Host immune potentiation of drug responses to a murine mammary adenocarcinoma

## Abstract The role of chemotherapy in influencing tumorspecific immunity to a mouse mammary adenocarcinoma was investigated. By studying different stages of tumor growth we were able to identify several factors important to drug‐induced tumor regression: (1) antibody response, (2) delayed hyperse

## Abstract The nature of host‐derived, specifically cytotoxic cells infiltrating solid murine mammary adenocarcinomas (line T1699) was investigated. Cell suspensions obtained from enzymatically dispersed tumors were separated by sedimentation velocity. The host cell fraction was heterogeneous and

## Abstract DBA/2 mice bearing a syngeneic mammary adenocarcioma T1699 produced high levels of tumor‐specific antibody, detected by indirect immunofluorescence and subsequently identified as the IgG~2a~ subclass. Tumor‐bearer sera passively administered to normal recipients protected the animals fr

## Abstract Sera from DBA/2 mice bearing a syngeneic T1699 mammary adenocarcinoma not only induced specific antibody‐dependent cellular cytotoxicity (ADCC) mediated by monocytes (and/or macrophages) but also armed (activated) such effector cells into specific killer cells __in vitro__. Removal of s

## Abstract Intravenously (i.v.) or subcutaneously (s.c.) injected T1699 tumor cell subpopulations (Ts, and TL1–1) were destroyed more rapidly in BALB/c __nu/nu__ athymic mice than in syngeneic DBA/2J mice. The number of artificial pulmonary metastases of TL1–1 tumors was significantly lower, and t

## Abstract The contribution of host immune factors to the therapeutic effect of cyclophosphamide (CPA) on an antigenic chemically‐induced sarcoma (MCA‐2) transplanted in syngeneic mice with different immunological reactivity was investigated. In non‐sensitized mice, CPA failed to prevent survival