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  • Title: Further observations on the effect of cyclophosphamide on intratumor and peripheral leukocyte levels.
    Author: Evans R.
    Journal: Am J Pathol; 1980 Jun; 99(3):667-84. PubMed ID: 7386598.
    Abstract:
    The injection of cyclophosphamide (CY) into C57BL/6J mice bearing intramuscularly transplanted, MCA-induced tumors (MCA/76-9, 76-64, 76-45, and 77-23) resulted in reproducible sequence of events involving tumor regression that was followed by recurrence in all but a few cases. Regression itself occurred whether tumors were immunogenic or not and whether tumors were growing in immunocompetent of immunosuppressed mice. Permanent CY-induced regressions, however, were rare under any conditions. The drug induced well-defined changes in the number of bone marrow and blood leukocytes. By 8 days after drug injecion, control or tumor-bearing mice showed normal bone marrow counts but elevated peripheral blood leukocyte counts. The latter involved only monocytes and granulocytes, lymphocytes requiring more than 21 days on return to control values. Tumor bearers not injected with CY also showed elevated blood monocyte and granulocyte numbers. After CY injection of mice, tumors showed distinctive histologic changes that were common for all four sarcomas. Within 3 days of injection, neoplastic cells showed evidence of damage, and mononuclear cells became prominent thoughout the tumor mass. By 7 days, there were many giant cells and polykaryons, which progressively decreased, so that by Days 10-14 few were discernible. At this time, the bulk of the tumor mass consisted of mononuclear cells having the morphologic characteristics of macrophages. However, between days 7 and 10 well-defined hyperchromatic areas could be seen peripherally in the capsule or the muscle into which the tumor cells were originally implanted. These areas consisted of relatively undifferentiated cell types, with which cells of the granulocyte series were often associated. By Day 14 these regions were packed with granulocytes. Regression usually stopped between Days 14 and 21, at which time the residual tumor mass consisted of birefringent, fibrous tissue containing relatively few cellular elements. Between 21 and 28 days, tumor recurrence was evident in most cases. The histologic changes were quantified by disaggregating the tumors with enzymes before and after CY injection. A good correlation was obtained between histologic appearance and the numbers and types of cells obtained at defined times. Both tumor-associated macrophage and granulocyte counts showed an increase over the first 10 days after CY injection. Frequently, both cell types declined numerically over the first 3 days in parallel with blood monocyte and granulocyte counts and with bone marrow cell counts. The decline depended to large extent on the total number of cells associated with the tumor mass and the overall effect exerted by CY on these cells. Intratumor macrophage numbers reached a peak by Day 8, whereas granulocytes did not reach maximum values until Day 10. Subsequently, both cell types decreased in number until recurrent tumor growth became apparent. These findings are discussed in terms of the possible relationship between peripheral and tumor-associated leukocytes and in terms of the functions of the latter during CY-induced tumor regression.
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