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Klin Padiatr 2000; 212(4): 177-184
DOI: 10.1055/s-2000-9674
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Georg Thieme Verlag Stuttgart ·New York

HIT-LGG: Effektivität von Carboplatin-Vincristin bei progredienten Gliomen niedrigen Malignitätsgrades im Kindesalter - Zwischenbericht

HIT-LGG: Therapy protocol for the treatment of children with low-grade glioma - Interim report. A.  K.  Gnekow1 , P.  Kaatsch2 , R.  Kortmann3 , O.  D.  Wiestler4
  • 1Klinik für Kinder und Jugendliche, KZV Augsburg
  • 2Institut für medizinische Statistik und Dokumentation (IMSD), Mainz
  • 3Universitätsstrahlenklinik, Tübingen
  • 4Institut für Neuropathologie und Hirntumorreferenzzentrum, Universität Bonn
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Publication History

Publication Date:
31 December 2000 (online)

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Zusammenfassung.

Hintergrund: Die Therapiestrategie des HIT-LGG-Protokolls prüft, ob für Kinder mit progredienten Gliomen niedrigen Malignitätsgrades im Alter unter 5 Jahren und bei älteren Kindern nach individueller Entscheidung eine Chemotherapie den Beginn einer Standardstrahlentherapie hinauszögern kann.

Patienten und Methoden: Bis 10. 10. 1999 wurden 402 Patienten aus 69 Kliniken gemeldet. 130 Kinder mit progredienten Tumoren wurden nach einer medianen Beobachtungszeit von 5 Monaten behandelt: 46 mit primärer Radiotherapie und 84 mit primärer Chemotherapie. Auf eine 10-wöchige Induktionsphase mit wöchentlichen Vincristingaben und Carboplatinpulsen zu Woche 1, 4, 7 und 10 folgt eine Konsolidierung mit simultaner Medikamentengabe im 4-Wochen-Rhythmus bis Woche 53.

Ergebnisse: Von den 84 Patienten im Chemotherapiearm (49 Jungen, 35 Mädchen, 23 mit NF I, medianes Alter 2,99 Jahre) wurden 36 bei Diagnosestellung und 43 nach einer Beobachtungszeit von median 19,7 Monaten behandelt (5 unbekannt). Klinisch und neuroradiologisch erreichten 94,3 % eine Response nach Protokollkriterien (5 CR, 30 PR/OR, 31 SD), welche im Median nach 5,1 Monaten eintrat. 4 Tumoren waren primär progredient (9 zu früh, 5 unbekannt). Nur 6/84 Kinder wurden bislang bei Progredienz während (2) oder nach (4) Chemotherapie, median nach 25, 6 Monaten, im medianen Alter von 6,0 Jahren bestrahlt. Bei einer medianen Nachbeobachtungszeit von 21,0 Monaten sind 6 Kinder in CR, 11 in PR, 48 in SD, 4 Tumoren sind progredient, 3 Kinder sind verstorben (9 zu früh, 3 unbekannt). Das PFS liegt bei 72 % nach 36 Monaten. 24/27 Kindern mit allergischen Reaktionen auf Carboplatin mussten die Therapie jedoch vorzeitig abbrechen.

Schlussfolgerung: Die Kombination von Carboplatin und Vincristin kann bei Kindern mit progredienten Gliomen niedrigen Malignitätsgrades den Beginn der Strahlentherapie wirkungsvoll hinauszögern. Die hohe Rate an Hypersensitivitätsreaktionen bedarf jedoch zukünftiger Therapiemodifikationen.

Background:The rationale of the HIT-LGG protocol is to delay standard radiotherapy through administration of chemotherapy for children with progressive low grade glioma at an age under 5 years and in older children upon individual decision.

Patients and Method: Until October 10th., 1999, 402 patients from 69 hospitals were registered. 130 children with progressive tumors were treated after a median observation time of 5 months: 46 patients received primary radiotherapy and 84 primary chemotherapy. A ten week induction period with weekly Vincristine and pulses of Carboplatin at weeks 1, 4, 7 and 10 is followed by consolidation with simultaneous application of both drugs every 4 weeks until week 53.

Results: Of 84 patients in the chemotherapy arm of the study (49 male, 35 female, 23 NF I, median age 2.99 years) 36 received treatment at diagnosis and 43 after a median observation time of 19.7 months. 94,3 % achieved a clinical and neuroradiological response according to protocol criteria (5 CR, 30 PR/OR, 31 SD) after a median of 5.1 months. 4 tumors showed primary progression (9 too early, 5 not known). Only 6 of 84 children received radiation therapy for progressive disease during (2) or after termination (4) of chemotherapy, after a median delay of 25.6 months at a median age of 6.0 years. At a median observation time of 21.0 months, 6 children are in CR, 11 in PR, 48 have SD, 4 tumors are progressive and 3 children died of their tumor. (9 too early, 3 not known). PFS is at 72 % after 36 months. 24 of 27 children experiencing allergic reactions to Carboplatin had to interrupt chemotherapy prematurely.

Conclusions: Combination therapy with Carboplatin and Vincristine can effectively delay the start of radiotherapy in children with progressive low-grade glioma. The high rate of hypersensitivity reactions has to prompt future modifications of treatment.

Schlüsselwörter:

Niedrig-maligne Gliome - Chemotherapie - Radiotherapie - Carboplatin - Vincristin

Key words:

low-grade glioma - chemotherapy - radiotherapy - Carboplatin - Vincristin

Literatur

  • 01 Aquino  V M, Fort  D W, Kamen  B A. Carboplatin for the treatment of children with newly diagnosed optic chiasm gliomas: a phase II study.  J Neuro-Oncology. 1999;;  41 255-259
    Google Scholar
  • 02 Brown  M T, Friedman  H S, Oakes  W J, Boyko  O B, Hockenberger  B, Schold  S C Jr. Chemotherapy for pilocytic astrocytoma.  Cancer. 1993;;  71 3165-3172
    Google Scholar
  • 03 Campbell  J W, Pollack  I F. Cerebellar astrocytomas in children.  J Neuro-Oncology. 1996;;  28 223-231
    Google Scholar
  • 04 Castello  M A, Schiavetti  A, Varrasso  G, Clerico  A, Capelli  C. Chemotherapy in low-grade astrocytoma management.  CNS. 1998;;  14 6-9
    Google Scholar
  • 05 Chamberlain  M C, Grafe  M R. Recurrent chiasmatic-hypothalamic glioma treated with oral etoposide.  J Clin Oncol. 1995;;  13 2072-2076
    Google Scholar
  • 06 Chang  S M, Fryberger  S, Crouse  V, Tilford  D, Prados  M D. Carboplatin hypersensitivity in children.  Cancer. 1995;;  75 1171-1175
    Google Scholar
  • 07 Fort  D W, Packer  R J, Kirkpatrick  G B, Kuttesch  J F Jr, Ater  J L. Carboplatin and vincristine for pediatric primary spinal cord astrocytomas.  CNS. 1998;;  14 484
    Google Scholar
  • 08 Flickinger  J C, Torres  C, Deutsch  M. Management of low-grade gliomas of the optic nerve and chiasm.  Cancer. 1988;;  61 635-642
    Google Scholar
  • 09 Friedman  J M, Birch  P. An association between optic glioma and other tumors of the central nervous system in neurofibromatosis type I.  Neuropediatrics. 1997;;  28 131-132
    Google Scholar
  • 10 Friedman  H S, Krischer  J P, Burger  P, Oakes  W J, Hockenberger  B, Weiner  M D, Falletta  J M, Norris  D, Ragab  A H, Mahoney  D H, Whitehead  M V, Kun  L E. Treatment of children with progressive or recurrent brain tumors with carboplatin or iproplatin: A pediatric oncology group randomized phase II study.  J Clin Oncol. 1992;;  10 249-256
    PubMedGoogle Scholar
  • 11 Gajjar  A, Sanford  R A, Heideman  R, Jenkins  J J, Walter  A, Li  Y, Langston  J W, Muhlbauer  M, Boyett  J M, Kun  L E. Low-grade astrocytoma: A decade of experience at St. Jude Children's Research Hospital.  J Clin Oncol. 1997;;  15 2792-2799
    PubMedGoogle Scholar
  • 12 Gajjar  A, Heideman  R L, Kovnar  E H, Langston  J A, Sanford  R A, Douglass  E C, Jenkins  J J, Horowitz  M E, Kun  L E. Response of pediatric low grade gliomas to chemotherapy.  Pediatr Neurosurg. 1993;;  19 113-118
    PubMedGoogle Scholar
  • 13 Garvey  M, Packer  R J. An integrated approach to the treatment of chiasmatic-hypothalamic gliomas.  J Neuro-Oncology. 1996;;  28 167-183
    PubMedGoogle Scholar
  • 14 Ghim  T. Efficacy of combination chemotherapy in children with recurrent low grade astrocytoma.  Proc Annu Meet Am Soc Clin Oncol. 1993;;  12 A1444
    PubMedGoogle Scholar
  • 15 Glauser  T A, Packer  R J. Cognitive deficits in long term survivors of childhood brain tumors.  CNS. 1991;;  7 2-12
    PubMedGoogle Scholar
  • 16 Griffin  T W, Beaufait  D, Blasko  J C. Cystic cerebellar astrocytomas in childhood.  Cancer. 1979;;  44 276-280
    PubMedGoogle Scholar
  • 17 Hirsch  J F, Rose  C S, Pierre-Kahn  A, Pfister  A, Hoppe-Hirsch  E. Benign astrocytic and oligodendrocytic tumors of the cerebral hemispheres in children.  J Neurosurg. 1989;;  70 568-572
    PubMedGoogle Scholar
  • 18 Hoffman  H J, Soloniuk  D S, Humphreys  R P, Drake  J M, Becker  L E, de Lima  B O, Piatt  J H Jr. Management and outcome of low-grade astrocytomas of the midline in children: A retrospective review.  Neurosurgery. 1993;;  33 964-971
    PubMedGoogle Scholar
  • 19 Janss  A J, Grundy  R, Cnaan  A, Savina  P J, Packer  R J, Zackai  E H, Goldwein  J W, Sutton  L N, Radcliffe  J, Molloy  P T, Phillips  P C, Lange  B J. Optic pathway and hypothalamic/chiasmatic gliomas in children younger than age 5 years with a 6-year follow-up.  Cancer. 1995;;  75 1051-1059
    PubMedGoogle Scholar
  • 20 Kadota  R P, Kun  L E, Langston  J W, Burger  P C, Cohen  M E, Mahoney  D H, Walter  A W, Rodman  J H, Parent  A, Buckley  E, Kepner  J L, Friedman  H S. Cyclophosphamide for the treatment of progressive low-grade-astrocytoma: A pediatric oncology group phase II study.  J Pediatr Hematology/Oncology. 1999;;  21 198-202
    PubMedGoogle Scholar
  • 21 Kato  T, Sawamura  Y, Tada  M, Ikeda  J, Ishii  N, Abc  H. Cisplatin/vincristine chemotherapy for hypothalamic/visual pathway astrocytomas in young children.  J Neuro-Oncology. 1998;;  37 263-270
    PubMedGoogle Scholar
  • 22 Kaplan  E L, Meier  P. Nonparametric estimation from incomplete observations.  J Am Stat Assoc. 1958;;  53 457-481
    CrossrefPubMedGoogle Scholar
  • 23 Kernan  J C, Horgan  M A, Piatt  J H, D'Agostino  A. Spontaneous involution of a diencephalic astrocytoma.  Pediatr Neurosurg. 1998;;  29 149-153
    CrossrefPubMedGoogle Scholar
  • 24 Kleihues  P, Burger  P C, Scheithauer  B W. Histological typing of tumors of the central nervous system, 2. Aufl. Springer, Berlin; 1993:
    Google Scholar
  • 25 Listernik  R, Charrow  J, Greenwald  M, Mets  M. Natural history of optic pathway tumors in children with neurofibromatosis type 1: A longitudinal study.  J Pediatr. 1994;;  125 63-66
    CrossrefPubMedGoogle Scholar
  • 26 Moghrabi  A, Friedman  H S, Burger  P C, Tien  R, Oakes  W J. Carboplatin treatment of progressive optic pathway gliomas to delay radiotherapy.  J Neurosurg. 1993;;  79 223-227
    PubMedGoogle Scholar
  • 27 Packer  R J, Ater  J, Allen  J, Phillips  P, Geyer  R, Nicholson  H S, Jakacki  R, Kurczynski  E, Needle  M, Finlay  J, Reaman  G, Boyett  J M. Carboplatin and vincristine chemotherapy for children with newly diagnosed progressive low-grade gliomas.  J Neurosurg. 1997;;  86 747-754
    PubMedGoogle Scholar
  • 28 Packer  R J, Lange  B, Ater  J, Nicholson  H S, Allen  J, Walker  R, Prados  M, Jakacki  R, Reaman  G R, Needles  M N, Phillips  P C, Ryan  J, Boyett  J M, Geyer  R, Finlay  J. Carboplatin and Vincristine for recurrent and newly diagnosed low-grade Gliomas of childhood.  J Clin Oncol. 1993;;  11 850-856
    PubMedGoogle Scholar
  • 29 Packer  R J, Sutton  L N, Bilaniuk  L T, Radcliffe  J, Rosenstock  J G, Siegel  K R, Bunin  G R, Savino  P J, Bruce  D A, Schut  L. Treatment of Chiasmatic/hypothalamic gliomas of childhood with chemotherapy: An update.  Ann Neurol. 1988;;  23 79-85
    CrossrefPubMedGoogle Scholar
  • 30 Pencalet  P, Maixner  W, Sainte-Rose  C, Lellouch-Tubiana  A, Cinalli  G, Zerah  M, Pierre-Kahn  A, Hoppe-Hirsch  E, Bourgeois  M, Renier  D. Benign cerebellar astrocytomas in children.  J Neurosurg. 1999;;  90 265-273
    PubMedGoogle Scholar
  • 31 Perilongo  G, Moras  P, Carollo  C, Battistella  A, Clementi  M, Laverda  A M, Murgia  A. Spontaneous partial regression of low-grade glioma in children with neurofibromatosis-1: A real possibility.  J Child Neurol. 1999;;  14 352-356
    PubMedGoogle Scholar
  • 32 Pierce  S M, Barnes  P D, Loeffler  J S, McGinn  C, Tarbell  N J. Definitive radiation therapy in the management of symptomatic patients with optic glioma.  Cancer. 1990;;  65 45-52
    CrossrefPubMedGoogle Scholar
  • 33 Pollack  I F, Claassen  D, Al-Shboul  Q, Janosky  J E, Deutsch  M. Low-grade gliomas of the cerebral hemispheres in children: an analysis of 71 cases.  J Neurosurg. 1995;;  82 536-547
    CrossrefPubMedGoogle Scholar
  • 34 Pons  M de los A, Finlay  J L, Walker  R W, Puccetti  D, Packer  R J, McElwain  M. Chemotherapy with vincristine (VCR) and etoposide (VP-16) in children with low-grade astrocytoma.  J Neuro-Oncology. 1992;;  14 151-158
    PubMedGoogle Scholar
  • 35 Poussaint  T Y, Barnes  P D, Nichols  K, Anthony  D C, Cohen  L, Tarbell  N J, Goumnerova  L. Diencephalic syndrome: clinical features and imaging findings.  Am J Neuroradiol. 1997;;  18 1499-1505
    PubMedGoogle Scholar
  • 36 Prados  M D, Edwards  M SB, Rabbitt  J, Lamborn  K, Davis  R L, Levin  V A. Treatment of pediatric low-grade gliomas with a nitrosourea-based multiagent chemotherapy regimen.  J Neuro-Oncology. 1997;;  32 235-241
    PubMedGoogle Scholar
  • 37 Smoots  D W, Geyer  J R, Lieberman  D M, Berger  M S. Predicting disease progression in childhood cerebellar astrocytoma.  CNS. 1998;;  14 636-648
    PubMedGoogle Scholar
  • 38 Souweidane  M M, Hoffman  H J. Current treatment of thalamic gliomas in children.  J Neuro-Oncology. 1996;;  28 157-166
    PubMedGoogle Scholar
  • 39 Sutton  L N, Molloy  P T, Sernyak  H, Goldwein  J, Phillips  P L, Rorke  L B, Moshang  T Jr, Lange  B, Packer  R J. Long-term outcome of hypothalamic/chiasmatic astrocytomas in children treated with conservative surgery.  J Neurosurg. 1995;;  83 583-589
    PubMedGoogle Scholar
  • 40 Tarbell  N J, Loeffler  J S. Recent trends in the radiotherapy of pediatric gliomas.  J Neuro-Oncology. 1996;;  28 233-244
    PubMedGoogle Scholar
  • 41 Wallner  K E, Gonzales  M F, Edwards  M SB, Wara  W M, Sheline  G E. Treatment results of juvenile pilocytic astrocytoma.  J Neurosurg. 1988;;  69 171-176
    PubMedGoogle Scholar
  • 42 West  C GH, Gattamaneni  R, Blair  V. Radiotherapy in the treatment of low-grade astrocytomas. I. A survival analysis.  CNS. 1995;;  11 438-442
    PubMedGoogle Scholar

Dr. Astrid K. Gnekow

I. Klinik für Kinder und Jugendliche

Stenglinstraße 2

86156 Augsburg

Phone: Tel. 08 21-400 34 05

Fax: Fax 0821-400 33 32

Email: E-mail: KZVA.HIT-LGG@t-online.de

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