Structure Based Design of Non-Natural Peptidic Macrocyclic Mcl-1 Inhibitors

Johannes, Jeffrey W.; Bates, Stephanie M.; Beigie, Carl; Belmonte, Matthew A.; Breen, John; Cao, Shenggen; Centrella, Paolo A.; Clark, Matthew; Cuozzo, John W.; Dumelin, Christoph E.; Ferguson, Andrew D.; Habeshian, Sevan; Hargreaves, David; Joubran, Camil; Kazmirski, Steven L.; Keefe, Anthony D.; Lamb, Michelle L.; Lan, Haiye; Li, Yunxia; Ma, Hao; Mlynarski, Scott N.; Packer, Martin J.; Rawlins, Philip; Robbins, Daniel W.; Shen, Haidong; Sigel, Eric A.; Soutter, Holly H.; Su, Nancy; Troast, Dawn M.; Wang, Haiyun; Wickson, Kate; Wu, Chengyan; Zhang, Ying; Zhao, Qiuying; Zheng, Xiaolan; Hird, Alexander W.

doi:10.1021/acsmedchemlett.6b00464

Cited by 53 publications

(53 citation statements)

References 20 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These findings may have clinical relevance in that certain TNBCs overexpressing MCL-1 and BCL2A1 could exhibit resistance to MCL-1 inhibitors that are under development. 38 – 40 In this context, we found that BT-20/ABT-737R cells, which overexpress MCL-1 and BCL2A1, were sensitive to targeting MCL-1 with MS1/NPs. By contrast, MDA-MB-468/ABT-737R cells, which also overexpress MCL-1 and BCL2A1, were resistant to targeting MCL-1.…”

Section: Discussionmentioning

confidence: 95%

Targeting MUC1-C suppresses BCL2A1 in triple-negative breast cancer

Hiraki

Maeda

Mehrotra

et al. 2018

Sig Transduct Target Ther

View full text Add to dashboard Cite

B-cell lymphoma 2-related protein A1 (BCL2A1) is a member of the BCL-2 family of anti-apoptotic proteins that confers resistance to treatment with anti-cancer drugs; however, there are presently no agents that target BCL2A1. The MUC1-C oncoprotein is aberrantly expressed in triple-negative breast cancer (TNBC) cells, induces the epithelial–mesenchymal transition (EMT) and promotes anti-cancer drug resistance. The present study demonstrates that targeting MUC1-C genetically and pharmacologically in TNBC cells results in the downregulation of BCL2A1 expression. The results show that MUC1-C activates the BCL2A1 gene by an NF-κB p65-mediated mechanism, linking this pathway with the induction of EMT. The MCL-1 anti-apoptotic protein is also of importance for the survival of TNBC cells and is an attractive target for drug development. We found that inhibiting MCL-1 with the highly specific MS1 peptide results in the activation of the MUC1-C→NF-κB→BCL2A1 pathway. In addition, selection of TNBC cells for resistance to ABT-737, which inhibits BCL-2, BCL-xL and BCL-W but not MCL-1 or BCL2A1, is associated with the upregulation of MUC1-C and BCL2A1 expression. Targeting MUC1-C in ABT-737-resistant TNBC cells suppresses BCL2A1 and induces death, which is of potential therapeutic importance. These findings indicate that MUC1-C is a target for the treatment of TNBCs unresponsive to agents that inhibit anti-apoptotic members of the BCL-2 family.

show abstract

Section: Discussionmentioning

confidence: 95%

Targeting MUC1-C suppresses BCL2A1 in triple-negative breast cancer

Hiraki

Maeda

Mehrotra

et al. 2018

Sig Transduct Target Ther

View full text Add to dashboard Cite

show abstract

“…These compounds, however, show poor aqueous solubility and cell permeability and therefore will require further optimization (Rosenthal et al, 2013) In addition to peptidomemetics, macrocyles have shown promise in providing a distinct solution to the problem effectively competing with macromolecular-macromolecular interactions. Johannes and colleagues (Johannes et al, 2017) recently employed a DNA-encoded library of non-natural peptides in a screening campaign against Mcl-1, a pro-apoptotic protein. Importantly, structures of the initial hits allowed the researchers to link the terminal ends of the ligand, to form a macrocylic analog, which led to a binding enhancement of more than an order of magnitude.…”

Section: Challenges In Developing Inhibitors/modulators Of Dna Repairmentioning

confidence: 99%

Small-Molecule Inhibitors Targeting DNA Repair and DNA Repair Deficiency in Research and Cancer Therapy

Hengel

Spies

2017

Cell Chemical Biology

114

123

View full text Add to dashboard Cite

To maintain stable genomes and to avoid cancer and aging, cells need to repair a multitude of deleterious DNA lesions, which arise constantly in every cell. Processes that support genome integrity in normal cells, however, allow cancer cells to develop resistance to radiation and DNA damaging chemotherapeutics. Chemical inhibition of the key DNA repair proteins and pharmacologically induced synthetic lethality have become instrumental in both dissecting the complex DNA repair networks and as promising anticancer agents. The difficulty in capitalizing on synthetically lethal interactions in cancer cells is that many potential targets do not possess well-defined small molecule binding determinates. In this review we will discuss several successful campaigns to identify and leverage small-molecule inhibitors of the DNA repair proteins, from PARP1, a paradigm case for clinically successful small molecule inhibitors, to coveted new targets, such as RAD51 recombinase, RAD52 DNA repair protein, MRE11 nuclease and WRN DNA helicase.

show abstract

“…A range of recent structure-based drug discovery case studies demonstrate the power of nuclear magnetic resonance (NMR) conformational analysis to elucidate SAR trends with respect to conformational preferences of the free ligand [4][5][6][7][8][9][10][11][12][13][14]. In the majority of cases, knowledge of the free ligand conformational preference clearly aided structure-based design.…”

mentioning

confidence: 99%

“…If we combine this information with target affinity, we can often rationalize SAR which is independent of any specific ligand-protein interaction. A recent example was described by Johannes et al [4] in their design of macrocyclic inhibitors of MCL1. In this case they used knowledge of anomalous proton NMR chemical shifts caused by anisotropic shielding to understand that their most potent macrocycle, containing a methylated amide, had a conformational lock which biased it towards adopting the bioactive conformation in solution.…”

mentioning

confidence: 99%