Paul Dalhaimer scite author profile

Interaction of spherical particles with cells and within animals has been studied extensively, but the effects of shape have received little attention. Here we use highly stable, polymer micelle assemblies known as filomicelles to compare the transport and trafficking of flexible filaments with spheres of similar chemistry. In rodents, filomicelles persisted in the circulation up to one week after intravenous injection. This is about ten times longer than their spherical counterparts and is more persistent than any known synthetic nanoparticle. Under fluid flow conditions, spheres and short filomicelles are taken up by cells more readily than longer filaments because the latter are extended by the flow. Preliminary results further demonstrate that filomicelles can effectively deliver the anticancer drug paclitaxel and shrink human-derived tumours in mice. Although these findings show that long-circulating vehicles need not be nanospheres, they also lend insight into possible shape effects of natural filamentous viruses.

show abstract

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)¹

Klionsky

et al. 2021

View full text Add to dashboard Cite

Cooperativity in Forced Unfolding of Tandem Spectrin Repeats

Law

Carl

Harper

et al. 2003

Biophysical Journal

158

198

View full text Add to dashboard Cite

Force-driven conformational changes provide a broad basis for protein extensibility, and multidomain proteins broaden the possibilities further by allowing for a multiplicity of forcibly extended states. Red cell spectrin is prototypical in being an extensible, multidomain protein widely recognized for its contribution to erythrocyte flexibility. Atomic force microscopy has already shown that single repeats of various spectrin family proteins can be forced to unfold reversibly under extension. Recent structural data indicates, however, that the linker between triple-helical spectrin repeats is often a contiguous helix, thus raising questions as to what the linker contributes and what defines a domain mechanically. We have examined the extensible unfolding of red cell spectrins as monomeric constructs of just two, three, or four repeats from the actin-binding ends of both alpha- and beta-chains, i.e., alpha(18-21) and beta(1-4) or their subfragments. In addition to single repeat unfolding evident in sawtooth patterns peaked at relatively low forces (<50 pN at 1 nm/ms extension rates), tandem repeat unfolding is also demonstrated in ensemble-scale analyses of thousands of atomic force microscopy contacts. Evidence for extending two chains and loops is provided by force versus length scatterplots which also indicate that tandem repeat unfolding occurs at a significant frequency relative to single repeat unfolding. Cooperativity in forced unfolding of spectrin is also clearly demonstrated by a common force scale for the unfolding of both single and tandem repeats.

show abstract

Single Molecule Visualization of Stable, Stiffness-Tunable, Flow-Conforming Worm Micelles

2003

View full text Add to dashboard Cite

We describe fluorescence visualization of highly stable worm micelle superpolymers. The worm micelles are self-assembled in water from nonionic, block copolymer amphiphiles. By blending and polymerizing inert and cross-linkable copolymers, we form micelles up to tens of microns long with persistence lengths that continuously span more than 2 orders of magnitude from submicron to submillimeter. In flow, pristine worms orient and stretch with DNA-like scaling, and their stability, loading capacity, and stealthiness make them ideal candidates for flow-intensive delivery applications such as phage-mimetic drug carriers and micropore delivery.

show abstract

Polymeric worm micelles as nano-carriers for drug delivery

Kim¹,

Dalhaimer²,

Christian³

et al. 2005

Nanotechnology

200

137

View full text Add to dashboard Cite

Nanoscale carriers of active compounds, especially drugs, need not be spherical in shape. Worm micelles as blends of degradable polylactic acid (PLA) and inert block copolymer amphiphiles were prepared for controlled release and initial study of carrier transport through nano-porous media. The loading capacity of a typical hydrophobic drug, Triamterene, and the release of hydrophobic dyes were evaluated together with morphological changes of the micelles. Degradation of PLA by hydrolysis led to the self-shortening of worms and a clear transition towards spherical micelles, correlating with the release of hydrophobic dyes. Perhaps equally important for application is the flexibility of worm micelles, which we show allows them to penetrate nanoporous gels where 100 nm sized vesicles cannot enter. Such gels have served as tissue models, and so the results here collectively suggest a new class of hydrophobic drug nano-carriers that are capable of tissue permeation as well as controlled release.

show abstract

Targeted Worm Micelles

et al. 2004

View full text Add to dashboard Cite

Giant and stable worm micelles formed from poly(ethylene glycol) (PEG)-based diblock copolymer amphiphiles have the potential advantage compared to smaller assemblies for delivery of a large quantity of hydrophobic drugs or dyes per carrier. Here we show that worm micelles can be targeted to cells with internalization and delivery of nontoxic dyes as well as cytotoxic drugs. Constituent copolymers are end-biotinylated to mediate high affinity binding of worm micelles to both avidin-bearing surfaces and biotin-specific receptors on smooth muscle cells. Pristine worm micelles, that lack biotin, show much less frequent and nonspecific point attachments to the same surfaces. Biotinylated worm micelles prove stable in aqueous solution for at least a month and also prove capable of loading, retaining, and delivering hydrophobic dyes and drugs. The results thus demonstrate the feasibility of targeted delivery by polymeric worm micelles.

show abstract

Nucleotide-Mediated Conformational Changes of Monomeric Actin and Arp3 Studied by Molecular Dynamics Simulations

Dalhaimer

Pollard

Nolen

2008

Journal of Molecular Biology

View full text Add to dashboard Cite

Members of the actin family of proteins exhibit different biochemical properties when ATP, ADP-P i , ADP, or no nucleotide is bound. We used molecular dynamics simulations to study the effect of nucleotides on the behavior of actin and actin-related protein 3 (Arp3). In all of the actin simulations, the nucleotide cleft stayed closed, as in most crystal structures. ADP was much more mobile within the cleft than ATP, despite the fact that both nucleotides adopt identical conformations in actin crystal structures. The nucleotide cleft of Arp3 opened in most simulations with ATP, ADP, and no bound nucleotide. Deletion of a C-terminal region of Arp3 that extends beyond the conserved actin sequence reduced the tendency of the Arp3 cleft to open. When the Arp3 cleft opened, we observed multiple instances of partial release of the nucleotide. Cleft opening in Arp3 also allowed us to observe correlated movements of the phosphate clamp, cleft mouth, and barbed-end groove, providing a way for changes in the nucleotide state to be relayed to other parts of Arp3. The DNase binding loop of actin was highly flexible regardless of the nucleotide state. The conformation of Ser14/Thr14 in the P1 loop was sensitive to the presence of the γ-phosphate, but other changes observed in crystal structures were not correlated with the nucleotide state on nanosecond timescales. The divalent cation occupied three positions in the nucleotide cleft, one of which was not previously observed in actin or Arp2/3 complex structures. In sum, these simulations show that subtle differences in structures of actin family proteins have profound effects on their nucleotide-driven behavior.

show abstract

Biopolymer mimicry with polymeric wormlike micelles: Molecular weight scaled flexibility, locked‐in curvature, and coexisting microphases

Dalhaimer

Bermudez

Discher

2003

J Polym Sci B Polym Phys

View full text Add to dashboard Cite

Giant and stable wormlike micelles formed in water from a series of poly(ethylene oxide) (PEO)‐based diblock copolymer amphiphiles mimicked the flexibility of various cytoskeletal filaments. The worm diameter (d) was found by cryo‐transmission electron microscopy to scale with the length of the hydrophobic chain (Nh) of the copolymer as d ∼ Nh0.61. By fluorescence video imaging of worm dynamics, we also showed that the persistence length (lP) of wormlike micelles scaled as lP ∼ d2.8, consistent with a fluid aggregate (∼d3) rather than a solid rod (∼d4). By polymerizing the unsaturated bonds of assembled copolymers, fluid worms were converted to solid‐core worms, extending the bending rigidity from that of intermediate filament biopolymers to actin filaments and, in principle, microtubules. Through partial crosslinking, polymerized worms further locked in spontaneous curvature at a novel fluid‐to‐solid percolation point. The dynamics of distinct, branched conformations were also imaged for recently discovered Y‐junctioned wormlike micelles composed of diblocks of high molecular weight (>10–15 kg/mol). Finally, block copolymers of hydrophilic weight fraction close to the transition between a vesicle‐ and worm‐former assembled into both structures, allowing encapsulation of wormlike micelles in giant vesicles reminiscent of cytoskeletal filaments enclosed within cells. © 2003 Wiley Periodicals, Inc. J Polym Sci Part B: Polym Phys 42: 168–176, 2004

show abstract

12 3 4 5 6

scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.

Contact Info

hi@scite.ai

10624 S. Eastern Ave., Ste. A-614

Henderson, NV 89052, USA

Blog Terms and Conditions API Terms Privacy Policy Contact Cookie Preferences Do Not Sell or Share My Personal Information

Made with 💙 for researchers

Part of the Research Solutions Family.

Paul Dalhaimer

Shape effects of filaments versus spherical particles in flow and drug delivery

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)¹

Cooperativity in Forced Unfolding of Tandem Spectrin Repeats

Single Molecule Visualization of Stable, Stiffness-Tunable, Flow-Conforming Worm Micelles

Polymeric worm micelles as nano-carriers for drug delivery

Targeted Worm Micelles

Nucleotide-Mediated Conformational Changes of Monomeric Actin and Arp3 Studied by Molecular Dynamics Simulations

Biopolymer mimicry with polymeric wormlike micelles: Molecular weight scaled flexibility, locked‐in curvature, and coexisting microphases

Contact Info

Product

Resources

About

Paul Dalhaimer

Shape effects of filaments versus spherical particles in flow and drug delivery

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)1

Cooperativity in Forced Unfolding of Tandem Spectrin Repeats

Single Molecule Visualization of Stable, Stiffness-Tunable, Flow-Conforming Worm Micelles

Polymeric worm micelles as nano-carriers for drug delivery

Targeted Worm Micelles

Nucleotide-Mediated Conformational Changes of Monomeric Actin and Arp3 Studied by Molecular Dynamics Simulations

Biopolymer mimicry with polymeric wormlike micelles: Molecular weight scaled flexibility, locked‐in curvature, and coexisting microphases

Contact Info

Product

Resources

About

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)¹