Alpha 2.0

» Articles » PMID: 2337902

Eradication of a Large MOPC-315 Tumor in Athymic Nude Mice by Chemoimmunotherapy with Lyt2+ Splenic T Cells from Melphalan-treated BALB/c Mice Bearing a Large MOPC-315 Tumor

Overview

Overview

Journal Cancer Immunol Immunother

Specialties Allergy & Immunology
Oncology
Pharmacology

Date 1990 Jan 1

PMID 2337902

Citations 3

Authors

Authors

L M Weiskirch

E Barker

M B Mokyr

Affiliations

Affiliations

Soon will be listed here.

Abstract

We have previously shown that spleen cells from BALB/c mice that are in the process of eradicating a large MOPC-315 tumor following low-dose (2.5 mg/kg) melphalan (L-phenylalanine mustard) therapy are effective in preventing tumor progression upon adoptive transfer into BALB/c mice bearing a barely palpable tumor that had been treated with a subcurative dose of melphalan [Mokyr et al. (1989) Cancer Res 49:4597]. Here we show that such spleen cells in conjunction with a subcurative dose of drug (adoptive chemoimmunotherapy, ACIT) can cause the complete regression of a large (15-20 mm) s.c. MOPC-315 tumor in a large percentage of T-cell-deficient (athymic nude) tumor-bearing mice. Spleen cells that were effective in ACIT of athymic nude mice displayed in vitro a substantial direct lytic activity against MOPC-315 tumor cells, and the lytic activity was greatly enhanced when the spleen cells were cultured for 5 days with or without mitomycin-C-treated MOPC-315 stimulator tumor cells. The cells responsible for the therapeutic effectiveness of the spleen cells in ACIT of athymic nude mice, as well as the cells responsible for the direct in vitro anti-MOPC-315 lytic activity of the spleen cells, were of the Lyt 2 and not the L3T4 phenotype. Most of the athymic nude mice that completely eradicated a large MOPC-315 tumor as a consequence of ACIT were capable of rejecting a challenge with 30-100 times the minimal lethal tumor dose for 100% of normal BALB/c mice administered more than 1 month after the ACIT. The ability of these athymic nude mice to resist the tumor challenge was associated with the presence of a greatly elevated percentage of cells expressing T cell surface markers in their spleens. Thus, it is conceivable that splenic Lyt 2+T cells from melphalan-treated BALB/c mice bearing a large MOPC-315 tumor mediate their therapeutic effectiveness in ACIT of athymic nude mice bearing a large MOPC-315 tumor, at least in part, through direct cytotoxicity for MOPC-315 tumor cells. In addition, eradication of a large MOPC-315 tumor through cooperation between antitumor immunity and melphalan toxicity endues the athymic nude mice with an elevated percentage of T cells in their secondary lymphoid organs, and these T cells are probably responsible for the long-lasting protective antitumor immunity exhibited by these mice.

Citing Articles

Cure of mice bearing a late-stage, highly metastatic, drug-resistant tumor by adoptive chemoimmunotherapy.

Laude M, Russo K, Mokyr M, Dray S Cancer Immunol Immunother. 1993; 36(4):229-36.

PMID: 8439986 PMC: 11038904. DOI: 10.1007/BF01740904.

Transforming growth factor-beta-mediated down-regulation of antitumor cytotoxicity of spleen cells from MOPC-315 tumor-bearing mice engaged in tumor eradication following low-dose melphalan therapy.

Weiskirch L, Mokyr M Cancer Immunol Immunother. 1994; 38(4):215-24.

PMID: 8168116 PMC: 11038867. DOI: 10.1007/BF01533512.

Phorbol ester-induced enhancement in lytic activity of CD8+ splenic T cells from low-dose melphalan-treated MOPC-315-tumor bearers.

Weiskirch L, Baumgartel B, Barker E, Mokyr M Cancer Immunol Immunother. 1991; 32(6):353-63.

PMID: 1901031 PMC: 11038474. DOI: 10.1007/BF01741330.

References

1.

Hengst J, Mokyr M, Dray S . Importance of timing in cyclophosphamide therapy of MOPC-315 tumor-bearing mice. Cancer Res. 1980; 40(7):2135-41. View

2.

Kung J, Thomas 3rd C . Athymic nude CD4+8- T cells produce IL-2 but fail to proliferate in response to mitogenic stimuli. J Immunol. 1988; 141(11):3691-6. View

3.

Mokyr M, Hengst J, Dray S . Role of antitumor immunity in cyclophosphamide-induced rejection of subcutaneous nonpalpable MOPC-315 tumors. Cancer Res. 1982; 42(3):974-9. View

4.

Cheever M, Thompson D, Klarnet J, Greenberg P . Antigen-driven long term-cultured T cells proliferate in vivo, distribute widely, mediate specific tumor therapy, and persist long-term as functional memory T cells. J Exp Med. 1986; 163(5):1100-12. PMC: 2188098. DOI: 10.1084/jem.163.5.1100. View

5.

Schwartz H, GRINDEY G . Adriamycin and daunorubicin: a comparison of antitumor activities and tissue uptake in mice following immunosuppression. Cancer Res. 1973; 33(8):1837-44. View

6.

Barker E, Mokyr M . Importance of Lyt-2+ T-cells in the resistance of melphalan-cured MOPC-315 tumor bearers to a challenge with MOPC-315 tumor cells. Cancer Res. 1988; 48(17):4834-42. View

7.

Bocian R, Ben-Efraim S, Dray S, Mokyr M . Melphalan-mediated potentiation of antitumor immune responsiveness of immunosuppressed spleen cells from mice bearing a large MOPC-315 tumor. Cancer Immunol Immunother. 1984; 18(1):41-8. PMC: 11039127. DOI: 10.1007/BF00205398. View

8.

MATHE G, Bourut C . Effectiveness of murine leukemia chemotherapy according to the immune state: reconsideration of correlations between chemotherapy, tumour cell killing, and survival time. Recent Results Cancer Res. 1977; (62):9-12. DOI: 10.1007/978-3-642-81174-6_3. View

9.

Shu S, Chou T, Rosenberg S . Generation from tumor-bearing mice of lymphocytes with in vivo therapeutic efficacy. J Immunol. 1987; 139(1):295-304. View

10.

Economou J, McBride W, Essner R, Rhoades K, Golub S, Holmes E . Tumour necrosis factor production by IL-2-activated macrophages in vitro and in vivo. Immunology. 1989; 67(4):514-9. PMC: 1385323. View

11.

Hunig T, Bevan M . Specificity of cytotoxic T cells from athymic mice. J Exp Med. 1980; 152(3):688-702. PMC: 2185925. DOI: 10.1084/jem.152.3.688. View

12.

Zangemeister-Wittke U, Kyewski B, Schirrmacher V . Recruitment and activation of tumor-specific immune T cells in situ. CD8+ cells predominate the secondary response in sponge matrices and exert both delayed-type hypersensitivity-like and cytotoxic T lymphocyte activity. J Immunol. 1989; 143(1):379-85. View

13.

Kung J . Impaired clonal expansion in athymic nude CD8+CD4- T cells. J Immunol. 1988; 140(11):3727-35. View

14.

Hengst J, Mokyr M, Dray S . Cooperation between cyclophosphamide tumoricidal activity and host antitumor immunity in the cure of mice bearing large MOPC-315 tumors. Cancer Res. 1981; 41(6):2163-7. View

15.

Hilgard P, Pohl J, Stekar J, Voegeli R . Oxazaphosphorines as biological response modifiers--experimental and clinical perspectives. Cancer Treat Rev. 1985; 12(3):155-62. DOI: 10.1016/0305-7372(85)90036-2. View

16.

Glaser M . Regulation of specific cell-mediated cytotoxic response against SV40-induced tumor associated antigens by depletion of suppressor T cells with cyclophosphamide in mice. J Exp Med. 1979; 149(3):774-9. PMC: 2184834. DOI: 10.1084/jem.149.3.774. View

17.

Ben-Efraim S, Bocian R, Mokyr M, Dray S . Increase in the effectiveness of melphalan therapy with progression of MOPC-315 plasmacytoma tumor growth. Cancer Immunol Immunother. 1983; 15(2):101-7. PMC: 11039118. DOI: 10.1007/BF00199699. View

18.

Burton R, Thompson J, Warner N . In vitro induction of tumour-specific immunity. I. Development of optimal conditions for induction and assay of cytotoxic lymphocytes. J Immunol Methods. 1975; 8(1-2):133-49. DOI: 10.1016/0022-1759(75)90090-3. View

19.

Rollinghoff M, Rouse B, Warner N . Tumor immunity to murine plasma cell tumors. I. Tumor-associated transplantation antigens of NZB and BALB-c plasma cell tumors. J Natl Cancer Inst. 1973; 50(1):159-72. DOI: 10.1093/jnci/50.1.159. View

20.

NORTH R . Down-regulation of the antitumor immune response. Adv Cancer Res. 1985; 45:1-43. DOI: 10.1016/s0065-230x(08)60265-1. View