Inhibition of bromodomain and extra‐terminal proteins increases sensitivity to venetoclax in chronic lymphocytic leukaemia

Carrà, Giovanna; Nicoli, Paolo; Lingua, Marcello Francesco; Maffeo, Beatrice; Cartellà, Antonio; Circosta, Paola; Brancaccio, Mara; Parvis, Guido; Gaidano, Valentina; Guerrasio, Angelo; Saglio, Giuseppe; Taulli, Riccardo; Morotti, Alessandro

doi:10.1111/jcmm.14857

Cited by 16 publications

(11 citation statements)

References 28 publications

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“…Similarly, we found that MEC1 or MEC1-ROR1 cells transfected to express high levels of BCL2 WT , BCL2 A113P , or BCL2 G101V also had reduced sensitivity to venetoclax compared to the parent MEC1 or MEC1-ROR1 cells. Despite the noted resistance of MEC1 cells to venetoclax [ 45 ], we still found that MEC1-ROR1 were even less sensitive to this drug, indicating that the expression of ROR1 per se can enhance drug resistance.…”

Section: Discussioncontrasting

confidence: 56%

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High expression level of ROR1 and ROR1-signaling associates with venetoclax resistance in chronic lymphocytic leukemia

et al. 2022

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Although the BH3-mimetic venetoclax is highly cytotoxic for chronic lymphocytic leukemia (CLL) cells, some patients with CLL fail to clear minimal residual disease (MRD). We examined the CLL cells of seven such patients (CLL1-7) and found each had high-level expression of ROR1. By examining the CLL cells from such patients prior to therapy at SC1 and then more than 1 year later (Sample Collection 2 (SC2)), when they had progressive increases in MRD despite continued venetoclax therapy, we found the levels of ROR1 expressed on CLL cells at SC2 were significantly higher than that on CLL cells collected at SC1. At SC2, we also observed upregulation of genes induced by Wnt5a-induced ROR1 signaling, including BCL2L1. Transduction of the CLL-cell-line MEC1 to express ROR1 enhanced expression of target genes induced by ROR1-signaling, increased expression of BCL-XL, and enhanced resistance to venetoclax, even in MEC1 made to express mutant forms of BCL2, which are associated with venetoclax resistance. Treatment of primary CLL cells with Wnt5a also increased their resistance to venetoclax, an effect that could be inhibited by the anti-ROR1 mAb (UC-961, zilovertamab). Collectively, these studies indicate that Wnt5a-induced ROR1-signaling can enhance resistance to venetoclax therapy.

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Section: Discussioncontrasting

confidence: 56%

“…MEC1 leukemia cells already are relatively resistant to venetoclax compared to the primary leukemia cells of patients with CLL [ 45 ]. Nonetheless, we examined whether the expression of ROR1 could enhance the resistance of this cell line to venetoclax in vitro.…”

Section: Resultsmentioning

confidence: 99%

High expression level of ROR1 and ROR1-signaling associates with venetoclax resistance in chronic lymphocytic leukemia

et al. 2022

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“…Indeed, a wide range of BETi have now been tested together with various BH3-mimetics, though most studies have focussed on Venetoclax where enhanced responses from combining the drugs have been seen in vitro and in vivo in many haematological malignancies including T cell lymphoma, CLL, T cell acute lymphoblastic leukaemia, and diffuse large B cell lymphoma [ 289 , 290 , 291 , 292 , 293 , 294 , 295 , 296 , 297 ], and some solid tumours such as small cell lung cancer [ 298 ]. The dual BCL-XL/BCL-2 inhibitor Navitoclax was also shown to synergise with BETi in small cell lung cancer, colorectal cancer, glioma and B-cell lymphomas [ 299 , 300 , 301 , 302 ], whilst BH3-mimetics targeting MCL-1 enhance BETi activity in AML and melanoma [ 292 , 303 ].…”

Section: Therapeutic Strategies Targeting Bcl-2 and Mycmentioning

confidence: 99%

Co-Operativity between MYC and BCL-2 Pro-Survival Proteins in Cancer

Fairlie

Lee

2021

IJMS

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B-Cell Lymphoma 2 (BCL-2), c-MYC and related proteins are arguably amongst the most widely studied in all of biology. Every year there are thousands of papers reporting on different aspects of their biochemistry, cellular and physiological mechanisms and functions. This plethora of literature can be attributed to both proteins playing essential roles in the normal functioning of a cell, and by extension a whole organism, but also due to their central role in disease, most notably, cancer. Many cancers arise due to genetic lesions resulting in deregulation of both proteins, and indeed the development and survival of tumours is often dependent on co-operativity between these protein families. In this review we will discuss the individual roles of both proteins in cancer, describe cancers where co-operativity between them has been well-characterised and finally, some strategies to target these proteins therapeutically.

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“…Despite the remarkable preclinical activity of BET inhibitors in hematological malignancies, studies to identify beneficial combination therapy approaches to enhance efficacy have been reported [31]. As expected, synergism was observed when combining BET inhibitors (e.g., BAY 1238097, GS-5829, OTX015) with inhibitors of BTK (ibrutinib), SYK (entospletinib), PI3K (copanlisib, idelalisib), or BCL2 (venetoclax) in preclinical models of CLL [32][33][34] and DLBCL-RT [35]. Interestingly, the anti-leukemic activity of BET inhibitor, GS-5829, proved to be synergistic in combination with ibrutinib or idelalisib in primary CLL / nurse-like cell co-cultures reflective of the LN TME in CLL [32].…”

Section: Introductionmentioning

confidence: 90%

A novel triple-action inhibitor targeting B-cell receptor signaling and BRD4 demonstrates preclinical activity in chronic lymphocytic leukemia

Smith

Eiken

Moore

et al. 2022

Preprint

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B-cell chronic lymphocytic leukemia (CLL) results from intrinsic genetic defects and complex microenvironment stimuli that fuel CLL cell growth through an array of survival-signaling pathways. Novel small-molecule agents targeting the B-cell receptor pathway and anti-apoptotic proteins alone or in combination have revolutionized the management of CLL, yet combination therapy carries significant toxicity and CLL still remains an incurable disease due to residual disease and relapse. Single-molecule inhibitors that can target multiple disease-driving factors are thus an attractive approach to combat both drug resistance and combination therapy-related toxicities. Using SRX3305, a novel small-molecule BTK/PI3K/BRD4 inhibitor that targets three distinctive facets of CLL biology, we demonstrate that SRX3305 attenuates CLL cell proliferation and promotes apoptosis in a dose-dependent fashion. SRX3305 also inhibits activation-induced proliferation of primary CLL cells in vitro, and effectively blocks microenvironment-mediated survival signals including stromal cell contact. Furthermore, SRX3305 blocks CLL cell migration toward CXCL-12 and CXCL-13, major chemokines involved in CLL cell homing and retention in microenvironment niches. Importantly, SRX3305 maintains its anti-tumor effects in ibrutinib-resistant CLL cells. Collectively, this study establishes the preclinical efficacy of SRX3305 in CLL providing significant rationale for its development as a therapeutic agent for CLL and related disorders.

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Inhibition of bromodomain and extra‐terminal proteins increases sensitivity to venetoclax in chronic lymphocytic leukaemia

Cited by 16 publications

References 28 publications

High expression level of ROR1 and ROR1-signaling associates with venetoclax resistance in chronic lymphocytic leukemia

High expression level of ROR1 and ROR1-signaling associates with venetoclax resistance in chronic lymphocytic leukemia

Co-Operativity between MYC and BCL-2 Pro-Survival Proteins in Cancer

A novel triple-action inhibitor targeting B-cell receptor signaling and BRD4 demonstrates preclinical activity in chronic lymphocytic leukemia

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