A method of determining the immune response of a mammal to circulating tumor marker proteins is described in which a sample of bodily fluid, for example plasma or serum, is contacted with a panel of two or more distinct tumor marker antigen. The presence of complexes between the tumor marker antigen
A method of determining the immune response of a mammal to circulating tumor marker proteins is described in which a sample of bodily fluid, for example plasma or serum, is contacted with a panel of two or more distinct tumor marker antigen. The presence of complexes between the tumor marker antigens and any autoantibodies to the antigens present in the sample are detected and provide an indication of an immune response to a circulating tumor marker protein. The method is useful for the diagnosis of cancer, particularly for identifying new or recurrent cancer in an otherwise assymptomatic patient.
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1. A method of detecting the immune response of a mammal to circulating tumour marker proteins or tumour cells expressing the tumour marker proteins comprising: (a) diluting a sample of bodily fluids from the mammal;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two
1. A method of detecting the immune response of a mammal to circulating tumour marker proteins or tumour cells expressing the tumour marker proteins comprising: (a) diluting a sample of bodily fluids from the mammal;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two or more tumour marker antigens immobilized on a solid support, wherein at least one of the two or more tumour antigens is selected from the group consisting of MUC1, p53, c-erbB2, Ras, c-myc, BRCA1, BRCA2, PSA, APC and CA125, wherein the two or more tumor marker antigens are recombinantly produced; and(c) detecting autoantibody-antigen complexes by contacting said complexes with labeled anti-IgG and/or labeled anti-IgM to determine the presence or absence of complexes of the tumour marker antigens bound to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker proteins;whereby the presence of the complexes is indicative of the immune response to circulating tumor marker proteins or tumour cells expressing the tumour marker proteins. 2. The method of claim 1 wherein the panel comprises p53 and c-erbB2. 3. The method of claim 2 wherein the complexes detected are indicative of cancer, the cancer is breast cancer, and the panel also includes at least one tumour marker antigen selected from the group consisting of MUC1, c-myc, BRCA1, BRCA2, and PSA. 4. The method of claim 1 wherein the cancer is bladder cancer and the panel is selected from at least two tumour marker antigens selected from the group consisting of p53, c-erbB2, MUC1 and c-myc. 5. The method of claim 1 wherein the cancer is colorectal cancer and the panel is selected from at least two tumour marker antigens selected from the group consisting of p53, Ras, c-erbB2 and APC. 6. The method of claim 1 wherein the cancer is prostate cancer and the panel is selected from at least two tumour marker antigens selected from the group consisting of p53, PSA, BRCA1 and c-erbB2. 7. The method of claim 1 wherein the cancer is ovarian cancer and the panel is selected from at least two tumour marker antigens selected from the group consisting of p53, CA125, c-erbB2 and BRCA1. 8. The method of claim 1 wherein the cancer is breast cancer and the panel is selected from at least two tumour marker antigens selected from the group consisting of p53, MUC1, c-erbB2, c-myc, BRCA1, BRCA2 and PSA. 9. A method of determining the immune response of a patient to two or more circulating tumour marker proteins or to tumour cells expressing the tumour marker proteins and identifying which one of the two or more tumour marker proteins elicits the strongest immune response in the patient, comprising: (a) diluting a sample of bodily fluids from the patient;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two or more distinct tumour marker antigens immobilized on a solid support, wherein the two or more tumour marker antigens are recombinantly produced;(c) measuring the amount of complexes formed by binding of each of the tumour marker antigens to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker proteins; whereby the presence of the complexes is indicative of the immune response to circulating tumour marker proteins or tumour cells expressing the tumour marker proteins,wherein the measurement obtained acts as an indicator of the relative strength of the immune response to each tumour marker protein and thereby identifies which one of the tumour marker proteins elicits the strongest immune response in the patient wherein at least one of the tumour marker antigens is selected from the group consisting of MUC1, c-erbB2, c-myc, Ras, p53, BRCA1, BRCA2, PSA, APC or CA125. 10. The method of claim 9 wherein the relative strength of the immune response to each of the tumour marker proteins or tumor cells indicates selection of a course of anti-cancer treatment. 11. The method of claim 10 wherein one or more tumour marker proteins identified as eliciting a strong immune response in the patient indicate selection of the course of the anti-cancer treatment. 12. A method of detecting the immune response of a mammal to circulating tumour marker proteins or tumour cells expressing the tumour marker proteins comprising: (a) diluting a sample of bodily fluids from the mammal;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two or more distinct tumour marker antigens immobilized on a solid support, wherein the two or more tumour marker antigens are recombinantly produced;(c) determining the presence or absence of complexes of the tumour marker antigens bound to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker proteins;whereby the presence of the complexes is indicative of the immune response to circulating tumour marker proteins or tumour cells expressing the tumour marker proteinsfurther comprising quantifying the immune response of a mammal to circulating tumour marker proteins or tumour cells expressing the tumour marker proteins wherein at least one of the tumour marker proteins is selected from the group consisting of c-erbB2, Ras, c-myc, p53, BRCA1, BRCA2, APC, PSA and CA125, and wherein the method further comprisesmeasuring the quantity of complexes formed by binding of at least one tumour marker antigen to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker protein;wherein the measurement of the quantity of complexes indicates the amount of the autoantibodies present in the sample. 13. The method of claim 12 wherein the amount of autoantibodies present identifies those individuals who are at increased risk of developing cancer in a population of asymptomatic individuals. 14. A method for the detection of cancer comprising: (a) diluting a sample of bodily fluids;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two or more tumor marker antigens immobilized on a solid support selected from the group consisting of c-erbB2, ras, biotinylated c-myc, BRCA1, BRCA2, APC, PSA, CA125 and biotinylated p53 or antigentic fragments thereof, wherein the two or more tumour marker antigens or antigentic fragments are recombinantly produced;(c) measuring the quantity of complexes formed by binding of at least one tumour marker antigen to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker protein; and(d) using the measurement obtained in (b) as an indicator of the amount of the autoantibodies present in the sample. 15. The method of claim 14 wherein the cancer is recurrent disease in a patient previously diagnosed as carrying tumour cells, wherein the patient has undergone treatment to reduce the number of the tumour cells. 16. The method of claim 15 wherein the amount of autoantibodies present monitors the progress of neoplastic disease. 17. The method of claim 15 wherein the amount of autoantibodies present predicts the response of the patient with cancer to anti-cancer treatment. 18. The method of claim 17 wherein the anti-cancer treatment is hormone therapy, chemotherapy, radiotherapy, anti-growth factor therapy, immune therapy or vaccination. 19. A method for the detection of the recurrence of cancer, wherein the cancer is early neoplastic or early carcinogenic change in an asymptomatic patient comprising: (a) diluting a sample of bodily fluids;(b) contacting the diluted sample of bodily fluids from step (a) with at least two tumour marker antigens immobilized on a solid support selected from the group consisting of c-erbB2, ras, biotinylated c-myc, BRCA1, BRCA2, APC, PSA, CA125 and biotinylated p53 or antigenic fragments thereof, wherein the two or more tumour marker antigens or antigentic fragments are recombinantly produced;(c) measuring the quantity of complexes formed by binding of the tumour marker antigens to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to tumour marker proteins; and(d) using the measurement obtained in (b) as an indicator of the amount of the autoantibodies present in the sample,wherein the cancer is recurrent disease in a patient previously diagnosed as carrying tumour cells, and wherein the patient has undergone treatment to reduce the number of the tumour cells. 20. A method of detecting the immune response of a mammal to circulating tumour marker proteins or tumour cells expressing the tumour marker proteins wherein the tumour marker proteins are MUC1, p53, c-erbB2, Ras, c-myc, BRCA1, BRCA2, PSA, APC or CA125, the method comprising: (a) diluting a sample of bodily fluids from the mammal;(b) contacting the diluted sample of bodily fluids from step (a) with two or more of MUC1, p53, c-erbB2, Ras, c-myc, BRCA1, BRCA2, PSA, APC or CA125 or antigenic fragments thereof immobilized on a solid support, wherein the two or more tumour marker antigens or antigenic fragments are recombinantly produced; and,(c) detecting autoantibody-antigen complexes by contacting said complexes with labeled anti-IgG and/or labeled anti-IgM to determine the presence or absence of complexes of the tumour marker proteins or antigenic fragments thereof bound to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker proteins or antigenic fragments thereof;whereby the presence of the complexes is indicative of the immune response to circulating tumor marker proteins or tumour cells expressing the tumour marker proteins. 21. The method of claim 20 wherein the presence of complexes indicates the presence of cancer. 22. The method of claim 21 wherein the cancer is early neoplastic or early carcinogenic change in asymptomatic patients. 23. The method of claim 21 wherein the cancer is recurrent disease in a patient previously diagnosed as carrying tumour cells, wherein the patient has undergone treatment to reduce the number of the tumour cells. 24. The method of claim 21 wherein the presence of complexes indicates the progress of cancer or other neoplastic disease. 25. The method of claim 21 wherein the presence of complexes identifies those individuals who are at increased risk of developing cancer in a population of asymptomatic individuals. 26. A method for the determination of the tumour marker profile of an individual suffering from cancer, wherein the cancer is neoplastic or early carcinogenic change in an asymptomatic patient, comprising: (a) diluting a sample of bodily fluids from the individual;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two or more distinct tumour marker antigens immobilized on a solid support, wherein the two or more tumour marker antigens are recombinantly produced;(c) determining the presence or absence of complexes of the tumour marker antigens bound to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker proteins;wherein the presence of the complexes is indicative of the tumour marker profile of the individual. 27. A method for the determination of the tumour marker profile of a patient at increased risk of recurrent cancer in a population of asymptomatic individuals, wherein the patient was previously diagnosed as carrying cancer cells and wherein the patient has undergone treatment to reduce the number of the cancer cells, comprising: (a) diluting a sample of bodily fluids from the patient;(b) contacting the diluted sample of bodily fluids from step (a) with a panel of two or more distinct tumour marker antigens immobilized on a solid support, wherein the two or more tumour marker antigens are recombinantly produced;(c) determining the presence or absence of complexes of the tumour marker antigens bound to autoantibodies present in the sample of bodily fluids, the autoantibodies being immunologically specific to the tumour marker proteins;wherein the presence of the complexes is indicative of the tumour marker profile of the patient.
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