Activation of complement by spontaneous leukemic cells of AKR mice

## Abstract Non‐specific activation of complement (NAC) on cell membranes via the alternative pathway was studied by using leukemic cells and cells from a generalized reticulohistiocytosis. The cells were treated with normal human serum in veronal‐buffered saline containing ethyleneglycoltetra‐acet

## Abstract The intrasplenic inoculation of AKR lymphoma cells into 1‐month‐old BALB mice, followed by a syngeneic intraperitoneal passage, led to the development of short‐latency leukemia of host origin within 24 days; the incidence of leukemia averaged 83% in 88 mice. Electron microscopic studies

Grafting of 5-month-old thymuses of AKR mice into young adult A K R and ( A K R x S L ) F , recipients shortened markedly the latent period for leukemia development, but thymus

## Abstract The sensitivity of different wild‐type and 5‐azacytidine‐resistant lines of AKR leukemic mice to 5‐azacytidine varies in relation to the activity of uridine kinase isolated from corresponding leukemic livers. The enhancement of liver uridine kinase activity observed in leukemic mice fol

## Abstract Culture of WEHI‐3B myelomonocytic leukemic cells in semi‐solid agar medium containing post‐endotoxin serum led to the development of maturing granulocytes and macrophages in most leukemic colonies. Colony size was consistently increased but the colony content of colony‐forming cells (st

demonstration of the induction T of rodent leukemia in mature mice by cell-free materials was reported by Schwartz and coworkers.11 I n the original experiment,ll a n acceleration of the development of leukemia in the high leukemic incidence strain of AKR mice was demonstrated by inoculation of mice