Detection of residual disease in chronic myeloid leukemia utilizing genomic next generation sequencing reveals persistence of differentiated Ph+ B cells but not bone marrow stem/progenitors

Daiki Karigane; Hidenori Kasahara; Kouhei Shiroshita; Shinya Fujita; Hiroshi Kobayashi; Shinpei Tamaki; Rie Yamazaki; Kaori Yahagi; Yoko Yatabe; Naomi Kondoh; Tomoko Arai; Hisako Katagiri; Nobuko Shimizu; Masatoshi Sakurai; Taku Kikuchi; Jun Kato; Takayuki Shimizu; Taeko Hayakawa; Tomonori Yaguchi; Maiko Matsushita; Hideaki Nakajima; Yutaka Kawakami; Mitsuru Murata; Takehiko Mori; Takashi Sasaki; Shinichiro Okamoto; Keiyo Takubo

doi:10.1080/10428194.2020.1837366

Detection of residual disease in chronic myeloid leukemia utilizing genomic next generation sequencing reveals persistence of differentiated Ph⁺ B cells but not bone marrow stem/progenitors

Daiki Karigane, Hidenori Kasahara, Kouhei Shiroshita, Shinya Fujita, Hiroshi Kobayashi, Shinpei Tamaki, Rie Yamazaki, Kaori Yahagi, Yoko Yatabe, Naomi Kondoh, Tomoko Arai, Hisako Katagiri, Nobuko Shimizu, Masatoshi Sakurai, Taku Kikuchi, Jun Kato, Takayuki Shimizu, Taeko Hayakawa, Tomonori Yaguchi, Maiko MatsushitaHideaki Nakajima, Yutaka Kawakami, Mitsuru Murata, Takehiko Mori, Takashi Sasaki, Shinichiro Okamoto, Keiyo Takubo

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

Abstract

Persistence of leukemic stem cells (LSCs) results in the recurrence of chronic myeloid leukemia (CML) after the administration of tyrosine kinase inhibitors (TKIs). Thus, the detection of minimal residual disease (MRD) with LSC potential can improve prognosis. Here, we analyzed 115 CML patients and found that CD25 was preferentially expressed on the phenotypic stem and progenitor cells (SPCs), and TKI therapy decreased the number of CD25-positive cells in the SPC fraction. To detect MRD harboring BCR-ABL1 fusion DNA, we developed a highly-sensitive method using patient-specific primers and next-generation sequencing. By using this method, we identified that in patients who achieved molecular remission, almost all residual CD25-positive SPCs were BCR-ABL1-negative. Moreover, in some patients BCR-ABL1 was detectable in peripheral B cells but not in SPCs. We conclude that CD25 marks LSCs at diagnosis but does not mark MRD following TKI treatment and that analysis of peripheral B cells can allow sensitive detection of MRD.

Original language	English
Pages (from-to)	679-687
Number of pages	9
Journal	Leukemia and Lymphoma
Volume	62
Issue number	3
DOIs	https://doi.org/10.1080/10428194.2020.1837366
Publication status	Published - 2021

Keywords

CD25
Chronic myeloid leukemia
minimal residual disease
tyrosine kinase inhibitor

ASJC Scopus subject areas

Hematology
Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1080/10428194.2020.1837366

Cite this

Karigane, D., Kasahara, H., Shiroshita, K., Fujita, S., Kobayashi, H., Tamaki, S., Yamazaki, R., Yahagi, K., Yatabe, Y., Kondoh, N., Arai, T., Katagiri, H., Shimizu, N., Sakurai, M., Kikuchi, T., Kato, J., Shimizu, T., Hayakawa, T., Yaguchi, T., ... Takubo, K. (2021). Detection of residual disease in chronic myeloid leukemia utilizing genomic next generation sequencing reveals persistence of differentiated Ph⁺ B cells but not bone marrow stem/progenitors. Leukemia and Lymphoma, 62(3), 679-687. https://doi.org/10.1080/10428194.2020.1837366

Detection of residual disease in chronic myeloid leukemia utilizing genomic next generation sequencing reveals persistence of differentiated Ph⁺ B cells but not bone marrow stem/progenitors. / Karigane, Daiki; Kasahara, Hidenori; Shiroshita, Kouhei et al.
In: Leukemia and Lymphoma, Vol. 62, No. 3, 2021, p. 679-687.

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

Karigane, D, Kasahara, H, Shiroshita, K, Fujita, S, Kobayashi, H, Tamaki, S, Yamazaki, R, Yahagi, K, Yatabe, Y, Kondoh, N, Arai, T, Katagiri, H, Shimizu, N, Sakurai, M, Kikuchi, T, Kato, J , Shimizu, T, Hayakawa, T, Yaguchi, T, Matsushita, M, Nakajima, H, Kawakami, Y, Murata, M, Mori, T, Sasaki, T, Okamoto, S & Takubo, K 2021, 'Detection of residual disease in chronic myeloid leukemia utilizing genomic next generation sequencing reveals persistence of differentiated Ph⁺ B cells but not bone marrow stem/progenitors', Leukemia and Lymphoma, vol. 62, no. 3, pp. 679-687. https://doi.org/10.1080/10428194.2020.1837366

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title = "Detection of residual disease in chronic myeloid leukemia utilizing genomic next generation sequencing reveals persistence of differentiated Ph+ B cells but not bone marrow stem/progenitors",

abstract = "Persistence of leukemic stem cells (LSCs) results in the recurrence of chronic myeloid leukemia (CML) after the administration of tyrosine kinase inhibitors (TKIs). Thus, the detection of minimal residual disease (MRD) with LSC potential can improve prognosis. Here, we analyzed 115 CML patients and found that CD25 was preferentially expressed on the phenotypic stem and progenitor cells (SPCs), and TKI therapy decreased the number of CD25-positive cells in the SPC fraction. To detect MRD harboring BCR-ABL1 fusion DNA, we developed a highly-sensitive method using patient-specific primers and next-generation sequencing. By using this method, we identified that in patients who achieved molecular remission, almost all residual CD25-positive SPCs were BCR-ABL1-negative. Moreover, in some patients BCR-ABL1 was detectable in peripheral B cells but not in SPCs. We conclude that CD25 marks LSCs at diagnosis but does not mark MRD following TKI treatment and that analysis of peripheral B cells can allow sensitive detection of MRD.",

keywords = "CD25, Chronic myeloid leukemia, minimal residual disease, tyrosine kinase inhibitor",

author = "Daiki Karigane and Hidenori Kasahara and Kouhei Shiroshita and Shinya Fujita and Hiroshi Kobayashi and Shinpei Tamaki and Rie Yamazaki and Kaori Yahagi and Yoko Yatabe and Naomi Kondoh and Tomoko Arai and Hisako Katagiri and Nobuko Shimizu and Masatoshi Sakurai and Taku Kikuchi and Jun Kato and Takayuki Shimizu and Taeko Hayakawa and Tomonori Yaguchi and Maiko Matsushita and Hideaki Nakajima and Yutaka Kawakami and Mitsuru Murata and Takehiko Mori and Takashi Sasaki and Shinichiro Okamoto and Keiyo Takubo",

note = "Funding Information: The authors thank all patients who participated in this study. We thank Y. Niizuma, A. Tajima, K. Yanai, S. Yamanaka, M. Haraguchi, M. Furuhashi, and A. Azizi for technical support and laboratory management; and E. Lamar, D. Martinez-Krams and J. Morriss for preparation of the manuscript. D.K. was supported in part by a KAKENHI grant from MEXT/JSPS (19K17877), JB Research Grants and the Takeda Science Foundation. H. Kasahara was supported in part by a KAKENHI grant from MEXT/JSPS (JP19J00502). H. Kobayashi was supported in part by a KAKENHI grant from MEXT/JSPS (19K17847) and a grant from the National Center for Global Health and Medicine (29-1015). Y.K. was supported in part by a KAKENHI Grant from MEXT/JSPS (26221005). K.T. was supported in part by KAKENHI Grants from MEXT/JSPS (18H02845, 18K19570), grants from the National Center for Global Health and Medicine (26-001, 29-2007), AMED grants (JP18ck0106444, JP18ae0201014) and grants from the Ono Medical Research Foundation, the Kanzawa Medical Research Foundation and the Takeda Science Foundation. Publisher Copyright: {\textcopyright} 2020 Informa UK Limited, trading as Taylor & Francis Group.",

year = "2021",

doi = "10.1080/10428194.2020.1837366",

language = "English",

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AU - Karigane, Daiki

AU - Kasahara, Hidenori

AU - Shiroshita, Kouhei

AU - Fujita, Shinya

AU - Kobayashi, Hiroshi

AU - Tamaki, Shinpei

AU - Yamazaki, Rie

AU - Yahagi, Kaori

AU - Yatabe, Yoko

AU - Kondoh, Naomi

AU - Arai, Tomoko

AU - Katagiri, Hisako

AU - Shimizu, Nobuko

AU - Sakurai, Masatoshi

AU - Kikuchi, Taku

AU - Kato, Jun

AU - Shimizu, Takayuki

AU - Hayakawa, Taeko

AU - Yaguchi, Tomonori

AU - Matsushita, Maiko

AU - Nakajima, Hideaki

AU - Kawakami, Yutaka

AU - Murata, Mitsuru

AU - Mori, Takehiko

AU - Sasaki, Takashi

AU - Okamoto, Shinichiro

AU - Takubo, Keiyo

N1 - Funding Information: The authors thank all patients who participated in this study. We thank Y. Niizuma, A. Tajima, K. Yanai, S. Yamanaka, M. Haraguchi, M. Furuhashi, and A. Azizi for technical support and laboratory management; and E. Lamar, D. Martinez-Krams and J. Morriss for preparation of the manuscript. D.K. was supported in part by a KAKENHI grant from MEXT/JSPS (19K17877), JB Research Grants and the Takeda Science Foundation. H. Kasahara was supported in part by a KAKENHI grant from MEXT/JSPS (JP19J00502). H. Kobayashi was supported in part by a KAKENHI grant from MEXT/JSPS (19K17847) and a grant from the National Center for Global Health and Medicine (29-1015). Y.K. was supported in part by a KAKENHI Grant from MEXT/JSPS (26221005). K.T. was supported in part by KAKENHI Grants from MEXT/JSPS (18H02845, 18K19570), grants from the National Center for Global Health and Medicine (26-001, 29-2007), AMED grants (JP18ck0106444, JP18ae0201014) and grants from the Ono Medical Research Foundation, the Kanzawa Medical Research Foundation and the Takeda Science Foundation. Publisher Copyright: © 2020 Informa UK Limited, trading as Taylor & Francis Group.

PY - 2021

Y1 - 2021

N2 - Persistence of leukemic stem cells (LSCs) results in the recurrence of chronic myeloid leukemia (CML) after the administration of tyrosine kinase inhibitors (TKIs). Thus, the detection of minimal residual disease (MRD) with LSC potential can improve prognosis. Here, we analyzed 115 CML patients and found that CD25 was preferentially expressed on the phenotypic stem and progenitor cells (SPCs), and TKI therapy decreased the number of CD25-positive cells in the SPC fraction. To detect MRD harboring BCR-ABL1 fusion DNA, we developed a highly-sensitive method using patient-specific primers and next-generation sequencing. By using this method, we identified that in patients who achieved molecular remission, almost all residual CD25-positive SPCs were BCR-ABL1-negative. Moreover, in some patients BCR-ABL1 was detectable in peripheral B cells but not in SPCs. We conclude that CD25 marks LSCs at diagnosis but does not mark MRD following TKI treatment and that analysis of peripheral B cells can allow sensitive detection of MRD.

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KW - Chronic myeloid leukemia

KW - minimal residual disease

KW - tyrosine kinase inhibitor

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