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29 results on '"Epenetos, A.A."'

1. Activation of cellular immunity after intracavitary monoclonal antibody therapy of ovarian cancer

Author

Kosmas, C. Epenetos, A.A. Courtenay‐Luck, N.S.

Abstract

Background. Murine monoclonal antibodies (MoAbs) are now used for targeted tumor therapy. A major obstacle in their successful application is the development of a humoral antiglobulin response, which limits the use of repeated cycles of therapy. The cellular aspects of that response are not well understood. Methods. Fifteen patients who had one (12 patients) or two (3 patients) courses of MoAb treatment, 13 agematched patients with the same histologic types of tumors who had not received MoAbs, and 4 healthy control subjects were studied. Peripheral blood mononuclear cells (PBMCs) were obtained and tested for the ability of T‐cells to proliferate in vitro in the presence of the MoAb administered for therapy (HMFG1), a control antibody (11.4.1), and, in some cases, their F(ab)2 fragments. In addition, PBMCs from these patients were phenotyped after in vitro MoAb stimulation with antibodies against CD2, CD3, CD4, CD8, CD16, CD20, CD25 (interleukin‐2 receptor [IL‐2R]), CD45RA, and UCHL1, and the production of interleukin‐2 (IL‐2) was evaluated by the CTLL‐2 bioassay. Results. A dose‐dependent in vitro T‐cell proliferation was observed in 13 of the 15 patients after MoAb therapy. This was not observed in the pretherapy group of patients or healthy control subjects. The mean stimulation index (SI) in the posttherapy group was significantly higher than that of the pretherapy patients and that of healthy control subjects (P = 0.007). When the in vitro T‐cell proliferative responses of these patients were measured in the presence of HMFG1 MoAb (IgG1) and 11.4.1 MoAb, there was no significant difference in the mean SI for HMFG1 versus 11.4.1 for the whole group of treated patients (P = 0.67). A significant increase in the mean SI was observed in the presence of HMFG1 over 11.4.1 and their F(ab)2 fragments (P = 0.02) in patients treated twice. A significant increase in the percentage of cells expressing IL‐2R was observed after in vitro MoAb stimulation. CD4+ lymphocytes, particularly the CD4+/UCHL1+ memory, the CD4+/IL‐2R+ subpopulation, and the CD4/CD8 ratio, increased in all the cases studied after MoAb stimulation, where B‐cell and natural killer‐cell numbers remained relatively constant (

Published
1994

3. Antibody guided irradiation of brain glioma by arterial infusion of radioactive monoclonal antibody against epidermal growth factor receptor and blood group A antigen.

Author

Epenetos, A.A., Courtney-Luck, N., Pickering, D., Hooker, G., Durbin, H., Lavender, J.P., and McKenzie, C.G.

Subjects
*THERAPEUTIC use of monoclonal antibodies, *GLIOMA treatment, *DRUG efficacy
Abstract

Examines the clinical value of delivering irradiation guided by monoclonal antibody in the treatment of brain gliomas. Description of Grade IV glioma; Reason for choosing an antibody 9A; Method of delivering antibody guided irradiation.

Published
1985
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7. Imaging thrombus with radiolabelled monoclonal antibody to platelets.

Author

Peters, A.M., Lavender, J.P., Needham, S.G., Loutfi, I., Snook, D., Epenetos, A.A., Lumley, P., Keery, R.J., and Hogg, N.

Subjects
RADIOLOGY, MONOCLONAL antibodies, BLOOD platelet examination
Abstract

Evaluates the method of imaging thrombus with radiolabelled monoclonal antibody to platelets. Lack of immunoreactivity impairment; Absence of platelet activation after intravenous P256 and radiolabelling of platelets; Potential of imaging thrombus as a simple and non-invasive approach to the diagnosis of thrombosis.

Published
1986
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8. Comparison of two combination chemotherapy regimens in advanced colorectal cancer.

Author

Epenetos, A.A., Amos, C., Collis, C., Slevin, M., Rohatiner, A., Baille-Johnson, H., Pitts, J., and Wrigley, P.F.M.

Subjects
*COLON cancer, *RESPONSE rates, *MEDICAL care surveys, *MITOMYCIN C, *DRUG therapy, *DRUG efficacy
Abstract

Examines the response rate of methylchoroethyl-cyclohexyl-nitrosourea in colorectal cancer. Efficacy of adding mitomycin C to survival and response; Treatment of patients with chemotherapy; Confirmation on histological adenocarcinoma of colorectum.

Published
1980
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