Two New C3H Mouse Ascites Tumor Cell Lines Capable of Proliferation in vivo and in Suspension Culture: Morphological, Karyological, Kinetic, and Immunological Properties

Two New C3H Mouse Ascites Tumor Cell Lines Capable of Proliferation in vivo and in Suspension Culture: Morphological, Karyological, Kinetic, and Immunological Properties

The establishment of mouse tumor cell lines capable of proliferating in vivo and in suspension culture was undertaken. The MM-46 tumor line, initiated from primary mammary carcinoma arising in a C3H/He mouse, was maintained for over 100 generations in the peritoneal cavities of syngenic mice. At the...

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Veröffentlicht in:In Vitro 1980-07, Vol.16 (7), p.600-608
Hauptverfasser: Tsuboi, Atsushi, Mieko Matsui, Hayata, Isamu, Tsuchiya, Takehiko
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Antiserum
Ascites
Cancer
Cell Division
Cell growth
Cell Line
Cell lines
Cell Nucleus - ultrastructure
Chromosomes
Cultured cells
Cultured tumor cells
Cytoplasm - ultrastructure
Cytotoxicity, Immunologic
Karyotyping
Mammary Neoplasms, Experimental - etiology
Mice
Mice, Inbred C3H
Neoplasm Transplantation
Transplantation, Homologous
Tumor cell line
Tumors
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Mieko Matsui
Hayata, Isamu
Tsuchiya, Takehiko
description The establishment of mouse tumor cell lines capable of proliferating in vivo and in suspension culture was undertaken. The MM-46 tumor line, initiated from primary mammary carcinoma arising in a C3H/He mouse, was maintained for over 100 generations in the peritoneal cavities of syngenic mice. At the 50th generation of the tumor suspension, cultures were initiated. The established cell lines, designated TMT-1 and TMT-2, were characterized in vitro and in vivo. The morphological finding indicated that TMT-1 and TMT-2 cells from mice closely resembled the MM-46 tumor cells. The oncogenic potential of the cultured cells was comparable to that of the original ascites tumor. The population doubling time of TMT-1 and TMT-2 cell lines was about 12 hr in mice, whereas the population doubling time of both cell lines lengthened to 20 hr in suspension culture. The increase of doubling time in culture was due to the prolongation of the G1, period. The cell lines, TMT-1 and TMT-2, whether from culture or mice, possessed colony forming ability in soft agar medium. The colony forming ability of the cells decreased gradually through in vivo passages but it recovered upon recultivation of the cells from mouse to culture. Chromosome analysis and cytotoxicity test by anti-MM antiserum indicated that TMT-1 and TMT-2 cell lines closely resembled and had been derived from MM-46 tumor line. Therefore, it is possible to assay cell survival in vitro after in vivo experiments on these cells.
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The MM-46 tumor line, initiated from primary mammary carcinoma arising in a C3H/He mouse, was maintained for over 100 generations in the peritoneal cavities of syngenic mice. At the 50th generation of the tumor suspension, cultures were initiated. The established cell lines, designated TMT-1 and TMT-2, were characterized in vitro and in vivo. The morphological finding indicated that TMT-1 and TMT-2 cells from mice closely resembled the MM-46 tumor cells. The oncogenic potential of the cultured cells was comparable to that of the original ascites tumor. The population doubling time of TMT-1 and TMT-2 cell lines was about 12 hr in mice, whereas the population doubling time of both cell lines lengthened to 20 hr in suspension culture. The increase of doubling time in culture was due to the prolongation of the G1, period. The cell lines, TMT-1 and TMT-2, whether from culture or mice, possessed colony forming ability in soft agar medium. 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The colony forming ability of the cells decreased gradually through in vivo passages but it recovered upon recultivation of the cells from mouse to culture. Chromosome analysis and cytotoxicity test by anti-MM antiserum indicated that TMT-1 and TMT-2 cell lines closely resembled and had been derived from MM-46 tumor line. Therefore, it is possible to assay cell survival in vitro after in vivo experiments on these cells.</abstract><cop>United States</cop><pub>Tissue Culture Association, Inc</pub><pmid>7409830</pmid><doi>10.1007/BF02618385</doi><tpages>9</tpages></addata></record>
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source MEDLINE; JSTOR Archive Collection A-Z Listing; SpringerLink Journals - AutoHoldings
subjects Animals
Antiserum
Ascites
Cancer
Cell Division
Cell growth
Cell Line
Cell lines
Cell Nucleus - ultrastructure
Chromosomes
Cultured cells
Cultured tumor cells
Cytoplasm - ultrastructure
Cytotoxicity, Immunologic
Karyotyping
Mammary Neoplasms, Experimental - etiology
Mice
Mice, Inbred C3H
Neoplasm Transplantation
Transplantation, Homologous
Tumor cell line
Tumors
title Two New C3H Mouse Ascites Tumor Cell Lines Capable of Proliferation in vivo and in Suspension Culture: Morphological, Karyological, Kinetic, and Immunological Properties
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