Summary
Autochthonous neurogenic tumors of the rat induced by transplacental application of ethylnitrosourea were used for the first time to study their suitability as tumor models for experimental chemotherapy. Of 189 transplacentally treated rats, 87% developed neurogenic tumors. After the initial clinical diagnosis of a neurogenic tumor, additional malignant tumors often occurred. The mean number of neurogenic tumors from 62 untreated control rats increased from 1.0 per rat at the time of randomization to 1.2 as revealed by autopsy and 1.5 tumors by histological examinations. Out of all neurogenic tumors, tumors of the brain were observed in 31%, tumors of cranial nerves in 36% (90% tumors of trigeminal nerve), tumors of spinal cord in 21%, and tumors of peripheral nerves in 10%. The median survival time until natural death of 62 control rats was 228 days. Rats with tumors of peripheral nerves lived shortest, followed by rats with tumors of cranial nerves, tumors of the spinal cord, and brain tumors. Brain tumors were mainly astrocytomas and oligodendrogliomas. The survival time of untreated rats from randomization to natural death was longest for those with brain tumors, followed by tumors of peripheral nerves, cranial nerves, and tumors of the spinal cord. There was great variation in survival time from a few days to more than 6 months. To study the responsiveness to chemotherapy, 62 rats received BCNU as a single intravenous dose of 9 and later 10 mg/kg. Sixty-two untreated control rats had a median survival time of 36 days (95% confidence interval 26–52 days), the treated rats 43.5 days (26–62 days) The difference was not statistically significant. BCNU produced a remission or a no change of neurologic symptoms in 60% (37 out of 62) in comparison to 39% (24 out of 62) in the control group (p<0.05). The advantages and disadvantages of the present models are discussed. Due to methodical problems and the marginal response to BCNU, autochthonous neurogenic tumors of the rat are not suitable as models for chemotherapeutic studies.
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References
Bürkle G (1975) Autochthone Tiertumoren als Testmodelle für die Chemotherapie mit Bleomycin. In: Wilmanns W (ed) Bleomycin. Experimentelle Grundlagen und erste klinische Ergebnisse. Ahnen KG, Laupheim
Druckrey H, Schagen B, Ivankovic S (1970) Erzeugung neurogener Malignome durch einmalige Gabe von ÄNH an neugeborene und junge BD-IX-Ratten. Z Krebsforsch 74:141–161
Fiebig HH, Schmähl D (1977a) Synergismus von Adriamycin mit 5-Fluorouracil, mit Prednisolon und mit Cyclophosphamid am autochthonen Mammakarzinom der Ratte. Klin Wochenschr 55:445–450
Fiebig HH, Schmähl, D (1977b) The effect of ovariectomy, Tamoxifen and the combination Adriamycin and 5-FU on 7,12Dimethylbenz(a)-anthracene induced mammary cancer of the rat. Oncology 34:58–61
Fiebig HH, Schmähl D (1978) Das experimentelle Mammakarzinom als Modell für chemotherapeutische Studien. In: Schmähl D (Hrsg) Behandlung und Nachbehandlung des Mammakarzinoms. Thieme, S 36–56)
Fiebig HH, Schmähl D (1980) Endocrine and cytostatic treatment of experimental mammary cancer. Recent Results Cancer Res 71:80–95
Fiebig, HH, Zeller WJ, Schmähl D (1976) An experimental model for meningeal leukemia in rats (L 5222). Effect of treatment with BCNU and cyclophosphamid. Int J Cancer 18:710–716
Fiebig HH, Eisenbrand G, Zeller WJ, Zentraf R (1980) Anticancer activity of new nitrosoureas against Walker carcinosarcoma 256 und DMBA induced mammary cancer of the rat. Oncology 37:177–183
Frei E, Schabel FM Jr, Goldin A (1974) Comparative chemotherapy of AKR lymphoma and human hematological neoplasia. Cancer Res 34:184–193
Fretz J, Rohde W, Schmähl D, Thomas C (1969) Therapieversuche am autochthonen Mammakarzino der Ratte. Arzneimittel-Forsch 19:1291–1295
Gabriel KR (1966) Simultaneous test procedures for multiple comparisons on categorical data. J Am Stat Assoc 61:1081–1096
Goldin, A, Sandberg JS, Henderson ES, Newmann JW, Frei E, Holland JF (1971) The Chemotherapy of human and animal acute leukemia. Cancer Chemother Rep 55:309–507
Habs M (1981) Methoden, Ergebnisse und Probleme der experimentellen Chemotherapie. In: Schmähl D (Hrsg) Maligne Tumoren — Entstehung. Wachstum und Chemotherapie. Editio Cantor, Aulendorf, S 455–498
Habs M, Ang J, Schmähl (1977a) Chemotherapy studies in autochthonous rat tumours, forestomach and bladder cancer. Z Krebsforsch 89:119–136
Habs M, Habs G, Schmähl D (1977b) Chemotherapy studies in autochthonous rat tumors, hepatomas. Z Krebsforsch 90:167–173
Ivankovic S (1968) Erzeugung maligner Tumoren im Gehirn, Rückenmark und Nervensystem bei den Nachkommen von Ratten und Hamstern durch transplazentare Einwirkung von Äthyl-Nitroso-Harnstoff. Habilitationsschrift, Universität Freiburg i. Br.
Ivankovic S, Druckrey H (1968) Transplazentare Erzeugung maligner Tumoren des Nervensystems an BD IX-Ratten. I. Äthylnitrosoharnstoff. Z Krebsforsch 71:320–360
Killmann SA (1979) Review on proliferative kinetics in human acute leukemias with special reference to the relevance of both rat leukemia models. Leukemia Res 1:107–111
Levin VA, Wilson CB (1975) Chemotherapy: The agents in current use. Semin Oncol 2:63–67
Schabel FM Jr (1976) Nitrosoureas: A review of experimental antitumor activity. Cancer Treatment Rep 60:665–698
Schmähl D, Mundt D, Schmidt KG (1974) Experimental investigations on the influence upon the chemical carcinogenesis. First Communication: Studies with Ethylnitrosourea. Z Krebsforsch 82:91–100
Schmähl D, Schrick G, König K (1963) Chemotherapieversuche an Hepatomen. Arzneim-Forsch 13:370–371
Schmähl D, Osswald H, Brune H (1968) Einfluß von Dosis und Tumorgröße für das Ansprechen autochthoner Benzpyren-Sarkomen bei Ratten und Mäusen auf chemotherapeutische Behandlung mit Endoxan. Z Krebsforsch 70:246–251
Schmähl D, Osswald H, Brune H (1966) Chemotherapieversuche mit Endoxan an autochthonen Benzpyren-Sarkomen bei Ratten und Mäusen. Z Krebsforsch 68:293–302
Schmähl D (1970) Autochthone Tiertumoren als Testmodelle für Krebs-Chemotherapeutika. Arch Pharmazie 303:173–174
Schmähl D (1966) Die heutige Situation in der experimentellen Chemotherapie von Tumoren. Dtsch Med Wochenschr 91:2132–2135
Schmähl D (1981) Maligne Tumoren — Entstehung, Wachstum und Chemotherapie. Editio Cantor, Aulendorf
Schmähl D (1976) Utilization of Nitrosamine-induced tumors as models for cancer chemotherapy. Chemother 7:233–238
Schneidermann MA (1978) Eighty percent of cancer is related to the environment. Laryngoscope 88:559–574
Steel GG (1977) Growth kinetics of tumors. Clarendon Press, Oxford
Strobel H (1980) Autochthone, chemisch induzierte, neurogene Tumoren der Ratte als Modelle für chemotherapeutische Studien. Dissertation, Universität Heidelberg
Sych F, Habs M, Schmähl D (1978) Chemotherapy studies in autochthonous rat tumors: intestinal cancer. Z Krebsforsch 92:105–117
Wechsler W, Kleihues P, Matsumoto S, Zülch KJ, Ivankovic S, Preussmann R, Druckrey H (1969) Pathology of experimental neurogenic tumors chemically induced during prenatal and postnatal life. Ann NY Acad Sciences 159:360–408
Zeller WJ, Berger M, Schmähl D (1980) Chemotherapy of autochthonous leukemias induced by 7,12-Dimethylbenz(a)anthracene in Long Evans rats. J Cancer Res Clin Oncol 96:157–162
Zeller WJ, Ivankovic S, Zeller J (1978) Induction of malignant tumors in Wistar and Sprague-Dawley rats by single dose of n-butylnitrosourea in prenatal and juvenile phases of development. Arch Geschwulstforsch 48:9–16
Zeller WJ, Schmähl D (1979) Leukemias induced by ethylnitrosourea in Wistar rats: Incidence and chemotherapy. Leukemia 3:239–248
Zeller WJ (1981) Das Krebswachstum — Experimentelle und klinische Beobachtungen In: Schmähl D (Hrsg) Maligne Tumoren, Entstehung, Wachstum und Chemotherapie. Editio Cantor, Aulendorf, S 324–363
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Fiebig, H.H., Strobel, H. & Schmähl, D. Experimental chemotherapy with N′N′-bis(2-chloroethyl)-N-nitrosourea (BCNU) in autochthonous neurogenic tumors of the rat transplacentally induced by ethylnitrosourea. J Cancer Res Clin Oncol 104, 89–98 (1982). https://doi.org/10.1007/BF00402057
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DOI: https://doi.org/10.1007/BF00402057