These novel, sensitive, and specific assays that we develop, rely first on out findings regarding the fragmentation of CBE-Ags with simultaneous clearance from the blood compartment. These fragments are much longer-lived in blood, and hence more useful, than the intact CBE-Ags. Our present incorporation of recombinant epitopes into assays for these long-lived fragments represents a totally novel approach to serum marker measurement in breast cancer. These approaches, if successful, will identify not only minimal tumor load in breast cancer, but also the 10% of the female population that will eventually develop breast cancer, in which early diagnosis could lead to life-saving, curative treatment. The creation of such assays for CBE-Ags and their fragments will depend on immunological and recombinant DNA approaches. We will screen breast cDNA libraries for sequences encoding epitopes on CBE-Ags, and especially on their catabolic fragments, both with MoAbs we already possess and with new ones generated specifically for this purpose. The corresponding cDNA will be characterized, sequenced, inserted into expression vectors, and recombinant molecules containing epitopes for the CBE-Ags and their catabolic fragments synthesized or expressed and new customized MoAbs generated for the immunoassays. These assays will then be tested in clinical trials for their sensitivity, specificity and predictive value. Since we have demonstrated both epitopic and antigenic heterogeneity and the individuality of tumor cell populations, several CBE-Ag tests will be assembled in panels to allow the choice of the most prevalent CBE-Ags for each breast tumor to be tested. The recombinant epitope assay configuration that we propose, will make the use of a panel of CBE-Ags assays both expedient and simple. Thus, we propose to develop a second generation of breast cancer serum markers to provide the desired test for the detection of residual disease in the axillary node negative patient, for early prediction of relapse in the disease-free period, for monitoring therapeutic response and possibly for screening female populations at risk.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA039932-07
Application #
3179319
Study Section
Pathology B Study Section (PTHB)
Project Start
1984-09-16
Project End
1993-06-30
Budget Start
1990-07-06
Budget End
1991-06-30
Support Year
7
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
John Muir Memorial Hosp (Walnut Crk, CA)
Department
Type
DUNS #
City
Walnut Creek
State
CA
Country
United States
Zip Code
94598

  Publications

Peterson, J A; Scallan, C D; Ceriani, R L et al. (2001) Structural and functional aspects of three major glycoproteins of the human milk fat globule membrane. Adv Exp Med Biol 501:179-87
Peterson, J A; Hamosh, M; Scallan, C D et al. (1998) Milk fat globule glycoproteins in human milk and in gastric aspirates of mother's milk-fed preterm infants. Pediatr Res 44:499-506
Newburg, D S; Peterson, J A; Ruiz-Palacios, G M et al. (1998) Role of human-milk lactadherin in protection against symptomatic rotavirus infection. Lancet 351:1160-4
Peterson, J A; Blank, E W; Ceriani, R L (1997) Effect of multiple, repeated doses of radioimmunotherapy on target antigen expression (breast MUC-1 mucin) in breast carcinomas. Cancer Res 57:1103-8
DeNardo, S J; Kramer, E L; O'Donnell, R T et al. (1997) Radioimmunotherapy for breast cancer using indium-111/yttrium-90 BrE-3: results of a phase I clinical trial. J Nucl Med 38:1180-5
Couto, J R; Taylor, M R; Godwin, S G et al. (1996) Cloning and sequence analysis of human breast epithelial antigen BA46 reveals an RGD cell adhesion sequence presented on an epidermal growth factor-like domain. DNA Cell Biol 15:281-6
Peterson, J A; Couto, J R; Taylor, M R et al. (1995) Selection of tumor-specific epitopes on target antigens for radioimmunotherapy of breast cancer. Cancer Res 55:5847s-5851s
Ceriani, R L; Blank, E W; Couto, J R et al. (1995) Biological activity of two humanized antibodies against two different breast cancer antigens and comparison to their original murine forms. Cancer Res 55:5852s-5856s
Ortel, T L; Quinn-Allen, M A; Keller, F G et al. (1994) Localization of functionally important epitopes within the second C-type domain of coagulation factor V using recombinant chimeras. J Biol Chem 269:15898-905
Peterson, J A; Ceriani, R L (1994) Breast mucin and associated antigens in diagnosis and therapy. Adv Exp Med Biol 353:1-8

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