@article{8e11679f06a94299970942f351f4169c,
title = "A pilot precision medicine trial for children with diffuse intrinsic pontine glioma—PNOC003: A report from the Pacific Pediatric Neuro-Oncology Consortium",
abstract = "This clinical trial evaluated whether whole exome sequencing (WES) and RNA sequencing (RNAseq) of paired normal and tumor tissues could be incorporated into a personalized treatment plan for newly diagnosed patients (<25 years of age) with diffuse intrinsic pontine glioma (DIPG). Additionally, whole genome sequencing (WGS) was compared to WES to determine if WGS would further inform treatment decisions, and whether circulating tumor DNA (ctDNA) could detect the H3K27M mutation to allow assessment of therapy response. Patients were selected across three Pacific Pediatric Neuro-Oncology Consortium member institutions between September 2014 and January 2016. WES and RNAseq were performed at diagnosis and recurrence when possible in a CLIA-certified laboratory. Patient-derived cell line development was attempted for each subject. Collection of blood for ctDNA was done prior to treatment and with each MRI. A specialized tumor board generated a treatment recommendation including up to four FDA-approved agents based upon the genomic alterations detected. A treatment plan was successfully issued within 21 business days from tissue collection for all 15 subjects, with 14 of the 15 subjects fulfilling the feasibility criteria. WGS results did not significantly deviate from WES-based therapy recommendations; however, WGS data provided further insight into tumor evolution and fidelity of patient-derived cell models. Detection of the H3F3A or HIST1H3B K27M (H3K27M) mutation using ctDNA was successful in 92% of H3K27M mutant cases. A personalized treatment recommendation for DIPG can be rendered within a multicenter setting using comprehensive next-generation sequencing technology in a clinically relevant timeframe.",
keywords = "circulating tumor DNA, diffuse intrinsic pontine glioma, genomics-guided clinical trial, next generation sequencing, precision medicine",
author = "Sabine Mueller and Payal Jain and Liang, {Winnie S.} and Lindsay Kilburn and Cassie Kline and Nalin Gupta and Eshini Panditharatna and Magge, {Suresh N.} and Bo Zhang and Yuankun Zhu and Crawford, {John R.} and Anu Banerjee and Kellie Nazemi and Packer, {Roger J.} and Petritsch, {Claudia K.} and Nathalene Truffaux and Alison Roos and Sara Nasser and Phillips, {Joanna J.} and David Solomon and Annette Molinaro and Waanders, {Angela J.} and Byron, {Sara A.} and Berens, {Michael E.} and John Kuhn and Javad Nazarian and Michael Prados and Resnick, {Adam C.}",
note = "Funding Information: The authors would like to acknowledge the generosity of all patients and their families for participating in this study. We thank all clinical staff at the PNOC sites who cared for these patients. We acknowledge John Carpten and David Craig for having pioneered the implementation pipeline underlying TGEN Genomics-Guided Treatment Practice. We appreciate help from the Brain Tumor Center Tissue Core at UCSF for handling and shipping both clinical trial and autopsy samples. We thank members of the Children{\textquoteright}s Brain tumor Tissue Consortium (CBTTC) and its operation center including Jennifer Mason, Elizabeth Appert, Mateusz Koptyra, David Stokes and Jena Lilly along with Pichai Raman and Allison Heath from the D3b team. We would also like to thank all members of PNOC for their support. We also thank Mitch Berger, UCSF for his ongoing support of this study and guidance. This work was funded by the V Foundation (Atlanta, GA), Pediatric Brain Tumor Foundation (Asheville, NC), TGEN Foundation, Dragon Master Foundation, Kortney Rose Foundation, Musella Foundation, Project Open DIPG, The Gabriella Miller Kids First Data Resource Center, Goldwin foundation, Smashing Walnuts Foundation, Piedmont Community Foundation, Matthew Larson Foundation, Kaminsky Foundation, the PNOC Foundation, the Jenny{\textquoteright}s Qust Foundation as well as generous donations from families and patients. Funding Information: The authors would like to acknowledge the generosity of all patients and their families for participating in this study. We thank all clinical staff at the PNOC sites who cared for these patients. We acknowledge John Carpten and David Craig for having pioneered the implementation pipeline underlying TGEN Genomics-Guided Treatment Practice. We appreciate help from the Brain Tumor Center Tissue Core at UCSF for handling and shipping both clinical trial and autopsy samples. We thank members of the Children's Brain tumor Tissue Consortium (CBTTC) and its operation center including Jennifer Mason, Elizabeth Appert, Mateusz Koptyra, David Stokes and Jena Lilly along with Pichai Raman and Allison Heath from the D3b team. We would also like to thank all members of PNOC for their support. We also thank Mitch Berger, UCSF for his ongoing support of this study and guidance. This work was funded by the V Foundation (Atlanta, GA), Pediatric Brain Tumor Foundation (Asheville, NC), TGEN Foundation, Dragon Master Foundation, Kortney Rose Foundation, Musella Foundation, Project Open DIPG, The Gabriella Miller Kids First Data Resource Center, Goldwin foundation, Smashing Walnuts Foundation, Piedmont Community Foundation, Matthew Larson Foundation, Kaminsky Foundation, the PNOC Foundation, the Jenny's Qust Foundation as well as generous donations from families and patients. Funding Information: Key words: diffuse intrinsic pontine glioma, precision medicine, next generation sequencing, circulating tumor DNA, genomics-guided clinical trial Abbreviations: CNS: central nervous system; CSF: cerebrospinal fluid; ctDNA: circulating tumor DNA; CLIA: clinical laboratory improvement amendments; CWL: common workflow language; CNAs: copy number alterations; CNV: copy number variation; DIPG: diffuse intrinsic pontine glioma; ddPCR: droplet digital polymerase chain reaction; FDA: food and drug administration; GEM: genomic-enabled medicine; H3K27M: histone 3 K27M mutation; HDAC: histone deacetylase; KMS: Kaplan–Meier survival; LCR: low-complexity regions; MRI: magnetic resonance imaging; MAF: mutation allele frequency; NIH: National Institutes of Health; QC: quality control; RIN: RNA integrity number; RNAseq: RNA sequencing; SV: structural variant; TGEN: Translational Genomic Research Institute; UCSF: University of California San Francisco; WES: whole exome sequencing; WGS: whole genome sequencing Additional Supporting Information may be found in the online version of this article. Conflict of interest: The authors have no conflict of interest to declare. *J.N., M.P. and A.C.R. shared senior authorship Grant sponsor: Dragon Master Foundation; Grant sponsor: Gabriella Kids First Data Resource Center; Grant sponsor: Goldwin foundation; Grant sponsor: Kaminsky Foundation; Grant sponsor: Kortney Rose Foundation; Grant sponsor: Matthew Larson Foundation for Pediatric Brain Tumors; Grant sponsor: Musella Foundation For Brain Tumor Research and Information; Grant sponsor: Piedmont Community Foundation; Grant sponsor: Project Open DIPG; Grant sponsor: Smashing Walnuts Foundation; Grant sponsor: TGEN Foundation; Grant sponsor: V Foundation for Cancer Research; Grant sponsor: Pediatric Brain Tumor Foundation (Asheville, NC); Grant sponsor: PNOC Foundation and Jennys Quest for Cure Foundation DOI: 10.1002/ijc.32258 History: Received 12 Nov 2018; Accepted 15 Feb 2019; Online 12 Mar 2019. Correspondence to: Sabine Mueller, MD PhD MAS, Department of Neurology, Neurosurgery and Pediatrics, University of California, Sandler Neuroscience Building, 675 Nelson Rising Lane, Room 402B, San Francisco, CA 94148, USA, Tel.: +1-415-502-7301, Fax: +1-415-502-7299, E-mail: sabine.mueller@ucsf.edu Publisher Copyright: {\textcopyright} 2019 UICC",
year = "2019",
doi = "10.1002/ijc.32258",
language = "English (US)",
volume = "145",
pages = "1889--1901",
journal = "International Journal of Cancer",
issn = "0020-7136",
publisher = "Wiley-Liss Inc.",
number = "7",
}