Structure-Guided Design of a Series of MCL-1 Inhibitors with High Affinity and Selectivity

Bruncko, Milan; Wang, Le; Sheppard, George S.; Phillips, Darren C.; Tahir, Stephen K.; Xue, John; Erickson, Scott; Fidanze, Steve; Fry, Elizabeth E.; Hasvold, Lisa; Jenkins, Gary J.; Jin, Sha; Judge, Russell A.; Kovar, Peter; Madar, David J.; Nimmer, Paul; Park, Chang; Petros, Andrew M.; Rosenberg, Saul H.; Smith, Morey L.; Song, Xiaohong; Sun, Chaohong; Tao, Zhi‐Fu; Wang, Xilu; Xiao, Yu; Zhang, Haichao; Tse, Chris; Leverson, Joel D.; Elmore, Steve W.; Souers, Andrew J.

doi:10.1021/jm501258m

Cited by 132 publications

(122 citation statements)

References 39 publications

Supporting

Mentioning

116

Contrasting

Unclassified

Order By: Relevance

“…Where indicated, cells were pretreated for 60 minutes with z-VADfmk (ICN). Navitoclax and A-1210477 were synthesized as described previously (28,29). Unless otherwise indicated, all chemical reagents were obtained from Sigma-Aldrich.…”

Section: Reagents Cell Culture and Treatmentmentioning

confidence: 99%

“…It is, therefore, of considerable therapeutic interest to inhibit the expression and/or function of MCL-1 in cancer and in particular, breast cancer. We recently described the synthesis of small molecules that selectively inhibit MCL-1 function (28). Here, we describe the identification of breast cancer cell lines that are addicted to the oncogene MCL-1, evaluate the mechanism of cell death resulting from selective loss of MCL-1 function, and discuss the consequences for breast cancer therapy.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

MCL-1 Is a Key Determinant of Breast Cancer Cell Survival: Validation of MCL-1 Dependency Utilizing a Highly Selective Small Molecule Inhibitor

Xiao

Nimmer

Sheppard

et al. 2015

Molecular Cancer Therapeutics

Self Cite

103

116

View full text Add to dashboard Cite

Hyperexpression of antiapoptotic BCL-2 family proteins allows cells to survive despite the receipt of signals that would ordinarily induce their deletion, a facet frequently exploited by tumors. Tumors addicted to the BCL-2 family proteins for survival are now being targeted therapeutically. For example, navitoclax, a BCL-2/ BCL-X L /BCL-W inhibitor, is currently in phase I/II clinical trials in numerous malignancies. However, the related family member, MCL-1, limits the efficacy of navitoclax and other chemotherapeutic agents. In the present study, we identify breast cancer cell lines that depend upon MCL-1 for survival and subsequently determine the mechanism of apoptosis mediated by the MCL-1 selective inhibitor A-1210477. We demonstrate that apoptosis resulting from a loss in MCL-1 function requires expression of the proapoptotic protein BAK. However, expression of BCL-X L can limit apoptosis resulting from loss in MCL-1 function through sequestration of free BIM. Finally, we demonstrate substantial synergy between navitoclax and MCL-1 siRNA, the direct MCL-1 inhibitor A-1210477, or the indirect MCL-1 inhibitor flavopiridol, highlighting the therapeutic potential for inhibiting BCL-X L and MCL-1 in breast cancer.

show abstract

Section: Reagents Cell Culture and Treatmentmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

MCL-1 Is a Key Determinant of Breast Cancer Cell Survival: Validation of MCL-1 Dependency Utilizing a Highly Selective Small Molecule Inhibitor

Xiao

Nimmer

Sheppard

et al. 2015

Molecular Cancer Therapeutics

Self Cite

103

116

View full text Add to dashboard Cite

show abstract

“…Despite the difficulties of this challenge, a series of MCL-1 inhibitors derived from indole-2-carboxilic acid has been obtained by high-throughput screening and structure-guided design. 37 The compounds bind to MCL-1 with excellent high affinity (0.45 nM) and selectivity over other prosurvival BCL-2 family proteins. A mechanistic study has shown that the lead compound A-1210477 and related analogs can disrupt the interactions of MCL-1 with BIM and NOXA, penetrate living cells, and act via an on-target mechanism.…”

Section: Discovery Of Novel Bh3 Mimeticsmentioning

confidence: 99%

Apoptosis as a Therapeutic Target in Chronic Lymphocytic Leukemia

Billard¹

2015

Lymphoma and Chronic Lymphocytic Leukemias

View full text Add to dashboard Cite

Despite significant advances in chemoimmunotherapy, chronic lymphocytic leukemia (CLL) is still incurable. This has prompted the development of new drugs and therapeutic strategies that include reactivating the impaired apoptosis (programed cell death). Several approaches to target apoptosis-regulating proteins have attracted attention. Among them, the approach to inhibit the activity of prosurvival members of the BCL-2 family with small-molecule BH3 mimetics (navitoclax, ABT-199) has proved to be most promising in clinical trials with CLL patients. Recently, the first BH3 mimetics targeting selectively the particular prosurvival protein MCL-1 (whose overexpression is involved in therapeutic resistance) have been identified. Furthermore, small molecules capable of directly activating proapoptotic proteins of the BCL-2 family have been characterized, indicating that novel BH3-mimetic drugs displaying this property may be designed. These discoveries are opening a new era in the development of BH3 mimetics for improving CLL therapy.

show abstract

“…Concerns over the Fmoc protecting group were considered, but as these compounds are primarily meant as chemical probes or potential leads, further development may discover more effective alternatives. Indeed, the Fmoc group is somewhat reminiscent of structural features present in Souers’ A‐121047716d and Fesik's 2‐indole‐acylsulfonamides,20 which are highly potent and selective Mcl‐1 binders. Interestingly, the most potent small molecules did not result from the combination of the most potent small‐molecule peptide hybrids 2 and 9 , as might be expected.…”

mentioning

confidence: 99%

“…Two compounds, 18 and 21 , were ineffective against AsPC‐1 cells at the concentrations evaluated in our assay, which may suggest that they are acting through the inhibition of Mcl‐1. The difference in the magnitude of activity in cells compared to the in vitro FA assay is a commonly observed phenomenon, and largely due to cell permeability 16d, 23. Indeed, some of the more potent compounds in the FA assay showed no activity in the cellular assays, such as compound 17 (IC 50 =102±14 n m ), suggesting an inability to cross the cell membrane.…”

mentioning

confidence: 99%

Peptide‐Directed Binding for the Discovery of Modulators of α‐Helix‐Mediated Protein–Protein Interactions: Proof‐of‐Concept Studies with the Apoptosis Regulator Mcl‐1

2017

View full text Add to dashboard Cite

Targeting PPIs with small molecules can be challenging owing to large, hydrophobic binding surfaces. Herein, we describe a strategy that exploits selective α‐helical PPIs, transferring these characteristics to small molecules. The proof of concept is demonstrated with the apoptosis regulator Mcl‐1, commonly exploited by cancers to avoid cell death. Peptide‐directed binding uses few synthetic transformations, requires the production of a small number of compounds, and generates a high percentage of hits. In this example, about 50 % of the small molecules prepared showed an IC50 value of less than 100 μm, and approximately 25 % had IC50 values below 1 μm to Mcl‐1. Compounds show selectivity for Mcl‐1 over other anti‐apoptotic proteins, possess cytotoxicity to cancer cell lines, and induce hallmarks of apoptosis. This approach represents a novel and economic process for the rapid discovery of new α‐helical PPI modulators.

show abstract

Structure-Guided Design of a Series of MCL-1 Inhibitors with High Affinity and Selectivity

Cited by 132 publications

References 39 publications

MCL-1 Is a Key Determinant of Breast Cancer Cell Survival: Validation of MCL-1 Dependency Utilizing a Highly Selective Small Molecule Inhibitor

MCL-1 Is a Key Determinant of Breast Cancer Cell Survival: Validation of MCL-1 Dependency Utilizing a Highly Selective Small Molecule Inhibitor

Apoptosis as a Therapeutic Target in Chronic Lymphocytic Leukemia

Peptide‐Directed Binding for the Discovery of Modulators of α‐Helix‐Mediated Protein–Protein Interactions: Proof‐of‐Concept Studies with the Apoptosis Regulator Mcl‐1

Contact Info

Product

Resources

About