HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia

Jong Ho Park; Young Min Woo; Emilia Moonkyung Youm; Nada Hamad; Hong Hee Won; Kazuhito Naka; Eun Ju Park; June Hee Park; Hee Jin Kim; Sun Hee Kim; Hyeoung Joon Kim; Jae Sook Ahn; Sang Kyun Sohn; Joon Ho Moon; Chul Won Jung; Silvia Park; Jeffrey H. Lipton; Shinya Kimura; Jong Won Kim; Dennis (Dong Hwan) Kim

doi:10.1038/s41375-018-0321-8

HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia

Jong Ho Park, Young Min Woo, Emilia Moonkyung Youm, Nada Hamad, Hong Hee Won, Kazuhito Naka, Eun Ju Park, June Hee Park, Hee Jin Kim, Sun Hee Kim, Hyeoung Joon Kim, Jae Sook Ahn, Sang Kyun Sohn, Joon Ho Moon, Chul Won Jung, Silvia Park, Jeffrey H. Lipton, Shinya Kimura, Jong Won Kim, Dennis (Dong Hwan) Kim

Department of Internal Medicine

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

17 Scopus citations

Abstract

Achieving a deep molecular response (DMR) to tyrosine kinase inhibitor (TKI) therapy for chronic myeloid leukemia (CML) remains challenging and at present, there is no biomarker to predict DMR in this setting. Herein, we report that an HMGCLL1 genetic variant located in 6p12.1 can be used as a predictive genetic biomarker for intrinsic sensitivity to imatinib (IM) therapy. We measured DMR rate according to HMGCLL1 variant in a discovery set of CML patients (n = 201) and successfully replicated it in a validation set (n = 270). We also investigated the functional relevance of HMGCLL1 blockade with respect to response to TKI therapy and showed that small interfering RNA mediated blockade of HMGCLL1 isoform 3 results in significant decrease in viability of BCR-ABL1-positive cells including K562, CML-T1 or BaF3 cell lines with or without ABL1 kinase domain mutations such as T315I mutation. Decreased cell viability was also demonstrated in murine CML stem cells and human hematopoietic progenitor cells. RNA sequencing showed that blockade of HMGCLL1 was associated with G0/G1 arrest and the cell cycle. In summary, the HMGCLL1 gene polymorphism is a novel genetic biomarker for intrinsic sensitivity to IM therapy in CML patients that predicts DMR in this setting.

Original language	English
Pages (from-to)	1439-1450
Number of pages	12
Journal	Leukemia
Volume	33
Issue number	6
DOIs	https://doi.org/10.1038/s41375-018-0321-8
State	Published - 1 Jun 2019

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© 2018, Springer Nature Limited.

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Park, J. H., Woo, Y. M., Youm, E. M., Hamad, N., Won, H. H., Naka, K., Park, E. J., Park, J. H., Kim, H. J., Kim, S. H., Kim, H. J., Ahn, J. S., Sohn, S. K., Moon, J. H., Jung, C. W., Park, S., Lipton, J. H., Kimura, S., Kim, J. W., & Kim, D. (2019). HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia. Leukemia, 33(6), 1439-1450. https://doi.org/10.1038/s41375-018-0321-8

@article{a7d08fcc879c49a6b0883450531e5215,

title = "HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia",

abstract = "Achieving a deep molecular response (DMR) to tyrosine kinase inhibitor (TKI) therapy for chronic myeloid leukemia (CML) remains challenging and at present, there is no biomarker to predict DMR in this setting. Herein, we report that an HMGCLL1 genetic variant located in 6p12.1 can be used as a predictive genetic biomarker for intrinsic sensitivity to imatinib (IM) therapy. We measured DMR rate according to HMGCLL1 variant in a discovery set of CML patients (n = 201) and successfully replicated it in a validation set (n = 270). We also investigated the functional relevance of HMGCLL1 blockade with respect to response to TKI therapy and showed that small interfering RNA mediated blockade of HMGCLL1 isoform 3 results in significant decrease in viability of BCR-ABL1-positive cells including K562, CML-T1 or BaF3 cell lines with or without ABL1 kinase domain mutations such as T315I mutation. Decreased cell viability was also demonstrated in murine CML stem cells and human hematopoietic progenitor cells. RNA sequencing showed that blockade of HMGCLL1 was associated with G0/G1 arrest and the cell cycle. In summary, the HMGCLL1 gene polymorphism is a novel genetic biomarker for intrinsic sensitivity to IM therapy in CML patients that predicts DMR in this setting.",

author = "Park, {Jong Ho} and Woo, {Young Min} and Youm, {Emilia Moonkyung} and Nada Hamad and Won, {Hong Hee} and Kazuhito Naka and Park, {Eun Ju} and Park, {June Hee} and Kim, {Hee Jin} and Kim, {Sun Hee} and Kim, {Hyeoung Joon} and Ahn, {Jae Sook} and Sohn, {Sang Kyun} and Moon, {Joon Ho} and Jung, {Chul Won} and Silvia Park and Lipton, {Jeffrey H.} and Shinya Kimura and Kim, {Jong Won} and Kim, {Dennis (Dong Hwan)}",

note = "Publisher Copyright: {\textcopyright} 2018, Springer Nature Limited.",

year = "2019",

month = jun,

day = "1",

doi = "10.1038/s41375-018-0321-8",

language = "English",

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Park, JH, Woo, YM, Youm, EM, Hamad, N, Won, HH, Naka, K, Park, EJ, Park, JH, Kim, HJ, Kim, SH, Kim, HJ, Ahn, JS, Sohn, SK, Moon, JH, Jung, CW, Park, S, Lipton, JH, Kimura, S, Kim, JW & Kim, D 2019, 'HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia', Leukemia, vol. 33, no. 6, pp. 1439-1450. https://doi.org/10.1038/s41375-018-0321-8

TY - JOUR

T1 - HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia

AU - Park, Jong Ho

AU - Woo, Young Min

AU - Youm, Emilia Moonkyung

AU - Hamad, Nada

AU - Won, Hong Hee

AU - Naka, Kazuhito

AU - Park, Eun Ju

AU - Park, June Hee

AU - Kim, Hee Jin

AU - Kim, Sun Hee

AU - Kim, Hyeoung Joon

AU - Ahn, Jae Sook

AU - Sohn, Sang Kyun

AU - Moon, Joon Ho

AU - Jung, Chul Won

AU - Park, Silvia

AU - Lipton, Jeffrey H.

AU - Kimura, Shinya

AU - Kim, Jong Won

AU - Kim, Dennis (Dong Hwan)

PY - 2019/6/1

Y1 - 2019/6/1

N2 - Achieving a deep molecular response (DMR) to tyrosine kinase inhibitor (TKI) therapy for chronic myeloid leukemia (CML) remains challenging and at present, there is no biomarker to predict DMR in this setting. Herein, we report that an HMGCLL1 genetic variant located in 6p12.1 can be used as a predictive genetic biomarker for intrinsic sensitivity to imatinib (IM) therapy. We measured DMR rate according to HMGCLL1 variant in a discovery set of CML patients (n = 201) and successfully replicated it in a validation set (n = 270). We also investigated the functional relevance of HMGCLL1 blockade with respect to response to TKI therapy and showed that small interfering RNA mediated blockade of HMGCLL1 isoform 3 results in significant decrease in viability of BCR-ABL1-positive cells including K562, CML-T1 or BaF3 cell lines with or without ABL1 kinase domain mutations such as T315I mutation. Decreased cell viability was also demonstrated in murine CML stem cells and human hematopoietic progenitor cells. RNA sequencing showed that blockade of HMGCLL1 was associated with G0/G1 arrest and the cell cycle. In summary, the HMGCLL1 gene polymorphism is a novel genetic biomarker for intrinsic sensitivity to IM therapy in CML patients that predicts DMR in this setting.

AB - Achieving a deep molecular response (DMR) to tyrosine kinase inhibitor (TKI) therapy for chronic myeloid leukemia (CML) remains challenging and at present, there is no biomarker to predict DMR in this setting. Herein, we report that an HMGCLL1 genetic variant located in 6p12.1 can be used as a predictive genetic biomarker for intrinsic sensitivity to imatinib (IM) therapy. We measured DMR rate according to HMGCLL1 variant in a discovery set of CML patients (n = 201) and successfully replicated it in a validation set (n = 270). We also investigated the functional relevance of HMGCLL1 blockade with respect to response to TKI therapy and showed that small interfering RNA mediated blockade of HMGCLL1 isoform 3 results in significant decrease in viability of BCR-ABL1-positive cells including K562, CML-T1 or BaF3 cell lines with or without ABL1 kinase domain mutations such as T315I mutation. Decreased cell viability was also demonstrated in murine CML stem cells and human hematopoietic progenitor cells. RNA sequencing showed that blockade of HMGCLL1 was associated with G0/G1 arrest and the cell cycle. In summary, the HMGCLL1 gene polymorphism is a novel genetic biomarker for intrinsic sensitivity to IM therapy in CML patients that predicts DMR in this setting.

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U2 - 10.1038/s41375-018-0321-8

DO - 10.1038/s41375-018-0321-8

M3 - Article

C2 - 30555164

AN - SCOPUS:85058615743

SN - 0887-6924

VL - 33

SP - 1439

EP - 1450

JO - Leukemia

JF - Leukemia

IS - 6

ER -

HMGCLL1 is a predictive biomarker for deep molecular response to imatinib therapy in chronic myeloid leukemia

Abstract

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