Your search keyword '"Jonathan L Finlay"' showing total 490 results

1. Continuous and bolus intraventricular topotecan prolong survival in a mouse model of leptomeningeal medulloblastoma.

Author

Gregory M Shackleford, Min Y Mahdi, Rex A Moats, Debra Hawes, Hung C Tran, Jonathan L Finlay, Tuan Q Hoang, Ellis F Meng, and Anat Erdreich-Epstein

Subjects

Medicine, Science

Abstract

Leptomeningeal metastasis remains a difficult clinical challenge. Some success has been achieved by direct administration of therapeutics into the cerebrospinal fluid (CSF) circumventing limitations imposed by the blood brain barrier. Here we investigated continuous infusion versus bolus injection of therapy into the CSF in a preclinical model of human Group 3 medulloblastoma, the molecular subgroup with the highest incidence of leptomeningeal disease. Initial tests of selected Group 3 human medulloblastoma cell lines in culture showed that D283 Med and D425 Med were resistant to cytosine arabinoside and methotrexate. D283 Med cells were also resistant to topotecan, whereas 1 μM topotecan killed over 99% of D425 Med cells. We therefore introduced D425 Med cells, modified to express firefly luciferase, into the CSF of immunodeficient mice. Mice were then treated with topotecan or saline in five groups: continuous intraventricular (IVT) topotecan via osmotic pump (5.28 μg/day), daily bolus IVT topotecan injections with a similar daily dose (6 μg/day), systemic intraperitoneal injections of a higher daily dose of topotecan (15 μg/day), daily IVT pumped saline and daily intraperitoneal injections of saline. Bioluminescence analyses revealed that both IVT topotecan treatments effectively slowed leptomeningeal tumor growth in the brains. Histological analysis showed that they were associated with localized brain necrosis, possibly due to backtracking of topotecan around the catheter. In the spines, bolus IVT topotecan showed a trend towards slower tumor growth compared to continuous (pump) IVT topotecan, as measured by bioluminescence. Both continuous and bolus topotecan IVT showed longer survival compared to other groups. Thus, both direct IVT topotecan CSF delivery methods produced better anti-medulloblastoma effect compared to systemic therapy at the dosages used here.

Published

2019

2. Molecular characterization of gliomas and glioneuronal tumors amid Noonan syndrome: cancer predisposition examined

Author

Margaret Shatara, Kathleen M. Schieffer, Marilena Melas, Elizabeth A. Varga, Diana Thomas, Brianna A. Bucknor, Heather M. Costello, Gregory Wheeler, Benjamin J. Kelly, Katherine E. Miller, Diana P. Rodriguez, Mariam T. Mathew, Kristy Lee, Erin Crotty, Sarah Leary, Vera A. Paulson, Bonnie Cole, Mohamed S. Abdelbaki, Jonathan L. Finlay, Margot A. Lazow, Ralph Salloum, Maryam Fouladi, Daniel R. Boué, Elaine R. Mardis, and Catherine E. Cottrell

Subjects

glioma, glioneuronal tumor, Noonan syndrome, cancer predisposition, PTPN11, germline, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

IntroductionIn the setting of pediatric and adolescent young adult cancer, increased access to genomic profiling has enhanced the detection of genetic variation associated with cancer predisposition, including germline syndromic conditions. Noonan syndrome (NS) is associated with the germline RAS pathway activating alterations and increased risk of cancer. Herein, we describe our comprehensive molecular profiling approach, the association of NS with glioma and glioneuronal tumors, and the clinical and histopathologic characteristics associated with the disease.MethodsWithin an institutional pediatric cancer cohort (n = 314), molecular profiling comprised of paired somatic disease–germline comparator exome analysis, RNA sequencing, and tumor classification by DNA methylation analysis was performed.ResultsThrough the implementation of paired analysis, this study identified 4 of 314 (1.3%) individuals who harbored a germline PTPN11 variant associated with NS, of which 3 individuals were diagnosed with a glioma or glioneuronal tumor. Furthermore, we extend this study through collaboration with a peer institution to identify two additional individuals with NS and a glioma or glioneuronal tumor. Notably, in three of five (60%) individuals, paired genomic profiling led to a previously unrecognized diagnosis of Noonan syndrome despite an average age of cancer diagnosis of 16.8 years. The study of the disease-involved tissue identified signaling pathway dysregulation through somatic alteration of genes involved in cellular proliferation, survival, and differentiation.DiscussionComparative pathologic findings are presented to enable an in-depth examination of disease characteristics. This comprehensive analysis highlights the association of gliomas and glioneuronal tumors with RASopathies and the potential therapeutic challenges and importantly demonstrates the utility of genomic profiling for the identification of germline cancer predisposition.

Published

2024

3. False-positive magnetic resonance imaging findings in follow-up of pediatric patients with tumors of the central nervous system

Author

Satiro Nakamura De Oliveira, Ignacio Gonzalez-Gomez, Ashok Panigrahy, Mark Krieger, Gordon McComb, Jonathan L Finlay, and Girish Dhall

Subjects

Medicine (General), R5-920

Abstract

Management of patients with central nervous system tumors relies largely on magnetic resonance imaging scans to document disease progression or recurrence. The finding of new lesions always presents the challenge of differentiating between post-surgical changes, radiation necrosis, gliosis, and tumor, submitting these patients to more aggressive therapy and more toxicity. We reviewed the medical records of three patients with primary central nervous system tumors treated at the Children’s Hospital Los Angeles who had new false-positive magnetic resonance imaging findings suggestive of tumor recurrence. All of them had complete total resection of primary tumor, had received involved-field radiation therapy, had biopsies confirming absence of viable tumor, and all three patients are long-term survivors. These cases exemplify that not everything that enhances on brain or spine magnetic resonance imaging is viable tumor, and a biopsy should always be considered in the decision-making process in evaluation of potentially recurrent central nervous system tumors in pediatric patients. A step-wise approach for such challenging cases is presented in this article.

Published

2016

4. Disseminated medulloblastoma in a child with germline BRCA2 6174delT mutation and without Fanconi anemia

Author

Jingying eXu, Ashley Sloane Margol, Anju eShukla, Xiuhai eRen, Jonathan L Finlay, Mark D Krieger, Floyd H Gilles, Fergus J Couch, Meraj eAziz, Eric T Fung, Shahab eAsgharzadeh, Michael T Barrett, and Anat eErdreich-Epstein

Subjects

Fanconi Anemia, MYC, BRCA2 6174delT, Group 4 medulloblastoma, medulloblastoma cell lines, Recurrenct medulloblastoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Medulloblastoma, the most common malignant brain tumor in children, occurs with increased frequency in individuals with Fanconi anemia who have biallelic germline mutations in BRCA2. We describe an 8 year old child who had disseminated anaplastic medulloblastoma and a deleterious heterozygous BRCA2 6174delT germline mutation. Molecular profiling was consistent with Group 4 medulloblastoma. The posterior fossa mass was resected and the patient received intensive chemotherapy and craniospinal irradiation. Despite this, the patient succumbed to a second recurrence of his medulloblastoma, which presented eight months after diagnosis as malignant pleural and peritoneal effusions. Continuous medulloblastoma cell lines were isolated from the original tumor (CHLA-01-MED) and the malignant pleural effusion (CHLA-01R-MED). Here we provide their analyses, including in vitro and in vivo growth, drug sensitivity, comparative genomic hybridization and next generation sequencing analysis. In addition to the BRCA2 6174delT, the medulloblastoma cells had amplification of MYC, deletion at Xp11.2 and isochromosome 17, but no structural variations or overexpression of GFI1 or GFI1B. To our knowledge, this is the first pair of diagnosis/recurrence medulloblastoma cell lines, the only medulloblastoma cell lines with BRCA2 6174delT described to date, and the first reported case of a child with medulloblastoma associated with a germline BRCA2 6174delT who did not also have Fanconi anemia.

Published

2015

5. Intracranial non-germinomatous germ cell tumors in children and adolescents: how can the experience from an uppermiddle-income country contribute to the worldwide effort to improve outcomes?

Author

Andrea M. Cappellano, Natalia Dassi, Bruna M. Mançano, Sidnei Epelman, Daniela B. Almeida, Sergio Cavalheiro, Patricia A. Dastoli, Maria T. S. Alves, Jardel M. Nicacio, Marcos D. S. Costa, Frederico A. Silva, Simone S. Aguiar, Maria L. Figueiredo, Michael Chen, Nasjla S. Silva, and Jonathan L. Finlay

Subjects

intracranial germ cell tumors (iGCTs), middle income countries (MIC), reduced radiotherapy, autologous stem cell transplantation (ASCT), non-germinomatous cell tumor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

BackgroundNon-germinomatous germ cell tumors (NGGCT) accounts for one third of intracranial GCT. While the germinoma group have an excellent overall survival, the standard of practice for children with NGGCT is still under evaluation.AimsDescribe the results of the of the Brazilian consortium protocol.MethodsSince 2013, 15 patients with a diagnosis of NGGCT by histopathology and/or serum/cerebrospinal fluid (CSF) tumor markers, βHCG >200mlU/ml and/or positive alpha-fetoprotein were treated with neoadjuvant chemotherapy with carboplatin, cyclophosphamide and etoposide followed by ventricular radiotherapy (RTV) of 18Gy with boost (32Gy) to the primary site. Metastatic patients underwent craniospinal irradiation (CSI) and “slow responders” to the four initial cycles of CT, to autologous stem cell transplantation (ASCT) followed by CSI.ResultsMean age, 13.1 years. Thirteen males. Primary sites: pineal (n=12), suprasellar (n=2) and bifocal (n=1). Four patients were metastatic at diagnosis. Eight patients had CSF and/or serum alpha-fetoprotein levels > 1,000ng/ml. Tumor responses after chemotherapy demonstrated complete in six cases and partial in seven, with “second-look” surgery being performed in five cases, and two patients presenting viable lesions being referred to ASCT. The main toxicity observed was hematological grades 3/4. Two patients with metastatic disease, one with Down Syndrome and AFP > 1,000ng/ml and the other with choriocarcinoma and pulmonary metastases, developed progressive disease resulting in death, as well as two other patients without evidence of disease, due to endocrinological disorders. Event-free and overall survival at 2 and 5 years were 80% and 72.7%, respectively, with a mean follow-up of 48 months (range, 7-107).ConclusionsDespite the small number of patients, in our series, treatment with six cycles of chemotherapy and RTV with focal boost for localized disease (n=11) and ACST for identified slow responders (n=2) seem to be effective strategies contributing to the overall effort to improve outcomes of this group of patients.

Published

2024

6. Characterizing temporal genomic heterogeneity in pediatric low-grade gliomas

Author

Margot A. Lazow, Lindsey Hoffman, Austin Schafer, Diana S. Osorio, Daniel R. Boué, Sarah Rush, Erin Wright, Adam Lane, Mariko D. DeWire-Schottmiller, Teresa Smolarek, Jared Sipple, Heather Taggert, Jaime Reuss, Ralph Salloum, Trent R. Hummel, Peter de Blank, Natasha Pillay-Smiley, Mary E. Sutton, Anthony Asher, Charles B. Stevenson, Rachid Drissi, Jonathan L. Finlay, Maryam Fouladi, and Christine Fuller

Subjects

Pediatric low-grade gliomas, Genomics, Paired, Recurrence, Tumor evolution, BRAF, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Recent discoveries have provided valuable insight into the genomic landscape of pediatric low-grade gliomas (LGGs) at diagnosis, facilitating molecularly targeted treatment. However, little is known about their temporal and therapy-related genomic heterogeneity. An adequate understanding of the evolution of pediatric LGGs’ genomic profiles over time is critically important in guiding decisions about targeted therapeutics and diagnostic biopsy at recurrence. Fluorescence in situ hybridization, mutation-specific immunohistochemistry, and/or targeted sequencing were performed on paired tumor samples from primary diagnostic and subsequent surgeries. Ninety-four tumor samples from 45 patients (41 with two specimens, four with three specimens) from three institutions underwent testing. Conservation of BRAF fusion, BRAF V600E mutation, and FGFR1 rearrangement status was observed in 100%, 98%, and 96% of paired specimens, respectively. No loss or gain of IDH1 mutations or NTRK2, MYB, or MYBL1 rearrangements were detected over time. Histologic diagnosis remained the same in all tumors, with no acquired H3K27M mutations or malignant transformation. Changes in CDKN2A deletion status at recurrence occurred in 11 patients (42%), with acquisition of hemizygous CDKN2A deletion in seven and loss in four. Shorter time to progression and shorter time to subsequent surgery were observed among patients with acquired CDKN2A deletions compared to patients without acquisition of this alteration [median time to progression: 5.5 versus 16.0 months (p = 0.048); median time to next surgery: 17.0 months versus 29.0 months (p = 0.031)]. Most targetable genetic aberrations in pediatric LGGs, including BRAF alterations, are conserved at recurrence and following chemotherapy or irradiation. However, changes in CDKN2A deletion status over time were demonstrated. Acquisition of CDKN2A deletion may define a higher risk subgroup of pediatric LGGs with a poorer prognosis. Given the potential for targeted therapies for tumors harboring CDKN2A deletions, biopsy at recurrence may be indicated in certain patients, especially those with rapid progression.

Published

2020

7. Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

Vallijah Subasri, Nicholas Light, Nisha Kanwar, Jack Brzezinski, Ping Luo, Jordan R. Hansford, Elizabeth Cairney, Carol Portwine, Christine Elser, Jonathan L. Finlay, Kim E. Nichols, Noa Alon, Ledia Brunga, Jo Anson, Wendy Kohlmann, Kelvin C. de Andrade, Payal P. Khincha, Sharon A. Savage, Joshua D. Schiffman, Rosanna Weksberg, Trevor J. Pugh, Anita Villani, Adam Shlien, Anna Goldenberg, and David Malkin

Abstract

Li-Fraumeni syndrome (LFS) is an autosomal dominant cancer-predisposition disorder. Approximately 70% of individuals who fit the clinical definition of LFS harbor a pathogenic germline variant in the TP53 tumor suppressor gene. However, the remaining 30% of patients lack a TP53 variant and even among variant TP53 carriers, approximately 20% remain cancer-free. Understanding the variable cancer penetrance and phenotypic variability in LFS is critical to developing rational approaches to accurate, early tumor detection and risk-reduction strategies. We leveraged family-based whole-genome sequencing and DNA methylation to evaluate the germline genomes of a large, multi-institutional cohort of patients with LFS (n = 396) with variant (n = 374) or wildtype TP53 (n = 22). We identified alternative cancer-associated genetic aberrations in 8/14 wildtype TP53 carriers who developed cancer. Among variant TP53 carriers, 19/49 who developed cancer harbored a pathogenic variant in another cancer gene. Modifier variants in the WNT signaling pathway were associated with decreased cancer incidence. Furthermore, we leveraged the noncoding genome and methylome to identify inherited epimutations in genes including ASXL1, ETV6, and LEF1 that confer increased cancer risk. Using these epimutations, we built a machine learning model that can predict cancer risk in patients with LFS with an area under the receiver operator characteristic curve (AUROC) of 0.725 (0.633–0.810). Significance: Our study clarifies the genomic basis for the phenotypic variability in LFS and highlights the immense benefits of expanding genetic and epigenetic testing of patients with LFS beyond TP53. More broadly, it necessitates the dissociation of hereditary cancer syndromes as single gene disorders and emphasizes the importance of understanding these diseases in a holistic manner as opposed to through the lens of a single gene.

Published

2023

8. Incidence and survival of choroid plexus tumors in the United States

Author

Kailey Takaoka, Gino Cioffi, Kristin A Waite, Jonathan L Finlay, Daniel Landi, Kaitlyn Greppin, Carol Kruchko, Quinn T Ostrom, and Jill S Barnholtz-Sloan

Subjects

Medicine (miscellaneous)

Abstract

Background There are limited data available on incidence and survival of patients with choroid plexus tumors (CPT). This study provides the most current epidemiological analysis of choroid plexus tumors from 2004 to 2017 in the United States. Methods Data on 2013 patients with CPT were acquired from the Central Brain Tumor Registry of the United States in collaboration with the Centers for Disease Control and Prevention (CDC) and the National Cancer Institute, from 2004 to 2017. CPT cases were classified by the following pathological subtypes: choroid plexus papilloma (CPP), atypical choroid plexus papilloma (aCPP), and choroid plexus carcinoma (CPC). Frequencies and age-adjusted incidence rates (AAIR) per 100 000 and rate ratios per 100 000 (IRR) were reported for age, sex, race, and ethnicity for each pathological subtype with 95% confidence intervals (95% CI). Using CDC’s National Program of Cancer Registries survival database, survival curves and hazard ratios (HRs) evaluated overall survival from 2001 to 2016. Results CPP had the highest overall incidence (AAIR: 0.034, 95% CI: 0.033–0.036), followed by CPC (AAIR: 0.008, 95% CI: 0.008–0.009) and aCPP (AAIR: 0.005, 95% CI: 0.005–0.006). Incidence was highest among children less than one year old among all subtypes (CPP AAIR: 0.278; aCPP AAIR: 0.140; CPC AAIR: 0.195), reducing as patients aged. Overall survival was worse among patients with CPC, being five times more likely to die compared to patients with CPP (HR: 5.23, 95% CI: 4.05–7.54, P Conclusions This analysis is the most current and comprehensive study in the US on the incidence and survival for CPT. Population based statistics provide critical information in understanding disease characteristics, which impact patient care and prognosis.

Published

2022

9. FIGURE 4 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Secondary constitutional epimutations in LFS. A, Concordance between enrichment scores of 931 EWAS probes found significantly associated with cancer status in the discovery cohort and the validation cohort, for both the internal (left) and external (right) validation cohort. Blue = associated with cancer status and a cis-CSCE; Red = associated with cancer status but not a cis-CSCE. B, Manhattan plot of adjusted P values from meQTL association tests between the 931 EWAS probes and their most correlated rsSNP. Red line: FDR = 0.1; Blue line: FDR = 0.01; Green points: probes in cancer genes with FDR < 0.1. C, Top cis-CSCE in ETV6, TET3, MIR143, ASXL1, PARVB, and LRG1.D, Feature enrichment heatmap of the 259 significant cis-CSCE loci showing adjusted P value (p) and effect size (d). E, ROC curve of the epimutation cancer risk model on the test set. F, UMAP projection of methylation at 259 cis-CSCE for all patients, colored by cancer status. G, UMAP projection of methylation at 259 cis-CSCE for all patients, colored by clusters associated with risk. H, Kaplan–Meier survival curve demonstrating significant differences in survival probability between the three epimutation clusters.

Published

2023

10. TABLE 1 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Variants in cancer predisposition genes (class 1–2) in the wildtype and variant TP53 cohorts, annotated with cancer type, sex, LFS criteria, inheritance status, segregation, variant location, variant function, and zygosity

Published

2023

11. Supplementary Data S6 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

cisCSCE

Published

2023

12. FIGURE 3 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Pedigrees and class 1–3 variants for two wildtype TP53 families that fit the classic LFS criteria. A, Pedigree of wildtype TP53 family (WT4) that fits the classic LFS criteria with four family members sequenced, two that developed cancer and two that are cancer-free. B, Pedigree of wildtype TP53 family (WT6) that fits the classic LFS criteria with six family members sequenced: five that developed cancer and one that is cancer-free.

Published

2023

13. TABLE 2 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Genomics informed risk stratification guidelines for patients with LFS with a germline TP53 variant

Published

2023

14. Supplementary Figures S1-S12 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Supplementary Figures

Published

2023

15. Data from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Li-Fraumeni syndrome (LFS) is an autosomal dominant cancer-predisposition disorder. Approximately 70% of individuals who fit the clinical definition of LFS harbor a pathogenic germline variant in the TP53 tumor suppressor gene. However, the remaining 30% of patients lack a TP53 variant and even among variant TP53 carriers, approximately 20% remain cancer-free. Understanding the variable cancer penetrance and phenotypic variability in LFS is critical to developing rational approaches to accurate, early tumor detection and risk-reduction strategies. We leveraged family-based whole-genome sequencing and DNA methylation to evaluate the germline genomes of a large, multi-institutional cohort of patients with LFS (n = 396) with variant (n = 374) or wildtype TP53 (n = 22). We identified alternative cancer-associated genetic aberrations in 8/14 wildtype TP53 carriers who developed cancer. Among variant TP53 carriers, 19/49 who developed cancer harbored a pathogenic variant in another cancer gene. Modifier variants in the WNT signaling pathway were associated with decreased cancer incidence. Furthermore, we leveraged the noncoding genome and methylome to identify inherited epimutations in genes including ASXL1, ETV6, and LEF1 that confer increased cancer risk. Using these epimutations, we built a machine learning model that can predict cancer risk in patients with LFS with an area under the receiver operator characteristic curve (AUROC) of 0.725 (0.633–0.810).Significance:Our study clarifies the genomic basis for the phenotypic variability in LFS and highlights the immense benefits of expanding genetic and epigenetic testing of patients with LFS beyond TP53. More broadly, it necessitates the dissociation of hereditary cancer syndromes as single gene disorders and emphasizes the importance of understanding these diseases in a holistic manner as opposed to through the lens of a single gene.

Published

2023

16. FIGURE 2 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Germline genetic variants in LFS. A, Classification scheme for genetic variants identified from WGS. The pyramid (top) shows how genes were prioritized into four tiers from highest known cancer predisposition potential to lowest. All variants were then classified using a Cancer Variant Classification Schema (Materials and Methods) into five classes (bottom) based on pathogenicity and whether the gene fell into Tier 1–4. AD: autosomal dominant; AR: autosomal recessive; CPG: cancer predisposition gene. B, Frequency of P/LP variants in known cancer genes (class 1–3) in LFS, KiCS and 1kGP. Fisher exact test P values for comparisons between the LFS cohorts and KiCS/1kGP shown. C, Kaplan–Meier survival curve comparing patients with P/LP variants in the WNT signaling pathway (yellow), patients with at least one class 1–3 variant (red) and patients with neither WNT signaling or class 1–3 variants (blue). D, Landscape of genetic alterations in cancer genes (class 1–3) in LFS. Annotated with family, cancer type and TP53 variant status. Genetic variants are indicated as a deletion (blue), SNV or indel (red) or duplication (purple). E, The proportion of individuals in the wildtype and variant TP53 cohorts with classes 1–5 variants (Materials and Methods). F, The number of P/LP variants in cancer genes (class 1–3) in individuals that developed cancer compared with unaffected individuals, stratified by TP53 status. G, The number of P/LP variants (class 1–3) in wildtype versus variant TP53 carriers, stratified by cancer status. On the basis of the premise that variants in the WNT signaling pathway are associated with decreased cancer incidence in LFS, these variants were removed from the comparisons made in F and G.

Published

2023

17. FIGURE 5 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

Differential regulation of WNT signaling and LEF1 in LFS. A, Probes in the WNT signaling pathway (WNT4, SMAD3, SFRP4, SERPINF) significantly associated with cancer status. B, Probe in the body of LEF1 (cg03041109) associated with cancer status (FDR = 0.07). C, Methylation of probe in body of LEF1 (cg03041109) across members within each LFS family. Probands almost unanimously have higher LEF1 methylation than their unaffected family members. D, Plasma cfDNA methylation of the body of LEF1 (chr4:109056901-109057200), between patients with LFS and HBCs. E, Tumor methylation of the body of LEF1 (cg03041109) in CPTs, with and without a germline variant in TP53.

Published

2023

18. FIGURE 1 from Multiple Germline Events Contribute to Cancer Development in Patients with Li-Fraumeni Syndrome

Author

David Malkin, Anna Goldenberg, Adam Shlien, Anita Villani, Trevor J. Pugh, Rosanna Weksberg, Joshua D. Schiffman, Sharon A. Savage, Payal P. Khincha, Kelvin C. de Andrade, Wendy Kohlmann, Jo Anson, Ledia Brunga, Noa Alon, Kim E. Nichols, Jonathan L. Finlay, Christine Elser, Carol Portwine, Elizabeth Cairney, Jordan R. Hansford, Ping Luo, Jack Brzezinski, Nisha Kanwar, Nicholas Light, and Vallijah Subasri

Abstract

The LFS cohort. A, Patient cohort and characteristics (age of first cancer onset, tumor type) by TP53 status and whether profiling was performed using WGS, methylation or both. AA = adrenal adenoma; ACC = adrenocortical carcinoma; ALL = acute lymphoid leukemia; CPC = choroid plexus carcinoma; CSA = chondrosarcoma; GCT = germ cell tumor; LMS = leiomyosarcoma; MFH = malignant fibrous histiocytoma; MFS = myxofibrosarcoma; NHL = non–Hodgkin lymphoma; OS = osteosarcoma; RMS = rhabdomyosarcoma. B, Lollipop plot displaying the location and number of SNVs and indels on the canonical TP53 transcript: NM_000546, which consists of a TAD, DBD, and tetramerization domain. TP53 hotspot variants present in our cohort (175, 245, 248, 273, 282) are highlighted.

Published

2023

19. Outcome of Children and Adolescents With Primary Intracranial Germinoma Treated With Chemotherapy and Reduced Dose-Field Irradiation: A Prospective Brazilian Experience

Author

Andrea Maria Cappellano, Natalia Dassi, Bruna Mançano, Sidnei Epelman, Daniela B. Almeida, Sergio Cavalheiro, Patricia A. Dastoli, Maria Teresa Seixas, Jardel M. Nicacio, Marcos D. Costa, Frederico A. Silva, Simone S. Aguiar, Carlos R. Almeida, Gustavo R. Teixeira, Michael Chen, Maria Luisa Figueiredo, Nasjla S. Silva, and Jonathan L. Finlay

Subjects

Cancer Research, Oncology

Abstract

PURPOSE This prospective Brazilian single-arm trial was conducted to determine response to chemotherapy and survival after response-based radiotherapy in children with intracranial germinomas, in the setting of a multi-institutional study in a middle-income country (MIC) with significant disparity of subspecialty care. PATIENTS AND METHODS Since 2013, 58 patients with histologic and/or serum and CSF tumor marker evaluations of primary intracranial germ cell tumors were diagnosed; 43 were germinoma with HCGβ levels ≤200 mIU/mL and five between 100 and 200 mIU/mL. The treatment plan consisted of four cycles of carboplatin and etoposide followed by 18 Gy whole-ventricular field irradiation (WVFI) and primary site(s) boost up to 30 Gy; 24 Gy craniospinal was prescribed for disseminated disease. RESULTS Mean age 13.2 years (range, 4.7-25.5 years); 29 were males. Diagnosis was made by tumor markers (n = 6), surgery (n = 25), or both (n = 10). Two bifocal cases with negative tumor markers were treated as germinoma. Primary tumor location was pineal (n = 18), suprasellar (n = 14), bifocal (n = 10), and basal ganglia/thalamus (n = 1). Fourteen had ventricular/spinal spread documented by imaging studies. Second-look surgery occurred in three patients after chemotherapy. Thirty-five patients achieved complete responses after chemotherapy, and eight showed residual teratoma/scar. Toxicity was mostly grade 3/4 neutropenia/thrombocytopenia during chemotherapy. At a median follow-up of 44.5 months, overall and event-free survivals were 100%. CONCLUSION The treatment is tolerable, and WVFI dose reduction to 18 Gy preserves efficacy; we have demonstrated the feasibility of successfully conducting a prospective multicenter trial in a large MIC despite resource disparity.

Published

2023

20. Appendix from Molecular Characterization of Choroid Plexus Tumors Reveals Novel Clinically Relevant Subgroups

Author

David Malkin, Richard J. Gilbertson, David W. Ellison, Uri Tabori, Michael D. Taylor, Cynthia Hawkins, Eric Bouffet, Rosanna Weksberg, Jonathan L. Finlay, Nada Jabado, Maria Isabel Achatz, Stefan M. Pfister, Rishi Lulla, Eugene I. Hwang, Brent T. Harris, Myran Ben-Arush, Rina Dvir, Sanaa Choufani, Ana Novokmet, Ruth Tatevossian, David Shih, Vijay Ramaswamy, Stephen Mack, Malgorzata Pienkowska, Anita Villani, Adam Shlien, and Diana M. Merino

Abstract

Appendix

Published

2023

21. Data from Tumor-Associated Macrophages in SHH Subgroup of Medulloblastomas

Author

Shahab Asgharzadeh, Richard Sposto, Alexander R. Judkins, Floyd H. Gilles, Maryam Fouladi, Rachid Drissi, Mark D. Krieger, Anat Erdreich-Epstein, Jonathan L. Finlay, Girish Dhall, Marzieh Vali, Rebekah J. Kennedy, Long T. Hung, Janahan Gnanachandran, Nathan J. Robison, and Ashley S. Margol

Abstract

Purpose: Medulloblastoma in children can be categorized into at least four molecular subgroups, offering the potential for targeted therapeutic approaches to reduce treatment-related morbidities. Little is known about the role of tumor microenvironment in medulloblastoma or its contribution to these molecular subgroups. Tumor microenvironment has been shown to be an important source for therapeutic targets in both adult and pediatric neoplasms. In this study, we investigated the hypothesis that expression of genes related to tumor-associated macrophages (TAM) correlates with the medulloblastoma molecular subgroups and contributes to a diagnostic signature.Methods: Gene-expression profiling using human exon array (n = 168) was analyzed to identify medulloblastoma molecular subgroups and expression of inflammation-related genes. Expression of 45 tumor-related and inflammation-related genes was analyzed in 83 medulloblastoma samples to build a gene signature predictive of molecular subgroups. TAMs in medulloblastomas (n = 54) comprising the four molecular subgroups were assessed by immunohistochemistry (IHC).Results: A 31-gene medulloblastoma subgroup classification score inclusive of TAM-related genes (CD163 and CSF1R) was developed with a misclassification rate of 2%. Tumors in the Sonic Hedgehog (SHH) subgroup had increased expression of inflammation-related genes and significantly higher infiltration of TAMs than tumors in the Group 3 or Group 4 subgroups (P < 0.0001 and P < 0.0001, respectively). IHC data revealed a strong association between location of TAMs and proliferating tumor cells.Conclusions: These data show that SHH tumors have a unique tumor microenvironment among medulloblastoma subgroups. The interactions of TAMs and SHH medulloblastoma cells may contribute to tumor growth revealing TAMs as a potential therapeutic target. Clin Cancer Res; 21(6); 1457–65. ©2014 AACR.

Published

2023

22. Figure S1 from Molecular Characterization of Choroid Plexus Tumors Reveals Novel Clinically Relevant Subgroups

Author

David Malkin, Richard J. Gilbertson, David W. Ellison, Uri Tabori, Michael D. Taylor, Cynthia Hawkins, Eric Bouffet, Rosanna Weksberg, Jonathan L. Finlay, Nada Jabado, Maria Isabel Achatz, Stefan M. Pfister, Rishi Lulla, Eugene I. Hwang, Brent T. Harris, Myran Ben-Arush, Rina Dvir, Sanaa Choufani, Ana Novokmet, Ruth Tatevossian, David Shih, Vijay Ramaswamy, Stephen Mack, Malgorzata Pienkowska, Anita Villani, Adam Shlien, and Diana M. Merino

Abstract

Figure S1. Sample flow-chart describing the number of biological samples and clinical data obtained through an international multi-institutional effort and the distribution of samples in each microarray

Published

2023

23. Supplemental Methods and Supplemental Figures 1-9 from Tumor-Associated Macrophages in SHH Subgroup of Medulloblastomas

Author

Shahab Asgharzadeh, Richard Sposto, Alexander R. Judkins, Floyd H. Gilles, Maryam Fouladi, Rachid Drissi, Mark D. Krieger, Anat Erdreich-Epstein, Jonathan L. Finlay, Girish Dhall, Marzieh Vali, Rebekah J. Kennedy, Long T. Hung, Janahan Gnanachandran, Nathan J. Robison, and Ashley S. Margol

Abstract

Supplemental Methods and Supplemental Figures 1-9 Supplemental Figure 1. Overview of samples studies and 31-gene signature development Supplemental Figure. 2. Non-negative matrix factorization (NMF) analysis of the combined cohort of medulloblastoma samples (n=168) (A) Cophenetic correlation coefficient based on 2000 clustering runs for 2-10 clusters utilizing genes obtained at varying coefficients of variation; the data demonstrate that the highest cophenetic correlation coefficient was obtained at 4 clusters with 369 genes. (B) NMF consensus heatmap of 4 subgroups using the dataset containing 369 genes with high coefficient of variation. (C) Silhouette plot for identification of outliers. Outliers (n=31) were defined as samples with a silhouette width

Published

2023

24. Supplemental Tables 1-6 from Tumor-Associated Macrophages in SHH Subgroup of Medulloblastomas

Author

Shahab Asgharzadeh, Richard Sposto, Alexander R. Judkins, Floyd H. Gilles, Maryam Fouladi, Rachid Drissi, Mark D. Krieger, Anat Erdreich-Epstein, Jonathan L. Finlay, Girish Dhall, Marzieh Vali, Rebekah J. Kennedy, Long T. Hung, Janahan Gnanachandran, Nathan J. Robison, and Ashley S. Margol

Abstract

Supplemental Tables 1-6 Supplemental Table 1. Patient and tumor characteristics Supplemental Table 2. TLDA design (45 genes) Supplemental Table 3. Information for samples evaluated using HuE Supplemental Table 4. TLDA 31-gene molecular classification of core samples Supplemental Table 5. TLDA 31-gene classification for samples without HuEx data Supplemental Table 6. TLDA 31-gene Confusion Matrix

Published

2023

25. Table S1-S3 from Molecular Characterization of Choroid Plexus Tumors Reveals Novel Clinically Relevant Subgroups

Author

David Malkin, Richard J. Gilbertson, David W. Ellison, Uri Tabori, Michael D. Taylor, Cynthia Hawkins, Eric Bouffet, Rosanna Weksberg, Jonathan L. Finlay, Nada Jabado, Maria Isabel Achatz, Stefan M. Pfister, Rishi Lulla, Eugene I. Hwang, Brent T. Harris, Myran Ben-Arush, Rina Dvir, Sanaa Choufani, Ana Novokmet, Ruth Tatevossian, David Shih, Vijay Ramaswamy, Stephen Mack, Malgorzata Pienkowska, Anita Villani, Adam Shlien, and Diana M. Merino

Abstract

Table S1-S3. S1Choroid plexus tumor chromosomal instability reported in literature S2-Characterization of patient and sample cohort used in analysis S3 Frequency of TP53 mutations in CPTs and characterization of mutation types. Abbreviations: CPC: choroid plexus carcinoma, CPP: choroid plexus papilloma, aCPP: atypical choroid plexus papilloma, SH3: SRC Homology 3 Domain

Published

2023

26. supplemental figure and table legend from Molecular Characterization of Choroid Plexus Tumors Reveals Novel Clinically Relevant Subgroups

Author

David Malkin, Richard J. Gilbertson, David W. Ellison, Uri Tabori, Michael D. Taylor, Cynthia Hawkins, Eric Bouffet, Rosanna Weksberg, Jonathan L. Finlay, Nada Jabado, Maria Isabel Achatz, Stefan M. Pfister, Rishi Lulla, Eugene I. Hwang, Brent T. Harris, Myran Ben-Arush, Rina Dvir, Sanaa Choufani, Ana Novokmet, Ruth Tatevossian, David Shih, Vijay Ramaswamy, Stephen Mack, Malgorzata Pienkowska, Anita Villani, Adam Shlien, and Diana M. Merino

Abstract

supplemental figure and table legend

Published

2023

27. Data from Molecular Characterization of Choroid Plexus Tumors Reveals Novel Clinically Relevant Subgroups

Author

David Malkin, Richard J. Gilbertson, David W. Ellison, Uri Tabori, Michael D. Taylor, Cynthia Hawkins, Eric Bouffet, Rosanna Weksberg, Jonathan L. Finlay, Nada Jabado, Maria Isabel Achatz, Stefan M. Pfister, Rishi Lulla, Eugene I. Hwang, Brent T. Harris, Myran Ben-Arush, Rina Dvir, Sanaa Choufani, Ana Novokmet, Ruth Tatevossian, David Shih, Vijay Ramaswamy, Stephen Mack, Malgorzata Pienkowska, Anita Villani, Adam Shlien, and Diana M. Merino

Abstract

Purpose: To investigate molecular alterations in choroid plexus tumors (CPT) using a genome-wide high-throughput approach to identify diagnostic and prognostic signatures that will refine tumor stratification and guide therapeutic options.Experimental Design: One hundred CPTs were obtained from a multi-institutional tissue and clinical database. Copy-number (CN), DNA methylation, and gene expression signatures were assessed for 74, 36, and 40 samples, respectively. Molecular subgroups were correlated with clinical parameters and outcomes.Results: Unique molecular signatures distinguished choroid plexus carcinomas (CPC) from choroid plexus papillomas (CPP) and atypical choroid plexus papillomas (aCPP); however, no significantly distinct molecular alterations between CPPs and aCPPs were observed. Allele-specific CN analysis of CPCs revealed two novel subgroups according to DNA content: hypodiploid and hyperdiploid CPCs. Hyperdiploid CPCs exhibited recurrent acquired uniparental disomy events. Somatic mutations in TP53 were observed in 60% of CPCs. Investigating the number of mutated copies of p53 per sample revealed a high-risk group of patients with CPC carrying two copies of mutant p53, who exhibited poor 5-year event-free (EFS) and overall survival (OS) compared with patients with CPC carrying one copy of mutant p53 (OS: 14.3%, 95% confidence interval, 0.71%–46.5% vs. 66.7%, 28.2%–87.8%, respectively, P = 0.04; EFS: 0% vs. 44.4%, 13.6%–71.9%, respectively, P = 0.03). CPPs and aCPPs exhibited favorable survival.Discussion: Our data demonstrate that differences in CN, gene expression, and DNA methylation signatures distinguish CPCs from CPPs and aCPPs; however, molecular similarities among the papillomas suggest that these two histologic subgroups are indeed a single molecular entity. A greater number of copies of mutated TP53 were significantly associated to increased tumor aggressiveness and a worse survival outcome in CPCs. Collectively, these findings will facilitate stratified approaches to the clinical management of CPTs. Clin Cancer Res; 21(1); 184–92. ©2014 AACR.

Published

2023

28. Germline TP53 mutations undergo copy number gain years prior to tumor diagnosis

Author

Nicholas Light, Mehdi Layeghifard, Ayush Attery, Vallijah Subasri, Matthew Zatzman, Nathaniel D. Anderson, Rupal Hatkar, Sasha Blay, David Chen, Ana Novokmet, Fabio Fuligni, James Tran, Richard de Borja, Himanshi Agarwal, Larissa Waldman, Lisa M. Abegglen, Daniel Albertson, Jonathan L. Finlay, Jordan R. Hansford, Sam Behjati, Anita Villani, Moritz Gerstung, Ludmil B. Alexandrov, Gino R. Somers, Joshua D. Schiffman, Varda Rotter, David Malkin, Adam Shlien, Layeghifard, Mehdi [0000-0002-6224-3628], Subasri, Vallijah [0000-0002-6584-877X], Anderson, Nathaniel D [0000-0003-4523-6327], Blay, Sasha [0000-0002-5611-2330], Agarwal, Himanshi [0000-0003-1738-4525], Abegglen, Lisa M [0000-0003-3607-3001], Hansford, Jordan R [0000-0001-7733-383X], Behjati, Sam [0000-0002-6600-7665], Gerstung, Moritz [0000-0001-6709-963X], Alexandrov, Ludmil B [0000-0003-3596-4515], Schiffman, Joshua D [0000-0002-6968-7694], Malkin, David [0000-0001-5752-9763], Shlien, Adam [0000-0002-0368-5370], and Apollo - University of Cambridge Repository

Subjects

Multidisciplinary, DNA Copy Number Variations, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology, Li-Fraumeni Syndrome, Phosphatidylinositol 3-Kinases, Neoplastic Syndromes, Hereditary, Mutation, Humans, Genetic Predisposition to Disease, Tumor Suppressor Protein p53, Phylogeny, Germ-Line Mutation

Abstract

Li-Fraumeni syndrome (LFS) is a hereditary cancer predisposition syndrome associated with germline TP53 pathogenic variants. Here, we perform whole-genome sequence (WGS) analysis of tumors from 22 patients with TP53 germline pathogenic variants. We observe somatic mutations affecting Wnt, PI3K/AKT signaling, epigenetic modifiers and homologous recombination genes as well as mutational signatures associated with prior chemotherapy. We identify near-ubiquitous early loss of heterozygosity of TP53, with gain of the mutant allele. This occurs earlier in these tumors compared to tumors with somatic TP53 mutations, suggesting the timing of this mark may distinguish germline from somatic TP53 mutations. Phylogenetic trees of tumor evolution, reconstructed from bulk and multi-region WGS, reveal that LFS tumors exhibit comparatively limited heterogeneity. Overall, our study delineates early copy number gains of mutant TP53 as a characteristic mutational process in LFS tumorigenesis, likely arising years prior to tumor diagnosis.

Published

2023

29. Outcomes of Infants and Young Children With Relapsed Medulloblastoma After Initial Craniospinal Irradiation-Sparing Approaches : An International Cohort Study

Author

Craig Erker, Martin Mynarek, Simon Bailey, Claire M. Mazewski, Lorena Baroni, Maura Massimino, Juliette Hukin, Dolly Aguilera, Andrea M. Cappellano, Vijay Ramaswamy, Alvaro Lassaletta, Sébastien Perreault, Cassie N. Kline, Revathi Rajagopal, George Michaiel, Michal Zapotocky, Vicente Santa-Maria Lopez, Andres Morales La Madrid, Chantel Cacciotti, Eric S. Sandler, Lindsey M. Hoffman, Darren Klawinski, Sara Khan, Ralph Salloum, Anna L. Hoppmann, Valérie Larouche, Kathleen Dorris, Helen Toledano, Stephen W. Gilheeney, Mohamed S. Abdelbaki, Beverly Wilson, Derek S. Tsang, Jeffrey Knipstein, Michal Yalon Oren, Shafqat Shah, Jeffrey C. Murray, Kevin F. Ginn, Zhihong J. Wang, Gudrun Fleischhack, Denise Obrecht, Svenja Tonn, Virginia L. Harrod, Kara Matheson, Bruce Crooks, Douglas R. Strother, Kenneth J. Cohen, Jordan R. Hansford, Sabine Mueller, Ashley Margol, Amar Gajjar, Girish Dhall, Jonathan L. Finlay, Paul A. Northcott, Stefan Rutkowski, Steven C. Clifford, Giles Robinson, Eric Bouffet, and Lucie Lafay-Cousin

Subjects

Cancer Research, Oncology, Medizin

Abstract

PURPOSE Infant and young childhood medulloblastoma (iMB) is usually treated without craniospinal irradiation (CSI) to avoid neurocognitive late effects. Unfortunately, many children relapse. The purpose of this study was to assess salvage strategies and prognostic features of patients with iMB who relapse after CSI-sparing therapy. METHODS We assembled a large international cohort of 380 patients with relapsed iMB, age younger than 6 years, and initially treated without CSI. Univariable and multivariable Cox models of postrelapse survival (PRS) were conducted for those treated with curative intent using propensity score analyses to account for confounding factors. RESULTS The 3-year PRS, for 294 patients treated with curative intent, was 52.4% (95% CI, 46.4 to 58.3) with a median time to relapse from diagnosis of 11 months. Molecular subgrouping was available for 150 patients treated with curative intent, and 3-year PRS for sonic hedgehog (SHH), group 4, and group 3 were 60%, 84%, and 18% ( P = .0187), respectively. In multivariable analysis, localized relapse ( P = .0073), SHH molecular subgroup ( P = .0103), CSI use after relapse ( P = .0161), and age ≥ 36 months at initial diagnosis ( P = .0494) were associated with improved survival. Most patients (73%) received salvage CSI, and although salvage chemotherapy was not significant in multivariable analysis, its use might be beneficial for a subset of children receiving salvage CSI < 35 Gy ( P = .007). CONCLUSION A substantial proportion of patients with relapsed iMB are salvaged after initial CSI-sparing approaches. Patients with SHH subgroup, localized relapse, older age at initial diagnosis, and those receiving salvage CSI show improved PRS. Future prospective studies should investigate optimal CSI doses and the role of salvage chemotherapy in this population.

Published

2023

30. Evaluation of the Pediatric Neuro-Oncology Resources Available in Chile

Author

Nicolás Rojas del Río, Alvaro Lassaletta, Ibrahim Qaddoumi, Felipe Espinoza, José Santander, Katherine Kopp, Juan Tordecilla, Andres Morales La Madrid, Scott L. Coven, Ximena Espinoza, Eduardo Fernandez, Miguel Valero, Jonathan L. Finlay, Diana S Osorio, Verónica Pérez, Rosa Moreno, Ute Bartels, Veronica Oyarce, Adrián Cáceres, Mauricio Reyes, and Mohammad H Abu-Arja

Subjects

Cancer Research, business.industry, Hematopoietic Stem Cell Transplantation, MEDLINE, ORIGINAL REPORTS, Medical Oncology, medicine.disease, Central Nervous System Neoplasms, 03 medical and health sciences, Cross-Sectional Studies, 0302 clinical medicine, Oncology, Pediatric Oncology, Pediatric Neuro-Oncology, 030225 pediatrics, 030220 oncology & carcinogenesis, Material resources, Humans, Medicine, Medical emergency, Chile, Child, business

Abstract

PURPOSE Pediatric neuro-oncology resources are mostly unknown in Chile. We report the human and material resources available in Chilean hospitals providing pediatric neuro-oncology services. METHODS A cross-sectional survey was distributed to 17 hospitals providing pediatric neuro-oncology services (Programa Infantil Nacional de Drogas Antineoplásicas [PINDA] hospitals, 11; private, 6). RESULTS Response rate was 71% (PINDA, 8; private, 4). Pediatric neuro-oncology services were mainly provided within general hospitals (67%). Registries for pediatric CNS tumors and chemotherapy-related toxicities were available in 100% and 67% of hospitals, respectively. CNS tumors were treated by pediatric oncologists in 92% of hospitals; none were formally trained in neuro-oncology. The most used treatment protocols were the national PINDA protocols. All WHO essential medicines for childhood cancer were available in more than 80% of the hospitals except for gemcitabine, oxaliplatin, paclitaxel, and procarbazine. The median number of pediatric neurosurgeons per hospital was two (range, 2-6). General neuroradiologists were available in 83% of the centers. Pathology specimens were sent to neuropathologists (58%), adult pathologists (25%), and pediatric pathologists (17%). Intensity-modulated radiotherapy, conformal radiotherapy, and cobalt radiotherapy were used by 67%, 58%, and 42% of hospitals, respectively. Only one private hospital performed autologous hematopoietic cell transplant for children with CNS tumors. CONCLUSION A wide range of up-to-date treatment modalities are available for children with CNS tumors. Our survey highlights future directions to improve the pediatric neuro-oncology services available in Chile such as the expansion of multidisciplinary clinics, palliative care services, long-term cancer survivorship programs, dedicated clinical research support teams, establishing standardized mechanism for sending pathologic specimen for second opinion to international specialized centers, and establishing specialized neuro-oncology training program.

Published

2021

31. STAT3 inhibitor in combination with irradiation significantly inhibits cell viability, cell migration, invasion and tumorsphere growth of human medulloblastoma cells

Author

Li Pan, Jonathan L. Finlay, Ruijie Zhang, Ling Ma, Jiayuh Lin, Christopher R. Pierson, and Chenglong Li

Subjects

STAT3 Transcription Factor, Cancer Research, Cell Survival, Apoptosis, Stat3 inhibitor, Cell Movement, Cell Line, Tumor, medicine, Humans, Viability assay, Cerebellar Neoplasms, STAT3, Pharmacology, Medulloblastoma, biology, Chemistry, Cell migration, medicine.disease, Oncology, Tumor progression, Cancer research, STAT protein, biology.protein, Molecular Medicine, Research Paper

Abstract

Persistent activation of signal transducer and activator of transcription 3 (STAT3) is frequently reported in cancers and plays important roles in tumor progression. Therefore, directly targeting persistent STAT3 signaling is an attractive cancer therapeutic strategy. The aim of this study is to test the inhibitory efficacy of novel STAT3 small molecule inhibitors, LLY17 and LLL12B, in combination with irradiation in human medulloblastoma cells. Both LLY17 and LLL12B inhibit the IL-6-induced and persistent STAT3 phosphorylation in human medulloblastoma cells. Irradiation using 4 Gy alone exhibits some inhibitory effects on medulloblastoma cell viability, and these effects are further enhanced by combining with either STAT3 inhibitor. Irradiation alone also shows certain inhibitory effects on medulloblastoma cell migration and invasion and the combination of LLY17 or LLL12B with irradiation further demonstrates greater inhibitory effects than monotherapy. STAT3 inhibitor alone or irradiation alone exhibits some suppression of medulloblastoma tumorsphere growth, and the combination of LLY17 or LLL12B and irradiation exhibits greater suppression of tumorsphere growth than monotherapy. Combining either STAT3 inhibitor with irradiation reduces the expression of STAT3 downstream targets, Cyclin D1 and Survivin, and induces apoptosis in medulloblastoma cells. These results support that combination of a potent STAT3 inhibitor such as LLY17 or LLL12B with irradiation is an effective and novel therapeutic approach for medulloblastoma.

Published

2021

32. Infantile metastatic ependymoma with a novel molecular profile and favorable outcome to intensive chemotherapy without irradiation: Case-based review

Author

Flavia Watusi De Faria, Kathleen M. Schieffer, Christopher R. Pierson, Daniel R. Boue, Stephanie LaHaye, Katherine E. Miller, Nisreen Amayiri, Daniel C. Koboldt, Tara Lichtenberg, Kristen Leraas, Patrick Brennan, Ben Kelly, Peter White, Vincent Magrini, Richard K. Wilson, Elaine R. Mardis, Catherine E. Cottrell, Jerome Rusin, Jonathan L. Finlay, and Diana S. Osorio

Subjects

Male, Cancer Research, Adolescent, Ependymoma, Brain Neoplasms, Child, Preschool, Genetics, Hematopoietic Stem Cell Transplantation, Humans, Infant, Neoplasm Recurrence, Local, Child

Abstract

Ependymal tumors are the third most common brain tumor under 14 years old. Even though metastatic disease is a rare event, it affects mostly young children and carries an adverse prognosis. The factors associated with dissemination and the best treatment approach have not yet been established and there is limited published data on how to manage metastatic disease, especially in patients under 3 years of age. We provide a review of the literature on clinical characteristics and radiation-sparing treatments for metastatic ependymoma in children under 3 years of age treated. The majority (73%) of the identified cases were above 12 months old and had the PF as the primary site at diagnosis. Chemotherapy-based approaches, in different regimens, were used with radiation reserved for progression or relapse. The prognosis varied among the studies, with an average of 50%-58% overall survival. This study also describes the case of a 7-month-old boy with metastatic posterior fossa (PF) ependymoma, for whom we identified a novel SPECC1L-RAF1 gene fusion using a patient-centric comprehensive molecular profiling protocol. The patient was successfully treated with intensive induction chemotherapy followed by high-dose chemotherapy and autologous hematopoietic progenitor cell rescue (AuHSCR). Currently, the patient is in continuous remission 5 years after his diagnosis, without radiation therapy. The understanding of the available therapeutic approaches may assist physicians in their management of such patients. This report also opens the perspective of newly identified molecular alterations in metastatic ependymomas that might drive more chemo-sensitive tumors.

Published

2022

33. Long-term neuropsychological outcomes of survivors of young childhood brain tumors treated on the Head Start II protocol

Author

Cara F Levitch, Whitney Guerry, Sharon Gardner, Jonathan L. Finlay, Stephen A. Sands, Benjamin Malkin, and Lauren Latella

Subjects

Pediatrics, medicine.medical_specialty, business.industry, medicine.medical_treatment, Neuropsychology, Medicine (miscellaneous), Original Articles, Chemotherapy regimen, Radiation therapy, Transplantation, 03 medical and health sciences, 0302 clinical medicine, Borderline intellectual functioning, 030220 oncology & carcinogenesis, Head start, Cohort, medicine, business, Neurocognitive, 030217 neurology & neurosurgery

Abstract

Background The Head Start treatment protocols have focused on curing young children with brain tumors while avoiding or delaying radiotherapy through using a combination of high-dose, marrow-ablative chemotherapy and autologous hematopoietic cell transplantation (AuHCT). Late effects data from treatment on the Head Start II (HS II) protocol have previously been published for short-term follow-up (STF) at a mean of 39.7 months post-diagnosis. The current study examines long-term follow-up (LTF) outcomes from the same cohort. Methods Eighteen HS II patients diagnosed with malignant brain tumors Results There was no significant change in Full Scale IQ at LTF compared to baseline or STF. Similarly, most domains had no significant change from STF, including verbal IQ, performance IQ, academics, receptive language, learning/memory, visual-motor integration, and externalizing behaviors. Internalizing behaviors increased slightly at LTF. Clinically, most domains were within the average range, except for low average mathematics and receptive language. Additionally, performance did not significantly differ by age at diagnosis or time since diagnosis. Of note, children treated with high-dose methotrexate for disseminated disease or atypical teratoid/rhabdoid tumor displayed worse neurocognitive outcomes. Conclusions These results extend prior findings of relative stability in intellectual functioning for a LTF period. Ultimately, this study supports that treatment strategies for avoiding or delaying radiotherapy using high-dose, marrow-ablative chemotherapy and AuHCT may decrease the risk of neurocognitive and social-emotional declines in young pediatric brain tumor survivors.

Published

2021

34. Recurrent Wnt medulloblastoma treated with marrow-ablative chemotherapy and autologous hematopoietic progenitor cell rescue: a dual case report and review of the literature

Author

Micah K. Harris, Jonathan L. Finlay, Margaret Shatara, Zachary Funk, Daniel R. Boue, Joseph Stanek, Jeremy Jones, and Mohamed S. AbdelBaki

Subjects

Medulloblastoma, Oncology, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, Cell, Wnt signaling pathway, General Medicine, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Hematopoietic progenitor, 030220 oncology & carcinogenesis, Internal medicine, Pediatrics, Perinatology and Child Health, Ablative case, medicine, Treatment strategy, Neurology (clinical), Neurosurgery, business, 030217 neurology & neurosurgery

Abstract

Wnt-activated medulloblastoma (MB) confers an excellent prognosis. However, specific treatment strategies for patients with relapsed Wnt-MB are unknown. We report two patients with recurrent beta-catenin nucleopositive Wnt-MB successfully treated by incorporating marrow-ablative chemotherapy and autologous hematopoietic progenitor cell rescue (HDCx/AuHPCR). We also present a review of the literature for previously reported cases of relapsed Wnt-MB. We propose that patients with recurrent Wnt-MB may be treated using a multi-disciplinary approach that includes HDCx/AuHPCR with or without re-irradiation.

Published

2021

35. LLL12B, a small molecule STAT3 inhibitor, induces growth arrest, apoptosis, and enhances cisplatin-mediated cytotoxicity in medulloblastoma cells

Author

Shengling Fu, Ruijie Zhang, Jiayuh Lin, Jinhua Song, Jia Wei, Li Pan, Jonathan L. Finlay, Chenglong Li, Xiang Chen, Christopher R. Pierson, Ren Yuan Bai, and Xiaozhi Yang

Subjects

STAT3 Transcription Factor, Cancer therapy, Carcinogenesis, Cell Survival, Science, Anthraquinones, Apoptosis, Article, Interferon-gamma, Mice, Cell Movement, In vivo, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Viability assay, STAT1, Phosphorylation, STAT3, Cancer, Cell Proliferation, Medulloblastoma, Cisplatin, Sulfonamides, Multidisciplinary, Oncogene, biology, Interleukin-6, Chemistry, medicine.disease, nervous system diseases, CNS cancer, stomatognathic diseases, STAT1 Transcription Factor, Tumor progression, Cancer research, biology.protein, Heterografts, Medicine, medicine.drug

Abstract

Signal Transducer and Activator of Transcription 3 (STAT3) is a transcription factor and an oncogene product, which plays a pivotal role in tumor progression. Therefore, targeting persistent STAT3 signaling directly is an attractive anticancer strategy. The aim of this study is to test the efficacy of a novel STAT3 small molecule inhibitor, LLL12B, in suppressing medulloblastoma cells in vitro and tumor growth in vivo. LLL12B selectively inhibited the induction of STAT3 phosphorylation by interleukin-6 but not induction of STAT1 phosphorylation by INF-γ. LLL12B also induced apoptosis in human medulloblastoma cells. In addition, LLL12B exhibited good oral bioavailability in vivo and potent suppressive activity in tumor growth of medulloblastoma cells in vivo. Besides, combining LLL12B with cisplatin showed greater inhibition of cell viability and tumorsphere formation as well as induction of apoptosis comparing to single agent treatment in medulloblastoma cells. Furthermore, LLL12B and cisplatin combination exhibited greater suppression of medulloblastoma tumor growth than monotherapy in vivo. The present study supported that LLL12B is a novel therapeutic agent for medulloblastoma and the combination of LLL12B with a chemotherapeutic agent cisplatin may be an effective approach for medulloblastoma therapy.

Published

2021

36. Factors influencing outcomes of older children with medulloblastoma over 15 years in Peru, a resource‐limited setting

Author

Rosdali Y. Diaz‐Coronado, James Brandon Reinecke, Joseph R. Stanek, Jonathan L. Finlay, Eddy Hernández Broncano, Sharon Chávez Paredes, Yesenia Miranda Tunque, Adela Heredia Zelaya, Sandro Casavilca Zambrano, Pamela García‐Corrochano Medina, Luis Ojeda Medina, Enrique Orrego Puelles, Ebert Torres Malca, Raymundo Sernaque Quintana, William Quispe Valverde, Juan L. García León, and Diana S. Osorio

Subjects

Adolescent, Brain Neoplasms, Hematology, Prognosis, Disease-Free Survival, Oncology, Risk Factors, Child, Preschool, Peru, Pediatrics, Perinatology and Child Health, Humans, Cerebellar Neoplasms, Child, Medulloblastoma

Abstract

Medulloblastoma is the most common malignant brain tumor in children. While survival has improved in high-income countries (HIC), the outcomes for patients in low-to-middle-income countries (LMIC) are unclear. Therefore, we sought to determine the survival of children with medulloblastoma at the Instituto Nacional de Enfermedades Neoplasicas (INEN) between 1997 and 2013 in Peru.Between 1997 and 2013, data from 103 children older than 3 years with medulloblastoma were analyzed. Fourteen patients were excluded. The patients were split into two distinct cohorts, 1997-2008 and 2009-2013, corresponding with chemotherapy regimen changes. Event-free (EFS) and overall survival (OS) were calculated using the Kaplan-Meier method, whereas prognostic factors were determined by univariate analysis (log-rank test).Eighty-nine patients were included; median age was 8.1 years (range: 3-13.9 years). The 5-year OS was 62% (95% CI: 53%-74%), while EFS was 57% (95% CI: 48%-69%). The variables adversely affecting survival were anaplastic histology (compared to desmoplastic; OS: HR = 3.4, p = .03), metastasis (OS: HR = 3.5, p = .01; EFS: HR = 4.3, p = .004), delay in radiation therapy of 31-60 days (compared to ≤30 days; EFS: HR = 2.1, p = .04), and treatment 2009-2013 cohort (OS: HR = 2.2, p = .02; EFS: HR = 2.0, p = .03).Outcomes for medulloblastoma at INEN were low compared with HIC. Anaplastic subtype, metastasis at diagnosis, delay in radiation therapy, and treatment in the period 2009-2013 negatively affected the outcomes in our study. Multidisciplinary teamwork, timely delivery of treatment, and partnerships with loco-regional groups and colleagues in HIC is likely beneficial.

Published

2022

37. Meta-Analysis of Treatment Modalities in Metastatic Atypical Teratoid/Rhabdoid Tumors in Children

Author

Mostafa Eltobgy, Reena M. Underiner, Jonathan L. Finlay, Mohamed S. AbdelBaki, and Joseph Stanek

Subjects

Male, Oncology, medicine.medical_specialty, medicine.medical_treatment, Antineoplastic Agents, Neurosurgical Procedures, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Developmental Neuroscience, 030225 pediatrics, Internal medicine, medicine, Humans, Progression-free survival, Stage (cooking), Rhabdoid Tumor, Univariate analysis, Radiotherapy, Brain Neoplasms, business.industry, Hazard ratio, Hematopoietic Stem Cell Transplantation, Teratoma, Infant, medicine.disease, Combined Modality Therapy, Primary tumor, Radiation therapy, Outcome and Process Assessment, Health Care, Neurology, Child, Preschool, Pediatrics, Perinatology and Child Health, Atypical teratoid rhabdoid tumor, Female, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Metastatic atypical teratoid/rhabdoid tumors (AT/RTs) are aggressive central nervous system tumors that present during infancy and are associated with dismal outcomes. Patients receive multimodal treatment including surgical resection, systemic chemotherapy, and one or more of intrathecal chemotherapy (IT), marrow-ablative chemotherapy with autologous hematopoietic cell rescue (AuHCR) and radiation therapy (XRT). While data regarding treatment modalities for AT/RT patients exist, no comprehensive data have been published regarding the metastatic patients.We performed a meta-analysis of 1578 articles published through September 2018, including 44 studies with a total of 123 subjects. In addition, seven patients were included through chart review of patients treated at Nationwide Children's Hospital.Analysis of 130 patients revealed a 3-year overall survival (OS) of 25%. Age at diagnosis had a significant effect on survival (P = 0.0355); 3-year OS for infants less than 18 months was 21%, 18 to 36 months was 26%, and greater than 36 months was 36%. Location of the primary tumor, metastatic stage, and extent of surgical resection did not have a significant impact on OS. On univariate analysis, XRT (P0.0001), IT (P = 0.01), and AuHCR (P0.0001) were found to significantly improve survival. The most substantial effect was noted in patients who received AuHCR (3-year OS of 60% vs 9% in those who did not). On multivariable analysis, XRT (P = 0.0006), IT (P = 0.0124), and AuHCR (P0.0001) were independently associated with reduced risk of death.Although more research is warranted to make generalizable conclusions, these results suggest that treatment regimens for patients with metastatic AT/RTs should include AuHCR, XRT, and IT.

Published

2020

38. EANO, SNO and Euracan consensus review on the current management and future development of intracranial germ cell tumors in adolescents and young adults

Author

Thomas Czech, Mark M. Souweidane, D Haas-Kogen, Alexandre Vasiljevic, P Wen, C Faure Conter, Eric Bouffet, Jonathan L. Finlay, D. Frappaz, Matthew J. Murray, RD Kortmann, Ute Bartels, Dennis W. W. Shaw, Ching C. Lau, David Schiff, S Schöenberger, Jeffrey C. Allen, Girish Dhall, James Nicholson, P Robertson, Gabriele Calaminus, Claire Alapetite, Giovanni Morana, A Albanese, Stewart Goldman, Murray, Matthew J [0000-0002-4480-1147], Bartels, Ute [0000-0003-2112-5251], Albanese, Assunta [0000-0003-4051-6661], Czech, Thomas [0000-0001-8112-2795], Bouffet, Eric [0000-0002-6832-6539], and Apollo - University of Cambridge Repository

Subjects

Male, Cancer Research, medicine.medical_specialty, Consensus, Adolescent, medicine.medical_treatment, Medizin, germinoma, Disease, Craniospinal Irradiation, Young Adult, Testicular Neoplasms, Medicine, Humans, Young adult, Radical surgery, Retrospective Studies, non-germinomatous germ cell tumor, Chemotherapy, Germinoma, adolescents and young adults, brain tumors, germ cell tumor, business.industry, Brain Neoplasms, Neoplasms, Germ Cell and Embryonal, medicine.disease, Radiation therapy, Oncology, Neurology (clinical), Germ cell tumors, Radiology, business

Abstract

The incidence of intracranial germ cell tumors (iGCT) is much lower in European and North American (E&NA) than in Asian population. However, E&NA cooperative groups have simultaneously developed with success treatment strategies with specific attention paid to long-term sequelae. Neurological sequelae may be reduced by establishing a diagnosis with an endoscopic biopsy and/or cerebrospinal fluid (CSF) and/or serum analysis, deferring the need to perform a radical surgery. Depending on markers and/or histological characteristics, patients are treated as either germinoma or non-germinomatous germ cell tumors (NGGCT). Metastatic disease is defined by a positive CSF cytology and/or distant drops in craniospinal MRI. The combination of surgery and/or chemotherapy and radiation therapy is tailored according to grouping and staging. With more than 90% 5-year event-free survival (EFS), localized germinomas can be managed without aggressive surgery, and benefit from chemotherapy followed by whole ventricular irradiation with local boost. Bifocal germinomas are treated as non-metastatic entities. Metastatic germinomas may be cured with craniospinal irradiation. With a 5-year EFS over 70%, NGGCT benefit from chemotherapy followed by delayed surgery in case of residual disease, and some form of radiotherapy. Future strategies will aim at decreasing long-term side effects while preserving high cure rates.

Published

2022

39. Discovery of clinically relevant fusions in pediatric cancer

Author

Stephanie LaHaye, James R. Fitch, Kyle J. Voytovich, Adam C. Herman, Benjamin J. Kelly, Grant E. Lammi, Jeremy A. Arbesfeld, Saranga Wijeratne, Samuel J. Franklin, Kathleen M. Schieffer, Natalie Bir, Sean D. McGrath, Anthony R. Miller, Amy Wetzel, Katherine E. Miller, Tracy A. Bedrosian, Kristen Leraas, Elizabeth A. Varga, Kristy Lee, Ajay Gupta, Bhuvana Setty, Daniel R. Boué, Jeffrey R. Leonard, Jonathan L. Finlay, Mohamed S. Abdelbaki, Diana S. Osorio, Selene C. Koo, Daniel C. Koboldt, Alex H. Wagner, Ann-Kathrin Eisfeld, Krzysztof Mrózek, Vincent Magrini, Catherine E. Cottrell, Elaine R. Mardis, Richard K. Wilson, and Peter White

Subjects

Pediatric neoplasms, Genome, Gene fusions, Sequence Analysis, RNA, Methodology Article, Genomics, Sequence Analysis, DNA, QH426-470, Neoplasms, Genetics, Humans, RNA-Seq, Transcriptomics, Child, TP248.13-248.65, Biotechnology, Cancer

Abstract

Background Pediatric cancers typically have a distinct genomic landscape when compared to adult cancers and frequently carry somatic gene fusion events that alter gene expression and drive tumorigenesis. Sensitive and specific detection of gene fusions through the analysis of next-generation-based RNA sequencing (RNA-Seq) data is computationally challenging and may be confounded by low tumor cellularity or underlying genomic complexity. Furthermore, numerous computational tools are available to identify fusions from supporting RNA-Seq reads, yet each algorithm demonstrates unique variability in sensitivity and precision, and no clearly superior approach currently exists. To overcome these challenges, we have developed an ensemble fusion calling approach to increase the accuracy of identifying fusions. Results Our Ensemble Fusion (EnFusion) approach utilizes seven fusion calling algorithms: Arriba, CICERO, FusionMap, FusionCatcher, JAFFA, MapSplice, and STAR-Fusion, which are packaged as a fully automated pipeline using Docker and Amazon Web Services (AWS) serverless technology. This method uses paired end RNA-Seq sequence reads as input, and the output from each algorithm is examined to identify fusions detected by a consensus of at least three algorithms. These consensus fusion results are filtered by comparison to an internal database to remove likely artifactual fusions occurring at high frequencies in our internal cohort, while a “known fusion list” prevents failure to report known pathogenic events. We have employed the EnFusion pipeline on RNA-Seq data from 229 patients with pediatric cancer or blood disorders studied under an IRB-approved protocol. The samples consist of 138 central nervous system tumors, 73 solid tumors, and 18 hematologic malignancies or disorders. The combination of an ensemble fusion-calling pipeline and a knowledge-based filtering strategy identified 67 clinically relevant fusions among our cohort (diagnostic yield of 29.3%), including RBPMS-MET, BCAN-NTRK1, and TRIM22-BRAF fusions. Following clinical confirmation and reporting in the patient’s medical record, both known and novel fusions provided medically meaningful information. Conclusions The EnFusion pipeline offers a streamlined approach to discover fusions in cancer, at higher levels of sensitivity and accuracy than single algorithm methods. Furthermore, this method accurately identifies driver fusions in pediatric cancer, providing clinical impact by contributing evidence to diagnosis and, when appropriate, indicating targeted therapies.

Published

2021

40. Epidemiological characteristics and survival outcomes of children with medulloblastoma treated at the National Cancer Institute (INCA) in Rio de Janeiro, Brazil

Author

Diana S Osorio, Joseph Stanek, Marcio de Miranda Chaves Christiani, Antonio Aversa, Sima Ferman, Denizar Vianna, Denise Maria Araújo Magalhães, Gabriela Oigman, and Jonathan L. Finlay

Subjects

Male, Pediatrics, medicine.medical_specialty, Nausea, medicine.medical_treatment, Disease, Disease-Free Survival, Health care, Epidemiology, medicine, Humans, Cerebellar Neoplasms, Child, Survival analysis, Retrospective Studies, Medulloblastoma, business.industry, Medical record, Cancer, Hematology, medicine.disease, Radiation therapy, Malnutrition, Treatment Outcome, Oncology, Pediatrics, Perinatology and Child Health, Vomiting, Female, medicine.symptom, business, Brazil

Abstract

BACKGROUND: Medulloblastoma (MB), the most malignant brain tumor of childhood has survival outcomes exceeding 80% for standard risk and 60% for high risk patients in high-income countries (HIC). These results have not been replicated in low-to-middle income countries (LMIC), where 80% of children with cancer live. METHODS: Retrospective review of 114 children (3-18 years) diagnosed with MB from 1997 to 2016 at INCA. Data on patients, disease characteristics and treatment information were retrieved from the charts and summarized descriptively. Overall survival (OS) and event-free survival (EFS) were calculated using the Kaplan-Meier Method. RESULTS: The male/female ratio was 1.32 and the median age at diagnosis was 8.2 years. Headache (83%) and nausea/vomiting (78%) were the most common presenting symptoms. Overall survival (5y) was 59,1% and EFS (5y) was 58,4%. The OS for standard-risk patients was 69% and 53% for high-risk patients. Forty-five patients (35%) had metastatic disease at admission. Lower maternal education correlated with lower OS (71.3% versus 49% p=0.25). Patients who lived >40km from INCA fared better (OS= 68.2% versus 51.1% p=0.032). Almost 20% of families lived below the Brazilian minimum wage. CONCLUSIONS: The epidemiological characteristics of this series possibly explain the differences in survival that medulloblastoma patients have in Brazil. Issues related to limited health care resources, poverty, delayed diagnosis, treatment abandonment, and malnutrition are reflected in inferior survival outcomes when compared to high-income countries. Despite the difficulties encountered in an upper-middle income country, it was possible to deliver treatment with good results.

Published

2021

41. Clinically aggressive pediatric spinal ependymoma with novel MYC amplification demonstrates molecular and histopathologic similarity to newly described MYCN-amplified spinal ependymomas

Author

Margaret Shatara, Kathleen M. Schieffer, Darren Klawinski, Diana L. Thomas, Christopher R. Pierson, Eric A. Sribnick, Jeremy Jones, Diana P. Rodriguez, Carol Deeg, Elizabeth Hamelberg, Stephanie LaHaye, Katherine E. Miller, James Fitch, Benjamin Kelly, Kristen Leraas, Ruthann Pfau, Peter White, Vincent Magrini, Richard K. Wilson, Elaine R. Mardis, Mohamed S. Abdelbaki, Jonathan L. Finlay, Daniel R. Boué, Catherine E. Cottrell, David R. Ghasemi, Kristian W. Pajtler, and Diana S. Osorio

Subjects

Male, Pediatric, N-Myc Proto-Oncogene Protein, Spinal Neoplasms, Spinal, Amplification, Case Report, MYC, DNA methylation array, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, FISH, Ependymoma, MYCN, Humans, Neurology. Diseases of the nervous system, Neurology (clinical), Spinal Cord Neoplasms, RC346-429, Child

Abstract

Primary spinal cord tumors contribute to ≤ 10% of central nervous system tumors in individuals of pediatric or adolescent age. Among intramedullary tumors, spinal ependymomas make up ~ 30% of this rare tumor population. A twelve-year-old male presented with an intradural, extramedullary mass occupying the dorsal spinal canal from C6 through T2. Gross total resection and histopathology revealed a World Health Organization (WHO) grade 2 ependymoma. He recurred eleven months later with extension from C2 through T1-T2. Subtotal resection was achieved followed by focal proton beam irradiation and chemotherapy. Histopathology was consistent with WHO grade 3 ependymoma. Molecular profiling of the primary and recurrent tumors revealed a novel amplification of the MYC (8q24) gene, which was confirmed by fluorescence in situ hybridization studies. Although MYC amplification in spinal ependymoma is exceedingly rare, a newly described classification of spinal ependymoma harboring MYCN (2p24) amplification (SP-MYCN) has been defined by DNA methylation-array based profiling. These individuals typically present with a malignant progression and dismal outcomes, contrary to the universally excellent survival outcomes seen in other spinal ependymomas. DNA methylation array-based classification confidently classified this tumor as SP-MYCN ependymoma. Notably, among the cohort of 52 tumors comprising the SP-MYCN methylation class, none harbor MYC amplification, highlighting the rarity of this genomic amplification in spinal ependymoma. A literature review comparing our individual to reported SP-MYCN tumors (n = 26) revealed similarities in clinical, histopathologic, and molecular features. Thus, we provide evidence from a single case to support the inclusion of MYC amplified spinal ependymoma within the molecular subgroup of SP-MYCN.

Published

2021

42. Prognostic factors for patients with relapsed central nervous system nongerminomatous germ cell tumors

Author

Scott L. Coven, Diana S Osorio, Jonathan L. Finlay, Richard T Graham, Mohamed S. AbdelBaki, Mohammad H Abu-Arja, Eric Bouffet, Alvaro Lassaletta, and Joseph Stanek

Subjects

Central Nervous System, medicine.medical_specialty, End of therapy, medicine.medical_treatment, Central nervous system, Gastroenterology, Central Nervous System Neoplasms, Cerebrospinal fluid, Testicular Neoplasms, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Complete response, Continued Complete Response, Chemotherapy, business.industry, Hematology, Neoplasms, Germ Cell and Embryonal, Prognosis, medicine.disease, Combined Modality Therapy, Radiation therapy, medicine.anatomical_structure, Oncology, Pediatrics, Perinatology and Child Health, alpha-Fetoproteins, Germ cell tumors, Neoplasm Recurrence, Local, business

Abstract

We aimed toidentify prognostic factors that may help better understand the behavior of relapsed central nervous system nongerminomatous germ cell tumors. We identified nine studies, including 101 patients; 33 patients (33%) were alive 12 months post-initial relapse. Sixty percent of patients with serum/cerebrospinal fluid (CSF) alpha-fetoprotein (AFP) level ≤25 ng/mL at initial diagnosis were survivors compared with 28% among patients with serum/CSF AFP level >25 ng/mL (P = 0.01). Seventy-one percent of patients who achieved complete response/continued complete response (CR/CCR) by the end of therapy at relapse were survivors compared with 7% among patients who had less than CR/CCR (P < 0.0001). Forty-eight percent of patients who received marrow-ablative chemotherapy followed by autologous hematopoietic cell rescue (HDCx/AuHCR) following relapse were survivors compared with 12% among patients who did not receive HDCx/AuHCR (P = 0.0001). Local relapse site, gross total surgical resection, and radiotherapy at relapse were not associated with improved outcomes.

Published

2021

43. Multi‐institutional analysis of treatment modalities in basal ganglia and thalamic germinoma

Author

Mohamed S. AbdelBaki, Christopher L. Tinkle, Girish Dhall, Rebecca Ronsley, Juliette Hukin, Roger J. Packer, Sabine Mueller, Jonathan L. Finlay, Joseph Stanek, Gregory K. Friedman, Kee Kiat Yeo, Tabitha Cooney, Ashley Margol, Lindsey Hoffman, Susan N. Chi, Amar Gajjar, Christina Coleman, Stephanie Villeneuve, Karen Gauvain, Jacob G. Ellen, Michael Fisher, Richard T Graham, Andrea Cappellano, Ute Bartels, Jack Su, Mohammad H Abu-Arja, Pournima Navalkele, John T. Lucas, Nicholas G. Gottardo, and Jeffrey C. Allen

Subjects

medicine.medical_specialty, medicine.medical_treatment, Basal Ganglia, Article, Central Nervous System Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Thalamus, Treatment plan, Basal ganglia, medicine, Humans, Retrospective Studies, Chemotherapy, Germinoma, Brain Neoplasms, business.industry, Radiotherapy Dosage, Hematology, medicine.disease, humanities, Radiation therapy, Clinical trial, Oncology, Treatment modality, 030220 oncology & carcinogenesis, Pediatrics, Perinatology and Child Health, Radiology, Neoplasm Recurrence, Local, business, Craniospinal, 030215 immunology

Abstract

BACKGROUND: Central nervous system (CNS) germinomas are treatment-sensitive tumors with excellent survival outcomes. Current treatment strategies combine chemotherapy with radiotherapy (RT) in order to reduce the field and dose of RT. Germinomas originating in the basal ganglia/thalamus (BGTGs) have proven challenging to treat given their rarity and poorly defined imaging characteristics. Craniospinal (CSI), whole brain (WBI), whole ventricle (WVI), and focal RT have all been utilized; however, the best treatment strategy remains unclear. METHODS: Retrospective multi-institutional analysis has been conducted across 18 institutions in four countries. RESULTS: For 43 cases of non-metastatic BGTGs, the 5- and 10-year event-free survival (EFS) were 85.8% and 81.0%, respectively, while the 5- and 10-year overall survival (OS) were 100%, and 95.5%, respectively (one patient fatality from unrelated cause). Median RT doses were as follows: CSI: 2250 cGy/cGy(RBE) (1980 to 2400 cGy/cGy[RBE]), WBI: 2340 (1800 to 3000 cGy/cGy[RBE]), WVI: 2340 cGy/cGy(RBE) (1800 to 2550 cGy/cGy[RBE]), focal: 3600 cGy (3060 to 5400 cGy). Thirty-eight patients (90.5%) received chemotherapy. There was no statistically significant difference in the EFS based on initial field extent (p=0.84). Nevertheless, no relapses were reported in patients who received CSI or WBI. Chemotherapy alone had significantly inferior EFS compared to combined therapy (p=0.0092), but patients were salvageable with RT. CONCLUSION: Patients with BGTGs have excellent outcomes and RT proved to be an integral component of the treatment plan. This group of patients should be included in future prospective clinical trials and the best RT field should be investigated further.

Published

2021

44. Alterations in ALK/ROS1/NTRK/MET drive a group of infantile hemispheric gliomas

Author

Elisabeth J. Rushing, Bruce Crooks, Scott L. Coven, Uri Tabori, Eric Bouffet, Claire Li, Christopher Li, Josef Zamecnik, Ute Bartels, Cynthia Hawkins, P. Daniel McNeely, Inmaculada de Prada, Michael Brudno, Michael D. Taylor, Bev Wilson, Claudia C. Faria, Livia Garzia, Vijay Ramaswamy, Lenka Krskova, Christopher Dunham, Roberto Silva, Andres Morales La Madrid, Sylvia Cheng, Ofelia Cruz, Arun K. Ramani, Michael A. Grotzer, Donna L. Johnston, Jonathan L. Finlay, David Sumerauer, Maria Joao Gil-da-Costa, Scott Ryall, Ana Guerreiro Stucklin, Yvonne Zhong, Pasqualino De Antonellis, Anthony Arnoldo, Daniel R. Boue, Koichi Ichimura, Miguel Garcia Ariza, Jean Michaud, Marta Perez-Somarriba, Motoo Nagane, Frank van Landeghem, Kohei Fukuoka, Hiroaki Sakamoto, Paul E. Kowalski, Meredith S. Irwin, Michal Zapotocky, Taylor Bridge, Iris Fried, Liana Nobre, Monique Johnson, Jordan R. Hansford, Robert Siddaway, Mary Shago, Nataliya Zhukova, Byungjin Kim, Palma Solano, Yoshiko Nakano, Keita Terashima, Alvaro Lassaletta, Angelica Oviedo, Amulya NageswaraRao, Repositório da Universidade de Lisboa, Guerreiro Stucklin, A. S., Ryall, S., Fukuoka, K., Zapotocky, M., Lassaletta, A., Li, C., Bridge, T., Kim, B., Arnoldo, A., Kowalski, P. E., Zhong, Y., Johnson, M., Ramani, A. K., Siddaway, R., Nobre, L. F., de Antonellis, P., Dunham, C., Cheng, S., Boue, D. R., Finlay, J. L., Coven, S. L., de Prada, I., Perez-Somarriba, M., Faria, C. C., Grotzer, M. A., Rushing, E., Sumerauer, D., Zamecnik, J., Krskova, L., Garcia Ariza, M., Cruz, O., Morales La Madrid, A., Solano, P., Terashima, K., Nakano, Y., Ichimura, K., Nagane, M., Sakamoto, H., Gil-da-Costa, M. J., Silva, R., Johnston, D. L., Michaud, J., Wilson, B., van Landeghem, F. K. H., Oviedo, A., Mcneely, P. D., Crooks, B., Fried, I., Zhukova, N., Hansford, J. R., Nageswararao, A., Garzia, L., Shago, M., Brudno, M., Irwin, M. S., Bartels, U., Ramaswamy, V., Bouffet, E., Taylor, M. D., Tabori, U., and Hawkins, C.

Subjects

MAPK/ERK pathway, Oncology, Epigenomics, Male, General Physics and Astronomy, Whole Exome Sequencing, Receptor tyrosine kinase, 0302 clinical medicine, Protein-Tyrosine Kinase, Cancer genomics, Anaplastic lymphoma kinase, Anaplastic Lymphoma Kinase, lcsh:Science, Exome sequencing, Proto-Oncogene Protein, Multidisciplinary, Molecular medicine, biology, Brain Neoplasms, Glioma, Protein-Tyrosine Kinases, Proto-Oncogene Proteins c-met, Receptor Protein-Tyrosine Kinase, Gene Expression Regulation, Neoplastic, 030220 oncology & carcinogenesis, Female, Survival Analysi, Human, medicine.medical_specialty, Epigenomic, Science, Article, General Biochemistry, Genetics and Molecular Biology, Brain Neoplasm, 03 medical and health sciences, Internal medicine, Proto-Oncogene Proteins, Exome Sequencing, medicine, ROS1, Humans, Receptor, trkA, Survival analysis, business.industry, Infant, Newborn, Infant, Receptor Protein-Tyrosine Kinases, General Chemistry, DNA Methylation, medicine.disease, Survival Analysis, biology.protein, lcsh:Q, business, 030217 neurology & neurosurgery

Abstract

© The Author(s) 2019. Open Access. This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/., Infant gliomas have paradoxical clinical behavior compared to those in children and adults: low-grade tumors have a higher mortality rate, while high-grade tumors have a better outcome. However, we have little understanding of their biology and therefore cannot explain this behavior nor what constitutes optimal clinical management. Here we report a comprehensive genetic analysis of an international cohort of clinically annotated infant gliomas, revealing 3 clinical subgroups. Group 1 tumors arise in the cerebral hemispheres and harbor alterations in the receptor tyrosine kinases ALK, ROS1, NTRK and MET. These are typically single-events and confer an intermediate outcome. Groups 2 and 3 gliomas harbor RAS/MAPK pathway mutations and arise in the hemispheres and midline, respectively. Group 2 tumors have excellent long-term survival, while group 3 tumors progress rapidly and do not respond well to chemoradiation. We conclude that infant gliomas comprise 3 subgroups, justifying the need for specialized therapeutic strategies.

Published

2019

45. Targeting Upstream Kinases of STAT3 in Human Medulloblastoma Cells

Author

Christopher R. Pierson, Jiayuh Lin, Chenglong Li, Jia Wei, Jonathan L. Finlay, and Ling Ma

Subjects

STAT3 Transcription Factor, 0301 basic medicine, Cancer Research, Dasatinib, Apoptosis, Article, 03 medical and health sciences, 0302 clinical medicine, Piperidines, Cell Movement, Antineoplastic Combined Chemotherapy Protocols, Nitriles, Drug Discovery, Tumor Cells, Cultured, medicine, Humans, Pyrroles, Cerebellar Neoplasms, STAT3, Protein Kinase Inhibitors, Cell Proliferation, Pharmacology, Medulloblastoma, biology, Kinase, Chemistry, Drug Synergism, medicine.disease, Pyrimidines, src-Family Kinases, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, STAT protein, Pyrazoles, Phosphorylation, Cisplatin, Tyrosine kinase, Proto-oncogene tyrosine-protein kinase Src, medicine.drug

Abstract

Background:Medulloblastoma is the most common malignant brain tumor in children. Despite improvement in overall survival rate, it still lacks an effective targeted treatment strategy. The Janus family of cytoplasmic tyrosine kinases (JAKs) and Src kinases, upstream protein kinases of signal transducer and activator of transcription 3 (STAT3), play important roles in medulloblastoma pathogenesis and therefore represent potential therapeutic targets.Methods:In this report, we examined the inhibitory efficacy of the JAK1/2 inhibitor, ruxolitinib, the JAK3 inhibitor, tofacitinib and two Src inhibitors, KX2-391 and dasatinib.Results:These small molecule drugs significantly reduce cell viability and inhibit cell migration and colony formation in human medulloblastoma cells in vitro. Src inhibitors have more potent efficacy than JAK inhibitors in inhibiting medulloblastoma cell migration ability. The Src inhibitors can inhibit both phosphorylation of STAT3 and Src while JAK inhibitors reduce JAK/STAT3 phosphorylation. We also investigated the combined effect of the Src inhibitor, dasatinib with cisplatin. The results show that dasatinib exerts synergistic effects with cisplatin in human medulloblastoma cells through the inhibition of STAT3 and Src.Conclusion:Our results suggest that the small molecule inhibitors of STAT3 upstream kinases, ruxolitinib, tofacitinib, KX2-391, and dasatinib could be novel and attractive candidate drugs for the treatment of human medulloblastoma.

Published

2019

46. Descriptive epidemiology of germ cell tumors of the central nervous system diagnosed in the United States from 2006 to 2015

Author

Quinn T. Ostrom, Carol Kruchko, Jill S. Barnholtz-Sloan, Haley Gittleman, Diana S Osorio, Jonathan L. Finlay, Gino Cioffi, and Toni Vecchione-Koval

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Time Factors, Adolescent, Population, Brain tumor, Central Nervous System Neoplasms, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Epidemiology, medicine, Humans, Registries, Child, education, education.field_of_study, Germinoma, business.industry, Incidence, Incidence (epidemiology), Age Factors, Infant, Newborn, Infant, Cancer, Middle Aged, Neoplasms, Germ Cell and Embryonal, Prognosis, medicine.disease, United States, Survival Rate, Neurology, Child, Preschool, 030220 oncology & carcinogenesis, Pacific islanders, Female, Neurology (clinical), Germ cell tumors, business, 030217 neurology & neurosurgery, Follow-Up Studies

Abstract

Germ cell tumors (GCT) in the central nervous system (CNS) are rare tumors that occur with highest frequency in males, Asian populations, and children less than age 20 years. Due to the rarity of these tumors, their patterns of incidence are not well-described. The aim of this study is to provide the most up-to-date data on incidence and survival patterns for CNS GCT by sex, race, and age at diagnosis. The Central Brain Tumor Registry of the United States (CBTRUS) is the largest aggregation of population-based incidence data on primary brain and other CNS tumors in the United States, containing incidence data from 51 central cancer registries and representing 100% of the US population. The current study used the CBTRUS analytic file to examine incidence (IR) of CNS GCT from 2006 to 2015, as well as registry data from the Surveillance, Epidemiology, and End Results (SEER) program to examine survival. Males had greater IR than females in all CNS GCT histologies examined. Asian and Pacific Islanders had a significantly greater IR of CNS GCT than the other race categories. We confirmed that CNS GCT IR was greatest for those age 10–14 years and male. Overall survival rates were high for malignant CNS GCT, germinoma, mixed GCT, and malignant teratoma. There is significant variation in CNS GCT incidence by sex, race, and age at diagnosis. Ascertaining accurate incidence and survival rates of CNS GCT provides vital information usable in real time for clinicians, public health planners, patients, and their families.

Published

2019

47. Germinoma Involving the Retina: An Unusual Presentation of Recurrent Intracranial Mixed Germ Cell Tumor

Author

Daniel R. Boue, Mohammad H Abu Arja, Christopher R. Pierson, Melissa Stalling, Lance S. Governale, Jonathan L. Finlay, Randal Olshefski, Joshua D. Palmer, and Jerome Rusin

Subjects

Retina, Pathology, medicine.medical_specialty, genetic structures, Germinoma, medicine.diagnostic_test, business.industry, Central nervous system, Magnetic resonance imaging, Malignant Germ Cell Tumor, medicine.disease, eye diseases, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Biopsy, Optic nerve, Medicine, Surgery, sense organs, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Background We report a patient with primary central nervous system mixed malignant germ cell tumor (GCT) who presented with recurrent malignant germinomatous infiltration of the retina. Case Description A 10-year-old girl initially presented with a large suprasellar mixed malignant GCT with a near-complete response after initial induction of chemotherapy and irradiation. Three and a half years after initial therapy, she presented with progressively worsening vision in her left eye. Magnetic resonance imaging showed infiltrative changes within the left optic nerve but no discrete mass. Serum and cerebrospinal fluid tumor markers were not elevated and cerebrospinal fluid cytology was negative. Left optic nerve biopsy confirmed the presence of mature teratoma and pure germinoma components. She was treated with gross-total resection of the left eye and optic nerve and chemotherapy. Histopathologic evaluation of the optic nerve showed only mature teratoma elements, but with pure germinoma cells infiltrating the inner layers of the retina. Conclusions Loco-regional extension of suprasellar GCT to the optic nerve is not uncommon; however, to the best of our knowledge, infiltration of the tumor into the retina is not reported in the literature. Early detection of optic pathway involvement and proper delineation of the irradiation field may prevent GCT infiltration of the retina with subsequent vision loss.

Published

2019

48. Abstract 1428: DNA methylation predicts early onset of primary tumor in patients with Li-Fraumeni syndrome

Author

Vallijah Subasri, Benjamin Brew, Lauren Erdman, Tanya Guha, Jordan R. Hansford, Elizabeth Cairney, Carol Portwine, Christine Elser, Jonathan L. Finlay, Kim E. Nichols, Wendy Kohlmann, Noa Alon, Ana Novokmet, Ledia Brunga, Anita Villani, Kelvin C. de Andrade, Payal P. Khincha, Sharon A. Savage, Joshua D. Schiffman, David Malkin, and Anna Goldenberg

Subjects

Cancer Research, Oncology

Abstract

Background: Li-Fraumeni syndrome (LFS) is an autosomal dominant cancer predisposition syndrome. Approximately 80% of individuals with LFS harbor a germline TP53 pathogenic variant rendering them susceptible to a wide spectrum of early-onset malignancies. A comprehensive surveillance regimen termed the ‘Toronto Protocol’, has recently been adopted for early tumor detection, demonstrating significant improvement in survival among TP53 pathogenic variant carriers. However, the protocol’s “one-size-fits-all” approach fails to consider an individual patient's risk of cancer. We built a machine learning model that predicts early-onset of primary tumors in LFS by estimating the probability of cancer onset before the age of six years, leveraging patient peripheral blood leukocyte methylation profiles. Methods: We built a gradient-boosted tree model to predict the probability of cancer onset before the age of six using methylation data from 288 TP53 pathogenic variant carriers. An external test set of 82 TP53 pathogenic variant carriers was used to validate our model. To increase the signal-to-noise ratio, methylation probes associated with TP53 status were retained and probes associated with aging were removed. In our study, we were primarily interested in minimizing the false negative rate (i.e. to reduce the number of patients who developed cancer before the age of six but were undetected by our algorithm. Findings: We correctly predicted whether the first tumor will occur before the age of six with an accuracy of 79% in our external test set. Importantly, our model classified 90% of the patients that developed cancer prior to the age of six correctly. In addition, 81% of the individuals without cancer in the external test set were predicted correctly. Interpretation: Our tool provides additional value to clinicians in stratifying patients into low- or high-risk groups of developing early-onset malignancies, and helps inform rational use of clinical surveillance tools for early cancer detection, with the ultimate aim to improve overall patient outcomes. Citation Format: Vallijah Subasri, Benjamin Brew, Lauren Erdman, Tanya Guha, Jordan R. Hansford, Elizabeth Cairney, Carol Portwine, Christine Elser, Jonathan L. Finlay, Kim E. Nichols, Wendy Kohlmann, Noa Alon, Ana Novokmet, Ledia Brunga, Anita Villani, Kelvin C. de Andrade, Payal P. Khincha, Sharon A. Savage, Joshua D. Schiffman, David Malkin, Anna Goldenberg. DNA methylation predicts early onset of primary tumor in patients with Li-Fraumeni syndrome [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 1428.

Published

2022

49. LINC-10. The Adequate Treatment of Children and Adolescents with Primary Central Nervous System Germ Cell Tumors (CNS GCT) in a Developing Country

Author

Andréa M Cappellano, Natalia Dassi, Bruna Mançano, Sidnei Epelman, Daniela B Almeida, Sergio Cavalheiro, Patricia A Dastoli, Maria Teresa Seixas, Jardel M Nicácio, Marcos D Costa, Frederico A Silva, Simone S Aguiar, Carlos R Almeida Jr, Gustavo R Teixeira, Nasjla S Silva, and Jonathan L Finlay

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

INTRODUCTION: Primary central nervous system germ cell tumors (CNS GCT) are a heterogeneous group of malignancies that can be divided into germinomas and non-germinomatous GCT (NGGCT), accounting for 2-3% of brain tumors in children/adolescents in the Western hemisphere. The study aim is to report the ability to adequately treat Brazilian patients with CNSGCT through a consortium protocol, reporting their treatment, response and survival. Methods: Since 2013, 58 patients with histologic and/or tumor marker (TM) diagnosis of germinoma with/without HCGβ levels ≤200mIU/ml (n=43), five of them between 100-200mIU/ml, received carboplatin/ etoposide (4 cycles) and NGGCT (n=15), received carboplatin/etoposide/cyclophosphamide (6 cycles), all followed by 18Gy ventricular field irradiation and primary site(s) boost. Autologous hematopoietic cell transplant (AuHCT) was undertaken for NGGCT slow responders. Results: Mean age 13.2 years, 42 males. Diagnosis was made by TM (n=19), surgery (n=25) and both (n=12). Two bifocal cases with negative TM and inconclusive biopsy were treated as germinoma. Primary tumor location was pineal (n=30), suprasellar (n=16), bifocal (n=11) and basal ganglia/thalamus (n=1). Eighteen had ventricular/spinal spread. Second-look surgery occurred in seven patients. For the germinoma group, 36 achieved complete responses (CR) after chemotherapy, seven showed residual teratoma/scar. For the NGGCT after 4/6 cycles, six patients showed CR, two failure/progression and seven partial responses (five with negative TM). Two with positive TM underwent AuHCT. Radiotherapy was utilized as described, except in three patients. Four NGGCT patients died (two disease progression, two other causes with no disease). Toxicity was mostly grade 3/4 neutropenia/thrombocytopenia during chemotherapy. At a median follow-up of 40 months, event-free and overall survival was 100% for germinoma and 64.5% NGGCT. Conclusion: The proposed treatment was feasible to be performed in a developing country, with suitable survival even with VFI dose reduction to 18Gy.

Published

2022

50. MEDB-49. Relapsed SHH medulloblastomas in young children. Are there alternatives to full-dose craniospinal irradiation?

Author

Craig Erker, Brandon Craig, Simon Bailey, Maura Massimino, Valerie Larouche, Jonathan L Finlay, Cassie Kline, George Michaiel, Ashley Margol, Kenneth Cohen, Chantel Cacciotti, Virginia Harrods, Kathleen Doris, Mohammed AbdelBaki, Nisreen Amayiri, Zhihong Wang, Jordan Hansford, Juliette Hukin, Ralph Salloum, Lindsay Hoffman, Jeffrey Muray, Kevin Ginn, Zapotocky Zapotocky, Lorena Baroni, Vijay Ramaswamy, Stephen Gilheens, Dolli Aguiera, Claire Mazewski, Shafqat Shah, Douglas Strother, Sabine Muller, Amar Gajjar, Paul Northcott, Steve Clifford, Giles Robinson, Eric Bouffet, and Lucie Lafay-Cousin

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

BACKGROUND/RATIONAL: Following initial irradiation sparing therapy, many young children with relapsed medulloblastoma can be salvaged with craniospinal irradiation (CSI). However, the interval to relapse is short and neurocognitive sequelae remain a major concern. The contribution of molecular subgrouping may help refine indications and modalities of salvage strategies in this population. METHOD: From a cohort of 151 young children with molecularly characterized relapsed medulloblastoma, subset analysis of the SHH medulloblastoma was conducted to describe the practice of salvage radiotherapy and associated post-relapse survival (PRS). RESULTS: Sixty-seven SHH medulloblastoma patients (46 M0; 54 GTR; 11 non-ND/MBEN) received salvage therapy with curative intent. Before relapse, 54 (80.6%) received conventional chemotherapy (CC), 13 (19.4%) high-dose chemotherapy (HDC), while seven had additional focal radiotherapy (fRT). Median time to relapse was 11.1 months (range 3.8-41.0) and 43.3% were localized. Thirty patients (16 localized relapse) underwent surgery. Forty-seven (71.2%) received salvage radiotherapy (20 with CC; 10 with HDC; 15 alone, two unknown). CSI and fRT accounted for 82% and 18% respectively. CSI median dose was 36Gy (range 18-39Gy). Ten patients (eight with localized relapse) received CSI doses ≤23.4Gy. Nineteen patients (28.8%) did not receive any radiotherapy (nine HDC; 10 CC only). Radiotherapy was associated with better 3-year PRS (73.0% versus 36.1%; p=0.001). All patients treated with CSI ≤ 23.4Gy were alive at median follow-up of 69 months(24-142). Six of nine patients treated with HDC without irradiation were alive at last follow-up. Sixty-three percent of patients received reduced dose CSI(≤23.4Gy), fRT, or no radiotherapy, and their PRS did not significantly differ from those who received CSI ≥ 30.6Gy (p = 0.54). CONCLUSION: While salvage CSI provided PRS benefit in this SHH medulloblastoma cohort, we report the use of reduced salvage radiotherapy and irradiation avoidance in 63% of the patients, with 60% alive at last follow-up.

Published

2022