Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs

Dereje D. Jima; Jenny Zhang; Cassandra Jacobs; Kristy L. Richards; Cherie H. Dunphy; William W.L. Choi; Wing Yan Au; Gopesh Srivastava; Magdalena B. Czader; David A. Rizzieri; Anand S. Lagoo; Patricia L. Lugar; Karen P. Mann; Christopher R. Flowers; Leon Bernal-Mizrachi; Kikkeri N. Naresh; Andrew M. Evens; Leo I. Gordon; Micah Luftig; Daphne R. Friedman; J. Brice Weinberg; Michael A. Thompson; Javed I. Gill; Qingquan Liu; Tam How; Vladimir Grubor; Yuan Gao; Amee Patel; Han Wu; Jun Zhu; Gerard C. Blobe; Peter E. Lipsky; Amy Chadburn; Sandeep S. Dave

doi:10.1182/blood-2010-05-285403

Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs

Dereje D. Jima, Jenny Zhang, Cassandra Jacobs, Kristy L. Richards, Cherie H. Dunphy, William W.L. Choi, Wing Yan Au, Gopesh Srivastava, Magdalena B. Czader, David A. Rizzieri, Anand S. Lagoo, Patricia L. Lugar, Karen P. Mann, Christopher R. Flowers, Leon Bernal-Mizrachi, Kikkeri N. Naresh, Andrew M. Evens, Leo I. Gordon, Micah Luftig, Daphne R. FriedmanJ. Brice Weinberg, Michael A. Thompson, Javed I. Gill, Qingquan Liu, Tam How, Vladimir Grubor, Yuan Gao, Amee Patel, Han Wu, Jun Zhu, Gerard C. Blobe, Peter E. Lipsky, Amy Chadburn, Sandeep S. Dave

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

182 Scopus citations

Abstract

A role for microRNA (miRNA) has been recognized in nearly every biologic system examined thus far. A complete delineation of their role must be preceded by the identification of all miRNAs present in any system. We elucidated the complete small RNA transcriptome of normal and malignant B cells through deep sequencing of 31 normal and malignant human B-cell samples that comprise the spectrum of B-cell differentiation and common malignant phenotypes. We identified the expression of 333 known miRNAs, which is more than twice the number previously recognized in any tissue type. We further identified the expression of 286 candidate novel miRNAs in normal and malignant B cells. These miRNAs were validated at a high rate (92%) using quantitative polymerase chain reaction, and we demonstrated their application in the distinction of clinically relevant subgroups of lymphoma. We further demonstrated that a novel miRNA cluster, previously annotated as a hypothetical gene LOC100130622, contains 6 novel miRNAs that regulate the transforming growth factor-β pathway. Thus, our work suggests that more than a third of the miRNAs present in most cellular types are currently unknown and that these miRNAs may regulate important cellular functions.

Original language	English (US)
Pages (from-to)	e118-e127
Journal	Blood
Volume	116
Issue number	23
DOIs	https://doi.org/10.1182/blood-2010-05-285403
State	Published - Dec 2 2010
Externally published	Yes

ASJC Scopus subject areas

Biochemistry
Immunology
Hematology
Cell Biology

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Jima, D. D., Zhang, J., Jacobs, C., Richards, K. L., Dunphy, C. H., Choi, W. W. L., Au, W. Y., Srivastava, G., Czader, M. B., Rizzieri, D. A., Lagoo, A. S., Lugar, P. L., Mann, K. P., Flowers, C. R., Bernal-Mizrachi, L., Naresh, K. N., Evens, A. M., Gordon, L. I., Luftig, M., ... Dave, S. S. (2010). Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs. Blood, 116(23), e118-e127. https://doi.org/10.1182/blood-2010-05-285403

Jima, DD, Zhang, J, Jacobs, C, Richards, KL, Dunphy, CH, Choi, WWL, Au, WY, Srivastava, G, Czader, MB, Rizzieri, DA, Lagoo, AS, Lugar, PL, Mann, KP, Flowers, CR, Bernal-Mizrachi, L, Naresh, KN, Evens, AM, Gordon, LI, Luftig, M, Friedman, DR, Weinberg, JB, Thompson, MA, Gill, JI, Liu, Q, How, T, Grubor, V, Gao, Y, Patel, A, Wu, H, Zhu, J, Blobe, GC, Lipsky, PE, Chadburn, A & Dave, SS 2010, 'Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs', Blood, vol. 116, no. 23, pp. e118-e127. https://doi.org/10.1182/blood-2010-05-285403

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title = "Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs",

abstract = "A role for microRNA (miRNA) has been recognized in nearly every biologic system examined thus far. A complete delineation of their role must be preceded by the identification of all miRNAs present in any system. We elucidated the complete small RNA transcriptome of normal and malignant B cells through deep sequencing of 31 normal and malignant human B-cell samples that comprise the spectrum of B-cell differentiation and common malignant phenotypes. We identified the expression of 333 known miRNAs, which is more than twice the number previously recognized in any tissue type. We further identified the expression of 286 candidate novel miRNAs in normal and malignant B cells. These miRNAs were validated at a high rate (92%) using quantitative polymerase chain reaction, and we demonstrated their application in the distinction of clinically relevant subgroups of lymphoma. We further demonstrated that a novel miRNA cluster, previously annotated as a hypothetical gene LOC100130622, contains 6 novel miRNAs that regulate the transforming growth factor-β pathway. Thus, our work suggests that more than a third of the miRNAs present in most cellular types are currently unknown and that these miRNAs may regulate important cellular functions.",

author = "Jima, {Dereje D.} and Jenny Zhang and Cassandra Jacobs and Richards, {Kristy L.} and Dunphy, {Cherie H.} and Choi, {William W.L.} and Au, {Wing Yan} and Gopesh Srivastava and Czader, {Magdalena B.} and Rizzieri, {David A.} and Lagoo, {Anand S.} and Lugar, {Patricia L.} and Mann, {Karen P.} and Flowers, {Christopher R.} and Leon Bernal-Mizrachi and Naresh, {Kikkeri N.} and Evens, {Andrew M.} and Gordon, {Leo I.} and Micah Luftig and Friedman, {Daphne R.} and Weinberg, {J. Brice} and Thompson, {Michael A.} and Gill, {Javed I.} and Qingquan Liu and Tam How and Vladimir Grubor and Yuan Gao and Amee Patel and Han Wu and Jun Zhu and Blobe, {Gerard C.} and Lipsky, {Peter E.} and Amy Chadburn and Dave, {Sandeep S.}",

year = "2010",

month = dec,

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doi = "10.1182/blood-2010-05-285403",

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T1 - Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs

AU - Jima, Dereje D.

AU - Zhang, Jenny

AU - Jacobs, Cassandra

AU - Richards, Kristy L.

AU - Dunphy, Cherie H.

AU - Choi, William W.L.

AU - Au, Wing Yan

AU - Srivastava, Gopesh

AU - Czader, Magdalena B.

AU - Rizzieri, David A.

AU - Lagoo, Anand S.

AU - Lugar, Patricia L.

AU - Mann, Karen P.

AU - Flowers, Christopher R.

AU - Bernal-Mizrachi, Leon

AU - Naresh, Kikkeri N.

AU - Evens, Andrew M.

AU - Gordon, Leo I.

AU - Luftig, Micah

AU - Friedman, Daphne R.

AU - Weinberg, J. Brice

AU - Thompson, Michael A.

AU - Gill, Javed I.

AU - Liu, Qingquan

AU - How, Tam

AU - Grubor, Vladimir

AU - Gao, Yuan

AU - Patel, Amee

AU - Wu, Han

AU - Zhu, Jun

AU - Blobe, Gerard C.

AU - Lipsky, Peter E.

AU - Chadburn, Amy

AU - Dave, Sandeep S.

PY - 2010/12/2

Y1 - 2010/12/2

N2 - A role for microRNA (miRNA) has been recognized in nearly every biologic system examined thus far. A complete delineation of their role must be preceded by the identification of all miRNAs present in any system. We elucidated the complete small RNA transcriptome of normal and malignant B cells through deep sequencing of 31 normal and malignant human B-cell samples that comprise the spectrum of B-cell differentiation and common malignant phenotypes. We identified the expression of 333 known miRNAs, which is more than twice the number previously recognized in any tissue type. We further identified the expression of 286 candidate novel miRNAs in normal and malignant B cells. These miRNAs were validated at a high rate (92%) using quantitative polymerase chain reaction, and we demonstrated their application in the distinction of clinically relevant subgroups of lymphoma. We further demonstrated that a novel miRNA cluster, previously annotated as a hypothetical gene LOC100130622, contains 6 novel miRNAs that regulate the transforming growth factor-β pathway. Thus, our work suggests that more than a third of the miRNAs present in most cellular types are currently unknown and that these miRNAs may regulate important cellular functions.

AB - A role for microRNA (miRNA) has been recognized in nearly every biologic system examined thus far. A complete delineation of their role must be preceded by the identification of all miRNAs present in any system. We elucidated the complete small RNA transcriptome of normal and malignant B cells through deep sequencing of 31 normal and malignant human B-cell samples that comprise the spectrum of B-cell differentiation and common malignant phenotypes. We identified the expression of 333 known miRNAs, which is more than twice the number previously recognized in any tissue type. We further identified the expression of 286 candidate novel miRNAs in normal and malignant B cells. These miRNAs were validated at a high rate (92%) using quantitative polymerase chain reaction, and we demonstrated their application in the distinction of clinically relevant subgroups of lymphoma. We further demonstrated that a novel miRNA cluster, previously annotated as a hypothetical gene LOC100130622, contains 6 novel miRNAs that regulate the transforming growth factor-β pathway. Thus, our work suggests that more than a third of the miRNAs present in most cellular types are currently unknown and that these miRNAs may regulate important cellular functions.

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SP - e118-e127

JO - Blood

JF - Blood

IS - 23

ER -

Deep sequencing of the small RNA transcriptome of normal and malignant human B cells identifies hundreds of novel microRNAs

Abstract

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