Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on <i>MIR300</i> Antiproliferative and PP2A-Activating Functions

Silvestri, Giovannino; Trotta, Rossana; Stramucci, Lorenzo; Ellis, Justin J.; Harb, Jason G.; Neviani, Paolo; Wang, Shuzhen; Eisfeld, Ann‐Kathrin; Walker, Christopher J.; Zhang, Bin; Srutova, Klara; Gambacorti‐Passerini, Carlo; Pineda, Gabriel; Stagno, Fabio; Vigneri, Paolo; Nteliopoulos, Georgios; May, Philippa C.; Reid, Alistair; Garzon, Ramiro; Roy, Denis‐Claude; Moutuou, Moutuaata M.; Guimond, Martin; Hokland, Peter; Deininger, Michael W.; Fitzgerald, Garrett; Harman, Christopher; Dazzi, Francesco; Milojković, Dragana; Apperley, Jane F.; Marcucci, Guido; Qi, Jianfei; Poláková, Kateřina Machová; Zou, Ying; Fan, Xiaoxuan; Calabretta, Bruno; Perrotti, Danilo

doi:10.1158/0008-5472.bcd-19-0039

Cited by 28 publications

(35 citation statements)

References 70 publications

(100 reference statements)

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“…In the rapidly evolving genomic era of precision medicine, a transition towards dynamic monitoring of tumor molecular characteristics is being witnessed. In this regard, easily accessible markers that would reflect the entire heterogeneity of the tumor such as liquid biopsy including CTCs, circulating tumor-derived DNA (ctDNA), plasma cell-free DNA (cfDNA), microRNAs (miRNA), and exosomes have emerged as biomarkers with immense potential (Bronkhorst et al, 2019;Cervena et al, 2019;Silvestri et al, 2020). Plasma cfDNA facilitates non-invasive peripheral blood sampling of tumor-associated actionable alterations that are present in its ctDNA fraction and is gradually finding clinical utility in several cancers.…”

Section: Mrd Assessment In Aml and Current Challengesmentioning

confidence: 99%

Real-Time Molecular Monitoring in Acute Myeloid Leukemia With Circulating Tumor DNA

Thakral

Gupta

Sahoo

et al. 2020

Front. Cell Dev. Biol.

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The clonal evolution of acute myeloid leukemia (AML), an oligoclonal hematological malignancy, is driven by a plethora of cytogenetic abnormalities, gene mutations, abnormal epigenetic patterns, and aberrant gene expressions. These alterations in the leukemic blasts promote clinically diverse manifestations with common characteristics of high relapse and drug resistance. Defining and real-time monitoring of a personalized panel of these predictive genetic biomarkers is rapidly being adapted in clinical setting for diagnostic, prognostic, and therapeutic decision-making in AML. A major challenge remains the frequency of invasive biopsy procedures that can be routinely performed for monitoring of AML disease progression. Moreover, a single-site biopsy is not representative of the tumor heterogeneity as it is spatially and temporally constrained and necessitates the understanding of longitudinal and spatial subclonal dynamics in AML. Hematopoietic cells are a major contributor to plasma cell-free DNA, which also contain leukemia-specific aberrations as the circulating tumor-derived DNA (ctDNA) fraction. Plasma cell-free DNA analysis holds immense potential as a minimally invasive tool for genomic profiling at diagnosis as well as clonal evolution during AML disease progression. With the technological advances and increasing sensitivity for detection of ctDNA, both genetic and epigenetic aberrations can be qualitatively and quantitatively evaluated. However, challenges remain in validating the utility of liquid biopsy tools in clinics, and universal recommendations are still awaited towards reliable diagnostics and prognostics. Here, we provide an overview on the scope of ctDNA analyses for prognosis, assessment of response to treatment and measurable residual disease, prediction of disease relapse, development of acquired resistance and beyond in AML.

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Section: Mrd Assessment In Aml and Current Challengesmentioning

confidence: 99%

Real-Time Molecular Monitoring in Acute Myeloid Leukemia With Circulating Tumor DNA

Thakral

Gupta

Sahoo

et al. 2020

Front. Cell Dev. Biol.

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“…However, certain stem cell classes, especially pre-leukemic neoplastic stem cells may be resistant because they are slowly cycling cells and exhibit multiple forms of stem cell resistance ( Valent et al, 2012 ; Valent et al, 2013 ). TKI-resistance of CML LSC has been associated to both cell-autonomous ( Corbin et al, 2011 ; Kumari et al, 2012 ) and extrinsic factors ( Arrigoni et al, 2018 ; Zhang et al, 2018 ; Silvestri et al, 2020 ). Sometimes even LSC may survive TKI therapy and thus persist in CML patients.…”

Section: Introductionmentioning

confidence: 99%

“…One report has shown the involvement of microRNAs in TKI sensitivity in CML LSC ( Salati et al, 2017 ). Recent evidence has shown that miR-300 is a tumor suppressor microRNA able to induce quiescence in CML LSCs ( Silvestri et al, 2020 ), and that miR-126-3p regulates quiescence, self-renewal and engraftment capacity of CML LSCs ( Zhang et al, 2018 ). Advances in the characterization of aberrant expression of surface markers have allowed the prospective isolation of LSC and HSC from CML patients ( Herrmann et al, 2014 ; Warfvinge et al, 2017 ).…”

Section: Introductionmentioning

confidence: 99%

miRNome profiling of LSC-enriched CD34+CD38−CD26+ fraction in Ph+ CML-CP samples from Argentinean patients: a potential new pharmacogenomic tool

et al. 2021

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Chronic myeloid leukemia (CML) is a myeloid stem cell neoplasm characterized by an expansion of myeloid progenitor cells and the presence of BCR-ABL1 oncoprotein. Since the introduction of specific BCR-ABL1 tyrosine kinase inhibitors (TKI), overall survival has improved significantly. However, under long-term therapy patients may have residual disease that originates from TKI-resistant leukemic stem cells (LSC). In this work, we analyzed the miRNome of LSC-enriched CD34+CD38−CD26+ and normal hematopoietic stem cells (HSC) fractions obtained from the same chronic phase (CP) CML patients, and stem and progenitor cells obtained from healthy donors (HD) by next-generation sequencing. We detected a global decrease of microRNA levels in LSC-enriched CD34+CD38−CD26+ and HSC fractions from CML-CP patients, and decreased levels of microRNAs and snoRNAs from a genomic cluster in chromosome 14, suggesting a mechanism of silencing of multiple non-coding RNAs. Surprisingly, HSC from CML-CP patients, despite the absence of BCR-ABL1 expression, showed an altered miRNome. We confirmed by RT-qPCR that the levels of miR-196a-5p were increased more than nine-fold in CD26+ (BCR-ABL1+) vs. CD26− (BCR-ABL1−) CD34+CD38− fractions from CML-CP patients at diagnosis, and in silico analysis revealed a significant association to lipid metabolism and hematopoiesis functions. In the light of recent descriptions of increased oxidative metabolism in CML LSC-enriched fractions, these results serve as a guide for future functional studies that evaluate the role of microRNAs in this process. Metabolic vulnerabilities in LSCs open the road for new therapeutic strategies. This is the first report of the miRNome of CML-CP CD34+CD38− fractions that distinguishes between CD26+ (BCR-ABL1+) and their CD26− (BCR-ABL1-) counterparts, providing valuable data for future studies.

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“…As noted by Silvestri and colleagues (1), chronic myelogenous leukemia (CML) treatment does not result in cured disease for many patients (2,3). Thus, therapeutic challenges remain.…”

mentioning

confidence: 99%

“…It will be of interest to see how more stringent low oxygen assessments might affect the results reported by Silvestri and colleagues (1) and others for LS/ICs and other CS/ICs in terms of ex vivo growth characteristics, gene and protein expression patterns, and responsiveness to agents used to modulate these activities for eventual health benefit. More importantly, will this and the studies of Silvestri and colleagues (1) eventually be able to be used in a clinical setting?…”

mentioning

confidence: 99%

Players in Drug-Resistant Leukemia Stem/Initiating Cells and Immunity in Patients with CML in Context of Oxygen Levels: Would Collecting/Processing Cells in Hypoxia Offer Additional Information? A Next Frontier of Investigation

Broxmeyer

2020

Blood Cancer Discovery

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Chronic myelogenous leukemia (CML) is a stem cell disorder once considered an eventual death sentence upon progression to the terminal acute/blastic cell phase, a terrible clinical outcome that has improved with the introduction of tyrosine kinase inhibitors. A major continuing problem with treating CML is the persistence of drug-resistant leukemia stem/initiating cells (LS/IC). In this issue of Blood Cancer Discovery, Silvestri and colleagues describe an incredibly in-depth mechanistic study using genetic and pharmacologic modulation of the miRNA MiR300 with and without treatment with activators of the serine-threonine protein phosphatase 2A (PP2A) in human cells. In vitro studies and in vivo mouse models of patient-derived xenografts were used to address the need to target LS/ICs and restore immunity of impaired natural killer cells for attenuation of CML progression. See related article by Silvestri et al., p. 48 (1).

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Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Cited by 28 publications

References 70 publications

Real-Time Molecular Monitoring in Acute Myeloid Leukemia With Circulating Tumor DNA

Real-Time Molecular Monitoring in Acute Myeloid Leukemia With Circulating Tumor DNA

miRNome profiling of LSC-enriched CD34+CD38−CD26+ fraction in Ph+ CML-CP samples from Argentinean patients: a potential new pharmacogenomic tool

Players in Drug-Resistant Leukemia Stem/Initiating Cells and Immunity in Patients with CML in Context of Oxygen Levels: Would Collecting/Processing Cells in Hypoxia Offer Additional Information? A Next Frontier of Investigation

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