<i>DICER1</i> and Associated Conditions: Identification of At-risk Individuals and Recommended Surveillance Strategies

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

doi:10.1158/1078-0432.ccr-17-3089

Cited by 303 publications

(369 citation statements)

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“…In families afflicted with tumor predisposition syndromes, determining the specific genetic defect in affected individuals and then screening for additional at‐risk family members is key to timely implementation of appropriate surveillance and treatment protocols. Standardized screening regimens are still being developed for DICER1 syndrome, but recommended strategies are emerging (Schultz et al, ). Some of the considerations for such strategies include the risk for development of DICER1 tumors being highest in early childhood and waning into adulthood, and that the DICER1 phenotypes vary widely in terms of rarity, age range of onset, severity, rapidity of development, means of detection, and effectiveness of early detection.…”

Section: Variant Impact and Clinical Relevancementioning

confidence: 99%

“…PPB, which is most often diagnosed before age 6 years, is plausibly the greatest threat to patient well‐being, particularly Types II and III which have 5‐year overall survival rates of 71% and 53%, respectively (Messinger et al, ). As such, and given the possible progression of some of the tumor types to fulminant disease (including cystic PPB to the solid variants, and possibly, more rarely, MNG to DTC, and pCN to anaplastic sarcoma of the kidney), it is advised that identification and screening of DICER1 pathogenic variant heterozygotes be implemented as early as possible with the aim of detecting precancerous or lower‐stage lesions that may be more amendable to treatment (Schultz et al, ; van Engelen et al, ). Timely counseling, genetic testing, and accurate variant classification are therefore of significant clinical importance.…”

Section: Variant Impact and Clinical Relevancementioning

confidence: 99%

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Ten years of DICER1 mutations: Provenance, distribution, and associated phenotypes

2019

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DICER1 syndrome is a pleiotropic tumor predisposition syndrome characterized by a distinctive constellation of neoplastic and dysplastic lesions, which are generally rare and affect children and young adults. Germline pathogenic variants in the DICER1 gene are the underlying cause of the syndrome; variants are typically inherited in an autosomal dominant pattern but may arise de novo in the germline or in a somatic mosaic distribution. The encoded DICER1 protein is a key component of the microRNA processing pathway. In this Mutation Update, we present a comprehensive review of all DICER1 genetic alterations reported in articles published before January 31st, 2019. A total of 1,136 DICER1 alterations were catalogued from 808 individuals and the tumors that occurred in these persons. We provide an inventory of these DICER1 alterations and discuss them with respect to their provenance, distribution across the gene, associated phenotypes and ages of onset, and penetrance. We also address approaches to classification of DICER1 variants of uncertain significance and discuss the clinical significance of DICER1 variant identification.

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Section: Variant Impact and Clinical Relevancementioning

confidence: 99%

Section: Variant Impact and Clinical Relevancementioning

confidence: 99%

Ten years of DICER1 mutations: Provenance, distribution, and associated phenotypes

2019

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“…Another series has reported pleomorphic differentiation with prominent eosinophilic cytoplasmic globules . Interestingly, among two infants with posterior‐fossa embryonal tumors, one had chondroid differentiation, which has been described in DICER1‐associated extracranial tumors such as nasal chondromesenchymal hamartoma, RMS, and renal anaplastic sarcoma …”

mentioning

confidence: 88%

“…To the Editor: Pediatric intracranial sarcomas are rare tumors with poor prognoses . Mutations in the DICER1 gene on chromosome 4, which encodes a RNase‐IIIb endonuclease involved in microRNA processing and thereby controlling gene expression, has recently been reported to be associated with intracranial spindle‐cell sarcomas with rhabdomyosarcoma (RMS)‐like features . We describe the multimodal management of a case with germline DICER1 mutation and pulmonary metastases.…”

mentioning

confidence: 99%

“…DICER1 syndrome, classically associated with pleuropulmonary blastoma, is an autosomal‐dominant condition with reduced penetrance, increasingly being recognized as predisposing to benign and malignant neoplasms, including CNS tumors such as pinealoblastoma, pituitary blastoma, and ciliary‐body medulloepithelioma, and genitourinary sarcomas . Recently, a group of DICER1‐mutant pediatric intracranial sarcomas were described, which are histologically heterogeneous, but homogeneous at the molecular level, with a characteristic methylation profile .…”

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confidence: 99%

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Germline DICER1‐mutant intracranial sarcoma with dual chondroid and spindle cell morphology and pulmonary metastases treated with multimodal therapy

Das

Roy

Modi

et al. 2019

Pediatric Blood & Cancer

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A Genome-First Approach to Characterize DICER1 Pathogenic Variant Prevalence, Penetrance, and Phenotype

et al. 2021

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Key Points Question What are the prevalence, risk, and phenotypic spectrum of individuals with a germline putative loss-of-function (pLOF) variant in DICER1 according to a genome-first approach in a population-scale cohort? Findings In this cohort study, DICER1 pLOF variants were more than twice as common (even after adjustment for relatedness) than previously observed. Malignant tumors were observed in 16% of participants with a DICER1 pLOF variant, which is comparable to the frequency of neoplasms in the largest phenotype-first DICER1 studies published to date. Meaning The genome-first approach complements more traditional approaches to syndrome delineation and may be an efficient approach for risk estimation in monogenic disorders.

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DICER1 and Associated Conditions: Identification of At-risk Individuals and Recommended Surveillance Strategies

Cited by 303 publications

References 58 publications

Ten years of DICER1 mutations: Provenance, distribution, and associated phenotypes

Ten years of DICER1 mutations: Provenance, distribution, and associated phenotypes

Germline DICER1‐mutant intracranial sarcoma with dual chondroid and spindle cell morphology and pulmonary metastases treated with multimodal therapy

A Genome-First Approach to Characterize DICER1 Pathogenic Variant Prevalence, Penetrance, and Phenotype

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