Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia

Apollinaire Ngankeu; Parvathi Ranganathan; Violaine Havelange; Deedra Nicolet; Stefano Volinia; Bayard L. Powell; Jonathan E. Kolitz; Geoffrey L. Uy; Richard M. Stone; Steven M. Kornblau; Michael Andreeff; Carlo M. Croce; Clara D. Bloomfield; Ramiro Garzon

doi:10.18632/oncotarget.23150

Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia

Apollinaire Ngankeu, Parvathi Ranganathan, Violaine Havelange, Deedra Nicolet, Stefano Volinia, Bayard L. Powell, Jonathan E. Kolitz, Geoffrey L. Uy, Richard M. Stone, Steven M. Kornblau, Michael Andreeff, Carlo M. Croce, Clara D. Bloomfield, Ramiro Garzon

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

We previously reported that microRNA (miR)-29b is down-regulated and has a tumor suppressor role in acute myeloid leukemia (AML). However, little is known about the mechanisms responsible for miR-29b expression downregulation in AML. In this work we screened for mutations that could affect miR-29b expression. Using Sanger sequencing, we identified a germline thymidine (T) base deletion within the miR-29b-1/miR-29a cluster precursor in 16% of AML patients. Remarkably we found a significant enrichment for the presence of the miR-29 polymorphism in core binding factor (CBF) newly diagnosed AML patients (n = 61/303; 20%) with respect to age, sex and race matched controls (n = 43/402:11%, P < 0.01). Mechanistically, this polymorphism affects the expression ratio of mature miR-29b and miR-29a by dampening the processing of miR-29a. RNA immunoprecipitation assays showed reduced DROSHA binding capacity to the polymorphism with respect to the controls. Finally, we showed that this polymorphism negatively impacts the ability of miR- 29b-1/miR-29a cluster to target MCL-1 and CDK6, both known miR-29 targets.

Original language	English (US)
Pages (from-to)	4354-4365
Number of pages	12
Journal	Oncotarget
Volume	9
Issue number	4
DOIs	https://doi.org/10.18632/oncotarget.23150
State	Published - 2018
Externally published	Yes

Keywords

AML
Polymorphism
miR-29b-1/miR-29a cluster

ASJC Scopus subject areas

Oncology

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Ngankeu, A., Ranganathan, P., Havelange, V., Nicolet, D., Volinia, S., Powell, B. L., Kolitz, J. E., Uy, G. L., Stone, R. M., Kornblau, S. M., Andreeff, M., Croce, C. M., Bloomfield, C. D., & Garzon, R. (2018). Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia. Oncotarget, 9(4), 4354-4365. https://doi.org/10.18632/oncotarget.23150

Ngankeu, A, Ranganathan, P, Havelange, V, Nicolet, D, Volinia, S, Powell, BL, Kolitz, JE, Uy, GL, Stone, RM, Kornblau, SM , Andreeff, M, Croce, CM, Bloomfield, CD & Garzon, R 2018, 'Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia', Oncotarget, vol. 9, no. 4, pp. 4354-4365. https://doi.org/10.18632/oncotarget.23150

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title = "Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia",

abstract = "We previously reported that microRNA (miR)-29b is down-regulated and has a tumor suppressor role in acute myeloid leukemia (AML). However, little is known about the mechanisms responsible for miR-29b expression downregulation in AML. In this work we screened for mutations that could affect miR-29b expression. Using Sanger sequencing, we identified a germline thymidine (T) base deletion within the miR-29b-1/miR-29a cluster precursor in 16% of AML patients. Remarkably we found a significant enrichment for the presence of the miR-29 polymorphism in core binding factor (CBF) newly diagnosed AML patients (n = 61/303; 20%) with respect to age, sex and race matched controls (n = 43/402:11%, P < 0.01). Mechanistically, this polymorphism affects the expression ratio of mature miR-29b and miR-29a by dampening the processing of miR-29a. RNA immunoprecipitation assays showed reduced DROSHA binding capacity to the polymorphism with respect to the controls. Finally, we showed that this polymorphism negatively impacts the ability of miR- 29b-1/miR-29a cluster to target MCL-1 and CDK6, both known miR-29 targets.",

keywords = "AML, Polymorphism, miR-29b-1/miR-29a cluster",

author = "Apollinaire Ngankeu and Parvathi Ranganathan and Violaine Havelange and Deedra Nicolet and Stefano Volinia and Powell, {Bayard L.} and Kolitz, {Jonathan E.} and Uy, {Geoffrey L.} and Stone, {Richard M.} and Kornblau, {Steven M.} and Michael Andreeff and Croce, {Carlo M.} and Bloomfield, {Clara D.} and Ramiro Garzon",

note = "Funding Information: We thank Donna Bucci for assistance with primary AML samples handling. This work was supported by the National Institute of Health grants P01CA055164. The Publisher Copyright: {\textcopyright} Ngankeu et al.",

year = "2018",

doi = "10.18632/oncotarget.23150",

language = "English (US)",

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T1 - Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia

AU - Ngankeu, Apollinaire

AU - Ranganathan, Parvathi

AU - Havelange, Violaine

AU - Nicolet, Deedra

AU - Volinia, Stefano

AU - Powell, Bayard L.

AU - Kolitz, Jonathan E.

AU - Uy, Geoffrey L.

AU - Stone, Richard M.

AU - Kornblau, Steven M.

AU - Andreeff, Michael

AU - Croce, Carlo M.

AU - Bloomfield, Clara D.

AU - Garzon, Ramiro

N1 - Funding Information: We thank Donna Bucci for assistance with primary AML samples handling. This work was supported by the National Institute of Health grants P01CA055164. The Publisher Copyright: © Ngankeu et al.

PY - 2018

Y1 - 2018

N2 - We previously reported that microRNA (miR)-29b is down-regulated and has a tumor suppressor role in acute myeloid leukemia (AML). However, little is known about the mechanisms responsible for miR-29b expression downregulation in AML. In this work we screened for mutations that could affect miR-29b expression. Using Sanger sequencing, we identified a germline thymidine (T) base deletion within the miR-29b-1/miR-29a cluster precursor in 16% of AML patients. Remarkably we found a significant enrichment for the presence of the miR-29 polymorphism in core binding factor (CBF) newly diagnosed AML patients (n = 61/303; 20%) with respect to age, sex and race matched controls (n = 43/402:11%, P < 0.01). Mechanistically, this polymorphism affects the expression ratio of mature miR-29b and miR-29a by dampening the processing of miR-29a. RNA immunoprecipitation assays showed reduced DROSHA binding capacity to the polymorphism with respect to the controls. Finally, we showed that this polymorphism negatively impacts the ability of miR- 29b-1/miR-29a cluster to target MCL-1 and CDK6, both known miR-29 targets.

AB - We previously reported that microRNA (miR)-29b is down-regulated and has a tumor suppressor role in acute myeloid leukemia (AML). However, little is known about the mechanisms responsible for miR-29b expression downregulation in AML. In this work we screened for mutations that could affect miR-29b expression. Using Sanger sequencing, we identified a germline thymidine (T) base deletion within the miR-29b-1/miR-29a cluster precursor in 16% of AML patients. Remarkably we found a significant enrichment for the presence of the miR-29 polymorphism in core binding factor (CBF) newly diagnosed AML patients (n = 61/303; 20%) with respect to age, sex and race matched controls (n = 43/402:11%, P < 0.01). Mechanistically, this polymorphism affects the expression ratio of mature miR-29b and miR-29a by dampening the processing of miR-29a. RNA immunoprecipitation assays showed reduced DROSHA binding capacity to the polymorphism with respect to the controls. Finally, we showed that this polymorphism negatively impacts the ability of miR- 29b-1/miR-29a cluster to target MCL-1 and CDK6, both known miR-29 targets.

KW - AML

KW - Polymorphism

KW - miR-29b-1/miR-29a cluster

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Discovery and functional implications of a miR-29b-1/miR-29a cluster polymorphism in acute myeloid leukemia

Abstract

Keywords

ASJC Scopus subject areas

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