Variant generation and selection: An In vitro model of tumor progression

## Abstract The stability of a cloned murine tumor for sensitivity to NR was examined following growth __in vivo__ in order to test the hypothesis that tumor progression proceeds through the generation and selection of variants. Clonal sensitivity to the [^131^l]‐dUrd elimination assay of NR was as

Following sequential interactions between activated syngeneic Mas and 3LL tumor cells, stable M\*-resistant 3LL variants were isolated. Unlike the unselected 3LL cells, these Maselected variants were relatively resistant to the cytostatic and cytolytic activity of activated effector Mas. Such Maresi

## Abstract ## BACKGROUND. Intraperitoneal tumors expressing high amounts of mesothelin such as malignant mesothelioma and ovarian cancers tend to develop ascites and result in significant morbidity and mortality in the patient. A suitable preclinical intraperitoneal model will assist in the illus

## Abstract Inflammatory neutrophils elicited by intraperitoneal injection of __Corynebacterium parvum__, thioglycollate or proteose peptone were capable of lysing different murine and human tumor targets in a shortterm chromium‐release assay. A single‐cell cytotoxicity assay, which evaluated effec

## Abstract Immunoselection of a non‐metastatic variant of the highly metastatic MDAY‐D2 tumor of DBA/2 mice was achieved by means of an antiserum directed to the LY6.2 surface marker of MDAY‐D2. While the new tumor (MDAY‐D2.L61) expresses no detectable LY6.2, other measurable surface markers inclu

## Abstract C~3~H mouse embryos were supported in an __in vitro__ culture system over 28‐h periods between 8 and 10 days post‐conception. Morphological development over this critical period of organogenesis was monitored in the following respects: somite count; presence or absence of heart beat; ce