RSS-Feed abonnieren
DOI: 10.1055/s-2002-33175
Topotecan in the treatment of refractory neuroblastoma and other malignant tumors in childhood - a phase-II-study
Topotecan in der Therapie refraktärer Neuroblastome und anderer maligner Erkankungen im Kindesalter - eine Phase-II-StudiePublikationsverlauf
Publikationsdatum:
07. August 2002 (online)
Abstract
Background: The topoisomerase-I-inhibitor Topotecan (TPT) has shown a broad activity in the therapy of adult malignant diseases. In pediatric oncology TPT has been rarely used. Methods: From 1/98 to 8/99 we conducted a multicenter phase-II-study of TPT (1.5 mg/m2/d in 30 min i. v. for 5 days every 21 days) in pediatric patients (pts) with malignant tumors refractory to conventional therapy (either second line or any relapse). Patients: A total of 20 pts received 81 cycles. The 7 female and 13 male pts had a median age of 10.2 years at the beginning of the TPT therapy. Results: The median number of administered TPT cycles was 4 with an interval of 23.5 days. The median administered TPT dose was 1.48 mg/m2/d . No complete responses, but 2 partial responses and 9 stable diseases were observed. In 9 pts the disease progressed. The mean duration until progression for SD was 130 and not different from PR with 131 days. The median cumulative TPT dose until progression in responders was 30 mg/m2. For all study-pts the median overall survival time was 235 days with 1 pt. still alive. The main toxicity was hematological with anemia grade III/IV (10/42 % of all evaluable TPT cycles), neutropenia grade III/IV (49/18 %) and thrombopenia grade III/IV (35/36 %). Non-hematologic toxicity was mild with the exception of 4 cycles with infection grade III and 1 grade IV. No patient died of therapy-related complications. Conclusions: TPT as monotherapy has shown an antitumor activity in pediatric pts with various malignancies. Toxicity was mainly hematological and manageable. Further evaluation of TPT treatment is planned using combinations with other cytostatic drugs.
Zusammenfassung
Hintergrund: Der Topoisomerase-I-Hemmer Topotecan (TPT) zeigte in der Therapie von malignen Tumoren im Erwachsenenalter eine breite klinische Wirksamkeit. In der pädiatrischen Onkologie gab es hierzu bislang wenig Erfahrung. Methode: Von 1/98 bis 8/99 führten wir eine multizentrische Phase-II-Studie mit TPT (1,5 mg/m2/d 30 min i. v. an 5 Tagen; alle 21 Tage) bei pädiatrischen Patienten mit therapierefraktären oder rezidivierten malignen Tumoren durch. Patienten: 20 Patienten erhielten insgesamt 81 Therapiezyklen. Die 7 weiblichen und 13 männlichen Patienten hatten ein medianes Alter von 10,2 Jahren bei Therapiebeginn. Ergebnisse: Die mediane Anzahl der TPT-Zyklen war 4 in einem medianen Intervall von 23,5 Tagen. Die applizierte mediane TPT-Dosis war 1,48 mg/m2/d. Keine komplette Remission, jedoch 2 partielle Remissionen und 9 stabile Erkrankungen wurden beobachtet. Bei 9 Patienten war die Erkrankung primär progredient. Die mediane Dauer bis zur erneuten Progression war bei den Patienten mit stabiler Erkrankung (130 Tage) die gleiche wie bei Patienten mit partieller Remission (131 Tage). Die kumulative TPT-Dosis bis zur Progression betrug 30 mg/m2. Die mediane Überlebenszeit für alle Patienten betrug 235 Tage, wobei ein Patient noch lebt. Die wesentliche Toxizität war hämatologisch: Anämie III/IV ° (10/42 % aller auswertbarer Zyklen), Neutropenie III/IV ° (49/18 %), Thrombopenie III/IV ° (35/36 %). Die nicht-hämatologische Toxizität war gering, bis auf Infektion III/IV in 4 bzw. 1 Zyklus. Kein Patient verstarb an therapie-assoziierten Komplikationen. Schlussfolgerung: TPT als Monotherapie zeigt eine antitumoröse Aktivität bei pädiatrisch-onkologischen Patienten. Die Toxizität war i.w. hämatologisch und beherrschbar. Weitere Studien z. B. in Kombinationstherapien sind erforderlich.
Key words
Topotecan - Neuroblastoma - Childhood tumors - Phase II study
Schlüsselwörter
Topotecan - Neuroblastom - kindliche Tumoren - Phase-II-Studie
Literatur
- 1 Lock R B, Ross W E. Topoisomerases in cancer therapy. Anticancer Drug Design. 1987; 2 151-164
- 2 Pommier Y. Eukaryotic DNA topoisomerase I: genome gatekeeper and it's intruders. Semin Oncol. 1996; 23 (3) 3-10
- 3 Wall M E, Wani M C, Cook C E, Palmer K H, McPhail A T, Sim G A. Plant antitumor agents. J Am Chemotherapy Soc. 1996; 88 3888-3890
- 4 Burris H A, Hanauske A R, Johnson R K, Marshall M H, Kuhn J G. Activity of topotecan, a new topoisomerase I inhibitor against tumor colony forming units in vitro. J Natl Cancer Inst. 1992; 23 1816-1819
- 5 Friedman H S, Houghton P J, Schold S C, Keir S, Bigner D D. Activity of 9-dimethylaminomethyl-10-hydroxycampthotecin against pediatric and adult central nervous system tumor xenografts. Cancer Chemother Pharmacol. 1994; 34 171-174
- 6 Friedman H S, Houghton P J, Schold S C, Bigner D D. Activity of 9-dimethylaminoethl-10-hydroxycamptothecin against CNS xenografts. Proc Annu Meet Am Assoc Cancer Res (Abstract). 1993; 34 A2520
- 7 Houghton P J, Ceshire P J, Hallman J C, Bissery M C, Mathieur-Boue, Haughton J A. Therapeutic efficacy of the topoisomerase-I-inhibitor-camptothecin against human tumor xenografts. Cancer Res. 1993; 53 2823-2829
- 8 Thompson J, Stewart C, Zamboni W, Houghton P J. Systemic exposure to topotecan related to antitumor response in human neuroblastoma xenografts. Proc Am Ass Cancer Res. 1997; 38 305
- 9 Zamboni W C, Stewart C F, Thompson J, Santana V M, Cheshire P J, Richmond L B, Luo X, Poquette C, Houghton J A, Houghton P J. Relationship between topotecan systemic exposure and tumor response in human neuroblastoma xenografts. J Natl Cancer Inst. 1998; 90 505-511
- 10 Tubergen D G, Stewart C F, Pratt C B, Zamboni W C, Winick N, Santana V M, Dryer Z A, Kurtzberg J, Bell B, Grier H, Vietti T J. Phase I Trial and Pharmacokinetic and Pharmacodynamics Study of Topotecan Using a Five-Day Course in Children with Refractory Solid Tumors: A Pediatric Oncology Group Study. J Pediatr Hematol Oncol. 1996; 18 352-361
- 11 Blaney S M, Phillips P C, Packer R J, Heideman R L, Berg S L, Adamson P C, Allen J C, Sallan S E, Jakacki R I, Lange B J, Reaman G H, Horowitz M E, Poplack D G, Balis F M. Evaluation of Topotecan for Pediatric Central Nervous System Tumors. Cancer. 1996; 78 527-531
- 12 Blaney S M, Needle M N, Gillespie A, Sato J K, Reaman G H, Berg S L, Adamson P C, Krailo M D, Bleyer W A, Poplack D G, Balis F M. Phase II trial of topotecan administered as 72 h-infusion in children with refractory solid tumors. Clin Cancer Res. 1998; 4 357-360
- 13 Broom C. Clinical studies of Topotecan. Ann N Y Acad Sci. 1996; 803 264-271
- 14 Furman W L, Baker S D, Pratt C B, Rivera G K, Evans W E, Stewart C F. Escalating systemic exposure of continuous infusion topotecan in children with recurrent acute leukemia. J Clin Oncol. 1996; 14 1504-1511
- 15 Nitschke R, Parkhurst J, Sullivan J, Harris M B, Bernstein M, Bratt C. Topotecan in pediatric patients with recurrent and progressive tumors. J Pediatr Hematol Oncol. 1998; 20 315-318
-
16 Santana V, Zamboni W, Gajjar A, Pappo A, Houghton P, Meyer W, Stewart C.
Pharmacokinetically-guided use of topotecan given (daily*5)*2 in children with relapsed solid tumors. ASCO-meeting 1997: 1839 - 17 The National Cancer Institute .Investigators handbook, a manual for participants in clinical trials of investigational agents sponsored by the Division of Cancer Tratement. The National Cancer Insitute 1986
- 18 Saylors R L, Stine K C. Cyclophosphamide plus topotecan in children with recurrent or refractory solid timors: a pediatric oncology group phase II study. J Pediatr Hematol Oncol (Abstract). 1999; 21 465
- 19 Buchholz E, Manegold C, Drings P, Mayer U, Heuser A. Sequential administration of topotecan and etoposide in extensive small cell lung cancer - a phase-I-study. Proc ASCO (Abstract). 1998; 17 1843
Dr. med. Alfred Längler
Gemeinschaftskrankenhaus, Department of Pediatrics
Gerhard-Kienle-Weg 4
58313 Herdecke
Telefon: + 49-2330-623893
Fax: + 49-2330-624103
eMail: a.laengler@gemeinschaftskrankenhaus.de