Decreased NOTCH1 Activation Correlates with Response to Ibrutinib in Chronic Lymphocytic Leukemia

Papa, Beatrice Del; Baldoni, Stefano; Dorillo, Erica; Falco, Filomena De; Rompietti, Chiara; Cecchini, Debora; Cantelmi, Maria Grazia; Sorcini, Daniele; Nogarotto, Manuel; Adamo, Francesco Maria; Mezzasoma, Federica; Barcelos, Estevão Carlos Silva; Albi, Elisabetta; Ostini, Roberta Iacucci; Tommaso, Ambra Di; Marra, Andrea; Montanaro, Guido; Martelli, Maria Paola; Falzetti, Franca; Ianni, Mauro Di; Rosati, Emanuela; Sportoletti, Paolo

doi:10.1158/1078-0432.ccr-19-1009

Cited by 24 publications

(25 citation statements)

References 59 publications

(66 reference statements)

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“…Ibrutinib treatment has been shown to reduce NOTCH1 activation, most pronounced at 12 months of continuous therapy. 13 In the setting of cardiac ischemia, NOTCH1 -activated bone marrow–derived mesenchymal stem cells promote CM survival through an antifibrotic mechanism. 14 Although this hypothesis is predicated on myocardial injury, subclinical ischemia is possible in a cohort with a median age over 75.…”

Section: Discussionmentioning

confidence: 99%

High-grade heart block associated with ibrutinib therapy

Vartanov

Lampson

Jacobsen

et al. 2021

HeartRhythm Case Reports

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Section: Discussionmentioning

confidence: 99%

High-grade heart block associated with ibrutinib therapy

Vartanov

Lampson

Jacobsen

et al. 2021

HeartRhythm Case Reports

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“…The aberrant NOTCH1 signaling in CLL cells regulates several genes that influence key biological aspects of neoplastic cells, such as apoptosis, cell growth, cell migration, interactions with the microenvironment and B Cell Receptor (BCR) activation. It has been shown that a synergistic cooperation between NOTCH1 and BCR strongly supports the survival/proliferation of CLL cells and contributes to a progression of the disease ( 11 ) but also to the transformation into Richter’s syndrome (RS) ( 12 ). Furthermore, it has been recently shown that ligand-dependent activation of NOTCH1 signaling, via constitutive PI3K/AKT activation, promotes CLL transformation towards RS in Eμ- TCL1 mice in vivo ( 13 ), thus further supporting the association between non-mutational NOTCH1 activation and a poor prognosis.…”

Section: Resultsmentioning

confidence: 99%

NOTCH1 Activation Negatively Impacts on Chronic Lymphocytic Leukemia Outcome and Is Not Correlated to the NOTCH1 and IGHV Mutational Status

et al. 2021

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NOTCH1 mutations and deregulated signal have been commonly found in chronic lymphocytic leukemia (CLL) patients. Whereas the impact of NOTCH1 mutations on clinical course of CLL has been widely studied, the prognostic role of NOTCH1 activation in CLL remains to be defined. Here, we analyzed the activation of NOTCH1/NOTCH2 (ICN1/ICN2) and the expression of JAGGED1 (JAG1) in 163 CLL patients and evaluated their impact on TTFT (Time To First Treatment) and OS (Overall Survival). NOTCH1 activation (ICN1+) was found in 120/163 (73.6%) patients. Among them, 63 (52.5%) were NOTCH1 mutated (ICN1+/mutated) and 57 (47.5%) were NOTCH1 wild type (ICN1+/WT). ICN1+ patients had a significant reduction of TTFT compared to ICN1-negative (ICN1−). In the absence of NOTCH1 mutations, we found that the ICN1+/WT group had a significantly reduced TTFT compared to ICN1− patients. The analysis of IGHV mutational status showed that the distribution of the mutated/unmutated IGHV pattern was similar in ICN1+/WT and ICN1− patients. Additionally, TTFT was significantly reduced in ICN1+/ICN2+ and ICN1+/JAG1+ patients compared to ICN1−/ICN2− and ICN1−/JAG1− groups. Our data revealed for the first time that NOTCH1 activation is a negative prognosticator in CLL and is not correlated to NOTCH1 and IGHV mutational status. Activation of NOTCH2 and JAGGED1 expression might also influence clinical outcomes in this group, indicating the need for further dedicated studies. The evaluation of different NOTCH network components might represent a new approach to refine CLL risk stratification.

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“…RO4929097 inhibited the NOTCH3/NR4A1 axis, upregulated the NOTCH2/FCER2 (CD23) axis, and enhanced the NOTCH2/CSL transcription factor complex ( Figure 5 B, right panel), which stands in sharp contrast to the effect of gliotoxin. The NOTCH1 target gene MYC was downregulated by RO4929097 ( Figure 5 B, right panel) [ 9 , 43 , 44 , 45 ].…”

Section: Resultsmentioning

confidence: 99%

“…Therefore, compounds that interfere with B-cell activation might affect the expression of both NOTCH receptors in CLL cells. This would explain why CLL cells pre-treated with Duvelisib (a dual PI3K-δ/γ inhibitor) [69] or Ibrutinib (a Bruton's tyrosine kinase inhibitor) [2,44] express lower amounts of CD23 and NOTCH3 and are less sensitive to apoptosis.…”

Section: Discussionmentioning

confidence: 99%

“…NOTCH1 is not detectable in nuclear NOTCH/CSL transcription factor complexes in CLL cells [ 7 , 8 , 18 , 32 ]. However, NOTCH1 is frequently mutated and/or overexpressed in advanced stage CLL cells, where it has a CLL-driving role by regulating MYC expression [ 8 , 9 , 16 , 17 , 43 , 44 , 45 ]. In this context, NOTCH1 may indirectly account for the relative GSI sensitivity of NOTCH2, keeping in mind that active NOTCH1 is a positive regulator of the NOTCH2 gene in CLL cells ( Figure 5 G) [ 12 ].…”

Section: Discussionmentioning

confidence: 99%

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Targeting Nuclear NOTCH2 by Gliotoxin Recovers a Tumor-Suppressor NOTCH3 Activity in CLL

Hubmann

Schnabl

Araghi

et al. 2020

Cells

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NOTCH signaling represents a promising therapeutic target in chronic lymphocytic leukemia (CLL). We compared the anti-neoplastic effects of the nuclear NOTCH2 inhibitor gliotoxin and the pan-NOTCH γ-secretase inhibitor RO4929097 in primary CLL cells with special emphasis on the individual roles of the different NOTCH receptors. Gliotoxin rapidly induced apoptosis in all CLL cases tested, whereas RO4929097 exerted a variable and delayed effect on CLL cell viability. Gliotoxin-induced apoptosis was associated with inhibition of the NOTCH2/FCER2 (CD23) axis together with concomitant upregulation of the NOTCH3/NR4A1 axis. In contrast, RO4929097 downregulated the NOTCH3/NR4A1 axis and counteracted the spontaneous and gliotoxin-induced apoptosis. On the cell surface, NOTCH3 and CD23 expression were mutually exclusive, suggesting that downregulation of NOTCH2 signaling is a prerequisite for NOTCH3 expression in CLL cells. ATAC-seq confirmed that gliotoxin targeted the canonical NOTCH signaling, as indicated by the loss of chromatin accessibility at the potential NOTCH/CSL site containing the gene regulatory elements. This was accompanied by a gain in accessibility at the NR4A1, NFκB, and ATF3 motifs close to the genes involved in B-cell activation, differentiation, and apoptosis. In summary, these data show that gliotoxin recovers a non-canonical tumor-suppressing NOTCH3 activity, indicating that nuclear NOTCH2 inhibitors might be beneficial compared to pan-NOTCH inhibitors in the treatment of CLL.

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Decreased NOTCH1 Activation Correlates with Response to Ibrutinib in Chronic Lymphocytic Leukemia

Cited by 24 publications

References 59 publications

High-grade heart block associated with ibrutinib therapy

High-grade heart block associated with ibrutinib therapy

NOTCH1 Activation Negatively Impacts on Chronic Lymphocytic Leukemia Outcome and Is Not Correlated to the NOTCH1 and IGHV Mutational Status

Targeting Nuclear NOTCH2 by Gliotoxin Recovers a Tumor-Suppressor NOTCH3 Activity in CLL

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