Somatic mutations in DROSHA and DICER1 impair microRNA biogenesis through distinct mechanisms in Wilms tumours

Dinesh Rakheja; Kenneth Chen; Yangjian Liu; Abhay A. Shukla; Vanessa Schmid; Tsung-Cheng Chang; Shama Khokhar; Jonathan E Wickiser; Nitin J. Karandikar; James S Malter; Joshua T Mendell; James F Amatruda

doi:10.1038/ncomms5802

Somatic mutations in DROSHA and DICER1 impair microRNA biogenesis through distinct mechanisms in Wilms tumours

Dinesh Rakheja, Kenneth Chen, Yangjian Liu, Abhay A. Shukla, Vanessa Schmid, Tsung-Cheng Chang, Shama Khokhar, Jonathan E Wickiser, Nitin J. Karandikar, James S Malter, Joshua T Mendell, James F Amatruda

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Abstract

Wilms tumour is the most common childhood kidney cancer. Here we report the whole-exome sequencing of 44 Wilms tumours, identifying missense mutations in the microRNA (miRNA)-processing enzymes DROSHA and DICER1, and novel mutations in MYCN, SMARCA4 and ARID1A. Examination of tumour miRNA expression, in vitro processing assays and genomic editing in human cells demonstrates that DICER1 and DROSHA mutations influence miRNA processing through distinct mechanisms. DICER1 RNase IIIB mutations preferentially impair processing of miRNAs deriving from the 5 2-arm of pre-miRNA hairpins, while DROSHA RNase IIIB mutations globally inhibit miRNA biogenesis through a dominant-negative mechanism. Both DROSHA and DICER1 mutations impair expression of tumour-suppressing miRNAs, including the let-7 family, important regulators of MYCN, LIN28 and other Wilms tumour oncogenes. These results provide new insights into the mechanisms through which mutations in miRNA biogenesis components reprogramme miRNA expression in human cancer and suggest that these defects define a distinct subclass of Wilms tumours.

Original language	English (US)
Article number	4802
Journal	Nature communications
Volume	2
DOIs	https://doi.org/10.1038/ncomms5802
State	Published - Sep 5 2014

ASJC Scopus subject areas

Chemistry(all)
Biochemistry, Genetics and Molecular Biology(all)
Physics and Astronomy(all)

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@article{4287db155bb24af9af89c0df28788171,

title = "Somatic mutations in DROSHA and DICER1 impair microRNA biogenesis through distinct mechanisms in Wilms tumours",

abstract = "Wilms tumour is the most common childhood kidney cancer. Here we report the whole-exome sequencing of 44 Wilms tumours, identifying missense mutations in the microRNA (miRNA)-processing enzymes DROSHA and DICER1, and novel mutations in MYCN, SMARCA4 and ARID1A. Examination of tumour miRNA expression, in vitro processing assays and genomic editing in human cells demonstrates that DICER1 and DROSHA mutations influence miRNA processing through distinct mechanisms. DICER1 RNase IIIB mutations preferentially impair processing of miRNAs deriving from the 5 2-arm of pre-miRNA hairpins, while DROSHA RNase IIIB mutations globally inhibit miRNA biogenesis through a dominant-negative mechanism. Both DROSHA and DICER1 mutations impair expression of tumour-suppressing miRNAs, including the let-7 family, important regulators of MYCN, LIN28 and other Wilms tumour oncogenes. These results provide new insights into the mechanisms through which mutations in miRNA biogenesis components reprogramme miRNA expression in human cancer and suggest that these defects define a distinct subclass of Wilms tumours.",

author = "Dinesh Rakheja and Kenneth Chen and Yangjian Liu and Shukla, {Abhay A.} and Vanessa Schmid and Tsung-Cheng Chang and Shama Khokhar and Wickiser, {Jonathan E} and Karandikar, {Nitin J.} and Malter, {James S} and Mendell, {Joshua T} and Amatruda, {James F}",

note = "Funding Information: We acknowledge patients and families who participated in this study. We thank Thomas Tuschl and V. Narry Kim for providing expression constructs, Eric Olson and Stephen Skapek for helpful comments on the manuscript, and Jose Cabrera for assistance with figures. This study was supported by grants from the Children{\textquoteright}s Medical Center Foundation, Dallas, TX, and a Young Investigator Research Grant from the Society for Pediatric Pathology (to D.R.); from NIH (R01CA120185 and P01CA134292 to J.T.M.; R01CA135731 to J.F.A.); and the Cancer Prevention and Research Institute of Texas (R1008 to J.T.M. and RP110394 to J.F.A.). K.S.C. is a Damon Runyon-Sohn Pediatric Fellow supported by the Damon Runyon Cancer Research Foundation (DRSG-4P-13) and is also supported by the Children{\textquoteright}s Medical Center Foundation and Physician Scientist Oncology T32 Training Grant 5T32CA136515-03 to the UT Southwestern Harold C. Simmons Comprehensive Cancer Center. Publisher Copyright: {\textcopyright} 2014 Macmillan Publishers Limited. All rights reserved.",

year = "2014",

month = sep,

day = "5",

doi = "10.1038/ncomms5802",

language = "English (US)",

volume = "2",

journal = "Nature Communications",

issn = "2041-1723",

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TY - JOUR

T1 - Somatic mutations in DROSHA and DICER1 impair microRNA biogenesis through distinct mechanisms in Wilms tumours

AU - Rakheja, Dinesh

AU - Chen, Kenneth

AU - Liu, Yangjian

AU - Shukla, Abhay A.

AU - Schmid, Vanessa

AU - Chang, Tsung-Cheng

AU - Khokhar, Shama

AU - Wickiser, Jonathan E

AU - Karandikar, Nitin J.

AU - Malter, James S

AU - Mendell, Joshua T

AU - Amatruda, James F

N1 - Funding Information: We acknowledge patients and families who participated in this study. We thank Thomas Tuschl and V. Narry Kim for providing expression constructs, Eric Olson and Stephen Skapek for helpful comments on the manuscript, and Jose Cabrera for assistance with figures. This study was supported by grants from the Children’s Medical Center Foundation, Dallas, TX, and a Young Investigator Research Grant from the Society for Pediatric Pathology (to D.R.); from NIH (R01CA120185 and P01CA134292 to J.T.M.; R01CA135731 to J.F.A.); and the Cancer Prevention and Research Institute of Texas (R1008 to J.T.M. and RP110394 to J.F.A.). K.S.C. is a Damon Runyon-Sohn Pediatric Fellow supported by the Damon Runyon Cancer Research Foundation (DRSG-4P-13) and is also supported by the Children’s Medical Center Foundation and Physician Scientist Oncology T32 Training Grant 5T32CA136515-03 to the UT Southwestern Harold C. Simmons Comprehensive Cancer Center. Publisher Copyright: © 2014 Macmillan Publishers Limited. All rights reserved.

PY - 2014/9/5

Y1 - 2014/9/5

N2 - Wilms tumour is the most common childhood kidney cancer. Here we report the whole-exome sequencing of 44 Wilms tumours, identifying missense mutations in the microRNA (miRNA)-processing enzymes DROSHA and DICER1, and novel mutations in MYCN, SMARCA4 and ARID1A. Examination of tumour miRNA expression, in vitro processing assays and genomic editing in human cells demonstrates that DICER1 and DROSHA mutations influence miRNA processing through distinct mechanisms. DICER1 RNase IIIB mutations preferentially impair processing of miRNAs deriving from the 5 2-arm of pre-miRNA hairpins, while DROSHA RNase IIIB mutations globally inhibit miRNA biogenesis through a dominant-negative mechanism. Both DROSHA and DICER1 mutations impair expression of tumour-suppressing miRNAs, including the let-7 family, important regulators of MYCN, LIN28 and other Wilms tumour oncogenes. These results provide new insights into the mechanisms through which mutations in miRNA biogenesis components reprogramme miRNA expression in human cancer and suggest that these defects define a distinct subclass of Wilms tumours.

AB - Wilms tumour is the most common childhood kidney cancer. Here we report the whole-exome sequencing of 44 Wilms tumours, identifying missense mutations in the microRNA (miRNA)-processing enzymes DROSHA and DICER1, and novel mutations in MYCN, SMARCA4 and ARID1A. Examination of tumour miRNA expression, in vitro processing assays and genomic editing in human cells demonstrates that DICER1 and DROSHA mutations influence miRNA processing through distinct mechanisms. DICER1 RNase IIIB mutations preferentially impair processing of miRNAs deriving from the 5 2-arm of pre-miRNA hairpins, while DROSHA RNase IIIB mutations globally inhibit miRNA biogenesis through a dominant-negative mechanism. Both DROSHA and DICER1 mutations impair expression of tumour-suppressing miRNAs, including the let-7 family, important regulators of MYCN, LIN28 and other Wilms tumour oncogenes. These results provide new insights into the mechanisms through which mutations in miRNA biogenesis components reprogramme miRNA expression in human cancer and suggest that these defects define a distinct subclass of Wilms tumours.

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U2 - 10.1038/ncomms5802

DO - 10.1038/ncomms5802

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SN - 2041-1723

VL - 2

JO - Nature Communications

JF - Nature Communications

M1 - 4802

ER -

Somatic mutations in DROSHA and DICER1 impair microRNA biogenesis through distinct mechanisms in Wilms tumours

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