COMBINED IMMUNOCHEMOTHERAPY OF HUMAN SOLID TUMORS IN NUDE-MICE

被引:0
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作者
WEILHILLMAN, G
UCKUN, FM
MANSKE, JM
VALLERA, DA
机构
[1] UNIV MINNESOTA, DEPT THERAPEUT RADIOL,BOX 367,MAYO MEM BLDG, 420 DELAWARE ST SE, MINNEAPOLIS, MN 55455 USA
[2] UNIV MINNESOTA, MED PATHOL LAB, MINNEAPOLIS, MN 55455 USA
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中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
In vivo immunochemotherapy of human solid tumors was studied in a nude mouse model. Large tumors (3 to 6 cm3) were induced by s.c. injection of the acute lymphoblastic leukemia T-cell line CEM. Transient tumor inhibition could be achieved by intratumoral injection of an intact-ricin immunotoxin that specifically recognizes a determinant CD5 (T,p67) expressed on the cell surface. Injection of the in vitro active cyclophosphamide congener mafosfamid had little effect on the progression of tumor growth. A combination regimen of immunotoxin and mafosfamid induced the most dramatic antitumor effect; a 72 to 100% reduction in tumor volume was observed within 3 to 4 days posttreatment. However, tumor relapsed within 5 to 13 days. Persistent, tumor regression was observed only when protocols using successive injections of combined immunotoxin/mafosfamid were used. All seven mice undergoing this treatment had a precipitous decrease in tumor size, and 86% survived greater than 30 days posttreatment. No residual tumor was detectable on Day 30 in five of seven mice. Regression was partly attributed to the selective activity of immunotoxin, since successive injections of an irrelevant control immunotoxin coupled to ricin in combination with mafosfamid did not release tumor size. Thus, we have demonstrated that a combination of anticancer chemotherapy and immunotoxin therapy yielded a greater antitumor effect than either therapy alone.
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页码:579 / 585
页数:7
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