Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

Stephanie M Dobson; Laura García-Prat; Robert J Vanner; Jeffrey Wintersinger; Esmé Waanders; Zhaohui Gu; Jessica McLeod; Olga I Gan; Ildiko Grandal; Debbie Payne-Turner; Michael N Edmonson; Xiaotu Ma; Yiping Fan; Veronique Voisin; Michelle Chan-Seng-Yue; Stephanie Z Xie; Mohsen Hosseini; Sagi Abelson; Pankaj Gupta; Michael Rusch; Ying Shao; Scott R Olsen; Geoffrey Neale; Steven M Chan; Gary Bader; John Easton; Cynthia J Guidos; Jayne S Danska; Jinghui Zhang; Mark D Minden; Quaid Morris; Charles G Mullighan; John E Dick

doi:10.1158/2159-8290.CD-19-1059

Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

Stephanie M Dobson, Laura García-Prat, Robert J Vanner, Jeffrey Wintersinger, Esmé Waanders, Zhaohui Gu, Jessica McLeod, Olga I Gan, Ildiko Grandal, Debbie Payne-Turner, Michael N Edmonson, Xiaotu Ma, Yiping Fan, Veronique Voisin, Michelle Chan-Seng-Yue, Stephanie Z Xie, Mohsen Hosseini, Sagi Abelson, Pankaj Gupta, Michael RuschYing Shao, Scott R Olsen, Geoffrey Neale, Steven M Chan, Gary Bader, John Easton, Cynthia J Guidos, Jayne S Danska, Jinghui Zhang, Mark D Minden, Quaid Morris, Charles G Mullighan, John E Dick^*

^*Corresponding author for this work

Section genome diagnostics

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

Abstract

Disease recurrence causes significant mortality in B-progenitor acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples shows relapse often arising from minor diagnosis subclones. However, why therapy eradicates some subclones while others survive and progress to relapse remains obscure. Elucidation of mechanisms underlying these differing fates requires functional analysis of isolated subclones. Here, large-scale limiting dilution xenografting of diagnosis and relapse samples, combined with targeted sequencing, identified and isolated minor diagnosis subclones that initiate an evolutionary trajectory toward relapse [termed diagnosis Relapse Initiating clones (dRI)]. Compared with other diagnosis subclones, dRIs were drug-tolerant with distinct engraftment and metabolic properties. Transcriptionally, dRIs displayed enrichment for chromatin remodeling, mitochondrial metabolism, proteostasis programs, and an increase in stemness pathways. The isolation and characterization of dRI subclones reveals new avenues for eradicating dRI cells by targeting their distinct metabolic and transcriptional pathways before further evolution renders them fully therapy-resistant. SIGNIFICANCE: Isolation and characterization of subclones from diagnosis samples of patients with B-ALL who relapsed showed that relapse-fated subclones had increased drug tolerance and distinct metabolic and survival transcriptional programs compared with other diagnosis subclones. This study provides strategies to identify and target clinically relevant subclones before further evolution toward relapse.

Original language	English
Pages (from-to)	568-587
Number of pages	20
Journal	Cancer Discovery
Volume	10
Issue number	4
DOIs	https://doi.org/10.1158/2159-8290.CD-19-1059
Publication status	Published - Apr 2020

Keywords

Clone Cells
Female
Humans
Leukemia, Myeloid, Acute/genetics
Male
Recurrence

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10.1158/2159-8290.CD-19-1059

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Dobson, S. M., García-Prat, L., Vanner, R. J., Wintersinger, J., Waanders, E., Gu, Z., McLeod, J., Gan, O. I., Grandal, I., Payne-Turner, D., Edmonson, M. N., Ma, X., Fan, Y., Voisin, V., Chan-Seng-Yue, M., Xie, S. Z., Hosseini, M., Abelson, S., Gupta, P., ... Dick, J. E. (2020). Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs. Cancer Discovery, 10(4), 568-587. https://doi.org/10.1158/2159-8290.CD-19-1059

@article{ebcb2651c48a4e8ca234850f3aa76dda,

title = "Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs",

abstract = "Disease recurrence causes significant mortality in B-progenitor acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples shows relapse often arising from minor diagnosis subclones. However, why therapy eradicates some subclones while others survive and progress to relapse remains obscure. Elucidation of mechanisms underlying these differing fates requires functional analysis of isolated subclones. Here, large-scale limiting dilution xenografting of diagnosis and relapse samples, combined with targeted sequencing, identified and isolated minor diagnosis subclones that initiate an evolutionary trajectory toward relapse [termed diagnosis Relapse Initiating clones (dRI)]. Compared with other diagnosis subclones, dRIs were drug-tolerant with distinct engraftment and metabolic properties. Transcriptionally, dRIs displayed enrichment for chromatin remodeling, mitochondrial metabolism, proteostasis programs, and an increase in stemness pathways. The isolation and characterization of dRI subclones reveals new avenues for eradicating dRI cells by targeting their distinct metabolic and transcriptional pathways before further evolution renders them fully therapy-resistant. SIGNIFICANCE: Isolation and characterization of subclones from diagnosis samples of patients with B-ALL who relapsed showed that relapse-fated subclones had increased drug tolerance and distinct metabolic and survival transcriptional programs compared with other diagnosis subclones. This study provides strategies to identify and target clinically relevant subclones before further evolution toward relapse.",

keywords = "Clone Cells, Female, Humans, Leukemia, Myeloid, Acute/genetics, Male, Recurrence",

author = "Dobson, {Stephanie M} and Laura Garc{\'i}a-Prat and Vanner, {Robert J} and Jeffrey Wintersinger and Esm{\'e} Waanders and Zhaohui Gu and Jessica McLeod and Gan, {Olga I} and Ildiko Grandal and Debbie Payne-Turner and Edmonson, {Michael N} and Xiaotu Ma and Yiping Fan and Veronique Voisin and Michelle Chan-Seng-Yue and Xie, {Stephanie Z} and Mohsen Hosseini and Sagi Abelson and Pankaj Gupta and Michael Rusch and Ying Shao and Olsen, {Scott R} and Geoffrey Neale and Chan, {Steven M} and Gary Bader and John Easton and Guidos, {Cynthia J} and Danska, {Jayne S} and Jinghui Zhang and Minden, {Mark D} and Quaid Morris and Mullighan, {Charles G} and Dick, {John E}",

note = "Publisher Copyright: {\textcopyright} 2020 American Association for Cancer Research.",

year = "2020",

month = apr,

doi = "10.1158/2159-8290.CD-19-1059",

language = "English",

volume = "10",

pages = "568--587",

journal = "Cancer Discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "4",

}

Dobson, SM, García-Prat, L, Vanner, RJ, Wintersinger, J, Waanders, E, Gu, Z, McLeod, J, Gan, OI, Grandal, I, Payne-Turner, D, Edmonson, MN, Ma, X, Fan, Y, Voisin, V, Chan-Seng-Yue, M, Xie, SZ, Hosseini, M, Abelson, S, Gupta, P, Rusch, M, Shao, Y, Olsen, SR, Neale, G, Chan, SM, Bader, G, Easton, J, Guidos, CJ, Danska, JS, Zhang, J, Minden, MD, Morris, Q, Mullighan, CG & Dick, JE 2020, 'Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs', Cancer Discovery, vol. 10, no. 4, pp. 568-587. https://doi.org/10.1158/2159-8290.CD-19-1059

TY - JOUR

T1 - Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

AU - Dobson, Stephanie M

AU - García-Prat, Laura

AU - Vanner, Robert J

AU - Wintersinger, Jeffrey

AU - Waanders, Esmé

AU - Gu, Zhaohui

AU - McLeod, Jessica

AU - Gan, Olga I

AU - Grandal, Ildiko

AU - Payne-Turner, Debbie

AU - Edmonson, Michael N

AU - Ma, Xiaotu

AU - Fan, Yiping

AU - Voisin, Veronique

AU - Chan-Seng-Yue, Michelle

AU - Xie, Stephanie Z

AU - Hosseini, Mohsen

AU - Abelson, Sagi

AU - Gupta, Pankaj

AU - Rusch, Michael

AU - Shao, Ying

AU - Olsen, Scott R

AU - Neale, Geoffrey

AU - Chan, Steven M

AU - Bader, Gary

AU - Easton, John

AU - Guidos, Cynthia J

AU - Danska, Jayne S

AU - Zhang, Jinghui

AU - Minden, Mark D

AU - Morris, Quaid

AU - Mullighan, Charles G

AU - Dick, John E

PY - 2020/4

Y1 - 2020/4

N2 - Disease recurrence causes significant mortality in B-progenitor acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples shows relapse often arising from minor diagnosis subclones. However, why therapy eradicates some subclones while others survive and progress to relapse remains obscure. Elucidation of mechanisms underlying these differing fates requires functional analysis of isolated subclones. Here, large-scale limiting dilution xenografting of diagnosis and relapse samples, combined with targeted sequencing, identified and isolated minor diagnosis subclones that initiate an evolutionary trajectory toward relapse [termed diagnosis Relapse Initiating clones (dRI)]. Compared with other diagnosis subclones, dRIs were drug-tolerant with distinct engraftment and metabolic properties. Transcriptionally, dRIs displayed enrichment for chromatin remodeling, mitochondrial metabolism, proteostasis programs, and an increase in stemness pathways. The isolation and characterization of dRI subclones reveals new avenues for eradicating dRI cells by targeting their distinct metabolic and transcriptional pathways before further evolution renders them fully therapy-resistant. SIGNIFICANCE: Isolation and characterization of subclones from diagnosis samples of patients with B-ALL who relapsed showed that relapse-fated subclones had increased drug tolerance and distinct metabolic and survival transcriptional programs compared with other diagnosis subclones. This study provides strategies to identify and target clinically relevant subclones before further evolution toward relapse.

AB - Disease recurrence causes significant mortality in B-progenitor acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples shows relapse often arising from minor diagnosis subclones. However, why therapy eradicates some subclones while others survive and progress to relapse remains obscure. Elucidation of mechanisms underlying these differing fates requires functional analysis of isolated subclones. Here, large-scale limiting dilution xenografting of diagnosis and relapse samples, combined with targeted sequencing, identified and isolated minor diagnosis subclones that initiate an evolutionary trajectory toward relapse [termed diagnosis Relapse Initiating clones (dRI)]. Compared with other diagnosis subclones, dRIs were drug-tolerant with distinct engraftment and metabolic properties. Transcriptionally, dRIs displayed enrichment for chromatin remodeling, mitochondrial metabolism, proteostasis programs, and an increase in stemness pathways. The isolation and characterization of dRI subclones reveals new avenues for eradicating dRI cells by targeting their distinct metabolic and transcriptional pathways before further evolution renders them fully therapy-resistant. SIGNIFICANCE: Isolation and characterization of subclones from diagnosis samples of patients with B-ALL who relapsed showed that relapse-fated subclones had increased drug tolerance and distinct metabolic and survival transcriptional programs compared with other diagnosis subclones. This study provides strategies to identify and target clinically relevant subclones before further evolution toward relapse.

KW - Clone Cells

KW - Female

KW - Humans

KW - Leukemia, Myeloid, Acute/genetics

KW - Male

KW - Recurrence

UR - http://www.scopus.com/inward/record.url?scp=85082780481&partnerID=8YFLogxK

U2 - 10.1158/2159-8290.CD-19-1059

DO - 10.1158/2159-8290.CD-19-1059

M3 - Article

C2 - 32086311

SN - 2159-8274

VL - 10

SP - 568

EP - 587

JO - Cancer Discovery

JF - Cancer Discovery

IS - 4

ER -

Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

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Keywords

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