Descriptor: "Leukemia P388 pathology" / Topic: leukemia, experimental - Searchworks@Jio Institute Digital Library Search Results

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93 results on '"Leukemia P388 pathology"'

1. Comparison of the effects of genistein and amsacrine on leukemia cell proliferation.

Author: Finlay GJ, Holdaway KM, and Baguley BC
Subjects: Animals, Cell Cycle drug effects, Cell Division drug effects, Drug Resistance, Multiple, G2 Phase drug effects, Genistein, Humans, Leukemia P388 drug therapy, Leukemia P388 pathology, Leukemia, Experimental enzymology, Mice, Topoisomerase II Inhibitors, Tumor Cells, Cultured drug effects, Amsacrine pharmacology, Antineoplastic Agents pharmacology, Isoflavones pharmacology, Leukemia, Experimental drug therapy, Leukemia, Experimental pathology
Abstract: Genistein is an inhibitor of the enzymes protein tyrosine kinase and topoisomerase-II. It induces G2-phase arrest in human Jurkat and murine P388 leukemia cells at concentrations at which it is also cytotoxic. The effects of genistein have been investigated on Jurkat and P388 leukemia sublines that manifest multidrug resistance. Cells that possess altered topoisomerase-II activity ("atypical" multidrug resistance) are resistant to both the G2 phase-arresting and cytotoxic effects of genistein. The ability of genistein to impede progression through the cell cycle and kill cells is similar to that of amsacrine, a classical topoisomerase-II poison. This result identifies topoisomerase-II rather than tyrosine kinase activity as the target of genistein-mediated cytotoxicity and G2-phase arrest.
Published: 1994

2. [Cross-resistance of HO-221 and various antitumor agents in sublines of mouse leukemia].

Author: Nakajima T, Masuda H, Okamoto T, Watanabe M, Yokoyama K, Yamada N, Fujimoto S, Tsukagoshi S, and Taguchi T
Subjects: Animals, Cisplatin pharmacology, Doxorubicin pharmacology, Drug Resistance, Leukemia L1210 drug therapy, Leukemia L1210 pathology, Leukemia P388 drug therapy, Leukemia P388 pathology, Leukemia, Experimental pathology, Mice, Mitomycin, Mitomycins pharmacology, Tumor Cells, Cultured drug effects, Antineoplastic Agents pharmacology, Benzamides pharmacology, Leukemia, Experimental drug therapy, Nitrobenzenes pharmacology
Abstract: HO-221, N-[4-(5-bromo-2-pyrimidinyloxy)-3-chlorophenyl]-N'-(2- nitrobenzoyl) urea is a new benzoylphenylurea derivative. The compound exhibits significant antitumor effects against various animal tumors, and was especially effective against the solid tumors implanted subcutaneously. HO-221 inhibits DNA polymerase alpha activity strongly in vitro. In this study, we examined the cross-resistance of HO-221 to various antitumor agents using sublines of mouse leukemia. HO-221 showed antitumor effects in mice bearing L 1210 or P 388 leukemia resistant to 10 antitumor agents, DM (daunomycin), MMC (mitomycin C), CDDP (cisplatin), 5-FU (5-fluorouracil), Ara-C (cytosine arabinoside), MTX (methotrexate), CPA (cyclophosphamide), CQ (carboquone), ADM (adriamycin) and VCR (vincristine), respectively. These antitumor agents were also effective in P 388 leukemia resistant to HO-221 (P 388/HO-221). Furthermore, CDDP- and MMC-resistant sublines showed a collateral sensitivity to HO-221 in vivo. The grow the inhibitory effects were also noted in vitro in ADM-, CDDP- and MMC-resistant cells by HO-221. However, the in vitro experiments didn't show such collateral sensitivity on the resistant sublines. These results suggest that there is no cross-resistance between HO-221 and other known antitumor agents, and that HO-221 seemed to be worth for evaluating clinical usefulness.
Published: 1991

3. Antitumor effect of a new organic selenium compound, 6-phenyl-7 (6H)-isoselenazolo [4,3-d] pyrimidone (ISP), on the growth of P388 mouse leukemia.

Author: Ito H, Wang JZ, Shimura K, Sakakibara J, and Ueda T
Subjects: Animals, Azoles, Fatty Acids analysis, Female, Leukemia P388 metabolism, Lipids analysis, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Nucleic Acids biosynthesis, Organoselenium Compounds, Phospholipids analysis, Tumor Cells, Cultured, Amides pharmacology, Antineoplastic Agents pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Organometallic Compounds, Pyrazoles pharmacology, Pyrimidinones pharmacology, Selenium pharmacology
Abstract: The organic selenium compound, ISP [6-phenyl-7(6H)-isoselenazolo [4,3-d] pyrimidone] markedly inhibited the growth of P388 mouse leukemia at dose of 100 micrograms/mouse per day x 10 with no sign of toxicity. The antitumor activity of 4,5-dihydro-4-methyl-6-oxo-5-phenyl-6H-pyrazolo [4,5-c] isoselenazole (PIS) was weaker than that of ISP. The total lipid and phospholipid contents in the leukemic cells treated with ISP were significantly decreased. The fatty acid pattern of cholesterol esters, phosphatidyl choline and phosphatidyl ethanolamine from the ISP-treated P388 leukemic cells differed markedly from that of the corresponding lipids from the control leukemic cells. In addition, the synthesis of DNA or RNA was depressed in the ISP-treated leukemic cells. The present results indicate that ISP may open new perspectives in cancer chemotherapy.
Published: 1990

4. The antitumor effects of adriamycin entrapped in liposomes on lymph node metastases.

Author: Konno H, Tadakuma T, Kumai K, Takahashi T, Ishibiki K, Abe O, and Sakaguchi S
Subjects: Animals, Doxorubicin therapeutic use, Drug Administration Schedule, Drug Carriers, Drug Screening Assays, Antitumor, Injections, Subcutaneous, Leukemia P388 pathology, Liposomes, Lymphatic Metastasis, Mice, Mice, Inbred Strains, Tumor Cells, Cultured drug effects, Doxorubicin administration & dosage, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy
Abstract: Adriamycin (ADM) entrapped in liposomes (Lip-ADM) was prepared and its therapeutic effects studied using the mouse leukemia cell line, P388, which metastasized to axillary lymph nodes after inoculation into the foot pads of CDF1 mice. Lip-ADM injections (7.5 mg/kg) were given into the foot pad at two-day intervals. Two series of experiments were performed; one in which Lip-ADM was administered on days 1,3 and 5 following tumor inoculation, and the other in which it was administered on days 5 and 7. Both Lip-ADM injection regimens significantly inhibited metastases to the lymph nodes as compared with mice given injection of saline solution. Furthermore, the therapeutic effects of three Lip-ADM injections were significantly greater than the effects of free ADM. Histological examinations of lymph nodes revealed that three injections of Lip-ADM completely eliminated tumor cells, whereas viable tumor cells were still observed in the lymph nodes after treatment with free ADM. The results of this study suggest that Lip-ADM is useful for the treatment of lymph nodes metastases and that the local injection of Lip-ADM, through such means as endoscopy, would be recommended as a clinical mode of application.
Published: 1990
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5. Evaluation of quinidine effect on the antitumor activity of adriamycin and mitoxantrone in adriamycin-sensitive and -resistant P388 leukemia cells.

Author: Parekh H and Chitnis M
Subjects: Animals, Cell Survival drug effects, DNA, Neoplasm biosynthesis, Drug Resistance, Female, Leukemia P388 pathology, Male, Mice, Neoplasm Transplantation, Antineoplastic Agents, Doxorubicin pharmacology, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy, Mitoxantrone pharmacology, Quinidine pharmacology
Abstract: Utilizing the P388 murine leukemia cells sensitive (P388/S) and resistant (P388/ADR) to Adriamycin (ADR), we evaluated the effect of quinidine, an anti-arrhythmic agent, on the cytotoxic activity of ADR and Mitoxantrone (MITO), both in vitro as well as in vivo. Quinidine enhanced the cytotoxicity of both ADR and MITO in P388/S and P388/ADR cells, as assessed by the decrease in color intensity of formazan crystal in the MTT (3-[4,5-dimethylthiazol-2-yl]-2,5 diphenyl tetrazolium bromide) assay. A dose dependent inhibition of 3H-thymidine and 3H-uridine incorporation was observed when the P388/S and P388/ADR cells were exposed to quinidine alone. A non-toxic concentration of quinidine (5 microM) enhanced the DNA biosynthesis inhibition induced by ADR (55 to 65%) and MITO (37 to 44%) in P388/ADR cells, indicating reversal of resistance, while in P388/S cells only a minimal increase in DNA biosynthesis inhibition was observed. The combination of quinidine at doses of 50 to 100 mg/kg significantly potentiated the antitumor activity of ADR and MITO in P388/ADR bearing mice, whereas the potentiation of ADR and MITO antitumor response was lower in P388/S bearing mice. Quinidine increased the cellular levels of ADR by 53 to 126% in P388/ADR cells in vitro, but failed to indicate such elevated levels of cellular ADR in P388/S cells. This enhanced intracellular accumulation of ADR in P388/ADR cells, explains the therapeutic efficacy of ADR and MITO in P388/ADR, both in vitro as well as in vivo. Results suggest the efficacy of quinidine to ameliorate the antitumor effects of ADR and MITO in drug resistant tumor cells.
Published: 1990
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6. Tumor inhibiting [1,2-bis(fluorophenyl)ethylenediamine]platinum(II) complexes. Part II: Biological evaluation-in vitro studies on the P 388 D1 leukemia cell line.

Author: Reile H, Müller R, Gust R, Laske R, Krischke W, Bernhardt G, Spruss T, Jennerwein M, Engel J, and Seeber S
Subjects: Animals, Cell Survival drug effects, Cisplatin pharmacology, Mice, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured pathology, Antineoplastic Agents pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Organoplatinum Compounds pharmacology
Abstract: Experiments on the P 388 D1 cell line (48 h exposure) demonstrate that [1,2-bis-(fluorophenyl)ethylenediamine]platinum(II) complexes are comparably active on the cell number and 3H-thymidine incorporation, irrespective of the position of the fluorine atom (ortho, meta, or para) and the nature of the "leaving group" (Cl- or H2O). However, the compounds of the R,R/S,S series are more active than those of the R,S series and comparable to cisplatin. In the "tumor colony forming assay" the R,R/S,S configurated compounds are about ten times as active as cisplatin. The R,R/S,S configurated diaqua[1,2-bis(4-fluorophenyl)ethylenediamine]platinum(II) salts reach their half maximum effect more readily (t1/2 approximately equal to 1.6 h) than their R,S configurated analogues (t1/2 approximately equal to 20 h). A time limited contact of the cells with R,R/S,S configurated diaqua[1,2-bis(4-fluorophenyl)ethylenediamine]platinum(II) salts (-1h) leads to a similar inhibition like a permanent drug exposure indicating a fast uptake of the complex by the tumor cell. In experiments on the Ehrlich ascites tumor of the mouse and on the L 1210 leukemia cell line R,R/S,S-[1,2-bis(4-fluorophenyl)ethylenediamine]dichloroplatinum(II) turns out to be equipotent with cisplatin.
Published: 1990
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7. [An efficient method for establishing murine tumor cell lines].

Author: Mi JX
Subjects: Animals, Culture Media, Friend murine leukemia virus, Leukemia L1210 pathology, Leukemia P388 pathology, Leukemia, Erythroblastic, Acute pathology, Leukemia, Lymphoid pathology, Liver Neoplasms, Experimental pathology, Mice, Mice, Inbred DBA, Sarcoma 180 pathology, Leukemia, Experimental pathology, Tumor Cells, Cultured
Abstract: Tumor cells were cultured in RPMI1640 medium with 16% fetal calf serum and 5% conditioned medium of PHA-stimulated murine spleen cells. After cloning, the tumor cells were reinoculated into normal susceptible mouse. When tumor developed, they grew easily in subsequent cultures in vitro, thus establishing tumor cell lines. By this method, 5 leukemia cell lines and 2 tumor cell lines have been established.
Published: 1990

8. P-glycoprotein expression and modulation of cell-membrane morphology in adriamycin-resistant P388 leukemia cells.

Author: Radel S, Fredericks W, Mayhew E, and Baker R
Subjects: ATP Binding Cassette Transporter, Subfamily B, Member 1, Animals, Blotting, Western, Cell Membrane ultrastructure, Drug Resistance, Leukemia P388 drug therapy, Leukemia P388 metabolism, Mice, Mice, Inbred DBA, Microscopy, Electron methods, Microscopy, Electron, Scanning, Neoplasm Transplantation, Tumor Cells, Cultured, Doxorubicin pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Membrane Glycoproteins analysis, Neoplasm Proteins analysis
Abstract: Electron microscopy of cultured P388 leukemia cells revealed morphological differences between the Adriamycin-resistant (P388/ADR) and -sensitive (P388/0) cell lines. P388/ADR cells showed longer villus-like protrusions and large foldings of the plasma cell membrane, whereas P388/0 cells had only short membrane protrusions. Western blot analysis of cells revealed the increased expression of a glycoprotein of 170-180 kDa (P-glycoprotein) in P388/ADR cells as compared with P388/0 cells, which is consistent with the findings of other studies. A modulation of the membrane morphology of in vitro P388/ADR cells was evident from one i.p. in vivo passage for 10 days, by a reversion to the non-ruffled sensitive-cell morphology. Long-term P388/ADR culture cells showed a reduction in membrane folding with as little as a 4-h exposure to the peritoneal ascitic fluid obtained when the tumor was harvested. However, there was no alteration in the expression of P-glycoprotein or in the sensitivity to Adriamycin in either of the P388 cell lines when grown in vivo or when exposed to ascites fluid from an i.p. tumor. Thus, the modulation of membrane morphology was related to the tumor cell environment rather than the abundance of P-glycoprotein in the plasma membrane.
Published: 1990
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9. [14Co-dimetinur distribution in mice in relation to the stage of the development of tumor process].

Author: Ostrovskaia LA, Rykova VA, Kondarov AA, Etvesh L, Shimon-Trompler E, Sokolova IS, and Korman DB
Subjects: Administration, Oral, Animals, Antineoplastic Agents administration & dosage, Leukemia P388 pathology, Male, Methylnitrosourea administration & dosage, Methylnitrosourea pharmacokinetics, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Tissue Distribution, Antineoplastic Agents pharmacokinetics, Cobalt Isotopes, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy
Abstract: Pharmacokinetics of the antitumour agent 14CO-dimetinur (100 mg/kg) after oral administration to the intact mice and those with solid leukemia P 388 is characterized by its rapid delivery to organs and tumours with the achievement of maximum radioactivity 5 hours later and the further gradually decline during 4 days. The increased accumulation of the 14CO-products in kidneys and their retarded output from the brain and lungs against a background of the relatively equal distribution of radioactivity between other tested organs have been established. The same level of carbamoylated products in large tumours (the 16th day after leukemia transplantation) as well as in small tumours (the 9th day after inoculation) is in agreement with the conservation of the initial marked inhibitory effect of the drug against advanced tumours.
Published: 1990

10. Modulation of in vitro chemosensitivity by extracellular Ca++ in adriamycin sensitive and resistant P388 leukemic cells.

Author: Adwankar MK and Chitnis MP
Subjects: Animals, DNA, Neoplasm biosynthesis, Drug Resistance, Mice, Mice, Inbred DBA, Tumor Cells, Cultured drug effects, Verapamil pharmacology, Calcium pharmacology, Doxorubicin pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology
Abstract: P388 mouse lymphocytic leukemia cells sensitive (P388/S) and resistant to adriamycin (P388/Adr), respectively, were exposed in vitro to 3 dose concentrations of adriamycin, mitoxantrone, vincristine and cisplatin in the presence and absence of extracellular Ca++ at 37 degrees C for 1 h. The absence of extracellular Ca++ enhanced the cytotoxicity of all the four drugs by 25 to 30% in P388/S cells. P388/Adr cells retained their resistance to adriamycin irrespective of the presence or absence of Ca++, however, vincristine and cisplatin to which P388/Adr cells, in normal course, show cross-resistance, exhibited a 30-40% enhancement of cytotoxicity in the absence of extracellular Ca++. Cross-resistance of P388/Adr to mitoxantrone was totally circumvented in the absence of extracellular Ca++.
Published: 1990

11. Some determinants of partitioning behavior of lymphoblasts in aqueous biphasic systems.

Author: Kessel D
Subjects: Animals, Cell Line, Cell Separation, Lymphocytes drug effects, Mice, Neuraminidase pharmacology, Tunicamycin pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Lymphocytes cytology
Abstract: Partitioning behavior of murine lymphoblasts was examined in biphasic aqueous systems containing dextran and poly(ethylene glycol) with no potential difference across the interface. Persistence of cells in the upper phase of the system could be promoted by addition of the palmitate ester of poly(ethylene glycol). Partitioning effects seen here may derive from affinity of membrane sialic acid residues for dextran-rich lower-phase droplets, and antagonism of these interactions by poly(ethylene glycol) palmitate. Several determinants of partitioning behavior were examined: 1. Membrane glycosylation. Partitioning behavior of P388 and P388/ADR lymphoblasts were compared. The latter has an inherently higher degree of membrane glycosylation, resulting in a lower partition coefficient in poly(ethylene glycol) palmitate-supplemented systems. 2. Degree of esterification. Singly-esterified poly(ethylene glycol) was substantially more effective at promoting cell partition into the upper phase than was doubly-esterified glycol. Use of the latter was associated with cell-cell aggregation. 3. Relative numbers of lower-phase droplets present. Decreasing the numbers of such droplets initially present markedly increased the partition coefficient. 4. Time-dependence. Even in the presence of poly(ethylene glycol) palmitate, the partition coefficient fell with time, indicating an interaction between cells and lower-phase droplets not antagonized by the ester.
Published: 1981
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12. [Effect of harringtonine and homoharringtonine on the traverse of cell cycle of P388 leukemic cells by flow cytometry].

Author: Xue SB, Xu P, Li SW, Hu YY, Xiao JJ, Han R, and Feng JB
Subjects: Animals, Cell Cycle drug effects, Homoharringtonine, Leukemia P388 drug therapy, Mice, Alkaloids pharmacology, Flow Cytometry, Harringtonines pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology
Published: 1984

13. Effect of hyperthermia and X-irradiation on survival and occurrence of metastases in mice bearing P388 tumor.

Author: Perlaky L, Fónagy A, Unger E, and Hidvégi EJ
Subjects: Animals, Cell Survival radiation effects, Combined Modality Therapy, Leukemia P388 pathology, Leukemia P388 radiotherapy, Mice, Neoplasm Metastasis, Hot Temperature therapeutic use, Leukemia P388 therapy, Leukemia, Experimental therapy
Abstract: Survival of P388 lymphoid tumor-bearing mice and the occurrence of metastasis was studied after combined modality treatment with hyperthermia and X-irradiation. P388 ascites tumor cells were treated at 42 degrees C or 43.5 degrees C for 1 hr in vitro and transplanted on B6D2F1 mice intraperitoneally (i.p.) or intramuscularly (i.m.). Hyperthermic treatment at 43.5 degrees C increased the median survival time (MST). Increased life-span (ILS) was found after i.p. transplantation (54%) and after i.m. transplantation (30%). During the life-span of tumor-bearing animals, significantly fewer metastases were observed in liver and spleen after hyperthermia and 5-10% metastasis occurred after transplantation of ascites tumor cells treated at 43.5 degrees C in vitro compared with 90% in the untreated control animals. The lower occurrence of metastasis could not be ascribed to the higher cell-killing effect of hyperthermia. When both modalities were combined the best tumor growth retardation effect was obtained when ascites tumor cells were treated at 43.5 degrees C for 1 hr before being transplanted i.m. and 1 day later locally X-irradiated with 6 Gy. In this case, 77% ILS was found demonstrating a synergistic effect of the two modalities. While X-irradiation alone did not change the occurrence of metastasis, after combined modality treatment it was as low as with hyperthermia alone (5-10%). In connection with the significantly lower occurrence of metastasis, the possible alterations of P388 tumor cell membrane and surface proteins induced by in vitro hyperthermic treatment are discussed.
Published: 1989
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14. [Influence of homoharringtonine on the ultrastructure of murine leukemia P388 cells].

Author: Zhou JX, Zhou PQ, Dai ZQ, and Xu B
Subjects: Animals, Cells, Cultured, Cytoplasm ultrastructure, Homoharringtonine, Mice, Mitochondria ultrastructure, Ribosomes ultrastructure, Alkaloids pharmacology, Harringtonines pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology
Published: 1985

15. Vincristine-resistant P388 leukemia cells contain a large amount of calcium.

Author: Tsuruo T, Iida H, Tsukagoshi S, and Sakurai Y
Subjects: Animals, Drug Resistance, Leukemia P388 pathology, Mice, Calcium analysis, Leukemia P388 analysis, Leukemia, Experimental analysis, Vincristine pharmacology
Abstract: P388 leukemia cells resistant to vincristine contained more calcium in the cells than the parent sensitive line, especially in the form of EGTA-removable (surface-bound) calcium. Although the relationship, if any, between the high cellular calcium of resistant cells and drug-resistant phenotype is not clear, the possible implications of this result for the elucidation of the mechanisms of drug resistance are interesting.
Published: 1983

16. Novel cytotoxic and antitumor agents. IV. Withaferin A: relation of its structure to the in vitro cytotoxic effects on P388 cells.

Author: Fuska J, Fusková A, Rosazza JP, and Nicholas AW
Subjects: Animals, Cell Division drug effects, Cell Line, Cell Survival drug effects, Ergosterol pharmacology, Mice, Structure-Activity Relationship, Withanolides, Antineoplastic Agents, Phytogenic pharmacology, Ergosterol analogs & derivatives, Leukemia P388 pathology, Leukemia, Experimental pathology
Abstract: In vitro effects of withaferin A and its 9 new derivatives on P388 cells have been studied. The cytotoxicity was calculated from the utilization of precursors in protein and nucleic acid (NA) synthesis and from capacity to suppress cell proliferation. The most potent agents proved to be 4-dehydrowithaferin A and withaferin A diacetate exhibited an equal inhibitory effect on thymidine, uridine, and L-valine incorporation. They stopped cell proliferation and, at the same time, killed the cells. Cytotoxicity was found to be due to a double bond at position C2-3, by dissociating this bond the cytotoxicity markedly decreased in all derivatives. A dissociation of the double bond at C24-25 or a removal of OH group from C27 did not cause any significant changes in the biological effects of the derivatives. An addition of a carbonyl group at C4 increased the effects of the agent. An addition of OH groups to the molecule of withaferin A resulted chiefly in a qualitative change in the action of derivatives manifested by a significant decrease in L-valine inhibition. As withaferin A promptly reacted with L-cysteine, it was presumed that one of the possible target sites in the cell might be the SH groups of enzymes which react with the lactone and epoxide groups of the agent.
Published: 1984

17. Collateral sensitivity of 6-mercaptopurine-resistant sublines of P388 and L1210 leukemia to the new purine antagonists, 5-carbamoyl-1H-imidazol-4-yl piperonylate and 4-carbamoylimidazolium 5-olate.

Author: Inaba M, Fukui M, Yoshida N, Tsukagoshi S, and Sakurai Y
Subjects: Animals, Biotransformation, Cells, Cultured, Dose-Response Relationship, Drug, Drug Administration Schedule, Female, Guanosine Monophosphate metabolism, Hypoxanthine Phosphoribosyltransferase metabolism, Leukemia L1210 metabolism, Leukemia L1210 pathology, Leukemia P388 pathology, Mercaptopurine administration & dosage, Mice, Mice, Inbred BALB C, Neoplasm Transplantation, Antineoplastic Agents pharmacology, Imidazoles pharmacology, Leukemia P388 metabolism, Leukemia, Experimental metabolism, Purines biosynthesis
Abstract: Two new purine antagonists, 5-carbamoyl-1H-imidazol-4-yl piperonylate (SL-1250) and 4-carbamoylimidazolium 5-olate (SM-108), were investigated for their antitumor activities against 6-mercaptopurine (6-MP)-resistant sublines of P388 and L1210 leukemia. It was found that both resistant sublines exhibited collateral sensitivity instead of cross-resistance to these new antipurine drugs. Since more potent cytotoxic activities of these drugs against 6-MP-resistant cells were observed even in vivo cell culture systems, this collateral sensitivity was proved on a cellular basis. Biochemical studies revealed that 6-MP-resistant sublines of both P388 and L1210 leukemia are deficient in hypoxanthine-guanine phosphoribosyltransferase activity. In these cells, not only the activation of 6-MP to its nucleotide but also the synthesis of guanosine 5'-monophosphate via the salvage pathway seems to be severely restricted. However, SL-1250 and SM-108 can be activated to their nucleotide even in these 6-MP-resistant cells because the activation of these compounds is proceeded by adenine phosphoribosyltransferase. In conclusion, suppression of de novo purine synthesis with SL-1250 and SM-108 seems to be a very efficient means of killing these 6-MP-resistant cells, which lack a salvage pathway for guanosine 5'-monophosphate.
Published: 1982

18. Activity of a novel anthracenyl bishydrazone, 9,10-anthracenedicarboxyaldehyde Bis[(4,5-dihydro-1H-imidazol-2-yl)hydrazone] dihydrochloride, against experimental tumors in mice.

Author: Citarella RV, Wallace RE, Murdock KC, Angier RB, Durr FE, and Forbes M
Subjects: Animals, Anthracenes administration & dosage, Doxorubicin therapeutic use, Drug Administration Schedule, Drug Evaluation, Preclinical, Female, Fluorouracil therapeutic use, Injections, Intraperitoneal, Injections, Intravenous, Injections, Subcutaneous, Leukemia L1210 drug therapy, Leukemia P388 drug therapy, Leukemia P388 pathology, Male, Melanoma drug therapy, Melanoma pathology, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Neoplasm Transplantation, Plasmacytoma drug therapy, Plasmacytoma pathology, Anthracenes therapeutic use, Antineoplastic Agents, Leukemia, Experimental drug therapy, Neoplasms, Experimental drug therapy
Abstract: 9,10-Anthracenedicarboxaldehyde bis[(4,5-dihydro-1H-imidazol-2-yl)hydrazone] dihydrochloride (CL 216942; bisantrene hydrochloride; NSC 337766), a member of a new chemical class of compounds with antineoplastic properties, has been evaluated for antitumor activity in experimental murine tumor systems. The compound produced significant increases in life span (LS) and long-term survivors among mice bearing transplantable leukemias and solid tumors. Optimal treatment regimens resulted in an ILS of greater than 173 and 151% in mice with P388 and L1210 leukemia, respectively, an ILS of greater than 85% in mice with Lieberman plasma cell tumor, and an ILS of greater than 200, 150, and 63%, respectively, in mice with B16 melanoma, colon tumor 26, and Ridgway osteogenic sarcoma. An adriamycin-resistant subline of P388 leukemia showed complete cross-resistance to CL of 216942. The compound was active when administered by the i.p., i.v., and s.c. routes, but p.o. activity was not observed. Significant schedule dependency was not observed when the drug was administered once daily for 9 days, once every 4 days, or as a single dose, but single doses typically produced the best effects. CL 216942 was a potent inhibitor of DNA and RNA synthesis in L5178Y lymphoma cells cultured in vitro, and preliminary studies indicated the drug was a DNA-intercalating agent. The drug was cytotoxic for rapidly proliferating and nonproliferating (G0) human colon carcinoma WiDR cells in vitro.U
Published: 1982

19. Reversal of acquired resistance to doxorubicin in P388 murine leukemia cells by tamoxifen and other triparanol analogues.

Author: Ramu A, Glaubiger D, and Fuks Z
Subjects: Animals, Cell Division drug effects, Cell Survival drug effects, Drug Resistance, Estradiol metabolism, Mice, Receptors, Estrogen analysis, Structure-Activity Relationship, Doxorubicin toxicity, Leukemia P388 pathology, Leukemia, Experimental pathology, Tamoxifen pharmacology, Triparanol analogs & derivatives, Triparanol pharmacology
Abstract: The effects of the triparanol analogues chlorotrianisene, clomiphene, tamoxifen, 5-[p-(fluoren-9-ylidenemethyl)phenyl]-2-piperidineethanol (MDL 10393), MDL 8917v, nafoxidine, 2-[p-(6-methoxy-2-phenylinden-3-yl)phenoxy]triethylamine (U-11555A), 2-[p-(3,4-dihydro-6-methoxy-2-phenyl-1-naphthyl)phenoxy]triethylamine (U-10520A), and nitromifene, as well as triparanol itself, were studied in the P388 murine leukemia cell line and in a doxorubicin-resistant subline (P388/ADR). At noninhibitory concentrations, all the analogues increased the sensitivity of P388/ADR cells to doxorubicin but did not have such an effect on the doxorubicin-sensitive cells. Diethylstilbestrol, deacetylated cyclofenil (F6060), hexestrol, and 17 beta-estradiol did not have such an activity. The effects of tamoxifen on doxorubicin sensitivity of P388/ADR cells could not be reversed by 17 beta-estradiol. Estrogen receptors could not be demonstrated in either cell line. It is therefore suggested that the reversal of the doxorubicin-acquired resistance by the triparanol analogues is unrelated to their estrogenic or antiestrogenic activities. The possible clinical implications of these findings are discussed.
Published: 1984

20. [Cytometric study of the effects of destruxin E on leukemic cells in mice].

Author: Odier F, Vago P, Quiot JM, Devauchelle G, and Bureau JP
Subjects: Animals, Cell Cycle drug effects, Cell Division drug effects, Cell Line, DNA, Neoplasm analysis, Flow Cytometry, Mice, Mice, Inbred DBA, Leukemia L1210 pathology, Leukemia P388 pathology, Leukemia, Experimental pathology, Mycotoxins pharmacology
Abstract: The activity of destruxin E, a cryptogamic toxin isolated from the hyphomycete Metarhizium anisopliae, was studied on mouse leukemia cells (L 1210 and P 388) in culture. Besides a cytotoxic effect, a cytostatic effect (increase of diploïd cells proportion) was observed with all doses for P 388 (from 10 micrograms/ml to 0.001 microgram/ml) and to a concentration of 0.1 microgram/ml for L 1210. At the lower doses, the effect on cellular DNA content appears distinctly.
Published: 1987

21. Influence of 60-Hertz magnetic fields on leukemia.

Author: Thomson RA, Michaelson SM, and Nguyen QA
Subjects: Animals, Body Weight radiation effects, Female, Leukemia P388 pathology, Leukemia, Radiation-Induced pathology, Mice, Mice, Inbred DBA, Organ Size radiation effects, Spleen pathology, Spleen radiation effects, Electromagnetic Fields adverse effects, Electromagnetic Phenomena adverse effects, Leukemia P388 etiology, Leukemia, Experimental etiology, Leukemia, Radiation-Induced etiology
Abstract: Female DBA/2 mice at 8 weeks of age were implanted with P388 leukemia cells in groups of ten mice and exposed to a 60-Hz 1.4-microT, 200-microT, or 500-microT magnetic field 2-3 hours after the implant for 6 hours daily, 5 days/week until all the exposed P388-treated and nontreated mice died. Parallel exposed groups of non-P388-treated mice and P388-treated mice exposed at 0 microT were included for study. No statistically significant differences (P greater than .05) in survival, spleen weight, or body weight resulted between P388-treated or nontreated mice from exposure to the magnetic field. No effect on the incidence or progression of P388 leukemia was apparent.
Published: 1988
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22. [Colony-forming ability of bone marrow hematopoietic cells in mice with transplanted leukemia during administration of carminomycin].

Author: Kozinets GI, Ivanova LE, Khanykova OK, Kuznetsova TV, and Rudneva NA
Subjects: Animals, Carubicin therapeutic use, Colony-Forming Units Assay, Female, Hematopoietic Stem Cells pathology, Leukemia P388 drug therapy, Leukemia P388 pathology, Leukemia, Experimental drug therapy, Mice, Mice, Inbred CBA, Neoplasm Transplantation, Rats, Carubicin toxicity, Daunorubicin analogs & derivatives, Hematopoietic Stem Cells drug effects, Leukemia, Experimental pathology
Abstract: Effects of carminomycin on the colony-forming ability of bone marrow haemopoietic stem cells (CFUs) were compared in normal mice with steady state and actively regenerating bone marrow, and in P-388 and La leukemia-bearing mice. CFUs assays were performed 24 h after treatment of donor mice with the increasing doses of the drug. Leukemia-bearing mice received carminomycin on the 5th day after transplantation. The dose-effect curves were exponential for CFUS normal mice with both the steady state and active proliferation state of bone marrow. The maximal effect was found 24 h after injection of 0.7 mg/kg of carminomycin (ED50 for CFUS) being more pronounced in regenerating bone marrow. The dose-effect curves for leukemias were also exponential. In the case of La leukemia the killing of CFUs by carminomycin was the highest as compared with P-388 leukemia.
Published: 1984

23. Effects of quinidine and related compounds on cytotoxicity and cellular accumulation of vincristine and adriamycin in drug-resistant tumor cells.

Author: Tsuruo T, Iida H, Kitatani Y, Yokota K, Tsukagoshi S, and Sakurai Y
Subjects: Animals, Anti-Arrhythmia Agents pharmacology, Biological Transport drug effects, Cell Survival drug effects, Doxorubicin metabolism, Drug Resistance, Female, Kinetics, Mice, Mice, Inbred Strains, Vincristine metabolism, Doxorubicin toxicity, Leukemia P388 pathology, Leukemia, Experimental pathology, Quinidine analogs & derivatives, Quinidine pharmacology, Vincristine toxicity
Abstract: Quinidine, which has antiarrhythmic activity, greatly enhanced the cytotoxicity of vincristine (VCR) in tumor cells and especially in VCR-resistant sublines of P388 leukemia (P388/VCR) and human myelogenous leukemia. A nontoxic concentration of quinidine increased VCR cytotoxicity in these resistant tumor cells about 50 to 80 times, and the drug in combination with VCR could completely reverse VCR resistance of these cell lines. Quinidine also enhanced the cytotoxicity of Adriamycin, especially in the Adriamycin-resistant subline of P388 leukemia; this enhancement (8-fold) was less than that of VCR toxicity in the VCR-resistant tumor line. When administered daily for 10 days with VCR, quinidine at doses of 50 to 125 mg/kg significantly enhanced the chemotherapeutic effect of VCR in P388/VCR-bearing mice. Some other antiarrhythmic agents also showed similar effects in vitro, but these effects were considerably lower than that of quinidine. Quinidine increased the cellular levels of VCR and daunomycin in VCR-resistant sublines of mouse and human tumors and the ADM-resistant mouse tumor line in vitro, respectively. Quinidine also enhanced the cellular accumulation of VCR in P388/VCR cells in vivo. Thus, the therapeutic effect observed in P388/VCR-bearing mice might be due to the enhanced accumulation of VCR in P388/VCR cells by quinidine. The increase of cellular accumulation of VCR was partly explained by inhibition of efflux of VCR and daunomycin from the resistant tumor cells. The mechanism of this phenomenon is discussed in relation to previous findings on calcium channel blockers.
Published: 1984

24. Cross-resistance of cultured murine leukemia vincristine-resistant P388 cells to vinblastine, vindesine, and bis (N-ethylidene vindesine) disulfide, disulfate.

Author: Wilkoff LJ and Dulmadge EA
Subjects: Animals, Cell Survival, Cells, Cultured, Dose-Response Relationship, Drug, Drug Resistance, Mice, Mice, Inbred C57BL, Probability, Vinblastine pharmacology, Vincristine pharmacology, Vindesine, Antineoplastic Agents, Phytogenic pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Vinblastine analogs & derivatives
Abstract: Cultured P388 leukemia cells derived from vincristine (VCR)-resistant cell populations developed in vivo in (C57BL X DBA/2)F1 mice (P388/VCR) were cross-resistant to vinblastine (VLB), vindesine (VDS), and bis(N-ethylidene vindesine)disulfide, disulfate (bis-VDS). Cross-resistance was a function of concentration and time of exposure. Cultured P388/VCR cells were more sensitive to 6.1x10-5Mbis- VDS than to 6.1x10-5MVDS or to 6.1x10-5MVLB. Cultured P388 cells derived from VCR-sensitive P388 leukemia passaged in vivo (P388/0)were significantly more sensitive to VDS and bis-VDS than to VLB. This degree of difference in sensitivity was also a function of concentration and time of exposure.
Published: 1982

25. Role of the calmodulin inhibitor trifluoperazine on the induction and expression of cell cycle traverse perturbations and cytotoxicity of daunorubicin and doxorubicin (adriamycin) in doxorubicin-resistant P388 mouse leukaemia cells.

Author: Ganapathi R, Yen A, Grabowski D, Schmidt H, Turinic R, and Valenzuela R
Subjects: Animals, Cell Cycle drug effects, Cell Survival drug effects, Cells, Cultured, Drug Resistance, Mice, Time Factors, Daunorubicin pharmacology, Doxorubicin pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Trifluoperazine pharmacology
Published: 1986
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26. Induction of functional Fc receptors in P388 leukemia cells. Requirement for multiple differentiation signals.

Author: Cohen DA, Stotelmyer NL, and Kaplan AM
Subjects: Animals, Cell Adhesion, Cell Division drug effects, Cell Line, Immunoglobulin G immunology, Leukemia P388 pathology, Lymphokines pharmacology, Mice, Phagocytosis, Tetradecanoylphorbol Acetate pharmacology, Leukemia P388 immunology, Leukemia, Experimental immunology, Receptors, Fc immunology
Abstract: The development of functional Fc receptors (FcR) during induced differentiation with the tumor promoter, phorbol myristate acetate (PMA), was studied in the murine tumor cell line, P388. PMA induced the appearance of FcR on the membranes of P388 cells as indicated by the binding of IgG-coated sheep red blood cells (IgG-SRBC). Concentrations of PMA as low as 1 ng/ml were sufficient to induce the expression of FcR as well as to inhibit cellular division and to induce adherence in the P388 tumor cell line; however, optimal FcR induction occurred at PMA concentrations of 10-100 ng/ml. Immunofluorescent analysis with heat-aggregated myeloma proteins indicated that PMA induced FcR which were capable of binding IgG2a and IgG2b immunoglobulins, but not IgG1. Adherence to a substratum was determined to be a second required signal for expression of FcR, since PMA induction of P388 tumor cells in teflon dishes failed to fully develop FcR and adherence of P388 cells to poly-L-lysine-coated culture dishes in the absence of PMA was insufficient for FcR expression. FcR which appeared after PMA induction were non-functional in the sense that membrane-bound IgG-SRBC were not ingested to any significant extent by the tumor cells. However, if FcR induction occurred in the presence conA-induced rat spleen cell culture supernatants, phagocytosis of membrane-bound erythrocytes occurred. These findings suggest that for the expression of FcR which are capable of particle internalization, at least three identifiable membrane-transmitted signals are required during differentiation.
Published: 1985
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27. Increased plasma membrane traffic in daunorubicin resistant P388 leukaemic cells. Effect of daunorubicin and verapamil.

Author: Sehested M, Skovsgaard T, van Deurs B, and Winther-Nielsen H
Subjects: Animals, Drug Resistance, Endocytosis, Exocytosis, Female, Leukemia P388 pathology, Male, Mice, Mice, Inbred Strains, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured ultrastructure, Cell Membrane drug effects, Daunorubicin therapeutic use, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy, Verapamil therapeutic use
Abstract: Numerous studies have indicated that the plasma membrane plays an important role in the development of resistance to anthracycline and vinca alkaloid drugs (pleiotropic resistance). We have previously shown that pleiotropically resistant Ehrlich ascites tumour cells, which are of epithelial origin, have a significantly increased plasma membrane traffic (endo/exocytosis) to the endosomal compartment compared to sensitive cells. The present study, using the same ultrastructural morphometric technique, has demonstrated a similar significant difference in plasma membrane traffic between daunorubicin resistant and sensitive P388 cell lines (which are of lymphoid origin). Furthermore, we have shown that this difference between the P388 sublines is accompanied by an approximately 4 fold increase in the plasma membrane area participating in recycling together with an increased endosomal volume, number and membrane area in resistant cells. Plasma membrane traffic in resistant cells was significantly inhibited by the calcium channel blocker verapamil, a well known modulator of anthracycline resistance, but unaffected by daunorubicin itself. The confirmation of this phenotype in an additional pleiotropically resistant cell type with a different histogenesis further supports a hypothesis of endosomal drug trapping and vesicular extrusion as a possible resistance mechanism.
Published: 1987
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28. Comparative studies on biological activity of /+/R and /-/S enantiomers of cyclophosphamide and ifosfamide. II. Antiproliferative activity of cyclophosphamide and ifosfamide enantiomers.

Author: Paprocka M and Radzikowski C
Subjects: Animals, Cyclophosphamide pharmacology, Ifosfamide pharmacology, Lung Neoplasms pathology, Mice, Mice, Inbred Strains, Neoplasm Metastasis, Stereoisomerism, Structure-Activity Relationship, Tumor Stem Cell Assay, Cyclophosphamide analogs & derivatives, Cyclophosphamide therapeutic use, Ifosfamide analogs & derivatives, Leukemia P388 pathology, Leukemia, Experimental pathology, Lung Neoplasms drug therapy
Abstract: The present studies on antiproliferative activity of cyclophosphamide and ifosfamide /+/R and /-/S enantiomers followed the earlier described differences in their antitumour activity. P-388 leukemic cells in LCFU (Leukemic Colony Forming Units) assay and Lewis lung cells in experimental metastasis assay were used as models of tumour cells. Bone marrow stem cells were applied as models of normal proliferating cells in NCFU-(Normal Colony Forming Units) and RPNCFU (Rapidly Proliferating Normal Colony Forming Units) tests. In all four models /-/S enantiomers exerted higher antiproliferative effect, than their counterparts. Antiproliferative activity of /+/RS cyclophosphamide and ifosfamide appeared to be exactly intermediate between /+/R and /-/S forms. These data, precisely differentiating the effect of /+/R, /-/S and / +/- /RS forms, confirmed the earlier described, higher antitumour effect of /-/S enantiomers of cyclophosphamide and ifosfamide.
Published: 1986

29. [Behavior and role of mastocytes and eosinophils in natural and transplantable lymphatic leukemia in mice].

Author: Madej JA and Kaszubkiewicz C
Subjects: Animals, Lymph Nodes pathology, Male, Mice, Neoplasm Transplantation, Eosinophils pathology, Leukemia L1210 pathology, Leukemia P388 pathology, Leukemia, Experimental pathology, Mast Cells pathology
Abstract: The behavior and role of mast cells and eosinophils, to the spleen cooperations between this cells at the natural and transplantable lymphatic leukaemia L 1210 and P 388 in mice. Mast cells and eosinophils are treated at the differences leukaemia organism in addition to the smearing blood. The growth and the quantity for this cells has been elevated at the beginning of the initial phase of neoplasia and the second decrease is very fast in comparing for the sort of leukaemia (natural, transplantable). The describe for this phenomenon in the bind for the heavy metals part in leukemogenesis.
Published: 1986

30. Formation, resealing and persistence of DNA breaks produced by 4-demethoxydaunorubicin in P388 leukemia cells.

Author: Capranico G, Tinelli S, and Zunino F
Subjects: Animals, Cell Survival drug effects, Drug Resistance, Idarubicin metabolism, Kinetics, Leukemia P388 metabolism, Leukemia P388 pathology, Mice, Topoisomerase II Inhibitors, Tumor Cells, Cultured, DNA drug effects, DNA Damage, Idarubicin pharmacology, Leukemia P388 genetics, Leukemia, Experimental genetics
Abstract: The formation and disappearance of DNA single-strand breaks (SSB) produced by 4-demethoxydaunorubicin (4-dmDR) in P388 murine leukemia cells and in a resistant subline were examined by alkaline elution methods in relation to cellular pharmacokinetics. DNA strand breaks produced by this intercalating agent were essentially DNA lesions mediated by topoisomerase II, even at very high drug concentrations, since they were detected as protein-associated breaks by filter elution. Similarly, the appearance of delayed DNA breaks in cells exposed to high concentrations, following drug removal, showed predominance of protein-associated breaks, thus supporting a similar mechanism of breakage induction. This finding indirectly suggests that, in this experimental model, free radical production makes little (if any) contribution to DNA damage, and also that DNA effects are not the consequence of early cell death. In contrast to a rapid disappearance of protein-associated strand breaks produced by intercalating agents and topoisomerase II inhibitors of different classes, DNA breaks induced by low concentrations of the anthracycline derivative are only partially reversible following drug removal, but they persisted and even increased with high concentrations. Thus, not only the extent of DNA breaks but also their persistence may contribute to the cytotoxic potency of anthracyclines. The importance of DNA lesions to cytotoxic action of the anthracycline is also emphasized by drug effect on the resistant line. A negligible effect on DNA of resistant cells was detected at drug concentrations lethal to sensitive cells. However, exposure to equitoxic drug concentrations resulted in a comparable amount of DNA breaks in sensitive and resistant cells. Although faster DNA rejoining in resistant cells may be in part attributable to increased efflux of drug, no correlation exists between cell drug accumulation and extent of DNA lesions. With equitoxic drug concentrations cellular drug content was higher in resistant cells, suggesting an intrinsic insensitivity of this variant to DNA cleavage effects of the anthracycline.
Published: 1989
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31. Identification of Vinca alkaloid acceptors in P388 murine leukemia cells with a photoactive analogue of vinblastine.

Author: Safa AR, Glover CJ, and Felsted RL
Subjects: Animals, Azides pharmacology, Leukemia P388 drug therapy, Leukemia P388 pathology, Mice, Molecular Weight, Vinblastine metabolism, Vinblastine pharmacology, Vindesine metabolism, Vindesine pharmacology, Affinity Labels metabolism, Azides metabolism, Leukemia P388 metabolism, Leukemia, Experimental metabolism, Receptors, Drug analysis, Vinca Alkaloids metabolism, Vindesine analogs & derivatives
Abstract: The cytotoxic, antimitotic, and growth inhibition properties of a photoactive analogue of vinblastine, N-(p-azidobenzoyl)-N'-beta-aminoethylvindesine (NABV), and vinblastine on P388 murine leukemia cells were compared. After 72-h exposure, the 50% drug-inhibitory concentrations for exponentially growing P388 leukemic cells were 1.2 nM for NABV and 0.6 nM for vinblastine. The ultrastructural effects of NABV and vinblastine on P388 cells were similar: formation of tubulin paracrystals; mitotic arrest (C-mitosis); increased post-C-mitotic multinucleated cells; increased number of annulate lamellae; and the appearance of intracytoplasmic paired cisternae. [3H]NABV was used to identify Vinca alkaloid binding sites in P388 cells by photoaffinity labeling. After irradiation at 302 nm, radioactive Vinca alkaloid binding components were resolved by sodium dodecyl sulfate-polyacrylamide gel electrophoresis and identified in 1-mm gel slices. The most prominent photolabeled species were Mr 44,000, 54,000, and 75,000 polypeptides located in the 100,000 X g supernatant fraction. The Mr 54,000 component was also observed in the membrane fraction. Specific photolabeling of Mr 54,000 and 44,000 polypeptides was blocked in the presence of 20 microM excess of vinblastine and was saturable with half-maximal saturation concentrations of 0.18 and 0.4 microM [3H]NABV, respectively. The Mr 54,000 component was identified as a tubulin subunit by immunoprecipitation with antitubulin monoclonal antibodies. Since NABV and vinblastine have similar pharmacological and biological properties, this photoactive analogue may be useful for identifying important Vinca alkaloid cellular acceptors which may be responsible for drug cytotoxic and antineoplastic activities.
Published: 1987

32. Antitumor activity and toxicity in animals of RR-150 (7-cysteaminomitosane), a new mitomycin derivative.

Author: Bradner WT, Rose WC, Schurig JE, Schlein A, and Huftalen JB
Subjects: Animals, Colonic Neoplasms pathology, Drug Evaluation, Preclinical, Drug Resistance, Leukemia L1210 pathology, Leukemia P388 pathology, Leukocyte Count, Lung Neoplasms pathology, Male, Melanoma pathology, Mice, Mice, Inbred DBA, Mice, Inbred Strains, Mitomycin, Antibiotics, Antineoplastic toxicity, Leukemia, Experimental pathology, Mitomycins toxicity, Neoplasms, Experimental pathology
Abstract: The experimental antitumor activity of a new mitomycin derivative, 7-cysteaminomitosane (RR-150), was evaluated in mice. When administered i.p. to mice bearing i.p.-implanted tumors, RR-150 was superior to mitomycin C (MMC) in increasing the life span of animals bearing P388 leukemia, B16 melanoma, and a line of L1210 leukemia partially resistant to MMC. RR-150 appeared comparable to MMC in increasing life span of mice bearing Madison 109 lung carcinoma, Colon 26 carcinoma, or parental (nonresistant) L1210 leukemia. Mice immunosuppressed with 550 rads whole-body irradiation prior to i.p. implantation of B16 still benefited (e.g., 40% cure rate) following optimal RR-150 therapy when compared to nonirradiated, B16-implanted mice given RR-150 (e.g., 70% cure rate). RR-150 had inconsistent activity in the treatment of s.c.-implanted tumors. In toxicity evaluations, RR-150 was comparable to MMC in suppression of total while blood cell counts but appeared to be less neutropenic. RR-150 also caused less cumulative leukopenia than did MMC in a weekly chronic dose experiment. Based on serum chemistries, RR-150 did not have significant nephrotoxicity, but there was evidence of possible liver toxicity at doses near the 50% lethal dose. Because of the balance of favorable antitumor and toxicity properties of RR-150, work is under way to prepare a more bioavailable form for advanced evaluation.
Published: 1984

33. The cytotoxicity of T-2 toxin and related 12,13-epoxytrichothecenes to Adriamycin-sensitive and -resistant P388 leukemia cells.

Author: Ramu A, Yagen B, and Ramu N
Subjects: Animals, Cell Division drug effects, Chemical Phenomena, Chemistry, Drug Resistance, Drug Screening Assays, Antitumor, Esterification, Hydroxylation, Mice, Solubility, Structure-Activity Relationship, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured pathology, Verapamil pharmacology, Water, Antineoplastic Agents, Doxorubicin pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Sesquiterpenes pharmacology, T-2 Toxin pharmacology, Trichothecenes pharmacology
Abstract: The cytotoxicity of T-2 toxin and related trichothecenes was studied in Adriamycin-sensitive and -resistant P388 leukemia cells in vitro. The structure-activity relationship indicated that a free hydroxyl in the C-3 position contributed to the activity. Free hydroxyls at the 4, 8, and 15 positions interfered with the activity, and their estrification resulted in improved cytotoxicity. The cytotoxic activity of these trichothecenes did not seem to be related to their degree of lipophilicity. Adriamycin-resistant P388 cells were cross-resistant to the trichothecenes, and this resistance could be circumvented by verapamil.
Published: 1989
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34. Evidence for indirect involvement of thymidine kinase in excision repair processes in mouse cell lines.

Author: McKenna PG, Yasseen AA, and McKelvey VJ
Subjects: Animals, Cell Line, Cell Survival drug effects, Cell Survival radiation effects, Clone Cells, Drug Resistance, Leukemia L5178 enzymology, Leukemia L5178 pathology, Leukemia P388 enzymology, Leukemia P388 pathology, Mice, Mutagens toxicity, Mutation, Thioguanine pharmacology, Thymidine Kinase deficiency, Ultraviolet Rays, DNA Repair drug effects, DNA Repair radiation effects, DNA, Neoplasm biosynthesis, Leukemia L5178 genetics, Leukemia P388 genetics, Leukemia, Experimental genetics, Thymidine Kinase genetics
Abstract: Wild-type cells and thymidine kinase-deficient clones from two mouse lymphoma cell lines, P388 and L5178Y, were compared for sensitivity to killing by the mutagens, ultraviolet irradiation (UV), ethyl methane sulfonate (EMS), and N-methyl-N'-nitro-N-nitrosoguanidine (MNNG). Two out of three thymidine kinase-deficient P388 clones showed significantly enhanced sensitivity to killing by all three mutagens. This increased sensitivity to killing was also reflected in increased mutagenesis by the three mutagens. In the L5178Y cell line, wild-type cells showed little difference to two thymidine kinase-deficient clones in terms of mutagen sensitivity. This indicates that thymidine kinase may be significant for DNA repair processes in P388 but not in L5178Y cells. Unscheduled DNA synthesis (UDS) experiments were carried out on P388 and L5178Y wild-type cells and wild-type Friend leukemia cells (which are mutagen-sensitive when deficient in thymidine kinase). The UDS experiments showed the L5178Y cells were low in excision repair abilities relative to the P388 cells and the Friend cell clone. This indicates that the increased mutagen sensitivity in thymidine kinase-deficient P388 and clone 707 Friend cells may be due to thymidine kinase playing an indirect role in DNA excision repair, a process which is of little significance in the L5178Y cell line.
Published: 1985
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35. Platinum incorporation and differential effects of cis- and trans-diamminedichloroplatinum(II) on the growth of mouse leukemia P388/D1.

Author: Just G and Holler E
Subjects: Animals, Cell Division drug effects, DNA, Neoplasm analysis, Flow Cytometry, Mice, Neoplasm Proteins analysis, Platinum pharmacokinetics, Spectrometry, Fluorescence, Tumor Cells, Cultured, Cisplatin pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology
Abstract: The parallel effects of cis-diamminedichloroplatinum(II) (1 microM) or trans-diamminedichloroplatinum(II) (20 microM) on the growth of mouse leukemia P388/D1 in culture, on the cellular content of protein/DNA, on the average cell volume, and on the distribution in different phases of the cell cycle were measured over a period of 70 h and compared with the amount of platinum residing in the cells. Despite different concentrations in the culture medium, similar amounts of cis- and trans-diamminedichloroplatinum(II) were incorporated. The platinum content of cells passed through an early concentration maximum in the millimolar range and decreased during prolonged times of incubation. Effects of cis-diamminedichloroplatinum(II) were marked and irreversible whereas those of trans-diamminedichloroplatinum(II) were small and transient. Proliferation was inhibited, while synthesis of protein and DNA continued almost unaffected. Cells were arrested in G2-phase of the cell cycle, and their volume increased correspondingly. The results suggested an inhibition of mitotic events, rather than of DNA replication, that caused cell arrest.
Published: 1989

36. Restoration of doxorubicin responsiveness in doxorubicin-resistant P388 murine leukaemia cells.

Author: Ramu A, Spanier R, Rahamimoff H, and Fuks Z
Subjects: Animals, Calcium metabolism, Cell Line, Cell Membrane metabolism, Drug Resistance, Drug Synergism, Leukemia P388 pathology, Mice, Synaptic Vesicles metabolism, Cardiovascular Agents pharmacology, Doxorubicin pharmacology, Leukemia P388 metabolism, Leukemia, Experimental metabolism
Abstract: The effects of certain compounds on the in vitro growth rate and the sensitivity to doxorubicin of P388 murine leukaemia cell line and of a doxorubicin-resistant subline (P388/ADR) were studied. The calcium channel blocking activity of these compounds was evaluated by measuring their effects on the sodium-dependent and membrane potential-dependent calcium uptake in synaptic plasma membrane vesicles. At non-inhibitory concentrations, verapamil, dipyridamole, meclizine and nicardipine were highly active in restoring the sensitivity to doxorubicin of P388/ADR cells. Moderately active were propranolol, N-(beta-diethylaminoethyl)-N-(beta-hydroxy-beta-phenylethyl)-2,5-dich loranaline (MDL-6792), thioridazine and chlorocyclizine, while nifedipine, guanethidine, phentolamine, chloroquine and papaverine had zero or only minimal synergistic activity to doxorubicin in this cell line. Doxorubicin synergistic activity could not be demonstrated in the parent drug-sensitive cell line. No sodium-dependent or membrane potential-dependent calcium uptake could be demonstrated in vesicles prepared from plasma membranes of either cell line. There is no correlation between the ability of these compounds to inhibit calcium uptake in synaptic vesicles and their potency in restoring the sensitivity of P388/ADR cells to doxorubicin.
Published: 1984
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37. Carcinogenesis and aging. VIII. Effect of host age on tumour growth, metastatic potential, and chemotherapeutic sensitivity to 1.4-benzoquinone-guanylhydrazonethiosemicarbazone (ambazone) and 5-fluorouracil in mice and rats.

Author: Baumgart J, Zhukovskaya NV, and Anisimov VN
Subjects: Adenocarcinoma drug therapy, Animals, Cell Division, Female, Leukemia P388 drug therapy, Male, Mammary Neoplasms, Experimental drug therapy, Melanoma, Experimental drug therapy, Mice, Mice, Inbred C57BL, Mitoguazone therapeutic use, Neoplasm Metastasis, Rats, Rhabdomyosarcoma drug therapy, Adenocarcinoma pathology, Aging physiology, Antineoplastic Agents therapeutic use, Fluorouracil therapeutic use, Leukemia P388 pathology, Leukemia, Experimental pathology, Mammary Neoplasms, Experimental pathology, Melanoma, Experimental pathology, Mitoguazone analogs & derivatives, Rhabdomyosarcoma pathology
Abstract: Mice and rats of various ages (3, 10-12, and 18-19 months) were inoculated with the transplantation tumours murine melanoma B16 (B16), mammary adenocarcinoma 755 (Ca-755), leukemia P388 (P388), and rat rhabdomyosarcoma RA-2 (RA-2). Subcutaneous (sc) growth of B16 was not markedly affected by the age of the syngeneic host whereas intravenously (iv) inoculated 12 months old C57BL/6 mice developed more pulmonary metastases than animals 3 months of age. Median survival time (MST) of 18 months old mice bearing Ca-755 was significantly shorter than that of younger individuals. In contrast, old rats that had been injected RA-2 iv survived longer than controls. Survival of DBA/2 mice inoculated intraperitoneally (ip) with P388 cells was not influenced by the age of the host. The antineoplastic activity of ambazone and, to a less extent, of 5-fluorouracil against P388 was drastically lower in 12 months old mice than in 3 months old tumour bearers. Likewise a graduate loss of antineoplastic activity of ambazone against Ca-755 was observed with increasing age of the mice, whereas the effect of ambazone and 5-fluorouracil against RA-2 did not depend on the age of the rats. It is suggested that tumour-host interactions as well as pharmacokinetics of a given drug may underlie age-related changes.
Published: 1988

38. Effect of RC-18, a new anticancer principle isolated from Rubia cordifolia, Linn. on cell cycle of P388 tumour system.

Author: Adwankar MK and Chitnis MP
Subjects: Animals, Cell Cycle drug effects, Mice, Antineoplastic Agents, Phytogenic pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Plant Extracts
Published: 1982

39. Glutathione cycle activity and pyridine nucleotide levels in oxidant-induced injury of cells.

Author: Schraufstätter IU, Hinshaw DB, Hyslop PA, Spragg RG, and Cochrane CG
Subjects: Animals, Glutathione analogs & derivatives, Glutathione Disulfide, Humans, Leukemia P388 pathology, Oxidation-Reduction, Pentose Phosphate Pathway drug effects, Glutathione metabolism, Hydrogen Peroxide toxicity, Leukemia P388 metabolism, Leukemia, Experimental metabolism, NAD metabolism, NADP metabolism
Abstract: Exposure of target cells to a bolus of H2O2 induced cell lysis after a latent period of several hours, which was prevented only when the H2O2 was removed within the first 30 min of injury by addition of catalase. This indicated that early metabolic events take place that are important in the fate of the cell exposed to oxidants. In this study, we described two early and independent events of H2O2-induced injury in P388D1 macrophagelike tumor cells: activation of the glutathione cycle and depletion of cellular NAD. Glutathione cycle and hexose monophosphate shunt (HMPS) were activated within seconds after the addition of H2O2. High HMPS activity maintained glutathione that was largely reduced. However, when HMPS activity was inhibited--by glucose depletion or by incubation at 4 degrees C--glutathione remained in the oxidized state. Total pyridine nucleotide levels were diminished when cells were exposed to H2O2, and the breakdown product, nicotinamide, was recovered in the extracellular medium. Intracellular NAD levels fell by 80% within 20 min of exposure of cells to H2O2. The loss of NADP(H) and stimulation of the HMPS could be prevented when the glutathione cycle was inhibited by either blocking glutathione synthesis with buthionine sulfoximine (BSO) or by inhibiting glutathione reductase with (1,3-bis) 2 chlorethyl-1-nitrosourea. The loss of NAD developed independently of glutathione cycle and HMPS activity, as it also occurred in BSO-treated cells.
Published: 1985
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40. In vitro antiproliferative activity of 2'-(2-hydroxyphenyl)-2'-thiazoline-4'-carboxylic acid and its methyl ester on L1210 and P388 murine neoplasms.

Author: Elliot GT, Kelly KF, Bonna RL, Wardlaw TR, and Burns ER
Subjects: Animals, Cell Cycle drug effects, Cell Division drug effects, Depression, Chemical, Hydroxyurea pharmacology, Mice, Tumor Cells, Cultured drug effects, Imides pharmacology, Leukemia L1210 pathology, Leukemia P388 pathology, Leukemia, Experimental pathology, Thiazoles pharmacology
Abstract: The activity of three iron chelators, methyl [2'-(2-hydroxyphenyl)-2'-thiazoline-4'-carboxylate] (MTL); 2'-(2-hydroxyphenyl)-2'-thiazoline-4'-carboxylic acid (TFAL); and 2-hydroxyphenyl-imido-ethyl-ether (Imidate), regarding antiproliferative, cytocidal, and cell-cycle effects are reported and compared with hydroxyurea (HU). In vitro, against L1210 and P388 murine neoplasms, MTL and TFAL displayed substantially greater antiproliferative activity than HU, although Imidate displayed no appreciable activity. MTL also induced a statistically more complete G1/S cell-boundary block than did HU at equimolar concentrations (100 microM). The IC50 values produced by MTL and TFAL were low enough (less than or equal to 20 microM) to warrant further testing of these chelators as potential antineoplastic agents.
Published: 1988
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41. In the search for new anticancer drugs. XX: A comparison of the in vitro growth inhibition of P388 cells by TEPA and N,N;N',N'-bis (1,2-ethanediyl)-N''-(1-oxyl-2,2,6,6-tetramethyl-4- piperidinylaminocarbonyl) phosphoric triamide and congeners.

Author: Miller B, Sosnovsky G, Rao NU, and Gutierrez PL
Subjects: Animals, Cell Line, Structure-Activity Relationship, Thiotepa pharmacology, Triethylenephosphoramide analogs & derivatives, Triethylenephosphoramide metabolism, Antineoplastic Agents pharmacology, Azirines pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Triethylenephosphoramide pharmacology
Abstract: We tested the in vitro growth inhibitory activity of TEPA, and three analogs against P388 murine lymphocytic leukemia cells in culture. The analogs consist of spin-labeled TEPA and two reduced forms containing the NH and NOH groups instead of the nitroxyl function. Spin label TEPA was obtained by replacing one of the aziridine groups in TEPA with spin-labeled urea. In a concentration range of 10(-6)-10(-5) M, only the reduced analog containing the NH group was active. That is, to achieve a 50% inhibition of cell growth, a five-fold excess in concentration of this analog (IC50 = 10 X 10(-6) M) was needed as compared to the parent compound TEPA (IC50 = 2 X 10(-6) M). These results are in contrast with those obtained in vivo against the same leukemia cell line, indicating inherent discrepancies between in vivo and in vitro evaluation of antitumor agents.
Published: 1987
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42. Cross resistance and cellular uptake of 4'-O-methyldoxorubicin in experimental tumors with acquired resistance to doxorubicin.

Author: Di Marco A, Skovsgaard T, Casazza AM, Pratesi G, Nissen NI, and Danø K
Subjects: Absorption, Animals, Antineoplastic Agents metabolism, Carcinoma, Ehrlich Tumor pathology, Doxorubicin metabolism, Drug Resistance, Leukemia P388 pathology, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Carcinoma, Ehrlich Tumor metabolism, Doxorubicin analogs & derivatives, Doxorubicin pharmacology, Leukemia P388 metabolism, Leukemia, Experimental metabolism
Abstract: A new analog of doxorubicin, 4'-O-methyldoxorubicin, was previously reported to have a pronounced activity against L1210 leukemia, which shows a natural partial resistance to doxorubicin itself. In the present study, lines of P388 leukemia and Ehrlich ascites tumor with acquired resistance to doxorubicin were found to be cross-resistant to 4'-O-methyldoxorubicin, indicating that the natural and the acquired resistance to doxorubicin involve different mechanisms. In vitro studies on the uptake of 4'-O-methyldoxorubicin in the Ehrlich ascites tumor cells indicated that the observed cross-resistance was partly due to a decreased drug uptake in the resistant cells because of an increased extrusion of the drug, in accordance with previous findings on the mechanism of acquired resistance to doxorubicin.
Published: 1981
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43. [Kinetics of etoposide cytotoxicity against mouse P388 leukemia].

Author: Takahashi K and Iwabuchi M
Subjects: Animals, Bleomycin pharmacology, Cell Cycle drug effects, Cell Survival drug effects, Cisplatin pharmacology, Cytarabine pharmacology, Doxorubicin pharmacology, Fluorouracil pharmacology, Melphalan pharmacology, Mice, Peplomycin, Podophyllotoxin pharmacology, Vinblastine pharmacology, Colony-Forming Units Assay, Etoposide pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology, Podophyllotoxin analogs & derivatives, Tumor Stem Cell Assay
Abstract: The in vitro cytotoxicity of etoposide against mouse P388 leukemia cells was kinetically studied and compared with those of podophyllotoxin, the parent compound, and other antitumor agents. When P388 cells were exposed to etoposide, surviving-cell fraction decreased with etoposide concentration and exposure time. Similar results were obtained with doxorubicin, peplomycin and cisplatin. The cytotoxicity of melphalan was dependent on concentration but scarcely on exposure time. From these data, n in Cn X T = K where T, C and K are exposure time, concentration required for killing 90% of P388 cells and a constant, respectively, was calculated. Etoposide gave an n value of 1.16. n values for doxorubicin, peplomycin and cisplatin, all belonging to the Shimoyama type Ib group where the cytotoxicity of the agent depends on both concentration and exposure time, were 1.29, 1.28 and 3.03, respectively. The n value for melphalan, belonging to the type Ia group where cytotoxicity depends only on concentration, was 54.0. From these results, it was concluded that etoposide is of type Ib. The cytotoxicities of podophyllotoxin, 5-fluorouracil, cytarabine and vinblastine were greatly dependent on exposure time. Podophyllotoxin may be an agent of type II whose cytotoxicity depends only on exposure time.
Published: 1985

44. Biological characterization of three new spontaneous mouse lymphomas and comparison with the leukemia P388.

Author: Baumgart J, Güttner J, Zborowska E, and Czarnomska A
Subjects: Animals, Antineoplastic Agents therapeutic use, Female, Leukemia P388 pathology, Lymphoma pathology, Mice, Mitoguazone analogs & derivatives, Mitoguazone therapeutic use, Neoplasm Transplantation, Drug Screening Assays, Antitumor, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy, Lymphoma drug therapy
Abstract: Three spontaneous lymphomas of 23- to 24-month-old (AB/Jena X DBA/2 Jena)F1 females were serially transplanted into syngeneic hosts. They were histologically classified as malignant lymphoblastic lymphomas (ABDt2 and ABDt5) and as a malignant lymphoma of histiocytic type (ABDt6). All lymphomas disseminated into the liver, spleen, and pancreas, whereas ABDt2 and ABDt5 additionally infiltrated the bone marrow and leptomeninx. None of the tumors showed a leukemic growth form, but extreme granulocytosis was observed in leukemia P388-bearing mice. Since the lymphomas ABDt2 and ABDt5 expressed T-cell differentiation antigens Ly-1, Ly-2, and Ly-3, they are thought to be of T-cell origin. On the contrary to the lymphocytes of parental mouse strain ABDt2 and ABDt5 cells reacted with anti H-2.23 allosera. All tumors have been found to be sensitive to at least 5/7 clinically used anticancer drugs. But only ABDt2- and P388-bearing mice survived longer than 60 days after treatment with the potent anticancer drug 1,4-benzoquinone-guanylhydrazone-thiosemicarbazone (ambazone). Successful chemotherapy of both tumors was accompanied with resistance of the hosts against the second transplant of the same tumor. Summarizing the characteristics of the newly established transplantation tumors it is concluded that they can be recommended as screening models in the search for new antineoplastic agents.
Published: 1988

45. Effects of p-(3,3-dimethyl-1-triazeno)benzoic acid potassium salt on leukemic infiltration of brain and liver in mice bearing P388 leukemia.

Author: Sava G, Giraldi T, Bartoli-Klugmann F, Decorti G, and Mallardi F
Subjects: Animals, Leukemia P388 pathology, Leukemia, Experimental pathology, Mice, Mice, Inbred Strains, Neoplasm Transplantation, Time Factors, Antineoplastic Agents therapeutic use, Brain pathology, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy, Liver pathology, Triazenes therapeutic use
Published: 1984
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46. Potentiation of harringtonine cytotoxicity by calcium antagonist diltiazem and biscoclaurine alkaloid cepharanthine in adriamycin-resistant P388 murine leukemia and K562 human leukemia cells.

Author: Yamamoto S, Hui PZ, Fukuda Y, Tatsumi K, and Mino M
Subjects: Animals, Benzylisoquinolines, Biological Transport drug effects, Cell Count, Cell Line, Cell Survival drug effects, Doxorubicin pharmacology, Drug Resistance, Growth Inhibitors pharmacology, Harringtonines therapeutic use, Humans, Leukemia P388 drug therapy, Leukemia P388 pathology, Vincristine pharmacology, Alkaloids pharmacology, Diltiazem pharmacology, Harringtonines pharmacology, Leukemia, Experimental pathology
Abstract: Harringtonine showed cross resistance in adriamycin-resistant murine leukemia P388 (P388/ADM) and human leukemia K562 (K562/ADM) cells. The relative resistance of the P388/ADM and K562/ADM cells to harringtonine was about 7 and 40, respectively. Calcium influx blockers, diltiazem and the biscoclaurine alkaloid cepharanthine enhanced the cytotoxicity of harringtonine in P388/ADM and K562/ADM cells. The extent of enhancement was different for the two drugs, and up to a 9- to 10-fold increase in harringtonine cytotoxicity occurred in P388/ADM cells, and 14- to 22-fold enhancement in K562/ADM cells with diltiazem or cepharanthine. Harringtonine resistance of P388/ADM was circumvented completely, and the resistance of K562/ADM was circumvented partially, by diltiazem or cepharanthine. The mechanism of enhanced cytotoxicity by diltiazem and cepharanthine is probably inhibition of active efflux of harringtonine in P388/ADM and K562/ADM cells.
Published: 1989

47. Comparison of in vitro assays for detecting subpopulations of P388 leukemic cells resistant to AraC.

Author: Raza A, Kuliczkowski K, Weidong G, and Preisler HD
Subjects: Animals, Cell Survival drug effects, Cytarabine metabolism, DNA, Neoplasm biosynthesis, Drug Resistance, Leukemia P388 drug therapy, Mice, Tritium, Cytarabine pharmacology, Leukemia P388 pathology, Leukemia, Experimental pathology
Abstract: The kinetics of cytosine arabinoside (AraC) were studied in vitro using P388 murine leukemia lines sensitive (P388-S) and resistant (P388-R) to the drug. Using P388-S cells, the 3H-thymidine index (L.I.) was paralleled by the 3H-AraC index, i.e. any cell in the S-phase of the cycle also incorporated the 3H-AraC into DNA. With the resistant line, the 3H-AraC index was zero in spite of high L.I. This discrepancy between the L.I. and 3H-AraC index could be used to predict the percentage of resistant cells when known mixtures of sensitive and resistant populations were used. The reason for lack of incorporation into DNA by the resistant cells was shown to be the presence of very low levels of the enzyme deoxycytidine kinase in P388-R cells resulting in an inability to phosphorylate AraC to its active form AraCTP. Immediate inhibition of DNA synthesis caused by AraC was directly proportional to the number of sensitive cells present in the population, but was not as accurate a predictor of sensitivity as the 3H-AraC index. Cloning in methylcellulose was found to be the least sensitive predictor of the percentage of sensitive and resistant cells, most likely related to the difference in cloning efficiency of the sensitive and resistant lines.
Published: 1984

48. Interactions between three subpopulations of Ehrlich ascites tumor and a P388 murine leukemia in mixed solid tumors in immune competent mice.

Author: Aabo K, Vindeløv LL, Christensen IB, and Spang-Thomsen M
Subjects: Animals, Carcinoma, Ehrlich Tumor immunology, Cell Cycle, Female, Leukemia P388 immunology, Mice, Tumor Cells, Cultured, Carcinoma, Ehrlich Tumor pathology, Cell Communication, Leukemia P388 pathology, Leukemia, Experimental pathology
Abstract: Cellular interactions between three subpopulations of Ehrlich ascites tumor and between these and the P388 murine leukemia were studied during growth of solid tumors obtained by mixtures of the cells in immune competent N/D mice. An immunogenic Ehrlich cell line (E1.15) induced an immunologically based growth inhibition of the two other Ehrlich cell lines (E1.80 and E1.95) which themselves were non-immunogenic. E1.15 was, however, unable to induce an immunological response against the P388 cell line. It is therefore suggested that when in close contact, immunologically induced cellular responses imposed by an immunogenic cell line on other cell lines require genetic and thereby close immunogenic resemblance between the cell lines. Another type of interaction was found between the E1.95 cell line and the P388 line which showed nearly identical growth characteristics as determined by tumor weight day 14, tumor growth curves, cell cycle times (per cent labelled mitoses) and cell cycle distributions (flow cytometric DNA analysis). After 2 weeks of growth of mixed P388/E1.95 tumors, flow cytometric DNA analysis on fine-needle tumor aspirates showed nearly total dominance of P388. This type of interaction required close cellular contact of viable cells, and no cellular immune response was elicited by the host animals. A third finding was that a faster growing Ehrlich cell line E1.95 dominated the tumors when inoculated in mixture with a slower growing subpopulation E1.80. This could be explained on the basis of the cell kinetic differences between these two cell lines.
Published: 1989
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49. [Antitumor activity of trewiasine in vitro and in vivo].

Author: Yang JL, Shen ZM, Lu LJ, Han JX, and Xu CH
Subjects: Animals, Leukemia P388 pathology, Maytansine analogs & derivatives, Maytansine pharmacology, Mice, Neoplasm Proteins biosynthesis, Tumor Cells, Cultured drug effects, Antineoplastic Agents, Phytogenic, Carcinoma, Ehrlich Tumor drug therapy, Leukemia P388 drug therapy, Leukemia, Experimental drug therapy, Maytansine therapeutic use, Oxazines therapeutic use
Published: 1988

50. Phagosome-lysosome fusion in P388D1 macrophages infected with Histoplasma capsulatum.

Author: Eissenberg LG, Schlesinger PH, and Goldman WE
Subjects: Acridine Orange, Animals, Dextrans, Fluoresceins, Host-Parasite Interactions, Leukemia P388 pathology, Lysosomes microbiology, Macrophages physiology, Mice, Phagosomes microbiology, Toxoplasma physiology, Cell Fusion, Fluorescein-5-isothiocyanate analogs & derivatives, Histoplasma physiology, Leukemia P388 microbiology, Leukemia, Experimental microbiology, Lysosomes physiology, Macrophages microbiology, Phagosomes physiology
Abstract: The issue of whether or not phagocytized Histoplasma capsulatum yeasts evade phagosome-lysosome fusion (P-LF) has been debated by several investigators. To resolve this problem, yet avoid drawbacks associated with the conventional assays of P-LF (electron microscopy and the acridine orange assay), we used fluorescein isothiocyanate-labeled dextran (FITC-dextran) to monitor P-LF in the macrophage-like cell line P388D1.D2. Controls indicated that FITC-dextran could be used to distinguish between evasion of P-LF by Toxoplasma gondii and phagolysosome formation following ingestion of Saccharomyces cerevisiae. Phagosomes containing H. capsulatum clearly fused with FITC-dextran-labeled lysosomes at a rate comparable to that observed for S. cerevisiae. This was true for several strains of H. capsulatum including two avirulent strains derived in this laboratory. Varying the dose of H. capsulatum did not alter the percentage of phagolysosomes formed. Our results indicate that H. capsulatum is one of a small number of organisms which is able to survive in phagolysosomes.
Published: 1988
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