Chronic myeloid leukaemia cells require the bone morphogenic protein pathway for cell cycle progression and self-renewal

Toofan, Parto; Busch, Caroline; Morrison, Heather; O’Brien, Stephen G.; Jørgensen, Heather G.; Copland, Mhairi; Wheadon, Helen

doi:10.1038/s41419-018-0905-2

Cited by 12 publications

(22 citation statements)

References 64 publications

(76 reference statements)

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“…Laperrousaz et al revealed deregulation of BMPR1B/ALK6 and downstream signalling elements, such as SMAD1, SMAD4, SMAD5, SMAD6, ID2 and RUNX1 in CP CML patients compared to healthy controls [103] . Deregulation of the pathway was also confirmed by Toofan et al who showed that differential expression of BMP pathway genes such as ACV1C, INHBA, SMAD7, SNAIL1 and SMURF2 could be linked to treatment response [105] . BMPR1B/ALK6 was identified as the main driver for myeloid progenitor expansion with BCR-ABL1 oncogene being sufficient to increase BMPR1B/ALK6 cell membrane expression in CML [103] .…”

Section: Role Of the Bmp Pathway In Sustaining CML Lsc In The Bm Nichementioning

confidence: 62%

“…Our results showed that dual targeting of BMP pathway signalling and BCR-ABL1 leads to altered cell cycle gene transcription, irreversible cell cycle arrest, along with increased apoptosis compared to single treatments. More importantly, inhibition resulted in fewer cell divisions, reduced numbers of CD34 + cells and colony formation from CML patient samples compared with healthy controls [105] . These promising results suggest that this approach warrants further investigations.…”

Section: Targeting the Bmp Pathwaymentioning

confidence: 95%

“…Recent studies indicate both an intrinsic and extrinsic deregulation of the BMP pathway in CML patients, with alterations most prevalent in TKI resistant patients [103][104][105], [106] . Laperrousaz et al revealed deregulation of BMPR1B/ALK6 and downstream signalling elements, such as SMAD1, SMAD4, SMAD5, SMAD6, ID2 and RUNX1 in CP CML patients compared to healthy controls [103] .…”

Section: Role Of the Bmp Pathway In Sustaining CML Lsc In The Bm Nichementioning

confidence: 99%

“…Deregulation of BMP signalling in CML upon TKI pressure needs to be further investigated in the future with the aim to identify key downstream target genes and to understand the crosstalk between BMP receptors, integrins and the ECM within the BM niche. Preliminary experiments have shown that combinatorial treatment of TKIs along with BMP receptor antagonists are a promising therapeutic approach to target the deregulated intrinsic and extrinsic BMP pathway in CML [105] . However, many current BMP receptor inhibitors display off target effects and often inhibit more than one type of receptor.…”

Section: Targeting the Bmp Pathwaymentioning

confidence: 99%

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Bone marrow niche crosses paths with BMPs: a road to protection and persistence in CML

Busch

Wheadon

2019

Biochemical Society Transactions

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Chronic myeloid leukaemia (CML) is a paradigm of precision medicine, being one of the first cancers to be treated with targeted therapy. This has revolutionised CML therapy and patient outcome, with high survival rates. However, this now means an ever-increasing number of patients are living with the disease on life-long tyrosine kinase inhibitor (TKI) therapy, with most patients anticipated to have near normal life expectancy. Unfortunately, in a significant number of patients, TKIs are not curative. This low-level disease persistence suggests that despite a molecularly targeted therapeutic approach, there are BCR-ABL1-independent mechanisms exploited to sustain the survival of a small cell population of leukaemic stem cells (LSCs). In CML, LSCs display many features akin to haemopoietic stem cells, namely quiescence, self-renewal and the ability to produce mature progeny, this all occurs through intrinsic and extrinsic signals within the specialised microenvironment of the bone marrow (BM) niche. One important avenue of investigation in CML is how the disease highjacks the BM, thereby remodelling this microenvironment to create a niche, which enables LSC persistence and resistance to TKI treatment. In this review, we explore how changes in growth factor levels, in particular, the bone morphogenetic proteins (BMPs) and pro-inflammatory cytokines, impact on cell behaviour, extracellular matrix deposition and bone remodelling in CML. We also discuss the challenges in targeting LSCs and the potential of dual targeting using combination therapies against BMP receptors and BCR-ABL1.

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Section: Role Of the Bmp Pathway In Sustaining CML Lsc In The Bm Nichementioning

confidence: 62%

Section: Targeting the Bmp Pathwaymentioning

confidence: 95%

Section: Role Of the Bmp Pathway In Sustaining CML Lsc In The Bm Nichementioning

confidence: 99%

Section: Targeting the Bmp Pathwaymentioning

confidence: 99%

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Bone marrow niche crosses paths with BMPs: a road to protection and persistence in CML

Busch

Wheadon

2019

Biochemical Society Transactions

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“…The generation of immunosuppressive/tolerogenic DCs and M2 MØs has been proposed to be induced by different tumour-mediated mechanisms such as hypoxia, endoplasmic reticulum stress, and mainly exposition to several tumour-derived cytokines and growth factors [6,8,13,48]. In this context, the components of the TGF-β superfamily, including the BMPs, have been extensively reported to participate in multiple aspects of tumour biology including immune evasion [21,49,50,51] but the relevance of BMP pathway in the origin and progression of leukaemias and lymphomas is now beginning to be uncovered [24,52]. Our present data show that Nalm-6 ALL cells mainly secrete BMP4, but not other BMP ligands previously reported to be involved in lymphoid malignancies [24,53].…”

Section: Discussionmentioning

confidence: 99%

Acute Lymphoblastic Leukaemia Cells Impair Dendritic Cell and Macrophage Differentiation: Role of BMP4

Valencia

Fernández-Sevilla

Fraile-Ramos

et al. 2019

Cells

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Dendritic cells and macrophages are common components of the tumour immune microenvironment and can contribute to immune suppression in both solid and haematological cancers. The Bone Morphogenetic Protein (BMP) pathway has been reported to be involved in cancer, and more recently in leukaemia development and progression. In the present study, we analyse whether acute lymphoblastic leukaemia (ALL) cells can affect the differentiation of dendritic cells and macrophages and the involvement of BMP pathway in the process. We show that ALL cells produce BMP4 and that conditioned media from ALL cells promote the generation of dendritic cells with immunosuppressive features and skew M1-like macrophage polarization towards a less pro-inflammatory phenotype. Likewise, BMP4 overexpression in ALL cells potentiates their ability to induce immunosuppressive dendritic cells and favours the generation of M2-like macrophages with pro-tumoral features. These results suggest that BMP4 is in part responsible for the alterations in dendritic cell and macrophage differentiation produced by ALL cells.

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Targeting BMP signaling in the bone marrow microenvironment of myeloid leukemia

Lefort

Maguer-Satta

2020

Biochemical Society Transactions

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The bone morphogenetic protein (BMP) pathway regulates the fate and proliferation of normal hematopoietic stem cells (HSC) as well as interactions with their niche. While BMP2 and BMP4 promote HSC differentiation, only BMP4 maintains HSC pool and favors interactions with their niche. In myeloid leukemia, we have identified intrinsic and extrinsic dysregulations of the BMP pathway in Chronic Myeloid Leukemia (CML) and Acute Myeloid leukemia (AML) responsible for leukemic stem cells (LSC) survival. In AML, BMP pathway alterations sustain and promote resistant immature-like leukemic cells by activating a new signaling cascade. Binding of BMP4 to BMPR1A leads to ΔNp73 expression, which in turn induces NANOG, altogether associated with a poor patient's prognosis. Despite efficient targeted therapies, like Tyrosine Kinase Inhibitors (TKI) in CML, many patients retain LSCs. Our laboratory demonstrated that the BMP pathway sustains a permanent pool of LSCs expressing high levels of BMPR1B receptor, that evolve upon treatment to progressively implement a BMP4 autocrine loop, leading to TKI-resistant cells. Single cell RNA-Seq analysis of TKI-persisting LSCs showed a co-enrichment of BMP with Jak2-signaling, quiescence and stem cell (SC) signatures. Using a new model of persisting LSCs, we recently demonstrated that BMPR1B+ cells display co-activated Smad1/5/8 and Stat3 pathways and could be targeted by blocking BMPR1B/Jak2 signal. Lastly, a specific BMPR1B inhibitor impaired BMP4-mediated LSC protection against TKIs. Altogether, data based on various studies including ours, indicate that BMP targeting could eliminate leukemic cells within a protective bone marrow microenvironment to efficiently impact residual resistance or persistence of LSCs in myeloid leukemia.

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Chronic myeloid leukaemia cells require the bone morphogenic protein pathway for cell cycle progression and self-renewal

Cited by 12 publications

References 64 publications

Bone marrow niche crosses paths with BMPs: a road to protection and persistence in CML

Bone marrow niche crosses paths with BMPs: a road to protection and persistence in CML

Acute Lymphoblastic Leukaemia Cells Impair Dendritic Cell and Macrophage Differentiation: Role of BMP4

Targeting BMP signaling in the bone marrow microenvironment of myeloid leukemia

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