Getting Across the Cell Membrane: An Overview for Small Molecules, Peptides, and Proteins

Yang, Nicole J.; Hinner, Marlon J.

doi:10.1007/978-1-4939-2272-7_3

Cited by 606 publications

(507 citation statements)

References 192 publications

Supporting

Mentioning

493

Contrasting

Unclassified

Order By: Relevance

“…Various factors could cause a lack of bioactivity including targeting of a nonfunctional site (binding has no downstream effect), inadequate cellular permeability, and compound localization to an undesired compartment. Chemotypes have been identified that improve cellular uptake,(70) including conjugation of polyarginine,(71) as well as those that influence localization. (72) Such data could be incorporated into a traditional medicinal chemistry approach or chemical similarity searching.…”

Section: Resultsmentioning

confidence: 99%

Inforna 2.0: A Platform for the Sequence-Based Design of Small Molecules Targeting Structured RNAs

et al. 2016

View full text Add to dashboard Cite

The development of small molecules that target RNA is challenging yet, if successful, could advance the development of chemical probes to study RNA function or precision therapeutics to treat RNA-mediated disease. Previously, we described Inforna, an approach that can mine motifs (secondary structures) within target RNAs, which is deduced from the RNA sequence, and compare them to a database of known RNA motif–small molecule binding partners. Output generated by Inforna includes the motif found in both the database and the desired RNA target, lead small molecules for that target, and other related meta-data. Lead small molecules can then be tested for binding and affecting cellular (dys)function. Herein, we describe Inforna 2.0, which incorporates all known RNA motif–small molecule binding partners reported in the scientific literature, a chemical similarity searching feature, and an improved user interface and is freely available via an online web server. By incorporation of interactions identified by other laboratories, the database has been doubled, containing 1936 RNA motif–small molecule interactions, including 244 unique small molecules and 1331 motifs. Interestingly, chemotype analysis of the compounds that bind RNA in the database reveals features in small molecule chemotypes that are privileged for binding. Further, this updated database expanded the number of cellular RNAs to which lead compounds can be identified.

show abstract

Section: Resultsmentioning

confidence: 99%

Inforna 2.0: A Platform for the Sequence-Based Design of Small Molecules Targeting Structured RNAs

et al. 2016

View full text Add to dashboard Cite

show abstract

“…[11] Given that many of the drug targets are localized in the subcellular compartments, an efficient translocation of the particles across the cell membrane is essential to attain desired therapeutic outcomes. [12] Endocytosis provides a means of cellular uptake of polymersomes that cannot enter the cells by passive diffusion. [13,14] Polymersomes initiate endocytosis by forming contacts with cell surface receptors.…”

Section: Controlling Polymersome Sizementioning

confidence: 99%

Engineering Polymersomes for Diagnostics and Therapy

Leong

Teo

Aakalu

et al. 2018

Adv Healthcare Materials

104

View full text Add to dashboard Cite

Engineered polymer vesicles, termed as polymersomes, confer a flexibility to control their structure, properties, and functionality. Self-assembly of amphiphilic copolymers leads to vesicles consisting of a hydrophobic bilayer membrane and hydrophilic core, each of which is loaded with a wide array of small and large molecules of interests. As such, polymersomes are increasingly being studied as carriers of imaging probes and therapeutic drugs. Effective delivery of polymersomes necessitates careful design of polymersomes. Therefore, this review article discusses the design strategies of polymersomes developed for enhanced transport and efficacy of imaging probes and therapeutic drugs. In particular, the article focuses on overviewing technologies to regulate the size, structure, shape, surface activity, and stimuli- responsiveness of polymersomes and discussing the extent to which these properties and structure of polymersomes influence the efficacy of cargo molecules. Taken together with future considerations, this article will serve to improve the controllability of polymersome functions and accelerate the use of polymersomes in biomedical applications.

show abstract

“…C 10 to C 12 ) result in improved selectivities for bacterial membranes hinting at an amphiphilic “sweet spot” that can be further leveraged by structural modifications enabled by organic synthesis. We are also interested in investigating whether some QACs simply permeabilize the membrane as opposed to fully lysing the cell, and if this varies by QAC architecture; such experiments are precedented [22] and represent a future direction for our groups.…”

mentioning

confidence: 99%

An Investigation into Rigidity–Activity Relationships in BisQAC Amphiphilic Antiseptics

et al. 2018

View full text Add to dashboard Cite

Twenty-one mono- and biscationic quaternary ammonium amphiphiles (monoQACs and bisQACs) were rapidly prepared in order to investigate the effects of rigidity of a diamine core structure on antiseptic activity. As anticipated, bioactivity against a panel of 6 bacteria including MRSA strains was strong for bisQAC structures, and clearly correlated to the length of non-polar side chains. Modest advantages were noted for amide-containing side chains, as compared to straight-chained alkyl substituents. Surprisingly, antiseptics with more rigidly disposed side chains, such as those in DABCO-12,12, showed the highest level of antimicrobial activity, with single-digit MIC values or better against the entire bacterial panel, including submicromolar activity against a MRSA strain.

show abstract

Getting Across the Cell Membrane: An Overview for Small Molecules, Peptides, and Proteins

Cited by 606 publications

References 192 publications

Inforna 2.0: A Platform for the Sequence-Based Design of Small Molecules Targeting Structured RNAs

Inforna 2.0: A Platform for the Sequence-Based Design of Small Molecules Targeting Structured RNAs

Engineering Polymersomes for Diagnostics and Therapy

An Investigation into Rigidity–Activity Relationships in BisQAC Amphiphilic Antiseptics

Contact Info

Product

Resources

About