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2. Case report: Tisagenlecleucel for treatment of relapsed B- acute lymphoblastic leukemia in a patient with CHEK2 mutation

Author

Abraham Ipe, Anne Angiolillo, David Jacobsohn, Jinjun Cheng, Miriam Bornhorst, Joyce Turner, and Anant Vatsayan

Subjects
CAR-T, tisagenlecleucel, B-ALL, CHEK2 mutation, MDS, Pediatrics, RJ1-570
Abstract

BackgroundGermline Checkpoint Kinase 2 gene (CHEK2) mutations can increase the risk of solid tumors. Recently, they have been identified as risk factors for hematologic malignancies. However, to the best of our knowledge, B-acute lymphoblastic leukemia (B-ALL) has never been described as a presenting manifestation of germline CHEK2 mutation. Chimeric antigen receptor-T (CAR-T) cell therapy directed against CD19 antigen (tisagenlecleucel) is a novel cellular therapy for treatment of relapsed/refractory (R/R) B-ALL. The use of tisagenlecleucel has not been described in patients with CHEK2 mutation.Case PresentationWe describe a case of a pediatric patient with a heterozygous pathogenic germline CHEK2 mutation (c.1100delC; p.Thr367Metfs*15) successfully treated with tisagenlecleucel for relapsed B-ALL to avoid hematopoietic cell transplant (HCT). The twelve-year-old boy was diagnosed with National Cancer Institute (NCI) high-risk B-ALL (white blood cell count >50,000/mcL), with no extramedullary disease. Cytogenetic analysis revealed normal karyotype but fluorescent in situ hybridization (FISH) showed 93% positivity for CRLF2::P2RY8 rearrangement. He was treated as per Children's Oncology Group (COG) AALL1131 therapy and achieved a complete remission. Seven months after diagnosis, he was found to have papillary thyroid carcinoma with no evidence of metastatic disease. The patient underwent a total thyroidectomy with central lymph node biopsy and radioactive iodine therapy. The patient's biological mother and fraternal twin brother carry the same germline CHEK2 mutation with no history of malignancy. The biological father tested negative for the familial mutation. The patient's genetic panel also identified three variants of unclear significance: CDKN2A (c.37 °C > T; p.Arg124Cys), FLCN (c.62G > A; p.Cys21Tyr) and SDHAF2 (c.139A > G; p.Met47Val). Extended family history also revealed a diagnosis of anaplastic thyroid cancer in maternal uncle at the age of 44 years. Fifteen months after diagnosis the patient had a relapse of B-ALL (both medullary and extramedullary with blasts in CSF), which was successfully treated with tisagenlecleucel. The patient remains in remission 3 years after receiving tisagenlecleucel.ConclusionAs conventional chemotherapy and radiation can potentially increase the risk of DNA damage and development of secondary malignancies, CD19 CAR-T therapy (tisagenlecleucel) can be used as a substitute for intensive re-induction chemotherapy and HCT in patients with a germline CHEK2 mutation.

Published
2023
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3. Atypical Presentations among Older Adults with COVID-19 Disease: A Need for Broadening the Differential Diagnosis

Author

Ugochi Ohuabunwa MD, Joyce Turner MSN, ANP-BC, and Ted Johnson MD, MPH

Subjects
Geriatrics, RC952-954.6
Abstract

Typical presenting symptoms of COVID-19 have been reported to be common in older adults. Current guidelines by the World Health Organization (WHO) and Centers for Disease Control (CDC) for testing and diagnosis are based on the presence of these typical symptoms. Several older adults seen at our hospital have presented atypically with symptoms such as delirium, falls, increasing the need for attention to diagnostic protocols since this has significant implications for early detection and patient outcomes, infection control and promotion of safety among healthcare providers. With the increased risk of fatality among older adults with COVID-19, appropriate diagnostic protocols are needed to ensure early diagnosis and management. Recognizing these atypical presentations in nursing homes would also facilitate early screening and cohorting in these congregate living facilities where older adults have had disproportionately high morbidity and mortality rates. We present two patients who presented with delirium and falls, found to have COVID-19 infection.

Published
2021
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4. Somatic Mosaicism of IDH1 R132H Predisposes to Anaplastic Astrocytoma: A Case of Two Siblings

Author

Sulgi Lee, Madhuri Kambhampati, M. Isabel Almira-Suarez, Cheng-Ying Ho, Eshini Panditharatna, Seth I. Berger, Joyce Turner, David Van Mater, Lindsay Kilburn, Roger J. Packer, John S. Myseros, Eric Vilain, Javad Nazarian, and Miriam Bornhorst

Subjects
anaplastic astrocytoma, mosaicism, cancer predisposition, ddPCR, AYA (adolescents and young adults), IDH1 R132H mutation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Anaplastic astrocytomas are aggressive glial cancers that present poor prognosis and high recurrence. Heterozygous IDH1 R132H mutations are common in adolescent and young adult anaplastic astrocytomas. In a majority of cases, the IDH1 R132H mutation is unique to the tumor, although rare cases of anaplastic astrocytoma have been described in patients with mosaic IDH1 mutations (Ollier disease or Maffucci syndrome). Here, we present two siblings with IDH1 R132H mutant high grade astrocytomas diagnosed at 14 and 26 years of age. Analysis of IDHR132H mutations in the siblings' tumors and non-neoplastic tissues, including healthy regions of the brain, cheek cells, and primary teeth indicate mosaicism of IDHR132H. Whole exome sequencing of the tumor tissue did not reveal any other common mutations between the two siblings. This study demonstrates the first example of IDH1 R132H mosaicism, acquired during early development, that provides an alternative mechanism of cancer predisposition.

Published
2020
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5. Temporal order of RNase IIIb and loss-of-function mutations during development determines phenotype in pleuropulmonary blastoma / DICER1 syndrome: a unique variant of the two-hit tumor suppression model [version 2; referees: 2 approved]

Author

Mark Brenneman, Amanda Field, Jiandong Yang, Gretchen Williams, Leslie Doros, Christopher Rossi, Kris Ann Schultz, Avi Rosenberg, Jennifer Ivanovich, Joyce Turner, Heather Gordish-Dressman, Douglas Stewart, Weiying Yu, Anne Harris, Peter Schoettler, Paul Goodfellow, Louis Dehner, Yoav Messinger, and D. Ashley Hill

Subjects
Lung Cancer, Pediatric Oncology, Medicine, Science
Abstract

Pleuropulmonary blastoma (PPB) is the most frequent pediatric lung tumor and often the first indication of a pleiotropic cancer predisposition, DICER1 syndrome, comprising a range of other individually rare, benign and malignant tumors of childhood and early adulthood. The genetics of DICER1-associated tumorigenesis are unusual in that tumors typically bear neomorphic missense mutations at one of five specific “hotspot” codons within the RNase IIIb domain of DICER 1, combined with complete loss of function (LOF) in the other allele. We analyzed a cohort of 124 PPB children for predisposing DICER1 mutations and sought correlations with clinical phenotypes. Over 70% have inherited or de novo germline LOF mutations, most of which truncate the DICER1 open reading frame. We identified a minority of patients who have no germline mutation, but are instead mosaic for predisposing DICER1 mutations. Mosaicism for RNase IIIb domain hotspot mutations defines a special category of DICER1 syndrome patients, clinically distinguished from those with germline or mosaic LOF mutations by earlier onsets and numerous discrete foci of neoplastic disease involving multiple syndromic organ sites. A final category of PBB patients lack predisposing germline or mosaic mutations and have sporadic (rather than syndromic) disease limited to a single PPB tumor bearing tumor-specific RNase IIIb and LOF mutations. We propose that acquisition of a neomorphic RNase IIIb domain mutation is the rate limiting event in DICER1-associated tumorigenesis, and that distinct clinical phenotypes associated with mutational categories reflect the temporal order in which LOF and RNase IIIb domain mutations are acquired during development.

Published
2018
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7. Comfort with Pharmacogenetic Testing Amongst Pediatric Oncology Providers and Their Patients

Author

Catriona Mowbray, Joyce Turner, Jiaxiang Gai, and Shana Jacobs

Subjects
Pharmacogenetics, Research, Humans, Genetic Testing, Precision Medicine, Child, Medical Oncology, Pharmacogenomic Testing
Abstract

Background: Pharmacogenetic (PGx) testing, a component of personalized medicine, aims to ensure treatment efficacy while reducing side effects and symptoms. Before this testing becomes routine in the pediatric oncology population, nurses need to understand the knowledge and concerns of providers, patients, and family members with regard to the timing, extent, interpretation, and incorporation of PGx testing. Methods: As part of a comprehensive PGx study (larger study) for children diagnosed with cancer, we surveyed providers and caregivers of children with cancer about their knowledge of and comfort with PGx testing. Caregivers who declined to participate in the larger PGx study were also asked to participate in the survey. Chi-square tests and a two-sample t-test were used to compare variables. Results: One hundred and two participants from the larger PGx study and 12 families who refused (response rate of 77% and 54%, respectively) as well as 29 providers (88%) completed surveys. Families not on the study were less interested in and comfortable with PGx results. Both groups were concerned about health or life insurance discrimination and payment. Providers would like support in ordering PGx testing and interpreting PGx. Discussion: Providers remain wary of most PGx testing, uncomfortable with interpreting and applying the results. Families are interested in the possibilities of personalized prescribing while worried about who has access to their child's genetic information. Further education on relevant tests for providers, including nurses, and the testing process for families, including details on privacy and sharing of genetic information, appear necessary.

Published
2023

8. Data from DICER1 and Associated Conditions: Identification of At-risk Individuals and Recommended Surveillance Strategies

Author

D. Ashley Hill, Yoav H. Messinger, Louis P. Dehner, David Malkin, Dominik T. Schneider, Daniel Orbach, A. Lindsay Frazier, Shari Baldinger, Laura A. Harney, Ann Garrity Carr, Kami Wolfe Schneider, Katherine Schneider, Rachana Shah, Joyce Turner, Andrew J. Bauer, Anne K. Harris, Douglas R. Stewart, Junne Kamihara, Gretchen M. Williams, and Kris Ann P. Schultz

Abstract

Pathogenic germline DICER1 variants cause a hereditary cancer predisposition syndrome with a variety of manifestations. In addition to conferring increased cancer risks for pleuropulmonary blastoma (PPB) and ovarian sex cord–stromal tumors, particularly Sertoli–Leydig cell tumor, individuals with pathogenic germline DICER1 variants may also develop lung cysts, cystic nephroma, renal sarcoma and Wilms tumor, nodular hyperplasia of the thyroid, nasal chondromesenchymal hamartoma, ciliary body medulloepithelioma, genitourinary embryonal rhabdomyosarcoma, and brain tumors including pineoblastoma and pituitary blastoma. In May 2016, the International PPB Registry convened the inaugural International DICER1 Symposium to develop consensus testing and surveillance and treatment recommendations. Attendees from North America, Europe, and Russia provided expert representation from the disciplines of pediatric oncology, endocrinology, genetics, genetic counseling, radiology, pediatric surgery, pathology, and clinical research. Recommendations are provided for genetic testing; prenatal management; and surveillance for DICER1-associated pulmonary, renal, gynecologic, thyroid, ophthalmologic, otolaryngologic, and central nervous system tumors and gastrointestinal polyps. Risk for most DICER1-associated neoplasms is highest in early childhood and decreases in adulthood. Individual and caregiver education and judicious imaging-based surveillance are the primary recommended approaches. These testing and surveillance recommendations reflect a consensus of expert opinion and current literature. As DICER1 research expands, guidelines for screening and treatment will continue to be updated. Clin Cancer Res; 24(10); 2251–61. ©2018 AACR.

Published
2023

9. Supplementary Table S1: Searches on PubMed using keyword(s) and DICER1 from DICER1 and Associated Conditions: Identification of At-risk Individuals and Recommended Surveillance Strategies

Author

D. Ashley Hill, Yoav H. Messinger, Louis P. Dehner, David Malkin, Dominik T. Schneider, Daniel Orbach, A. Lindsay Frazier, Shari Baldinger, Laura A. Harney, Ann Garrity Carr, Kami Wolfe Schneider, Katherine Schneider, Rachana Shah, Joyce Turner, Andrew J. Bauer, Anne K. Harris, Douglas R. Stewart, Junne Kamihara, Gretchen M. Williams, and Kris Ann P. Schultz

Abstract

Searches on PubMed using keyword(s) and DICER1

Published
2023

10. Optical Genome Mapping Identifies a Novel Pediatric Embryonal Tumor Subtype with a ZNF532-NUTM1 Fusion

Author

Miriam Bornhorst, Augustine Eze, Surajit Bhattacharya, Ethan Putnam, M. Isabel Almira-Suarez, Christopher Rossi, Madhuri Kambhampati, Miguel Almalvez, Mariam Barseghyan, Nicole Del Risco, David Dotson, Joyce Turner, John Myseros, Eric Vilain, Roger Packer, Javad Nazarian, Brian Rood, and Hayk Barseghyan

Abstract

Molecular characteristics of pediatric brain tumors have not only allowed for tumor subgrouping but have introduced novel treatment options for patients with specific tumor alterations. Therefore, an accurate histologic and molecular diagnosis is critical for optimized management of all pediatric patients with brain tumors, including central nervous system embryonal tumors. We present a case where optical genome mapping identified a ZNF532-NUTM1 fusion in a patient with a unique tumor best characterized histologically as a central nervous system embryonal tumor with rhabdoid features. Additional analyses including immunohistochemistry for NUT protein, methylation array, whole genome, and RNA-sequencing was done to confirm the presence of the fusion in the tumor. This is the first description of a pediatric patient with a ZNF532-NUTM1 fusion, yet the histology of this tumor is similar to that of adult cancers with ZNF-NUTM1 fusions and other NUTM1-fusion positive brain tumors reported in literature. Although rare, the distinct pathology and underlying molecular characteristics of these tumors separate them from other embryonal tumors. Therefore, the NUTM-rearrangement appears to define a novel subgroup of pediatric central nervous system embryonal tumors with rhabdoid/epithelioid features that may have a unique response to treatment. Screening for a NUTM1-rearrangement should be considered for all patients with unclassified central nervous system tumors with rhabdoid features to ensure accurate diagnosis so this can ultimately inform therapeutic management for these patients.

Published
2022

11. Surveillance imaging and early surgical intervention for improved CNS tumor outcomes in children with Li-Fraumeni syndrome: Children's National Hospital experience and literature review

Author

Nirali Patel, Kathleen Felton, Surajit Bhattacharya, Maria Isabel Almira-Suarez, Augustine Eze, Joyce Turner, Robert Keating, Chima Oluigbo, Reuven J. Schore, Lindsay Kilburn, Roger J. Packer, John S. Myseros, and Miriam Bornhorst

Subjects
General Medicine
Abstract

OBJECTIVE Li-Fraumeni syndrome (LFS) is a cancer predisposition syndrome caused by germline mutations in the TP53 gene. CNS tumors are the fourth most common tumor type in LFS, and recent screening guidelines demonstrate that early tumor detection is associated with improved long-term survival. However, there is a paucity of data regarding surgical intervention when lesions are identified in asymptomatic patients on surveillance imaging. The authors investigated this through their cohort and literature review. METHODS The cohort consisted of children seen in the Pediatric Cancer Genetics Program at Children’s National Hospital between August 2012 and August 2021. The authors also include a PubMed (MEDLINE) literature search of articles from 2006 to 2021 related to surveillance and CNS tumors in patients with LFS. Studies in which CNS tumors were not identified or detailed patient information was not provided were excluded. Patients from the selected articles and the authors’ cohort were added for further analysis. RESULTS Between August 2012 and August 2021, 10 children with LFS and CNS tumors were assessed at Children’s National Hospital: 4 who were known carriers of the TP53 mutation had CNS lesions found on surveillance imaging, whereas 6 presented with symptomatic CNS lesions and were either known or subsequently found to have germline TP53 mutations. The literature search identified 148 articles, 7 of which were included in this review. Patients from the literature and the present cohort were added for a total of 56 CNS lesions. A majority of the low-grade CNS lesions (22/24, 92%) were found on surveillance protocols in asymptomatic patients, whereas the majority of the high-grade lesions (22/26, 85%) presented in symptomatic patients who were not undergoing routine surveillance or as the initial diagnosis of LFS. The authors noted a significant survival advantage in pediatric patients with low-grade lesions, with an overall survival of 100% at 30 months. Minor limitations of the study include patient sample size and limitations in the patient cohort due to this being a retrospective rather than a prospective study. CONCLUSIONS Data presented in this study support surveillance protocols in LFS and demonstrate the importance of dedicated CNS imaging and early surgical intervention when lesions are identified. Systematic review registration no.: CRD42022372610 (www.crd.york.ac.uk/prospero)

Published
2022

12. Cancer genetic counseling for childhood cancer predisposition is associated with improved levels of knowledge and high satisfaction in parents

Author

Joyce Turner, Kami Wolfe Schneider, Christopher C. Porter, Cecelia Bellcross, Olivia A Juarez, and Bojana Pencheva

Subjects
Adult, Counseling, Parents, Genetic counseling, media_common.quotation_subject, Childhood cancer, Genetic Counseling, Context (language use), Personal Satisfaction, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Humans, Medicine, Child, Genetics (clinical), media_common, 0303 health sciences, business.industry, Cancer predisposition, 030305 genetics & heredity, Cancer, medicine.disease, Pediatric cancer, 030220 oncology & carcinogenesis, Cohort, Worry, business, Clinical psychology
Abstract

Previous surveys of adults with cancer have revealed increased levels of genetic knowledge, varying levels of worry, and high satisfaction with cancer genetic counseling. We sought to determine the impact of cancer genetic counseling on parental levels of genetic knowledge, worry about cancer, and satisfaction in the context of suspected cancer predisposition in a child. We hypothesized that parents would be satisfied with cancer genetic counseling and that cancer genetic counseling would improve baseline parental genetic knowledge and decrease levels of worry. Parents were recruited from a pediatric cancer predisposition clinic in the United States. A survey was administered to two cohorts: One cohort had received cancer genetic counseling in the past and only completed one survey (post-only, n = 26), and another cohort completed the survey before and after cancer genetic counseling (pre/post, n = 23). The survey included questions on demographics, knowledge of genetics, worry levels, and satisfaction with the cancer genetic counseling service. The post-genetic counseling survey also contained a free-text section for parents to indicate what they took away from the sessions. Parental levels of genetics knowledge increased by an average of 1.9 points (p = .01), with 65.2% of parents demonstrating an increase in genetics knowledge score. Average worry levels did not change significantly (p = .37), with 52.2% of parents indicating decreased worry, and 34.8% indicating increased worry. Overall, 91.8% of parents reported high levels of satisfaction. Our results show that cancer genetic counseling in a pediatric cancer predisposition clinic improves parental levels of genetics knowledge. Satisfaction rates suggest that parents find this service beneficial. These results demonstrate the positive impacts of cancer genetic counseling on parents of children in which a hereditary cancer syndrome is known or suspected.

Published
2020

14. Temporal order of RNase IIIb and loss-of-function mutations during development determines phenotype in DICER1 syndrome: a unique variant of the two-hit tumor suppression model [version 1; referees: 2 approved with reservations]

Author

Mark Brenneman, Amanda Field, Jiandong Yang, Gretchen Williams, Leslie Doros, Christopher Rossi, Kris Ann Schultz, Avi Rosenberg, Jennifer Ivanovich, Joyce Turner, Heather Gordish-Dressman, Douglas Stewart, Weiying Yu, Anne Harris, Peter Schoettler, Paul Goodfellow, Louis Dehner, Yoav Messinger, and D. Ashley Hill

Subjects
Research Article, Articles, Lung Cancer, Pediatric Oncology, DICER1 truncation, PPB, Pleuropulmonary blastoma, Mosaicism, Paediatric cancer, RNAse IIIb
Abstract

Pleuropulmonary blastoma (PPB) is the most frequent pediatric lung tumor and often the first indication of a pleiotropic cancer predisposition, DICER1 syndrome, comprising a range of other individually rare, benign and malignant tumors of childhood and early adulthood. The genetics of DICER1-associated tumorigenesis are unusual in that tumors typically bear neomorphic missense mutations at one of five specific “hotspot” codons within the RNase IIIb domain of DICER 1, combined with complete loss of function (LOF) in the other allele. We analyzed a cohort of 124 PPB children for predisposing DICER1 mutations and sought correlations with clinical phenotypes. Over 70% have inherited or de novo germline LOF mutations, most of which truncate the DICER1 open reading frame. We identified a minority of patients who have no germline mutation, but are instead mosaic for predisposing DICER1 mutations. Mosaicism for RNase IIIb domain hotspot mutations defines a special category of DICER1 syndrome patients, clinically distinguished from those with germline or mosaic LOF mutations by earlier onsets and numerous discrete foci of neoplastic disease involving multiple syndromic organ sites. A final category of patients lack predisposing germline or mosaic mutations and have disease limited to a single PPB tumor bearing tumor-specific RNase IIIb and LOF mutations. We propose that acquisition of a neomorphic RNase IIIb domain mutation is the rate limiting event in DICER1-associated tumorigenesis, and that distinct clinical phenotypes associated with mutational categories reflect the temporal order in which LOF and RNase IIIb domain mutations are acquired during development.

Published
2015
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15. A Pediatric Case of Transformed Mycosis Fungoides in a BRCA2 Positive Patient

Author

Anna Y. Kirkorian, Reuven J. Schore, Andrea M. Gross, Joyce Turner, Shana Jacobs, Ginette A. Okoye, Kirsten M. Williams, Miriam Bornhorst, and Dragos C. Luca

Subjects
medicine.medical_specialty, Skin Neoplasms, Malignancy, 03 medical and health sciences, Mycosis Fungoides, 0302 clinical medicine, BRCA2 Mutation, Germline mutation, Humans, Medicine, BRCA2 Protein, Mycosis fungoides, business.industry, Cutaneous T-cell lymphoma, Cancer, Hematology, Prognosis, medicine.disease, Positive patient, Dermatology, Lymphoma, T-Cell, Cutaneous, Oncology, Child, Preschool, 030220 oncology & carcinogenesis, Mutation, Pediatrics, Perinatology and Child Health, Female, business, 030215 immunology, Pediatric population
Abstract

Cutaneous T-cell lymphomas are very rare in children. Although mycosis fungoides is the most common of these rare cutaneous T-cell lymphomas in children, transformation to an aggressive malignancy remains extremely uncommon, and there are no clear guidelines for clinical management in the pediatric population. In addition, the increased usage of next-generation sequencing for pediatric patients with unusual malignancies may result in the discovery of pathogenic germline mutations, though the association between these mutations and the patient's cancer is not always clear. We present here a unique pediatric case of transformed mycosis fungoides in a patient with BRCA2 mutation.

Published
2019

16. An integrated model of care utilizing community health workers to promote safe transitions of care

Author

Ugochi Ohuabunwa, Joyce Turner, Ebony Johnson, Queenie Jordan, Jonathan M. Flacker, and Victor O. Popoola

Subjects
African american, Community Health Workers, Male, medicine.medical_specialty, business.industry, Primary care, Transitional Care, Cohort Studies, Healthcare utilization, Intervention (counseling), Family medicine, Models, Organizational, medicine, Community health workers, Humans, Transitional care, Female, Geriatrics and Gerontology, Intervention evaluation, business, Cohort study, Aged
Abstract

BACKGROUND/OBJECTIVES Healthcare systems' adoption and sustenance of successful transitional care models (TCMs) have been limited by cost-prohibitive resource needs. Cost-effective TCMs that improve patient outcomes are needed to promote adoption by healthcare systems and sustainability. This study evaluated the effectiveness of a TCM utilizing community health workers (CHWs) in reducing inappropriate healthcare utilization and costs. DESIGN A cohort study with a pre-post intervention evaluation of the intervention group. SETTING A 953-bed academic urban safety-net hospital. PARTICIPANTS Eligible participants (N = 154) were hospitalized or had repeated emergency room (ER) visits, identified to be at high risk for readmission. INTERVENTION Promotion of self-management skills acquisition and care coordination by CHWs achieved through predischarge interdisciplinary team meetings, regular home visits and phone contact, accompaniment to primary care physicians' (PCP) appointments, support with transportation, medications, and self-management education. MEASUREMENTS Outcome measures were readmissions, ER visits, and PCP establishment. RESULTS Mean age of participants was 67, 65% were male, 92% African American. There was a significant reduction in overall number of readmissions (Z = 9.6, p

Published
2021

17. A Comprehensive Review of Pediatric Tumors and Associated Cancer Predisposition Syndromes

Author

Joyce Turner, Amanda Knoth Anglin, Sarah Scollon, Kami Wolfe Schneider, and Martha H. Thomas

Subjects
Adult, Male, 0301 basic medicine, medicine.medical_specialty, Pediatrics, Adolescent, Referral, Genetic counseling, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Neoplastic Syndromes, Hereditary, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Young adult, Child, Intensive care medicine, Referral and Consultation, Genetics (clinical), Genetic testing, medicine.diagnostic_test, business.industry, Public health, Infant, Cancer, medicine.disease, Pediatric cancer, Human genetics, 030104 developmental biology, Child, Preschool, 030220 oncology & carcinogenesis, Practice Guidelines as Topic, Female, business
Abstract

An understanding of the role of inherited cancer predisposition syndromes in pediatric tumor diagnoses continues to develop as more information is learned through the application of genomic technology. Identifying patients and their relatives at an increased risk for developing cancer is an important step in the care of this patient population. The purpose of this review is to highlight various tumor types that arise in the pediatric population and the cancer predisposition syndromes associated with those tumors. The review serves as a guide for recognizing genes and conditions to consider when a pediatric cancer referral presents to the genetics clinic.

Published
2017

18. Somatic Mosaicism of IDH1 R132H Predisposes to Anaplastic Astrocytoma: A Case of Two Siblings

Author

Sulgi Lee, Madhuri Kambhampati, M. Isabel Almira-Suarez, Cheng-Ying Ho, Eshini Panditharatna, Seth I. Berger, Joyce Turner, David Van Mater, Lindsay Kilburn, Roger J. Packer, John S. Myseros, Eric Vilain, Javad Nazarian, Miriam Bornhorst, University of Zurich, and Nazarian, Javad

Subjects
0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, IDH1, cancer predisposition, ddPCR, Case Report, 610 Medicine & health, medicine.disease_cause, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, medicine, 1306 Cancer Research, Young adult, Ollier disease, Exome sequencing, Mutation, IDH1 R132H mutation, AYA (adolescents and young adults), business.industry, anaplastic astrocytoma, Cheek, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, mosaicism, 030104 developmental biology, medicine.anatomical_structure, Oncology, Maffucci syndrome, 10036 Medical Clinic, 030220 oncology & carcinogenesis, 2730 Oncology, business, Anaplastic astrocytoma
Abstract

Anaplastic astrocytomas are aggressive glial cancers that present poor prognosis and high recurrence. Heterozygous IDH1 R132H mutations are common in adolescent and young adult anaplastic astrocytomas. In a majority of cases, the IDH1 R132H mutation is unique to the tumor, although rare cases of anaplastic astrocytoma have been described in patients with mosaic IDH1 mutations (Ollier disease or Maffucci syndrome). Here, we present two siblings with IDH1 R132H mutant high grade astrocytomas diagnosed at 14 and 26 years of age. Analysis of IDHR132H mutations in the siblings' tumors and non-neoplastic tissues, including healthy regions of the brain, cheek cells, and primary teeth indicate mosaicism of IDHR132H. Whole exome sequencing of the tumor tissue did not reveal any other common mutations between the two siblings. This study demonstrates the first example of IDH1 R132H mosaicism, acquired during early development, that provides an alternative mechanism of cancer predisposition.

Published
2019
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19. PATH-14. GENETIC SUSCEPTIBILITY AND OUTCOMES OF PEDIATRIC, ADOLESCENT AND YOUNG ADULT IDH-MUTANT ASTROCYTOMAS

Author

Sabine Mueller, Alberto Bronischer, Miriam Bornhorst, Lindsay Kilburn, Hayk Barseghyan, Eric Vilain, Tobey J. MacDonald, Joyce Turner, Brian R. Rood, Matthew Schniederjan, Jeremy Goecks, Denise Leung Leung, Enrico Opocher, Javad Nazarian, Cheng-Ying Ho, Cynthia Hawkins, Eugene Hwang, Eric Bouffet, Daniel R. Boue, Carl Koschmann, Brent A. Orr, Uri Tabori, Alexander O. Vortmeyer, Rajen Mody, Michal Zapotocky, Roger J. Packer, Surajit Bhattacharya, Asher Marks, Liana Nobre, and David A. Solomon

Subjects
Genetics, Cancer Research, Oncology, Mutant, Path (graph theory), Genetic predisposition, AcademicSubjects/MED00300, AcademicSubjects/MED00310, Neurology (clinical), Biology, Young adult, Pathology and Molecular Diagnosis
Abstract

INTRODUCTION Previously thought to be rare, recent case series have shown that IDH mutations in young patients are more common than previously described. In this study, we analyzed IDH-mutant tumors to determine clinical significance of these mutations in children, adolescents and young adults. METHODS Through this multi-institution study (10 institutions), we collected 64 IDH1/2-mutant infiltrating astrocytoma specimens from 58 patients aged 4–26 (M:F, 0.4:0.6). Specimens included 46 low-grade (LGG) and 18 high-grade (HGG) astrocytomas. Tumor sequencing data (n=45), germline sequencing data (n=37) and outcome data (n=40) was analyzed. RESULTS Similar to adults, most sequenced tumors had a co-mutation in the TP53 gene, while ATRX mutations were less common and primarily seen in HGGs. Approximately 60% (n=21) of patients with germline data available had a mutation in a cancer predisposition gene. Mismatch repair (MMR) mutations were most common (n=12; MSH6 n=9), followed by TP53mutations (n=7). All patients with MMR gene mutations had HGGs and poor progression free (PFS=10% at 2 years, mean TTP=9 months) and overall (OS CONCLUSION IDH-mutant tumors in pediatric patients are strongly associated with cancer predisposition and increased risk for progression/recurrence or malignant transformation. Routine screening for IDH1/2 mutations in children with grade 2–4 astrocytomas could greatly impact patient management.

Published
2020

20. HGG-37. DETECTION OF IDH1 R132H MOSAICISM IN ANAPLASTIC ASTROCYTOMA PATIENTS

Author

Sulgi Lee, Miriam Bornhorst, Eshini Panditharatna, Madhuri Kambhamptai, Joyce Turner, Roger J Packer, Lindsay Kilburn, and Javad Nazarian

Subjects
Cancer Research, Abstracts, Oncology, Neurology (clinical)
Abstract

Anaplastic astrocytomas are aggressive glial cancers that present poor prognosis and high recurrence. Heterozygous mutations in the IDH1 (R132H) gene are common in adult anaplastic astrocytomas, but are uncommon in the pediatric population. In a majority of cases, the IDH1 R132H mutation is somatic, although rare cases of anaplastic astrocytoma have been described in patients with mosaic germline mutations of IDH1 (Ollier disease or Maffucci syndrome). Here, we present two siblings who developed IDH1 R132H mutant high grade astrocytomas at 15 and 26 years of age. Our analysis of IDH1 R132H mutations in the siblings’ tumors and non-neoplastic tissues, including healthy regions of the brain (post-mortem samples from one sibling), cheek cells and primary teeth identified IDH1 R132H mosaicism, using digital PCR system. While both tumors had IDH1 R132H mutant allelic frequencies around 50%, mutant allelic frequencies ranging from 0.01% to 0.64% were detected in teeth, cheek cells, blood and non-tumorous brain tissue. Whole exome sequencing of the tumor tissue did not reveal any other common mutations between the two siblings. Our study demonstrates an example of IDH1 R132H mosaicism in two siblings with anaplastic astrocytoma, which could have gone unnoticed by traditional sequencing technologies. This finding supports a trend, seen in other cancers, of mosaic-like mutant allelic gene frequencies associated with cancer development. Further large-scale studies are needed to better understand the prevalence of mosaic IDH1, or other mutations, in patients with brain tumors, as this could impact the diagnosis and management of these patients.

Published
2018

21. DICER1 and associated conditions: Identification of at-risk individuals and recommended surveillance strategies

Author

Gretchen M. Williams, Junne Kamihara, Katherine A. Schneider, Andrew J. Bauer, Daniel Orbach, Joyce Turner, Dominik T. Schneider, Laura A. Harney, Shari Baldinger, Rachana Shah, Kami Wolfe Schneider, D. Ashley Hill, Douglas R. Stewart, Anne K. Harris, Louis P. Dehner, Yoav H. Messinger, Kris Ann P. Schultz, A. Lindsay Frazier, David Malkin, and Ann G. Carr

Subjects
0301 basic medicine, Cancer Research, Pediatrics, medicine.medical_specialty, endocrine system, medicine.diagnostic_test, business.industry, Cystic nephroma, Genetic counseling, Cancer, Pleuropulmonary blastoma, medicine.disease, Article, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, medicine, Blastoma, business, Mass screening, DICER1 Syndrome, Genetic testing
Abstract

Pathogenic germline DICER1 variants cause a hereditary cancer predisposition syndrome with a variety of manifestations. In addition to conferring increased cancer risks for pleuropulmonary blastoma (PPB) and ovarian sex cord–stromal tumors, particularly Sertoli–Leydig cell tumor, individuals with pathogenic germline DICER1 variants may also develop lung cysts, cystic nephroma, renal sarcoma and Wilms tumor, nodular hyperplasia of the thyroid, nasal chondromesenchymal hamartoma, ciliary body medulloepithelioma, genitourinary embryonal rhabdomyosarcoma, and brain tumors including pineoblastoma and pituitary blastoma. In May 2016, the International PPB Registry convened the inaugural International DICER1 Symposium to develop consensus testing and surveillance and treatment recommendations. Attendees from North America, Europe, and Russia provided expert representation from the disciplines of pediatric oncology, endocrinology, genetics, genetic counseling, radiology, pediatric surgery, pathology, and clinical research. Recommendations are provided for genetic testing; prenatal management; and surveillance for DICER1-associated pulmonary, renal, gynecologic, thyroid, ophthalmologic, otolaryngologic, and central nervous system tumors and gastrointestinal polyps. Risk for most DICER1-associated neoplasms is highest in early childhood and decreases in adulthood. Individual and caregiver education and judicious imaging-based surveillance are the primary recommended approaches. These testing and surveillance recommendations reflect a consensus of expert opinion and current literature. As DICER1 research expands, guidelines for screening and treatment will continue to be updated. Clin Cancer Res; 24(10); 2251–61. ©2018 AACR.

Published
2018

22. DICER1 and Associated Conditions: Identification of At-risk Individuals and Recommended Surveillance Strategies—Response

Author

Andrew J. Bauer, Douglas R. Stewart, Junne Kamihara, Anne K. Harris, Joyce Turner, Rachana Shah, Kami Wolfe Schneider, Katherine Schneider, Ann Garrity Carr, Laura A. Harney, A. Lindsay Frazier, Daniel Orbach, Dominik T. Schneider, David Malkin, Louis P. Dehner, Yoav H. Messinger, D. Ashley Hill, and Kris Ann P. Schultz

Subjects
DEAD-box RNA Helicases, Ribonuclease III, Cancer Research, Oncology, Humans
Published
2019

23. PDTM-25. GENETIC SUSCEPTIBILITY AND EVOLUTION OF PEDIATRIC IDH-MUTANT INFILTRATING ASTROCYTOMAS

Author

Javad Nazarian, Rajen Mody, David A. Solomon, Cheng-Ying Ho, Sabine Mueller, Brent A. Orr, Alberto Broniscer, Miriam Bornhorst, Jeremy Goecks, Asher Marks, Roger J. Packer, Joyce Turner, Carl Koschmann, Daniel R. Boue, Alexander O. Vortmeyer, and Eugene Hwang

Subjects
0301 basic medicine, Cancer Research, Mutation, Mutant, Astrocytoma, Biology, medicine.disease, medicine.disease_cause, Loss of heterozygosity, 03 medical and health sciences, Abstracts, 030104 developmental biology, Oncology, Glioma, medicine, Genetic predisposition, Cancer research, Neurology (clinical), Gene, Allele frequency, neoplasms
Abstract

IDH mutations are considered rare in pediatric gliomas, especially in children under 14 years of age. Therefore, IDH-mutant pediatric gliomas have not been well characterized. Through this multi-institution study (5 institutions), we analyzed a total of 20 IDH1/2-mutant pediatric/AYA infiltrating astrocytoma specimens from 18 patients aged 4-26. The specimens include 15 low-grade (WHO grade II) and 5 high-grade (WHO grade III or IV) astrocytomas. A majority of the tumors appear to be early lesions based on the low cellularity, making them suitable for studying the order of driver mutations. Similar to their adult counterparts, nearly all pediatric IDH-mutant infiltrating astrocytomas (17 tumors, 85%) harbor TP53 mutation. In comparison, ATRX mutations are less frequent, detected in only 9 tumors (45%) including 4 low-grade (26% of all low-grade) and 5 high-grade tumors (100% of all high-grade). Six patients (30%) carry germline mutations in tumor suppressor or mismatch repair genes including TP53, MSH6, and RB1. All patients (N=3) with a germline mutation in MSH6 (a mismatch repair gene) had high-grade IDH-mutant astrocytomas with high genomic instability. In contrast, patients with germline TP53 mutation (Li-Fraumeni syndrome, LFS-N=2) had low-grade tumors with low mutation burden, morphologically and genetically similar to the sporadic cases. Notably, 7 out of 12 sporadic tumors harboring TP53 mutations had a TP53 mutant allele frequency that is greater than twice the IDH1/2 allelic frequency, after adjustment for TP53 loss of heterozygosity in 2 cases. This finding, together with the LFS-associated tumors, suggests that TP53 mutation may precede, or predispose to, IDH mutations in a significant fraction of astrocytomas in young patients. Our results not only define the molecular architecture of pediatric IDH-mutant infiltrating astrocytomas, but also provide insight into the genetic evolution of these tumors.

Published
2017

24. DICER1-Related Sertoli-Leydig Cell Tumor and Gynandroblastoma: Clinical and Genetic Findings from the International Ovarian and Testicular Stromal Tumor Registry

Author

Yoav H. Messinger, Kris Ann P. Schultz, Michael Finch, A. Lindsay Frazier, David M. Gershenson, Jubilee Brown, Weiying Yu, D. Ashley Hill, Anne K. Harris, Joyce Turner, Douglas R. Stewart, Robert H. Young, Amanda Field, Dominik T. Schneider, Nicholas G. Cost, and Louis P. Dehner

Subjects
0301 basic medicine, Adult, Ribonuclease III, Pathology, medicine.medical_specialty, Adolescent, Gynandroblastoma, Disease, Pleuropulmonary blastoma, Germline, Article, DEAD-box RNA Helicases, 03 medical and health sciences, Sertoli-Leydig Cell Tumor, Young Adult, 0302 clinical medicine, medicine, Humans, Sex Cord-Gonadal Stromal Tumors, Genetic Predisposition to Disease, Registries, Family history, Child, Germ-Line Mutation, Genetic testing, Ovarian Neoplasms, medicine.diagnostic_test, business.industry, Mosaicism, Obstetrics and Gynecology, Infant, Middle Aged, medicine.disease, Prognosis, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Child, Preschool, Female, business, Testicular stromal tumor
Abstract

Background Ovarian sex cord-stromal tumors (OSCST) include juvenile granulosa cell tumors (JGCT), Sertoli-Leydig cell tumor (SLCT) and gynandroblastoma (GAB) among others. These ovarian sex cord-stromal tumors as well as other tumors including pleuropulmonary blastoma (PPB) may be associated with DICER1 mutations. We sought to describe the clinical and genetic findings from the first 107 individuals enrolled in the International Ovarian and Testicular Stromal Tumor Registry. Methods Medical and family history were obtained for individuals consecutively enrolled in the International Ovarian and Testicular Stromal Tumor Registry. Pathology was centrally reviewed. DICER1 sequencing was performed on blood and tumor tissue. Results Of the 107 participants, 49 had SLCT, 25 had JGCT and 5 had GAB. Nearly all (36/37) SLCTs and 4/4 GAB tested had a DICER1 mutation in an RNase IIIb domain hotspot; approximately half of these individuals had a predisposing germline DICER1 mutation. Metachronous SLCTs were seen in 3 individuals with germline DICER1 mutations. Other DICER1 -associated conditions were seen in 19% of patients with SLCT or GAB. Three children of women with SLCT were diagnosed with PPB based on genetic testing and clinical screening during the course of this study. All were diagnosed with PPB in its earliest and most curable form (Type I), were treated with surgery alone, and are alive without evidence of disease. Conclusions Recognition of the distinct genetic basis for a group of these tumors improves precise classification in difficult cases and promotes mutation-based screening and early detection.

Published
2017

25. Childhood Rhabdomyosarcoma in Association With a RASopathy Clinical Phenotype and Mosaic Germline SOS1 Duplication

Author

Patroula Smpokou, Joyce Turner, Baheyeldin Salem, Sean E. Hofherr, and Leslie Doros

Subjects
0301 basic medicine, Pleuropulmonary blastoma, RASopathy, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Costello syndrome, Gene Duplication, Gene duplication, medicine, Humans, Rhabdomyosarcoma, Embryonal, Neurofibromatosis, Rhabdomyosarcoma, Germ-Line Mutation, Genetics, business.industry, Noonan Syndrome, Hematology, medicine.disease, 030104 developmental biology, Phenotype, Oncology, 030220 oncology & carcinogenesis, Child, Preschool, Chromosomes, Human, Pair 2, Pediatrics, Perinatology and Child Health, Cancer research, ras Proteins, Noonan syndrome, Female, business, SOS1 Protein
Abstract

Childhood rhabdomyosarcoma (RMS) accounts for approximately 3.5% of cancer cases among children 0 to 14 years of age. Genetic conditions associated with high risk of childhood RMS include Li-Fraumeni syndrome, pleuropulmonary blastoma, Beckwith-Wiedemann syndrome, and some RASopathies, such as neurofibromatosis type 1, Costello syndrome (CS), and Noonan syndrome (NS). Here, we report the rare case of a 4-year-old girl with clinical features of NS who developed an embryonal RMS of the chest and needed emergent treatment. Molecular genetic testing identified a de novo, large, mosaic duplication of chromosome 2 encompassing the SOS1 gene, presumably caused by a mosaic, unbalanced translocation between chromosomes 2 and 17 found on routine cytogenetic analysis. Sequence analysis of all known genes causing Noonan spectrum disorders was negative. RMS has been reported in a few patients with NS, associated in very few with germline SOS1 mutations, but none with copy number abnormalities. This is the first report to our knowledge of early-onset RMS developing in a child with features of NS and a mosaic RAS pathway gene aberration, a large SOS1 duplication. We hypothesize that the inciting event for tumor development in this case is due to the germline mosaic duplication of SOS1, which was duplicated in all cells of the tumor, and the ultimate development of the tumor was further driven by multiple chromosomal aberrations in the tumor itself, all described as somatic events in isolated RMS tumors.

Published
2016

26. Temporal order of RNase IIIb and loss-of-function mutations during development determines phenotype in pleuropulmonary blastoma / DICER1 syndrome: a unique variant of the two-hit tumor suppression model

Author

Gretchen M. Williams, Jennifer Ivanovich, Weiying Yu, Anne K. Harris, D. Ashley Hill, Joyce Turner, Christopher T. Rossi, Jiandong Yang, Leslie Doros, Kris Ann P. Schultz, Avi Z. Rosenberg, Paul J. Goodfellow, Amanda Field, Heather Gordish-Dressman, Louis P. Dehner, Mark Brenneman, Yoav H. Messinger, Peter Schoettler, and Douglas R. Stewart

Subjects
0301 basic medicine, Genetics, General Immunology and Microbiology, RNase P, General Medicine, Pleuropulmonary blastoma, Biology, medicine.disease_cause, medicine.disease, General Biochemistry, Genetics and Molecular Biology, Germline, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Germline mutation, 030220 oncology & carcinogenesis, medicine, Missense mutation, General Pharmacology, Toxicology and Pharmaceutics, Allele, Carcinogenesis, DICER1 Syndrome
Abstract

Pleuropulmonary blastoma (PPB) is the most frequent pediatric lung tumor and often the first indication of a pleiotropic cancer predisposition, DICER1 syndrome, comprising a range of other individually rare, benign and malignant tumors of childhood and early adulthood. The genetics of DICER1-associated tumorigenesis are unusual in that tumors typically bear neomorphic missense mutations at one of five specific “hotspot” codons within the RNase IIIb domain of DICER 1, combined with complete loss of function (LOF) in the other allele. We analyzed a cohort of 124 PPB children for predisposing DICER1 mutations and sought correlations with clinical phenotypes. Over 70% have inherited or de novo germline LOF mutations, most of which truncate the DICER1 open reading frame. We identified a minority of patients who have no germline mutation, but are instead mosaic for predisposing DICER1 mutations. Mosaicism for RNase IIIb domain hotspot mutations defines a special category of DICER1 syndrome patients, clinically distinguished from those with germline or mosaic LOF mutations by earlier onsets and numerous discrete foci of neoplastic disease involving multiple syndromic organ sites. A final category of PBB patients lack predisposing germline or mosaic mutations and have sporadic (rather than syndromic) disease limited to a single PPB tumor bearing tumor-specific RNase IIIb and LOF mutations. We propose that acquisition of a neomorphic RNase IIIb domain mutation is the rate limiting event in DICER1-associated tumorigenesis, and that distinct clinical phenotypes associated with mutational categories reflect the temporal order in which LOF and RNase IIIb domain mutations are acquired during development.

Published
2018

27. GENE-18. USE OF PRIMARY TEETH AND A TOOTH BRUSH AS SOURCES OF DNA IN AN ANAPLASTIC ASTROCYTOMA CASE

Author

Javad Nazarian, Miriam Bornhorst, Eshini Panditharatna, Joyce Turner, Sulgi Lee, and Cheng-Ying Ho

Subjects
Cancer Research, Ovarian fibroma, business.industry, Cancer, Dentistry, PTCH1 Gene, medicine.disease, Abstracts, Germline mutation, Oncology, Glioma, medicine, Cancer research, Basal cell carcinoma, Neurology (clinical), business, Exome, Anaplastic astrocytoma
Abstract

BACKGROUND Anaplastic astrocytomas (AA) are aggressive glial cancers with poor prognosis and high recurrence. Although a majority of astrocytomas are sporadic, recent studies have shown that up to 10% of patients with cancer may have an underlying cancer predisposition syndrome. Identification of germline mutations allows for proper management and screening for cancer in patients and their at-risk family members. In this study, we present a unique case of two siblings who developed AA within 8 years of each other. Clinical whole exome testing of our patient’s germline DNA revealed a maternally inherited PTCH2 mutation of unknown significance. The PTCH2 gene is highly homologous to the PTCH1 gene, which is associated with increased risk for basal cell carcinoma, medulloblastoma, rhabdomyoma and ovarian fibroma. However, this has never been described in a glioma before.

Published
2017

28. Temporal order of RNase IIIb and loss-of-function mutations during development determines phenotype in DICER1 syndrome: a unique variant of the two-hit tumor suppression model

Author

Kris Ann P. Schultz, Yoav H. Messinger, Amanda Field, Gretchen M. Williams, Avi Z. Rosenberg, Heather Gordish-Dressman, Paul J. Goodfellow, Louis P. Dehner, Peter Schoettler, D. Ashley Hill, Mark Brenneman, Christopher T. Rossi, Douglas R. Stewart, Jiandong Yang, Weiying Yu, Jennifer Ivanovich, Anne K. Harris, Leslie Doros, and Joyce Turner

Subjects
DICER1 truncation, RNase P, Pleuropulmonary blastoma, Biology, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Germline, Paediatric cancer, Germline mutation, medicine, Missense mutation, General Pharmacology, Toxicology and Pharmaceutics, Allele, DICER1 Syndrome, Genetics, General Immunology and Microbiology, Mosaicism, Lung Cancer, Articles, General Medicine, medicine.disease, Pediatric Oncology, Immunology, RNAse IIIb, Carcinogenesis, PPB, Research Article
Abstract

Pleuropulmonary blastoma (PPB) is the most frequent pediatric lung tumor and often the first indication of a pleiotropic cancer predisposition, DICER1 syndrome, comprising a range of other individually rare, benign and malignant tumors of childhood and early adulthood. The genetics of DICER1-associated tumorigenesis are unusual in that tumors typically bear neomorphic missense mutations at one of five specific “hotspot” codons within the RNase IIIb domain of DICER 1, combined with complete loss of function (LOF) in the other allele. We analyzed a cohort of 124 PPB children for predisposing DICER1 mutations and sought correlations with clinical phenotypes. Over 70% have inherited or de novo germline LOF mutations, most of which truncate the DICER1 open reading frame. We identified a minority of patients who have no germline mutation, but are instead mosaic for predisposing DICER1 mutations. Mosaicism for RNase IIIb domain hotspot mutations defines a special category of DICER1 syndrome patients, clinically distinguished from those with germline or mosaic LOF mutations by earlier onsets and numerous discrete foci of neoplastic disease involving multiple syndromic organ sites. A final category of patients lack predisposing germline or mosaic mutations and have disease limited to a single PPB tumor bearing tumor-specific RNase IIIb and LOF mutations. We propose that acquisition of a neomorphic RNase IIIb domain mutation is the rate limiting event in DICER1-associated tumorigenesis, and that distinct clinical phenotypes associated with mutational categories reflect the temporal order in which LOF and RNase IIIb domain mutations are acquired during development.

Published
2015

29. The DICER1 syndrome: Genotype-phenotype correlation in PPB patients

Author

Joyce Turner, Christopher T. Rossi, Yoav H. Messinger, Leslie Doros, Louis P. Dehner, Douglas R. Stewart, D. Ashley Hill, Gretchen M. Williams, and Kris Ann P. Schultz

Subjects
Cancer Research, Pathology, medicine.medical_specialty, Oncology, business.industry, medicine, Pleuropulmonary blastoma, medicine.disease, business, DICER1 Syndrome, Genotype phenotype
Abstract

10022 Background: Mutations in DICER1 were first described in 2009 from individuals diagnosed with pleuropulmonary blastoma (PPB). Since then, DICER1 mutations have been found in individuals with o...

Published
2015

30. A female with complete lack of Müllerian fusion, postaxial polydactyly, and tetralogy of fallot: genetic heterogeneity of McKusick-Kaufman syndrome or a unique syndrome?

Author

Anne M, Slavotinek, Amalia, Dutra, Dzifa, Kpodzo, Evgenia, Pak, Takaya, Nakane, Joyce, Turner, Margo, Whiteford, Leslie G, Biesecker, and Pamela, Stratton

Subjects
Adult, DNA Mutational Analysis, Chromosomes, Human, Pair 20, Group II Chaperonins, Proteins, Syndrome, Diagnosis, Differential, Cytoskeletal Proteins, Polydactyly, Karyotyping, Mutation, Vagina, Tetralogy of Fallot, Humans, Abnormalities, Multiple, Female, Chromosome Deletion, Bardet-Biedl Syndrome, Microtubule-Associated Proteins, Mullerian Ducts, In Situ Hybridization, Fluorescence, Adaptor Proteins, Signal Transducing, Molecular Chaperones
Abstract

We report a 19-year-old, non-Amish Caucasian female patient with primary amenorrhea caused by complete lack of Müllerian fusion with vaginal agenesis or Müllerian aplasia (MA), postaxial polydactyly (PAP), and tetralogy of Fallot. The genital tract anomaly of MA with and without renal or skeletal anomalies comprises Mayer-Rokitansky-Kuster-Hauser syndrome, which has not been reported with tetralogy of Fallot. The phenotypic triad of anomalies most closely resembled McKusick-Kaufman syndrome (MKS; OMIM 236700), a rare multiple congenital anomaly syndrome comprised of hydrometrocolpos (HMC), PAP, and congenital heart malformation that is inherited in an autosomal recessive pattern. While upper reproductive tract anomalies have not been reported with MKS, they have been reported with Bardet-Biedl syndrome (BBS), a syndrome that significantly overlaps with MKS. Both MKS and BBS can be caused by mutations in the MKKS or BBS6 gene on chromosome 20p12 and BBS is also associated with mutations in other genes (BBS1, BBS2, BBS4, and BBS7). To address this heterogenity, we sequenced the causative genes in MKS and BBS but no mutations in these five genes were identified. Fluorescence in situ hybridization (FISH) excluded large deletions of chromosome 20p12 and microsatellite marker studies confirmed biparental inheritance for all of the known BBS loci. The dual midline fusion defects of tetralogy of Fallot and MA suggests that either this patient has a unique syndrome with a distinct genetic etiology or that she has a genetically heterogeneous or variant form of MKS.

Published
2004

31. Clinical and molecular delineation of the Greig cephalopolysyndactyly contiguous gene deletion syndrome and its distinction from acrocallosal syndrome(Jennifer J. Johnston and Isabelle Olivos-Glander contributed equally to this work.)This article was...

Author

Jennifer J. Johnston, Isabelle Olivos-Glander, Joyce Turner, Kyrieckos Aleck, Lynne M. Bird, Lakshmi Mehta, R. Neil Schimke, Heidi Heilstedt, J. Edward Spence, Jan Blancato, and Leslie G. Biesecker

Subjects
CORPUS callosum, DEVELOPMENTAL disabilities, INTELLECTUAL disabilities, HUMAN abnormalities, PHENOTYPES
Abstract

Greig cephalopolysyndactyly syndrome (GCPS) is caused by haploinsufficiency of GLI3 on 7p13. Features of GCPS include polydactyly, macrocephaly, and hypertelorism, and may be associated with cognitive deficits and abnormalities of the corpus callosum. GLI3 mutations in GCPS patients include point, frameshift, translocation, and gross deletion mutations. FISH and STRP analyses were applied to 34 patients with characteristics of GCPS. Deletions were identified in 11 patients and the extent of their deletion was determined. Nine patients with deletions had mental retardation (MR) or developmental delay (DD) and were classified as severe GCPS. These severe GCPS patients have manifestations that overlap with the acrocallosal syndrome (ACLS). The deletion breakpoints were analyzed in six patients whose deletions ranged in size from 151 kb to 10.6 Mb. Junction fragments were found to be distinct with no common sequences flanking the breakpoints. We conclude that patients with GCPS caused by large deletions that include GLI3 are likely to have cognitive deficits, and we hypothesize that this severe GCPS phenotype is caused by deletion of contiguous genes. © 2003 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published
2003
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