The novel cereblon modulator CC-885 inhibits mitophagy via selective degradation of BNIP3L

Hao, Bingbing; Li, Xiaojing; Jia, Xinglong; Wang, Yuxing; Zhai, Linhui; Li, Duanzhuo; Liu, Jie; Zhang, Die; Chen, Yu-Lu; Xu, Yonghu; Lee, Sang‐Kyu; Xu, Guofeng; Chen, Xiaohua; Dang, Yongjun; Liu, Bin; Tan, Minjia

doi:10.1038/s41401-020-0367-9

Cited by 28 publications

(14 citation statements)

References 30 publications

(36 reference statements)

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“…The majority of the 51 compounds in the library exhibited no antiproliferative activity in either MM1.S wild-type (WT) or CRBN −/− up to a concentration of 20 μM. Seven compounds (8,25,36,42,43,44, and 47) had notable to slight antiproliferative activity in both cell lines (Table 1, Supplementary Figure S1). This indicated that these compounds have CRBN-independent cytotoxicity.…”

Section: ■ Results and Discussionmentioning

confidence: 99%

“…Screening for CRBN-dependent antiproliferative effects led to the identification of CRBN modulators that can induce the selective degradation of GSPT1. In contrast to CC-885, which induces degradation of GSPT1, IKZF1/3, and a large number of other proteins, 12,24,25 our tool compounds are highly selective GSPT1/2 degraders with little to no activity on IKZF1/3 and no observable offtarget activity in global proteomics. This is confirmed by our selective tool compounds exhibiting antiproliferative activity that is strictly dependent on the expression of CRBN, while CC-885 retains antiproliferative activity with unspecific toxicity in a CRBN −/− cell line (Figure 4D).…”

Section: ■ Conclusionmentioning

confidence: 88%

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Selective Degradation of GSPT1 by Cereblon Modulators Identified via a Focused Combinatorial Library

Powell

Che

et al. 2020

ACS Chem. Biol.

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Cereblon (CRBN) is an E3 ligase adapter protein that can be reprogrammed by imide-class compounds such as thalidomide, lenalidomide, and pomalidomide to induce the degradation of neo-substrate proteins. In order to identify additional small molecule CRBN modulators, we implemented a focused combinatorial library approach where we fused an imide-based CRBN-binding pharmacophore to a heterocyclic scaffold, which could be further elaborated. We screened the library for CRBN-dependent antiproliferative activity in the multiple myeloma cell line MM1.S and identified five hit compounds. Quantitative chemical proteomics of hit compounds revealed that they induced selective degradation of GSPT1, a translation termination factor that is currently being explored as a therapeutic target for the treatment of acute myeloid leukemia. Molecular docking studies with CRBN and GSPT1 followed by analogue synthesis identified a possible hydrogen bond interaction with the central pyrimidine ring as a molecular determinant of hit compounds’ selectivity. This study demonstrates that a focused combinatorial library design, phenotypic screening, and chemical proteomics can provide a suitable workflow to efficiently identify novel CRBN modulators.

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Section: ■ Results and Discussionmentioning

confidence: 99%

Section: ■ Conclusionmentioning

confidence: 88%

Selective Degradation of GSPT1 by Cereblon Modulators Identified via a Focused Combinatorial Library

Powell

Che

et al. 2020

ACS Chem. Biol.

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“…33 Another example showed that AML cells with BNIP3L deficiency were reported to be more sensitive to mitochondria-targeting drugs. 34 Furthermore, BNIP3L expression was also upregulated by decitabine in myeloid cells. 28 These studies will help incorporate BNIP3L into new therapeutic strategies for MM.…”

Section: Discussionmentioning

confidence: 99%

Expression and Clinical Significance of BCL2 Interacting Protein 3 Like in Multiple Myeloma

Chen

Dang

et al. 2021

Technol Cancer Res Treat

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Multiple myeloma (MM) is one of the main blood disorders threatening human health today. This study aimed to examine the expression of BCL-2/adenovirus E1B 19 kDa-interacting protein 3-like (BNIP3L) in patients with MM and explore its mechanisms in silico. Bone marrow samples (n = 36 from patients with MM and n = 12 from healthy donors) were used to conduct BNIP3L expression analysis using immunohistochemistry. Microarray or RNA sequencing data from the Sequence Read Archive, Gene Expression Omnibus, and ArrayExpress databases were used to appraise BNIP3L expression and its prognostic role in patients with MM. The co-expressed genes of BNIP3L were identified for enrichment and protein-protein interaction (PPI) analyses to determine the associated signaling pathways. Immunohistochemistry indicated that BNIP3L expression in bone marrow of patients with MM was significantly lower than that in bone marrow of healthy donors. BNIP3L mRNA expression was also significantly lower in patients with MM than in healthy donors. The overall standard mean difference (SMD) for downregulation of BNIP3L was −0.62 [−1.17, −0.06], and the area under the curve was 0.81 [0.78, 0.85] based on a total of 694 MM cases. The overall survival analysis demonstrated that BNIP3L levels could act as an independent protective indicator of MM patient survival (HR = 0.79). Moreover, 261 co-expressed genes of BNIP3L were confirmed and found to be mainly involved in the adipocytokine signaling pathway. We preliminarily proved that downregulation of BNIP3L may play an important role in the occurrence and development of MM, and the promoting cancer capacity may be related to the pathway of adipocytokine signaling pathway.

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“…Furthermore, a recent analysis based on mass-spectroscopy proteomics also identified dose- and time-dependent degradation of BNIP3L in CRBN +/+ , but not CRBN −/− cells exposed to CC-885 compound. That data uncover a novel role of CC-885 in regulating degradation of mitochondria (mitophagy) by targeting BNIP3L for CRL4 CRBN E3 ligase-dependent ubiquitination [ 83 ]. In MM cell lines, CC-885 selectively induced the ubiquitination and degradation of CDK4 in a CRBN-dependent manner, suggesting that CDK4 destruction contributed to its cytotoxicity in MM pre-clinical model [ 84 ].…”

Section: Cereblon E3 Ligase Modulators (Celmods)mentioning

confidence: 99%

CRL4CRBN E3 Ligase Complex as a Therapeutic Target in Multiple Myeloma

Barankiewicz

Salomon-Perzyński

Misiewicz-Krzemińska

et al. 2022

Cancers

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Multiple myeloma (MM) is the second most common hematological malignancy with a recurrent clinical course. The introduction of immunomodulatory drugs (IMiDs) was one of the milestones in MM therapy leading to a significant improvement in patients’ prognosis. Currently, IMiDs are the backbone of MM therapy in newly diagnosed and relapsed/refractory settings. It is now known that IMiDs exert their anti-myeloma activity mainly by binding cereblon (CRBN), the substrate receptor protein of the CRL4 E3 ubiquitin ligase (CRL4CRBN) complex. By binding CRBN, IMiDs alter its substrate specificity, leading to ubiquitination and proteasomal degradation of proteins essential for MM cell survival. Following the success of IMiDs, it is not surprising that the possibility of using the CRL4CRBN complex’s activity to treat MM is being further explored. In this review, we summarize the current state of knowledge about novel players in the MM therapeutic landscape, namely the CRBN E3 ligase modulators (CELMoDs), the next generation of IMiDs with broader biological activity. In addition, we discuss a new strategy of tailored proteolysis called proteolysis targeting chimeras (PROTACs) using the CRL4CRBN to degrade typically undruggable proteins, which may have relevance for the treatment of MM and other malignancies in the future.

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The novel cereblon modulator CC-885 inhibits mitophagy via selective degradation of BNIP3L

Cited by 28 publications

References 30 publications

Selective Degradation of GSPT1 by Cereblon Modulators Identified via a Focused Combinatorial Library

Selective Degradation of GSPT1 by Cereblon Modulators Identified via a Focused Combinatorial Library

Expression and Clinical Significance of BCL2 Interacting Protein 3 Like in Multiple Myeloma

CRL4CRBN E3 Ligase Complex as a Therapeutic Target in Multiple Myeloma

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