A Cell-Permeant Nanobody-Based Degrader That Induces Fetal Hemoglobin

Shen, Fangfang; Ge, Zheng; Setegne, Mekedlawit; Tenglin, Karin; Izadi, Manizheh; Xie, Henry; Zhai, Lu; Orkin, Stuart H.; Dassama, Laura M. K.

doi:10.1021/acscentsci.2c00998

Cited by 15 publications

(24 citation statements)

References 35 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We showed previously that the mini-protein ZF5.3 ,− is taken up by the endosomal pathway and released efficiently into the cytosol and nucleus of live cells, alone and when fused to certain protein cargos. Proteins successfully delivered using ZF5.3 include the self-labeling protein SNAP-tag, the metabolic enzyme argininosuccinate synthetase, the proximity labeling tool APEX2, and a nanobody-based degrader . These proteins differ in molecular weight, stoichiometry, isoelectric point, and the presence of bound cofactors.…”

Section: Introductionmentioning

confidence: 99%

Dose-Dependent Nuclear Delivery and Transcriptional Repression with a Cell-Penetrant MeCP2

et al. 2023

View full text Add to dashboard Cite

The vast majority of biologic-based therapeutics operate within serum, on the cell surface, or within endocytic vesicles, in large part because proteins and nucleic acids fail to efficiently cross cell or endosomal membranes. The impact of biologic-based therapeutics would expand exponentially if proteins and nucleic acids could reliably evade endosomal degradation, escape endosomal vesicles, and remain functional. Using the cell-permeant mini-protein ZF5.3, here we report the efficient nuclear delivery of functional Methyl-CpG-binding-protein 2 (MeCP2), a transcriptional regulator whose mutation causes Rett syndrome (RTT). We report that ZF-tMeCP2, a conjugate of ZF5.3 and MeCP2(Δaa13–71, 313–484), binds DNA in a methylation-dependent manner in vitro, and reaches the nucleus of model cell lines intact to achieve an average concentration of 700 nM. When delivered to live cells, ZF-tMeCP2 engages the NCoR/SMRT corepressor complex, selectively represses transcription from methylated promoters, and colocalizes with heterochromatin in mouse primary cortical neurons. We also report that efficient nuclear delivery of ZF-tMeCP2 relies on an endosomal escape portal provided by HOPS-dependent endosomal fusion. The Tat conjugate of MeCP2 (Tat-tMeCP2), evaluated for comparison, is degraded within the nucleus, is not selective for methylated promoters, and trafficks in a HOPS-independent manner. These results support the feasibility of a HOPS-dependent portal for delivering functional macromolecules to the cell interior using the cell-penetrant mini-protein ZF5.3. Such a strategy could broaden the impact of multiple families of biologic-based therapeutics.

show abstract

Section: Introductionmentioning

confidence: 99%

Dose-Dependent Nuclear Delivery and Transcriptional Repression with a Cell-Penetrant MeCP2

et al. 2023

View full text Add to dashboard Cite

show abstract

“…BCL11A subjugates HbF expression, thereby switching from fetal to adult hemoglobin expression during erythropoiesis [ 56 ]. Dassama et al (2022) developed a cell-permeant nanobody fused to a miniature protein and an E3 adaptor to form a degrader 21 ( Figure 18 ) [ 57 ]. This nanobody degrader 21 efficiently depleted cellular BCL11A in differentiated primary erythroid precursor cells.…”

Section: Discussionmentioning

confidence: 99%

Emerging Strategies in Proteolysis-Targeting Chimeras (PROTACs): Highlights from 2022

Tamatam

Shin

2023

IJMS

View full text Add to dashboard Cite

Targeted protein degradation (TPD) is a promising therapeutic modality that has garnered attention in academic, industrial, and pharmaceutical research for treating diseases such as cancer, neurodegenerative disorders, inflammation, and viral infections. In this context, proteolysis-targeting chimeras (PROTACs) present a reliable technology for degrading disease-causing proteins. PROTACs complement small-molecule inhibitors, which primarily rely on direct protein regulation. From concept-to-clinic, PROTACs have evolved from cell impermeable peptide molecules to orally bioavailable drugs. Despite their potential in medicinal chemistry, certain aspects regarding PROTACs remain unclear. The clinical significance of PROTACs is primarily limited owing to their lack of selectivity and drug-like properties. This review focused on recently reported PROTAC strategies, particularly in 2022. It aimed to address and overcome the challenges posed by classical PROTACs by correlating them with emerging approaches with improved selectivity and controllability, cell permeability, linker flexibility, druggability, and PROTAC-based approaches, developed in 2022. Furthermore, recently reported PROTAC-based approaches are discussed, highlighting each of their advantages and limitations. We predict that several improved PROTAC molecules will be accessible for treating patients exhibiting various conditions, including cancer, neurodegenerative disorders, inflammation, and viral infections.

show abstract

“…SEC-MALS was performed using an in-line Superdex 200 Increase 3.2/300 GL SEC column (Cytiva), as previously reported. [9,25] Proteins were separated at a flow rate of 0.15 mL/min at room temperature, and molecular masses were determined by the Astra6.1 software (Wyatt Technology).…”

Section: Size-exclusion Chromatography (Sec)-coupled Multi-angle Ligh...mentioning

confidence: 99%

“…His-tagged BstC, Tp0956, Es_TatT and Es_BstC were fluorescently labelled, as reported. [9,25] 4,4-dimethylsterol was extracted from M. capsulatus as previously described [9] while lanosterol (79630, Sigma-Aldrich), cholesterol (AAA1147018, Fisher Scientific), palmitic acid (P0500-10G, Sigma-Aldrich) and linoleic acid (L1376-5G, Sigma-Aldrich) were purchased. 50 nM of each labeled protein (diluted in assay buffer) was incubated with ligands (dissolved in 5 % DMSO) and loaded into Monolith NT.115 Capillaries (NanoTemper Technologies); MST measurements were performed and the data analyzed as reported previously.…”

Section: Microscale Thermophoresismentioning

confidence: 99%

See 1 more Smart Citation

Structures and Mechanisms of a Novel Bacterial Transport System for Fatty Acids

Zhai

Chou

et al. 2023

ChemBioChem

Self Cite

View full text Add to dashboard Cite

Bacterial acquisition of metabolites is largely facilitated by transporters with unique substrate scopes. The tripartite ATPindependent periplasmic (TRAP) transporters comprise a large family of bacterial proteins that facilitate the uptake of a variety of small molecules. It has been reported that some TRAP systems encode a fourth protein, the T component. The Tcomponent, or TatT, is predicted to be a periplasmic-facing lipoprotein that enables the uptake of metabolites from the outer membrane. However, no substrates were revealed for any TatT and their functional role(s) remained enigmatic. We recently identified a homolog in Methylococcus capsulatus that binds to sterols, and herein, we report two additional homologs that demonstrate a preference for long-chain fatty acids. Our bioinformatics, quantitative analyses of protein-ligand interactions, and high-resolution crystal structures suggest that TatTs might facilitate the trafficking of hydrophobic or lipophilic substrates and represent a new class of bacterial lipid and fatty acid transporters.

show abstract

A Cell-Permeant Nanobody-Based Degrader That Induces Fetal Hemoglobin

Cited by 15 publications

References 35 publications

Dose-Dependent Nuclear Delivery and Transcriptional Repression with a Cell-Penetrant MeCP2

Dose-Dependent Nuclear Delivery and Transcriptional Repression with a Cell-Penetrant MeCP2

Emerging Strategies in Proteolysis-Targeting Chimeras (PROTACs): Highlights from 2022

Structures and Mechanisms of a Novel Bacterial Transport System for Fatty Acids

Contact Info

Product

Resources

About