FOXO1 activation is an effector of SYK and AKT inhibition in tonic BCR signal-dependent diffuse large B-cell lymphomas

Szydłowski, Maciej; Kiliszek, Przemyslaw; Sewastianik, Tomasz; Jabłońska, Ewa; Białopiotrowicz, Emilia; Górniak, Patryk; Polak, Anna; Markowicz, Sergiusz; Nowak, Eliza; Grygorowicz, Monika Anna; Prochorec‐Sobieszek, Monika; Szumera‐Ciećkiewicz, Anna; Malenda, Agata; Lech-Maranda, Ewa; Warzocha, Krzysztof; Juszczyński, Przemysław

doi:10.1182/blood-2015-06-654111

Cited by 53 publications

(43 citation statements)

References 37 publications

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“…13,14 FOXO proteins regulate proapoptotic and antiproliferative genes, as well as antioxidant and DNA repair pathways. 15,16 Thus, FOXO1 has tumor-suppressor function in various solid tumors and B-cell lymphomas, [17][18][19][20][21] including Hodgkin lymphoma (HL). 22 Contradictory to these inhibitory effects are recent reports linking high FOXO expression to poor prognosis and tumor-promoting activity in intestinal, neuronal, and hematological malignancies.…”

Section: Introductionmentioning

confidence: 99%

Nuclear FOXO1 promotes lymphomagenesis in germinal center B cells

Kabrani

Chu

Tasouri

et al. 2018

Blood

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Abstract Forkhead box class O1 (FOXO1) acts as a tumor suppressor in solid tumors. The oncogenic phosphoinositide-3-kinase (PI3K) pathway suppresses FOXO1 transcriptional activity by enforcing its nuclear exclusion upon AKT-mediated phosphorylation. We show here abundant nuclear expression of FOXO1 in Burkitt lymphoma (BL), a germinal center (GC) B-cell–derived lymphoma whose pathogenesis is linked to PI3K activation. Recurrent FOXO1 mutations, which prevent AKT targeting and lock the transcription factor in the nucleus, are used by BL to circumvent mutual exclusivity between PI3K and FOXO1 activation. Using genome editing in human and mouse lymphomas in which MYC and PI3K cooperate synergistically in tumor development, we demonstrate proproliferative and antiapoptotic activity of FOXO1 in BL and identify its nuclear localization as an oncogenic event in GC B-cell–derived lymphomagenesis.

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Section: Introductionmentioning

confidence: 99%

Nuclear FOXO1 promotes lymphomagenesis in germinal center B cells

Kabrani

Chu

Tasouri

et al. 2018

Blood

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“…50, 51 Consequently, upregulation of Bim appears a common mechanism triggered by inhibition of BCR-inducible kinases. Although PI3Kδi-mediated Bim upregulation was evident in vitro in the absence of exogenous antigen, antigen contamination of in vitro cultures from murine tissues is likely.…”

Section: Discussionmentioning

confidence: 99%

PI3Kδ inhibition elicits anti-leukemic effects through Bim-dependent apoptosis

et al. 2016

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PI3Kδ plays pivotal roles in the maintenance, proliferation and survival of malignant B-lymphocytes. Although not curative, PI3Kδ inhibitors (PI3Kδi) demonstrate impressive clinical efficacy and, alongside other signaling inhibitors, are revolutionizing the treatment of hematological malignancies. However, only limited in vivo data are available regarding their mechanism of action. With the rising number of novel treatments, the challenge is to identify combinations that deliver curative regimes. A deeper understanding of the molecular mechanism is required to guide these selections. Currently, immunomodulation, inhibition of B-cell receptor signaling, chemokine/cytokine signaling and apoptosis represent potential therapeutic mechanisms for PI3Kδi. Here we characterize the molecular mechanisms responsible for PI3Kδi-induced apoptosis in an in vivo model of chronic lymphocytic leukemia (CLL). In vitro, PI3Kδi-induced substantive apoptosis and disrupted microenvironment-derived signaling in murine (Eμ-Tcl1) and human (CLL) leukemia cells. Furthermore, PI3Kδi imparted significant therapeutic responses in Eμ-Tcl1-bearing animals and enhanced anti-CD20 monoclonal antibody therapy. Responses correlated with upregulation of the pro-apoptotic BH3-only protein Bim. Accordingly, Bim−/− Eμ-Tcl1 Tg leukemias demonstrated resistance to PI3Kδi-induced apoptosis were refractory to PI3Kδi in vivo and failed to display combination efficacy with anti-CD20 monoclonal antibody therapy. Therefore, Bim-dependent apoptosis represents a key in vivo therapeutic mechanism for PI3Kδi, both alone and in combination therapy regimes.

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“…In line with previous reports, CLL cells from our cohort expressed higher levels of all PIM kinase isoforms when compared to healthy B lymphocytes ( Figure S1). Patients with advanced FISHnegative 30 (21) *Number of patients is indicated in parentheses when the entire cohort was not investigated for that variable.…”

Section: Pim1 and Pim2 Are Associated With Unfavourable Cll Prognosismentioning

confidence: 99%

Microenvironment‐induced PIM kinases promote CXCR4‐triggered mTOR pathway required for chronic lymphocytic leukaemia cell migration

Białopiotrowicz

Górniak

Noyszewska‐Kania

et al. 2018

J Cellular Molecular Medi

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Lymph node microenvironment provides chronic lymphocytic leukaemia (CLL) cells with signals promoting their survival and granting resistance to chemotherapeutics. CLL cells overexpress PIM kinases, which regulate apoptosis, cell cycle and migration. We demonstrate that BCR crosslinking, CD40 stimulation, and coculture with stromal cells increases PIMs expression in CLL cells, indicating microenvironment‐dependent PIMs regulation. PIM1 and PIM2 expression at diagnosis was higher in patients with advanced disease (Binet C vs. Binet A/B) and in those, who progressed after first‐line treatment. In primary CLL cells, inhibition of PIM kinases with a pan‐PIM inhibitor, SEL24‐B489, decreased PIM‐specific substrate phosphorylation and induced dose‐dependent apoptosis in leukaemic, but not in normal B cells. Cytotoxicity of SEL24‐B489 was similar in TP53‐mutant and TP53 wild‐type cells. Finally, inhibition of PIM kinases decreased CXCR4‐mediated cell chemotaxis in two related mechanisms‐by decreasing CXCR4 phosphorylation and surface expression, and by limiting CXCR4‐triggered mTOR pathway activity. Importantly, PIM and mTOR inhibitors similarly impaired migration, indicating that CXCL12‐triggered mTOR is required for CLL cell chemotaxis. Given the microenvironment‐modulated PIM expression, their pro‐survival function and a role of PIMs in CXCR4‐induced migration, inhibition of these kinases might override microenvironmental protection and be an attractive therapeutic strategy in this disease.

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FOXO1 activation is an effector of SYK and AKT inhibition in tonic BCR signal-dependent diffuse large B-cell lymphomas

Cited by 53 publications

References 37 publications

Nuclear FOXO1 promotes lymphomagenesis in germinal center B cells

Nuclear FOXO1 promotes lymphomagenesis in germinal center B cells

PI3Kδ inhibition elicits anti-leukemic effects through Bim-dependent apoptosis

Microenvironment‐induced PIM kinases promote CXCR4‐triggered mTOR pathway required for chronic lymphocytic leukaemia cell migration

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