<p>The second Paediatric Therapeutic Development Workshop focused on medulloblastoma. Between 60–70% of patients with medulloblastoma survive, but survivors have significant long-term side effects, and the highest-risk groups have a probability of survival &lt;10%. Thus, the unmet need is to develop therapeutics targeting specific vulnerabilities in medulloblastoma including poor prognosis disease groups (SHH-medulloblastoma, <i>MYCN</i> amplified or <i>TP53</i> mutated; and Group 3 medulloblastoma, c-<i>MYC</i> amplified) and developing less-toxic therapies for good prognosis disease (WNT-medulloblastoma). The Workshop concluded that (i) targeting SRC by a degrader is a high priority, (ii) inhibition of c-<i>MYC</i> and <i>MYCN</i> tumour-relevant functions for poor prognosis groups is a priority, (iii) targeting WNT-medulloblastoma via a radiolabelled theranostic antibody is an innovative approach for good prognosis tumours to further reduce toxicity, and (iv) B7-H3 has many advantages for CAR T-cell and ADC-based approaches. Based on currently available evidence, combinations of central nervous system penetrant selective PARP-1, CHK1/2 or CDK9 inhibitors with an ATR inhibitor could potentially be evaluated in early-phase trials for high-risk patients; however, these combinations require robust evaluation in pre-clinical models first. Early-phase clinical studies should be international, have novel designs to address small patient numbers and based on an understanding of biology with correlative biological studies. Both developing therapeutics targeting specific vulnerabilities in medulloblastoma and evaluating combinations of existing medicinal products are required to improve outcome and reduce long term sequalae.</p>

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Paediatric therapeutic development workshop on medulloblastoma

  • Claudia Montiel Equihua,
  • Joseph S. Baxter,
  • Jan J. Molenaar,
  • Itziar Areso,
  • Samuel Abbou,
  • John Anderson,
  • Nicolas Andre,
  • Olivier Ayrault,
  • Patricia Blanc,
  • Natalie Carpenter,
  • Sam Daems,
  • Vicenzo D’Angiolella,
  • Laura Danielson,
  • Laura Donovan,
  • Adam D. Durbin,
  • Maryam Fouladi,
  • Amar Gajjar,
  • Richard Gilbertson,
  • Géraldine Giraud,
  • Nick Gottardo,
  • Rebecca Hill,
  • Pamela Kearns,
  • Marcel Kool,
  • Geffen Lass,
  • Silvia Marino,
  • Sabine Mueller,
  • Simon Newman,
  • James Olson,
  • Sheena Patel,
  • Stefan M. Pfister,
  • John Rainsbury,
  • Vijay Ramaswamy,
  • Stefan Rutkowski,
  • Karin Straathof,
  • Frederik J. Swartling,
  • Robert J. Wechsler-Reya,
  • Andrew D. J. Pearson,
  • David Jenkinson,
  • Francois Doz,
  • Steven C. Clifford,
  • Joseph S. Baxter,
  • Itziar Areso,
  • Geffen Lass,
  • Andrew D. J. Pearson,
  • David Jenkinson,
  • Jan J. Molenaar,
  • Pamela Kearns,
  • Sheena Patel,
  • Patricia Blanc,
  • Sam Daems

摘要

The second Paediatric Therapeutic Development Workshop focused on medulloblastoma. Between 60–70% of patients with medulloblastoma survive, but survivors have significant long-term side effects, and the highest-risk groups have a probability of survival <10%. Thus, the unmet need is to develop therapeutics targeting specific vulnerabilities in medulloblastoma including poor prognosis disease groups (SHH-medulloblastoma, MYCN amplified or TP53 mutated; and Group 3 medulloblastoma, c-MYC amplified) and developing less-toxic therapies for good prognosis disease (WNT-medulloblastoma). The Workshop concluded that (i) targeting SRC by a degrader is a high priority, (ii) inhibition of c-MYC and MYCN tumour-relevant functions for poor prognosis groups is a priority, (iii) targeting WNT-medulloblastoma via a radiolabelled theranostic antibody is an innovative approach for good prognosis tumours to further reduce toxicity, and (iv) B7-H3 has many advantages for CAR T-cell and ADC-based approaches. Based on currently available evidence, combinations of central nervous system penetrant selective PARP-1, CHK1/2 or CDK9 inhibitors with an ATR inhibitor could potentially be evaluated in early-phase trials for high-risk patients; however, these combinations require robust evaluation in pre-clinical models first. Early-phase clinical studies should be international, have novel designs to address small patient numbers and based on an understanding of biology with correlative biological studies. Both developing therapeutics targeting specific vulnerabilities in medulloblastoma and evaluating combinations of existing medicinal products are required to improve outcome and reduce long term sequalae.